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	<title>Adrenocortical Carcinoma</title>
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	<pubDate>Thu, 04 Dec 2008 12:23:52 +0000</pubDate>
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		<title>Adrenocortical carcinoma. An immunohistochemical comparison with renal cell carcinoma</title>
		<link>http://theadrenocorticalcarcinoma.com/2008/05/22/adrenocortical-carcinoma-an-immunohistochemical-comparison-with-renal-cell-carcinoma/</link>
		<comments>http://theadrenocorticalcarcinoma.com/2008/05/22/adrenocortical-carcinoma-an-immunohistochemical-comparison-with-renal-cell-carcinoma/#comments</comments>
		<pubDate>Thu, 22 May 2008 18:16:40 +0000</pubDate>
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		<category><![CDATA[Adrenocortical carcinoma. An immunohistochemical compar]]></category>

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		<description><![CDATA[MR Wick, DL Cherwitz, RC McGlennen and LP Dehner 
The diagnosis of adrenocortical carcinoma (ACC) is often difficult, because this tumor may present with direct extension into adjacent renal parenchyma or with metastatic disease. Renal cell carcinoma and other histologically similar tumors are potentially confused with ACC by conventional light microscopy, and their separation from [...]]]></description>
			<content:encoded><![CDATA[<p style="text-align: justify"><strong><span style="font-size: 10pt; color: black">MR Wick, DL Cherwitz, RC McGlennen and LP Dehner </span></strong><span style="font-size: 10pt; color: black"><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">The diagnosis of adrenocortical carcinoma (ACC) is often difficult, because<sup> </sup>this tumor may present with direct extension into adjacent renal parenchyma<sup> </sup>or with metastatic disease. Renal cell carcinoma and other histologically<sup> </sup>similar tumors are potentially confused with ACC by conventional light<sup> </sup>microscopy, and their separation from the latter is often impossible<sup> </sup>without the aid of additional studies. Furthermore, the distinction between<sup> </sup>adrenal cortical adenoma and ACC may also be problematic. Because of these<sup> </sup>factors, the authors studied 10 cases each of ACC, adrenocortical adenoma,<sup> </sup>and renal cell carcinoma (RCC) immunohistochemically, in an attempt to<sup> </sup>develop objective parameters which may aid in this differential diagnostic<sup> </sup>dilemma. Nontrypsinized, formalin-fixed, paraffin-embedded specimens were<sup> </sup>used in all cases, and tissue from the adrenocortical tumors was also<sup> </sup>studied for intermediate filament content after protease digestion. All 20<sup> </sup>nontrypsinized adrenocortical neoplasms were positive for vimentin, but not<sup> </sup>for cytokeratin, epithelial membrane antigen, or blood group isoantigens.<sup> </sup>Conversely, each of 10 cases of RCC expressed epithelial membrane antigen,<sup> </sup>cytokeratin, and blood group isoantigens, but none was immunoreactive for<sup> </sup>vimentin. Two adrenocortical carcinomas and three adenomas manifested<sup> </sup>cytokeratin positivity after trypsin digestion. There were no significant<sup> </sup>differences between the immunostaining profiles of ACC and adrenocortical<sup> </sup>adenoma, which suggest that this distinction must still rely upon clinical<sup> </sup>and morphologic criteria.<o:p></o:p></span></p>
</p>
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		<title>Adrenocortical Carcinoma - Description</title>
		<link>http://theadrenocorticalcarcinoma.com/2008/05/22/adrenocortical-carcinoma-description/</link>
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		<pubDate>Thu, 22 May 2008 18:15:20 +0000</pubDate>
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		<category><![CDATA[Adrenocortical Carcinoma - Description]]></category>

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		<description><![CDATA[What is cancer of the adrenal cortex? 
Cancer of the adrenal cortex, a rare cancer, is a disease in which cancer (malignant) cells are found in the adrenal cortex, which is the outside layer of the adrenal gland. Cancer of the adrenal cortex is also called adrenocortical carcinoma. There are two adrenal glands, one above [...]]]></description>
			<content:encoded><![CDATA[<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><strong><span style="font-size: 10pt; color: black" lang="EN">What is cancer of the adrenal cortex?</span></strong><span style="font-size: 10pt; color: black" lang="EN"> <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black" lang="EN">Cancer of the adrenal cortex, a rare cancer, is a disease in which cancer (malignant) cells are found in the adrenal cortex, which is the outside layer of the adrenal gland. Cancer of the adrenal cortex is also called adrenocortical carcinoma. There are two adrenal glands, one above each kidney in the back of the upper abdomen. The adrenal glands are also called the suprarenal glands. The inside layer of the adrenal gland is called the adrenal medulla. Cancer that starts in the adrenal medulla is called pheochromocytoma and is discussed in a separate PDQ patient information summary. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black" lang="EN">The cells in the adrenal cortex make important hormones that help the body work properly. When cells in the adrenal cortex become cancerous, they may make too much of one or more hormones, which can cause symptoms such as high blood pressure, weakening of the bones, or diabetes. If male or female hormones are affected, the body may go through changes such as a deepening of the voice, growing hair on the face, swelling of the sex organs, or swelling of the breasts. Cancers that make hormones are called functioning tumors. Many cancers of the adrenal cortex do not make extra hormones and are called nonfunctioning tumors. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black" lang="EN">A doctor should be seen if the following symptoms appear and won’t go away: <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black" lang="EN">If there are symptoms, a doctor will order blood and urine tests to see whether the amounts of hormones in the body are normal. A doctor may also order a computed tomography scan of the abdomen, a special x-ray that uses a computer to make a picture of the inside of the abdomen. Other special x-rays may also be done to tell what kind of tumor is present. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black" lang="EN">The chance of recovery (prognosis) depends on how far the cancer has spread (stage) and on whether a doctor was able to surgically remove all of the cancer<o:p></o:p></span></p>
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		<title>Abstract</title>
		<link>http://theadrenocorticalcarcinoma.com/2008/05/22/abstract-2/</link>
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		<pubDate>Thu, 22 May 2008 18:14:55 +0000</pubDate>
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		<category><![CDATA[Abstract -1]]></category>

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		<description><![CDATA[A 43-year-old female patient underwent abdominal ultrasonography and CT scan because of uncharacteristic abdominal pain. A 3-cm homogeneous adrenal tumor was diagnosed. The endocrine tests revealed an adrenal preclinical Cushing&#8217;s syndrome (PCS). Due to the latent hormone excess we decided to operate on the adrenal tumor. Since the tumor was small, laparoscopic adrenalectomy was performed. [...]]]></description>
			<content:encoded><![CDATA[<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">A 43-year-old female patient underwent abdominal ultrasonography and CT scan because of uncharacteristic abdominal pain. A 3-cm homogeneous adrenal tumor was diagnosed. The endocrine tests revealed an adrenal preclinical Cushing&#8217;s syndrome (PCS). Due to the latent hormone excess we decided to operate on the adrenal tumor. Since the tumor was small, laparoscopic adrenalectomy was performed. Histological evaluation showed an adrenocortical tumor of undetermined nature. Four months later the patient presented with a metastasizing cortisol- and androgen-producing adrenocortical carcinoma (ACC). After pretreatment with ketoconazole to suppress the biosynthesis of adrenal steroids under substitution with hydrocortisone, we reduced the tumor load by surgery. Postoperatively we continued ketoconazole and started <em>o,p&#8217;</em>-dichlorodiphenyldichloroethane as well as chemotherapy with doxorubicin and suramin. However, the patient died from ACC 7 months after adrenalectomy. It is known from several reports that PCS may persist clinically silently or may progress to full-blown Cushing&#8217;s syndrome. This is the first time a malignant course of PCS is described. Independent of the initial therapeutic strategy of PCS, i.e. surgery or regular follow-up visits, we must be aware that also relatively small adrenal tumors can harbor malignancy.<o:p></o:p></span></p>
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		<title>Adrenocortical Carcinoma</title>
		<link>http://theadrenocorticalcarcinoma.com/2008/05/22/adrenocortical-carcinoma-4/</link>
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		<pubDate>Thu, 22 May 2008 18:14:41 +0000</pubDate>
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		<category><![CDATA[Adrenocortical Carcinoma -3]]></category>

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		<description><![CDATA[(ACC) is a cancer affecting the cortex, or outer layer, of the adrenal gland. It typically has a poor prognosis, partly because of the cancer and partly because it usually causes Cushing’s syndrome. With aggressive treatment, the five-year survival without recurrence of the disease is about 30%. About three percent of all cortical tumors are [...]]]></description>
			<content:encoded><![CDATA[<p style="text-align: justify"><span style="font-size: 10pt; color: black">(ACC) is a <a href="http://www.iscid.org/encyclopedia/Cancer"><span style="color: black; text-decoration: none">cancer</span></a> affecting the cortex, or outer layer, of the adrenal gland. It typically has a poor prognosis, partly because of the cancer and partly because it usually causes Cushing’s syndrome. With aggressive treatment, the five-year survival without recurrence of the disease is about 30%. About three percent of all cortical tumors are the malignant form of adrenocortical carcinoma.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">The adrenal glands are also called the suprarenal glands, and are located just behind each kidney (making it easy for the cancer to metastasize there). <a href="http://www.iscid.org/encyclopedia/The_Cell"><span style="color: black; text-decoration: none">The cell</span></a>s in the cortex produce <a href="http://www.iscid.org/encyclopedia/Cortisol"><span style="color: black; text-decoration: none">cortisol</span></a> and certain sex hormones like androgen. Symptoms of adrenocortical carcinoma may include abdominal pain, <a href="http://www.iscid.org/encyclopedia/Weight"><span style="color: black; text-decoration: none">weight</span></a> loss, and extreme weakness. Other, rarer symptoms include weak bones, diabetes, hirsutism (excess hair, esp. on the face), swelling of sex organs and breasts, and deeper voice.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Treatment for adrenocortical carcinoma involves a complete surgical excision of the cancer and sometimes the entire gland, as well as chemotherapy. Radiation therapy has been experimented with, but the results are unclear. While the cancer is still active, cortisol is heavily overproduced and may require suppression while the patient is waiting for surgery and chemotherapy.<o:p></o:p></span></p>
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		<title>THE ADRENOCORTICAL CARCINOMA</title>
		<link>http://theadrenocorticalcarcinoma.com/2008/05/22/the-adrenocortical-carcinoma-3/</link>
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		<pubDate>Thu, 22 May 2008 18:14:12 +0000</pubDate>
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		<category><![CDATA[THE ADRENOCORTICAL CARCINOMA -2]]></category>

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		<description><![CDATA[We present a case of aldosterone-secreting adrenocortical carcinoma with concomitant myelolipoma. To the best of our knowledge, this is the first such reported case. The patient was a 43-year-old man with severe hypertension. Clinical workup revealed an increased serum aldosterone level, hypokalemia, and metabolic alkalosis, and a left adrenal mass was found on computed tomography. [...]]]></description>
			<content:encoded><![CDATA[<p style="text-align: justify"><span style="font-size: 10pt; color: black">We present a case of aldosterone-secreting adrenocortical carcinoma with concomitant myelolipoma. To the best of our knowledge, this is the first such reported case. The patient was a 43-year-old man with severe hypertension. Clinical workup revealed an increased serum aldosterone level, hypokalemia, and metabolic alkalosis, and a left adrenal mass was found on computed tomography. The patient underwent a unilateral adrenalectomy, which led to improvement in blood pressure, the serum potassium level, and aldosterone concentration. The tumor weighed 70 g and measured 5.0 cm. On microscopic examination, we found necrosis, focal cytologic atypia, diffuse eosinophilic cells comprising more than 75% of the tumor, 5 to 7 mitotic figures per 50 high-power fields, rare atypical mitosis, and venous invasion. At the periphery of the tumor but within the capsule, microscopic areas of myelolipoma were seen. Ki-67 staining was positive in 20% of the tumor cells. Although rare, aldosterone-secreting carcinoma associated with myelolipoma should be included in the differential diagnosis of adrenal gland masses.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="s1"></a><span style="font-size: 10pt; color: black">Adrenocortical carcinoma is rare, with an annual incidence of about 1 case per million population,<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b1#i1543-2165-129-6-e144-b1"><sup><span style="color: black; text-decoration: none">1</span></sup></a> but it has a mortality rate of more than 50%.<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b2#i1543-2165-129-6-e144-b2"><sup><span style="color: black; text-decoration: none">2</span></sup></a> Aldosterone-secreting adrenocortical carcinomas are even rarer, accounting for only 2% to 7% of adrenocortical carcinomas in the largest series reported in the literature.<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b3#i1543-2165-129-6-e144-b3"><sup><span style="color: black; text-decoration: none">3</span></sup></a><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">Myelolipoma is a benign tumor that has been reported in association with adrenal hyperplasia, adrenocortical adenomas, ganglioneuroma,<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b4#i1543-2165-129-6-e144-b4"><sup><span style="color: black; text-decoration: none">4,</span></sup></a><a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b5#i1543-2165-129-6-e144-b5"><sup><span style="color: black; text-decoration: none">5</span></sup></a> pheochromocytoma,<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b5#i1543-2165-129-6-e144-b5"><sup><span style="color: black; text-decoration: none">5</span></sup></a> and corticomedullary mixed tumor.<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b6#i1543-2165-129-6-e144-b6"><sup><span style="color: black; text-decoration: none">6</span></sup></a> Only 4 cases of adrenocortical carcinoma with concomitant myelolipoma have been reported in the medical literature. To the best of our knowledge, myelolipoma associated with adrenocortical carcinoma and hyperaldosteronism has not been reported previously. Thus, we describe the first case of aldosterone-secreting adrenocortical carcinoma with a myelolipomatous component.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="s2"></a><strong><span style="font-size: 10pt; color: black">REPORT OF A CASE</span></strong><span style="font-size: 10pt; color: black"> <o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="r2a"></a><strong><span style="font-size: 10pt; color: black">Clinical History</span></strong><span style="font-size: 10pt; color: black"><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">A 43-year-old obese man (body weight, 107.8 kg; height, 1.73 m) with a family history of hypertension presented at our emergency room with vertigo in December 2003. Severe hypertension (206/110 mm Hg) was subsequently diagnosed with laboratory study results consistent with hyperaldosteronism (serum aldosterone, 26.6 ng/dL; normal, 1–21 ng/dL), hypokalemia (potassium, 3.1 mEq/L; normal, 3.6–4.8 mEq/L), and metabolic alkalosis (bicarbonate, 38 mEq/L; normal, 22–29 mEq/L). The levels of other cortical hormones and their metabolites were within normal limits. The results of pheochromocytoma workup were negative.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">Abdominal magnetic resonance imaging revealed a 4.3-cm nodular mass in the left adrenal gland. Computed tomography of the abdomen revealed a 4.5 × 4.2-cm nodular mass of mixed heterogeneity . The patient underwent an uneventful unilateral adrenalectomy in February 2004 with substantial improvements in blood pressure (143/91 mm Hg) and serum potassium and aldosterone concentrations. He was discharged several days later with triamterene, potassium chloride, and clonidine. No recurrence or metastasis was noted at the most recent follow-up visit in late May 2004. He had negative computed tomography findings and blood pressure of 143/84 mm Hg.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="s3"></a><strong><span style="font-size: 10pt; color: black">PATHOLOGIC FINDINGS</span></strong><span style="font-size: 10pt; color: black"> <o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="s3a"></a><strong><span style="font-size: 10pt; color: black">Gross Features</span></strong><span style="font-size: 10pt; color: black"><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">The left adrenal gland weighed 70 g and measured 5.0 × 4.4 × 4.0 cm. The adrenal gland was almost totally replaced by a well-encapsulated bosselated tumor. A small portion of compressed nonneoplastic adrenal gland was seen on the surface. The cut surface of the tumor was multinodular, yellow, and soft with extensive areas of hemorrhage and necrosis .<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="s3b"></a><strong><span style="font-size: 10pt; color: black">Microscopic Features</span></strong><span style="font-size: 10pt; color: black"><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">On microscopic examination, the tumor was entirely encapsulated by a fibrous capsule of variable thickness. The cells were arranged in a sheetlike or trabecular pattern separated by relatively thick fibrous bands. The tumor was composed of mostly (&gt;75%) round eosinophilic (compact) cells, with scattered foci of clear cells. There were extensive areas of hemorrhage, focal areas of necrosis, and areas of marked cytologic atypia with giant cells that had large, irregular, hyperchromatic nuclei. Five to 7 mitotic figures were seen in 50 high-power fields, with rare atypical mitosis. Focal vascular invasion was identified, but capsular invasion was not seen. At the periphery of the tumor but within the tumor capsule were few microscopic foci of myelolipoma composed of mature adipose tissue and normal-appearing trilineage hematopoietic cells. The transition between the tumor cells and the adipocytes was abrupt. The adjacent nonneoplastic adrenal gland was unremarkable.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="s3c"></a><strong><span style="font-size: 10pt; color: black">Immunohistochemical Findings</span></strong><span style="font-size: 10pt; color: black"><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">Immunohistochemical staining for cytokeratin, epithelial membrane antigen, carcinoembryonic antigen, vimentin, S100 protein, melanin A, chromogranin, synaptophysin, inhibin, and Ki-67 was performed on paraffin-embedded tissue. The tumor cells were strongly positive for vimentin and focally positive for synaptophysin and showed a moderately proliferative rate with Ki-67 (staining in 20% of tumor cells). The tumor cells were negative for the remaining markers. The adipocytes were positive for S100 protein. The normal adjacent cortical cells were positive for inhibin and melanin A. Cells in the normal medulla stained positive for chromogranin, synaptophysin, and S100 protein.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="s4"></a><strong><span style="font-size: 10pt; color: black">COMMENT</span></strong><span style="font-size: 10pt; color: black"> <o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">More than half of adrenocortical carcinomas secrete hormones, most commonly cortisol, followed by androgens, estrogen, and aldosterone.<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b7#i1543-2165-129-6-e144-b7"><sup><span style="color: black; text-decoration: none">7</span></sup></a> Pure aldosterone-secreting adrenocortical carcinomas are extremely rare, with fewer than 30 well-documented cases reported in the medical literature.<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b3#i1543-2165-129-6-e144-b3"><sup><span style="color: black; text-decoration: none">3</span></sup></a> To our knowledge, this is the first reported case of a pure aldosterone-secreting adrenocortical carcinoma associated with myelolipoma.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">Only 4 cases of adrenocortical carcinoma with a concomitant myelolipomatous component could be found in the medical literature.<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b5#i1543-2165-129-6-e144-b5"><sup><span style="color: black; text-decoration: none">5,</span></sup></a><a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b8#i1543-2165-129-6-e144-b8"><sup><span style="color: black; text-decoration: none">8,</span></sup></a><a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b9#i1543-2165-129-6-e144-b9"><sup><span style="color: black; text-decoration: none">9</span></sup></a> Two cases<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b8#i1543-2165-129-6-e144-b8"><sup><span style="color: black; text-decoration: none">8</span></sup></a> were reported with 49 other adrenal cortical carcinomas without specific description of the cases. The third case<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b9#i1543-2165-129-6-e144-b9"><sup><span style="color: black; text-decoration: none">9</span></sup></a> was found during the autopsy of a 57-year-old woman with multiple endocrine neoplasia syndrome type 1, which included hyperparathyroidism due to parathyroid hyperplasia, Zollinger-Ellison syndrome secondary to multiple islet cell adenomas, a 2.0-cm pituitary adenoma associated with a meningioma, a 23-g left adrenal adenoma, and a 325-g right adrenocarcinoma associated with myelolipoma. The fourth case<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b5#i1543-2165-129-6-e144-b5"><sup><span style="color: black; text-decoration: none">5</span></sup></a> was a 24-year-old man with Cushing syndrome; the size and weight of the lesion were not available. The myelolipoma component in these last 2 cases was similar to that in ours in that it was a lesion at the periphery of the adrenocortical carcinoma. In our case, the transition between the carcinoma and the myelolipoma was abrupt, and in some areas, the tumor nests within the myelolipoma simulated extracapsular extension.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">Myelolipoma is a benign tumor that usually does not secrete hormones; however, its associations with <st1:place w:st="on">Addison</st1:place> disease, Cushing syndrome, hermaphroditism, virilism, and extreme obesity have been reported.<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b9#i1543-2165-129-6-e144-b9"><sup><span style="color: black; text-decoration: none">9,</span></sup></a><a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b10#i1543-2165-129-6-e144-b10"><sup><span style="color: black; text-decoration: none">10</span></sup></a> One case of hyperaldosteronism due to an adrenal adenoma combined with a myelolipoma has been reported,<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b11#i1543-2165-129-6-e144-b11"><sup><span style="color: black; text-decoration: none">11</span></sup></a> but no cases of hyperaldosteronism secondary to a carcinoma with a myelolipoma have been reported. We believe that the elevated level of aldosterone found in our case was due to the adrenocortical carcinoma, not the myelolipoma. The pathogenesis of adrenal myelolipoma is unknown, and it is unclear in this case whether the myelolipoma was an incidental finding or was somehow related to the presence of the carcinoma or the obesity of the patient.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">The main conditions to be considered in the differential diagnosis of myelolipoma are lipomatous metaplasia (presence of adipose tissue only), which has been found in the adrenal glands and is associated with pseudocysts; hyperplasia; primary pigmented nodular adrenocortical disease; adenomas; and carcinomas.<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b12#i1543-2165-129-6-e144-b12"><sup><span style="color: black; text-decoration: none">12</span></sup></a> In our case, the adipose tissue was associated with myeloid elements, which are features of myelolipoma.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">Differentiating between adrenal adenoma and carcinoma in a small lesion can be challenging. Definitive diagnosis of malignancy in adrenocortical lesions is based on the presence of distant metastasis or local invasion. No single pathologic criterion of malignancy is reliable. Therefore, 3 multiparameter systems have been devised to help in delineating adrenocortical malignancies.<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b13#i1543-2165-129-6-e144-b13"><sup><span style="color: black; text-decoration: none">13</span></sup></a> Of the 3, the Weiss system,<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b2#i1543-2165-129-6-e144-b2"><sup><span style="color: black; text-decoration: none">2,</span></sup></a><a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b14#i1543-2165-129-6-e144-b14"><sup><span style="color: black; text-decoration: none">14</span></sup></a> which evaluates 9 histologic criteria commonly associated with metastasis or recurrence, is the most widely used because of its simplicity and reliability. The 9 criteria used are high nuclear grade (based on the Fuhrman nuclear grade on the highest-grade areas of the neoplasm), mitotic rate of more than 5 mitoses per 50 high-power fields, presence of atypical mitotic figures, more than 75% of tumor cells with eosinophilic cytoplasm, more than 33% of tumor cells forming sheets, confluent nests of tumor cell necrosis, venous invasion, sinusoidal invasion, and capsular invasion (invasion of nests or cords of tumor cells extending into or through the capsule with corresponding stromal reaction). Originally, the presence of 4 or more of these histologic findings was defined as indicative of malignancy<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b2#i1543-2165-129-6-e144-b2"><sup><span style="color: black; text-decoration: none">2</span></sup></a>; later, the threshold was modified to 3 or more.<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b14#i1543-2165-129-6-e144-b14"><sup><span style="color: black; text-decoration: none">14</span></sup></a> In this same study, Weiss et al<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b14#i1543-2165-129-6-e144-b14"><sup><span style="color: black; text-decoration: none">14</span></sup></a> found that the mitotic rate was a strong predictor of behavior and divided adrenocortical carcinomas into low-grade and high-grade lesions on the basis of mitotic count. Any carcinoma with more than 20 mitoses per 50 high-power fields is considered high grade. In their report, patients with high-grade tumors had a median survival of 14 months, versus 58 months for those with low-grade tumors. The tumor in our case met 6 of the 9 Weiss criteria for malignancy: diffuse growth, more than 75% eosinophilic cells, more than 5 mitoses per 50 high-power fields, rare atypical mitotic figures, necrosis, and venous invasion. On the basis of the mitotic rate, this tumor was classified as a low-grade adrenocortical carcinoma.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">Another feature that favored malignant diagnosis in our case was the proliferative rate as determined by Ki-67 immunostaining. Ki-67 is a monoclonal antibody that recognizes 2 nuclear proteins in proliferating cells during all non-G<sub>0</sub> phases of the cell cycle, and it has emerged as a promising, reliable indicator of cell proliferation.<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b15#i1543-2165-129-6-e144-b15"><sup><span style="color: black; text-decoration: none">15</span></sup></a> Although the exact Ki-67 threshold for malignancy in various studies has ranged from 4% to 10%,<a href="http://arpa.allenpress.com/arpaonline/?request=get-document&amp;doi=10.1043%2F1543-2165%282005%29129%5Be144:ACWCMI%5D2.0.CO%3B2#i1543-2165-129-6-e144-b15#i1543-2165-129-6-e144-b15"><sup><span style="color: black; text-decoration: none">15</span></sup></a> the cells in our case had 20% nuclear activity, a feature that supported the diagnosis of carcinoma.<o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">In summary, we present the first case of aldosterone-secreting adrenocortical carcinoma with concomitant myelolipoma. The pathogenesis of the myelolipoma and its effect on the adrenocortical carcinoma are unknown. Aldosterone-secreting adrenocortical carcinoma associated with myelolipoma should be considered in the differential diagnosis of any adrenal mass.<o:p></o:p></span></p>
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<p style="text-align: justify"><a name="i1543_2165_129_6_e144_b13"></a><span style="font-size: 10pt; color: black">13. </span><span style="font-size: 10pt; color: black">Medeiros LJ, Weiss LM. New developments in the pathologic diagnosis of adrenal cortical neoplasms: a review. <em>Am J Clin Pathol</em> 1992;97:73–83. [<a href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&amp;cmd=Retrieve&amp;list_uids=1728867&amp;dopt=Citation"><span style="color: black; text-decoration: none">PubMed Citation</span></a>] <o:p></o:p></span></p>
<p style="text-align: justify"><a name="i1543_2165_129_6_e144_b14"></a><span style="font-size: 10pt; color: black">14. </span><span style="font-size: 10pt; color: black">Weiss LM, Mederios LJ, Vickery AL. Pathological features of prognostic significance in adrenocortical carcinoma. <em>Am J Surg Pathol</em> 1989;13:202–206. [<a href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&amp;cmd=Retrieve&amp;list_uids=2919718&amp;dopt=Citation"><span style="color: black; text-decoration: none">PubMed Citation</span></a>] <o:p></o:p></span></p>
<p style="text-align: justify"><a name="i1543_2165_129_6_e144_b15"></a><span style="font-size: 10pt; color: black">15. </span><span style="font-size: 10pt; color: black">Terzolo M, Boccuzzi A, Bovio S. et al. Immunohistochemical assessment of Ki-67 in the differential diagnosis of adrenocortical tumors. <em>Urology</em> 2001;57:176–182. [<a href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&amp;cmd=Retrieve&amp;list_uids=11164177&amp;dopt=Citation"><span style="color: black; text-decoration: none">PubMed Citation</span></a>]<o:p></o:p></span></p>
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		<title>Adrenocortical Adenoma and Carcinoma: Histopathological and Molecular Comparative Analysis</title>
		<link>http://theadrenocorticalcarcinoma.com/2008/05/22/adrenocortical-adenoma-and-carcinoma-histopathological-and-molecular-comparative-analysis/</link>
		<comments>http://theadrenocorticalcarcinoma.com/2008/05/22/adrenocortical-adenoma-and-carcinoma-histopathological-and-molecular-comparative-analysis/#comments</comments>
		<pubDate>Thu, 22 May 2008 18:12:02 +0000</pubDate>
		<dc:creator>admin</dc:creator>
		
		<category><![CDATA[Adrenocortical Adenoma and Carcinoma: Histopathological]]></category>

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		<description><![CDATA[
Alexander Stojadinovic M.D.3, Murray F Brennan M.D.1, Axel Hoos M.D., Ph.D.1,2, 
Atilla Omeroglu M.D.2, Denis H Y Leung Ph.D.4, Maria E Dudas2, Aviram Nissan M.D.1, 
Carlos Cordon-Cardo M.D.2 and Ronald A Ghossein M.D.2
1.                    1Department of Surgery, Memorial Sloan-Kettering Cancer Center, New  York, New York 
2.                    2Department of Pathology, Memorial Sloan-Kettering Cancer Center, New  York, New York 
3.                    3Department of Surgery, Walter Reed Army Medical Center, Washington, D.C. 
4.                    4School of [...]]]></description>
			<content:encoded><![CDATA[<p style="border-style: solid none none; border-color: white -moz-use-text-color -moz-use-text-color; border-width: 1pt medium medium; padding: 0in; background: white none repeat scroll 0% 50%; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial">
<p style="border: medium none ; margin: 0in 0in 0.0001pt; padding: 0in; background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black" lang="EN">Alexander Stojadinovic M.D.<sup><a href="http://www.nature.com/modpathol/journal/v16/n8/full/3880834a.html#aff3#aff3" title="affiliated with 3"><span style="color: black">3</span></a></sup>, <st1:place w:st="on"><st1:city w:st="on">Murray</st1:city></st1:place> F Brennan M.D.<sup><a href="http://www.nature.com/modpathol/journal/v16/n8/full/3880834a.html#aff1#aff1" title="affiliated with 1"><span style="color: black">1</span></a></sup>, Axel Hoos M.D., Ph.D.<sup><a href="http://www.nature.com/modpathol/journal/v16/n8/full/3880834a.html#aff1#aff1" title="affiliated with 1"><span style="color: black">1</span></a>,<a href="http://www.nature.com/modpathol/journal/v16/n8/full/3880834a.html#aff2#aff2" title="affiliated with 2"><span style="color: black">2</span></a></sup>, <o:p></o:p></span></p>
<p style="border: medium none ; margin: 0in 0in 0.0001pt; padding: 0in; background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black" lang="EN">Atilla Omeroglu M.D.<sup><a href="http://www.nature.com/modpathol/journal/v16/n8/full/3880834a.html#aff2#aff2" title="affiliated with 2"><span style="color: black">2</span></a></sup>, Denis H Y Leung Ph.D.<sup><a href="http://www.nature.com/modpathol/journal/v16/n8/full/3880834a.html#aff4#aff4" title="affiliated with 4"><span style="color: black">4</span></a></sup>, Maria E Dudas<sup><a href="http://www.nature.com/modpathol/journal/v16/n8/full/3880834a.html#aff2#aff2" title="affiliated with 2"><span style="color: black">2</span></a></sup>, Aviram Nissan M.D.<sup><a href="http://www.nature.com/modpathol/journal/v16/n8/full/3880834a.html#aff1#aff1" title="affiliated with 1"><span style="color: black">1</span></a></sup>, <o:p></o:p></span></p>
<p style="border: medium none ; margin: 0in 0in 0.0001pt; padding: 0in; background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black" lang="EN">Carlos Cordon-Cardo M.D.<sup><a href="http://www.nature.com/modpathol/journal/v16/n8/full/3880834a.html#aff2#aff2" title="affiliated with 2"><span style="color: black">2</span></a></sup> and Ronald A Ghossein M.D.<sup><a href="http://www.nature.com/modpathol/journal/v16/n8/full/3880834a.html#aff2#aff2" title="affiliated with 2"><span style="color: black">2</span></a></sup><o:p></o:p></span></p>
<p class="MsoNormal" style="border: medium none ; padding: 0in; background: white none repeat scroll 0% 50%; margin-left: 0in; text-align: justify; text-indent: 0in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><!--[if !supportLists]--><span style="font-size: 10pt; color: black" lang="EN"><span>1.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><sup><span style="font-size: 10pt; color: black" lang="EN">1</span></sup><span style="font-size: 10pt; color: black" lang="EN">Department of Surgery, <st1:city w:st="on">Memorial Sloan-Kettering Cancer Center</st1:city>, <st1:state w:st="on">New  York</st1:state>, <st1:state w:st="on"><st1:place w:st="on">New York</st1:place></st1:state> <o:p></o:p></span></p>
<p class="MsoNormal" style="border: medium none ; padding: 0in; background: white none repeat scroll 0% 50%; margin-left: 0in; text-align: justify; text-indent: 0in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><!--[if !supportLists]--><span style="font-size: 10pt; color: black" lang="EN"><span>2.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><sup><span style="font-size: 10pt; color: black" lang="EN">2</span></sup><span style="font-size: 10pt; color: black" lang="EN">Department of Pathology, <st1:city w:st="on">Memorial Sloan-Kettering Cancer Center</st1:city>, <st1:state w:st="on">New  York</st1:state>, <st1:state w:st="on"><st1:place w:st="on">New York</st1:place></st1:state> <o:p></o:p></span></p>
<p class="MsoNormal" style="border: medium none ; padding: 0in; background: white none repeat scroll 0% 50%; margin-left: 0in; text-align: justify; text-indent: 0in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><!--[if !supportLists]--><span style="font-size: 10pt; color: black" lang="EN"><span>3.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><sup><span style="font-size: 10pt; color: black" lang="EN">3</span></sup><span style="font-size: 10pt; color: black" lang="EN">Department of Surgery, <st1:place w:st="on"><st1:city w:st="on">Walter Reed Army Medical Center</st1:city>, <st1:state w:st="on">Washington</st1:state></st1:place>, D.C. <o:p></o:p></span></p>
<p class="MsoNormal" style="border: medium none ; padding: 0in; background: white none repeat scroll 0% 50%; margin-left: 0in; text-align: justify; text-indent: 0in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><!--[if !supportLists]--><span style="font-size: 10pt; color: black" lang="EN"><span>4.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><sup><span style="font-size: 10pt; color: black" lang="EN">4</span></sup><span style="font-size: 10pt; color: black" lang="EN">School of Economics and Social Sciences, <st1:place w:st="on"><st1:city w:st="on">Singapore Management   University</st1:city>, <st1:country-region w:st="on">Singapore</st1:country-region></st1:place><o:p></o:p></span></p>
<p class="caff3" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black" lang="EN">Correspondence: Alexander Stojadinovic, M.D., Walter Reed Army Medical Center, General Surgery Service, 6900 Georgia Avenue, N.W., Washington, D.C. 20307; fax: 202-782-1234; e-mail: <a href="mailto:ta.stojadinovic@verizon.net"><span style="color: black">ta.stojadinovic@verizon.net</span></a>.<o:p></o:p></span></p>
<p class="prdates3" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black" lang="EN">Accepted 1 May 2003. <o:p></o:p></span></p>
<p class="abslead1" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black; font-weight: normal" lang="EN">We compared histomorphological features and molecular expression profiles of adrenocortical adenomas (ACAd) and carcinomas (ACCa). A critical histopathological review (mean, 11 slides per patient) was conducted of 37 ACAd and 67 ACCa. Paraffin-embedded tissue cores of ACAd (<em>n</em> = 33) and ACCa (<em>n</em> = 38) were arrayed in triplicate on tissue microarrays. Expression profiles of p53, mdm-2, p21, Bcl-2, cyclin D1, p27, and Ki-67 were investigated by immunohistochemistry and correlated with histopathology and patient outcome using standard statistical methodology. Median follow-up period was 5 years. Tumor necrosis, atypical mitoses, and &gt;1 mitosis per 50 high-power fields were factors that were highly specific for ACCa (<em>P</em> &lt; .001). Number (0 to 4) of unfavorable markers [Ki-67 (+), p21 (+), p27 (+), mdm-2(-)] expressed was significantly associated with mitotic activity and morphologic index (<em>i.e.</em>, number of adverse morphologic features) and highly predictive of malignancy (<em>P</em> &lt; .001). Ki-67 overexpression occurred in 0 ACAd and 36% ACCa (<em>P</em> &lt; .001) and was significantly associated with mitotic rate and unfavorable morphologic index (<em>P</em> &lt; .001). Tumor necrosis, atypical mitoses, &gt;5 mitoses per 50 high-power fields, sinusoidal invasion, histologic index of &gt;5, and presence of more than two unfavorable molecular markers were associated significantly with metastasis in ACCa. Well-established histopathologic criteria and Ki-67 can specifically distinguish <st1:place w:st="on">ACCAd</st1:place> from ACCa. Tumor cell proliferation (Ki-67) correlates with mitotic activity and morphologic index. Tumor morphology is a better predictor of metastatic risk in ACCa than current immunohistochemistry-detected cell cycle regulatory and proliferation–associated proteins.<o:p></o:p></span></p>
<h4 style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt" lang="EN">Keywords: <o:p></o:p></span></h4>
<p class="keywords3" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black" lang="EN">Adenoma, Adrenal, Carcinoma, IHC, Tissue microarray<o:p></o:p></span></p>
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		<title>Adrenocortical Carcinoma</title>
		<link>http://theadrenocorticalcarcinoma.com/2008/05/22/adrenocortical-carcinoma-3/</link>
		<comments>http://theadrenocorticalcarcinoma.com/2008/05/22/adrenocortical-carcinoma-3/#comments</comments>
		<pubDate>Thu, 22 May 2008 18:11:18 +0000</pubDate>
		<dc:creator>admin</dc:creator>
		
		<category><![CDATA[Adrenocortical Carcinoma -2]]></category>

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		<description><![CDATA[What is cancer of the adrenal cortex?
Cancer of the adrenal cortex, a rare cancer, is a disease in which cancer (malignant) cells are found in the adrenal cortex, which is the outside layer of the adrenal gland. Cancer of the adrenal cortex is also called adrenocortical carcinoma. There are two adrenal glands, one above each [...]]]></description>
			<content:encoded><![CDATA[<p style="text-align: justify"><span style="font-size: 10pt; color: black">What is cancer of the adrenal cortex?<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Cancer of the adrenal cortex, a rare cancer, is a disease in which cancer (malignant) cells are found in the adrenal cortex, which is the outside layer of the adrenal gland. Cancer of the adrenal cortex is also called adrenocortical carcinoma. There are two adrenal glands, one above each kidney in the back of the upper abdomen. The adrenal glands are also called the suprarenal glands. The inside layer of the adrenal gland is called the adrenal medulla. Cancer that starts in the adrenal medulla is called phaeochromocytoma and is discussed in a separate patient information summary.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">The cells in the adrenal cortex make important hormones that help the body work properly. When cells in the adrenal cortex become cancerous, they may make too much of one or more hormones, which can cause symptoms such as high blood pressure, weakening of the bones, or diabetes. If male or female hormones are affected, the body may go through changes such as a deepening of the voice, growing hair on the face, swelling of the sex organs, or swelling of the breasts. Cancers that make hormones are called functioning tumours. Many cancers of the adrenal cortex do not make extra hormones and are called nonfunctioning tumours.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">A doctor should be seen if the following symptoms appear and won’t go away:<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">* pain in the abdomen,<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">* loss of weight without dieting, or<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">* weakness.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">If there is a functioning tumour, there may be symptoms or signs caused by too many hormones.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">If there are symptoms, a doctor will order blood and urine tests to see whether the amounts of hormones in the body are normal. A doctor may also order a computed tomography scan of the abdomen, a special x-ray that uses a computer to make a picture of the inside of the abdomen. Other special x-rays may also be done to tell what kind of tumour is present.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">The chance of recovery (prognosis) depends on how far the cancer has spread (stage) and on whether a doctor was able to surgically remove all of the cancer.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black"> Stage Explanation<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black"> Stages of cancer of the adrenal cortex<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Once cancer of the adrenal cortex has been found, more tests will be done to see how far the cancer has spread. This is called staging. A doctor needs to know the stage of the cancer to plan treatment. The following stages are used for cancer of the adrenal cortex:<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Stage I<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">The cancer is less than 5 centimeters (less than 2 inches) and has not spread into tissues around the adrenal gland.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Stage II<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">The cancer is more than 5 centimeters (greater than 2 inches) and has not spread into tissues around the adrenal gland.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Stage III<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">The cancer has spread into tissues around the adrenal gland or has spread to the lymph nodes around the adrenal gland. Lymph nodes are part of the lymph system and are small, bean shaped organs that make and store infection-fighting cells.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Stage IV<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">The cancer has spread to tissues or organs in the area and to lymph nodes around the adrenal cortex, or the cancer has spread to other parts of the body.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Recurrent<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">The cancer has come back (recurred) after it has been treated. It may come back in the adrenal cortex or in another part of the body.<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black"> <o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">Treatment Option Overview<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">How cancer of the adrenal cortex is treated<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">There are treatments for all patients with cancer of the adrenal cortex. Three kinds of treatment are used:<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">* Surgery (taking out the cancer).<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">* Chemotherapy (using drugs to kill cancer cells).<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">* Radiation therapy (using high-dose x-rays or other high-energy rays to kill cancer cells).<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">A doctor may take out the adrenal gland in an operation called an adrenalectomy. Tissues around the adrenal glands that contain cancer may be removed. Lymph nodes in the area may also be removed (lymph node dissection).<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Chemotherapy uses drugs to kill cancer cells. Chemotherapy may be taken by pill, or it may be put into the body by a needle in a vein or muscle. Chemotherapy is called a systemic treatment because the drug enters the bloodstream, travels through the body, and kills cancer cells throughout the body.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Radiation therapy uses high-energy x-rays to kill cancer cells and shrink tumours. Radiation for cancer of the adrenal cortex usually comes from a machine outside the body (external radiation therapy).<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Besides treatment for cancer (chemotherapy, radiation therapy, and/or surgery), a patient may also receive therapy to prevent or treat symptoms caused by the extra hormones that are made by the cancer.<br />
Treatment by stage<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Treatment depends on how far the cancer has spread, and a patient’s age and overall health.<o:p></o:p></span></p>
<p style="text-align: justify"><span style="font-size: 10pt; color: black">Standard treatment may be considered because of its effectiveness in past studies, or participation in a clinical trial may be considered. Not all patients are cured with standard therapy, and some standard treatments may have more side effects than are desired. For these reasons, clinical trials are designed to find better ways to treat cancer patients and are based on the most up-to-date information. Clinical trials are ongoing in some parts of the country for patients with cancer of the adrenal cortex. For more information, call the Cancer Information Service at 1-800-4-CANCER (1-800-422-6237); TTY at 1-800-332-8615.<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">Stage I Adrenocortical Carcinoma<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">Treatment will probably be surgery to remove the cancer.<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">Stage II Adrenocortical Carcinoma<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">Treatment will probably be surgery to remove the cancer. Clinical trials are testing new treatments.<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">Stage III Adrenocortical Carcinoma<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">Treatment may be one of the following:<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">1. Surgery to remove the cancer. Lymph nodes in the area may also be removed (lymph node dissection).<br />
2. A clinical trial of radiation therapy.<br />
3. A clinical trial of chemotherapy if the size of the tumour can be measured with x-rays and/or if the tumour is making hormones. <o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">Stage IV Adrenocortical Carcinoma<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">Treatment may be one of the following:<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">1. Chemotherapy. Clinical trials are testing new drugs.<br />
2. Radiation therapy to bones where the cancer has spread.<br />
3. Surgery to remove the cancer in places where it has spread. <o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">Recurrent Adrenocortical Carcinoma<o:p></o:p></span></p>
<p><span style="font-size: 10pt; color: black">Treatment depends on many factors, including where the cancer came back and what treatment has already been received. In some cases, surgery can be effective in decreasing the symptoms of the disease by removing some of the tumour. Clinical trials are testing new treatments. <o:p></o:p></span></p>
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		<title>Adrenocortical Carcinoma</title>
		<link>http://theadrenocorticalcarcinoma.com/2008/05/22/adrenocortical-carcinoma-2/</link>
		<comments>http://theadrenocorticalcarcinoma.com/2008/05/22/adrenocortical-carcinoma-2/#comments</comments>
		<pubDate>Thu, 22 May 2008 18:09:44 +0000</pubDate>
		<dc:creator>admin</dc:creator>
		
		<category><![CDATA[Adrenocortical Carcinoma -1]]></category>

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		<description><![CDATA[General Information
Adrenocortical carcinoma is a rare tumor that affects only 1 to 2 persons per one million population. It usually occurs in adults, and the median age at diagnosis is 44 years. Although adrenal carcinoma is potentially curable at early stages, only 30% of these malignancies are confined to the adrenal gland at the time [...]]]></description>
			<content:encoded><![CDATA[<p class="Heading339" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; font-family: "Times New Roman"; color: black">General Information<o:p></o:p></span></p>
<p class="NormalWeb48" style="background: white none repeat scroll 0% 50%; text-align: justify; line-height: normal; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black">Adrenocortical carcinoma is a rare tumor that affects only 1 to 2 persons per one million population. It usually occurs in adults, and the median age at diagnosis is 44 years. Although adrenal carcinoma is potentially curable at early stages, only 30% of these malignancies are confined to the adrenal gland at the time of diagnosis.[<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">1</span></a>] Radical surgical excision is the treatment of choice for patients with localized malignancies and remains the only method by which long-term disease-free survival may be achieved. Overall 5-year survival for tumors resected for cure is approximately 40%.<o:p></o:p></span></p>
<p class="NormalWeb48" style="background: white none repeat scroll 0% 50%; text-align: justify; line-height: normal; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black">Retrospective studies have identified 2 important prognostic factors: completeness of resection and stage of disease. Patients without evidence of invasion into local tissues or spread to lymph nodes have an improved prognosis.[<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">2</span></a>] The role of DNA ploidy as a prognostic indicator is controversial, with some [<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">3</span></a>] studies showing correlation between aneuploidy and prognosis, and other studies [<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">2</span></a>,<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">4</span></a>] showing no correlation. <o:p></o:p></span></p>
<p class="NormalWeb48" style="background: white none repeat scroll 0% 50%; text-align: justify; line-height: normal; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black">Approximately 60% of patients present with symptoms related to excessive hormone secretion, but hormone testing reveals that 60% to 80% of tumors are functioning.[<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">5</span></a>,<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">6</span></a>] Nonfunctioning carcinomas may be heralded by symptoms of local invasion by tumor or by metastases. Initial evaluation should include, in addition to appropriate endocrine studies, computed tomography and/or magnetic resonance imaging of the abdomen. Selective angiography and adrenal venography may be helpful in identifying smaller lesions and for distinguishing tumors of the adrenal gland from tumors of the upper pole of the kidney. Although the use of positron emission tomography may be effective in identifying unsuspected sites of metastases, its role as a staging tool is unclear.[<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">7</span></a>] The detection of metastatic lesions may allow effective palliation of both functioning and nonfunctioning lesions. <o:p></o:p></span></p>
<p class="NormalWeb48" style="background: white none repeat scroll 0% 50%; text-align: justify; line-height: normal; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black">The most common sites of metastases are the peritoneum, lung, liver, and bone. Palliation of metastatic functioning tumors may be achieved by resection of both the primary tumor and metastatic lesions. Unresectable or widely disseminated tumors may be palliated by antihormonal therapy with mitotane, systemic chemotherapy, or (for localized lesions) radiation therapy. However, survival for patients with stage IV tumors is usually less than 9 months unless a complete remission is achieved.[<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">6</span></a>,<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">8</span></a>,<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">9</span></a>,<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">10</span></a>] To date, there is no convincing evidence that systemic therapy will improve the survival duration of patients with adrenal cancer. <o:p></o:p></span></p>
<p class="NormalWeb48" style="background: white none repeat scroll 0% 50%; text-align: justify; line-height: normal; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><strong><span style="font-size: 10pt; color: black">References:</span></strong><span style="font-size: 10pt; color: black"> <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.5in; text-align: justify; text-indent: -0.5in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><a title="s1_1" name="s1_1"></a><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>1.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Norton JA: Adrenal tumors. In: DeVita VT Jr, Hellman S, Rosenberg SA, eds.: Cancer: Principles and Practice of Oncology. 7th ed. <st1:place w:st="on"><st1:city w:st="on">Philadelphia</st1:city>, <st1:state w:st="on">Pa</st1:state></st1:place>: Lippincott Williams &amp; Wilkins, 2005, pp 1528-39 <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.5in; text-align: justify; text-indent: -0.5in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><a title="s1_2" name="s1_2"></a><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>2.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Lee JE, Berger DH, el-Naggar AK, et al.: Surgical management, DNA content, and patient survival in adrenal cortical carcinoma. Surgery 118 (6): 1090-8, 1995. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.5in; text-align: justify; text-indent: -0.5in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><a title="s1_3" name="s1_3"></a><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>3.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Camuto P, Schinella R, Gilchrist K, et al.: Adrenal cortical carcinoma: flow cytometric study of 22 cases, an ECOG study. Urology 37 (4): 380-4, 1991. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.5in; text-align: justify; text-indent: -0.5in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><a title="s1_4" name="s1_4"></a><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>4.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Haak HR, Cornelisse CJ, Hermans J, et al.: Nuclear DNA content and morphological characteristics in the prognosis of adrenocortical carcinoma. Br J Cancer 68 (1): 151-5, 1993. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.5in; text-align: justify; text-indent: -0.5in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><a title="s1_5" name="s1_5"></a><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>5.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Icard P, Chapuis Y, Andreassian B, et al.: Adrenocortical carcinoma in surgically treated patients: a retrospective study on 156 cases by the French Association of Endocrine Surgery. Surgery 112 (6): 972-9; discussion 979-80, 1992. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.5in; text-align: justify; text-indent: -0.5in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><a title="s1_6" name="s1_6"></a><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>6.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Luton JP, Cerdas S, Billaud L, et al.: Clinical features of adrenocortical carcinoma, prognostic factors, and the effect of mitotane therapy. N Engl J Med 322 (17): 1195-201, 1990. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.5in; text-align: justify; text-indent: -0.5in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><a title="s1_7" name="s1_7"></a><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>7.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Becherer A, Vierhapper H, Pötzi C, et al.: FDG-PET in adrenocortical carcinoma. Cancer Biother Radiopharm 16 (4): 289-95, 2001. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.5in; text-align: justify; text-indent: -0.5in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><a title="s1_8" name="s1_8"></a><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>8.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Brennan MF: Adrenocortical carcinoma. CA Cancer J Clin 37 (6): 348-65, 1987 Nov-Dec. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.5in; text-align: justify; text-indent: -0.5in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><a title="s1_9" name="s1_9"></a><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>9.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                    </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Cohn K, Gottesman L, Brennan M: Adrenocortical carcinoma. Surgery 100 (6): 1170-7, 1986. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.5in; text-align: justify; text-indent: -0.5in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><a title="s1_10" name="s1_10"></a><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>10.<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">                 </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Wooten MD, King DK: Adrenal cortical carcinoma. Epidemiology and treatment with mitotane and a review of the literature. Cancer 72 (11): 3145-55, 1993. <o:p></o:p></span></p>
<p class="Heading339" style="background: white none repeat scroll 0% 50%; text-align: justify; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><a title="ncicdr0000062907_cellular_classification" name="ncicdr0000062907_cellular_classification"></a><a title="Cellular_20Classification" name="Cellular_20Classification"></a><span style="font-size: 10pt; font-family: "Times New Roman"; color: black">Cellular Classification<o:p></o:p></span></p>
<p class="NormalWeb48" style="background: white none repeat scroll 0% 50%; text-align: justify; line-height: normal; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial"><span style="font-size: 10pt; color: black">Adrenocortical carcinoma can be classified as follows: <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.25in; text-align: left; text-indent: -0.25in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial" align="left"><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>—<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">      </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Differentiated: Functioning tumors are usually differentiated. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.25in; text-align: left; text-indent: -0.25in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial" align="left"><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>—<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">      </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Anaplastic: Production of hormones by anaplastic tumors is rare. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.25in; text-align: left; text-indent: -0.25in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial" align="left"><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>—<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">      </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Hormonal: Approximately 60% of adrenocortical carcinomas produce hormones. The associated clinical syndromes include the following:[<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">1</span></a>,<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">2</span></a>,<a href="http://health.yahoo.com/article/healthwise--ncicdr0000062907/"><span style="color: black">3</span></a>] <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.25in; text-align: left; text-indent: -0.25in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial" align="left"><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>—<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">      </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Hypercortisolism (Cushing’s syndrome). <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.25in; text-align: left; text-indent: -0.25in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial" align="left"><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>—<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">      </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Adrenogenital syndrome. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.25in; text-align: left; text-indent: -0.25in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial" align="left"><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>—<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">      </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Virilization. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.25in; text-align: left; text-indent: -0.25in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial" align="left"><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>—<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">      </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Feminization. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.25in; text-align: left; text-indent: -0.25in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial" align="left"><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>—<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">      </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Precocious puberty. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.25in; text-align: left; text-indent: -0.25in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial" align="left"><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>—<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">      </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Hyperaldosteronism. <o:p></o:p></span></p>
<p class="MsoNormal" style="background: white none repeat scroll 0% 50%; margin-left: 0.25in; text-align: left; text-indent: -0.25in; -moz-background-clip: -moz-initial; -moz-background-origin: -moz-initial; -moz-background-inline-policy: -moz-initial" align="left"><!--[if !supportLists]--><span style="font-size: 10pt; color: black"><span>—<span style="font-family: "Times New Roman"; font-style: normal; font-variant: normal; font-weight: normal; font-size: 7pt; line-height: normal; font-size-adjust: none; font-stretch: normal">      </span></span></span><!--[endif]--><span style="font-size: 10pt; color: black">Primary hyperaldosteronism (<st1:state w:st="on"><st1:place w:st="on">Conn</st1:place></st1:state>’s syndrome). <o:p></o:p></span></p>
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		<title>Context</title>
		<link>http://theadrenocorticalcarcinoma.com/2008/05/22/context/</link>
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		<pubDate>Thu, 22 May 2008 18:08:23 +0000</pubDate>
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		<category><![CDATA[Context]]></category>

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		<description><![CDATA[Adrenocortical carcinoma (ACC) is a rare and heterogeneous malignancy with incompletely understood pathogenesis and poor prognosis. Patients present with hormone excess (e.g. virilization, Cushing’s syndrome) or a local mass effect (median tumor size at diagnosis &#62; 10 cm). This paper reviews current diagnostic and therapeutic strategies in ACC. 
Evidence Acquisition: Original articles and reviews were [...]]]></description>
			<content:encoded><![CDATA[<p style="text-align: justify"><span style="font-size: 10pt; color: black">Adrenocortical carcinoma (ACC) is a rare and heterogeneous<sup> </sup>malignancy with incompletely understood pathogenesis and poor<sup> </sup>prognosis. Patients present with hormone excess (<em>e.g.</em> virilization,<sup> </sup>Cushing’s syndrome) or a local mass effect (median tumor<sup> </sup>size at diagnosis &gt; 10 cm). This paper reviews current diagnostic<sup> </sup>and therapeutic strategies in ACC.<sup> </sup><o:p></o:p></span></p>
<p style="text-align: justify"><strong><span style="font-size: 10pt; color: black">Evidence Acquisition:</span></strong><span style="font-size: 10pt; color: black"> Original articles and reviews were identified<sup> </sup>using a PubMed search strategy (<a href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi"><span style="color: black; text-decoration: none">http://www.ncbi.nlm.nih.gov/entrez/query.fcgi</span></a>)<sup> </sup>covering the time period up until November 2005. The following<sup> </sup>search terms were used in varying combinations: adrenal, adrenocortical,<sup> </sup>cancer, carcinoma, tumor, diagnosis, imaging, treatment, radiotherapy,<sup> </sup>mitotane, cytotoxic, surgery.<sup> </sup><o:p></o:p></span></p>
<p style="text-align: justify"><strong><span style="font-size: 10pt; color: black">Evidence synthesis:</span></strong><span style="font-size: 10pt; color: black"> Tumors typically appear inhomogeneous in<sup> </sup>both computerized tomography and magnetic resonance imaging<sup> </sup>with necroses and irregular borders and differ from benign adenomas<sup> </sup>by their low fat content. Hormonal analysis reveals evidence<sup> </sup>of steroid hormone secretion by the tumor in the majority of<sup> </sup>cases, even in seemingly hormonally inactive lesions. Histopathology<sup> </sup>is crucial for the diagnosis of malignancy and may also provide<sup> </sup>important prognostic information. In stages I–III open<sup> </sup>surgery by an expert surgeon aiming at an R0 resection is the<sup> </sup>treatment of choice. Local recurrence is frequent, particularly<sup> </sup>after violation of the tumor capsule. Surgery also plays a role<sup> </sup>in local tumor recurrence and metastatic disease. In patients<sup> </sup>not amenable to surgery, mitotane (alone or in combination with<sup> </sup>cytotoxic drugs) remains the treatment of choice. Monitoring<sup> </sup>of drug levels (therapeutic range 14–20 mg/liter) is mandatory<sup> </sup>for optimum results. In advanced disease, the most promising<sup> </sup>therapeutic options (etoposide, doxorubicin, cisplatin plus<sup> </sup>mitotane, and streptozotocin plus mitotane) are currently being<sup> </sup>compared in an international phase III trial (<a href="http://www.firm-act.org/"><span style="color: black; text-decoration: none">www.firm-act.org</span></a>).<sup> </sup>Adjuvant treatment options after complete tumor removal (<em>e.g.</em><sup> </sup>mitotane, radiotherapy) are urgently needed because postoperative<sup> </sup>disease-free survival at 5 yr is only around 30%, but options<sup> </sup>have still not been convincingly established. National registries,<sup> </sup>international cooperations, and trials provide important new<sup> </sup>structures for patients but also for researchers aiming at systematic<sup> </sup>and continuous progress in ACC. However, future advances in<sup> </sup>the management of ACC will mainly depend on a better understanding<sup> </sup>of the molecular pathogenesis facilitating the use of modern<sup> </sup>cancer treatments (<em>e.g.</em> tyrosine kinase inhibitors).<sup> </sup><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="SEC1"></a><span style="font-size: 10pt; color: black">ADRENOCORTICAL TUMORS ARE common tumors with a prevalence of<sup> </sup>at least 3% in a population over the age of 50 yr (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R1#R1"><span style="color: black; text-decoration: none">1</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R2#R2"><span style="color: black; text-decoration: none">2</span></a>). In<sup> </sup>contrast, adrenocortical carcinoma (ACC) is a rare malignancy<sup> </sup>(incidence 1–2 per 1 million population) with a heterogeneous<sup> </sup>presentation and a variable but generally poor prognosis (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R3#R3"><span style="color: black; text-decoration: none">3</span></a>,<sup> </sup><a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R4#R4"><span style="color: black; text-decoration: none">4</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R5#R5"><span style="color: black; text-decoration: none">5</span></a>). However, data on incidence are mainly based on the National<sup> </sup>Cancer Institute survey from the early 1970s and probably underestimate<sup> </sup>the true incidence. An exceptionally high annual incidence of<sup> </sup>ACC has been reported for children in southern Brazil (3.4–4.2<sup> </sup>per 1 million children <em>vs.</em> an estimated worldwide incidence<sup> </sup>of 0.3 per 1 million children younger than 15 yr) and is related<sup> </sup>to a TP53 tumor suppressor gene mutation (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R6#R6"><span style="color: black; text-decoration: none">6</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R7#R7"><span style="color: black; text-decoration: none">7</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R8#R8"><span style="color: black; text-decoration: none">8</span></a>). Women are<sup> </sup>more often affected than men (ratio 1.5) (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R9#R9"><span style="color: black; text-decoration: none">9</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R10#R10"><span style="color: black; text-decoration: none">10</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R11#R11"><span style="color: black; text-decoration: none">11</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R12#R12"><span style="color: black; text-decoration: none">12</span></a>). The<sup> </sup>age distribution is reported as bimodal with a first peak in<sup> </sup>childhood and a second higher peak in the fourth and fifth decade<sup> </sup>(<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R4#R4"><span style="color: black; text-decoration: none">4</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R12#R12"><span style="color: black; text-decoration: none">12</span></a>).<sup> </sup><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="SEC2"></a><span style="font-size: 10pt; color: black"><br clear="right" /> The molecular pathogenesis of ACC has been the topic of recent<sup> </sup>reviews (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R13#R13"><span style="color: black; text-decoration: none">13</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R14#R14"><span style="color: black; text-decoration: none">14</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R15#R15"><span style="color: black; text-decoration: none">15</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R16#R16"><span style="color: black; text-decoration: none">16</span></a>) but is still poorly understood. It<sup> </sup>is unclear whether ACCs evolve from adrenal adenomas after a<sup> </sup>second hit paradigm. Although such a sequence has been observed<sup> </sup>in occasional cases (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R17#R17"><span style="color: black; text-decoration: none">17</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R18#R18"><span style="color: black; text-decoration: none">18</span></a>), long-term follow-up data of incidentally<sup> </sup>discovered adrenal neoplasms suggest otherwise (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R19#R19"><span style="color: black; text-decoration: none">19</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R20#R20"><span style="color: black; text-decoration: none">20</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R21#R21"><span style="color: black; text-decoration: none">21</span></a>).<sup> </sup>Inactivating mutations at the 17p13 locus including the TP53<sup> </sup>tumor suppressor gene and alterations of the 11p15 locus leading<sup> </sup>to IGF-II overexpression are frequently observed. <em>In vitro</em> experiments<sup> </sup>suggest that overexpressed IGF-II acting via the IGF-I receptor<sup> </sup>is relevant for adrenal cancer cell proliferation (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R22#R22"><span style="color: black; text-decoration: none">22</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R23#R23"><span style="color: black; text-decoration: none">23</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R24#R24"><span style="color: black; text-decoration: none">24</span></a>).<sup> </sup>Thus, the IGF-II IGF-I receptor pathway is a promising target<sup> </sup>for future therapies in ACC (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R25#R25"><span style="color: black; text-decoration: none">25</span></a>).<sup> </sup><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="SEC3"></a><span style="font-size: 10pt; color: black">Patients present with evidence of adrenal steroid hormone excess<sup> </sup>in approximately 60% of cases. Rapidly progressing Cushing’s<sup> </sup>syndrome with or without virilization is the most frequent presentation.<sup> </sup>In patients from the German ACC Registry, autonomous cortisol<sup> </sup>secretion, either alone or in combination with other steroids,<sup> </sup>was detectable in 60% of the cases in which hormonal analysis<sup> </sup>had been performed prior to surgery (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R12#R12"><span style="color: black; text-decoration: none">12</span></a>). However, not in all<sup> </sup>of these cases was autonomous cortisol secretion clinically<sup> </sup>suspected. Androgen-secreting ACCs in women induce hirsutism<sup> </sup>and virilization with deepening of the voice, male pattern baldness,<sup> </sup>and oligoamenorrhea. Estrogen-secreting adrenal tumors in males<sup> </sup>lead to gynecomastia and testicular atrophy and are almost invariably<sup> </sup>malignant (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R26#R26"><span style="color: black; text-decoration: none">26</span></a>). High concentration of dehydroepiandrosterone<sup> </sup>sulfate (DHEA-S) is another clue suggesting ACC, whereas decreased<sup> </sup>serum DHEA-S concentrations are suggestive of a benign adenoma<sup> </sup>(<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R26#R26"><span style="color: black; text-decoration: none">26</span></a>). Aldosterone-producing adrenocortical carcinomas present<sup> </sup>with hypertensionand pronounced hypokalemia (mean serum potassium<sup> </sup>2.3 ± 0.08 mmol/liter) (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R27#R27"><span style="color: black; text-decoration: none">27</span></a>). However, severe hypokalemia<sup> </sup>is more likely caused by grossly elevated cortisol secretion,<sup> </sup>leading to insufficient renal cortisol inactivation by 11ß-hydroxysteroid<sup> </sup>dehydrogenase type 2 with consecutive activation of the mineralocorticoid<sup> </sup>receptor.<sup> </sup><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">In many patients with a seemingly hormonally inactive ACC, high<sup> </sup>concentrations of steroid precursors like androstenedione or<sup> </sup>17<!--[if gte vml 1]><v:shapetype  id="_x0000_t75" coordsize="21600,21600" o:spt="75" o:preferrelative="t"  path="m@4@5l@4@11@9@11@9@5xe" filled="f" stroked="f">  <v:stroke joinstyle="miter"/>  <v:formulas>   <v:f eqn="if lineDrawn pixelLineWidth 0"/>   <v:f eqn="sum @0 1 0"/>   <v:f eqn="sum 0 0 @1"/>   <v:f eqn="prod @2 1 2"/>   <v:f eqn="prod @3 21600 pixelWidth"/>   <v:f eqn="prod @3 21600 pixelHeight"/>   <v:f eqn="sum @0 0 1"/>   <v:f eqn="prod @6 1 2"/>   <v:f eqn="prod @7 21600 pixelWidth"/>   <v:f eqn="sum @8 21600 0"/>   <v:f eqn="prod @7 21600 pixelHeight"/>   <v:f eqn="sum @10 21600 0"/>  </v:formulas>  <v:path o:extrusionok="f" gradientshapeok="t" o:connecttype="rect"/>  <o:lock v:ext="edit" aspectratio="t"/> </v:shapetype><v:shape id="_x0000_i1025" type="#_x0000_t75" alt="{alpha}"  style='width:4.5pt;height:4.5pt'>  <v:imagedata src="file:///C:\DOCUME~1\IMRANB~1\LOCALS~1\Temp\msohtml1\01\clip_image001.png"   o:href="http://jcem.endojournals.org/math/agr.gif"/> </v:shape><![endif]--><!--[if !vml]--><img src="file:///C:/DOCUME%7E1/IMRANB%7E1/LOCALS%7E1/Temp/msohtml1/01/clip_image002.gif" alt="{alpha}" v:shapes="_x0000_i1025" border="0" height="6" width="6" /><!--[endif]-->-hydroxyprogesterone can often be demonstrated, thereby establishing<sup> </sup>the adrenocortical origin of the tumor.<sup> </sup><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">Hormonally inactive ACCs usually present with abdominal discomfort<sup> </sup>(nausea, vomiting, abdominal fullness) or back pain caused by<sup> </sup>a mass effect of the large tumor. In the Italian survey on adrenal<sup> </sup>incidentaloma, the occurrence of pain was significantly associated<sup> </sup>with ACC and was not fully explained by large tumor size <em>per<sup> </sup>se</em> (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R28#R28"><span style="color: black; text-decoration: none">28</span></a>). However, an increasing percentage of ACCs is discovered<sup> </sup>as incidentaloma during abdominal imaging (<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R28#R28"><span style="color: black; text-decoration: none">28</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R29#R29"><span style="color: black; text-decoration: none">29</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R30#R30"><span style="color: black; text-decoration: none">30</span></a>, <a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#R31#R31"><span style="color: black; text-decoration: none">31</span></a>).<sup> </sup><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">Only occasionally patients present with fever, weight loss,<sup> </sup>and anorexia, and it is a remarkable feature of non-cortisol-producing<sup> </sup>ACC that well-being is often little affected by even a large<sup> </sup>tumor burden.<sup> </sup><o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><a name="SEC4"></a><em><span style="font-size: 10pt; color: black">Hormonal work-up</span></em><span style="font-size: 10pt; color: black"> <o:p></o:p></span></p>
<p class="MsoNormal" style="text-align: justify"><span style="font-size: 10pt; color: black">Careful endocrine assessment is mandatory prior to surgery in<sup> </sup>ACC (Table 1<a href="http://jcem.endojournals.org/cgi/content/full/91/6/2027#T1#T1"><span style="color: black; text-decoration: none"><!--[if gte vml 1]><v:shape  id="_x0000_i1026" type="#_x0000_t75" alt="Go"  href="http://jcem.endojournals.org/cgi/content/full/91/6/202#T1#T" style='width:4.5pt;  height:4.5pt' o:button="t">  <v:imagedata src="file:/