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| Renal cell adenocarcinoma |
| Etiology Unknown. Evidence for genetic factors with association with von Hippel Lindau disease, an abnormality on chromosome 3. Evidence for environmental factors. |
| Pathogenesis Unknown. Proliferation of renal tubular cells., |
| Epidemiology Renal adenocarcinomas represent 1 to 3 precent of visceral cancers. Male to female ratio is about 2:1. Wide age range with peak incidence in the 6th decade of life. Seen in 20 to 50 percent of patients with von Hippel-Lindau disease. |
| General Gross Description Tumor may affect any region of the kidney. There is a predilection for the upper pole. On cut surface, the tumor may be bright yellow and this feature correlates with high lipid content. A geographic pattern to the cut surface is frequently seen due to ischemia, necrosis, and hemorrhage. Tumor-parenchymal interface is usually sharp. Large tumors may distort the calyces and pelvis Tumor can invade and exit the kidney as renal vein tumor thrombi. |
| General Microscopic Description Tumor cells may have abundant clear cytoplasm due to lipids and glycogen. Histologic patterns may be tubular, trabecular or solid. Tumor is graded on a scale from I to IV depending on cytologic nuclear features. A sarcomatoid variant is recognized which has a worse prognosis. |
| Clinical Correlation Patients may present with costovertebral angle pain, palpable mass and hematuria. Paraneoplastic clinical conditions include polycythemia, Cushings syndrome, feminization, masculinization, hypertension, and hypercalcemia. ization or masculinization. |
| References Cotran RS, Kumar V, Robbins SL: Robbins Pathologic Basis of Disease. 5th ed. Philadelphia, W.B. Saunders, 1994, pp. 986-987. Weiss LM et al: Adult renal epithelial neoplasmx, AJCP, 1995 (103) pp.624-635. |
| Renal cell adenocarcinoma |
| Synopsis by: Harold Yamase M.D. (T71000M83123)[196] |
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