Figure 13.1 Some histologic subtypes of kidney cancer. (A) Clear cell carcinoma with sarcomatoid differentiation. (B) Papillary renal cell carcinoma. (C) Collecting duct carcinoma. (D) Chromophobe carcinoma. (E) Mucinous tubular and spindle cell carcinoma.

Source: Courtesy of Dr. Thomas Wheeler.

VON HIPPEL–LINDAU SYNDROME

VHL is an inherited, autosomal dominant syndrome caused by a germline mutation in the VHL gene, a tumor suppressor gene located in chromosome 3p. The two hit hypothesis plays a role in pathogenesis. Inheritance of an ineffective VHL allele from a 83parent or a de novo mutation of one allele and further deactivation of second allele lead to cyst formation and tumorigenesis.

VHL mutations are associated with a wide range of tumors, including hemangioblastomas of the brain (mainly cerebellum and spine), which is the most common type of tumor, retinal angioma, clear cell variant of RCC, pheochromocytoma, endolymphatic tumors of the middle ear, serous cystadenoma, neuroendocrine tumors of the pancreas, and papillary cystadenoma of the epididymis and broad ligament.

The VHL syndrome can be further divided into type 1 and type 2 depending on mutations and the tendency to develop certain tumors. Type 1 patients have a lower risk of pheochromocytoma. Type 2 patients have a higher risk of pheochromocytoma and can be further subclassified into type 2A with high risk of RCC, type 2B with low risk of RCC, and type 2C with only pheochromocytomas without RCC or hemangiomas.

RCC associated with VHL is invariably of the clear cell subtype and tends to be bilateral and multifocal. It usually presents before age 60. VHL gene mutation is also seen in sporadic cases of RCC. VHL gene inactivation leads to upregulation of hypoxia-inducible factors (HIF), which in turn regulates downstream vascular endothelial growth factor (VEGF) that promotes angiogenesis and proliferation. Understanding the VHL gene mutations has opened doors toward targeted treatment of VEGF in the treatment of RCC.

The management of VHL is focused on early diagnosis and appropriate intervention via thorough history taking, familial genetic screening, routine imaging, and timely surgical removal of tumor. RCC less than 3 cm in size have a low rate of metastasis and can be monitored with close surveillance. Tumors more than 3 cm require immediate surgical intervention. Nephron sparing surgery is recommended whenever possible, since tumors are often bilateral. There are ongoing trials of VEGF inhibitors in VHL patients.

HEREDITARY PAPILLARY RENAL CELL CARCINOMA

Hereditary papillary renal cell carcinoma (HPRCC) is a rare autosomal dominant familial cancer syndrome associated with the development of type I papillary renal carcinomas. 84Lesions are bilateral and multifocal like other hereditary RCCs. HPRCC is caused by the HPRC gene, MET proto-oncogene, also known as hepatocyte growth factor receptor, which is located on the long arm of chromosome 7. MET gene mutation is also seen in 10% of sporadic papillary renal carcinomas.

HEREDITARY LEIOMYOMATOSIS AND RENAL CELL CARCINOMA

Hereditary leiomyomatosis and renal cell carcinoma (HLRCC) is an autosomal dominant familial cancer syndrome characterized by development of leiomyomas of the uterus and skin, and RCC. Type II papillary carcinoma is the most common tumor associated with HLRCC, but tumors of collecting ducts and chromophobe carcinomas are also seen. RCCs occur at an early age and are usually bilateral and aggressive in nature. Tumors have a high propensity to metastasize, even when as small as 1 cm in size. Uterine leiomyomas can be severe and present in up to 90% of women with HLRCC before the age of 30. Cutaneous leiomyomas are benign painful pinkish nodules of the skin, which can be disseminated throughout the body. A mutation in the fumarate hydratase gene (FH gene), which converts fumarate to malate in the Krebs cycle, is responsible for HLRCC.

BIRT–HOGG–DUBÉ SYNDROME

Birt–Hogg–Dubé syndrome (BHD) is an autosomal dominant disorder characterized by benign skin hamartomas, lung cysts and spontaneous pneumothorax, and RCC. BHD syndrome is caused by germline mutations in the folliculin gene (FLCN) located on chromosome 17p11.2, which encodes the protein folliculin. As many as 149 mutations of the FLCN gene have been identified in BHD syndrome. Skin manifestations are the earliest and most frequent manifestation of BHD syndrome. Renal cancer can occur around age 50 and is associated with different histologic subtypes, most commonly chromophobe carcinoma. Renal oncocytosis has been reported in BHD. There is also an association between BHD syndrome and colon polyposis and colorectal carcinoma.

85POLYCYSTIC KIDNEY DISEASE

Polycystic kidney disease (PCKD) is a very common autosomal dominant disorder, occurring in approximately one in every 400 to 1,000 live births. RCCs in PCKD are often bilateral and multifocal, and one third are sarcomatoid type. The risk of RCC in PCKD is found to be equal to that of the general population.

TUBEROUS SCLEROSIS COMPLEX

Tuberous sclerosis complex (TSC) is an autosomal dominant disorder characterized by the formation of hamartomas in multiple organs including brain, kidney, lung, and skin. TSC is caused by mutations in one of the tumor-suppressor gene products, hamartin (TSC1) or tuberin (TSC2). The clinical manifestations include bilateral, multifocal renal lesions, which typically are angiomyolipomas. Less than 5% of patients with TSC develop RCC. This occurs at a younger age than sporadic tumors, with a female predilection. The most common histologic subtype seen in TSC is clear cell carcinoma.

PTEN HAMARTOMA TUMOR SYNDROME (COWDEN DISEASE)

Cowden disease is a rare autosomal dominant disorder causing formation of hamartomas in skin and various organs. It is associated with increased risk of tumors of breast, endometrium, and thyroid caused by mutation in the phosphatase and tensin homolog (PTEN) gene. Clear cell RCCs have been reported in patients with Cowden disease, and they usually present at a late stage.

OTHER FAMILIAL CANCER SYNDROMES WITH INCREASED RISK OF RCC

Succinate dehydrogenase (SDH) gene associated familial cancer syndrome is one of the Krebs cycle enzyme disorders. It has been reported to increase the risk of RCC in addition to 86hereditary paraganglioma and pheochromocytoma. Various histologic subtypes of RCC are implicated and they are usually aggressive in nature.

BAP1 (BRCA-associated protein 1) mutation in the germline predisposes to familial renal cancer and uveal and cutaneous melanomas. BAP1 is associated with a higher tumor grade and worse overall survival. Clear cell RCCs are most commonly seen.

Chromosome 3 translocation has been identified in a familial RCC as Cohen et al. reported in 1979. Multiple genes including VHL and BAP1 are located on chromosome 3p, and thus translocation and loss of alleles predispose to increased risk of RCC.