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September 10, 2025Open Access

“Targeted Therapies and their Associated Molecular Alterations in the Treatment of Renal Cell Carcinoma”

Key Points

Targeted therapies improve outcomes for renal cell carcinoma patients, particularly those with ccRCC and VHL mutations.
Clear cell RCC (ccRCC) accounts for approximately 75% of cases, primarily driven by VHL gene mutations, impacting treatment effectiveness.
Histological analysis reveals clear cell cytology and strong vascularization in ccRCC, guiding targeted therapy decisions.
Loss of VHL gene function significantly contributes to tumor growth, indicating a critical therapeutic target in ccRCC management.

Abstract

Renal cell carcinoma, (RCC) the most prevalent of kidney cancers, is a relatively common cancer, constituting approximately 10% of all cancers in adults. Many molecular subtypes have been characterized for RCC, the most common being clear cell RCC, or ccRCC, which occurs in close to 75% of cases, and has a strong association with mutations in the von Hippel-Lindau (VHL) tumor suppressor gene 1. ccRCC constitutes close to 80% of metastatic presentations. Histology shows acinar growth and clear cell cytology, surrounded by a rich vasculature. Having a strong association with mutations in the von Hippel-Lindau tumor suppressor gene, ccRCC exhibits loss of VHL gene by 3p chromosomal loss at the 3p25 locus. Another histologic subtype includes non clear cell renal cell carcinoma nccRCC. Somatic ccRCC is characterized by inactivation of the protein products of VHL (pVHL), which promotes transcription of genes implicated in tumor formation and growth 1.

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