AI Article Synopsis

  • Molecular profiling of rare urothelial cancers has been limited due to a lack of targeted therapies, but this study explores two specific cases: an invasive sarcomatoid carcinoma and a poorly differentiated carcinoma with some neuroendocrine features.
  • In both cases, mutations in key genes were identified, highlighting important mechanisms like chromatin remodeling and cell cycle control that are common in bladder cancer.
  • The findings suggest that specific mutations could help classify these aggressive cancer subtypes more accurately and may have potential implications for future treatments.

Article Abstract

Molecular profiling of urothelial cancers for therapeutic and prognostic potential has been very limited due to the absence of cancer-specific targeted therapies. We describe here 2 clinical cases with a histological diagnosis of an invasive sarcomatoid and a poorly differentiated carcinoma favoring urothelial with some neuroendocrine differentiation, two of the rarer types of urothelial cancers, which were evaluated for mutations in 212 genes for single-nucleotide variants and copy-number variants and 53 genes for fusions associated with solid tumors. In both cases, we identified variants in 2 genes, and , indicative of the role of dysregulation of chromatin remodeling and cell cycle control as being common features of bladder cancer, consistent with the proposed model of tumorigenesis in these rare, highly aggressive pathological subtypes. The presence of a mutation in the poorly differentiated cancer and a 3 mutation in the sarcomatoid tumor is indicative of a distinctive profile and adds a potential layer of molecular stratification to these rarer histological subtypes. We present a comparative analysis of the histological, clinical, and molecular profile of both cases and discuss the potential to delineate these tumors at the molecular level keeping in mind the possible therapeutic implications.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5903146PMC
http://dx.doi.org/10.1159/000487882DOI Listing

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