AI Article Synopsis

  • Genomic research in hepatocellular carcinoma (HCC) has identified genetic variations that could influence treatment decisions, but larger clinical validations are needed to ensure these targets improve patient survival.
  • In a study involving 111 Chinese HCC patients, significant gene variations were found, with about 50% carrying mutations that could guide targeted therapies.
  • The study linked specific mutations to prognosis, revealing that while some mutations correlate with worse survival, the presence of mutant MUC16 may actually serve as an independent protective factor after surgery.

Article Abstract

Hepatocellular carcinoma (HCC) genomic research has discovered actionable genetic changes that might guide treatment decisions and clinical trials. Nonetheless, due to a lack of large-scale multicenter clinical validation, these putative targets have not been converted into patient survival advantages. So, it's crucial to ascertain whether genetic analysis is clinically feasible, useful, and whether it can be advantageous for patients. We sequenced tumour tissue and blood samples (as normal controls) from 111 Chinese HCC patients at Qingdao University Hospital using the 508-gene panel and the 688-gene panel, respectively. Approximately 95% of patients had gene variations related to targeted treatment, with 50% having clinically actionable mutations that offered significant information for targeted therapy. Immune cell infiltration was enhanced in individuals with TP53 mutations but decreased in patients with CTNNB1 and KMT2D mutations. More notably, we discovered that SPEN, EPPK1, and BRCA2 mutations were related to decreased median overall survival, although MUC16 mutations were not. Furthermore, we found mutant MUC16 as an independent protective factor for the prognosis of HCC patients after curative hepatectomy. In conclusion, this study connects genetic abnormalities to clinical practice and potentially identifies individuals with poor prognoses who may benefit from targeted treatment or immunotherapy.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11145829PMC
http://dx.doi.org/10.1186/s12885-024-12407-2DOI Listing

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