AI Article Synopsis

  • Primary liver cancer shows significant variation in causes, tissue structure, and treatment responses; understanding this can aid personalized treatments.
  • The study analyzed 259 liver cancer samples from Japanese patients, focusing on protein profiling, genetic mutations, and gene expression to uncover molecular differences.
  • Researchers identified three proteomic subclasses of tumors (R1, R2, R3) with distinct characteristics and prognoses, proposing 22 proteins as potential markers for better treatment decisions.

Article Abstract

Primary liver cancer is a heterogeneous disease in terms of its etiology, histology, and therapeutic response. Concurrent proteomic and genomic characterization of a large set of clinical liver cancer samples can help elucidate the molecular basis of heterogeneity and thus serve as a valuable resource for personalized liver cancer treatment. In this study, we perform proteomic profiling of ~300 proteins on 259 primary liver cancer tissues with reverse-phase protein arrays, mutational analysis using whole genome sequencing and transcriptional analysis with RNA-Seq. Patients are of Japanese ethnic background and mainly HBV or HCV positive, providing insight into this important liver cancer subtype. Unsupervised classification of tumors based on protein expression profiles reveal three proteomic subclasses R1, R2, and R3. The R1 subclass is immunologically hot and demonstrated a good prognosis. R2 contains advanced proliferative tumor with TP53 mutations, high expression of VEGF receptor 2 and the worst prognosis. R3 is enriched with CTNNB1 mutations and elevated mTOR signaling pathway activity. Twenty-two proteins, including CDK1 and CDKN2A, are identified as potential prognostic markers. The proteomic classification presented in this study can help guide therapeutic decision making for liver cancer treatment.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9617926PMC
http://dx.doi.org/10.1038/s41467-022-34249-xDOI Listing

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