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Genomic Mapping of Splicing-Related Genes Identify Amplifications in , and in Luminal Breast Cancer. | LitMetric

AI Article Synopsis

  • The study investigates alternative splicing and its impact on the diversity of the transcriptome in breast cancer, focusing on 304 splicing pathway-related genes using data from breast cancer patients in the TCGA dataset.* -
  • A significant number of genetic alterations were found, especially copy number alterations (CNAs), with some genes showing high amplification in various breast cancer subtypes, impacting prognosis in the Luminal subtype.* -
  • The research identifies three novel oncogenic genes that can be inhibited using BET inhibitors, resulting in decreased cell proliferation, indicating potential therapeutic avenues for breast cancer treatment.*

Article Abstract

Alternative splicing is an essential biological process, which increases the diversity and complexity of the human transcriptome. In our study, 304 splicing pathway-related genes were evaluated in tumors from breast cancer patients (TCGA dataset). A high number of alterations were detected, including mutations and copy number alterations (CNAs), although mutations were less frequently present compared with CNAs. In the four molecular subtypes, 14 common splice genes showed high level amplification in >5% of patients. Certain genes were only amplified in specific breast cancer subtypes. Most altered genes in each molecular subtype clustered to a few chromosomal regions. In the Luminal subtype, amplifications of , , and showed a strong significant association with prognosis. An even more robust association with OS and RFS was observed when expression of these three genes was combined. Inhibition of , , and , using siRNA in MCF7 and T47D cells, showed a decrease in cell proliferation. The mRNA expression of these genes was reduced by treatment with BET inhibitors, a family of epigenetic modulators. We map the presence of splicing-related genes in breast cancer, describing three novel genes, , , and , that have an oncogenic role and can be modulated with BET inhibitors.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8391113PMC
http://dx.doi.org/10.3390/cancers13164118DOI Listing

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