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Simul-seq: combined DNA and RNA sequencing for whole-genome and transcriptome profiling. | LitMetric

AI Article Synopsis

  • Paired DNA and RNA profiling is used in genomics to study disease mechanisms and genotype-phenotype relationships, introducing a new technique called Simul-seq for effective sequencing from small samples.
  • Simul-seq was applied to esophageal adenocarcinoma tissue, revealing genetic features like aneuploidy and allele-specific expression that relate to cancer therapy responses.
  • This method not only identifies mutations in known cancer genes but also highlights a recurrent mutation in KIF3B that impacts kinesin-microtubule interactions, making it valuable for profiling limited clinical samples.

Article Abstract

Paired DNA and RNA profiling is increasingly employed in genomics research to uncover molecular mechanisms of disease and to explore personal genotype and phenotype correlations. Here, we introduce Simul-seq, a technique for the production of high-quality whole-genome and transcriptome sequencing libraries from small quantities of cells or tissues. We apply the method to laser-capture-microdissected esophageal adenocarcinoma tissue, revealing a highly aneuploid tumor genome with extensive blocks of increased homozygosity and corresponding increases in allele-specific expression. Among this widespread allele-specific expression, we identify germline polymorphisms that are associated with response to cancer therapies. We further leverage this integrative data to uncover expressed mutations in several known cancer genes as well as a recurrent mutation in the motor domain of KIF3B that significantly affects kinesin-microtubule interactions. Simul-seq provides a new streamlined approach for generating comprehensive genome and transcriptome profiles from limited quantities of clinically relevant samples.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5734913PMC
http://dx.doi.org/10.1038/nmeth.4028DOI Listing

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