Versatile pathway-centric approach based on high-throughput sequencing to anticancer drug discovery

  • Hairi Li
  • , Hongyan Zhou
  • , Dong Wang
  • , Jinsong Qiu
  • , Yu Zhou
  • , Xiangqiang Li
  • , Michael G. Rosenfeld
  • , Sheng Ding
  • , Xiang Dong Fu

Research output: Contribution to journalArticlepeer-review

72 Scopus citations

Abstract

The advent of powerful genomics technologies has uncovered many fundamental aspects of biology, including the mechanisms of cancer; however, it has not been appropriately matched by the development of global approaches to discover new medicines against human diseases. Here we describe a unique high-throughput screening strategy by high-throughput sequencing, referred to as HTS 2, to meet this challenge. This technology enables large-scale and quantitative analysis of gene matrices associated with specific disease phenotypes, therefore allowing screening for small molecules that can specifically intervene with disease-linked gene-expression events. By initially applying this multitarget strategy to the pressing problem of hormone-refractory prostate cancer, which tends to be accelerated by the current antiandrogen therapy, we identify Peruvoside, a cardiac glycoside, which can potently inhibit both androgen-sensitive and -resistant prostate cancer cells without triggering severe cytotoxicity. We further show that, despite transcriptional reprogramming in prostate cancer cells at different disease stages, the compound can effectively block androgen receptor-dependent gene expression by inducing rapid androgen receptor degradation via the proteasome pathway. These findings establish a genomics-based phenotypic screening approach capable of quickly connecting pathways of phenotypic response to the molecular mechanism of drug action, thus offering a unique pathway-centric strategy for drug discovery.

Original languageEnglish
Pages (from-to)4609-4614
Number of pages6
JournalProceedings of the National Academy of Sciences of the United States of America
Volume109
Issue number12
DOIs
StatePublished - 20 Mar 2012
Externally publishedYes

Keywords

  • Chemical screening
  • Gene signature

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