4.6 Review

Pharmacology of Modulators of Alternative Splicing

Journal

PHARMACOLOGICAL REVIEWS
Volume 69, Issue 1, Pages 63-79

Publisher

AMER SOC PHARMACOLOGY EXPERIMENTAL THERAPEUTICS
DOI: 10.1124/pr.115.011239

Keywords

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Funding

  1. MRC [MR/N01247X/1, MR/L01985X/1, MR/K020366/1, MR/K013157/1]
  2. BBSRC [BB/J007293/1]
  3. BHF [PG/15/53/31371]
  4. ARUK [20400]
  5. Biotechnology and Biological Sciences Research Council [BB/J007293/1, BB/J007293/2, BB/P012035/1] Funding Source: researchfish
  6. British Heart Foundation [PG/15/53/31371] Funding Source: researchfish
  7. Medical Research Council [MR/K013157/1, MR/K020366/1, MR/N01247X/1] Funding Source: researchfish
  8. BBSRC [BB/J007293/2, BB/P012035/1, BB/J007293/1] Funding Source: UKRI
  9. MRC [MR/L01985X/1, MR/K020366/1, MR/N01247X/1, MR/K013157/1] Funding Source: UKRI

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More than 95% of genes in the human genome are alternatively spliced to form multiple transcripts, often encoding proteins with differing or opposing function. The control of alternative splicing is now being elucidated, and with this comes the opportunity to develop modulators of alternative splicing that can control cellular function. A number of approaches have been taken to develop compounds that can experimentally, and sometimes clinically, affect splicing control, resulting in potential novel therapeutics. Here we develop the concepts that targeting alternative splicing can result in relatively specific pathway inhibitors/activators that result in dampening down of physiologic or pathologic processes, from changes in muscle physiology to altering angiogenesis or pain. The targets and pharmacology of some of the current inhibitors/activators of alternative splicing are demonstrated and future directions discussed.

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