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Small Molecule Inhibitors Targeting the “Undruggable” Survivin: The Past, Present, and Future from a Medicinal Chemist’s Perspective

Qingbin Cui, Caoqinglong Huang, Jingyuan Liu, Jian‐Ting Zhang

2023Journal of Medicinal Chemistry21 citationsDOIOpen Access PDF

Abstract

Survivin, a homodimeric protein and a member of the IAP family, plays a vital function in cell survival and cycle progression by interacting with various proteins and complexes. Its expression is upregulated in cancers but not detectable in normal tissues. Thus, it has been regarded and validated as an ideal cancer target. However, survivin is "undruggable" due to its lack of enzymatic activities or active sites for small molecules to bind/inhibit. Academic and industrial laboratories have explored different strategies to overcome this hurdle over the past two decades, with some compounds advanced into clinical testing. These strategies include inhibiting survivin expression, its interaction with binding partners and homodimerization. Here, we provide comprehensive analyses of these strategies and perspective on different small molecule survivin inhibitors to help drug discovery targeting "undruggable" proteins in general and survivin specifically with a true survivin inhibitor that will prevail in the foreseeable future.

Topics & Concepts

SurvivinSmall moleculeChemistryFunction (biology)Drug discoveryComputational biologyCancer researchPharmacologyBiochemistryCell biologyBiologyApoptosisCell death mechanisms and regulationCancer-related Molecular PathwaysProtein Degradation and Inhibitors