Synthesis and biological evaluation of rapamycin-derived, next generation small molecules.

Shiva Krishna Reddy Guduru, Prabhat Arya
Author Information
  1. Shiva Krishna Reddy Guduru: Center for Drug Discovery , Department of Pharmacology and Chemical Biology , Baylor College of Medicine , One Baylor Plaza , Houston , Texas 77030 , USA . Email: gskreddy.chem@gmail.com ; Email: Shiva.Guduru@bcm.edu ; Tel: +1 713 798 8794. ORCID
  2. Prabhat Arya: Chemistry and Chemical Biology , Dr. Reddy's Institute of Life Sciences (DRILS) , University of Hyderabad Campus , Hyderabad 500046 , India.

Abstract

Over the years, rapamycin has attracted serious attention due to its remarkable biological properties and as a potent inhibitor of the mammalian target of rapamycin (mTOR) protein through its binding with FKBP-12. Several efficient strategies that utilize synthetic and biosynthetic approaches have been utilized to develop small molecule rapamycin analogs or for synthesizing hybrid compounds containing a partial rapamycin structure to improve pharmacokinetic properties. Herein, we report selected case studies related to the synthesis of rapamycin-derived compounds and hybrid molecules to explore their biological properties.

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