Gatorbulin-1, a distinct cyclodepsipeptide chemotype, targets a seventh tubulin pharmacological site

Author:

Matthew SusanORCID,Chen Qi-YinORCID,Ratnayake RanjalaORCID,Fermaintt Charles S.ORCID,Lucena-Agell DanielORCID,Bonato Francesca,Prota Andrea E.,Lim Seok TingORCID,Wang XiaomengORCID,Díaz J. FernandoORCID,Risinger April L.ORCID,Paul Valerie J.ORCID,Oliva Maria ÁngelaORCID,Luesch HendrikORCID

Abstract

Tubulin-targeted chemotherapy has proven to be a successful and wide spectrum strategy against solid and liquid malignancies. Therefore, new ways to modulate this essential protein could lead to new antitumoral pharmacological approaches. Currently known tubulin agents bind to six distinct sites at α/β-tubulin either promoting microtubule stabilization or depolymerization. We have discovered a seventh binding site at the tubulin intradimer interface where a novel microtubule-destabilizing cyclodepsipeptide, termed gatorbulin-1 (GB1), binds. GB1 has a unique chemotype produced by a marine cyanobacterium. We have elucidated this dual, chemical and mechanistic, novelty through multidimensional characterization, starting with bioactivity-guided natural product isolation and multinuclei NMR-based structure determination, revealing the modified pentapeptide with a functionally critical hydroxamate group; and validation by total synthesis. We have investigated the pharmacology using isogenic cancer cell screening, cellular profiling, and complementary phenotypic assays, and unveiled the underlying molecular mechanism by in vitro biochemical studies and high-resolution structural determination of the α/β-tubulin−GB1 complex.

Funder

HHS | NIH | National Cancer Institute

HHS | NIH | National Institute of General Medical Sciences

Debbie and Sylvia DeSantis Chair professorship

Ministerio de Ciencia e Innovación

Fondo de Investigaciones Sanitarias

European Union

MINECO | Consejo Superior de Investigaciones Científicas

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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