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This research investigates how AUTAC-mediated degradation of Mcl1 can turn resistance into vulnerability in multiple myeloma.

May 6, 2026

Turning adaptive resistance into vulnerability: AUTAC-Mediated degradation of Mcl1

Key Points

This research investigates how AUTAC-mediated degradation of Mcl1 can turn resistance into vulnerability in multiple myeloma.
Utilized U266B1 multiple myeloma xenograft model to assess tumor growth suppression.
Explored mechanisms of AUTAC-mediated degradation of Mcl1.
Analyzed the effects of cytoprotective autophagy on oncogenic factors.
Mcl1 degradation significantly suppresses tumor growth in the xenograft model.
Findings indicate that cytoprotective autophagy can be redirected to eliminate oncogenic survival factors.
Suggests a new strategy for enhancing lysosomal targeted protein degradation.

Abstract

and significantly suppresses tumor growth in a U266B1 multiple myeloma xenograft model. These findings reframe cytoprotective autophagy not as a resistance liability to be inhibited, but as an inducible degradation capacity that can be redirected to eliminate oncogenic survival factors, suggesting a generalizable strategy for amplifying lysosomal targeted protein degradation through controlled proteostasis stress.

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Turning adaptive resistance into vulnerability: AUTAC-Mediated degradation of Mcl1

Key Points

Abstract

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