Targeting YAP Degradation by a Novel 1,2,4-Oxadiazole Derivative via Restoration of the Function of the Hippo Pathway

Dokla, Eman; Fang, Chun Sheng; Chu, Po Chen; Chang, Chih Shiang; Chen, Ching S.; Khaled A M Abouzid;

Abstract


Recent evidence has linked the dysregulation of the Hippo pathway to tumorigenesis and cancer progression due to its pivotal role in regulating the stability of the oncoprotein YAP. Based on an unexpected finding from the SAR study of a recently reported oxadiazole-based EGFR/c-Met dual inhibitor (compound 1), we identified a closely related derivative, compound 2, which exhibited cogent antitumor activities while devoid of compound 1's ability to promote EGFR/c-Met degradation. Compound 2 acted, in part, by facilitating YAP degradation through activation of its upstream kinase LATS1. However, it did not alter the phosphorylation status of MST1/2, a LATS1 kinase, suggesting an alternative mechanism for LATS1 activation. Orally administered compound 2 was effective in suppressing MDA-MB-231 xenograft tumor growth while exhibiting a satisfactory safety profile. From a therapeutic perspective, compound 2 might help foster new therapeutic strategies for cancer treatment by restoring the Hippo pathway regulatory function to facilitate YAP degradation.


Other data

Title Targeting YAP Degradation by a Novel 1,2,4-Oxadiazole Derivative via Restoration of the Function of the Hippo Pathway
Authors Dokla, Eman ; Fang, Chun Sheng; Chu, Po Chen; Chang, Chih Shiang; Chen, Ching S.; Khaled A M Abouzid 
Keywords Hippo pathway;YAP degradation;oxadiazole derivative;anticancer;LATS1 activation;chemical library screening;YAP/TAZ;MST2;PHOSPHORYLATION;KINASES;BETA
Issue Date 9-Apr-2020
Publisher AMER CHEMICAL SOC
Journal ACS Medicinal Chemistry Letters 
Volume 11
Issue 4
Start page 426
End page 432
ISSN 1948-5875
DOI 10.1021/acsmedchemlett.9b00501
PubMed ID 32292545
Scopus ID 2-s2.0-85083842959
Web of science ID WOS:000526402700005

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