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The Crosstalk between Src and Hippo/YAP Signaling Pathways in Non-Small Cell Lung Cancer (NSCLC).

Authors :
Hsu, Ping-Chih
Hsu, Ping-Chih
Yang, Cheng-Ta
Jablons, David M
You, Liang
Hsu, Ping-Chih
Hsu, Ping-Chih
Yang, Cheng-Ta
Jablons, David M
You, Liang
Source :
Cancers; vol 12, iss 6, E1361; 2072-6694
Publication Year :
2020

Abstract

The advancement of new therapies, including targeted therapies and immunotherapies, has improved the survival of non-small-cell lung cancer (NSCLC) patients in the last decade. Some NSCLC patients still do not benefit from therapies or encounter progressive disease during the course of treatment because they have intrinsic resistance, acquired resistance, or lack a targetable driver mutation. More investigations on the molecular biology of NSCLC are needed to find useful biomarkers for current therapies and to develop novel therapeutic strategies. Src is a non-receptor tyrosine kinase protein that interacts with cell surface growth factor receptors and the intracellular signaling pathway to maintain cell survival tumorigenesis in NSCLC. The Yes-associated protein (YAP) is one of the main effectors of the Hippo pathway and has been identified as a promoter of drug resistance, cancer progression, and metastasis in NSCLC. Here, we review studies that have investigated the activation of YAP as mediated by Src kinases and demonstrate that Src regulates YAP through three main mechanisms: (1) direct phosphorylation; (2) the activation of pathways repressing Hippo kinases; and (3) Hippo-independent mechanisms. Further work should focus on the efficacy of Src inhibitors in inhibiting YAP activity in NSCLC. In addition, future efforts toward developing potentially reasonable combinations of therapy targeting the Src-YAP axis using other therapies, including targeted therapies and/or immunotherapies, are warranted.

Details

Database :
OAIster
Journal :
Cancers; vol 12, iss 6, E1361; 2072-6694
Notes :
application/pdf, Cancers vol 12, iss 6, E1361 2072-6694
Publication Type :
Electronic Resource
Accession number :
edsoai.on1367400441
Document Type :
Electronic Resource