Targeting yes-associated protein to overcome imatinib resistance in gastrointestinal stromal tumor drug-tolerant persister cells
Takashi Yokouchi, Tsuyoshi Takahashi, Toshirou Nishida, Koji Tanaka, Yukinori Kurokawa, Kazuyoshi Yamamoto, Takuro Saito, Takaomi Hagi, Kota Momose, Kotaro Yamashita, Tomoki Makino, Kunihiko Kawai, Satoshi Serada, Minoru Fujimoto, Seiichi Hirota, Kiyokazu Nakajima, Tetsuji Naka

TL;DR
This study shows that targeting YAP can help overcome imatinib resistance in gastrointestinal stromal tumor cells that survive treatment.
Contribution
The study identifies YAP as a key player in drug-tolerant persister cells and proposes a combination therapy with YAP inhibitors.
Findings
YAP activity is elevated in imatinib-resistant persister cells and is localized in the nucleus.
Combining imatinib with YAP inhibitors like verteporfin significantly reduces persister cell survival.
In mouse models, the combination therapy delays tumor regrowth after treatment stops.
Abstract
The tyrosine kinase inhibitor (TKI) imatinib targets KIT and PDGFRA, offering significant therapeutic benefits in advanced gastrointestinal stromal tumors (GISTs). However, the high rate of recurrence following treatment discontinuation suggests that drug-tolerant persister cells (DTPs) may contribute to therapy resistance. Elucidating the mechanisms underlying DTP survival is critical for the development of curative strategies. This study aimed to investigate the role of yes-associated protein (YAP) in DTP survival and to evaluate the efficacy of combining imatinib with YAP inhibitors as a potential therapeutic approach. Imatinib-sensitive GIST cell lines were treated with imatinib to generate DTPs. YAP activity was assessed via western blotting, fluorescence immunostaining, and nuclear-cytoplasmic fractionation. Proliferation and apoptosis assays were conducted to evaluate…
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Taxonomy
TopicsGastrointestinal Tumor Research and Treatment · Platelet Disorders and Treatments · Sarcoma Diagnosis and Treatment
