KLI

Targeting isoforms of RON kinase (MST1R) drives antitumor efficacy

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Abstract
Recepteur d’origine nantais (RON, MST1R) is a single-span transmembrane receptor tyrosine kinase (RTK) aberrantly expressed in numerous cancers, including various solid tumors. How naturally occurring splicing isoforms of RON, especially those which are constitutively activated, affect tumorigenesis and therapeutic response, is largely unknown. Here, we identified that presence of activated RON could be a possible factor for the development of resistance against anti-EGFR (cetuximab) therapy in colorectal cancer patient tissues. Also, we elucidated the roles of three splicing variants of RON, RON Δ155, Δ160, and Δ165 as tumor drivers in cancer cell lines. Subsequently, we designed an inhibitor of RON, WM-S1-030, to suppress phosphorylation thereby inhibiting the activation of the three RON variants as well as the wild type. Specifically, WM-S1-030 treatment led to potent regression of tumor growth in solid tumors expressing the RON variants Δ155, Δ160, and Δ165. Two mechanisms for the RON oncogenic activity depending on KRAS genotype was evaluated in our study which include activation of EGFR and Src, in a trimeric complex, and stabilization of the beta-catenin. In terms of the immunotherapy, WM-S1-030 elicited notable antitumor immunity in anti-PD-1 resistant cell derived mouse model, likely via repression of M1/M2 polarization of macrophages. These findings suggest that WM-S1-030 could be developed as a new treatment option for cancer patients expressing these three RON variants.
Issued Date
2023
Joseph Kim
Dong-In Koh
Minki Lee
Yoon Sun Park
Seung-Woo Hong
Jae-Sik Shin
Mi So Lee
Min-Hwa Kim
Jun Hyung Lee
Joonyee Jeong
Seunggeon Bae
Jun Ki Hong
Hong-Rae Jeong
Yea Seong Ryu
Seung-Mi Kim
Mingee Choi
Hyojin Kim
Hyun Ryu
Sun-Chul Hur
Junho Park
Dae Young Hur
Dong-Hoon Jin
Type
Article
DOI
10.1038/s41418-023-01235-9
URI
https://oak.ulsan.ac.kr/handle/2021.oak/16204
Publisher
CELL DEATH AND DIFFERENTIATION
Language
한국어
ISSN
1350-9047
Citation Volume
12
Citation Number
0
Citation Start Page
2491
Citation End Page
2507
Appears in Collections:
Medicine > Nursing
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