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Crizotinib Inhibits Viability, Migration, and Invasion by Suppressing the c-Met/PI3K/Akt Pathway in the Three-Dimensional Bladder Cancer Spheroid Modelopen access

Authors
Song, ByeongdoKim, DanhyoHo, Jin-NyoungLe, Van-HungLee, Sangchul
Issue Date
Apr-2025
Publisher
MDPI
Keywords
crizotinib; 3D cell culture; spheroid; cisplatin-resistant bladder cancer; bladder cancer
Citation
Current Oncology, v.32, no.4, pp 1 - 13
Pages
13
Indexed
SCIE
SCOPUS
Journal Title
Current Oncology
Volume
32
Number
4
Start Page
1
End Page
13
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/207471
DOI
10.3390/curroncol32040236
ISSN
1198-0052
1718-7729
Abstract
We aimed to evaluate the therapeutic potential of crizotinib, a broad-spectrum tyrosine kinase inhibitor against bladder cancer (BC) cells, based on a three-dimensional (3D) cell culture system. After proliferating cell masses (spheroids) using T24 cisplatin-na & iuml;ve and T24R2 cisplatin-resistant human BC cell lines, the spheroids were exposed to various crizotinib concentrations in order to derive an ideal crizotinib concentration to suppress cell survival, migration, and invasion. Crizotinib suppressed cell proliferation, migration, and invasion in both T24 and T24R2 BC cell lines under a 3D spheroid model, which was more appropriate than the conventional two-dimensional cell culture model. Real-time quantitative polymerase chain reaction analysis revealed a reduced expression of E-cadherin and an enhanced expression of vimentin, suggesting EMT suppression and the subsequent suppression of tumor aggressiveness following crizotinib administration. Meanwhile, the expressions of apoptosis-related genes increased. Western blot analysis revealed that the expression levels of phosphorylated mesenchymal-epithelial transition factor (c-Met) and phosphorylated Akt decreased following crizotinib administration, suggesting that the antitumor effect of crizotinib can be associated with the inhibition of the phosphorylated activation of the c-Met/PI3K/Akt pathway. Crizotinib showed a potential antitumor effect on both cisplatin-na & iuml;ve and cisplatin-resistant human BC cells, likely through c-Met-induced PI3K/Akt pathway inhibition.
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서울 의과대학 (DEPARTMENT OF UROLOGY)
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