Semaphorin3F Down-Regulates the Expression of Integrin αvβ3 and Sensitizes Multicellular Tumor Spheroids to Chemotherapy via the Neuropilin-2 Receptor in vitro

Background: Multicellular resistance (MCR), i.e. decreased sensitivity to anticancer drugs compared with common monolayer cell (MC) cultures, depends partly on tumor cell-cell adhesion. Previous studies have shown that anti-adhesive therapies, including integrin α v , β 1 and α v β 3 targeting, indu...

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Veröffentlicht in:Chemotherapy (Basel) 2009, Vol.55 (5), p.344-352
Hauptverfasser: Zheng, Chenhong, Zhou, Qi, Wu, Feng, Peng, Qiuping, Tang, Airong, Liang, Houjie, Zeng, Yanjun
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container_end_page 352
container_issue 5
container_start_page 344
container_title Chemotherapy (Basel)
container_volume 55
creator Zheng, Chenhong
Zhou, Qi
Wu, Feng
Peng, Qiuping
Tang, Airong
Liang, Houjie
Zeng, Yanjun
description Background: Multicellular resistance (MCR), i.e. decreased sensitivity to anticancer drugs compared with common monolayer cell (MC) cultures, depends partly on tumor cell-cell adhesion. Previous studies have shown that anti-adhesive therapies, including integrin α v , β 1 and α v β 3 targeting, induced apoptosis and reversed the sensitivity of MCR. Methods: A model of three-dimensional cell culture was used to establish HT29 multicellular spheroid cells (MCS) and explore the effect of semaphorin3F (Sema3F) on integrin-mediated cell-cell interactions in MCS of a human colorectal adenocarcinoma cell line (HT29) and sensitization of HT29 MCS to 5-fluorouracil and oxaliplatin via a decrease in integrin α v β 3 . Results: Elevated expression of Sema3F led to the up-regulation neuropilin-2 (Nrp2) receptor expression and the down-regulation of integrin α v β 3 expression. Furthermore, short interfering RNA of Nrp2 could reverse MCR. Conclusion: Our study demonstrates that Sema3F can sensitize MCR by decreasing integrin α v β 3 expression via the Nrp2 receptor.
doi_str_mv 10.1159/000232449
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title Semaphorin3F Down-Regulates the Expression of Integrin αvβ3 and Sensitizes Multicellular Tumor Spheroids to Chemotherapy via the Neuropilin-2 Receptor in vitro
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