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Up-regulation of neogenin-1 increases cell proliferation and motility in gastric cancer.


ABSTRACT: Although elevated expression of neogenin-1 has been detected in human gastric cancer tissue, its role in gastric tumorigenesis remains unclear due to the lack of neogenin-1 studies in cancer. Therefore, we demonstrated here the function and regulatory mechanism of neogenin-1 in gastric cancer. Neogenin-1 ablation decreased proliferation and migration of gastric cancer cells, whereas its over-expression reversed these effects. Xenografted analyses using gastric cancer cells displayed statistically significant inhibition of tumor growth by neogenin-1 depletion. Interestingly, galectin-3 interacted with HSF-1 directly, which facilitated nuclear-localization and binding on neogenin-1 promoter to drive its transcription and gastric cancer cell motility. The galectin-3-increased gastric cancer cell motility was down-regulated by HSF-1 depletion. Moreover, the parallel expression patterns of galectin-3 and neogenin-1, as well as those of HSF-1 and neogenin-1, were detected in the malignant tissues of gastric cancer patients. Taken together, high-expression of neogenin-1 promotes gastric cancer proliferation and motility and its expression is regulated by HSF-1 and galectin-3 interaction. In addition, we propose further studies for neogenin-1 and its associated pathways to provide them as a proper target for gastric cancer therapy.

SUBMITTER: Kim SJ 

PROVIDER: S-EPMC4102817 | biostudies-other | 2014 May

REPOSITORIES: biostudies-other

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Up-regulation of neogenin-1 increases cell proliferation and motility in gastric cancer.

Kim Seok-Jun SJ   Wang Yuan-Guo YG   Lee Hyun-Woo HW   Kang Hyeok Gu HG   La Sun-Hyuk SH   Choi Il Ju IJ   Irimura Tatsuro T   Ro Jae Y JY   Bresalier Robert S RS   Chun Kyung-Hee KH  

Oncotarget 20140501 10


Although elevated expression of neogenin-1 has been detected in human gastric cancer tissue, its role in gastric tumorigenesis remains unclear due to the lack of neogenin-1 studies in cancer. Therefore, we demonstrated here the function and regulatory mechanism of neogenin-1 in gastric cancer. Neogenin-1 ablation decreased proliferation and migration of gastric cancer cells, whereas its over-expression reversed these effects. Xenografted analyses using gastric cancer cells displayed statisticall  ...[more]

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