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Sp1-driven up-regulation of miR-19a decreases RHOB and promotes pancreatic cancer.


ABSTRACT: Cancer treatment alters microRNA (miRNA) expression, revealing potential therapeutic targets (oncotarget). Here we treated pancreatic cancer (ASPC-1) cells with either recombinant human endostatin (rh-endostatin) or gemcitabine. Then high-throughput sequencing assay was performed to screen for altered miRNAs. Both treatments decreased levels of MiR-19a. We found that miR-19a stimulated cell proliferation, migration, invasion in vitro and tumor growth in vivo. High levels of miR-19a correlated with poor prognosis in patients. Ras homolog family member B (RHOB) was identified as a direct target of miR-19a. Furthermore, RHOB was down-regulated in human pancreatic cancer samples. Restoration of RHOB induced apoptosis, inhibited proliferation and migration of ASPC-1 cells. SP-1 was identified as an upstream transcription factor of miR-19a gene, promoting miR-19a transcription. Rh-endostatin decreased miR-19a expression by down-regulating SP-1. These findings suggest that miR-19a is a potential therapeutic target in pancreatic cancer.

SUBMITTER: Tan Y 

PROVIDER: S-EPMC4627316 | biostudies-literature | 2015 Jul

REPOSITORIES: biostudies-literature

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Sp1-driven up-regulation of miR-19a decreases RHOB and promotes pancreatic cancer.

Tan Yonggang Y   Yin Hongzhuan H   Zhang Heying H   Fang Jun J   Zheng Wei W   Li Dan D   Li Yue Y   Cao Wei W   Sun Cheng C   Liang Yusi Y   Zeng Juan J   Zou Huawei H   Fu Weineng W   Yang Xianghong X  

Oncotarget 20150701 19


Cancer treatment alters microRNA (miRNA) expression, revealing potential therapeutic targets (oncotarget). Here we treated pancreatic cancer (ASPC-1) cells with either recombinant human endostatin (rh-endostatin) or gemcitabine. Then high-throughput sequencing assay was performed to screen for altered miRNAs. Both treatments decreased levels of MiR-19a. We found that miR-19a stimulated cell proliferation, migration, invasion in vitro and tumor growth in vivo. High levels of miR-19a correlated wi  ...[more]

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