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Clusterin confers gmcitabine resistance in pancreatic cancer
Authors:Qingfeng Chen  Zhengkun Wang  Kejun Zhang  Xiaoyi Liu  Weihong Cao  Lei Zhang  Shuhua Zhang  Bomin Yan  Yaoguang Wang  Chunping Xia
Affiliation:1.Surgery, the Affiliated Hospital of Medical College,QingDao University,QingDao,R.P. China;2.Pathology, the Affiliated Hospital of Medical College,QingDao University,P.R. China;3.Molecular Biology, the Affiliated Hospital of Medical College,QingDao University,P.R. China;4.Hepatobiliary surgery,Tianjin Medical university Cancer Institute and Hospital, Tianjin,Tianjin, Hexi District,China;5.Key Laboratory of Cancer Prevention and Therapy,Tianjin,China
Abstract:

Objective

To measure clusterin expression in pancreatic cancer tissues and cell lines and to evaluate whether clusterin confers resistance to gmcitabine in pancreatic cancer cells.

Methods

Immunohistochemistry for clusterin was performed on 50 primary pancreatic cancer tissues and 25 matched backgrounds, and clusterin expression in 5 pancreatic cancer cell lines was quantified by Western blot and PT-PCR. The correlation between clusterin expression level and gmcitabine IC50 in pancreatic cancer cell lines was evaluated. The effect of an antisense oligonucleotide (ASO) against clusterin(OGX-011) on gmcitabine resistance was evaluated by MTT assays. Xenograft model was used to demonstrate tumor growth.

Results

Pancreatic cancer tissues expressed significantly higher levels of clusterin than did normal pancreatic tissues (P < 0.01). Clusterin expression levels were correlated with gmcitabine resistance in pancreatic cancer cell lines, and OGX-011 significantly decreased BxPc-3 cells resistance to gmcitabine (P < 0.01). In vivo systemic administration of AS clusterin and gmcitabine significantly decreased the s.c. BxPC-3 tumor volume compared with mismatch control ODN plus gmcitabine.

Conclusion

Our finding that clusterin expression was significantly higher in pancreatic cancer than in normal pancreatic tissues suggests that clusterin may confer gmcitabine resistance in pancreatic cancer cells.
Keywords:
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