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通过上调DARPP-32逆转长春新碱耐药胃癌细胞的多药耐药性

Reversal of multidrug resistance of vincristine-resistant gastric adenocarcinoma cells through up-regulation of DARPP-32.

作者信息

Hong Liu, Wang Jin, Han Ying, Zhao Yunping, Gao Juan, Wang Jun, Han Yu, Zhang Xiaoyin, Yan Li, Zhou Xinmin, Qiao Taidong, Chen Zhen, Fan Daiming

机构信息

State Key Laboratory of Cancer Biology and Institute of Digestive Diseases, Xijing Hospital, Fourth Military Medical University, Changlexi ST 15, Xi'an 710032, Shaanxi Province, China.

出版信息

Cell Biol Int. 2007 Sep;31(9):1010-5. doi: 10.1016/j.cellbi.2007.03.020. Epub 2007 Mar 21.

Abstract

Here we investigated the roles of DARPP-32 in multidrug resistance (MDR) of gastric cancer cells and the possible underlying mechanisms. We constructed the eukaryotic expression vector of DARPP-32 and transfected it into human vincristine-resistant gastric adenocarcinoma cell line SGC7901/VCR. Up-regulation of DARPP-32 could significantly enhance the sensitivity of SGC7901/VCR cells towards vincristine, adriamycin, 5-fluorouracil and cisplatin, and could decrease the capacity of cells to efflux adriamycin. What's more, the results of subrenal capsule assay confirmed that DARPP-32 might play a certain role in MDR of gastric cancer. DARPP-32 could significantly down-regulate the expression of P-gp and zinc ribbon domain-containing 1 (ZNRD1), but not alter the expression of multidrug resistance-associated protein (MRP) or the glutathione S-transferase (GST). DARPP-32 could also significantly decrease the anti-apoptotic activity of SGC7901/VCR cells. Further study of the biological functions of DARPP-32 might be helpful for understanding the mechanisms of MDR in gastric cancer.

摘要

在此,我们研究了DARPP - 32在胃癌细胞多药耐药(MDR)中的作用及其潜在机制。我们构建了DARPP - 32的真核表达载体,并将其转染到人长春新碱耐药的胃腺癌细胞系SGC7901/VCR中。DARPP - 32的上调可显著增强SGC7901/VCR细胞对长春新碱、阿霉素、5 - 氟尿嘧啶和顺铂的敏感性,并可降低细胞外排阿霉素的能力。此外,肾包膜下实验结果证实DARPP - 32可能在胃癌的多药耐药中发挥一定作用。DARPP - 32可显著下调P - 糖蛋白(P - gp)和含锌带结构域1(ZNRD1)的表达,但不改变多药耐药相关蛋白(MRP)或谷胱甘肽S - 转移酶(GST)的表达。DARPP - 32还可显著降低SGC7901/VCR细胞的抗凋亡活性。进一步研究DARPP - 32的生物学功能可能有助于理解胃癌多药耐药的机制。

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