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首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Inhibition of Chemokine (CXC Motif) Ligand 12/Chemokine (CXC Motif) Receptor 4 Axis (CXCL12/CXCR4)-mediated Cell Migration by Targeting Mammalian Target of Rapamycin (mTOR) Pathway in Human Gastric Carcinoma Cells
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Inhibition of Chemokine (CXC Motif) Ligand 12/Chemokine (CXC Motif) Receptor 4 Axis (CXCL12/CXCR4)-mediated Cell Migration by Targeting Mammalian Target of Rapamycin (mTOR) Pathway in Human Gastric Carcinoma Cells

机译:通过靶向人胃癌细胞中雷帕霉素(mTOR)途径的哺乳动物靶标抑制趋化因子(CXC母体)配体12 /趋化因子(CXC母体)受体4轴(CXCL12 / CXCR4)介导的细胞迁移。

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CXCL12/CXCR4 plays an important role in metastasis of gastric carcinoma. Rapamycin has been reported to inhibit migration of gastric cancer cells. However, the role of mTOR pathway in CXCL12/CXCR4-mediated cell migration and the potential of drugs targeting PI3K/mTOR pathway remains unelucidated. We found that CXCL12 activated PI3K/Akt/mTOR pathway in MKN-45 cells. Stimulating CHO-K1 cells expressing pEGFP-C1-Grp1-PH fusion protein with CXCL12 resulted in generation of phosphatidylinositol (3,4,5)-triphosphate, which provided direct evidence of activating PI3K by CXCL12. Down-regulation of p110β by siRNA but not p110α blocked phosphorylation of Akt and S6K1 induced by CXCL12. Consistently, p110β-specific inhibitor blocked the CXCL12-activated PI3K/Akt/mTOR pathway. Moreover, CXCR4 immunoprecipitated by anti-p110β antibody increased after CXCL12 stimulation and Gi protein inhibitor pertussis toxin abrogated CXCL12-induced activation of PI3K. Further studies demonstrated that inhibitors targeting the PI3K/mTOR pathway significantly blocked the chemotactic responses of MKN-45 cells triggered by CXCL12, which might be attributed primarily to inhibition of mTORC1 and related to prevention of F-actin reorganization as well as down-regulation of active RhoA, Rac1, and Cdc42. Furthermore, rapamycin inhibited the secretion of CXCL12 and the expression of CXCR4, which might form a positive feedback loop to further abolish upstream signaling leading to cell migration. Finally, we found cells expressing high levels of cxcl12 were sensitive to rapamycin in its activity inhibiting migration as well as proliferation. In summary, we found that the mTOR pathway played an important role in CXCL12/CXCR4-mediated cell migration and proposed that drugs targeting the mTOR pathway may be used for the therapy of metastatic gastric cancer expressing high levels of cxcl12.
机译:CXCL12 / CXCR4在胃癌的转移中起重要作用。据报道雷帕霉素可抑制胃癌细胞的迁移。但是,尚不清楚mTOR途径在CXCL12 / CXCR4介导的细胞迁移中的作用以及靶向PI3K / mTOR途径的药物的潜力。我们发现CXCL12激活了MKN-45细胞中的PI3K / Akt / mTOR途径。用CXCL12刺激表达pEGFP-C1-Grp1-PH融合蛋白的CHO-K1细胞导致生成磷脂酰肌醇(3,4,5)-三磷酸,这提供了CXCL12激活PI3K的直接证据。 siRNA对p110β的下调而不是p110α的下调阻止了CXCL12诱导的Akt和S6K1的磷酸化。一致地,p110β特异性抑制剂阻断了CXCL12激活的PI3K / Akt / mTOR途径。此外,在CXCL12刺激后,抗p110β抗体免疫沉淀的CXCR4增加,Gi蛋白抑制剂百日咳毒素消除了CXCL12诱导的PI3K激活。进一步的研究表明,靶向PI3K / mTOR途径的抑制剂可显着阻断CXCL12触发的MKN-45细胞的趋化反应,这可能主要归因于mTORC1的抑制,并且与F-肌动蛋白的重组以及MKN-45的下调有关。活动RhoA,Rac1和Cdc42。此外,雷帕霉素抑制CXCL12的分泌和CXCR4的表达,这可能会形成一个正反馈回路,以进一步消除导致细胞迁移的上游信号传导。最后,我们发现表达高水平cxcl12的细胞对雷帕霉素敏感,因为它的活性抑制迁移和增殖。总之,我们发现mTOR途径在CXCL12 / CXCR4介导的细胞迁移中起着重要作用,并提出靶向mTOR途径的药物可用于治疗表达高水平cxcl12的转移性胃癌。

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