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Integrin α10, a Novel Therapeutic Target in Glioblastoma, Regulates Cell Migration, Proliferation, and Survival

机译:整合素α10,胶质母细胞瘤的新型治疗靶标,调节细胞迁移,增殖和存活。

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New, effective treatment strategies for glioblastomas (GBMs), the most malignant and invasive brain tumors in adults, are highly needed. In this study, we investigated the potential of integrin α10β1 as a therapeutic target in GBMs. Expression levels and the role of integrin α10β1 were studied in patient-derived GBM tissues and cell lines. The effect of an antibody–drug conjugate (ADC), an integrin α10 antibody conjugated to saporin, on GBM cells and in a xenograft mouse model was studied. We found that integrin α10β1 was strongly expressed in both GBM tissues and cells, whereas morphologically unaffected brain tissues showed only minor expression. Partial or no overlap was seen with integrins α3, α6, and α7, known to be expressed in GBM. Further analysis of a subpopulation of GBM cells selected for high integrin α10 expression demonstrated increased proliferation and sphere formation. Additionally, siRNA-mediated knockdown of integrin α10 in GBM cells led to decreased migration and increased cell death. Furthermore, the ADC reduced viability and sphere formation of GBM cells and induced cell death both in vitro and in vivo . Our results demonstrate that integrin α10β1 has a functional role in GBM cells and is a novel, potential therapeutic target for the treatment of GBM.
机译:迫切需要针对成胶质细胞瘤(GBM)(成人中最恶性和侵袭性脑瘤)的新的有效治疗策略。在这项研究中,我们研究了整联蛋白α10β1作为GBMs治疗靶标的潜力。研究了患者来源的GBM组织和细胞系中整联蛋白α10β1的表达水平和作用。研究了抗体-药物偶联物(ADC),一种与皂草素偶联的整联蛋白α10抗体,对GBM细胞和异种移植小鼠模型的影响。我们发现整联蛋白α10β1在GBM组织和细胞中均强烈表达,而在形态学上未受影响的脑组织仅表现出少量表达。已知在GBM中表达的整合素α3,α6和α7部分或没有重叠。选择用于高整合素α10表达的GBM细胞亚群的进一步分析表明,增殖和球形成增加。此外,siRNA介导的GBM细胞中整联蛋白α10的敲低导致迁移减少和细胞死亡增加。此外,ADC在体外和体内均降低了GBM细胞的活力和球形成,并诱导了细胞死亡。我们的结果表明,整联蛋白α10β1在GBM细胞中具有功能性作用,并且是治疗GBM的新型潜在治疗靶标。

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