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Inhibition of mouse SP2/0 myeloma cell growth by the B7-H4 protein vaccine

机译:B7-H4蛋白质疫苗抑制小鼠SP2 / 0骨髓瘤细胞生长

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B7-H4 is a member of B7 family of co-inhibitory molecules and B7-H4 protein is found to be overexpressed in many human cancers and which is usually associated with poor survival. In this study, we developed a therapeutic vaccine made from a fusion protein composed of a tetanus toxoid (TT) T-helper cell epitope and human B7-H4IgV domain (TT-rhB7-H4IgV). We investigated the anti-tumor effect of the TT-rhB7-H4IgV vaccine in BALB/c mice and SP2/0 myeloma growth was significantly suppressed in mice. The TT-rhB7-H4IgV vaccine induced high-titer specific antibodies in mice. Further, the antibodies induced by TT-rhB7-H4IgV vaccine were capable of depleting SP2/0 cells through complement-dependent cytotoxicity (CDC) in vitro. On the other hand, the poor cellular immune response was irrelevant to the therapeutic efficacy. These results indicate that the recombinant TT-rhB7-H4IgV vaccine might be a useful candidate of immunotherapy for the treatment of some tumors associated with abnormal expression of B7-H4.
机译:B7-H4是B7系列共同抑制分子的成员,并且发现B7-H4蛋白在许多人类癌症中过表达,并且通常与差的存活率相关。在这项研究中,我们开发了由由破伤风毒素(TT)T-辅助细胞表位和人B7-H4IGV结构域(TT-RHB7-H4IGV)组成的融合蛋白制成的治疗疫苗。我们研究了TT-rhB7-H4IGV疫苗的抗肿瘤作用在Balb / c小鼠中,小鼠在小鼠中显着抑制了SP2 / 0骨髓瘤生长。 TT-RHB7-H4IGV疫苗诱导小鼠中的高滴度特异性抗体。此外,TT-rhB7-H4IGV疫苗诱导的抗体能够通过体外通过补体依赖性细胞毒性(CDC)来消耗SP2 / 0细胞。另一方面,差的细胞免疫应答与治疗效果无关。这些结果表明重组TT-rhB7-H4IGV疫苗可能是免疫疗法的有用候选者,用于治疗与B7-H4异常表达相关的一些肿瘤。

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