首页> 外文期刊>Leukemia and lymphoma >Cytotoxic effect caspase activation dependent of a genetically engineered fusion protein with a CD154 peptide mimetic (OmpC-CD154(p)) on B-NHL cell lines is mediated by the inhibition of bcl-6 and YY1 through MAPK p38 activation
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Cytotoxic effect caspase activation dependent of a genetically engineered fusion protein with a CD154 peptide mimetic (OmpC-CD154(p)) on B-NHL cell lines is mediated by the inhibition of bcl-6 and YY1 through MAPK p38 activation

机译:在B-NHL细胞系上与CD154肽模拟物(OMPC-CD154(P))依赖于基因工程融合蛋白的细胞毒性效果依赖于B-NHL细胞系上的抑制通过MAPK P38活化介导BCL-6和YY1介导

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摘要

The interaction between CD40, and its ligand, CD154, is essential for the development of humoral and cellular immune responses. The selective inhibition or activation of this pathway forms the basis for the development of new therapeutics against immunologically based diseases and malignancies. We are developing a gene fusion of Salmonella typhi OmpC protein expressing the CD154 Tyr140-Ser-149 amino acid strand. This OmpC-CD154 binds CD40 and activates B cells. In this study, we demonstrate that OmpC-CD154(p) treatment inhibits cell growth, proliferation and induced apoptosis in the B-NHL cell lines Raji and Ramos. The Bcl-2 family proteins were regulated and the Bcl-6 and YY1 oncoproteins were inhibited. p38 MAPK activation is an important mechanism underlying the effect on proliferation and apoptosis mediated by this fusion protein. This study establishes a basis for the possible use of fusion protein OmpC-CD154 as an alternative treatment for B-NHL.
机译:CD40与其配体CD154之间的相互作用对于体液和细胞免疫应答的发展至关重要。 这种途径的选择性抑制或活化构成了对抗免疫基础疾病和恶性肿瘤的新治疗方法的发展的基础。 我们正在开发一种表达CD154 TYR140-SER-149氨基酸链的Salmonella Typhi OMPC蛋白的基因融合。 该OMPC-CD154结合CD40并激活B细胞。 在本研究中,我们证明OMPC-CD154(P)治疗抑制了B-NHL细胞系Raji和拉莫斯中的细胞生长,增殖和诱导的细胞凋亡。 调节Bcl-2家族蛋白质,抑制Bcl-6和YY1癌蛋白。 P38 MAPK激活是该融合蛋白介导的增殖和细胞凋亡效果的重要机制。 本研究确定了可能使用融合蛋白OMPC-CD154作为B-NHL的替代处理的基础。

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