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A novel BLyS antagonist peptide designed based on the 3-D complex structure of BCMA and BLyS

机译:基于BCMA和BLyS的3-D复合结构设计的新型BLyS拮抗剂肽

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B lymphocyte stimulator (BLyS) is a member of tumor necrosis factor (TNF) family. Because of its roles in autoimmune diseases such as systemic lupus erythematosus (SLE), rheumatoid arthritis (RA), and Sjogren syndrome (SS), BLyS antagonists have been tested to treat SLE- and RA-like symptoms in mice and obtained optimistic results. So far, reported BLyS antagonists were mostly decoyed BLyS receptors or anti-BLyS antibodies. In this study, a novel BLyS antagonist peptide, PT, was designed based on the modeling 3-D complex structure of BCMA and BLyS. The interaction mode of PT with BLyS was analyzed theoretically. The results of competitive ELISA demonstrated that PT could inhibit the binding of BCMA-Fc and anti-BLyS antibody to BLyS in vitro. In addition, PT could partly block the proliferating activity of BLyS on mice splenocytes. The BLyS antagonizing activity of PT was significant (p<0.05). This study highlights the possibility of using BLyS antagonist peptide to neutralize BLyS activity. Further optimization of PT with computer-guided molecular design method to enhance its biopotency may be useful in developing new BLyS antagonists to treat BLyS-related autoimmune diseases.
机译:B淋巴细胞刺激物(BLyS)是肿瘤坏死因子(TNF)家族的成员。由于它在全身性红斑狼疮(SLE),类风湿性关节炎(RA)和Sjogren综合征(SS)等自身免疫性疾病中的作用,已经测试了BLyS拮抗剂可治疗小鼠的SLE和RA样症状,并获得了乐观的结果。到目前为止,报道的BLyS拮抗剂大多是诱饵的BLyS受体或抗BLyS抗体。在这项研究中,基于BCMA和BLyS的3-D复杂结构模型,设计了一种新型的BLyS拮抗剂肽PT。从理论上分析了PT与BLyS的相互作用方式。竞争ELISA的结果表明,PT可以在体外抑制BCMA-Fc和抗BLyS抗体与BLyS的结合。另外,PT可以部分阻断BLyS对小鼠脾细胞的增殖活性。 PT的BLyS拮抗活性显着(p <0.05)。这项研究突出了使用BLyS拮抗剂肽中和BLyS活性的可能性。用计算机指导的分子设计方法进一步优化PT以增强其生物效能可能有助于开发新的BLyS拮抗剂来治疗BLyS相关的自身免疫性疾病。

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