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Identify the key amino acid of BAFF binding with TACI

机译:识别BAFF与TACI结合的关键氨基酸

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B-cell activating factor (BAFF) has been used as a therapeutic target. To develop BAFF-specific small molecular inhibitors, it is necessary to know the key amino acid in the BAFF binding with its receptor. The key binding amino acid of BAFF interacting with its receptor TACI (trans-membrane activator and calcium modulator and cyclophilin ligand interactor) was analyzed based on the computer-guided molecular modeling method. According to theoretical prediction, a series of key amino acid mutants of BAFF, including M204 (Lys204 to Ala), M208 (Met208 to Ala), M209 (Gly209 to Ala), M210 (His210 to Ala), M234 (Gln234 to Ala), M236 (Met236 to Ala), and M237 (Pro237 to Ala) were designed and evaluated with biological experiments. The results show that M208, M209, M236, and M237 of BAFF were the key amino acids and in accord with the theoretical results. The results highlight clues for the further development of BAFF-specific small molecular inhibitors.
机译:B细胞活化因子(BAFF)已被用作治疗目标。为了开发BAFF特异性小分子抑制剂,必须知道BAFF与其受体结合的关键氨基酸。基于计算机指导的分子建模方法,分析了BAFF与其受体TACI(跨膜激活剂和钙调节剂以及亲环蛋白配体相互作用剂)相互作用的关键结合氨基酸。根据理论预测,BAFF的一系列关键氨基酸突变体包括M204(Lys204至Ala),M208(Met208至Ala),M209(Gly209至Ala),M210(His210至Ala),M234(Gln234至Ala)设计M236(Met236至Ala)和M237(Pro237至Ala)并通过生物学实验进行评估。结果表明,BAFF的M208,M209,M236和M237是关键氨基酸,与理论结果相符。这些结果为进一步开发BAFF特异性小分子抑制剂提供了线索。

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