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作 者:汪成富[1] 黄超群[1] 张新堂[2] 钮经义[2]
机构地区:[1]苏州医学院生物化学教研组 [2]中国科学院上海生物化学研究所
出 处:《中国生物化学与分子生物学报》1998年第6期652-654,共3页Chinese Journal of Biochemistry and Molecular Biology
基 金:国家自然科学基金
摘 要:为了研究胰岛素受体结合部位的结构和功能,设计并用固相方法合成了3个六肽.在浓度大于1×103nmol/L时,cyclo(Phe-Phe-Val-Leu-Tyr-Gly)具有明显的胰岛素受体结合活力;H-Phe-Phe-Val-Leu-Tyr-Gly-OH的这一活力则不明显;而H-Gly-Glu-Arg-Gly-Phe-Phe-OH则增强胰岛素和其受体的亲和性.然而,它们都没有体内生物活性.这表明:环六肽部分模拟了胰岛素受体结合部位的空间构象;胰岛素受体结合部位的疏水性和其中的B23Gly-B24Phe-B25Phe对胰岛素和其受体的结合起重要作用.It is proposed that there exists in insulin a hydrophobic domain related to the binding of insulin with its receptor.In order to study the structure and function of this domain,three hexapeptides were designed and synthesized by the Boc solid phase synthetic strategy.When the concentration was higher than 1×10 3 nmol/L,cyclo(Phe Phe Val Leu Tyr Gly) had a definite capacity of binding to insulin receptor;H Phe Phe Val Leu Tyr Gly OH had very weak such activity;H Gly Glu Arg Gly Phe Phe OH enhanced the affinity of insulin with its receptor.However,all of them showed no in vivo activity.The results suggest that the cyclohexapeptide is to some extent similar to the conformation of the domain concerning the binding of insulin with its receptor.It is concluded that the B 23 Gly B 24 Phe B 25 Phe and the hydrophobility of this domain play an important part in the binding of insulin with its receptor.
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