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八肽胆囊收缩素的结构与活性关系
引用本文:黄晓明,陈钧辉,王新昌.八肽胆囊收缩素的结构与活性关系[J].中国生物化学与分子生物学报,1993,9(1):87-92.
作者姓名:黄晓明  陈钧辉  王新昌
作者单位:南京大学生物化学系,南京大学生物化学系,南京大学生物化学系 南京 210008,南京 210008,南京 210008
摘    要:本文采用液相多肽合成法制备了八肽胆囊收缩素(CCK_8)的六种类似物,并测定了它们诱导离体的豚鼠胆囊收缩的生物学活性。发现CCK_8的N-端乙酰化不改变其生物活性,脱去N-端氨基的CCK_8类似物即Suc-CCK_7与母体CCK_8相比,其活性明显增加。在Boc-CCK_7中,Met被NIe取代活性可完全保留,Gly~(29)被D-Ala取代后仍保留相当的活性,但Gly~(29)被β-Ala取代后则失去胆囊收缩活性;在Met~(28)-Gly~(29)区域引入刚性的r-内酰胺环作为构象限制,也导致活性完全丧失。

关 键 词:八肽胆囊收缩素  胆囊收缩素类似物  结构与功能  
收稿时间:1993-02-20

Structural-activity Relationships of Cholecystokinln Octapeptide
Huang,Xiao-ming Chen,Jun-hui Wang,Xin-chang.Structural-activity Relationships of Cholecystokinln Octapeptide[J].Chinese Journal of Biochemistry and Molecular Biology,1993,9(1):87-92.
Authors:Huang  Xiao-ming Chen  Jun-hui Wang  Xin-chang
Institution:(Department of biochemistry, Nanjing university, Nanjing 210008
Abstract:Six cholecystokinin C-terminal octapeptide (CCK_8) analogues were prepared by liquid peptide synthesis. The ability of CCK_8 analogues to induce the contraction of isolated guinea pig gall bladder were tested. The results showed that the N-terminal acetylation of CCK_8 didn't affect its potency; The desamino analog of CCK_8 (SucCCK_7) displayed a significantly increased potency as compared to that of CCK_8. In Boc-CCK_7, both methionine residues can be replaced by isosteric norleucine without change of biological activity; Substitution of the Gly~(29) residue by a D-Ala led to a peptide whose potency was reduced but still behavied as agonist. In contrast, introduction of a β-Ala in position 29 of Boc-CCK_7 led to complete loss of activity. The incorporation of a synthesized γ-lactam bridged dipeptide (γ-Lac-Gly) as a conformational constraint into the peptide backbone resulted in a compound which was inactive in gall bladder bioassay.
Keywords:Cholecystokinin  Cholecystokinin octapeptide analogue  Gall bladder contraction  Structure and activity
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