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清道夫受体介导的肠道固醇吸收受到两亲性肽和蛋白质的竞争性抑制。

Intestinal sterol absorption mediated by scavenger receptors is competitively inhibited by amphipathic peptides and proteins.

作者信息

Schulthess G, Compassi S, Werder M, Han C H, Phillips M C, Hauser H

机构信息

Institute of Biochemistry, Swiss Federal Institute of Technology, ETH Center, Universitätstrasse 16, CH-8092 Zurich, Switzerland.

出版信息

Biochemistry. 2000 Oct 17;39(41):12623-31. doi: 10.1021/bi0011633.

DOI:10.1021/bi0011633
PMID:11027142
Abstract

Exchangeable serum apolipoproteins and amphipathic alpha-helical peptides are effective inhibitors of sterol (free and esterified cholesterol) uptake at the small-intestinal brush border membrane. The minimal structural requirement of an inhibitor is an amphipathic alpha-helix of 18 amino acids. The inhibition is competitive, indicating that the inhibitor binds to scavenger receptor class B type I (SR-BI) present in the brush border membrane and responsible for sterol uptake. Binding of apolipoprotein A-I to SR-BI of rabbit brush border membrane is cooperative, characterized by a dissociation constant K(d) = 0.45 microM and a Hill coefficient of n = 2.8. The cooperativity of the interaction is due to binding of the inhibitor molecule to a dimeric or oligomeric form of SR-BI held together by disulfide bridges. Consistent with the competitive nature of the inhibition, the K(d) value agrees within experimental error with the IC(50) value of inhibition and with the inhibition constant K(I). After proteinase K treatment of brush border membrane vesicles, the affinity of the interaction of apolipoprotein A-I expressed as K(d) is reduced by a factor of 20, and the cooperativity is lost. The interaction of proteinase K-treated brush border membrane vesicles with apolipoprotein A-I is nonspecific partitioning of the apolipoprotein into the lipid bilayer of brush border membrane vesicles.

摘要

可交换血清载脂蛋白和两亲性α-螺旋肽是小肠刷状缘膜中固醇(游离胆固醇和酯化胆固醇)摄取的有效抑制剂。抑制剂的最小结构要求是一个由18个氨基酸组成的两亲性α-螺旋。这种抑制是竞争性的,表明抑制剂与存在于刷状缘膜中且负责固醇摄取的B类I型清道夫受体(SR-BI)结合。载脂蛋白A-I与兔刷状缘膜的SR-BI结合具有协同性,其解离常数K(d) = 0.45微摩尔,希尔系数n = 2.8。这种相互作用的协同性是由于抑制剂分子与通过二硫键结合在一起的SR-BI二聚体或寡聚体形式结合。与抑制的竞争性本质一致,K(d)值在实验误差范围内与抑制的IC(50)值以及抑制常数K(I)一致。用蛋白酶K处理刷状缘膜囊泡后,以K(d)表示的载脂蛋白A-I相互作用的亲和力降低了20倍,且协同性丧失。蛋白酶K处理的刷状缘膜囊泡与载脂蛋白A-I的相互作用是载脂蛋白非特异性地分配到刷状缘膜囊泡的脂质双层中。

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Intestinal sterol absorption mediated by scavenger receptors is competitively inhibited by amphipathic peptides and proteins.清道夫受体介导的肠道固醇吸收受到两亲性肽和蛋白质的竞争性抑制。
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