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The human alpha(2)-plasmin inhibitor: functional characterization of the unique plasmin(ogen)-binding region

机译:人类的alpha(2)-纤溶酶抑制剂:独特的纤溶酶(基因)结合区的功能表征

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摘要

The human alpha(2)-plasmin inhibitor (A2PI) possesses unique N- and C-terminal extensions that significantly influence its biological activities. The C-terminal segment, A2PIC (Asn(398)-Lys(452)), contains six lysines thought to be involved in the binding to lysine-binding sites in the kringle domains of human plasminogen, of which four (Lys(422), Lys(429), Lys(436), Lys(452)) are completely and two (Lys(406), Lys(415)) are partially conserved. Multiple Lys to Ala mutants of A2PIC were expressed in Escherichia coli and used in intrinsic fluorescence titrations with kringle domains K1, K4, K4 + 5, and K1 + 2 + 3 of human plasminogen. We were able to identify the C-terminal Lys(452) as the main binding partner in recombinant A2PIC (rA2PIC) constructs with isolated kringles. We could show a cooperative, zipper-like enhancement of the interaction between C-terminal Lys(452) and internal Lys(436) of rA2PIC and isolated K1 + 2 + 3, whereas the other internal lysine residues contribute only to a minor extent to the binding process. Sulfated Tyr(445) in the unique C-terminal segment revealed no influence on the binding affinity to kringle domains.
机译:人alpha(2)-纤溶酶抑制剂(A2PI)具有独特的N和C末端延伸,可显着影响其生物学活性。 C末端片段A2PIC(Asn(398)-Lys(452))包含六个赖氨酸,这些赖氨酸被认为与人纤溶酶原的kringle域中的赖氨酸结合位点结合,其中四个(Lys(422) ,Lys(429),Lys(436),Lys(452))是完全保守的,而两个(Lys(406),Lys(415))是部分保守的。 A2PIC的多个Lys to Ala突变体在大肠杆菌中表达,并用于人纤溶酶原的Kringle域K1,K4,K4 + 5和K1 + 2 + 3的固有荧光滴定中。我们能够确定C端Lys(452)为重组A2PIC(rA2PIC)构建体中的主要结合伴侣,并具有分离的环。我们可能显示出协同协同,拉链状增强rA2PIC和分离的K1 + 2 + 3的C末端Lys(452)和内部Lys(436)之间的相互作用,而其他内部赖氨酸残基仅对绑定过程。独特的C末端片段中的硫酸化Tyr(445)揭示了对环蛋白结构域的结合亲和力没有影响。

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