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纤溶酶原kringle 4结构域的宏观和微观稳定性。配体结合的影响。

Macro- and micro-stabilities of the kringle 4 domain from plasminogen. The effect of ligand binding.

作者信息

De Marco A, Motta A, Llinás M, Laursen R A

出版信息

Biophys J. 1985 Sep;48(3):411-22. doi: 10.1016/S0006-3495(85)83797-8.

Abstract

1H-NMR spectra of kringle 4 from human plasminogen have been recorded over wide pH* and temperature ranges, both in the presence and in the absence of p-benzylaminesulfonic acid (BASA). Several resonances exhibit chemical shift differences between kringle folded and unfolded forms which are sufficiently well resolved to allow for a determination of equilibrium Van't Hoff enthalpies and entropies for unfolding. The interaction with BASA shifts the kringle unfolding temperature from approximately 335 degrees K to approximately 343 degrees K. The pH* range of stability is also wider for the complex than for the free kringle: in the acidic range the pH* of half-unfolding, pHu*, is decreased from 2.8 for the unligated polypeptide to approximately 2.0 in the presence of BASA, while in the basic range pHu*, shifts from approximately 10.8 to 11.5. However, in contrast with what is observed at acidic pH*, unfolding at basic pH* leads to irreversible denaturation and exhibits a sharp, order-disorder transition both in the presence and in the absence of ligand. The structural stabilization conferred by the ligand is accompanied by a drastic reduction of the average rate of 1H-2H exchange in 2H2O under conditions that preclude a major cooperative unfolding. Thus, macro- and micro-stabilities of kringle domains appear to be highly correlated.

摘要

已在较宽的pH和温度范围内记录了人纤溶酶原kringle 4的1H-NMR谱,记录时分别处于有和没有对苄胺磺酸(BASA)的条件下。几种共振峰在kringle折叠和未折叠形式之间表现出化学位移差异,这些差异分辨得足够清晰,以便能够确定展开的平衡范特霍夫焓和熵。与BASA的相互作用将kringle的展开温度从约335K提高到约343K。复合物的稳定性pH范围也比游离kringle的更宽:在酸性范围内,半展开的pH*,即pHu*,从未连接多肽的2.8降至存在BASA时的约2.0,而在碱性范围内,pHu从约10.8变为11.5。然而,与在酸性pH下观察到的情况相反,在碱性pH*下展开会导致不可逆变性,并且在有和没有配体的情况下均表现出急剧的有序-无序转变。在排除主要协同展开的条件下,配体赋予的结构稳定性伴随着2H2O中1H-2H交换平均速率的大幅降低。因此,kringle结构域的宏观和微观稳定性似乎高度相关。

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Analysis of ligand-binding to the kringle 4 fragment from human plasminogen.
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