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X-ray crystal structure of the complex of human leukocyte elastase (PMN elastase) and the third domain of the turkey ovomucoid inhibitor.

机译:人白细胞弹性蛋白酶(PMN弹性蛋白酶)与火鸡卵类粘液抑制剂的第三个结构域的复合物的X射线晶体结构。

摘要

Orthorhombic crystals diffracting beyond 1.7 A resolution, have been grown from the stoichiometric complex formed between human leukocyte elastase (HLE) and the third domain of turkey ovomucoid inhibitor (OMTKY3). The crystal and molecular structure has been determined with the multiple isomorphous replacement technique. The complex has been modeled using the known structure of OMTKY3 and partial sequence information for HLE, and has been refined. The current crystallographic R-value is 0.21 for reflections from 25 to 1.8 A resolution. HLE shows the characteristic polypeptide fold of trypsin-like serine proteinases and consists of 218 amino acid residues. However, several loop segments, mainly arranged around the substrate binding site, have unique conformations. The largest deviations from the other vertebrate proteinases of known spatial structure are around Cys168. The specificity pocket is constricted by Val190, Val216 and Asp226 to preferentially accommodate medium sized hydrophobic amino acids at P1. Seven residues of the OMTKY3-binding segment are in specific contact with HLE. This interaction and geometry around the reactive site are similar as observed in other complexes. It is the first serine proteinase glycoprotein analysed, having two sugar chains attached to Asn159 and to residue 109.
机译:从人类白细胞弹性蛋白酶(HLE)与火鸡卵类粘液抑制剂的第三域(OMTKY3)之间形成的化学计量配合物中,生长出了衍射分辨率超过1.7 A的正交晶体。晶体和分子结构已通过多重同晶置换技术确定。已使用OMTKY3的已知结构和HLE的部分序列信息对复合物进行了建模,并对其进行了完善。对于25至1.8 A分辨率的反射,当前晶体学R值为0.21。 HLE显示出胰蛋白酶样丝氨酸蛋白酶的特征性多肽折叠,并由218个氨基酸残基组成。然而,主要围绕底物结合位点排列的几个环段具有独特的构象。与已知空间结构的其他脊椎动物蛋白酶的最大偏差在Cys168附近。 Val190,Val216和Asp226限制了特异性,以优先在P1处容纳中等大小的疏水氨基酸。 OMTKY3-结合区段的七个残基与HLE特异性接触。反应位点周围的这种相互作用和几何形状与其他配合物中观察到的相似。它是第一个被分析的丝氨酸蛋白酶糖蛋白,具有连接到Asn159和109残基的两条糖链。

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