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重组小鼠脂肪细胞脂质结合蛋白的晶体结构

Crystal structure of recombinant murine adipocyte lipid-binding protein.

作者信息

Xu Z, Bernlohr D A, Banaszak L J

机构信息

Department of Biochemistry, University of Minnesota Medical School, Minneapolis 55455.

出版信息

Biochemistry. 1992 Apr 7;31(13):3484-92. doi: 10.1021/bi00128a024.

Abstract

Adipocyte lipid-binding protein (ALBP) is the adipocyte member of an intracellular hydrophobic ligand-binding protein family. ALBP is phosphorylated by the insulin receptor kinase upon insulin stimulation. The crystal structure of recombinant murine ALBP has been determined and refined to 2.5 A. The final R factor for the model is 0.18 with good canonical properties. Crystalline ALBP has a conformation which is essentially identical to that of intestinal fatty acid binding protein and myelin P2 protein. Although the crystal structure is of the apo- form, a cavity resembling that in other family members is present. It contains a number of bound and implied unbound water molecules and shows no large obvious portal to the external milieu. The cavity of ALBP, which by homology is the ligand-binding site, is formed by both polar and hydrophobic residues among which is tyrosine 19. Y19 is phosphorylated by the insulin receptor kinase as described in the accompanying paper [Buelt, M. K., Xu, Z., Banaszak, L. J., & Bernlohr, D. A. (1992) Biochemistry (following paper in this issue)]. By comparing ALBP with the earlier structural results on intestinal fatty acid binding protein, it is now possible to delineate conserved amino acids which help form the binding site in this family.

摘要

脂肪细胞脂质结合蛋白(ALBP)是细胞内疏水配体结合蛋白家族的脂肪细胞成员。胰岛素刺激时,ALBP被胰岛素受体激酶磷酸化。重组鼠ALBP的晶体结构已被确定并精修至2.5埃。该模型的最终R因子为0.18,具有良好的典型特性。结晶态的ALBP具有与肠脂肪酸结合蛋白和髓磷脂P2蛋白基本相同的构象。虽然晶体结构是脱辅基形式,但存在一个类似于其他家族成员中的腔。它包含许多结合的和隐含的未结合水分子,并且没有明显的通向外部环境的大通道。ALBP的腔通过同源性是配体结合位点,由极性和疏水残基形成,其中包括酪氨酸19。如随附论文[Buelt, M. K., Xu, Z., Banaszak, L. J., & Bernlohr, D. A. (1992) Biochemistry(本期后续论文)]所述,Y19被胰岛素受体激酶磷酸化。通过将ALBP与早期关于肠脂肪酸结合蛋白的结构结果进行比较,现在可以描绘出有助于在该家族中形成结合位点的保守氨基酸。

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