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A LOCUS THAT CONTROLS FILAMENT FORMATION AND SENSITIVITY TO RADIATION IN ESCHERICHIA COLI K-12.一个控制大肠杆菌K-12中丝状形成和对辐射敏感性的基因座。
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J Exp Med. 1984 Oct 1;160(4):1126-46. doi: 10.1084/jem.160.4.1126.
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小鼠白细胞介素-2的结构-功能研究:第一个α-螺旋中的替换可特异性使p70受体结合失活,而第五个α-螺旋中的突变可特异性使p55受体结合失活。

Mouse interleukin-2 structure-function studies: substitutions in the first alpha-helix can specifically inactivate p70 receptor binding and mutations in the fifth alpha-helix can specifically inactivate p55 receptor binding.

作者信息

Zurawski S M, Zurawski G

机构信息

Department of Molecular Biology, DNAX Research Institute of Molecular and Cellular Biology, Palo Alto, CA 94304.

出版信息

EMBO J. 1989 Sep;8(9):2583-90. doi: 10.1002/j.1460-2075.1989.tb08397.x.

DOI:10.1002/j.1460-2075.1989.tb08397.x
PMID:2583124
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC401262/
Abstract

The function of two alpha-helical regions of mouse interleukin-2 were analyzed by saturation substitution analysis. The functional parts of the first alpha-helix (A) was defined as residues 31-39 by the observation that proline substitutions within this region inactivate the protein. Four residues within alpha-helix A, Leu31, Asp34, Leu35 and Leu38, were found to be crucial for biological activity. Structural modeling suggested that these four residues are clustered on one face of alpha-helix A. Residues 31 and 35 had to remain hydrophobic for the molecule to be functional. At residue 38 there was a preference for hydrophobic side chain residues, while at residue 34 some small side chain residues as well as acidic or amide side chain residues were functionally acceptable. Inactivating changes at residue 34 had no effect upon the ability of the protein to interact with the p55 receptor. Disruption of the fifth alpha-helix (E), which had little effect upon biological activity, resulted in an inability of the protein to interact with the p55 receptor. Mutagenesis of the alpha-helix E region demonstrated that alpha-helicity and the nature of the side chain residues in this region were unimportant for biological activity. The region immediately proximal to alpha-helix E was important only for the single intramolecular disulfide linkage.

摘要

通过饱和取代分析对小鼠白细胞介素-2的两个α螺旋区域的功能进行了分析。通过观察到该区域内脯氨酸取代会使蛋白质失活,第一个α螺旋(A)的功能部分被定义为31-39位残基。发现α螺旋A内的四个残基Leu31、Asp34、Leu35和Leu38对生物活性至关重要。结构建模表明,这四个残基聚集在α螺旋A的一侧。为使分子具有功能,31位和35位残基必须保持疏水性。在38位残基处,倾向于疏水性侧链残基,而在34位残基处,一些小侧链残基以及酸性或酰胺侧链残基在功能上是可接受的。34位残基处的失活变化对蛋白质与p55受体相互作用的能力没有影响。对生物活性影响不大的第五个α螺旋(E)的破坏导致蛋白质无法与p55受体相互作用。α螺旋E区域的诱变表明,该区域的α螺旋性和侧链残基的性质对生物活性并不重要。紧邻α螺旋E的区域仅对单个分子内二硫键连接很重要。