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链球菌 Pep M5 蛋白的一级结构:不存在广泛的序列重复。

Primary structure of streptococcal Pep M5 protein: Absence of extensive sequence repeats.

机构信息

The Rockefeller University, New York, New York 10021.

出版信息

Proc Natl Acad Sci U S A. 1983 Sep;80(18):5475-9. doi: 10.1073/pnas.80.18.5475.

DOI:10.1073/pnas.80.18.5475
PMID:16593365
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC384280/
Abstract

Extensive sequence repeats have been observed in a biologically active fragment of type 24 streptococcal M protein, namely Pep M24 [Beachey, E. H., Sayer, J. M. & Kang, A. H. (1978) Proc. Natl. Acad. Sci. USA 75, 3163-3167]. To determine whether such extensive repetition in sequence is a common characteristic of the antiphagocytic streptococcal M proteins, we have determined the sequences of the clostripain peptides of Pep M5, a biologically active fragment of the type 5 M protein that is analogous to Pep M24. These sequences, together with the amino-terminal sequence of the whole molecule, accounted for nearly two thirds of the Pep M5 molecule. However, extensive identical repeats of the kind observed in Pep M24 were not present in Pep M5. Preliminary study of the amino acid sequence analysis of the M protein from type 6 Streptococcus has also indicated the absence of sequence repeats within the regions of this molecule examined so far. These results suggest that extensive sequence repeats may not be a common characteristic of M-protein molecules. On the other hand, the seven-residue periodicity of the nonpolar residues, a characteristic of alpha-helical coiled-coil structures, appeared to extend over most of the Pep M5 molecule. This feature has been observed previously for the partial sequences of three M protein serotypes. Thus, the important element of the M-protein structure appears to be the seven-residue periodicity necessary for the maintenance of the coiled-coil structure rather than extensive identical amino acid sequence repeats.

摘要

在 24 型链球菌 M 蛋白的生物活性片段 PepM24 中观察到广泛的序列重复[Beachey,EH,Sayer,JM 和 Kang,AH(1978)Proc。Natl。Acad。Sci。美国 75,3163-3167]。为了确定序列中如此广泛的重复是否是抗吞噬性链球菌 M 蛋白的共同特征,我们已经确定了 PepM5 的凝乳蛋白酶肽序列,PepM5 是 5 型 M 蛋白的生物活性片段,类似于 PepM24。这些序列,连同整个分子的氨基末端序列,占 PepM5 分子的近三分之二。然而,在 PepM24 中观察到的那种广泛的相同重复并不存在于 PepM5 中。对 6 型链球菌 M 蛋白的氨基酸序列分析的初步研究也表明,迄今为止在该分子的检查区域内不存在序列重复。这些结果表明,广泛的序列重复可能不是 M 蛋白分子的共同特征。另一方面,非极性残基的七残基周期性,这是α-螺旋卷曲螺旋结构的特征,似乎延伸到 PepM5 分子的大部分区域。以前已经观察到三个 M 蛋白血清型的部分序列具有此特征。因此,M 蛋白结构的重要元素似乎是维持卷曲螺旋结构所必需的七残基周期性,而不是广泛的相同氨基酸序列重复。

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Tropomyosin-like seven residue periodicity in three immunologically distinct streptococal M proteins and its implications for the antiphagocytic property of the molecule.三种免疫特性不同的链球菌M蛋白中类似原肌球蛋白的七残基周期性及其对该分子抗吞噬特性的影响。
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Primary structural similarities between types 5 and 24 M proteins of Streptococcus pyogenes.化脓性链球菌5型和24型M蛋白之间的主要结构相似性。
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Studies on group A streptococcal M-proteins: purification of type 5 M-protein and comparison of its amino terminal sequence with two immunologically unrelated M-protein molecules.A组链球菌M蛋白的研究:5型M蛋白的纯化及其氨基末端序列与两种免疫无关的M蛋白分子的比较。
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Primary structure of protective antigens of type 24 streptococcal M protein.24型链球菌M蛋白保护性抗原的一级结构
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