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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。

Tropomyosin-like seven residue periodicity in three immunologically distinct streptococal M proteins and its implications for the antiphagocytic property of the molecule.

作者信息

Manjula B N, Fischetti V A

出版信息

J Exp Med. 1980 Mar 1;151(3):695-708. doi: 10.1084/jem.151.3.695.

Abstract

Partial sequences of three immunologically distinct group A streptococcal M proteins (M5, M6, and M24) revealed significant homology with each other, certain amino acid residues being conserved within the three molecules. In addition, a common feature of the sequenced regions of these M proteins was their high alpha-helical potential and the presence of a repeating seven residue periodicity that is characteristic of the double helical coiled-coil molecule, tropomyosin. The existence of a tropomyosin-like seven residue periodicity strongly suggests that regions of these three M proteins may participate in intra- and/or intermolecular coiled-coil interactions. Because of the constraints imposed by such a repeating periodicity, certain conserved residues within the M proteins would occupy spatially equivalent positions in the tertiary structure of these molecules. This common characteristic could play an important role in the common antiphagocytic property of the immunologically diverse M molecules. In addition to similarities in the secondary structure of M proteins and tropomyosin, significant sequence homology has also been observed between certain regions of these molecules with up to 50% identical residues. As a result of the striking structural similarity with tropomyosin, M proteins may play a regulatory role in the contractile mechanisms involved in phagocytosis.

摘要

三种免疫特性不同的A组链球菌M蛋白(M5、M6和M24)的部分序列显示出彼此之间有显著的同源性,某些氨基酸残基在这三种分子中是保守的。此外,这些M蛋白测序区域的一个共同特征是它们具有较高的α-螺旋潜力,并且存在一种重复的七残基周期性,这是双螺旋卷曲螺旋分子原肌球蛋白的特征。原肌球蛋白样七残基周期性的存在强烈表明,这三种M蛋白的区域可能参与分子内和/或分子间的卷曲螺旋相互作用。由于这种重复周期性的限制,M蛋白内的某些保守残基在这些分子的三级结构中会占据空间上等效的位置。这种共同特征可能在免疫上不同的M分子的共同抗吞噬特性中起重要作用。除了M蛋白和原肌球蛋白二级结构的相似性外,在这些分子的某些区域之间还观察到显著的序列同源性,相同残基高达50%。由于与原肌球蛋白惊人的结构相似性,M蛋白可能在吞噬作用涉及的收缩机制中起调节作用。

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