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革兰氏阴性菌四环素外排蛋白两个互补结构域进化过程中的基因复制。

Gene duplication in the evolution of the two complementing domains of gram-negative bacterial tetracycline efflux proteins.

作者信息

Rubin R A, Levy S B, Heinrikson R L, Kézdy F J

机构信息

Department of Molecular Biology and Microbiology, Tufts University School of Medicine, Boston, MA 02111.

出版信息

Gene. 1990 Mar 1;87(1):7-13. doi: 10.1016/0378-1119(90)90489-e.

DOI:10.1016/0378-1119(90)90489-e
PMID:2332166
Abstract

The resistance of Gram- bacteria to the broad-spectrum antibiotic tetracycline (Tc) results from energy-dependent drug efflux mediated by the tet gene product, the cytoplasmic membrane Tet protein. Amino acid (aa) sequences deduced from total tet nucleotide sequences of three different resistance determinants (classes A, B and C) indicate that the protein products [Tet(A), Tet(B), and Tet(C)] share a common ancestor. Hydropathic analysis of Tet sequences predicts twelve transmembrane segments in each protein, with six occurring in each half of the molecule. More importantly, the linear distributions of these segments in the N- and C-terminal halves are nearly identical, suggesting that the two halves of each Tet protein are related by a process of tandem gene duplication and divergence. Indeed, a variable but significant conservation of sequence was detected among the N- and C-terminal halves for all possible comparisons of the three proteins. Such conservation was not observed within other prokaryotic integral membrane proteins or when other prokaryotic proteins were compared to Tet halves. Similarity, both in sequence and in predicted transmembrane structural organization, strongly suggests that a common ancestor of Tet(A), Tet(B), and Tet(C) arose by duplication of a gene reading frame specifying a transmembrane protein of approximately 200 aa residues. The two halves of Tet proteins correspond to the two domains, alpha and beta, which have distinct, complementary roles in Tc efflux. Nevertheless, selective constraints to function in the cytoplasmic membrane have apparently led to maintenance of similar patterns of secondary structural organization in these complementary domains.

摘要

革兰氏阴性菌对广谱抗生素四环素(Tc)的耐药性源于tet基因产物(细胞质膜Tet蛋白)介导的能量依赖性药物外排。从三种不同耐药决定簇(A类、B类和C类)的总tet核苷酸序列推导的氨基酸(aa)序列表明,蛋白质产物[Tet(A)、Tet(B)和Tet(C)]有一个共同的祖先。对Tet序列的亲水性分析预测,每种蛋白质中有12个跨膜区段,分子的每一半各有6个。更重要的是,这些区段在N端和C端的线性分布几乎相同,这表明每个Tet蛋白的两半是通过串联基因复制和分化过程相关联的。实际上,在这三种蛋白质的所有可能比较中,在N端和C端之间检测到了可变但显著的序列保守性。在其他原核生物整合膜蛋白中未观察到这种保守性,或者当将其他原核生物蛋白与Tet的两半进行比较时也未观察到。在序列和预测的跨膜结构组织方面的相似性强烈表明,Tet(A)、Tet(B)和Tet(C)的共同祖先起源于一个指定约200个氨基酸残基的跨膜蛋白的基因阅读框的复制。Tet蛋白的两半对应于α和β两个结构域,它们在Tc外排中具有不同的互补作用。然而,在细胞质膜中发挥功能的选择性限制显然导致了这些互补结构域中二级结构组织的相似模式得以维持。

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