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来自大肠杆菌K-12的色氨酸阻遏物中第79和80位残基在色氨酸操纵基因识别中的可能作用。

The possible roles of residues 79 and 80 of the Trp repressor from Escherichia coli K-12 in trp operator recognition.

作者信息

Güneş C, Staacke D, von Wilcken-Bergmann B, Müller-Hill B

机构信息

Institut für Genetik, Universität zu Köln, Germany.

出版信息

Mol Gen Genet. 1995 Jan 20;246(2):180-95. doi: 10.1007/BF00294681.

Abstract

We constructed mutants of the Trp repressor from Escherichia coli K-12 with all possible single amino acid exchanges at positions 79 and 80 (residues 1 and 2 of the recognition helix). We tested these mutants in vivo by measuring the repression of synthesis of beta-galactosidase with symmetric variants of alpha- and beta-centered trp operators, which replace the lac operator in a synthetic lac system. The Trp repressor carrying a substitution of isoleucine 79 by lysine, showed a marked specificity change with respect to base pair 7 of the alpha-centered trp operator. Gel retardation experiments confirmed this result. Trp repressor mutant IR79 specifically recognizes a trp operator variant with substitutions in positions 7 and 8. Another mutant, with glycine in position 79, exhibited loss of contact at base pair 7. We speculate that the side chain of Ile79 interacts with the AT base pairs 7 and 8 of the alpha-centered trp operator, possibly with the methyl groups of thymines. Replacement of thymine in position 7 or 8 by uracil confirms the involvement of the methyl group of thymine 8 in repressor binding. Several Trp repressor mutants in position 80 (i.e. A180, AL80, AM80 and AP80) broaden the specificity of the Trp repressor for alpha-centered trp operator variants with exchanges in positions 3, 4 and 5.

摘要

我们构建了来自大肠杆菌K-12的色氨酸阻遏物突变体,在第79和80位(识别螺旋的第1和2个残基)进行了所有可能的单氨基酸替换。我们通过测量在合成乳糖系统中用α-和β-中心色氨酸操纵子的对称变体替代乳糖操纵子后β-半乳糖苷酶合成的抑制情况,在体内对这些突变体进行了测试。携带第79位异亮氨酸被赖氨酸替换的色氨酸阻遏物,在α-中心色氨酸操纵子的第7个碱基对方面表现出明显的特异性变化。凝胶阻滞实验证实了这一结果。色氨酸阻遏物突变体IR79特异性识别在第7和8位有替换的色氨酸操纵子变体。另一个突变体,第79位为甘氨酸,在第7个碱基对处失去了接触。我们推测,Ile79的侧链与α-中心色氨酸操纵子的第7和8个AT碱基对相互作用,可能与胸腺嘧啶的甲基相互作用。将第7或8位的胸腺嘧啶替换为尿嘧啶证实了胸腺嘧啶8的甲基参与阻遏物结合。第80位的几个色氨酸阻遏物突变体(即A180、AL80、AM80和AP80)拓宽了色氨酸阻遏物对在第3、4和5位有替换的α-中心色氨酸操纵子变体的特异性。

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