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氨基糖苷3'-磷酸转移酶-II类似核苷酸结合环(P环)内的氨基酸替换。

Amino acid substitutions within the analogous nucleotide binding loop (P-loop) of aminoglycoside 3'-phosphotransferase-II.

作者信息

Kocabivik S, Perlin M H

机构信息

Department of Biology, Middle East Technical University, Ankara, Turkey.

出版信息

Int J Biochem. 1994 Jan;26(1):61-6. doi: 10.1016/0020-711x(94)90196-1.

DOI:10.1016/0020-711x(94)90196-1
PMID:8138049
Abstract
  1. Oligonucleotide-directed mutagenesis of APH(3')-II was used to investigate the functions of key amino acids in the P-loop analogous motif of the enzyme. 2. The mutations of Gly205-->Glu, Gly210-->Ala and Arg211-->Pro considerably reduced the resistance of the resulting strains to KM and to related drugs, e.g. G418. 3. Similarly, enzyme activity in the crude extracts of these mutants was substantially reduced as well as the enzyme's affinity for Mg2+ ATP. 4. Alternatively substitutions at a highly conserved basic residue (Arg211-->Lys and Arg211-->His) were not sufficient for the enzyme to sustain the activity at a level comparable to that of the wildtype. 5. Moreover, an Arg211-->His mutation drastically reduced affinity of the enzyme for Mg2+ ATP. 6. This argues the importance of Arg211 residue in contributing to the formation of the P-loop structure in addition to its involvement in phosphoryl transfer reaction. 7. Computer analysis of the secondary structure predicted that the APH(3')-II loop connects a beta-strand to an alpha-helix and that the above mutations caused varying degrees of structural distortions at the corresponding regions of the protein.
摘要
  1. 采用寡核苷酸定向诱变APH(3')-II的方法来研究该酶P环类似基序中关键氨基酸的功能。2. Gly205突变为Glu、Gly210突变为Ala以及Arg211突变为Pro,使得所得菌株对卡那霉素及相关药物(如G418)的抗性大幅降低。3. 同样,这些突变体粗提物中的酶活性以及酶对Mg2+ ATP的亲和力也大幅降低。4. 另外,在高度保守的碱性残基处进行替代(Arg211突变为Lys和Arg211突变为His)不足以使该酶维持与野生型相当的活性水平。5. 此外,Arg211突变为His的突变极大地降低了酶对Mg2+ ATP的亲和力。6. 这表明Arg211残基除了参与磷酸转移反应外,在P环结构形成中也具有重要作用。7. 对二级结构的计算机分析预测,APH(3')-II环将一条β链与一个α螺旋相连,且上述突变在蛋白质的相应区域引起了不同程度的结构扭曲。

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Amino acid substitutions within the analogous nucleotide binding loop (P-loop) of aminoglycoside 3'-phosphotransferase-II.氨基糖苷3'-磷酸转移酶-II类似核苷酸结合环(P环)内的氨基酸替换。
Int J Biochem. 1994 Jan;26(1):61-6. doi: 10.1016/0020-711x(94)90196-1.
2
Site-specific mutations of conserved C-terminal residues in aminoglycoside 3'-phosphotransferase II: phenotypic and structural analysis of mutant enzymes.
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Mechanism of aminoglycoside antibiotic kinase APH(3')-IIIa: role of the nucleotide positioning loop.氨基糖苷类抗生素激酶APH(3')-IIIa的作用机制:核苷酸定位环的作用
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Structural basis for dual nucleotide selectivity of aminoglycoside 2''-phosphotransferase IVa provides insight on determinants of nucleotide specificity of aminoglycoside kinases.氨基糖苷 2''-磷酸转移酶 IVa 双重核苷酸选择性的结构基础为氨基糖苷激酶核苷酸特异性决定因素提供了新的见解。
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Molecular mechanism of aminoglycoside antibiotic kinase APH(3')-IIIa: roles of conserved active site residues.氨基糖苷类抗生素激酶APH(3')-IIIa的分子机制:保守活性位点残基的作用
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The crystal structure of aminoglycoside-3'-phosphotransferase-IIa, an enzyme responsible for antibiotic resistance.氨基糖苷-3'-磷酸转移酶-IIa的晶体结构,一种负责抗生素耐药性的酶。
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Purification and characterization of aminoglycoside 3'-phosphotransferase type IIa and kinetic comparison with a new mutant enzyme.IIa型氨基糖苷3'-磷酸转移酶的纯化与特性分析以及与一种新突变酶的动力学比较。
Antimicrob Agents Chemother. 1994 Apr;38(4):641-7. doi: 10.1128/AAC.38.4.641.
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Altered substrate specificity by substitutions at Tyr218 in bacterial aminoglycoside 3'-phosphotransferase-II.
FEMS Microbiol Lett. 1992 Jun 1;72(2):199-202. doi: 10.1016/0378-1097(92)90529-w.
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Structure-function analyses for aminoglycoside 3'-phosphotransferase II (APH(3')-II).氨基糖苷3'-磷酸转移酶II(APH(3')-II)的结构-功能分析
SAAS Bull Biochem Biotechnol. 1992 Jan;5:58-63.

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Active site comparisons highlight structural similarities between myosin and other P-loop proteins.
活性位点比较突出了肌球蛋白与其他P环蛋白之间的结构相似性。
Biophys J. 1996 Apr;70(4):1590-602. doi: 10.1016/S0006-3495(96)79745-X.