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Design of temperature-sensitive penicillinase repressors by replacement of Pro in predicted beta-turn structures.

机译:通过在预测的β-转角结构中替换Pro,设计温度敏感性青霉素酶阻遏物。

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Pro residues in predicted beta-turn structures were substituted with other amino acids to obtain temperature-sensitive penicillinase repressors (PenI). A mutant repressor (P70L; Pro-70 is substituted with Leu) was inactive at 48 degrees C and penP gene expression was derepressed (1,200 U/OD660 [optical density at 660 nm] ), although the mutant was still active at 30 degrees C (27 U). The heat induction ratio (penicillinase activity at 48 degrees C compared with that at 30 degrees C) of the mutant was 98 times higher than that of the wild type (i.e., 44 versus 0.45). This result indicated that the side chain of the Leu residue in P70L destroyed the proper folding of the repressor protein at the elevated temperature, whereas the Pro residue of the wild-type repressor stabilized this predicted beta-turn structure even at 48 degrees C. When the Pro residue was replaced by amino acid residues with smaller side chains (i.e., Gly and Ala), these mutant repressors were less temperature sensitive than P70L. These data suggest that the presence of the Pro residue in the beta-turn structure could be one of the key factors in stabilizing protein structure at elevated temperatures.
机译:预测的β-转弯结构中的Pro残基被其他氨基酸取代,以获得对温度敏感的青霉素酶阻遏物(PenI)。突变阻遏物(P70L; Pro-70被Leu取代)在48摄氏度时失活,并且penP基因表达被抑制(1200 U / OD660 [660 nm处的光密度]),尽管该突变体在30摄氏度时仍然有活性(27 U)。该突变体的热诱导率(48℃下的青霉素酶活性与30℃下的青霉素酶活性)比野生型高98倍(即44对0.45)。该结果表明,在升高的温度下,P70L中Leu残基的侧链破坏了阻遏蛋白的正确折叠,而野生型阻遏物的Pro残基甚至在48摄氏度时也稳定了这种预测的β-转角结构。 Pro残基被具有较小侧链的氨基酸残基(即Gly和Ala)取代,这些突变阻遏物对温度的敏感性低于P70L。这些数据表明,β-转角结构中Pro残基的存在可能是在高温下稳定蛋白质结构的关键因素之一。

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