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Widely applicable background depletion step enables transaminase evolution through solid-phase screening

机译:广泛适用的背景耗竭步骤可通过固相筛选实现转氨酶的进化

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摘要

Directed evolution of transaminases is a widespread technique in the development of highly sought-after biocatalysts for industrial applications. This process, however, is challenged by the limited availability of effective high-throughput protocols to evaluate mutant libraries. Here we report a rapid, reliable, and widely applicable background depletion method for solid-phase screening of transaminase variants, which was successfully applied to a transaminase from Halomonas elongata (HEWT), evolved through rounds of random mutagenesis towards a series of diverse prochiral ketones. This approach enabled the identification of transaminase variants in viable cells with significantly improved activity towards para-substituted acetophenones (up to 60-fold), as well as tetrahydrothiophen-3-one and related substrates. Rationalisation of the mutants was assisted by determination of the high-resolution wild-type HEWT crystal structure presented herein.
机译:转氨酶的定向进化是在工业应用中广受欢迎的生物催化剂的开发中的广泛技术。然而,该过程受到有效高通量方案评估突变体文库的有限可用性的挑战。在这里,我们报告了一种快速,可靠且广泛应用的背景耗竭方法,用于固相筛选转氨酶变体,该方法已成功应用于长形哈莫单胞菌(HEWT)的转氨酶,它是通过几轮随机诱变向一系列不同的前手性酮演变而来的。这种方法能够鉴定活细胞中的转氨酶变体,其对对位取代的苯乙酮(多达60倍)以及四氢噻吩3 -one和相关底物的活性显着提高。确定本文提出的高分辨率野生型HEWT晶体结构有助于突变体的合理化。

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