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A Mechanism-Based Approach to Screening Metagenomic Libraries for Discovery of Unconventional Glycosidases

机译:一种基于机制的筛选偏心糖苷类酶的映射文库的方法

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Functional metagenomics has opened new opportunities for enzyme discovery. To exploit the full potential of this new tool, the design of selective screens is essential, especially when searching for rare enzymes. To identify novel glycosidases that employ cleavage strategies other than the conventional Koshland mechanisms, a suitable screen was needed. Focusing on the unsaturated glucuronidases (UGLs), it was found that use of simple aryl glycoside substrates did not allow sufficient discrimination against -glucuronidases, which are widespread in bacteria. While conventional glycosidases cannot generally hydrolyze thioglycosides efficiently, UGLs follow a distinct mechanism that allows them to do so. Thus, fluorogenic thioglycoside substrates featuring thiol-based self-immolative linkers were synthesized and assessed as selective substrates. The generality of the approach was validated with another family of unconventional glycosidases, the GH4 enzymes. Finally, the utility of these substrates was tested by screening a small metagenomic library.
机译:功能性偏心神经对酶发现开辟了新的机会。为了利用这种新工具的全部潜力,选择性屏幕的设计至关重要,特别是在寻找稀有酶时。为了鉴定使用传统的Koshland机制以外的裂解策略的新型糖苷酶,需要合适的筛选。专注于不饱和葡萄糖醛酸酶(UGLS),发现使用简单的芳基糖苷基材的使用不允许对葡萄糖酶的充分辨别,这在细菌中普及。虽然常规的糖苷酶通常不能有效地水解硫代糖苷,但UGLS遵循允许它们这样做的明显机制。因此,合成并评估为基于硫醇的自侵略性接头具有基于硫醇的自侵略性接头的荧光硫代糖苷底物作为选择性底物。该方法的一般性与另一个非常规糖苷酶,GH4酶进行验证。最后,通过筛选小型偏心组织文库来测试这些底物的效用。

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