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一种修饰β-淀粉样蛋白的分选酶的实验室进化

Laboratory evolution of a sortase enzyme that modifies amyloid-β protein.

作者信息

Podracky Christopher J, An Chihui, DeSousa Alexandra, Dorr Brent M, Walsh Dominic M, Liu David R

机构信息

Merkin Institute of Transformative Technologies in Healthcare, Broad Institute of Harvard and MIT, Cambridge, MA, USA.

Department of Chemistry and Chemical Biology, Harvard University, Cambridge, MA, USA.

出版信息

Nat Chem Biol. 2021 Mar;17(3):317-325. doi: 10.1038/s41589-020-00706-1. Epub 2021 Jan 11.

Abstract

Epitope-specific enzymes are powerful tools for site-specific protein modification but generally require genetic manipulation of the target protein. Here, we describe the laboratory evolution of the bacterial transpeptidase sortase A to recognize the LMVGG sequence in endogenous amyloid-β (Aβ) protein. Using a yeast display selection for covalent bond formation, we evolved a sortase variant that prefers LMVGG substrates from a starting enzyme that prefers LPESG substrates, resulting in a >1,400-fold change in substrate preference. We used this evolved sortase to label endogenous Aβ in human cerebrospinal fluid, enabling the detection of Aβ with sensitivities rivaling those of commercial assays. The evolved sortase can conjugate a hydrophilic peptide to Aβ, greatly impeding the ability of the resulting protein to aggregate into higher-order structures. These results demonstrate laboratory evolution of epitope-specific enzymes toward endogenous targets as a strategy for site-specific protein modification without target gene manipulation and enable potential future applications of sortase-mediated labeling of Aβ peptides.

摘要

表位特异性酶是用于位点特异性蛋白质修饰的强大工具,但通常需要对目标蛋白质进行基因操作。在此,我们描述了细菌转肽酶分选酶A的实验室进化过程,使其能够识别内源性淀粉样β蛋白(Aβ)中的LMVGG序列。通过酵母展示筛选共价键形成,我们从偏好LPESG底物的起始酶进化出一种偏好LMVGG底物的分选酶变体,导致底物偏好发生了超过1400倍的变化。我们使用这种进化后的分选酶标记人脑脊液中的内源性Aβ,能够以与商业检测方法相当的灵敏度检测Aβ。进化后的分选酶可以将亲水性肽与Aβ偶联,极大地阻碍了所得蛋白质聚集成高阶结构的能力。这些结果证明了表位特异性酶针对内源性靶点的实验室进化,作为一种无需对靶基因进行操作的位点特异性蛋白质修饰策略,并为分选酶介导的Aβ肽标记的潜在未来应用提供了可能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1338/7904614/92830a2a3758/nihms-1644917-f0005.jpg

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