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CBM3d,在瘤胃产纤维素菌 Cel48A 外切葡聚糖酶中发现的家族 3 碳水化合物结合模块的一个新亚家族。

CBM3d, a novel subfamily of family 3 carbohydrate-binding modules identified in Cel48A exoglucanase of Cellulosilyticum ruminicola.

机构信息

State Key Laboratory of Microbial Resources, Institute of Microbiology, Chinese Academy of Sciences, No. 1 West Beichen Road, Chaoyang District, Beijing 100101, China.

出版信息

J Bacteriol. 2011 Oct;193(19):5199-206. doi: 10.1128/JB.05227-11. Epub 2011 Jul 29.

DOI:10.1128/JB.05227-11
PMID:21803997
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3187467/
Abstract

Previously, we found that exoglucanase Cel48A from Cellulosilyticum ruminicola H1 bound intensively to Avicel; however, no known carbohydrate-binding module (CBM) was observed in the protein. Bioinformatics suggested that a C-terminal fragment of 127 amino acids, named the Cellulosilyticum-specific paralogous module (CPM), could function in binding. CPM-appended proteins are all putative (hemi)cellulases from Cellulosilyticum spp. In the present work, we demonstrated that Cel48A without the CPM retained only exoglucanase activity and lost the Avicel-binding ability, while the isolated CPM exhibited a high affinity for Avicel. In addition, the CPM bound to chitin, but not to soluble polysaccharides, making it a type A CBM, which binds only insoluble polysaccharides. Phylogenetic analysis clustered the CPM and its homologs as a separate branch that was distantly related to CBM subfamilies 3a (28% identity), 3b (24% identity), and 3c (21% identity). Sequence alignment revealed distinct secondary structures of the new CBM 3 group, in particular, a conserved Pro66-Trp67 insert preceding strand β4', a deletion preceding strand β6, and incomplete strands β8 and β9. An alanine scan for six aromatic and three nonaromatic amino acid residues (D66, P66, and R111) by site-directed mutagenesis determined that Phe62, Pro66, Trp67, Tyr68, Arg111, and Trp117 were the functional residues for binding. Among them, Phe62, Pro66, and Trp67 were the newly determined key sites in the CPM for binding. Three-dimensional homolog modeling revealed two types of substrate-binding sites, planar and groove, in the CPM. Thus, a new subfamily, CBM family 3d, is proposed.

摘要

先前,我们发现瘤胃纤维梭菌来源的外切葡聚糖酶 Cel48A 能够强烈结合 Avicel;然而,在该蛋白中并未观察到已知的碳水化合物结合模块 (CBM)。生物信息学提示,一个由 127 个氨基酸组成的 C 端片段,命名为纤维梭菌特异的旁系同源模块 (CPM),可能具有结合功能。CPM 连接的蛋白均为纤维梭菌属的假定(半)纤维素酶。在本研究中,我们证实,没有 CPM 的 Cel48A 仅保留外切葡聚糖酶活性,且丧失结合 Avicel 的能力,而分离出的 CPM 对 Avicel 具有高亲和力。此外,CPM 与几丁质结合,但不与可溶性多糖结合,使其成为仅结合不溶性多糖的 A 型 CBM。系统发育分析将 CPM 及其同源物聚类为一个单独的分支,与 CBM 亚家族 3a(28%的同一性)、3b(24%的同一性)和 3c(21%的同一性)关系较远。序列比对揭示了新的 CBM3 组具有独特的二级结构,特别是在β4'前导链前存在一个保守的 Pro66-Trp67 插入,β6 前导链缺失以及β8 和β9 不完整。通过定点突变对六个芳香族和三个非芳香族氨基酸残基(D66、P66 和 R111)进行丙氨酸扫描,确定了结合的功能残基为 Phe62、Pro66、Trp67、Tyr68、Arg111 和 Trp117。其中,Phe62、Pro66 和 Trp67 是 CPM 中结合的新关键位点。三维同源建模揭示了 CPM 中存在两种类型的底物结合位点,即平面和槽型。因此,提出了一个新的亚家族,CBM 家族 3d。

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