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PG1058是细菌IX型分泌系统的一种新型多结构域蛋白成分。

PG1058 Is a Novel Multidomain Protein Component of the Bacterial Type IX Secretion System.

作者信息

Heath Jacqueline E, Seers Christine A, Veith Paul D, Butler Catherine A, Nor Muhammad Nor A, Chen Yu-Yen, Slakeski Nada, Peng Benjamin, Zhang Lianyi, Dashper Stuart G, Cross Keith J, Cleal Steven M, Moore Caroline, Reynolds Eric C

机构信息

Oral Health Cooperative Research Centre, Melbourne Dental School, Bio21 Institute, The University of Melbourne, Melbourne, Australia.

出版信息

PLoS One. 2016 Oct 6;11(10):e0164313. doi: 10.1371/journal.pone.0164313. eCollection 2016.

Abstract

Porphyromonas gingivalis utilises the Bacteroidetes-specific type IX secretion system (T9SS) to export proteins across the outer membrane (OM), including virulence factors such as the gingipains. The secreted proteins have a conserved carboxy-terminal domain essential for type IX secretion that is cleaved upon export. In P. gingivalis the T9SS substrates undergo glycosylation with anionic lipopolysaccharide (A-LPS) and are attached to the OM. In this study, comparative analyses of 24 Bacteroidetes genomes identified ten putative novel components of the T9SS in P. gingivalis, one of which was PG1058. Computer modelling of the PG1058 structure predicted a novel N- to C-terminal architecture comprising a tetratricopeptide repeat (TPR) domain, a β-propeller domain, a carboxypeptidase regulatory domain-like fold (CRD) and an OmpA_C-like putative peptidoglycan binding domain. Inactivation of pg1058 in P. gingivalis resulted in loss of both colonial pigmentation and surface-associated proteolytic activity; a phenotype common to T9SS mutants. Immunoblot and LC-MS/MS analyses of subcellular fractions revealed T9SS substrates accumulated within the pg1058 mutant periplasm whilst whole-cell ELISA showed the Kgp gingipain was absent from the cell surface, confirming perturbed T9SS function. Immunoblot, TEM and whole-cell ELISA analyses indicated A-LPS was produced and present on the pg1058 mutant cell surface although it was not linked to T9SS substrate proteins. This indicated that PG1058 is crucial for export of T9SS substrates but not for the translocation of A-LPS. PG1058 is a predicted lipoprotein and was localised to the periplasmic side of the OM using whole-cell ELISA, immunoblot and LC-MS/MS analyses of subcellular fractions. The structural prediction and localisation of PG1058 suggests that it may have a role as an essential scaffold linking the periplasmic and OM components of the T9SS.

摘要

牙龈卟啉单胞菌利用拟杆菌属特异性的IX型分泌系统(T9SS)将蛋白质输出到外膜(OM),这些蛋白质包括诸如牙龈蛋白酶等毒力因子。分泌的蛋白质具有一个保守的羧基末端结构域,该结构域对于IX型分泌至关重要,并且在输出时会被切割。在牙龈卟啉单胞菌中,T9SS底物会与阴离子脂多糖(A-LPS)发生糖基化反应,并附着在外膜上。在本研究中,对24个拟杆菌属基因组进行的比较分析确定了牙龈卟啉单胞菌中T9SS的10个假定新组分,其中之一是PG1058。PG1058结构的计算机建模预测了一种新的从N端到C端的结构,包括一个四肽重复(TPR)结构域、一个β-螺旋桨结构域、一个羧肽酶调节结构域样折叠(CRD)和一个OmpA_C样假定肽聚糖结合结构域。牙龈卟啉单胞菌中pg1058的失活导致菌落色素沉着和表面相关蛋白水解活性丧失;这是T9SS突变体常见的表型。亚细胞组分的免疫印迹和LC-MS/MS分析显示T9SS底物在pg1058突变体的周质中积累,而全细胞ELISA显示细胞表面不存在Kgp牙龈蛋白酶,证实了T9SS功能受到干扰。免疫印迹、透射电镜和全细胞ELISA分析表明,A-LPS在pg1058突变体细胞表面产生并存在,尽管它与T9SS底物蛋白没有联系。这表明PG1058对于T9SS底物的输出至关重要,但对于A-LPS的转运并非如此。PG1058是一种预测的脂蛋白,通过全细胞ELISA、亚细胞组分的免疫印迹和LC-MS/MS分析将其定位到外膜的周质侧。PG1058的结构预测和定位表明,它可能作为连接T9SS周质和外膜组分的必需支架发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/baff/5053529/52efae32c7d7/pone.0164313.g001.jpg

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