Hemophore-like proteins of the HmuY family in the oral and gut microbiome: unraveling the mystery of their evolution

血红素 生物 牙龈卟啉单胞菌 拟杆菌 微生物学 拟杆菌科 连翘 生物化学 微生物群 组氨酸 ATP结合盒运输机 细菌 遗传学 运输机 氨基酸 基因 替代医学 中医药 病理 金银花 医学
作者
Teresa Olczak,Michał Śmiga,S.V. Antonyuk,John W. Smalley
出处
期刊:Microbiology and Molecular Biology Reviews [American Society for Microbiology]
卷期号:88 (1) 被引量:2
标识
DOI:10.1128/mmbr.00131-23
摘要

SUMMARY Heme (iron protoporphyrin IX, FePPIX) is the main source of iron and PPIX for host-associated pathogenic bacteria, including members of the Bacteroidota (formerly Bacteroidetes) phylum. Porphyromonas gingivalis , a keystone oral pathogen, uses a unique heme uptake (Hmu) system, comprising a hemophore-like protein, designated as the first member of the novel HmuY family. Compared to classical, secreted hemophores utilized by Gram-negative bacteria or near-iron transporter domain-based hemophores utilized by Gram-positive bacteria, the HmuY family comprises structurally similar proteins that have undergone diversification during evolution. The best characterized are P. gingivalis HmuY and its homologs from Tannerella forsythia (Tfo), Prevotella intermedia (PinO and PinA), Bacteroides vulgatus (Bvu), and Bacteroides fragilis (BfrA, BfrB, and BfrC). In contrast to the two histidine residues coordinating heme iron in P. gingivalis HmuY, Tfo, PinO, PinA, Bvu, and BfrA preferentially use two methionine residues. Interestingly, BfrB, despite conserved methionine residue, binds the PPIX ring without iron coordination. BfrC binds neither heme nor PPIX in keeping with the lack of conserved histidine or methionine residues used by other members of the HmuY family. HmuY competes for heme binding and heme sequestration from host hemoproteins with other members of the HmuY family to increase P. gingivalis competitiveness. The participation of HmuY in the host immune response confirms its relevance in relation to the survival of P. gingivalis and its ability to induce dysbiosis not only in the oral microbiome but also in the gut microbiome or other host niches, leading to local injuries and involvement in comorbidities.

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