Iron-Utilization System in Vibrio vulnificus M2799

Author:

Miyamoto KatsushiroORCID,Kawano Hiroaki,Okai Naoko,Hiromoto Takeshi,Miyano Nao,Tomoo Koji,Tsuchiya Takahiro,Komano Jun,Tanabe Tomotaka,Funahashi Tatsuya,Tsujibo Hiroshi

Abstract

Vibrio vulnificus is a Gram-negative pathogenic bacterium that causes serious infections in humans and requires iron for growth. A clinical isolate, V. vulnificus M2799, secretes a catecholate siderophore, vulnibactin, that captures ferric ions from the environment. In the ferric-utilization system in V. vulnificus M2799, an isochorismate synthase (ICS) and an outer membrane receptor, VuuA, are required under low-iron conditions, but alternative proteins FatB and VuuB can function as a periplasmic-binding protein and a ferric-chelate reductase, respectively. The vulnibactin-export system is assembled from TolCV1 and several RND proteins, including VV1_1681. In heme acquisition, HupA and HvtA serve as specific outer membrane receptors and HupB is a sole periplasmic-binding protein, unlike FatB in the ferric-vulnibactin utilization system. We propose that ferric-siderophore periplasmic-binding proteins and ferric-chelate reductases are potential targets for drug discovery in infectious diseases.

Funder

Grant-aided Projects for Private Universities from the Ministry of Education, Culture, Sports, Science and Technology (MEXT), Japan

Publisher

MDPI AG

Subject

Drug Discovery,Pharmacology, Toxicology and Pharmaceutics (miscellaneous),Pharmaceutical Science

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