Borrelia burgdorferi oxidative stress regulator BosR directly represses lipoproteins primarily expressed in the tick during mammalian infection

P Wang, P Dadhwal, Z Cheng, MR Zianni… - Molecular …, 2013 - Wiley Online Library
P Wang, P Dadhwal, Z Cheng, MR Zianni, Y Rikihisa, FT Liang, X Li
Molecular microbiology, 2013Wiley Online Library
Differential gene expression is a key strategy adopted by the L yme disease spirochaete, B
orrelia burgdorferi, for adaptation and survival in the mammalian host and the tick vector.
Many B. burgdorferi surface lipoproteins fall into two distinct groups according to their
expression patterns: one group primarily expressed in the tick and the other group primarily
expressed in the mammal. Here, we show that the Fur homologue in this bacterium, also
known as B orrelia oxidative stress regulator (BosR), is required for repression of outer …
Summary
Differential gene expression is a key strategy adopted by the Lyme disease spirochaete, Borrelia burgdorferi, for adaptation and survival in the mammalian host and the tick vector. Many B. burgdorferi surface lipoproteins fall into two distinct groups according to their expression patterns: one group primarily expressed in the tick and the other group primarily expressed in the mammal. Here, we show that the Fur homologue in this bacterium, also known as Borrelia oxidative stress regulator (BosR), is required for repression of outer surface protein A (OspA) and OspD in the mammal. Furthermore, BosR binds directly to sequences upstream of the ospAB operon and the ospD gene through recognition of palindromic motifs similar to those recognized by other Fur homologues but with a 1 bp variation in the spacer length. Putative BosR binding sites have been identified upstream of 156 B. burgdorferi genes. Some of these genes share the same expression pattern as ospA and ospD. Most notably, 12 (67%) of the 18 genes previously identified in a genome‐wide microarray study to be most significantly repressed in the mammal are among the putative BosR regulon. These data indicate that BosR may directly repress transcription of many genes that are downregulated in the mammal.
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