Identification of Rv3852 as a nucleoid-associated protein in Mycobacterium tuberculosis

Werlang, Isabel Cristina Ribas; Schneider, Cristopher Z.; Mendonça, Jordana Dutra de; Palma, Mário Sérgio; Basso, Luiz Augusto; Santos, Daniel Silas Veras dos

doi:10.1099/mic.0.030148-0

Cited by 16 publications

(17 citation statements)

References 77 publications

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“…The protein bound to DNA in a sequence-independent manner, and with increasing protein concentrations, the DNA-protein complexes were increased. At higher concentrations (75 to 100 nM) of the protein, the DNA-protein complexes failed to enter the gel, suggesting the formation of higher-order oligomeric DNA-protein structures, as reported previously (28). These structures presumably formed due to the cooperative binding of the protein on DNA.…”

Section: Resultsmentioning

confidence: 66%

Regulation of Lipid Biosynthesis, Sliding Motility, and Biofilm Formation by a Membrane-Anchored Nucleoid-Associated Protein of Mycobacterium tuberculosis

2013

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bBacteria use a number of small basic proteins for organization and compaction of their genomes. By their interaction with DNA, these nucleoid-associated proteins (NAPs) also influence gene expression. Rv3852, a NAP of Mycobacterium tuberculosis, is conserved among the pathogenic and slow-growing species of mycobacteria. Here, we show that the protein predominantly localizes in the cell membrane and that the carboxy-terminal region with the propensity to form a transmembrane helix is necessary for its membrane localization. The protein is involved in genome organization, and its ectopic expression in Mycobacterium smegmatis resulted in altered nucleoid morphology, defects in biofilm formation, sliding motility, and change in apolar lipid profile. We demonstrate its crucial role in regulating the expression of KasA, KasB, and GroEL1 proteins, which are in turn involved in controlling the surface phenotypes in mycobacteria.

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Section: Resultsmentioning

confidence: 66%

Regulation of Lipid Biosynthesis, Sliding Motility, and Biofilm Formation by a Membrane-Anchored Nucleoid-Associated Protein of Mycobacterium tuberculosis

2013

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“…Together, this suggests that EspR and Lsr2 may control gene expression, including that of many cell wall functions, in a divergent manner with EspR possibly replacing Lsr2 at certain sites and vice-versa. It is striking that in all sequenced mycobacterial genomes espR is very close to the hns gene encoding another NAP [33] and this may also indicate functional interplay. These hypotheses can be tested experimentally by using the corresponding antibodies to perform ChIP-Seq experiments on Mtb strains at different stages in the growth cycle to localize their binding sites.…”

Section: Resultsmentioning

confidence: 99%

Virulence Regulator EspR of Mycobacterium tuberculosis Is a Nucleoid-Associated Protein

et al. 2012

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The principal virulence determinant of Mycobacterium tuberculosis ( Mtb ), the ESX-1 protein secretion system, is positively controlled at the transcriptional level by EspR. Depletion of EspR reportedly affects a small number of genes, both positively or negatively, including a key ESX-1 component, the espACD operon. EspR is also thought to be an ESX-1 substrate. Using EspR-specific antibodies in ChIP-Seq experiments (chromatin immunoprecipitation followed by ultra-high throughput DNA sequencing) we show that EspR binds to at least 165 loci on the Mtb genome. Included in the EspR regulon are genes encoding not only EspA, but also EspR itself, the ESX-2 and ESX-5 systems, a host of diverse cell wall functions, such as production of the complex lipid PDIM (phenolthiocerol dimycocerosate) and the PE/PPE cell-surface proteins. EspR binding sites are not restricted to promoter regions and can be clustered. This suggests that rather than functioning as a classical regulatory protein EspR acts globally as a nucleoid-associated protein capable of long-range interactions consistent with a recently established structural model. EspR expression was shown to be growth phase-dependent, peaking in the stationary phase. Overexpression in Mtb strain H37Rv revealed that EspR influences target gene expression both positively or negatively leading to growth arrest. At no stage was EspR secreted into the culture filtrate. Thus, rather than serving as a specific activator of a virulence locus, EspR is a novel nucleoid-associated protein, with both architectural and regulatory roles, that impacts cell wall functions and pathogenesis through multiple genes.

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“…Since Rv3852 had been hypothesized to play a role as a NAP (19), thus contributing to shaping the chromosome, the MICs of drugs that have an effect on the topology of DNA were measured (28). We used the fluoroquinolones moxifloxacin and novobiocin targeting the GyrA and GyrB subunits of DNA gyrase, respectively, for this purpose together with rifampin, inhibiting RNA synthesis, as a control.…”

Section: Resultsmentioning

confidence: 99%

“…Curiously, Werlang and colleagues reported that M. tuberculosis Rv3852 does not complement hns mutations in E. coli (19), whereas Lsr2, another NAP, does (20) and is therefore a functional homologue of E. coli H-NS. Ectopic expression of M. tuberculosis rv3852 in M. smegmatis led to a less-compacted nucleoid, altered biofilm formation, and decreased sliding motility (21).…”

Section: Abstract Tuberculosis Mycobacterium Tuberculosis H-ns Napmentioning

confidence: 99%

Rv3852 (H-NS) of Mycobacterium tuberculosis Is Not Involved in Nucleoid Compaction and Virulence Regulation

et al. 2017

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A handful of nucleoid-associated proteins (NAPs) regulate the vast majority of genes in a bacterial cell. H-NS, the histone-like nucleoid-structuring protein, is one of these NAPs and protects Escherichia coli from foreign gene expression. Though lacking any sequence similarity with E. coli H-NS, Rv3852 was annotated as the H-NS ortholog in Mycobacterium tuberculosis, as it resembles human histone H1. The role of Rv3852 was thoroughly investigated by immunoblotting, subcellular localization, construction of an unmarked rv3852 deletion in the M. tuberculosis genome, and subsequent analysis of the resulting Δrv3852 strain. We found that Rv3852 was predominantly present in the logarithmic growth phase with a decrease in protein abundance in stationary phase. Furthermore, it was strongly associated with the cell membrane and not detected in the cytosolic fraction, nor was it secreted. The Δrv3852 strain displayed no growth defect or morphological abnormalities. Quantitative measurement of nucleoid localization in the Δrv3852 mutant strain compared to that in the parental H37Rv strain showed no difference in nucleoid position or spread. Infection of macrophages as well as severe combined immunodeficient (SCID) mice demonstrated that loss of Rv3852 had no detected influence on the virulence of M. tuberculosis. We thus conclude that M. tuberculosis Rv3852 is not involved in pathogenesis and is not a typical NAP. The existence of an as yet undiscovered Rv3852 ortholog cannot be excluded, although this role is likely played by the well-characterized Lsr2 protein.IMPORTANCE Mycobacterium tuberculosis is the causative agent of the lung infection tuberculosis, claiming more than 1.5 million lives each year. To understand the mechanisms of latent infection, where M. tuberculosis can stay dormant inside the human host, we require deeper knowledge of the basic biology and of the regulatory networks. In our work, we show that Rv3852, previously annotated as H-NS, is not a typical nucleoid-associated protein (NAP) as expected from its initial annotation. Rv3852 from M. tuberculosis has neither influence on nucleoid shape or compaction nor a role in virulence. Our findings reduce the repertoire of identified nucleoid-associated proteins in M. tuberculosis to four transcription regulators and underline the importance of genetic studies to assign a function to bacterial genes. KEYWORDS tuberculosis, Mycobacterium tuberculosis, H-NS, NAP, global regulation, rv3852T he chromosome must be heavily compacted to fit into a bacterial cell about 1,000 times smaller than the length of its DNA. Similarly to eukaryotes, where DNA is wrapped around histones for condensation, prokaryotes possess nucleoid-associated proteins (NAPs), which influence DNA topology. Typically, NAPs interact with the chromosome at several hundred binding sites in a sequence-specific or non-sequencespecific manner (1). As a result, NAPs can bridge, loop, and bend DNA (2), thus

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Identification of Rv3852 as a nucleoid-associated protein in Mycobacterium tuberculosis

Cited by 16 publications

References 77 publications

Regulation of Lipid Biosynthesis, Sliding Motility, and Biofilm Formation by a Membrane-Anchored Nucleoid-Associated Protein of Mycobacterium tuberculosis

Regulation of Lipid Biosynthesis, Sliding Motility, and Biofilm Formation by a Membrane-Anchored Nucleoid-Associated Protein of Mycobacterium tuberculosis

Virulence Regulator EspR of Mycobacterium tuberculosis Is a Nucleoid-Associated Protein

Rv3852 (H-NS) of Mycobacterium tuberculosis Is Not Involved in Nucleoid Compaction and Virulence Regulation

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