Phylogeny to function: <scp>PE</scp>/<scp>PPE</scp> protein evolution and impact on <scp><i>M</i></scp><i>ycobacterium tuberculosis</i> pathogenicity

Fishbein, Skye; Wyk, Niël van; Warren, Robin M.; Sampson, Samantha L.

doi:10.1111/mmi.12981

Cited by 188 publications

(194 citation statements)

References 118 publications

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“…The pe and ppe genes are differentially regulated at the transcriptional level in response to a variety of environmental signals (29) and are frequently found among the differentially expressed genes in regulatory mutants (30,31). In addition, there is evidence that some PE_PGRS family members are expressed specifically in granulomatous lesions (32).…”

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confidence: 99%

Mycobacterium tuberculosis Resists Stress by Regulating PE19 Expression

et al. 2016

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cMycobacterium tuberculosis requires the phosphate-sensing signal transduction system Pst/SenX3-RegX3 to resist host immune responses. A ⌬pstA1 mutant lacking a Pst phosphate uptake system component is hypersensitive to diverse stress conditions in vitro and is attenuated in vivo due to constitutive expression of the phosphate starvation-responsive RegX3 regulon. Transcriptional profiling of the ⌬pstA1 mutant revealed aberrant expression of certain pe and ppe genes. PE and PPE proteins, defined by conserved N-terminal domains containing Pro-Glu (PE) or Pro-Pro-Glu (PPE) motifs, account for a substantial fraction of the M. tuberculosis genome coding capacity, but their functions are largely uncharacterized. Because some PE and PPE proteins localize to the cell wall, we hypothesized that overexpression of these proteins sensitizes M. tuberculosis to stress by altering cell wall integrity. To test this idea, we deleted pe and ppe genes that were overexpressed by ⌬pstA1 bacteria. Deletion of a single pe gene, pe19, suppressed hypersensitivity of the ⌬pstA1 mutant to both detergent and reactive oxygen species. Ethidium bromide uptake assays revealed increased envelope permeability of the ⌬pstA1 mutant that was dependent on PE19. The replication defect of the ⌬pstA1 mutant in NOS2 ؊/؊ mice was partially reversed by deletion of pe19, suggesting that increased membrane permeability due to PE19 overexpression sensitizes M. tuberculosis to host immunity. Our data indicate that PE19, which comprises only a 99-amino-acid PE domain, has a unique role in the permeability of the M. tuberculosis envelope that is regulated to resist stresses encountered in the host. O ver 15 years ago, the novel PE and PPE protein families were identified in the complete genome sequence of Mycobacterium tuberculosis; together, these proteins represent over 7% of the genome coding capacity (1). Despite the attention placed on these protein families, their functions remain largely uncharacterized. PE and PPE proteins are defined by conserved N-terminal domains of ϳ110 or ϳ180 amino acids that contain Pro-Glu (PE) or Pro-Pro-Glu (PPE) sequence motifs, respectively (1). Although PE and PPE proteins can be identified in the genomes of all sequenced members of the Mycobacterium genus, their expansion into large multiprotein families is restricted to the slow-growing pathogenic mycobacterial species, including M. tuberculosis, and associated with the expansion of the ESX type VII secretion systems (2). There is evidence that some PE and PPE proteins are exported to the bacterial cell surface or extracellular milieu in an ESX-dependent manner (3-6). ESX-dependent export requires specific sequences within the PE or PPE domain (7, 8), including a recently described YxxxD/E ESX secretion targeting motif located near the C terminus of the ϳ110-amino-acid PE domain (9).The 99 PE proteins and 69 PPE proteins encoded by the M. tuberculosis H37Rv genome can be further divided into subfamilies based on C-terminal sequence motifs (2). The PE_PGRS (polymorphic GC-...

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Mycobacterium tuberculosis Resists Stress by Regulating PE19 Expression

et al. 2016

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“…Unlike other PE-PPE proteins located in a row in the ESX region (20), MTBK_24820 exists independently, without PE proteins in the insertion region. MTBK_24820 is a PPE-MTPR subfamily with repeats of NxGxGNxG in the C terminus (17,21) and is orthologous to the M. tuberculosis H37Rv PPE39 protein (annotated Rv2353c) (22). PPE39 has a number of highly genetic variables among several M. tuberculosis isolates, caused by IS6110 integration and the addition of single-nucleotide polymorphisms (SNPs) (23).…”

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Protective Vaccine Efficacy of the Complete Form of PPE39 Protein from Mycobacterium tuberculosis Beijing/K Strain in Mice

Kim

Hur

et al. 2017

Clin Vaccine Immunol

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The aim of this study was to evaluate the protective efficacy of MTBK_ 24820, a complete form of PPE39 protein derived from a predominant Beijing/K strain of Mycobacterium tuberculosis in South Korea. Mice were immunized with MTKB_24820, M. bovis Bacilli Calmette-Guérin (BCG), or adjuvant prior to a high-dosed Beijing/K strain aerosol infection. After 4 and 9 weeks, bacterial loads were determined and histopathologic and immunologic features in the lungs and spleens of the M. tuberculosis-infected mice were analyzed. Putative immunogenic T-cell epitopes were examined using synthetic overlapping peptides. Successful immunization of MTBK_24820 in mice was confirmed by increased IgG responses (P Ͻ 0.05) and recalled gamma interferon (IFN-␥), interleukin-2 (IL-2), IL-6, and IL-17 responses (P Ͻ 0.05 or P Ͻ 0.01) to MTBK_24820. After challenge with the Beijing/K strain, an approximately 0.5 to 1.0 log 10 reduction in CFU in lungs and fewer lung inflammation lesions were observed in MTBK_24820-immunized mice compared to those for control mice. Moreover, MTBK_24820 immunization elicited significantly higher numbers of CD4 ϩ T cells producing protective cytokines, such as IFN-␥ and IL-17, in lungs and spleens (P Ͻ 0.01) and CD4 ϩ multifunctional T cells producing IFN-␥, tumor necrosis factor alpha (TNF-␣), and/or IL-17 (P Ͻ 0.01) than in control mice, suggesting protection comparable to that of BCG against the hypervirulent Beijing/K strain. The dominant immunogenic T-cell epitopes that induced IFN-␥ production were at the N terminus (amino acids 85 to 102 and 217 to 234). Its vaccine potential, along with protective immune responses in vivo, may be informative for vaccine development, particularly in regions where the M. tuberculosis Beijing/K-strain is frequently isolated from TB patients.

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“…PE and PPE family proteins, characterized by conserved Nterminal proline-glutamate (PE) and proline-proline-glutamate (PPE) motifs, are unique to mycobacteria [18]. There are 99 PE proteins and 69 PPE proteins in the M. tuberculosis H37Rv strain, and they represent about 10% of the total coding capacity of the M. tuberculosis genome [9].…”

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confidence: 99%

“…PE/PPE family proteins are mainly presented in pathogenic mycobacteria species and they are usually expressed during infection and secreted or exposed to the cell surface. All these factors imply that PE/PPE proteins play a critical role in mycobacterial pathogenicity [32,1,18]. Although the functions of these proteins are not fully understood, recent studies indicate that they were associated with antigenic diversity, hostepathogen interactions and immune evasion [2,20].…”

Section: Introductionmentioning

confidence: 99%

Mycobacterium tuberculosis PPE25 and PPE26 proteins expressed in Mycobacterium smegmatis modulate cytokine secretion in mouse macrophages and enhance mycobacterial survival

Bao

et al. 2017

Research in Microbiology

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Phylogeny to function: PE/PPE protein evolution and impact on Mycobacterium tuberculosis pathogenicity

Cited by 188 publications

References 118 publications

Mycobacterium tuberculosis Resists Stress by Regulating PE19 Expression

Mycobacterium tuberculosis Resists Stress by Regulating PE19 Expression

Protective Vaccine Efficacy of the Complete Form of PPE39 Protein from Mycobacterium tuberculosis Beijing/K Strain in Mice

Mycobacterium tuberculosis PPE25 and PPE26 proteins expressed in Mycobacterium smegmatis modulate cytokine secretion in mouse macrophages and enhance mycobacterial survival

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