Disruption of the ESX‐5 system of <i>Mycobacterium tuberculosis</i> causes loss of PPE protein secretion, reduction of cell wall integrity and strong attenuation

Bottai, Daria; Luca, Mariagrazia Di; Majlessi, Laleh; Frigui, Wafa; Siméone, Roxane; Sayes, Fadel; Bitter, Wilbert; Brennan, Michael J.; Leclerc, Claude; Batoni, Giovanna; Campa, Mario; Brosch, Roland; Esin, Semih

doi:10.1111/j.1365-2958.2012.08001.x

Cited by 169 publications

(256 citation statements)

References 56 publications

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“…S4, lanes 1-8). M. tuberculosis expresses and secretes endogenous PPE41 (30), and consequently PPE41 was detected in the supernatant of strains with and without plasmids. However, introduction of the WT operon on a plasmid resulted in elevated PPE41 levels in the culture supernatant, whereas in strains harboring plasmids with truncated forms of PE25, the PPE41 levels in the culture supernatant were reduced to background levels.…”

Section: Resultsmentioning

confidence: 99%

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General secretion signal for the mycobacterial type VII secretion pathway

Daleke

Ummels

Bawono³

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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178

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Mycobacterial pathogens use specialized type VII secretion (T7S) systems to transport crucial virulence factors across their unusual cell envelope into infected host cells. These virulence factors lack classical secretion signals and the mechanism of substrate recognition is not well understood. Here we demonstrate that the model T7S substrates PE25/PPE41, which form a heterodimer, are targeted to the T7S pathway ESX-5 by a signal located in the C terminus of PE25. Site-directed mutagenesis of residues within this C terminus resulted in the identification of a highly conserved motif, i.e., YxxxD/E, which is required for secretion. This motif was also essential for the secretion of LipY, another ESX-5 substrate. Pathogenic mycobacteria have several different T7S systems and we identified a PE protein that is secreted by the ESX-1 system, which allowed us to compare substrate recognition of these two T7S systems. Surprisingly, this ESX-1 substrate contained a C-terminal signal functionally equivalent to that of PE25. Exchange of these C-terminal secretion signals between the PE proteins restored secretion, but each PE protein remained secreted via its own ESX secretion system, indicating that an additional signal(s) provides system specificity. Remarkably, the YxxxD/E motif was also present in and required for efficient secretion of the ESX-1 substrates CFP-10 and EspB. Therefore, our data show that the YxxxD/E motif is a general secretion signal that is present in all known mycobacterial T7S substrates or substrate complexes.

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Section: Resultsmentioning

confidence: 99%

“…Previously, PPE41 was shown to be exported by ESX-5, both in its native host M. tuberculosis (30) and in M. marinum upon heterologous expression (20). The PPE41 gene forms an operon with PE25 (31) and both proteins form a heterodimer when expressed in Escherichia coli (32).…”

Section: Resultsmentioning

confidence: 99%

General secretion signal for the mycobacterial type VII secretion pathway

Daleke

Ummels

Bawono³

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

178

224

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“…Finally, although originally the esx family was considered to be as early secreted antigens, expressed only during the early stage of Mtb infection, new evidence suggests that this family of genes may be secreted and expressed at different stages of the life cycle of TB. [48][49][50] Accordingly these studies suggest that the RSQ-15 vaccine may not only be studied as a prophylactic vaccine, but may also be examined as a post-exposure vaccine against latent TB.…”

Section: Discussionmentioning

confidence: 99%

Multivalent TB vaccines targeting the esx gene family generate potent and broad cell-mediated immune responses superior to BCG

Villarreal¹,

Walters

Laddy

et al. 2014

Human Vaccines & Immunotherapeutics

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“…These structures define the key elements of the PPE-EspG interaction and, coupled with bioinformatics and biochemical interaction studies, suggest that EspGs function as adaptors to deliver PE-PPE complexes to their cognate ESX system for translocation across the plasma membrane. Moreover, our work shows that the vast majority of PE-PPE proteins in Mtb interact with EspG from the ESX-5 secretion system, which has been hypothesized to play a major role in PE-PPE protein secretion (9,20,23).…”

mentioning

confidence: 99%

Structure of a PE–PPE–EspG complex fromMycobacterium tuberculosisreveals molecular specificity of ESX protein secretion

Ekiert

Cox

2014

Proc. Natl. Acad. Sci. U.S.A.

131

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Nearly 10% of the coding capacity of the Mycobacterium tuberculosis genome is devoted to two highly expanded and enigmatic protein families called PE and PPE, some of which are important virulence/immunogenicity factors and are secreted during infection via a unique alternative secretory system termed "type VII." How PE-PPE proteins function during infection and how they are translocated to the bacterial surface through the five distinct type VII secretion systems [ESAT-6 secretion system (ESX)] of M. tuberculosis is poorly understood. Here, we report the crystal structure of a PE-PPE heterodimer bound to ESX secretion-associated protein G (EspG), which adopts a novel fold. This PE-PPE-EspG complex, along with structures of two additional EspGs, suggests that EspG acts as an adaptor that recognizes specific PE-PPE protein complexes via extensive interactions with PPE domains, and delivers them to ESX machinery for secretion. Surprisingly, secretion of most PE-PPE proteins in M. tuberculosis is likely mediated by EspG from the ESX-5 system, underscoring the importance of ESX-5 in mycobacterial pathogenesis. Moreover, our results indicate that PE-PPE domains function as cis-acting targeting sequences that are read out by EspGs, revealing the molecular specificity for secretion through distinct ESX pathways.tuberculosis | protein secretion | antigenic variation | virulence factor | host-pathogen interactions

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Disruption of the ESX‐5 system of Mycobacterium tuberculosis causes loss of PPE protein secretion, reduction of cell wall integrity and strong attenuation

Cited by 169 publications

References 56 publications

General secretion signal for the mycobacterial type VII secretion pathway

General secretion signal for the mycobacterial type VII secretion pathway

Multivalent TB vaccines targeting the esx gene family generate potent and broad cell-mediated immune responses superior to BCG

Structure of a PE–PPE–EspG complex fromMycobacterium tuberculosisreveals molecular specificity of ESX protein secretion

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