The p60 and NamA autolysins from<i>L</i><i>isteria monocytogenes</i>contribute to host colonization and induction of protective memory

Chandrabos, Ceena; Soudja, Saïdi M.; Weinrick, Brian; Gros, Marilyn; Frangaj, Aurel; Rahmoun, Massilva; Jacobs, William R.; Lauvau, Grégoire

doi:10.1111/cmi.12362

Cited by 10 publications

(6 citation statements)

References 46 publications

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“…First, we examined wild type Lm, Lm-∆ secA2 and Lm-∆ secA 2::SecA2 strep for changes in morphology during exponential growth phase using light microscopy. Lm-∆ secA2 form long cell chains due to a septal defect that results from lack of the secretion of p60/Iap and MurA/NamA [ 16 , 17 , 18 ] ( Figure 1 A). The complemented recombinant strain Lm-∆ secA 2::SecA2 strep had reverted to the single cell morphology seen with wild type (Lm) bacteria ( Figure 1 A).…”

Section: Resultsmentioning

confidence: 99%

“…L. monocytogenes secretes 19 proteins in a SecA2-dependent manner [ 4 , 16 ]. The cell wall-secreted hydrolases autolysin p60 (protein of 60 kDa, or Iap (Invasion associated protein) also called CwhA (cell wall hydrolase A)) and the muramidase MurA (also called NamA [N-acetylmuramidase A]), known to be involved in cell division, are well known SecA2 substrates [ 16 , 17 , 18 ]. Listeria lacking SecA2 show reduced secretion of both p60 and MurA in the supernatant of growing bacteria, and exhibit a chain-like cell morphology manifesting in a rough colony type [ 15 , 17 ].…”

Section: Introductionmentioning

confidence: 99%

“…Listeria lacking SecA2 show reduced secretion of both p60 and MurA in the supernatant of growing bacteria, and exhibit a chain-like cell morphology manifesting in a rough colony type [ 15 , 17 ]. The reduced secretion of SecA2-dependent proteins such as p60 has been implicated in the diminished virulence phenotype [ 16 , 18 , 19 , 20 ]. Additionally, SecA2-inactivation affects significantly the degree of hydrophilicity and Lewis acid-based properties, and thereby affects the cell surface properties of L. monocytogenes [ 21 ].…”

Section: Introductionmentioning

confidence: 99%

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SecA2 Associates with Translating Ribosomes and Contributes to the Secretion of Potent IFN-β Inducing RNAs

Teubner

Frantz

Pietra

et al. 2022

IJMS

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Protein secretion plays a central role in modulating interactions of the human pathogen Listeria monocytogenes with its environment. Recently, secretion of RNA has emerged as an important strategy used by the pathogen to manipulate the host cell response to its advantage. In general, the Sec-dependent translocation pathway is a major route for protein secretion in L. monocytogenes, but mechanistic insights into the secretion of RNA by these pathways are lacking. Apart from the classical SecA1 secretion pathway, L. monocytogenes also encodes for a SecA paralogue (SecA2) which targets the export of a specific subset of proteins, some of which are involved in virulence. Here, we demonstrated that SecA2 co-sediments with translating ribosomes and provided evidence that it associates with a subset of secreted small non-coding RNAs (sRNAs) that induce high levels of IFN-β response in host cells. We found that enolase, which is translocated by a SecA2-dependent mechanism, binds to several sRNAs, suggesting a pathway by which sRNAs are targeted to the supernatant of L. monocytogenes.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

SecA2 Associates with Translating Ribosomes and Contributes to the Secretion of Potent IFN-β Inducing RNAs

Teubner

Frantz

Pietra

et al. 2022

IJMS

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“…Fractions were dried in a lyophilizer and resuspended to their injection volume. The bioactive fraction was subsequently analyzed by ultra-performance liquid chromatography tandem MS (UPLC-MS/MS) (38). Fractions were separated on a Waters Acquity UPLC system in HILIC mode coupled to a Waters Synapt G2 quadrupole time-of-flight mass spectrometer, which was used to analyze the eluate.…”

Section: Reagentsmentioning

confidence: 99%

Vaginal microbiome modulates topical antiretroviral drug pharmacokinetics

Taneva¹,

Sinclair²,

Mesquita³

et al. 2018

JCI Insight

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Tenofovir gel and dapivirine ring provided variable HIV protection in clinical trials, reflecting poor adherence and possibly biological factors. We hypothesized that vaginal microbiota modulates pharmacokinetics and tested the effects of pH, individual bacteria, and vaginal swabs from women on pharmacokinetics and antiviral activity. Tenofovir, but not dapivirine, uptake by human cells was reduced as pH increased. Lactobacillus crispatus actively transported tenofovir leading to a loss in drug bioavailability and culture supernatants from Gardnerella vaginalis, but not Atopobium vaginae, blocked tenofovir endocytosis. The inhibition of endocytosis mapped to adenine. Adenine increased from 65.5 μM in broth to 246 μM in Gardnerella, but decreased to 9.5 μM in Atopobium supernatants. This translated into a decrease in anti-HIV activity when Gardnerella supernatants or adenine were added to cultures. Dapivirine was also impacted by microbiota, as drug bound irreversibly to bacteria, resulting in decreased antiviral activity. When drugs were incubated with vaginal swabs, 30.7% ± 5.7% of dapivirine and 63.9% ± 8.8% of tenofovir were recovered in supernatants after centrifugation of the bacterial cell pellet. In contrast, no impact of microbiota on the pharmacokinetics of the prodrugs, tenofovir disoproxil fumarate or tenofovir alafenamide, was observed. Together, these results demonstrate that microbiota may impact pharmacokinetics and contribute to inconsistent efficacy.

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“…Multi-substrate SecA2 systems export more than one substrate, although the number of exported substrates is still small when compared to the general Sec system. The multi-substrate SecA2 systems of Mycobacterium tuberculosis (46, 47), Listeria monocytogenes (48, 49) and likely Bacillus anthracis (50, 51) are required for pathogenesis. In Corynebacterium glutamicum (52) and Clostridium difficile (53) their multi-substrate systems are essential for bacterial viability.…”

Section: Introductionmentioning

confidence: 99%

The Two Distinct Types of SecA2-Dependent Export Systems

2019

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In addition to SecA of the general Sec system, many Gram-positive bacteria including mycobacteria express SecA2, a second, transport-associated ATPase. SecA2s can be subdivided into two mechanistically distinct types: 1) SecA2s that are part of the accessory Sec (aSec) system, a specialized transporter mediating the export of a family of serine-rich repeat (SRR) glycoproteins that function as adhesins; 2) SecA2s that are part of multi-substrate systems, in which SecA2 interacts with components of the general Sec system, specifically the SecYEG channel, to export multiple types of substrates. Found mainly in streptococci and staphylococci, the aSec system also contains SecY2 and novel accessory Sec proteins (Asps) that are required for optimal export. Asp2 also acetylates glucosamine residues on the SRR domains of the substrate during transport. Targeting of the SRR substrate to SecA2 and the aSec translocon is mediated by a specialized signal peptide. Multi-substrate SecA2 systems are present in mycobacteria, corynebacteria, listeria, clostridium and some bacillus. Although most substrates for this SecA2 have canonical signal peptides that are required for export, targeting to SecA2 appears to depend on structural features of the mature protein. The feature of the mature domains of these proteins that renders them dependent on SecA2 for export may be their potential to fold in the cytoplasm. The discovery of aSec and multi-substrate SecA2 systems expands our appreciation of the diversity of bacterial export pathways. Here, we present our current understanding of the mechanisms of each of these SecA2 systems.

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The p60 and NamA autolysins fromListeria monocytogenescontribute to host colonization and induction of protective memory

Cited by 10 publications

References 46 publications

SecA2 Associates with Translating Ribosomes and Contributes to the Secretion of Potent IFN-β Inducing RNAs

SecA2 Associates with Translating Ribosomes and Contributes to the Secretion of Potent IFN-β Inducing RNAs

Vaginal microbiome modulates topical antiretroviral drug pharmacokinetics

The Two Distinct Types of SecA2-Dependent Export Systems

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