Screening Mycobacterium tuberculosis Secreted Proteins Identifies Mpt64 as a Eukaryotic Membrane-Binding Bacterial Effector

Stamm, Chelsea E.; Pasko, Breanna L.; Chaisavaneeyakorn, Sujittra; Franco, Luis H.; Nair, Vidhya R.; Weigele, Bethany A.; Alto, Neal M.; Shiloh, Michael U.

doi:10.1128/msphere.00354-19

Cited by 24 publications

(19 citation statements)

References 150 publications

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“…yEGFP-SopF was produced at equivalent levels in all yeast strains upon galactose induction (S3C Fig). Notably, the steady-state subcellular localization of SopF in yeast (internal membrane sites; Fig 3A, S3B Fig) and mammalian cells (plasma membrane; Figs 2C and 3B) differed, similar to what has previously been reported for some secreted bacterial proteins [58,65]. This may be a consequence of imaging in live (yeast) versus formaldehyde-fixed (HeLa) cells.…”

Section: Resultssupporting

confidence: 78%

SopF, a phosphoinositide binding effector, promotes the stability of the nascent Salmonella-containing vacuole

et al. 2019

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The enteric bacterial pathogen Salmonella enterica serovar Typhimurium ( S . Typhimurium), utilizes two type III secretion systems (T3SSs) to invade host cells, survive and replicate intracellularly. T3SS1 and its dedicated effector proteins are required for bacterial entry into non-phagocytic cells and establishment and trafficking of the nascent Salmonella -containing vacuole (SCV). Here we identify the first T3SS1 effector required to maintain the integrity of the nascent SCV as SopF. SopF associates with host cell membranes, either when translocated by bacteria or ectopically expressed. Recombinant SopF binds to multiple phosphoinositides in protein-lipid overlays, suggesting that it targets eukaryotic cell membranes via phospholipid interactions. In yeast, the subcellular localization of SopF is dependent on the activity of Mss4, a phosphatidylinositol 4-phosphate 5-kinase that generates PI(4,5)P 2 from PI(4)P, indicating that membrane recruitment of SopF requires specific phospholipids. Ectopically expressed SopF partially colocalizes with specific phosphoinositide pools present on the plasma membrane in mammalian cells and with cytoskeletal-associated markers at the leading edge of cells. Translocated SopF concentrates on plasma membrane ruffles and around intracellular bacteria, presumably on the SCV. SopF is not required for bacterial invasion of non-phagocytic cells but is required for maintenance of the internalization vacuole membrane as infection with a S . Typhimurium Δ sopF mutant led to increased lysis of the SCV compared to wild type bacteria. Our structure-function analysis shows that the carboxy-terminal seven amino acids of SopF are essential for its membrane association in host cells and to promote SCV membrane stability. We also describe that SopF and another T3SS1 effector, SopB, act antagonistically to modulate nascent SCV membrane dynamics. In summary, our study highlights that a delicate balance of type III effector activities regulates the stability of the Salmonella internalization vacuole.

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Section: Resultssupporting

confidence: 78%

SopF, a phosphoinositide binding effector, promotes the stability of the nascent Salmonella-containing vacuole

et al. 2019

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“…This suggests that M. tuberculosis inhibits Perk signaling to delay apoptosis of the host cell thereby promoting bacterial replication. The Mpt64 protein ( Rv1980c ) has also been shown to localize to the ER to inhibit CHOP expression [ 39 ], although whether it inhibits upstream phosphorylation of Perk or eIF2α was not tested.…”

Section: Introductionmentioning

confidence: 99%

Effectors Targeting the Unfolded Protein Response during Intracellular Bacterial Infection

2021

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The unfolded protein response (UPR) is a homeostatic response to endoplasmic reticulum (ER) stress within eukaryotic cells. The UPR initiates transcriptional and post-transcriptional programs to resolve ER stress; or, if ER stress is severe or prolonged, initiates apoptosis. ER stress is a common feature of bacterial infection although the role of the UPR in host defense is only beginning to be understood. While the UPR is important for host defense against pore-forming toxins produced by some bacteria, other bacterial effector proteins hijack the UPR through the activity of translocated effector proteins that facilitate intracellular survival and proliferation. UPR-mediated apoptosis can limit bacterial replication but also often contributes to tissue damage and disease. Here, we discuss the dual nature of the UPR during infection and the implications of UPR activation or inhibition for inflammation and immunity as illustrated by different bacterial pathogens.

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“…Mycobacteria have several protein secretion systems including type VII secretion system for their housekeeping growth and modulation of infected host immune system (Ligon et al, 2012). By comparison with secreted proteins of M. tuberculosis reported previously (Penn et al, 2018;Stamm et al, 2019), we found that twenty-two M. tuberculosis proteins among 614 detected ones were indicated to be presumably secreted proteins (Supplementary Figure S8 and Supplementary Table S4). Six of these proteins are Mce family proteins which are secreted or on the cell surface to facilitate host cell entry (Chitale et al, 2001;Saini et al, 2008;Zhang et al, 2018).…”

Section: Detection Of Mycobacterial Proteins In Granulomatous Lesionsmentioning

confidence: 70%

“…FIGURE S8 | Venn diagram illustrating the number of proteins in common among the present (This_study) and previously reported studies (Penn et al, 2018;Stamm et al, 2019). The gene lists for Stamm_2019 and Penn_2018 were reported by Penn et al (2018) and Stamm et al (2019). TABLE S1 | Excel file of the raw and imputed data of all proteomic analyses for identification of human, M. tuberculosis, and MAH proteins in mycobacterial granulomatous lesions.…”

Section: Resultsmentioning

confidence: 97%

Proteomic Profiling Reveals the Architecture of Granulomatous Lesions Caused by Tuberculosis and Mycobacterium avium Complex Lung Disease

et al. 2020

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Tuberculosis (TB) and Mycobacterium avium complex lung disease (MAC-LD) are both characterized pathologically by granuloma lesions, which are typically composed of a necrotic caseum at the center surrounded by fibrotic cells and lymphocytes. Although the histological characterization of TB and MAC-LD granulomas has been well-documented, their molecular signatures have not been fully evaluated. In this research we applied mass spectrometry-based proteomics combined with laser microdissection to investigate the unique protein markers in human mycobacterial granulomatous lesions. Comparing the protein abundance between caseous and cellular sub-compartments of mycobacterial granulomas, we found distinct differences. Proteins involved in cellular metabolism in transcription and translation were abundant in cellular regions, while in caseous regions proteins related to antimicrobial response accumulated. To investigate the determinants of their heterogeneity, we compared the protein abundance in caseous regions between TB and MAC-LD granulomas. We found that several proteins were significantly abundant in the MAC-LD caseum of which proteomic profiles were different from those of the TB caseum. Immunohistochemistry demonstrated that one of these proteins, Angiogenin, specifically localized to the caseous regions of selected MAC-LD granulomas. We also detected peptides derived from mycobacterial proteins in the granulomas of both diseases. This study provides new insights into the architecture of granulomatous lesions in TB and MAC-LD.

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Screening Mycobacterium tuberculosis Secreted Proteins Identifies Mpt64 as a Eukaryotic Membrane-Binding Bacterial Effector

Cited by 24 publications

References 150 publications

SopF, a phosphoinositide binding effector, promotes the stability of the nascent Salmonella-containing vacuole

SopF, a phosphoinositide binding effector, promotes the stability of the nascent Salmonella-containing vacuole

Effectors Targeting the Unfolded Protein Response during Intracellular Bacterial Infection

Proteomic Profiling Reveals the Architecture of Granulomatous Lesions Caused by Tuberculosis and Mycobacterium avium Complex Lung Disease

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