Triggering role of acid sphingomyelinase in endothelial lysosome-membrane fusion and dysfunction in coronary arteries

Bao, Jun-Xiang; Xia, Min; Poklis, Justin L.; Han, Weiqing; Brimson, Christopher A.; Li, Pin‐Lan

doi:10.1152/ajpheart.00958.2009

Cited by 29 publications

(40 citation statements)

References 42 publications

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“…Finally, we showed that EBOV infection is completely blocked by vacuolin-1, a specific inhibitor of lysosomal exocytosis and ASMase translocation to the plasma membrane (4,8). This drug was specific for EBOV GP activity, as infection by VSV-G pseudotyped virus was unaffected after treatment.…”

Section: Discussionmentioning

confidence: 83%

“…ASMase appears to be recruited to sites of VLP binding or may induce binding of VLPs to cells. ASMase can be brought to the cell surface by an exocytosis-related mechanism (4,51). This may also bring other endosome-localized proteins to the cell surface.…”

Section: Discussionmentioning

confidence: 99%

“…Then, SM is either recycled back to the plasma membrane via exocytosis or delivered to lysosomes, where it is hydrolyzed to ceramide and phosphocholine by ASMase (31). However, membrane damage and the binding of microbial pathogens can result in the translocation of lysosomal ASMase to the outer leaflet of the plasma membrane, where it cleaves surface-exposed SM (4,51). The conversion of the SM in rafts to ceramide can result in raft enlargement, receptor clustering, membrane invagination, and macropinosome formation (22)(23)(24)59), all of which promote the uptake of particles, including viruses, into cells.…”

mentioning

confidence: 99%

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Ebolavirus Requires Acid Sphingomyelinase Activity and Plasma Membrane Sphingomyelin for Infection

Miller

Adhikary

Kolokoltsov

et al. 2012

J Virol

132

123

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Acid sphingomyelinase (ASMase) converts the lipid sphingomyelin (SM) to phosphocholine and ceramide and has optimum activity at acidic pH. Normally, ASMase is located in lysosomes and endosomes, but membrane damage or the interaction with some bacterial and viral pathogens can trigger its recruitment to the plasma membrane. Rhinovirus and measles viruses each require ASMase activity during early stages of infection. Both sphingomyelin and ceramide are important components of lipid rafts and are potent signaling molecules. Each plays roles in mediating macropinocytosis, which has been shown to be important for ebolavirus (EBOV) infection. Here, we investigated the role of ASMase and its substrate, SM, in EBOV infection. The work was performed at biosafety level 4 with wild-type virus with specificity and mechanistic analysis performed using virus pseudotypes and virus-like particles. We found that virus particles strongly associate with the SM-rich regions of the cell membrane and depletion of SM reduces EBOV infection. ASM-specific drugs and multiple small interfering RNAs strongly inhibit the infection by EBOV and EBOV glycoprotein pseudotyped viruses but not by the pseudotypes bearing the glycoprotein of vesicular stomatitis virus. Interestingly, the binding of virus-like particles to cells is strongly associated with surface-localized ASMase as well as SM-enriched sites. Our work suggests that ASMase activity and SM presence are necessary for efficient infection of cells by EBOV. The inhibition of this pathway may provide new avenues for drug treatment.

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Section: Discussionmentioning

confidence: 83%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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Ebolavirus Requires Acid Sphingomyelinase Activity and Plasma Membrane Sphingomyelin for Infection

Miller

Adhikary

Kolokoltsov

et al. 2012

J Virol

132

123

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“…Given that NOX activation requires many cofactors to work together, LRs provide a wonderful platform, for NOX and the other NADPH oxidase subunits and cofactors, to assemble and then work as an active enzymatic complex. Indeed, many studies, in house and outside, have demonstrated that LRs even provide the driving force that promotes the assembling of NOX with other NADPH oxidase subunits or cofactors (26,27,190,235,388,389,391,443,444,446,452,453).…”

Section: Redox Molecules Associated With Lrsmentioning

confidence: 99%

“…This leads to the activation of NADPH oxidase and production of O 2 -, resulting in prominent amplification of the transmembrane signals. Besides lipid components such as SM, ceramide and cholesterol, many other molecules, such as NADPH oxidase subunits, Rac, and other regulatory components are clustered to form complex signalosomes (27,190,335,446 (76,106,121,333).…”

Section: B Transmembrane Signaling Via Receptors In Nonphagocytic Cellsmentioning

confidence: 99%

Lipid Raft Redox Signaling: Molecular Mechanisms in Health and Disease

Jin

Zhang

Katirai

et al. 2011

Antioxidants & Redox Signaling

Self Cite

104

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Lipid rafts, the sphingolipid and cholesterol-enriched membrane microdomains, are able to form different membrane macrodomains or platforms upon stimulations, including redox signaling platforms, which serve as a critical signaling mechanism to mediate or regulate cellular activities or functions. In particular, this raft platform formation provides an important driving force for the assembling of NADPH oxidase subunits and the recruitment of other related receptors, effectors, and regulatory components, resulting, in turn, in the activation of NADPH oxidase and downstream redox regulation of cell functions. This comprehensive review attempts to summarize all basic and advanced information about the formation, regulation, and functions of lipid raft redox signaling platforms as well as their physiological and pathophysiological relevance. Several molecular mechanisms involving the formation of lipid raft redox signaling platforms and the related therapeutic strategies targeting them are discussed. It is hoped that all information and thoughts included in this review could provide more comprehensive insights into the understanding of lipid raft redox signaling, in particular, of their molecular mechanisms, spatial-temporal regulations, and physiological, pathophysiological relevances to human health and diseases. Antioxid. Redox Signal. 15, 1043-1083.

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Lysosomal Molecular Derangements in Atherosclerosis

Zhang

2015

Atherosclerosis

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Triggering role of acid sphingomyelinase in endothelial lysosome-membrane fusion and dysfunction in coronary arteries

Cited by 29 publications

References 42 publications

Ebolavirus Requires Acid Sphingomyelinase Activity and Plasma Membrane Sphingomyelin for Infection

Ebolavirus Requires Acid Sphingomyelinase Activity and Plasma Membrane Sphingomyelin for Infection

Lipid Raft Redox Signaling: Molecular Mechanisms in Health and Disease

Lysosomal Molecular Derangements in Atherosclerosis

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