TMEM41B and VMP1 modulate cellular lipid and energy metabolism for facilitating dengue virus infection

Transmembrane Protein 41B (TMEM41B) and Vacuole Membrane Protein 1 (VMP1) are two ER-associated lipid scramblases that play a role in autophagosome formation and cellular lipid metabolism. TMEM41B is also a recently validated host factor required by flaviviruses and coronaviruses. However, the exact...

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Autores principales: Yousefi, Meisam, Lee, Wai Suet, Yan, Biaoguo, Cui, Liang, Yong, Cythia Lingli, Yap, Xin, Tay, Kwan Sing Leona, Qiao, Wenjie, Tan, Dewei, Nurazmi, Nur Insyirah, Linster, Martin, Smith, Gavin J. D., Lee, Yie Hou, Carette, Jan E., Ooi, Eng Eong, Chan, Kuan Rong, Ooi, Yaw Shin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9387935/
https://www.ncbi.nlm.nih.gov/pubmed/35939522
http://dx.doi.org/10.1371/journal.ppat.1010763
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author Yousefi, Meisam
Lee, Wai Suet
Yan, Biaoguo
Cui, Liang
Yong, Cythia Lingli
Yap, Xin
Tay, Kwan Sing Leona
Qiao, Wenjie
Tan, Dewei
Nurazmi, Nur Insyirah
Linster, Martin
Smith, Gavin J. D.
Lee, Yie Hou
Carette, Jan E.
Ooi, Eng Eong
Chan, Kuan Rong
Ooi, Yaw Shin
author_facet Yousefi, Meisam
Lee, Wai Suet
Yan, Biaoguo
Cui, Liang
Yong, Cythia Lingli
Yap, Xin
Tay, Kwan Sing Leona
Qiao, Wenjie
Tan, Dewei
Nurazmi, Nur Insyirah
Linster, Martin
Smith, Gavin J. D.
Lee, Yie Hou
Carette, Jan E.
Ooi, Eng Eong
Chan, Kuan Rong
Ooi, Yaw Shin
author_sort Yousefi, Meisam
collection PubMed
description Transmembrane Protein 41B (TMEM41B) and Vacuole Membrane Protein 1 (VMP1) are two ER-associated lipid scramblases that play a role in autophagosome formation and cellular lipid metabolism. TMEM41B is also a recently validated host factor required by flaviviruses and coronaviruses. However, the exact underlying mechanism of TMEM41B in promoting viral infections remains an open question. Here, we validated that both TMEM41B and VMP1 are essential host dependency factors for all four serotypes of dengue virus (DENV) and human coronavirus OC43 (HCoV-OC43), but not chikungunya virus (CHIKV). While HCoV-OC43 failed to replicate entirely in both TMEM41B- and VMP1-deficient cells, we detected diminished levels of DENV infections in these cell lines, which were accompanied by upregulation of the innate immune dsRNA sensors, RIG-I and MDA5. Nonetheless, this upregulation did not correspondingly induce the downstream effector TBK1 activation and Interferon-beta expression. Despite low levels of DENV replication, classical DENV replication organelles were undetectable in the infected TMEM41B-deficient cells, suggesting that the upregulation of the dsRNA sensors is likely a consequence of aberrant viral replication rather than a causal factor for reduced DENV infection. Intriguingly, we uncovered that the inhibitory effect of TMEM41B deficiency on DENV replication, but not HCoV-OC43, can be partially reversed using exogenous fatty acid supplements. In contrast, VMP1 deficiency cannot be rescued using the metabolite treatment. In line with the observed phenotypes, we found that both TMEM41B- and VMP1-deficient cells harbor higher levels of compromised mitochondria, especially in VMP1 deficiency which results in severe dysregulations of mitochondrial beta-oxidation. Using a metabolomic profiling approach, we revealed distinctive global dysregulations of the cellular metabolome, particularly lipidome, in TMEM41B- and VMP1-deficient cells. Our findings highlight a central role for TMEM41B and VMP1 in modulating multiple cellular pathways, including lipid mobilization, mitochondrial beta-oxidation, and global metabolic regulations, to facilitate the replication of flaviviruses and coronaviruses.
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spelling pubmed-93879352022-08-19 TMEM41B and VMP1 modulate cellular lipid and energy metabolism for facilitating dengue virus infection Yousefi, Meisam Lee, Wai Suet Yan, Biaoguo Cui, Liang Yong, Cythia Lingli Yap, Xin Tay, Kwan Sing Leona Qiao, Wenjie Tan, Dewei Nurazmi, Nur Insyirah Linster, Martin Smith, Gavin J. D. Lee, Yie Hou Carette, Jan E. Ooi, Eng Eong Chan, Kuan Rong Ooi, Yaw Shin PLoS Pathog Research Article Transmembrane Protein 41B (TMEM41B) and Vacuole Membrane Protein 1 (VMP1) are two ER-associated lipid scramblases that play a role in autophagosome formation and cellular lipid metabolism. TMEM41B is also a recently validated host factor required by flaviviruses and coronaviruses. However, the exact underlying mechanism of TMEM41B in promoting viral infections remains an open question. Here, we validated that both TMEM41B and VMP1 are essential host dependency factors for all four serotypes of dengue virus (DENV) and human coronavirus OC43 (HCoV-OC43), but not chikungunya virus (CHIKV). While HCoV-OC43 failed to replicate entirely in both TMEM41B- and VMP1-deficient cells, we detected diminished levels of DENV infections in these cell lines, which were accompanied by upregulation of the innate immune dsRNA sensors, RIG-I and MDA5. Nonetheless, this upregulation did not correspondingly induce the downstream effector TBK1 activation and Interferon-beta expression. Despite low levels of DENV replication, classical DENV replication organelles were undetectable in the infected TMEM41B-deficient cells, suggesting that the upregulation of the dsRNA sensors is likely a consequence of aberrant viral replication rather than a causal factor for reduced DENV infection. Intriguingly, we uncovered that the inhibitory effect of TMEM41B deficiency on DENV replication, but not HCoV-OC43, can be partially reversed using exogenous fatty acid supplements. In contrast, VMP1 deficiency cannot be rescued using the metabolite treatment. In line with the observed phenotypes, we found that both TMEM41B- and VMP1-deficient cells harbor higher levels of compromised mitochondria, especially in VMP1 deficiency which results in severe dysregulations of mitochondrial beta-oxidation. Using a metabolomic profiling approach, we revealed distinctive global dysregulations of the cellular metabolome, particularly lipidome, in TMEM41B- and VMP1-deficient cells. Our findings highlight a central role for TMEM41B and VMP1 in modulating multiple cellular pathways, including lipid mobilization, mitochondrial beta-oxidation, and global metabolic regulations, to facilitate the replication of flaviviruses and coronaviruses. Public Library of Science 2022-08-08 /pmc/articles/PMC9387935/ /pubmed/35939522 http://dx.doi.org/10.1371/journal.ppat.1010763 Text en © 2022 Yousefi et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Yousefi, Meisam
Lee, Wai Suet
Yan, Biaoguo
Cui, Liang
Yong, Cythia Lingli
Yap, Xin
Tay, Kwan Sing Leona
Qiao, Wenjie
Tan, Dewei
Nurazmi, Nur Insyirah
Linster, Martin
Smith, Gavin J. D.
Lee, Yie Hou
Carette, Jan E.
Ooi, Eng Eong
Chan, Kuan Rong
Ooi, Yaw Shin
TMEM41B and VMP1 modulate cellular lipid and energy metabolism for facilitating dengue virus infection
title TMEM41B and VMP1 modulate cellular lipid and energy metabolism for facilitating dengue virus infection
title_full TMEM41B and VMP1 modulate cellular lipid and energy metabolism for facilitating dengue virus infection
title_fullStr TMEM41B and VMP1 modulate cellular lipid and energy metabolism for facilitating dengue virus infection
title_full_unstemmed TMEM41B and VMP1 modulate cellular lipid and energy metabolism for facilitating dengue virus infection
title_short TMEM41B and VMP1 modulate cellular lipid and energy metabolism for facilitating dengue virus infection
title_sort tmem41b and vmp1 modulate cellular lipid and energy metabolism for facilitating dengue virus infection
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9387935/
https://www.ncbi.nlm.nih.gov/pubmed/35939522
http://dx.doi.org/10.1371/journal.ppat.1010763
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