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The coronavirus disease 2019 (COVID-19) pandemic, caused by the novel coronavirus severe acute respiratory syndrome coronavirus type 2 (SARS-CoV-2), has rapidly spread worldwide since its emergence in late 2019. Its ongoing evolution poses challenges for antiviral drug development. Coronavirus nsp6, a multiple-spanning transmembrane protein, participates in the biogenesis of the viral replication complex, which accommodates the viral replication-transcription complex. The roles of its structural domains in viral replication are not well studied. Herein, we predicted the structure of the SARS-CoV-2 nsp6 protein using AlphaFold2 and identified a highly folded C-terminal region (nsp6C) downstream of the transmembrane helices. The enhanced green fluorescent protein (EGFP)-fused nsp6C was found to cluster in the cytoplasm and associate with membranes. Functional mapping identified a minimal membrane-associated element (MAE) as the region from amino acids 237 to 276 (LGV-KLL), which is mainly composed of the α-helix H1 and the α-helix H2; the latter exhibits characteristics of an amphipathic helix (AH). Mutagenesis studies and membrane flotation experiments demonstrate that AH-like H2 is required for MAE-mediated membrane association. This MAE was functionally conserved across MERS-CoV, HCoV-OC43, HCoV-229E, HCoV-HKU1, and HCoV-NL63, all capable of mediating membrane association. In a SARS-CoV-2 replicon system, mutagenesis studies of H2 and replacements of H1 and H2 with their homologous counterparts demonstrated requirements of residues on both sides of the H2 and properly paired H1-H2 for MAE-mediated membrane association and viral replication. Notably, mutations I266A and K274A significantly attenuated viral replication without dramatically affecting membrane association, suggesting a dual role of the MAE in viral replication: mediating membrane association as well as participating in protein-protein interactions.IMPORTANCESevere acute respiratory syndrome coronavirus type 2 (SARS-CoV-2) assembles a double-membrane vesicle (DMV) by the viral non-structural proteins for viral replication. Understanding the mechanisms of the DMV assembly is of paramount importance for antiviral development. Nsp6, a multiple-spanning transmembrane protein, plays an important role in the DMV biogenesis. Herein, we predicted the nsp6 structure of SARS-CoV-2 and other human coronaviruses using AlphaFold2 and identified a putative membrane-associated element (MAE) in the highly conserved C-terminal regions of nsp6. Experimentally, we verified a functionally conserved minimal MAE composed of two α-helices, the H1, and the amphipathic helix-like H2. Mutagenesis studies confirmed the requirement of H2 for MAE-mediated membrane association and viral replication and demonstrated a dual role of the MAE in viral replication, by mediating membrane association and participating in residue-specific interactions. This functionally conserved MAE may serve as a novel anti-viral target.

Competing Interests: The authors declare no conflict of interest.

Titel:	Identification of a membrane-associated element (MAE) in the C-terminal region of SARS-CoV-2 nsp6 that is essential for viral replication.
Autor/in / Beteiligte Person:	Han, Y ; Yuan, Z ; Yi, Z
Zeitschrift:	Journal of virology, Jg. 98 (2024-05-14), Heft 5, S. e0034924
Veröffentlichung:	Washington Dc : American Society For Microbiology ; <i>Original Publication</i>: Baltimore, American Society for Microbiology., 2024
Medientyp:	academicJournal
ISSN:	1098-5514 (electronic)
DOI:	10.1128/jvi.00349-24
Schlagwort:	Animals Humans Amino Acid Sequence Betacoronavirus genetics Betacoronavirus physiology Betacoronavirus metabolism Cell Membrane metabolism Chlorocebus aethiops COVID-19 virology HEK293 Cells Pandemics Vero Cells SARS-CoV-2 genetics SARS-CoV-2 physiology SARS-CoV-2 metabolism Viral Nonstructural Proteins metabolism Viral Nonstructural Proteins genetics Viral Nonstructural Proteins chemistry Virus Replication
Sonstiges:	Nachgewiesen in: MEDLINE Sprachen: English Publication Type: Journal Article Language: English [J Virol] 2024 May 14; Vol. 98 (5), pp. e0034924. <i>Date of Electronic Publication: </i>2024 Apr 19. MeSH Terms: SARS-CoV-2* / genetics ; SARS-CoV-2* / physiology ; SARS-CoV-2* / metabolism ; Viral Nonstructural Proteins* / metabolism ; Viral Nonstructural Proteins* / genetics ; Viral Nonstructural Proteins* / chemistry ; Virus Replication* ; Animals ; Humans ; Amino Acid Sequence ; Betacoronavirus / genetics ; Betacoronavirus / physiology ; Betacoronavirus / metabolism ; Cell Membrane / metabolism ; Chlorocebus aethiops ; COVID-19 / virology ; HEK293 Cells ; Pandemics ; Vero Cells References: Chem Soc Rev. 2021 Mar 21;50(6):3647-3655. (PMID: 33524090) ; Nature. 2023 Mar;615(7950):143-150. (PMID: 36630998) ; Nat Rev Microbiol. 2021 Nov;19(11):685-700. (PMID: 34535791) ; Cell. 2020 May 14;181(4):914-921.e10. (PMID: 32330414) ; PLoS Biol. 2008 Sep 16;6(9):e226. (PMID: 18798692) ; Trends Immunol. 2020 Dec;41(12):1100-1115. (PMID: 33132005) ; J Biol Chem. 2020 Sep 11;295(37):12910-12934. (PMID: 32661197) ; mBio. 2017 Nov 21;8(6):. (PMID: 29162711) ; Proc Natl Acad Sci U S A. 2022 Apr 12;119(15):e2119893119. (PMID: 35385354) ; J Biol Chem. 2020 Aug 14;295(33):11742-11753. (PMID: 32587094) ; Biomolecules. 2018 Jul 05;8(3):. (PMID: 29976879) ; Virology. 2022 Aug;573:96-110. (PMID: 35738174) ; PLoS Pathog. 2022 Sep 1;18(9):e1010752. (PMID: 36048900) ; Emerg Infect Dis. 2004 Feb;10(2):320-6. (PMID: 15030705) ; Cell Chem Biol. 2021 Sep 16;28(9):1366-1378.e4. (PMID: 33798447) ; Rev Med Virol. 2023 Sep;33(5):e2464. (PMID: 37322826) ; Nat Commun. 2023 Nov 30;14(1):7894. (PMID: 38036567) ; Microb Pathog. 2021 Jan;150:104641. (PMID: 33242646) ; Antiviral Res. 2021 Jan;185:104974. (PMID: 33217430) ; J Virol. 2003 May;77(10):6055-61. (PMID: 12719597) ; Nat Rev Microbiol. 2021 Mar;19(3):155-170. (PMID: 33116300) ; PLoS Pathog. 2009 Mar;5(3):e1000351. (PMID: 19325881) ; mBio. 2023 Aug 31;14(4):e0068823. (PMID: 37477426) ; Virology. 2019 Sep;535:283-296. (PMID: 31369938) ; Science. 2020 Sep 11;369(6509):1395-1398. (PMID: 32763915) ; Cell Host Microbe. 2020 Dec 9;28(6):853-866.e5. (PMID: 33245857) ; Trends Microbiol. 2020 Dec;28(12):1022-1033. (PMID: 32536523) ; Nature. 2021 Aug;596(7873):583-589. (PMID: 34265844) ; Nature. 2022 Jun;606(7915):761-768. (PMID: 35551511) ; J Virol. 2002 Apr;76(8):3697-708. (PMID: 11907209) ; mBio. 2013 Aug 13;4(4):. (PMID: 23943763) ; Antiviral Res. 2023 May;213:105590. (PMID: 37003304) ; Nat Protoc. 2008;3(4):619-28. (PMID: 18388944) ; J Proteins Proteom. 2021;12(3):161-175. (PMID: 34121824) ; Cell Mol Life Sci. 2021 Feb;78(3):1085-1100. (PMID: 32562023) ; Front Immunol. 2020 Sep 11;11:552909. (PMID: 33013925) ; Proc Natl Acad Sci U S A. 2019 Jul 9;116(28):14029-14038. (PMID: 31239341) ; Elife. 2020 Apr 02;9:. (PMID: 32228860) ; Nat Rev Microbiol. 2021 Mar;19(3):141-154. (PMID: 33024307) ; J Biomed Sci. 2022 Sep 12;29(1):68. (PMID: 36096815) ; Front Immunol. 2022 Jul 26;13:834098. (PMID: 35958548) ; Nat Rev Mol Cell Biol. 2022 Jan;23(1):21-39. (PMID: 34824452) ; Cell. 2020 Jul 23;182(2):417-428.e13. (PMID: 32526208) ; PLoS Biol. 2020 Jun 8;18(6):e3000715. (PMID: 32511245) ; J Virol. 2009 Jul;83(13):6957-62. (PMID: 19386712) ; J Med Virol. 2022 Jun;94(6):2376-2383. (PMID: 35118687) ; Nat Commun. 2023 Apr 21;14(1):2308. (PMID: 37085489) Grant Information: 32270155, 81971926 MOST \| National Natural Science Foundation of China (NSFC); ZD2021CY001 Shanghai Municipal Science and Technology Major Project Contributed Indexing: Keywords: SARS-CoV-2; coronavirus; nsp6; replication; α-helix Substance Nomenclature: 0 (Viral Nonstructural Proteins) ; 0 (NSP6 protein, SARS-CoV-2) Entry Date(s): Date Created: 20240419 Date Completed: 20240514 Latest Revision: 20240604 Update Code: 20240605 PubMed Central ID: PMC11092323

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Identification of a membrane-associated element (MAE) in the C-terminal region of SARS-CoV-2 nsp6 that is essential for viral replication.