Utilize este identificador para referenciar este registo: http://hdl.handle.net/10362/182879
Título: SARS-CoV2 Nsp1 is a metal-dependent DNA and RNA endonuclease
Autor: Salgueiro, Bruno A.
Saramago, Margarida
Tully, Mark D.
Issoglio, Federico
Silva, Sara T.N.
Paiva, Ana C.F.
Arraiano, Cecília M.
Matias, Pedro M.
Matos, Rute G.
Moe, Elin
Romão, Célia V.
Palavras-chave: Biophysics
Coronavirus
Magnesium
Manganese
Nuclease
SAXS
Biomaterials
Biochemistry, Genetics and Molecular Biology(all)
Agricultural and Biological Sciences(all)
Metals and Alloys
Data: 28-Mar-2024
Resumo: Over recent years, we have been living under a pandemic, caused by the rapid spread of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV2). One of the major virulence factors of Coronaviruses is the Non-structural protein 1 (Nsp1), known to suppress the host cells protein translation machinery, allowing the virus to produce its own proteins, propagate and invade new cells. To unveil the molecular mechanisms of SARS-CoV2 Nsp1, we have addressed its biochemical and biophysical properties in the presence of calcium, magnesium and manganese. Our findings indicate that the protein in solution is a monomer and binds to both manganese and calcium, with high affinity. Surprisingly, our results show that SARS-CoV2 Nsp1 alone displays metal-dependent endonucleolytic activity towards both RNA and DNA, regardless of the presence of host ribosome. These results show Nsp1 as new nuclease within the coronavirus family. Furthermore, the Nsp1 double variant R124A/K125A presents no nuclease activity for RNA, although it retains activity for DNA, suggesting distinct binding sites for DNA and RNA. Thus, we present for the first time, evidence that the activities of Nsp1 are modulated by the presence of different metals, which are proposed to play an important role during viral infection. This research contributes significantly to our understanding of the mechanisms of action of Coronaviruses.
Descrição: Funding Information: Open access funding provided by FCT|FCCN (b-on). This study was financially supported by the Portuguese Fundação para a Ciência e Tecnologia (FCT), Project MOSTMICRO-ITQB with references UIDB/04612/2020 and UIDP/04612/2020, iNOVA4Health (UIDB/04462/2020 and UIDP/04462/2020), and LS4FUTURE Associated Laboratory (LA/P/0087/2020). BAS is recipient of FCT PhD4COVID grant SFRH/BD/08066/2020; RGM is a recipient of an FCT CEEC contract (CEECIND/02065/2017); MS and EM are recipients of FCT DL57; CVR is recipient of FCT Institutional CEEC. Publisher Copyright: © The Author(s) 2024.
Peer review: yes
URI: http://hdl.handle.net/10362/182879
DOI: https://doi.org/10.1007/s10534-024-00596-z
ISSN: 0966-0844
Aparece nas colecções:Home collection (ITQB)

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