Genetic deficiency and polymorphisms of cyclophilin A reveal its essential role for Human Coronavirus 229E replication

Brunn, Albrecht von; Ciesek, Sandra; Brunn, Brigitte von; Carbajo-Lozoya, Javier

doi:10.1016/j.coviro.2015.08.004

Cited by 34 publications

(45 citation statements)

References 53 publications

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“…For HCoV-NL63, we have recently shown that CypA expression is essential in CaCo-2 cells (Carbajo-Lozoya et al, 2014). Utilizing a Huh-7.5 CypA KD (knockdown) cell line, originally constructed for the study of the requirement of stable CypA for HCV replication (von Hahn et al, 2012) we found significantly reduced replication of a HCoV-229E-Renilla luciferase expressing virus (von Brunn et al, 2015). This indicates the involvement of CypA also in replication of HCoV-229E.…”

Section: Discussionmentioning

confidence: 84%

Influences of cyclosporin A and non-immunosuppressive derivatives on cellular cyclophilins and viral nucleocapsid protein during human coronavirus 229E replication

et al. 2020

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The well-known immunosuppressive drug cyclosporin A inhibits replication of various viruses including coronaviruses by binding to cellular cyclophilins thus inactivating their cis-trans peptidyl-prolyl isomerase function. Viral nucleocapsid proteins are inevitable for genome encapsidation and replication. Here we demonstrate the interaction between the N protein of HCoV-229E and cyclophilin A, not cyclophilin B. Cyclophilin inhibitors abolish this interaction. Upon infection, cyclophilin A stays evenly distributed throughout the cell, whereas cyclophilin B concentrates at ER-bleb-like structures. We further show the inhibitory potential of non-immunosuppressive CsA derivatives Alisporivir, NIM811, compound 3 on HCoV-229E-GFP and -Luciferase replication in human Huh-7.5 hepatoma cells at 18 and 48 h time points post infection with EC 50 s at low micromolar ranges. Thus, non-immunosuppressive CsA derivatives effectively inhibit HCoV-229E replication suggesting them as possible candidates for the treatment of HCoV infection. The interruption of interaction between CypA and N protein by CsA and its derivatives suggest a mechanism how CypA inhibitors suppress viral replication.

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Section: Discussionmentioning

confidence: 84%

Influences of cyclosporin A and non-immunosuppressive derivatives on cellular cyclophilins and viral nucleocapsid protein during human coronavirus 229E replication

et al. 2020

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“…Subsequently, the importance of CypA as a host factor in CoV replication was further substantiated using knockdown or knockout of CypA expression, which was achieved using a variety of approaches. In Caco-2 and Huh7.5 cells, shRNA-mediated knockdown of CypA mRNA expression to below 3% of the normal levels was reported to nearly completely block HCoV-NL63 replication (Carbajo-Lozoya et al, 2014) and reduce HCoV-229E-driven luciferase expression by 10-to 20-fold (von Brunn et al, 2015). CypA-or CypB-knockout in feline fcwf-4 cells resulted in a near-complete block of FCoV replication.…”

Section: The Potential Role Of Cyps In Coronavirus Infectionmentioning

confidence: 95%

Cyclophilins and cyclophilin inhibitors in nidovirus replication

et al. 2018

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Cyclophilins (Cyps) belong to the family of peptidyl-prolyl isomerases (PPIases). The PPIase activity of most Cyps is inhibited by the immunosuppressive drug cyclosporin A and several of its non-immunosuppressive analogs, which can also block the replication of nidoviruses (arteriviruses and coronaviruses). Cyclophilins have been reported to play an essential role in the replication of several other RNA viruses, including human immunodeficiency virus-1, hepatitis C virus, and influenza A virus. Likewise, the replication of various nidoviruses was reported to depend on Cyps or other PPIases. This review summarizes our current understanding of this class of nidovirus-host interactions, including the potential function of in particular CypA and the inhibitory effect of Cyp inhibitors. Also the involvement of the FK-506-binding proteins and parvulins is discussed. The nidovirus data are placed in a broader perspective by summarizing the most relevant data on Cyp interactions and Cyp inhibitors for other RNA viruses.

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“…Previously, CypA and/or CypB were reported to play a role in the replication of a number of arteri-and coronaviruses (Carbajo-Lozoya et al, 2014;de Wilde et al, 2013a;Tanaka et al, 2017;von Brunn et al, 2015). The degree of sensitivity to Cyp depletion appeared to differ between these viruses, but was not compared directly.…”

Section: Nidovirus Replication In Cyclophilin-knockout Cell Poolsmentioning

confidence: 99%

“…Cyclophilins were initially implicated as host factors in nidovirus replication during studies with general Cyp inhibitors such as cyclosporine A (CsA). In cell culture, the replication of a variety of coronaviruses and arteriviruses was found to be strongly inhibited by lowmicromolar concentrations of CsA and the non-immunosuppressive CsA analogs Alisporivir (ALV) and NIM-811 (Carbajo-Lozoya et al, 2014de Wilde et al, 2017ade Wilde et al, , 2013bde Wilde et al, , 2011Kim and Lee, 2014;Tanaka et al, 2012;von Brunn, 2015;von Brunn et al, 2015). Subsequently, it was established that nidovirus replication can depend specifically on CypA and/or CypB.…”

Section: Introductionmentioning

confidence: 99%

Coronaviruses and arteriviruses display striking differences in their cyclophilin A-dependence during replication in cell culture

et al. 2018

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Cyclophilin A (CypA) is an important host factor in the replication of a variety of RNA viruses. Also the replication of several nidoviruses was reported to depend on CypA, although possibly not to the same extent. These prior studies are difficult to compare, since different nidoviruses, cell lines and experimental set-ups were used. Here, we investigated the CypA dependence of three distantly related nidoviruses that can all replicate in Huh7 cells: the arterivirus equine arteritis virus (EAV), the alphacoronavirus human coronavirus 229E (HCoV-229E), and the betacoronavirus Middle East respiratory syndrome coronavirus (MERS-CoV). The replication of these viruses was compared in the same parental Huh7 cells and in CypA-knockout Huh7 cells generated using CRISPR/Cas9-technology. CypA depletion reduced EAV yields by ~ 3-log, whereas MERS-CoV progeny titers were modestly reduced (3-fold) and HCoV-229E replication was unchanged. This study reveals that the replication of nidoviruses can differ strikingly in its dependence on cellular CypA.

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Genetic deficiency and polymorphisms of cyclophilin A reveal its essential role for Human Coronavirus 229E replication

Cited by 34 publications

References 53 publications

Influences of cyclosporin A and non-immunosuppressive derivatives on cellular cyclophilins and viral nucleocapsid protein during human coronavirus 229E replication

Influences of cyclosporin A and non-immunosuppressive derivatives on cellular cyclophilins and viral nucleocapsid protein during human coronavirus 229E replication

Cyclophilins and cyclophilin inhibitors in nidovirus replication

Coronaviruses and arteriviruses display striking differences in their cyclophilin A-dependence during replication in cell culture

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