| Literature DB >> 33016799 |
Nanna-Sophie Brinck Andersen1,2, Sofie Eg Jørgensen1,2, Kristian Alsbjerg Skipper2, Simon Müller Larsen1, Johanna Heinz1, Michelle Mølgaard Thomsen1,2, Ensieh Farahani2, Yujia Cai2, Alon Schneider Hait1,2, Lise Kay3, Jacob Giehm Mikkelsen2, Mariane Høgsbjerg Schleimann1, Martin Kristian Thomsen2, Søren R Paludan2, Trine H Mogensen1,2,4.
Abstract
Paralytic poliomyelitis is a rare disease manifestation following poliovirus (PV) infection. The disease determinants remain largely unknown. We used whole exome sequencing to uncover possible contributions of host genetics to the development of disease outcome in humans with poliomyelitis. We identified a patient with a variant in ATG7, an important regulatory gene in the macroautophagy/autophagy pathway. PV infection did not induce a prominent type I interferon response, but rather activated autophagy in neuronal-like cells, and this was essential for viral control. Importantly, virus-induced autophagy was impaired in patient fibroblasts and associated with increased viral burden and enhanced cell death following infection. Lack of ATG7 prevented control of infection in neuronal-like cells, and reconstitution of patient cells with wild-type ATG7 reestablished autophagy-mediated control of infection. Collectively, these data suggest that ATG7 defect contributes to host susceptibility to PV infection and propose autophagy as an unappreciated antiviral effector in viral infection in humans.Entities:
Keywords: ATG7; autophagy; host genetics; innate immunity; neuronal-like cells; poliomyelitis; poliovirus; whole exome sequencing
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Year: 2020 PMID: 33016799 PMCID: PMC8496727 DOI: 10.1080/15548627.2020.1831800
Source DB: PubMed Journal: Autophagy ISSN: 1554-8627 Impact factor: 16.016