Broadly neutralizing antibodies isolated from HEV convalescents confer protective effects in human liver-chimeric mice.

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Tác giả: Patrick Behrendt, Laura Corneillie, Maura Dandri, Viet Loan Dao Thi, Katja Dinkelborg, Lukas Fehlau, Jonathan Garn, Elina M Guzman, Florian Hinte, Lucas Hueffner, Carina Jacobsen, Anke R M Kraft, Thomas Krey, Marc Lütgehetmann, Ann-Kathrin Mehnert, Philip Meuleman, Nele Meyer, Prossie L Nankya, Thomas Pietschmann, Nina Plückebaum, Sarah Prallet, George Ssebyatika, Eike Steinmann, Luisa J Ströh, Lieven Verhoye, Abel Viejo-Borbolla, Heiner Wedemeyer

Ngôn ngữ: eng

Ký hiệu phân loại:

Thông tin xuất bản: England : Nature communications , 2025

Mô tả vật lý:

Bộ sưu tập: NCBI

ID: 681077

Hepatitis E virus (HEV) causes 3.3 million symptomatic cases and 44,000 deaths per year. Chronic infections can arise in immunocompromised individuals, and pregnant women may suffer from fulminant disease as a consequence of HEV infection. Despite these important implications for public health, no specific antiviral treatment has been approved to date. Here, we report combined functional, biochemical, and X-ray crystallographic studies that characterize the human antibody response in convalescent HEV patients. We identified a class of potent and broadly neutralizing human antibodies (bnAbs), targeting a quaternary epitope located at the tip of the HEV capsid protein pORF2 that contains an N-glycosylation motif and is conserved across members of the Hepeviridae. These glycan-sensitive bnAbs specifically recognize the non-glycosylated pORF2 present in infectious particles but not the secreted glycosylated form acting as antibody decoy. Our most potent bnAb protects human liver-chimeric mice from intraperitoneal HEV challenge and co-housing exposure. These results provide insights into the bnAb response to this important emerging pathogen and support the development of glycan-sensitive antibodies to combat HEV infection.
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