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一种基因工程治疗性凝集素可抑制甲型人流感病毒感染,并维持强大的病毒特异性CD8 T细胞扩增。

A genetically engineered therapeutic lectin inhibits human influenza A virus infection and sustains robust virus-specific CD8 T cell expansion.

作者信息

Yu Meng, Lin Ang, Baharom Faezzah, Li Shuijie, Legendre Maureen, Covés-Datson Evelyn, Sohlberg Ebba, Schlisio Susanne, Loré Karin, Markovitz David M, Smed-Sörensen Anna

出版信息

bioRxiv. 2024 Aug 17:2024.08.15.608041. doi: 10.1101/2024.08.15.608041.

Abstract

Native banana lectin (BanLec) is antiviral but highly mitogenic, which limits its therapeutic value. In contrast, the genetically engineered H84T BanLec (H84T) is not mitogenic but remains effective against influenza A virus (IAV) infection in mouse models. However, the potency and effect of H84T on human immune cells and IAV-specific immune responses is undetermined. We found that H84T efficiently inhibited IAV replication in human dendritic cells (DCs) from blood and tonsils, which preserved DC viability and allowed acquisition and presentation of viral antigen. Consequently, H84T-treated DCs initiated effective expansion of IAV-specific CD8 T cells. Furthermore, H84T preserved the capacity of IAV-exposed DCs to present a second non-IAV antigen and induce robust CD8 T cell expansion. This supports H84T as a potent antiviral in humans as it effectively inhibits IAV infection without disrupting DC function, and preserves induction of antigen-specific adaptive immune responses against diverse antigens, which likely is clinically beneficial.

摘要

天然香蕉凝集素(BanLec)具有抗病毒作用,但有很强的促有丝分裂活性,这限制了其治疗价值。相比之下,基因工程改造的H84T BanLec(H84T)没有促有丝分裂活性,但在小鼠模型中对甲型流感病毒(IAV)感染仍有疗效。然而,H84T对人类免疫细胞和IAV特异性免疫反应的效力和效果尚未确定。我们发现,H84T能有效抑制来自血液和扁桃体的人类树突状细胞(DC)中的IAV复制,这维持了DC的活力,并允许其获取和呈递病毒抗原。因此,经H84T处理的DC引发了IAV特异性CD8 T细胞的有效扩增。此外,H84T保留了暴露于IAV的DC呈递第二种非IAV抗原并诱导强大的CD8 T细胞扩增的能力。这支持H84T作为一种对人类有效的抗病毒药物,因为它能有效抑制IAV感染而不破坏DC功能,并保留针对多种抗原的抗原特异性适应性免疫反应的诱导能力,这可能具有临床益处。

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