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Human parainfluenza virus type 2 vector induces dendritic cell maturation without viral RNA replication/transcription

机译:人副流感病毒2型载体诱导树突状细胞成熟,而无病毒RNA复制/转录

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The dendritic cell (DC), a most potent antigen-presenting cell, plays a key role in vaccine therapy against infectious diseases and malignant tumors. Although advantages of viral vectors for vaccine therapy have been reported, potential risks for adverse effects prevent them from being licensed for clinical use. Human parainfluenza virus type 2 (hPIV2), one of the members of the Paramyxoviridae family, is a nonsegmented and negative-stranded RNA virus. We have developed a reverse genetics system for the production of infectious hPIV2 lacking the F gene (hPIV2ΔF), wherein various advantages for vaccine therapy exist, such as cytoplasmic replication/transcription, nontransmissible infectivity, and extremely high transduction efficacy in various types of target cells. Here we demonstrate that hPIV2ΔF shows high transduction efficiency in human DCs, while not so high in mouse DCs. In addition, hPIV2ΔF sufficiently induces maturation of both human and murine DCs, and the maturation state of both human and murine DCs is almost equivalent to that induced by lipopolysaccharide. Moreover, alkylating agent β-propiolactone- inactivated hPIV2ΔF (BPL-hPIV2ΔF) elicits DC maturation without viral replication/transcription. These results suggest that hPIV2ΔF may be a useful tool for vaccine therapy as a novel type of paramyxoviral vector, which is single-round infectious vector and has potential adjuvant activity.
机译:树突状细胞(DC)是最有效的抗原呈递细胞,在针对传染病和恶性肿瘤的疫苗治疗中起着关键作用。尽管已经报道了病毒载体在疫苗治疗中的优势,但潜在的不良反应风险使它们无法获得临床使用许可。人副流感病毒2型(hPIV2)是副粘病毒科的成员之一,是一种无节段的负链RNA病毒。我们已经开发了一种逆向遗传学系统,用于生产缺乏F基因的hPIV2传染性病毒(hPIV2ΔF),其中存在多种疫苗治疗优势,例如细胞质复制/转录,不可传播的传染性以及在各种类型靶细胞中的极高转导效率。在这里,我们证明了hPIV2ΔF在人DC中显示出高转导效率,而在小鼠DC中则没有那么高。另外,hPIV2ΔF足以诱导人和鼠DC的成熟,并且人和鼠DC的成熟状态几乎与脂多糖诱导的成熟状态相同。而且,烷基化剂β-丙内酯失活的hPIV2ΔF(BPL-hPIV2ΔF)引发DC成熟,而没有病毒复制/转录。这些结果表明,hPIV2ΔF作为一种新型的副粘病毒载体可能是用于疫苗治疗的有用工具,其是单轮传染性载体并且具有潜在的佐剂活性。

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