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用病毒修饰的肿瘤细胞进行免疫接种。

Immunization with virus-modified tumor cells.

作者信息

Schirrmacher V, Ahlert T, Pröbstle T, Steiner H H, Herold-Mende C, Gerhards R, Hagmüller E, Steiner H H

机构信息

Abteilung Zelluläre Immunologie (G0100), Deutsches Krebsforschungszentrum, Heidelberg, Germany.

出版信息

Semin Oncol. 1998 Dec;25(6):677-96.

PMID:9865682
Abstract

Direct infection of tumor cells with viruses transfering protective or therapeutic genes-a frequently used procedure for production of tumor vaccines in human gene therapy-is often limited by the number of tumor cells that can reliably be infected, as well as by issues of selectivity and safety. In this review, we describe an efficient, selective, and safe way of infecting human tumor cells with a natural virus with interesting pleiotropic immune stimulatory properties, the avian paramyxovirus Newcastle disease virus (NDV). Advantages of this virus are its good cell-binding properties, its selective replication in tumor cell cytoplasm, which is independent of cell proliferation, and its relative safety. Most important for its use as an adjuvant in human cancer vaccine are its ability to introduce T-cell costimulatory activity, to prevent anergy induction, and to induce locally chemokines (eg, RANTES, IP-10) and cytokines (eg, interferon alpha, beta [IFN-alpha, beta] and tumor necrosis factor-alpha [TNFalpha]) that affect T-cell recruitment and activation. A further development consists of attachment-via NDV-derived hemagluttinin-neuraminidase (HN) membrane-anchoring molecules-of universal defined bispecific reagents such as T-cell-activating anti-CD28 antibodies. Finally, we summarize the status of our clinical studies with the autologous virus modified live cell vaccine (ATV)-NDV.

摘要

用携带保护性或治疗性基因的病毒直接感染肿瘤细胞——这是人类基因治疗中生产肿瘤疫苗常用的方法——常常受到可被可靠感染的肿瘤细胞数量的限制,以及选择性和安全性问题的限制。在本综述中,我们描述了一种高效、选择性且安全的方法,用一种具有有趣的多效性免疫刺激特性的天然病毒——禽副粘病毒新城疫病毒(NDV)感染人类肿瘤细胞。这种病毒的优点包括其良好的细胞结合特性、在肿瘤细胞胞质中独立于细胞增殖的选择性复制以及相对安全性。对于其作为人类癌症疫苗佐剂的应用而言,最重要的是它能够引入T细胞共刺激活性、防止无反应性诱导,并诱导影响T细胞募集和激活的局部趋化因子(如RANTES、IP-10)和细胞因子(如干扰素α、β [IFN-α、β] 和肿瘤坏死因子-α [TNFα])。进一步的进展包括通过源自NDV的血凝素-神经氨酸酶(HN)膜锚定分子连接通用的、确定的双特异性试剂,如T细胞激活抗CD28抗体。最后,我们总结了我们使用自体病毒修饰活细胞疫苗(ATV)-NDV进行的临床研究的现状。

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