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采用佐剂系统方法研发的 AS04 佐剂 HPV 疫苗。

Development of an AS04-adjuvanted HPV vaccine with the adjuvant system approach.

机构信息

GlaxoSmithKline Biologicals, Wavre, Belgium.

出版信息

BioDrugs. 2011 Aug 1;25(4):217-26. doi: 10.2165/11591760-000000000-00000.

Abstract

A novel human papillomavirus (HPV) vaccine has been formulated with virus-like particles of the L1 protein of HPV-16 and HPV-18, and the Adjuvant System 04 (AS04). AS04 is a combination of the toll-like receptor 4 agonist monophosphoryl lipid A (MPL) and aluminum hydroxide. The AS04-adjuvanted HPV vaccine induces a high and sustained immune response against HPV, including high levels of neutralizing antibodies at the cervical mucosa in women aged 15-55 years. Recently, the mechanism of action of AS04 has been evaluated in vitro in human cells and in vivo in mice and the data provide evidence for the molecular and cellular basis of the observed immunogenicity, efficacy, and safety profile of this formulation. In this review, we discuss how the results of GlaxoSmithKline's clinical studies on immunogenicity, protection, and reactogenicity with the AS04-adjuvanted HPV vaccine are supported by the observed mechanism of action for the adjuvant. The adjuvant activity of AS04, as measured by enhanced antibody response to HPV antigens, was found to be strictly dependent on AS04 and the HPV antigens being injected at the same intramuscular site within 24 hours of each other. The addition of MPL to aluminum salt enhances humoral and cell-mediated response by rapidly triggering a local and transient cytokine response that leads to an increased activation of antigen-presenting cells and results in an improved presentation of antigen to CD4+ T cells. The added value of MPL in AS04 for an HPV vaccine was demonstrated in clinical studies by high vaccine-elicited antibody responses and the induction of high levels of memory B cells. The vaccine elicits cross protection against some other oncogenic HPV types (specifically HPV-31, -33, and -45) not contained in the vaccine. The localized and transient nature of the innate immune response supports the acceptable safety profile observed in clinical studies.

摘要

一种新型人乳头瘤病毒(HPV)疫苗采用 HPV-16 和 HPV-18 的 L1 蛋白病毒样颗粒和佐剂系统 04(AS04)配制而成。AS04 是 Toll 样受体 4 激动剂单磷酰脂质 A(MPL)和氢氧化铝的组合。AS04 佐剂 HPV 疫苗可诱导针对 HPV 的高且持续的免疫应答,包括在 15-55 岁女性的宫颈黏膜中产生高水平的中和抗体。最近,AS04 的作用机制在体外的人类细胞和体内的小鼠中进行了评估,数据为观察到的这种制剂的免疫原性、功效和安全性提供了证据。在这篇综述中,我们讨论了葛兰素史克公司关于 AS04 佐剂 HPV 疫苗的免疫原性、保护作用和不良反应的临床研究结果如何得到佐剂的观察到的作用机制的支持。AS04 的佐剂活性,如通过增强对 HPV 抗原的抗体反应来衡量,发现严格依赖于 AS04 和 HPV 抗原在彼此 24 小时内同一肌肉内注射。在铝盐中添加 MPL 通过迅速触发局部和短暂的细胞因子反应来增强体液和细胞介导的反应,从而导致抗原呈递细胞的激活增加,并导致抗原向 CD4+T 细胞的呈递改善。在 HPV 疫苗中添加 MPL 在临床试验中表现为疫苗引起的抗体反应高和记忆 B 细胞诱导水平高。该疫苗可针对疫苗中未包含的一些其他致癌 HPV 类型(特别是 HPV-31、-33 和 -45)产生交叉保护作用。先天免疫反应的局部和短暂性质支持在临床研究中观察到的可接受的安全性。

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