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用GM2神经节苷脂共轭疫苗免疫的黑色素瘤患者的血清学反应模式。

Serological response patterns of melanoma patients immunized with a GM2 ganglioside conjugate vaccine.

作者信息

Kitamura K, Livingston P O, Fortunato S R, Stockert E, Helling F, Ritter G, Oettgen H F, Old L J

机构信息

Ludwig Institute for Cancer Research, New York Unit, NY, USA.

出版信息

Proc Natl Acad Sci U S A. 1995 Mar 28;92(7):2805-9. doi: 10.1073/pnas.92.7.2805.

Abstract

Gangliosides, such as GM2, GD2, GD3, and 9-O-acetyl GD3, are receiving attention as targets for antibody-based and vaccine-based therapies of melanoma. GM2 appears to be a particularly immunogenic ganglioside in humans, as indicated by the presence of naturally occurring IgM anti-GM2 antibodies in approximately 5% of humans and the fact that immunization with irradiated GM2-expressing melanoma cells or purified GM2 adherent to bacillus Calmette-Guérin elicits GM2 antibodies of low to moderate titers in a high proportion of vaccinated patients. To develop vaccines that consistently induce high titers of IgM as well as IgG anti-GM2 antibodies, vaccines containing GM2 conjugated to keyhole limpet hemocyanin as the carrier protein and QS-21 as the adjuvant have been constructed. The serological response of vaccinated patients was monitored by ELISA using purified GM2 ganglioside for IgM and IgG anti-GM2 antibodies and for GM2 cell surface-reactive antibodies by immune adherence assays and cytotoxic tests (IgM antibodies) and mixed hemadsorption assays (IgG antibodies). The majority of vaccinated patients developed IgM and IgG antibodies detectable by ELISA. In most cases, the results of IgM ELISA correlated with assays for cell surface-reactive IgM antibodies. This was not true for IgG anti-GM2 antibodies, where strong discrepancies were seen between high titers in ELISA and little or no reactivity in mixed hemadsorption tests for cell surface-reactive antibodies. These IgG antibodies (and the less frequent IgM antibodies that show similar discrepancies) may be directed against GM2 determinants that are buried, hidden, or not present on GM2-expressing target cells. With regard to a major objective of ganglioside vaccines--i.e., generation of cytotoxic antibodies--the GM2-keyhole limpet hemocyanin/QS-21 vaccine is clearly superior to the previously tested GM2/bacillus Calmette-Guérin vaccine. However, variability in patient response and lack of persistence of high-titered IgM cytotoxic antibodies in many patients are problems that remain to be solved.

摘要

神经节苷脂,如GM2、GD2、GD3和9-O-乙酰基GD3,正作为黑色素瘤基于抗体和基于疫苗疗法的靶点而受到关注。GM2在人类中似乎是一种特别具有免疫原性的神经节苷脂,约5%的人类体内存在天然的IgM抗GM2抗体,以及用经辐射的表达GM2的黑色素瘤细胞或附着于卡介苗的纯化GM2进行免疫接种能在高比例的接种患者中引发低至中等滴度的GM2抗体这一事实都表明了这一点。为了开发能持续诱导高滴度IgM以及IgG抗GM2抗体的疫苗,已构建了含有与钥孔血蓝蛋白(作为载体蛋白)偶联的GM2以及QS-21作为佐剂的疫苗。对接种疫苗患者的血清学反应通过ELISA进行监测,使用纯化的GM2神经节苷脂检测IgM和IgG抗GM2抗体,通过免疫黏附试验和细胞毒性试验(检测IgM抗体)以及混合血细胞吸附试验(检测IgG抗体)检测GM2细胞表面反应性抗体。大多数接种疫苗的患者产生了ELISA可检测到的IgM和IgG抗体。在大多数情况下,IgM ELISA的结果与细胞表面反应性IgM抗体的检测结果相关。对于IgG抗GM2抗体情况并非如此,ELISA中的高滴度与细胞表面反应性抗体的混合血细胞吸附试验中几乎没有反应或无反应之间存在强烈差异。这些IgG抗体(以及显示类似差异的较罕见的IgM抗体)可能针对的是GM2决定簇,这些决定簇在表达GM2的靶细胞上是被掩埋、隐藏或不存在的。关于神经节苷脂疫苗的一个主要目标,即产生细胞毒性抗体,GM2-钥孔血蓝蛋白/QS-21疫苗明显优于先前测试的GM2/卡介苗疫苗。然而,患者反应的变异性以及许多患者中高滴度IgM细胞毒性抗体缺乏持久性仍是有待解决的问题。

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