利用合成碳水化合物抗原对人卵巢癌患者对常见癌(Thomsen-Friedenreich)决定因子的主动免疫。

G D MacLean, M B Bowen-Yacyshyn, J Samuel, A Meikle, G Stuart, J Nation, S Poppema, M Jerry, R Koganty, T Wong
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引用次数: 122

摘要

在一项I期研究中,10名患有广泛转移性疾病的卵巢癌患者接受了3至8次皮下免疫接种,免疫接种是由Thomsen-Friedenreich抗原偶联KLH (TF α -KLH)的免疫显性双糖(β Gal1----3 α GalNAc)合成形式加上DETOX佐剂。6名患者给予“低”剂量的TF α - klh(100微克/注射),4名患者给予“高”剂量(500微克/注射)。所有患者在开始一系列免疫接种前3天接受单次低剂量环磷酰胺治疗(200mg /m2静脉注射)。免疫接种间隔2周。很少或没有发现毒性。正如预期的那样,所有患者(在免疫前)都有天然存在的针对合成TF α半抗原的IgM抗体。没有患者检测到预先存在的针对合成TF α半抗原的IgG或IgA抗体。10例卵巢癌患者中有9例在接种TF α - klh + DETOX佐剂后,IgM滴度明显高于先前水平。这些患者也产生IgG抗tf α,其中8人也产生IgA抗tf α,尽管IgA反应较弱。大多数IgG应答比IgM应答晚2-4周。两名患者在第一次注射TF α - klh后产生了强烈的IgG反应,表明存在回忆反应。对各种固相合成碳水化合物抗原的直接elisa和半抗原抑制实验均证实了该抗体的TF α半抗原特异性。通过ELISA和FACS分析,IgM和IgG抗TF α特异性抗体与天然TF抗原反应,尽管其效价普遍低于免疫TF α半抗原的效价。免疫后10例患者中有8例检测到针对表达tf的肿瘤细胞靶标的细胞毒抗体水平升高。一名患者在免疫前没有检测到细胞毒性抗体,随着免疫次数的增加,细胞毒性抗体越来越强。低抗原剂量患者的体液免疫反应与高抗原剂量患者一样好或更好。所有4名高剂量患者和6名低剂量患者中的4名在接种部位出现了中度至强烈的DTH反应。我们的研究结果表明,KLH是人类碳水化合物半抗原的可接受载体,而DETOX是人类癌症患者产生高滴度特异性抗碳水化合物反应的合适无毒佐剂。(摘要删节为400字)
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Active immunization of human ovarian cancer patients against a common carcinoma (Thomsen-Friedenreich) determinant using a synthetic carbohydrate antigen.

In a phase I study, ten ovarian cancer patients with extensive metastatic disease despite chemotherapy were immunized three to eight times subcutaneously with the synthetic form of the immunodominant disaccharide (beta Gal1----3 alpha GalNAc) of the Thomsen-Friedenreich antigen conjugated to KLH (TF alpha-KLH) plus DETOX adjuvant. Six patients were given a "low" dose of TF alpha-KLH (100 micrograms/injection) and four patients were given a "high" dose (500 micrograms/injection). All patients received a single low-dose cyclophosphamide treatment (200 mg/m2 i.v.) 3 days prior to commencement of the series of immunizations. Immunizations were 2 weeks apart. Little or no toxicity was noted. As expected, all patients (prior to immunization) had naturally occurring IgM antibodies against the synthetic TF alpha hapten. None of the patients had detectable pre-existing IgG or IgA antibodies against synthetic TF alpha hapten. Nine of the ten ovarian cancer patients showed a significant increase in IgM titer above pre-existing levels following immunizations with TF alpha-KLH plus DETOX adjuvant. These same patients also produced IgG anti-TF alpha and eight of these also produced IgA anti-TF alpha, although the IgA responses were weaker. Most of the IgG responses followed the IgM responses by 2-4 weeks. Two patients produced a vigorous IgG response after their first TF alpha-KLH injection, suggesting a recall response. Both direct ELISAs on various solid-phase synthetic carbohydrate antigens and hapten inhibition experiments confirmed the TF alpha hapten specificity of the antibodies. IgM and IgG anti-TF alpha-specific antibodies reacted with natural TF antigen, by ELISA and FACS analysis, although the titers were generally lower than the titers against the immunizing TF alpha hapten. Increased levels of cytotoxic antibodies against TF-expressing tumor cell targets were detected in eight of the ten patients following immunization. One patient who had no detectable cytotoxic antibodies prior to immunization developed increasingly strong cytotoxic antibodies as a function of the number of immunizations. The low antigen dose patients showed as good or better humoral immune responses than the high antigen dose patients. All four high-dose and four of six low-dose patients developed moderate to strong DTH reactions at the vaccination sites. Our results demonstrate that KLH is an acceptable carrier for carbohydrate haptens in humans and that DETOX is an appropriate nontoxic adjuvant for the generation of high-titer specific anti-carbohydrate responses in human cancer patients.(ABSTRACT TRUNCATED AT 400 WORDS)

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