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研究影响 hCG 作为潜在癌症疫苗免疫原性的因素。

Investigation of factors influencing the immunogenicity of hCG as a potential cancer vaccine.

机构信息

Division of Infection and Immunity, University College London, London, UK.

Division of Immunology and Microbiology, Javakhishvili Tbilisi State University, Tbilisi, Georgia, USA.

出版信息

Clin Exp Immunol. 2018 Jul;193(1):73-83. doi: 10.1111/cei.13131. Epub 2018 May 7.

Abstract

Human chorionic gonadotrophin (hCG) and its β-subunit (hCGβ) are tumour autocrine growth factors whose presence in the serum of cancer patients has been linked to poorer prognosis. Previous studies have shown that vaccines which target these molecules and/or the 37 amino acid C-terminal hCGβ peptide (hCGβCTP) induce antibody responses in a majority of human recipients. Here we explored whether the immunogenicity of vaccines containing an hCGβ mutant (hCGβR68E, designed to eliminate cross-reactivity with luteinizing hormone) or hCGβCTP could be enhanced by coupling the immunogen to different carriers [keyhole limpet haemocyanin (KLH) or heat shock protein 70 (Hsp70)] using different cross-linkers [1-ethyl-3(3-dimethylaminopropyl)carboiimide (EDC) or glutaraldehyde (GAD)] and formulated with different adjuvants (RIBI or Montanide ISA720). While there was little to choose between KLH and Hsp70 as carriers, their influence on the effectiveness of a vaccine containing the BAChCGβR68E mutant was less marked, presumably because, being a foreign species, this mutant protein itself might provide T helper epitopes. The mutant provided a significantly better vaccine than the hCGβCTP peptide irrespective of the carrier used, how it was cross-linked to the carrier or which adjuvant was used when hCG was the target. Nonetheless, for use in humans where hCG is a tolerated self-protein, the need for a carrier is of fundamental importance. Highest antibody titres were obtained by linking the BAChCGβR68E to Hsp70 as a carrier by GAD and using RIBI as the adjuvant, which also resulted in antibodies with significantly higher affinity than those elicited by hCGβCTP peptide vaccine. This makes this mutant vaccine a promising candidate for therapeutic studies in hCGβ-positive cancer patients.

摘要

人绒毛膜促性腺激素(hCG)及其β亚基(hCGβ)是肿瘤自分泌生长因子,其在癌症患者血清中的存在与预后较差有关。先前的研究表明,针对这些分子和/或 37 个氨基酸的 C 末端 hCGβ 肽(hCGβCTP)的疫苗在大多数人类受者中引起抗体反应。在这里,我们探讨了含有 hCGβ 突变体(hCGβR68E,旨在消除与促黄体生成素的交叉反应性)或 hCGβCTP 的疫苗的免疫原性是否可以通过使用不同的交联剂[1-乙基-3(3-二甲基氨基丙基)碳二亚胺(EDC)或戊二醛(GAD)]将免疫原与不同载体[血蓝蛋白(KLH)或热休克蛋白 70(Hsp70)]连接,并使用不同的佐剂(RIBI 或 Montanide ISA720)进行配制来增强。虽然 KLH 和 Hsp70 作为载体之间几乎没有选择,但它们对含有 BAChCGβR68E 突变体的疫苗的有效性的影响并不明显,大概是因为作为一种外来物种,这种突变蛋白本身可能提供 T 辅助表位。无论使用哪种载体、如何与载体交联或使用哪种佐剂(当 hCG 为靶标时),突变体都提供了一种明显优于 hCGβCTP 肽疫苗的疫苗。然而,在使用 hCG 作为可耐受的自身蛋白的人类中,载体的需求至关重要。通过 GAD 将 BAChCGβR68E 与 Hsp70 作为载体连接,并使用 RIBI 作为佐剂,获得了最高的抗体滴度,这也导致抗体的亲和力明显高于 hCGβCTP 肽疫苗引起的抗体。这使得这种突变疫苗成为 hCGβ 阳性癌症患者治疗研究的有希望的候选者。

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