卵巢癌细胞膜上α-半乳糖表位的表达用作新型自体肿瘤疫苗。

Expression of alpha-gal epitopes on ovarian carcinoma membranes to be used as a novel autologous tumor vaccine.

作者信息

Galili Uri, Chen Zhao-chun, DeGeest Koen

机构信息

Department of Cardiovascular Thoracic Surgery, Rush University, Chicago, IL 60612, USA.

出版信息

Gynecol Oncol. 2003 Jul;90(1):100-8. doi: 10.1016/s0090-8258(03)00148-3.

DOI:10.1016/s0090-8258(03)00148-3

PMID:12821349

Abstract

OBJECTIVE

Poor presentation of tumor-associated antigens (TAA) to the immune system remains a major obstacle to effective anti-tumor vaccine therapy. The aim of this study is to demonstrate the feasibility of producing a novel autologous tumor vaccine from ovarian carcinoma that is expected to have increased immunogenicity. The strategy is based on the ability of the anti-Gal IgG antibody (a natural antibody comprising 1% of IgG in humans) to target tumor membranes expressing alpha-gal epitopes (Galalpha1-3Galbeta1-4GlcNAc-R) to antigen-presenting cells (APC).

STUDY DESIGN

Freshly obtained ovarian carcinoma tumors are homogenized, washed, and incubated with a mixture of neuraminidase, recombinant alpha1,3 galactosyltransferase (ralpha1,3GT) and uridine diphosphate galactose (UDP-Gal) to synthesize alpha-gal epitopes on carbohydrate chains of glycoproteins of these membranes. Subsequently, the processed membranes are analyzed for expression of alpha-gal epitopes and for the binding of anti-Gal.

RESULTS

Incubation of 3 g of ovarian carcinoma membranes, from five different patients, at 100 mg/ml, mixed together with ralpha1,3GT (50 microg/ml), neuraminidase (1 mU/ml), and UDP-Gal (2 mM), resulted in the effective synthesis of alpha-gal epitopes to the extent of approximately 2 x 10(11) epitopes/mg of tumor membranes. As a result of this de novo expression of alpha-gal epitopes, the tumor membranes readily bound purified anti-Gal antibody, as well as anti-Gal in autologous serum.

CONCLUSIONS

The method described in this study is very effective in the synthesis of many alpha-gal epitopes on tumor membranes obtained from ovarian carcinoma. These novel epitopes readily bind the naturally occurring anti-Gal antibody. This technique of opsonization of alpha-gal-modified autologous tumor membranes carrying TAA is expected to increase effective uptake of the vaccine by APC, which is key to successful anti-tumor vaccination.

摘要

目的

肿瘤相关抗原（TAA）向免疫系统的呈递不佳仍然是有效的抗肿瘤疫苗治疗的主要障碍。本研究的目的是证明从卵巢癌生产一种新型自体肿瘤疫苗的可行性，该疫苗预计具有增强的免疫原性。该策略基于抗Gal IgG抗体（一种占人类IgG 1%的天然抗体）将表达α-半乳糖表位（Galα1-3Galβ1-4GlcNAc-R）的肿瘤膜靶向抗原呈递细胞（APC）的能力。

研究设计

将新鲜获取的卵巢癌肿瘤匀浆、洗涤，并与神经氨酸酶、重组α1,3半乳糖基转移酶（ralpha1,3GT）和尿苷二磷酸半乳糖（UDP-Gal）的混合物孵育，以在这些膜糖蛋白的碳水化合物链上合成α-半乳糖表位。随后，分析处理后的膜上α-半乳糖表位的表达以及抗Gal的结合情况。

结果

将来自五名不同患者的3 g卵巢癌膜以100 mg/ml的浓度混合，与ralpha1,3GT（50 μg/ml）、神经氨酸酶（1 mU/ml）和UDP-Gal（2 mM）一起孵育，导致α-半乳糖表位的有效合成，达到约2×10¹¹个表位/mg肿瘤膜的程度。由于α-半乳糖表位的这种从头表达，肿瘤膜易于结合纯化的抗Gal抗体以及自体血清中的抗Gal。