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针对人类B细胞淋巴瘤的独特型疫苗接种。从活检材料中获取可变区基因序列以组装成单链Fv个人疫苗。

Idiotypic vaccination against human B-cell lymphoma. Rescue of variable region gene sequences from biopsy material for assembly as single-chain Fv personal vaccines.

作者信息

Hawkins R E, Zhu D, Ovecka M, Winter G, Hamblin T J, Long A, Stevenson F K

机构信息

Medical Research Council Laboratory of Molecular Biology, Cambridge, UK.

出版信息

Blood. 1994 Jun 1;83(11):3279-88.

PMID:8193363
Abstract

Idiotypic determinants on neoplastic B cells could provide tumor antigens for vaccination of patients with B-cell tumors. Because this approach requires an individual vaccine for each patient, simple methods for obtaining idiotypic antigen are desirable. Using polymerase chain reaction (PCR) with family-based V-gene and J-region primers, the variable region genes of heavy and light chains (VH and VL) of Ig have been obtained from biopsy material from 13 patients with B-cell tumors. In each case, analysis of random clones derived from the PCR product showed repeated, clonally-related sequences, whereas normal lymphoid tissue generated no repeated sequences. In 3/3 cases, the repeated sequences were found to be the same as those in a tumor-derived hybridoma. Mutational patterns in the V-genes differed among the tumors, with follicular lymphoma tending to be more highly mutated. The individual VH and VL sequences have been assembled with a flexible linker sequence to encode single-chain Fv (scFv). The scFv sequences can be cloned into bacterial expression vectors to produce protein, or into vectors suitable for direct vaccination using naked DNA. In a model system, expressed scFv protein retained all idiotypic determinants defined by a panel of five anti-idiotypic monoclonal antibodies (MoAbs). Similarly, expressed scFv proteins from two patients were shown to react with anti-idiotypic antibodies. This approach allows production of potential vaccines from surgical biopsies within 2 to 3 weeks.

摘要

肿瘤性B细胞上的独特型决定簇可为B细胞肿瘤患者的疫苗接种提供肿瘤抗原。由于这种方法需要为每位患者制备个性化疫苗,因此需要简单的方法来获取独特型抗原。使用基于家族的V基因和J区引物进行聚合酶链反应(PCR),已从13例B细胞肿瘤患者的活检材料中获得了Ig重链和轻链(VH和VL)的可变区基因。在每种情况下,对PCR产物衍生的随机克隆进行分析,均显示出重复的、克隆相关的序列,而正常淋巴组织未产生重复序列。在3/3的病例中,发现重复序列与肿瘤来源的杂交瘤中的序列相同。不同肿瘤的V基因中的突变模式有所不同,滤泡性淋巴瘤的突变往往更为频繁。单个VH和VL序列已与柔性接头序列组装在一起,以编码单链Fv(scFv)。scFv序列可克隆到细菌表达载体中以产生蛋白质,或克隆到适合使用裸DNA直接接种疫苗的载体中。在一个模型系统中,表达的scFv蛋白保留了由一组五种抗独特型单克隆抗体(MoAb)定义的所有独特型决定簇。同样,来自两名患者的表达的scFv蛋白也显示出与抗独特型抗体发生反应。这种方法可在2至3周内从手术活检中制备出潜在的疫苗。

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