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Challenges in Antibody Development against Tn and Sialyl-Tn Antigens

机译:针对Tn和Sialyl-Tn抗原的抗体开发面临的挑战

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摘要

The carbohydrate antigens Tn and sialyl-Tn (STn) are expressed in most carcinomas and usually absent in healthy tissues. These antigens have been correlated with cancer progression and poor prognosis, and associated with immunosuppressive microenvironment. Presently they are used in clinical trials as therapeutic vaccination, but with limited success due to their low immunogenicity. Alternatively, anti-Tn and/or STn antibodies may be used to harness the immune system against tumor cells. Whilst the development of antibodies against these antigens had a boost two decades ago for diagnostic use, so far no such antibody entered into clinical trials. Possible limitations are the low specificity and efficiency of existing antibodies and that novel antibodies are still necessary. The vast array of methodologies available today will allow rapid antibody development and novel formats. Following the advent of hybridoma technology, the immortalization of human B cells became a methodology to obtain human monoclonal antibodies with better specificity. Advances in molecular biology including phage display technology for high throughput screening, transgenic mice and more recently molecularly engineered antibodies enhanced the field of antibody production. The development of novel antibodies against Tn and STn taking advantage of innovative technologies and engineering techniques may result in innovative therapeutic antibodies for cancer treatment.
机译:碳水化合物抗原Tn和唾液酸基Tn(STn)在大多数癌症中表达,而在健康组织中通常不存在。这些抗原与癌症进展和不良预后相关,并与免疫抑制性微环境有关。目前,它们在临床试验中被用作治疗性疫苗,但由于其免疫原性低而获得的成功有限。或者,可以使用抗Tn和/或STn抗体来利用针对肿瘤细胞的免疫系统。尽管针对这些抗原的抗体的开发已在20年前用于诊断用途,但目前尚无此类抗体进入临床试验。可能的限制是现有抗体的特异性和效率低,并且仍然需要新型抗体。当今可用的各种方法将允许快速的抗体开发和新颖的形式。随着杂交瘤技术的出现,人类B细胞的永生化成为获得具有更好特异性的人类单克隆抗体的方法。分子生物学方面的进展包括用于高通量筛选的噬菌体展示技术,转基因小鼠以及最近进行分子工程改造的抗体,这些都增强了抗体生产领域。利用创新技术和工程技术开发针对Tn和STn的新型抗体可能会产生用于癌症治疗的创新性治疗性抗体。

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