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首页> 外文期刊>Infection and immunity >Listeria monocytogenes-Based Antibiotic Resistance Gene-Free Antigen Delivery System Applicable to Other Bacterial Vectors and DNA Vaccines
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Listeria monocytogenes-Based Antibiotic Resistance Gene-Free Antigen Delivery System Applicable to Other Bacterial Vectors and DNA Vaccines

机译:基于单核细胞增生李斯特菌的抗生素抗性无基因抗原递送系统,适用于其他细菌载体和DNA疫苗

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Plasmids represent a powerful tool to rapidly introduce genes into bacteria and help them reach high expression levels. In vaccine development, with live vaccine vectors, this allows greater flexibility and the ability to induce larger antigen amounts through multiple gene copies. However, plasmid retention often requires antibiotic resistance markers, the presence of which has been discouraged in clinical applications by the Food and Drug Administration. Therefore, we developed a Listeria monocytogenes-Escherichia coli shuttle plasmid that is retained by complementation of d-alanine racemase-deficient mutant strains both in vitro and in vivo. Our technology potentially allows the production of antibiotic resistance marker-free DNA vaccines as well as bacterial vaccine vectors devoid of engineered antibiotic resistances. As a proof of concept, we applied the d-alanine racemase complementation system to our Listeria cancer vaccine platform. With a transplantable tumor model, we compared the efficacy of the new Listeria vector to that of an established vector containing a conventional plasmid carrying a tumor-specific antigen. Both vaccine vector systems resulted in long-term regression of established tumors, with no significant difference between them. Thus, the Listeria vaccine vector presented here potentially complies with Food and Drug Administration regulations and could be developed further for clinical use.
机译:质粒是将基因快速引入细菌并帮助它们达到高表达水平的有力工具。在疫苗开发中,使用活疫苗载体,可以提供更大的灵活性,并具有通过多个基因拷贝诱导更大抗原量的能力。然而,质粒保留通常需要抗生素抗性标记,美国食品药品管理局在临床应用中不建议使用抗生素抗性标记。因此,我们开发了一种单核细胞增生李斯特菌-大肠杆菌穿梭质粒,该质粒在体内和体外都被d-丙氨酸消旋酶缺陷型突变体互补。我们的技术潜在地允许生产无抗生素抗性标记的DNA疫苗以及不含工程化抗生素抗性的细菌疫苗载体。作为概念的证明,我们将d-丙氨酸消旋酶互补系统应用于我们的 Listeria 癌症疫苗平台。在可移植的肿瘤模型中,我们将新的 Listeria 载体与已建立的包含带有肿瘤特异性抗原的常规质粒的载体的功效进行了比较。两种疫苗载体系统均可导致已建立肿瘤的长期消退,两者之间无显着差异。因此,此处介绍的李斯特菌疫苗载体可能符合食品药品监督管理局的规定,并可以进一步开发用于临床。

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