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Cholic Acid-based Delivery System for Vaccine Candidates against Group A Streptococcus

机译:基于胆酸的甲酸递送系统,用于疫苗候选者对群体的疫苗

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摘要

Peptide-based subunit vaccines require an immunostimulant (adjuvant) and/or delivery system to protect the antigenic peptide from degradation and induce the desired immunity. Currently available adjuvants are either too toxic for human use (experimental adjuvants) or they are limited for use in particular vaccines or licensed countries (commercial adjuvants). Therefore, there is an immediate need for novel adjuvants that are both safe and effective. Herein, we assessed the ability of cholic acid (a major bile acid) as a nontoxic, biodegradable, human-derived, potent vaccine delivery system. An antigenic peptide derived from Group A Streptococcus was conjugated to hydrophobic cholic acid via solid phase peptide synthesis to produce lipopeptide that self-assembled into rod-like nanoparticles under aqueous conditions. Following intranasal immunization in mice, this lipopeptide was capable of inducing the production of opsonic epitope-specific antibodies on its own and in liposomal formulation. The cholic acid-based conjugate induced significantly stronger humoral immune responses than cholera toxin based adjuvant. Thus, we demonstrated, for the first time, capability of the human-derived lipid to act as a built-in immunoadjuvant for vaccines.
机译:基于肽的亚基疫苗需要免疫刺激剂(佐剂)和/或递送系统,以保护抗原肽免于降解并诱导所需的免疫。目前可用的佐剂对于人类使用过于毒性(实验佐剂),或者它们仅限于特定疫苗或许可国家(商业佐剂)。因此,立即需要一种安全有效的新型佐剂。在此,我们评估了胆酸(主要胆汁酸)作为无毒,可生物降解的,人源性有效疫苗递送系统的能力。衍生自链球菌的抗原肽通过固相肽合成缀合与疏水性胆酸,以产生脂肽,其在水性条件下自组装成棒状纳米颗粒。在小鼠中鼻内免疫之后,这种脂肽能够在其自身和脂质体制物上诱导Opsonic表位特异性抗体。基于胆汁酸的浓度诱导胆酸基缀合物比基于霍乱毒素的佐剂显着强烈的体液免疫应答。因此,我们首次证明了人衍生的脂质的能力,以作为疫苗的内置免疫造成者。

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