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Mannosylated poly(beta-amino esters) for targeted antigen presenting cell immune modulation

机译:甘露糖基化的聚(β-氨基酯)用于靶向抗原呈递细胞的免疫调节

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摘要

Given the rise of antibiotic resistance and other difficult-to-treat diseases, genetic vaccination is a promising preventative approach that can be tailored and scaled according to the vector chosen for gene delivery. However, most vectors currently utilized rely on ubiquitous delivery mechanisms that ineffectively target important immune effectors such as antigen presenting cells (APCs). As such, APC targeting allows the option for tuning the direction (humoral vs cell-mediated) and strength of the resulting immune responses. In this work, we present the development and assessment of a library of mannosylated poly(beta-amino esters) (PBAEs) that represent a new class of easily synthesized APC-targeting cationic polymers. Polymeric characterization and assessment methodologies were designed to provide a more realistic physiochemical profile prior to in vivo evaluation. Gene delivery assessment in vitro showed significant improvement upon PBAE mannosylation and suggested that mannose-mediated uptake and processing influence the magnitude of gene delivery. Furthermore, mannosylated PBAEs demonstrated a strong, efficient, and safe in vivo humoral immune response without use of adjuvants when compared to genetic and protein control antigens. In summary, the gene delivery effectiveness provided by mannosylated PBAE vectors offers specificity and potency in directing APC activation and subsequent immune responses.
机译:鉴于抗生素耐药性和其他难以治疗的疾病的增加,基因疫苗是一种有前途的预防方法,可以根据选择用于基因传递的载体进行定制和调整规模。然而,当前使用的大多数载体依赖于普遍存在的递送机制,该机制无效地靶向重要的免疫效应物,例如抗原呈递细胞(APC)。这样,APC靶向可以选择调节所产生的免疫反应的方向(体液还是细胞介导的)和强度。在这项工作中,我们介绍了甘露糖基化的聚(β-氨基酯)(PBAEs)库的开发和评估,该库代表了一类易于合成的靶向APC的阳离子聚合物的新类别。聚合物表征和评估方法旨在在体内评估之前提供更现实的理化特性。体外基因传递评估显示,PBAE甘露糖基化显着改善,并表明甘露糖介导的摄取和加工影响基因传递的程度。此外,与遗传和蛋白质控制抗原相比,甘露糖基化的PBAE在不使用佐剂的情况下表现出强大,有效和安全的体内体液免疫反应。总之,由甘露糖基化的PBAE载体提供的基因递送效力在指导APC活化和随后的免疫应答中提供了特异性和效力。

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