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Nonimmunogenetic Viral Capsid Carrier with Cancer Targeting Activity

机译:具有癌症靶向活性的非免疫原性病毒衣壳载体

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摘要

Although protein nanoparticles (PNPs) (e.g., viral capsids) capable of delivering a broad range of drug agents have shown distinctive advantages over synthetic nanomaterials, PNPs have an intrinsic drawback that hampers their clinical application, that is, potential immunogenicity. Here, a novel method for resolving the immunogenicity problem of PNPs, which is based on the genetic presentation of albumin‐binding peptides (ABPs) on the surface of PNP, is reported. ABPs are inserted into the surface of a viral capsid (hepatitis B virus capsid/HBVC) while preserving the native self‐assembly function of HBVC. The ABPs effectively gather human serum albumins around HBVC and significantly reduce both inflammatory response and immunoglobulin titer in live mice compared to ABP‐free HBVC. Furthermore, ABP‐conjugated HBVCs remain within tumors for a longer period than HBVCs conjugated to tumor cell receptor‐bindingpeptides, indicating that the ABPs are also capable of enhancing tumor‐targeting performance. Although applied to HBVC for proof of concept, this novel approach may provide a general platform for resolving immunogenicity and cancer‐targeting problems of PNPs, which enables the development of a variety of PNP‐based drug delivery carriers with high safety and efficacy.
机译:尽管能够递送多种药物的蛋白质纳米颗粒(PNP)(例如病毒衣壳)已显示出优于合成纳米材料的独特优势,但PNP具有固有的缺陷,妨碍了其临床应用,即潜在的免疫原性。在此,已报道了一种解决PNP免疫原性问题的新方法,该方法基于PNP表面的白蛋白结合肽(ABP)的遗传表现。将ABP插入病毒衣壳(乙型肝炎病毒衣壳/ HBVC)的表面,同时保留HBVC的天然自组装功能。与不含ABP的HBVC相比,ABP可有效收集HBVC周围的人血清白蛋白,并显着降低活小鼠的炎症反应和免疫球蛋白滴度。此外,与结合了肿瘤细胞受体结合肽的HBVC相比,结合了ABP的HBVC在肿瘤中的保留时间更长,这表明ABP也能够增强靶向肿瘤的性能。尽管已应用于HBVC进行概念验证,但这种新颖的方法可能为解决PNP的免疫原性和癌症靶向问题提供了一个通用平台,从而使开发具有高安全性和有效性的多种基于PNP的药物递送载体成为可能。

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