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Merck

Nonimmunogenetic Viral Capsid Carrier with Cancer Targeting Activity.

Advanced science (Weinheim, Baden-Wurttemberg, Germany) (2018-08-22)
Bo-Ram Lee, Eunji Jo, Hong Yeol Yoon, Chul Joo Yoon, Hyo-Jung Lee, Koo Chul Kwon, Tae Woo Kim, Jeewon Lee
RÉSUMÉ

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.

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Sigma-Aldrich
Anticorps IgG de chèvre anti-souris, fragment Fc conjugué à la HRP, 0.8 mg/mL, Chemicon®