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Mitigation of Anti‐Drug Antibody Production for Augmenting Anticancer Efficacy of Therapeutic Protein via Co‐Injection of Nano‐Rapamycin

Ya ChangSchool of Pharmacy Shanghai Jiao Tong University Shanghai 200240 ChinaWei XiongArtemisinin Research Center Guangzhou University of Chinese Medicine Guangzhou 510450 ChinaChenming ZouSchool of Pharmacy Shanghai Jiao Tong University Shanghai 200240 ChinaPing ZengSchool of Pharmacy Shanghai Jiao Tong University Shanghai 200240 ChinaJiazhen HouSchool of Chinese Materia Medica Nanjing University of Chinese Medicine 138 Xianlin Avenue Nanjing 210023 ChinaBahtiyor MuhitdinovInstitute of Bioorganic Chemistry Uzbekistan Academy of Sciences Tashkent 100125 UzbekistanYuanyuan ShenSchool of Pharmacy Shanghai Jiao Tong University Shanghai 200240 ChinaYongzhuo HuangState Key Laboratory of Drug Research Shanghai Institute of Materia Medica Chinese Academy of Sciences Shanghai 201203 ChinaShengrong GuoSchool of Pharmacy Shanghai Jiao Tong University Shanghai 200240 China
Smalljournal2023en
ABI

Аннотация

The induction of anti-drug antibody (ADA) is a formidable challenge for protein-based therapy. Trichosanthin (TCS) as a class of ribosome-inactivating proteins is widely studied in tumor treatment. However, the immunogenicity can induce the formation of ADA, which can cause hypersensitivity reactions and neutralize the efficacy of TCS, thus limiting its clinical application in cancer therapy. Here, a promising solution to this issue is presented by co-administration of the rapamycin nanoparticles and TCS. PEGylated rapamycin amphiphilic molecule is designed and synthesized as a prodrug and a delivery carrier, which can self-assemble into a nanoparticle system with encapsulation of free rapamycin, a hydrophobic drug. It is found that co-injection of the PEGylated rapamycin nanoparticles and TCS could mitigate the formation of anti-TCS antibody via inducing durable immunological tolerance. Importantly, the combination of TCS and the rapamycin nanoparticles has an enhanced effect on inhibit the growth of breast cancer. This work provides a promising approach for protein toxin-based anticancer therapy and for promoting the clinical translation.

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