| Literature DB >> 34469031 |
Xuanjun Wu1,2,3, Jinfeng Ye1, Andrew T DeLaitsch4, Zahra Rashidijahanabad2,3, Shuyao Lang2,3, Tayeb Kakeshpour2, Yuetao Zhao2,3,5, Sherif Ramadan2,3,6, Paulo Vilar Saavedra7, Vilma Yuzbasiyan-Gurkan8, Herbert Kavunja2,9, Hongzhi Cao1, Jeffrey C Gildersleeve4, Xuefei Huang2,3,10.
Abstract
Ganglioside GD2 is an attractive tumor-associated carbohydrate antigen for anti-cancer vaccine development. However, its low immunogenicity and the significant side effects observed with anti-GD2 antibodies present significant obstacles for vaccines. To overcome these, a new GD2 derivative bearing an N-acetamide (NHAc) at its non-reducing end neuraminic acid (9NHAc-GD2) has been designed to mimic the 9-O-acetylated-GD2 (9OAc-GD2), a GD2 based antigen with a restricted expression on tumor cells. 9NHAc-GD2 was synthesized efficiently via a chemoenzymatic method and subsequently conjugated with a powerful carrier bacteriophage Qβ. Mouse immunization with the Qβ-9NHAc-GD2 conjugate elicited strong and long-lasting IgG antibodies, which were highly selective toward 9NHAc-GD2 with little cross-recognition of GD2. Immunization of canines with Qβ-9NHAc-GD2 showed the construct was immunogenic in canines with little adverse effects, paving the way for future clinical translation to humans.Entities:
Keywords: 9NHAc-GD2; cancer; glycoconjugates; synthesis design; vaccine
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Year: 2021 PMID: 34469031 PMCID: PMC8545922 DOI: 10.1002/anie.202108610
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 15.336