表位
低过敏性
生物
T细胞
原肌球蛋白
分子生物学
B细胞
过敏原
抗体
化学
生物化学
免疫学
免疫系统
过敏
肌球蛋白
作者
Fei Huan,Shuai Gao,Lingna Ni,Mingxuan Wu,Yi Gu,Xiao Yun,Meng Liu,Dong Lai,Anfeng Xiao,Guang‐Ming Liu
标识
DOI:10.1021/acs.jafc.4c04475
摘要
Tropomyosin was reported as an important allergen in Crassostrea angulata and designated as Cra a 1. The localization of the T cell epitopes and the reduction of the immunoreactivity of Cra a 1 are still lacking. In this study, four T cell epitopes were identified by using wild-type Cra a 1 (wtCra a 1)-immunized mouse splenocytes cultured with synthetic peptides. The immunoreactivity was maintained after chemical denaturation treatment, indicating that the linear epitope is an immunodominant epitope of wtCra a 1. Furthermore, the hypoallergenic derivative (mCra a 1) was developed by the deletion of linear B cell epitopes and retention of T cell epitopes. mCra a 1 could stimulate CD4+T cell proliferation and upregulate interleukin-10 secretion. Overall, basophil activation by mCra a 1 was low, but its ability to induce T cell proliferation was retained, suggesting that mCra a 1 may serve as a viable candidate for treating oyster allergy.
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