幽门螺杆菌黏附素A抗原H-2d（I-A）限制性免疫优势Th表位的筛选与鉴定  被引量：1

作　　者：杨武晨[1] 郭红[1] 陈立[2] 李滨[2] 李宁一[2] 章金勇[2] 何亚非[1] 胡健[1] 吴超[2] 

机构地区：[1]第三军医大学新桥医院消化内科,重庆400037 [2]第三军医大学医学检验系临床微生物及免疫学教研室,重庆400038

出　　处：《免疫学杂志》2012年第11期976-980,共5页Immunological Journal

基　　金：国家自然科学基金(30771992);重庆市自然科学基金(2011BB5043);"十一五"国家重大新药创制专项(2009ZX09102-220)

摘　　要：目的鉴定幽门螺杆菌(Helicobacter pylori,H.pylori)黏附素A抗原(HpaA)H-2d限制性免疫优势Th表位,为H.pylori表位疫苗的研究提供候选表位。方法采用体外扩增的HpaA抗原特异性T细胞和步移重叠合成肽筛选鉴定HpaA抗原的免疫优势Th表位,再利用抗体阻断实验对其H-2d限制性进行分析。结果 18mer氨基酸肽段筛选发现肽段H154-171、H184-201、H190-207、H202-219和H220-237能够激发HpaA特异性CD4+T细胞产生γ-干扰素。其中H154-171激发的应答最强。13mer氨基酸短肽鉴定结果显示:仅H158-170能刺激产生强于18mer氨基酸短肽H154-171的应答反应。同时,抗体阻断试验结果表明:抗H-2d(I-A)抗体能有效阻断该表位激发的应答。结论 H154-171、H184-201、H190-207、H202-219和H220-237是HpaA的小鼠H-2d限制性Th表位,其中H154-171为免疫优势表位肽,该表位的核心氨基酸序列为H158-170,并存在H-2d(I-A)限制性。该研究将为H.pylori表位疫苗研究提供了可能的候选分子。With the aim of design epitope-based vaccine against Helicobacter pylori（H.pylori）,we identified and characterized H-2d restricted immunodominant Th epitopes from HpaA of H.pylori in this study.Immunodominant Th epitope of HpaA was identified by using in vitro expanded HpaA-specific T cells and overlapping synthetic peptides.And then,the H-2d subtype restriction of the epitope was analyzed by antibody blocking test.Mapping of 18 mer overlapping peptides showed that H154-171,H184-201,H190-207,H202-219 and H220-237 could stimulate HpaA-specific T cells to produce IFN-γ,and the response stimulated by H154-171 was the strongest.Mapping of 13 mer overlapping peptides showed that only H158-170 could stimulate an equivalent HpaA-specific T cell response with H154-171.Antibody blocking test showed that epitope H158-170 was restricted by H-2d（I-A）.H154-171,H184-201,H190-207,H202-219 and H220-237 were H-2d restricted epitopes of HpaA,of which H154-171 was the immunodominant one,its core sequence was H158-170 and its restriction molecule was H-2d（I-A）.All the result indicated that the epitope could be used for epitope-based vaccine design.

关 键 词：幽门螺杆菌 黏附素A抗原 CD4+T细胞 免疫优势表位 

分 类 号：R392[医药卫生—免疫学]