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糖缀合物疫苗的抗原加工;肺炎球菌CRM(197)结合疫苗的多糖部分与抗原加工细胞表面的MHC II共定位。

Antigen processing of glycoconjugate vaccines; the polysaccharide portion of the pneumococcal CRM(197) conjugate vaccine co-localizes with MHC II on the antigen processing cell surface.

作者信息

Lai Zengzu, Schreiber John R

机构信息

Department of Pediatrics, Tufts University School of Medicine, Boston, MA 02111, USA.

出版信息

Vaccine. 2009 May 21;27(24):3137-44. doi: 10.1016/j.vaccine.2009.03.064. Epub 2009 Apr 10.

DOI:10.1016/j.vaccine.2009.03.064
PMID:19446183
Abstract

Pneumococcal (Pn) polysaccharides (PS) are T-independent (TI) antigens and do not induce immunological memory or antibodies in infants. Conjugation of PnPS to the carrier protein CRM(197) induces PS-specific antibody in infants, and memory similar to T-dependent (Td) antigens. Conjugates have improved immunogenicity via antigen processing and presentation of carrier protein with MHC II and recruitment of T cell help, but the fate of the PS attached to the carrier is unknown. To determine the location of the PS component of PnPS-CRM(197) in the APC, we separately labeled PS and protein and tracked their location. The PS of types 14-CRM(197) and 19F-CRM(197) was specifically labeled by Alexa Fluor 594 hydrazide (red). The CRM(197) was separately labeled red in a reaction that did not label PS. Labeled antigens were incubated with APC which were fixed, permeabilized and incubated with anti-MHC II antibody labeled green by Alexa Fluor 488, followed by confocal microscopy. Labeled CRM(197) was presented on APC surface and co-localized with MHC II (yellow). Labeled unconjugated 14 or 19F PS did not go to the APC surface, but PS labeled 14-CRM(197) and 19F-CRM(197) was internalized and co-localized with MHC II. Monoclonal antibody to type 14 PS bound to intracellular type 14 PS and PS-CRM(197). Brefeldin A and chloroquine blocked both CRM(197) and PS labeled 14-CRM(197) and 19F-CRM(197) from co-localizing with MHC II. These data suggest that the PS component of the CRM(197) glycoconjugate enters the endosome, travels with CRM(197) peptides to the APC surface and co-localizes with MHC II.

摘要

肺炎球菌(Pn)多糖(PS)是胸腺非依赖性(TI)抗原,不会在婴儿体内诱导免疫记忆或抗体产生。将PnPS与载体蛋白CRM(197)结合可在婴儿体内诱导产生PS特异性抗体,并产生类似于胸腺依赖性(Td)抗原的记忆。结合物通过抗原加工以及载体蛋白与MHC II的呈递和T细胞辅助的募集而提高了免疫原性,但与载体相连的PS的命运尚不清楚。为了确定PnPS-CRM(197)的PS成分在抗原呈递细胞(APC)中的位置,我们分别标记了PS和蛋白质并追踪它们的位置。14型-CRM(197)和19F型-CRM(197)的PS用Alexa Fluor 594酰肼(红色)特异性标记。CRM(197)在不标记PS的反应中单独标记为红色。将标记的抗原与APC一起孵育,然后固定、通透处理,并用Alexa Fluor 488标记为绿色的抗MHC II抗体孵育,随后进行共聚焦显微镜检查。标记的CRM(197)呈现在APC表面并与MHC II共定位(黄色)。标记的未结合的14型或19F型PS未到达APC表面,但标记的14-CRM(197)和19F-CRM(197)的PS被内化并与MHC II共定位。抗14型PS的单克隆抗体与细胞内的14型PS和PS-CRM(197)结合。布雷菲德菌素A和氯喹可阻止CRM(197)以及标记的14-CRM(197)和19F-CRM(197)的PS与MHC II共定位。这些数据表明,CRM(197)糖结合物的PS成分进入内体,与CRM(197)肽一起运输到APC表面并与MHC II共定位。

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