Brandtzaeg P, Bjerke K
Laboratory for Immunohistochemistry and Immunopathology (LIIPAT), University of Oslo, National Hospital, Norway.
Immunol Invest. 1989 Jan-May;18(1-4):29-45. doi: 10.3109/08820138909112225.
Human Peyers patches (PP) were studied by immunohistochemistry to characterize functional properties of the follicle-associated epithelium (FAE) including the "membrane" (M) cells. The FAE had no transporting capacity for polymeric IgA (pIgA) because it did not express the secretory component (SC) which acts as a pIgA receptor. However, it expressed MHC class II (HLA-DR) determinants, except for the M cells (which were tentatively identified by absence of brush border alkaline phosphatase). It is possible, therefore, that the FAE generally performs class II-restricted transport and presentation to T cells of antigens which have been adequately processed in the gut lumen. The function of M cells may be limited to transport of particulate or undegraded antigens to subjacent macrophages for processing and subsequent presentation. There were significantly more intra- and subepithelial T cells in PP than in distant villi, and the T cells were concentrated adjacent to M cells. The proportion of the CD4+ phenotype (putative helper T cells) was much higher in FAE (approximately 40%) than in villous epithelium where the CD8+ (putative suppressor) phenotype predominated strikingly (approximately 90%). This disparity might reflect differences in capacity for positive and negative immune regulation at the two sites. The B cells terminating with Ig production in PP and adjacent to solitary lymphoid follicles apparently belonged to relatively mature memory clones as they showed a large proportion of IgG immunocytes and reduced J-chain expression. Conversely, both IgG and IgA immunocytes in lamina propria (LP) showed a high percentage of J-chain positivity (80-100%); such positivity was also considerable (45-60%) in mesenteric lymph nodes (MLN) in contrast to peripheral lymph nodes (PLN) and palatine tonsils (PT). Moreover, there was a decreasing percentage of IgA2 immunocytes in the order of PP (52%), distant ileal LP (40%), MLN (32%), PLN (11%), and PT (5%). Taken together, our results suggested that dissemination of relatively immature memory B-cell clones with high J-chain expression takes place from PP through MLN and that preferential settlement of such clones occurs in LP.
采用免疫组织化学方法对人派伊尔结(PP)进行研究,以表征包括“膜”(M)细胞在内的滤泡相关上皮(FAE)的功能特性。FAE对聚合IgA(pIgA)没有转运能力,因为它不表达作为pIgA受体的分泌成分(SC)。然而,除了M细胞(暂通过缺乏刷状缘碱性磷酸酶来鉴定)外,它表达MHC II类(HLA-DR)决定簇。因此,FAE可能通常进行II类限制的抗原转运,并将在肠腔内已充分加工的抗原呈递给T细胞。M细胞的功能可能仅限于将颗粒状或未降解的抗原转运至下方的巨噬细胞进行加工并随后呈递。PP中的上皮内和上皮下T细胞明显多于远处的绒毛,并且T细胞集中在M细胞附近。FAE中CD4 +表型(假定的辅助性T细胞)的比例(约40%)远高于绒毛上皮,在绒毛上皮中CD8 +(假定的抑制性)表型占主导(约90%)。这种差异可能反映了两个部位在阳性和阴性免疫调节能力上的差异。在PP中以及与孤立淋巴滤泡相邻处终止于Ig产生的B细胞显然属于相对成熟的记忆克隆,因为它们显示出很大比例的IgG免疫细胞且J链表达降低。相反,固有层(LP)中的IgG和IgA免疫细胞均显示出高比例的J链阳性(80 - 100%);与外周淋巴结(PLN)和腭扁桃体(PT)相比,肠系膜淋巴结(MLN)中的这种阳性也相当可观(45 - 60%)。此外,IgA2免疫细胞的百分比按PP(52%)、远端回肠LP(40%)、MLN(32%)、PLN(11%)和PT(5%)的顺序递减。综上所述,我们的结果表明,具有高J链表达的相对不成熟记忆B细胞克隆从PP通过MLN扩散,并且此类克隆优先定居在LP中。
