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Association of mesenchymal cells and immunoglobulins with differentiating epithelial cells

机译:间充质细胞和免疫球蛋白与分化的上皮细胞的关联

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Background Mesenchymal-epithelial interactions play an important role in the physiology and pathology of epithelial tissues. Mesenchymal cells either associate with epithelium basement membrane [pericytes and perivascular monocyte-derived cells (MDC)] or reside within epithelium (MDC and T cells). Although intraepithelial mesenchymal cells were suggested to contribute to the epithelium physiology, their association with particular steps in differentiation of epithelial cells, interactions among themselves, and their fate remain unclear. We studied epitopes of mesenchymal cells and their products (immunoglobulins) in stratified epithelium of uterine ectocervix, which is one of the prototypes of complete cellular differentiation from stem into the aged cells. Results Perivascular CD14 primitive MDC associated with basal (stem) epithelial cells. Thy-1 pericytes of microvasculature secreted intercellular vesicles, which associated with Ki67 postmitotic epithelial cells expressing MHC class I. Intraepithelial T cells showed an association with veiled type MDC [dendritic cell (DC) precursors] among parabasal cells, and exhibited fragmentation after entering intermediate (mature) epithelial layers. Mature DC secreted CD68 and exhibited fragmentation after reaching mid intermediate layers. Binding of IgM was detected at the top of each layer: in the upper parabasal, upper intermediate, and most surface epithelial cells. IgG was confined to the entire superficial layer. Conclusions These data suggest that the phylogenetically and ontogenetically developed hierarchy of mesenchymal cells (MDC, pericytes, T cells) and immunoglobulins (IgM, IgG) accompanies differentiation of epithelial cells from immature into the mature and aged phenotype. Further studies of an involvement of mesenchymal cells in the regulation of tissue homeostasis may bring novel approaches to the prevention and therapy of tissue dysfunctions characterized by permanent tissue immaturity (muscular dystrophy) or accelerated aging (degenerative diseases).
机译:背景间充质-上皮相互作用在上皮组织的生理和病理中起重要作用。间充质细胞与上皮基底膜[周细胞和血管周单核细胞衍生的细胞(MDC)]缔合,或位于上皮内(MDC和T细胞)。尽管上皮内间充质细胞被认为有助于上皮的生理,但它们与上皮细胞分化的特定步骤,它们之间的相互作用以及它们的命运的关联尚不清楚。我们研究了子宫外宫颈分层上皮中的间充质细胞及其产物(免疫球蛋白)的表位,这是从干细胞到衰老细胞的完全细胞分化的原型之一。结果血管周围CD14原始MDC与基底(干)上皮细胞相关。 Thy-1微血管分泌的细胞周细胞与表达MHC I类的Ki67有丝分裂后上皮细胞相关。上皮内T细胞与副基底膜细胞之间的带遮盖型MDC [树突状细胞(DC)前体]缔合,进入中间体(成熟)上皮层。成熟的DC分泌CD68,并在到达中间中间层后显示出碎片。在每一层的顶部检测到IgM的结合:在基底旁上层,中间上层和大多数表面上皮细胞中。 IgG被限制在整个表层。结论这些数据表明,间质细胞(MDC,周细胞,T细胞)和免疫球蛋白(IgM,IgG)的系统发育和个体发育层次伴随着上皮细胞从未成熟分化为成熟和衰老的表型。对间充质细胞参与组织稳态调节的进一步研究可能会带来预防和治疗以永久性组织不成熟(肌营养不良)或加速衰老(变性疾病)为特征的组织功能障碍的新方法。

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