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人类脾脏的胎儿期及出生后早期发育:从原始动脉B细胞小叶到非分叶器官。

Fetal and early post-natal development of the human spleen: from primordial arterial B cell lobules to a non-segmented organ.

作者信息

Steiniger Birte, Ulfig Norbert, Risse Manfred, Barth Peter J

机构信息

Institute of Anatomy and Cell Biology, University of Marburg, Robert-Koch-Str. 8, 35037, Marburg, Germany.

出版信息

Histochem Cell Biol. 2007 Sep;128(3):205-15. doi: 10.1007/s00418-007-0296-4. Epub 2007 Jul 12.

DOI:10.1007/s00418-007-0296-4
PMID:17624541
Abstract

Immunohistological analysis of 31 human spleens from the 11th week of gestation to the early postnatal period suggested that fetal organ development may be preliminarily divided into four stages. At stage 0 the organ anlage contained erythrocyte precursors, few macrophages and almost no lymphocytes. Fetal spleens of stage I exhibited arterial vascular lobules and lymphocytes just began colonizing the organ. At stage II, B and T lymphocytes formed periarteriolar clusters. B cell clusters predominated, because B cells aggregated around the more peripheral branches of splenic arterioles, while T cells occupied the more centrally located parts of the vessels. The vascular lobules of stage I and II consisted of central arterioles surrounded by B cells, capillaries and peripheral venules. The lobular architecture slowly dissolved at late stage II when sinuses grew out from the peripheral venules into the centre of the lobule. Interestingly, the B cell accumulations around peripheral arterioles did not represent the precursors of follicles, but apparently persisted as periarteriolar B cell clusters in the adult splenic red pulp, while follicles containing FDCs developed at late stage II from B cells in direct contact to T cell clusters around larger arterial vessels. At stage III before birth the lobular architecture was no longer recognized. The chemokine CXCL13 was already present in vascular smooth muscle and adjacent stromal cells at stage I before B cells immigrated. CCL21, on the contrary, was only demonstrated in fibroblast-like cells supporting T cell clusters from stage II onwards.

摘要

对31例从妊娠第11周直至出生后早期的人类脾脏进行免疫组织学分析表明,胎儿器官发育可能初步分为四个阶段。在0期,器官原基含有红细胞前体、少量巨噬细胞且几乎没有淋巴细胞。I期胎儿脾脏呈现出动脉血管小叶,淋巴细胞刚开始在该器官中定植。在II期,B淋巴细胞和T淋巴细胞形成动脉周围簇。B细胞簇占主导,因为B细胞聚集在脾小动脉较外周的分支周围,而T细胞占据血管更靠中心的部位。I期和II期的血管小叶由被B细胞、毛细血管和外周小静脉围绕的中央小动脉组成。在II期末期,当血窦从小周静脉向小叶中心生长时,小叶结构逐渐溶解。有趣的是,外周小动脉周围的B细胞聚集并非滤泡前体,而是明显作为动脉周围B细胞簇持续存在于成人脾脏红髓中;而含有滤泡树突状细胞的滤泡在II期末期由与较大动脉血管周围T细胞簇直接接触的B细胞发育而来。在出生前的III期,不再能识别小叶结构。趋化因子CXCL13在B细胞迁入前的I期就已存在于血管平滑肌和相邻的基质细胞中。相反,CCL21仅从II期起在支持T细胞簇的成纤维细胞样细胞中被证实。

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