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人类脾脏的胎儿期和新生儿期发育:一项免疫组织学研究。

Fetal and neonatal development of human spleen: an immunohistological study.

作者信息

Timens W, Rozeboom T, Poppema S

出版信息

Immunology. 1987 Apr;60(4):603-9.

PMID:3294575
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1453267/
Abstract

Localization and immunophenotype of lymphocyte subsets in fetal human spleens were studied by employing a panel of monoclonal antibodies (McAb) in an immunoperoxidase staining procedure on frozen tissue sections. Spleens varied from 15 weeks of gestational age (gestational weeks, gw) to newborn. The white pulp consisted of intermediate-sized lymphocytes; no separate compartments could be discerned. Germinal centre development was not observed. Dendritic cells stained for B2, HB5, aC3bR, anti-DRC and OKIa, but in most cases not for immunoglobulin. Although low cellular immunity is observed in neonates, T cells showed adult phenotypes in proportions comparable to the adult situation; immature OKT6(+) lymphocytes were rarely seen. Very few cells stained with anti-NK cell antibody Leu7. B cells all expressed B1, Leu14, aC3bR, T10 and OKIa, were strongly positive for BA1, and mostly stained very weakly for B2 and HB5. Almost all B cells expressed IgM and IgD simultaneously, and very few expressed IgG. IgA-positive cells were absent. At 15 gw a considerable number of IgM(+) B cells showed Leu1 staining, but this decreased during development. These cells may represent the normal counterpart of Leu1(+) IgM(+) cells observed in B-CLL and immunocytic and centrocytic malignant lymphomas. After 25 gw only very few Leu1(+) IgM(+) cells were seen. Altogether, the morphology and immunophenotype of white pulp B cells were different from the predominating adult B-cell subsets, at least until birth. These 'immature' splenic B cells may be precursors for adult splenic B-cell subsets. Considering the presumed role of the marginal zone in the immunity against TI-2 antigens, the absence of a marginal zone at birth may be a main factor in the defective immunity against these antigens in neonates.

摘要

通过在冷冻组织切片上采用一组单克隆抗体(McAb)进行免疫过氧化物酶染色程序,研究了人胎儿脾脏中淋巴细胞亚群的定位和免疫表型。脾脏的胎龄从15周(孕周,gw)到新生儿不等。白髓由中等大小的淋巴细胞组成;无法分辨出单独的区域。未观察到生发中心的发育。树突状细胞对B2、HB5、aC3bR、抗DRC和OKIa染色,但在大多数情况下对免疫球蛋白不染色。尽管新生儿中观察到低细胞免疫,但T细胞表现出与成人情况相当比例的成人表型;很少见到未成熟的OKT6(+)淋巴细胞。用抗NK细胞抗体Leu7染色的细胞非常少。B细胞均表达B1、Leu14、aC3bR、T10和OKIa,对BA1呈强阳性,对B2和HB5大多染色非常弱。几乎所有B细胞同时表达IgM和IgD,很少表达IgG。不存在IgA阳性细胞。在15gw时,相当数量的IgM(+)B细胞显示Leu1染色,但在发育过程中这种染色减少。这些细胞可能代表在B-CLL以及免疫细胞性和中心细胞性恶性淋巴瘤中观察到的Leu1(+)IgM(+)细胞的正常对应物。在25gw之后,仅可见极少数Leu1(+)IgM(+)细胞。总之,至少在出生前,白髓B细胞的形态和免疫表型与占主导地位的成人B细胞亚群不同。这些“未成熟”的脾脏B细胞可能是成人脾脏B细胞亚群的前体。考虑到边缘区在针对TI-2抗原的免疫中的假定作用,出生时边缘区的缺失可能是新生儿对这些抗原免疫缺陷的主要因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d794/1453267/19fa1bac4e9a/immunology00173-0119-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d794/1453267/b2e6d6fd2037/immunology00173-0117-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d794/1453267/26a6310f42b8/immunology00173-0118-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d794/1453267/0934ebb66e34/immunology00173-0118-b.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d794/1453267/19fa1bac4e9a/immunology00173-0119-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d794/1453267/b2e6d6fd2037/immunology00173-0117-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d794/1453267/26a6310f42b8/immunology00173-0118-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d794/1453267/0934ebb66e34/immunology00173-0118-b.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d794/1453267/19fa1bac4e9a/immunology00173-0119-a.jpg

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