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人类胎儿及胚胎肝脏中的造血作用。

Hemopoiesis in human fetal and embryonic liver.

作者信息

Timens W, Kamps W A

机构信息

Department of Pathology, University of Groningen, The Netherlands.

出版信息

Microsc Res Tech. 1997 Dec 1;39(5):387-97. doi: 10.1002/(SICI)1097-0029(19971201)39:5<387::AID-JEMT1>3.0.CO;2-E.

Abstract

In this review, we describe the topographic distribution of hemopoietic cells of the lymphoid, myeloid, and erythroid lineages in the human fetal and embryonic liver. The data are based on studies of frozen tissue, allowing the determination of a broad range of hemopoietic antigens, and studies on paraffin-embedded tissue, allowing the combination of optimal morphology and immunodetection of lineage-specific antigens. The different hemopoietic lineages each show their own immunophenotype and distribution; intercellular and microenvironmental relationships were easily determined. In a few cases, some scarce CD34-positive early progenitor cells were seen. The number of proliferating cells, identified by monoclonal antibody (MAb) Ki-67, varied from 350 to 2500 (median = 1,500) per square millimeter of tissue. Erythroid cells reacted with antisera to glycophorin A, CDw75, and CD43 and partly surround a central macrophage, whereas the myelomonocytic cells reacted with CD45, CD43, CD74, and antilysozyme serum, and with LN3 from 14 weeks onward. Myelopoietic (CD15 positive) cells were localized mainly around portal triad vessels and increased in number with gestational age. The lymphoid cells showed CD45, CD43, CD45RA/MT2, CD45RA/MB1, MB2, and CD74 reactivity. B cells and their precursors were scattered among the hepatocytes without any sign of focal development in the age range studied. We seldom found cells positive for delta-H chain or C3bR (CD35); C3dR (CD21)-positive cells were even more scarce. Cells reactive with MAb WT1 (CD7) were present in a scattered single pattern (< or = 20/mm2) among the parenchymal cells; cells expressing mature T-cell markers (CD2, CD3, CD5) were rare. Large (> 15 mu) CD43-positive hemopoietic cells in the fetal liver were distinguished that exclusively expressed CD43, probably representing early hemopoietic progenitor cells.

摘要

在本综述中,我们描述了人类胎儿及胚胎肝脏中淋巴系、髓系和红系造血细胞的拓扑分布。数据基于对冷冻组织的研究(可确定多种造血抗原)以及对石蜡包埋组织的研究(可将最佳形态学与谱系特异性抗原的免疫检测相结合)。不同的造血谱系各自呈现出独特的免疫表型和分布;细胞间及微环境关系易于确定。在少数情况下,可见一些稀少的CD34阳性早期祖细胞。通过单克隆抗体(MAb)Ki-67鉴定的增殖细胞数量为每平方毫米组织350至2500个(中位数 = 1500)。红系细胞与抗血型糖蛋白A、CDw75和CD43抗血清发生反应,并部分围绕中央巨噬细胞,而髓单核细胞与CD45、CD43、CD74和抗溶菌酶血清发生反应,并从14周起与LN3发生反应。髓系造血(CD15阳性)细胞主要定位于门三联血管周围,且数量随胎龄增加。淋巴系细胞表现出CD45、CD43、CD45RA/MT2、CD45RA/MB1、MB2和CD74反应性。在所研究的年龄范围内,B细胞及其前体分散在肝细胞之间,无任何局灶性发育迹象。我们很少发现δ-H链或C3bR(CD35)阳性细胞;C3dR(CD21)阳性细胞甚至更为稀少。与MAb WT1(CD7)反应的细胞以散在的单个模式(≤20个/mm²)存在于实质细胞中;表达成熟T细胞标志物(CD2、CD3、CD5)的细胞罕见。胎儿肝脏中可区分出大的(>15μm)CD43阳性造血细胞,其仅表达CD43,可能代表早期造血祖细胞。

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