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人类正常髓系和红系分化过程中CD11/CD18(白细胞黏附分子1)及CD44黏附分子的表达

Expression of the CD11/CD18, leukocyte adhesion molecule 1, and CD44 adhesion molecules during normal myeloid and erythroid differentiation in humans.

作者信息

Kansas G S, Muirhead M J, Dailey M O

机构信息

Department of Pathology, University of Iowa College of Medicine, Iowa City.

出版信息

Blood. 1990 Dec 15;76(12):2483-92.

PMID:1702327
Abstract

We have used three-color flow cytometry to investigate the pattern of expression of the CD11/CD18, CD44, and leukocyte adhesion molecule 1 (LAM-1) adhesion molecules during myeloid and erythroid differentiation in humans. The earliest myeloid cells, identified as CD33loCD15-, were exclusively CD44hi but contained both leukocyte function-associated antigen 1 (LFA-1hi) and LFA-1lo cells, as well as LAM-1+ and LAM-1- cells. This CD33loCD15- myeloid subpopulation expressed only low levels of CD11c and failed to express CD11b, CD14, or any lymphoid (CD3, CD16, CD19) antigens or glycophorin. Commitment to monocyte differentiation, suggested by the presence of an LFA-1hi CD11c+ subset within the CD33loCD15- subpopulation, was clearly signaled by upregulation of CD33; these monocyte-lineage committed cells were exclusively CD33hi, CD44hi, CD11ahi, CD11c+, and exhibited a broad range of intensity of CD15 expression. Later stages of monopoiesis were identified by acquisition of CD11b, and subsequently of CD14. Myeloid cells committed to granulopoiesis remained LFA-1lo, and underwent a sharp upregulation of CD15 along with downregulation of both CD33 and CD44. Successive stages of granulocyte development were marked by expression of CD11b and, subsequently, of CD16. The earliest cells capable of erythroid differentiation were CD44hi, LFA-1lo, and LAM-1+. Both LFA-1 and LAM-1 were lost before the onset of glycophorin (glyco) expression, whereas CD44 expression remained high on glyco+ cells, which also expressed CD45. CD44 expression was intermediate on glyco+ CD71+ cells, and low on glyco+ CD45- CD71- cells, similar to normal, circulating erythrocytes. Our results allow us to phenotypically define discrete stages in the normal development of monocytes, neutrophils, and erythrocytes. The expression of LFA-1, LAM-1, and high levels of CD44 on the most primitive hematopoietic cells detectable by flow cytometry suggests that at least some of these molecules are critically involved in leukocyte adhesion during development.

摘要

我们运用三色流式细胞术,研究了人类髓系和红系分化过程中CD11/CD18、CD44和白细胞黏附分子1(LAM-1)黏附分子的表达模式。最早的髓系细胞被鉴定为CD33loCD15-,其仅表达高水平的CD44,但包含白细胞功能相关抗原1(LFA-1hi)和LFA-1lo细胞,以及LAM-1+和LAM-1-细胞。这个CD33loCD15-髓系亚群仅表达低水平的CD11c,且不表达CD11b、CD14或任何淋巴样(CD3、CD16、CD19)抗原或血型糖蛋白。CD33loCD15-亚群中存在LFA-1hi CD11c+亚群提示其向单核细胞分化,而CD33的上调则明确表明了这一过程;这些单核细胞系定向细胞仅为CD33hi、CD44hi、CD11ahi、CD11c+,并呈现出广泛的CD15表达强度范围。单核细胞生成的后期阶段通过获得CD11b得以识别,随后获得CD14。定向于粒细胞生成的髓系细胞仍为LFA-1lo,并伴随CD33和CD44的下调,CD15急剧上调。粒细胞发育的连续阶段以CD11b的表达为标志,随后是CD16的表达。最早能够进行红系分化的细胞为CD44hi、LFA-1lo和LAM-1+。在血型糖蛋白(glyco)表达开始之前,LFA-1和LAM-1均消失,而在glyco+细胞上CD44表达仍保持高水平,这些细胞也表达CD45。在glyco+ CD71+细胞上CD44表达处于中等水平,而在glyco+ CD45- CD71-细胞上表达较低,这与正常循环红细胞相似。我们的研究结果使我们能够从表型上定义单核细胞、中性粒细胞和红细胞正常发育过程中的离散阶段。通过流式细胞术可检测到的最原始造血细胞上LFA-1、LAM-1和高水平CD44的表达表明,这些分子中的至少一些在发育过程中对白细胞黏附起着关键作用。

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