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人类成人及新生儿单核细胞表面决定簇的表达与调节

Expression and modulation of cell surface determinants on human adult and neonatal monocytes.

作者信息

Marwitz P A, Van Arkel-Vigna E, Rijkers G T, Zegers B J

机构信息

Department of Immunology, University Hospital for Children and Youth Het Wilhelmina Kinderziekenhuis, Utrecht, The Netherlands.

出版信息

Clin Exp Immunol. 1988 May;72(2):260-6.

Abstract

The difference between newborn and adult mononuclear cells in the antigen dose required for optimal antibody production in vitro can be ascribed to differences in the antigen-presenting capacities of the respective monocytes (Van Tol et al., 1984b). We have therefore studied the expression of cell surface determinants on human neonatal and adult monocytes by the use of monoclonal antibodies to membrane proteins including MHC antigens. No difference was observed in the expression of LeuM3 with regard to both the percentage of positive cells and the density of the respective determinant. In contrast, neonatal cells express the antigens OKM5, LFA1, OKM1 and LeuM5 at a lower density than adult cells do. The same holds for beta 2-microglobulin, but neonatal and adult monocytes express MHC class I alpha-chains at a similar density, whereas among the class II MHC antigens, HLA-DR is significantly more highly expressed on neonatal cells. This difference remains after treatment in vitro with gamma-interferon (gamma-IFN). Treatment with gamma-IFN also resulted in a less dense expression of the LeuM3 antigen. Preincubation of monocytes with LeuM3 monoclonal antibody partially abrogates subsequent upregulation of class II MHC antigens by gamma-IFN, a phenomenon observed with both neonatal and adult monocytes. These data indicate a functional involvement of LeuM3 with the cellular action of gamma-IFN. Taken together, the cell surface phenotype of neonatal monocytes is that of a highly efficient antigen presenting cell.

摘要

体外产生最佳抗体所需的抗原剂量,新生儿与成人单核细胞之间的差异可归因于各自单核细胞抗原呈递能力的差异(范托尔等人,1984b)。因此,我们通过使用针对包括MHC抗原在内的膜蛋白的单克隆抗体,研究了人新生儿和成人单核细胞表面决定簇的表达。在阳性细胞百分比和各自决定簇密度方面,未观察到LeuM3表达的差异。相比之下,新生儿细胞表达OKM5、LFA1、OKM1和LeuM5抗原的密度低于成人细胞。β2-微球蛋白也是如此,但新生儿和成人单核细胞表达MHC I类α链的密度相似,而在II类MHC抗原中,HLA-DR在新生儿细胞上的表达明显更高。用γ干扰素(γ-IFN)体外处理后,这种差异仍然存在。用γ-IFN处理也导致LeuM3抗原的表达密度降低。用LeuM3单克隆抗体对单核细胞进行预孵育,可部分消除γ-IFN随后对II类MHC抗原的上调作用,新生儿和成人单核细胞均观察到这一现象。这些数据表明LeuM3与γ-IFN的细胞作用存在功能关联。综上所述,新生儿单核细胞的细胞表面表型是高效抗原呈递细胞的表型。

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