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Phenotypic and functional heterogeneity of murine intestinal intraepithelial lymphocytes defined by cell density: implications for route of differentiation and responsiveness to proliferation induction.

机译:由细胞密度定义的鼠肠上皮内淋巴细胞的表型和功能异质性:对分化途径和对增殖诱导的响应性的影响。

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摘要

The phenotype and function of murine intestinal intraepithelial lymphocytes (IEL) was studied in a Percoll-fractionated preparation that consisted of low-density cells which migrated to the 40-50% Percoll interface (IEL-40), medium-density cells which migrated to the 50-55% interface (IEL-50), and high-density cells which migrated to the 55-70% interface (IEL-55). IEL-40 and IEL-50 cells, the subsets phenotypically most similar to mature IEL, consisted of CD3+ T cells that included CD4- CD8+ and CD4+ CD8+ cells; CD4+ CD8- cells were present only in the IEL-50 fraction. T-cell receptor (TcR)alpha beta and TcR gamma delta cells were present in both IEL-40 and IEL-50 fractions. In contrast, most IEL-55 were CD3-, heat-stable antigen (HSA)+ cells that were not B cells; some IEL-55 cells were CD3lo HSA- or CD3lo HSA+ suggesting that IEL-55 are immature T cells. TcR alpha beta but not TcR gamma delta was expressed in the IEL-55 fraction. All three IEL fractions consisted of both CD8 alpha alpha and CD8 alpha beta cells. There was considerable functional heterogeneity between the three IEL fractions such that CD3-induced proliferation was greatest for IEL-50 cells and least for IEL-55 cells; that activity correlated with the proportion of Thy-1+ cells within the fractions. Both IEL-40 and IEL-50 fractions contained activated cytotoxic T lymphocytes (CTL) that were 8-16-fold more lytic than IEL-55 cells. That IEL-55 cells may be precursors of some IEL-40 and IEL-50 cells was demonstrated by a shift in cell density and by an increase in proportions of cells expressing markers of IEL-40 and IEL-50 cells following in vitro stimulation via CD3. The relevance of these findings to differences in functional activities reported for murine IEL is discussed.
机译:在Percoll分离制剂中研究了小鼠肠道上皮内淋巴细胞(IEL)的表型和功能,该制剂由低密度细胞迁移至40-50%Percoll界面(IEL-40)组成,中等密度细胞迁移至50-55%的界面(IEL-50),以及迁移到55-70%的界面(IEL-55)的高密度单元。 IEL-40和IEL-50细胞,在表型上与成熟IEL最相似,由CD3 + T细胞组成,其中包括CD4- CD8 +和CD4 + CD8 +细胞。 CD4 + CD8-细胞仅存在于IEL-50级分中。 T细胞受体(TcR)alphaβ和TcRγδ细胞同时存在于IEL-40和IEL-50馏分中。相反,大多数IEL-55是CD3-而不是B细胞的热稳定抗原(HSA)+细胞。一些IEL-55细胞是CD3lo HSA-或CD3lo HSA +,这表明IEL-55是未成熟的T细胞。在IEL-55馏分中表达了TcR alpha beta,但没有TcRγδ。所有三个IEL级分均由CD8 alpha alpha和CD8 alpha beta细胞组成。在三个IEL部分之间存在相当大的功能异质性,因此CD3诱导的增殖对IEL-50细胞最大,而对IEL-55细胞最小;该活性与级分中Thy-1 +细胞的比例有关。 IEL-40和IEL-50馏分均包含活化的细胞毒性T淋巴细胞(CTL),其裂解性比IEL-55细胞高8-16倍。通过体外刺激,通过改变细胞密度和表达IEL-40和IEL-50细胞标记的细胞比例的增加,证明了IEL-55细胞可能是某些IEL-40和IEL-50细胞的前体。 CD3。讨论了这些发现与鼠IEL报道的功能活动差异的相关性。

著录项

  • 期刊名称 Immunology
  • 作者

    M Hamad; J R Klein;

  • 作者单位
  • 年(卷),期 1994(82),4
  • 年度 1994
  • 页码 611–616
  • 总页数 6
  • 原文格式 PDF
  • 正文语种
  • 中图分类 免疫学;
  • 关键词

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