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人类粒系集落生成单位(CFU-GM)亚群中HLA-DR抗原的差异表达。

Differential expression of HLA-DR antigens in subsets of human CFU-GM.

作者信息

Griffin J D, Sabbath K D, Herrmann F, Larcom P, Nichols K, Kornacki M, Levine H, Cannistra S A

出版信息

Blood. 1985 Oct;66(4):788-95.

PMID:3929858
Abstract

Expression of HLA-DR surface antigens by granulocyte/monocyte colony-forming cells (CFU-GM) may be important in the regulation of proliferation of these cells. Using immunological techniques to enrich for progenitor cells, we investigated the expression of HLA-DR in subsets of CFU-GM. "Early" (day 14) CFU-GM express higher levels of HLA-DR than do "late" (day 7) CFU-GM. Among late CFU-GM, cells destined to form monocyte (alpha-naphthyl acetate esterase-positive) colonies express higher levels of HLA-DR than do CFU-GM destined to form granulocyte (chloroacetate esterase-positive) colonies. Because high-level expression of DR antigen was a marker for monocyte differentiation, we examined several lymphokines for their effects on both DR expression and in vitro commitment to monocyte differentiation by myeloid precursor cells. DR antigen density could be increased by more than twofold over 48 hours upon exposure to gamma-interferon (gamma-IFN), whereas colony-stimulating factors had no effect. This was associated with a dose-dependent inhibition of total CFU-GM number, and a relative, but not absolute, increase in the ratio of monocyte colonies to granulocyte colonies. Similarly, in day 7 suspension cultures of purified myeloid precursor cells, gamma-IFN inhibited cell proliferation and increased the ratio of monocytes to granulocytes. Thus, despite the induction of high levels of HLA-DR antigen on precursor cells (a marker of monocyte commitment), the dominant in vitro effect of gamma-IFN was inhibition of granulocyte differentiation.

摘要

粒细胞/单核细胞集落形成细胞(CFU-GM)表面HLA-DR抗原的表达可能在这些细胞的增殖调节中起重要作用。我们利用免疫技术富集祖细胞,研究了CFU-GM亚群中HLA-DR的表达。“早期”(第14天)CFU-GM比“晚期”(第7天)CFU-GM表达更高水平的HLA-DR。在晚期CFU-GM中,注定形成单核细胞(α-萘乙酸酯酶阳性)集落的细胞比注定形成粒细胞(氯乙酸酯酶阳性)集落的CFU-GM表达更高水平的HLA-DR。由于DR抗原的高水平表达是单核细胞分化的标志物,我们检测了几种淋巴因子对DR表达以及髓系前体细胞向单核细胞分化的体外定向作用的影响。暴露于γ-干扰素(γ-IFN)后,48小时内DR抗原密度可增加两倍以上,而集落刺激因子则无作用。这与CFU-GM总数的剂量依赖性抑制以及单核细胞集落与粒细胞集落比例的相对增加(但不是绝对增加)相关。同样,在纯化的髓系前体细胞的第7天悬浮培养物中,γ-IFN抑制细胞增殖并增加单核细胞与粒细胞的比例。因此,尽管在前体细胞上诱导了高水平的HLA-DR抗原(单核细胞定向的标志物),γ-IFN在体外的主要作用是抑制粒细胞分化。

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