Yamaguchi K, Near R I, Matulka R A, Shneider A, Toselli P, Trombino A F, Sherr D H
Department of Environmental Health, Boston University Schools of Medicine and Public Health, MA 02118, USA.
J Immunol. 1997 Mar 1;158(5):2165-73.
In the absence of known endogenous ligands, investigators have exploited ubiquitous environmental pollutants, including polycyclic aromatic hydrocarbons, to gain insight into the physiologic functions of the aryl hydrocarbon (dioxin) receptor/transcription factor (AhR). AhR ligands induce cell transformation and steroid-like immunosuppression, suggesting a role for the AhR in regulation of cell growth and/or function. However, mechanisms through which the AhR influences cells in general and lymphocytes in particular remain unresolved. A murine model of B cell development was created to: 1) examine a role for the AhR in immunosuppression; 2) define mechanisms of AhR ligand immunosuppression; 3) characterize AhR expression in preB cells, in bone marrow stromal cells that support preB cells, or in primary bone marrow B cells; and 4) determine if AhR ligands suppress lymphopoiesis by acting directly on preB cells or indirectly via the microenvironment, as represented by bone marrow stromal cells. Results indicate that: 1) low doses (> or = 10(-8) M) of the prototypic AhR ligand, 7,12-dimethylbenz[a]anthracene (DMBA), induce preB cell apoptosis in 12 to 24 h; 2) alpha-naphthoflavone, an AhR and cytochrome P-450 inhibitor, blocks DMBA-induced apoptosis; 3) AhR mRNA and functional AhR protein are expressed at high levels in bone marrow stromal cells (little or no AhR is present in preB cell lines), and 4) preB cells maintained in rIL-7 do not undergo DMBA-induced apoptosis unless cultured with stromal cells. Results underscore the regulatory role played by bone marrow stromal cells in lymphopoiesis and support the hypothesis that the AhR effects immunosuppression by inducing stromal cells to deliver a death signal to lymphocytes.
在缺乏已知内源性配体的情况下,研究人员利用包括多环芳烃在内的普遍存在的环境污染物,来深入了解芳烃(二噁英)受体/转录因子(AhR)的生理功能。AhR配体可诱导细胞转化和类固醇样免疫抑制,提示AhR在细胞生长和/或功能调节中发挥作用。然而,AhR影响一般细胞尤其是淋巴细胞的机制仍未明确。构建了一个B细胞发育的小鼠模型,目的是:1)研究AhR在免疫抑制中的作用;2)确定AhR配体免疫抑制的机制;3)描述前B细胞、支持前B细胞的骨髓基质细胞或原代骨髓B细胞中AhR的表达特征;4)确定AhR配体是直接作用于前B细胞还是通过骨髓基质细胞所代表的微环境间接抑制淋巴细胞生成。结果表明:1)原型AhR配体7,12-二甲基苯并[a]蒽(DMBA)的低剂量(≥10^(-8) M)在12至24小时内可诱导前B细胞凋亡;2)AhR和细胞色素P-450抑制剂α-萘黄酮可阻断DMBA诱导的凋亡;3)AhR mRNA和功能性AhR蛋白在骨髓基质细胞中高水平表达(前B细胞系中存在很少或不存在AhR),以及4)在rIL-7中培养的前B细胞除非与基质细胞一起培养,否则不会发生DMBA诱导的凋亡。结果强调了骨髓基质细胞在淋巴细胞生成中所起的调节作用,并支持以下假设:AhR通过诱导基质细胞向淋巴细胞传递死亡信号来影响免疫抑制。
