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白细胞介素-2基因诱导性发育变化的分子基础。

Molecular basis for developmental changes in interleukin-2 gene inducibility.

作者信息

Chen D, Rothenberg E V

机构信息

Division of Biology, California Institute of Technology, Pasadena 91125.

出版信息

Mol Cell Biol. 1993 Jan;13(1):228-37. doi: 10.1128/mcb.13.1.228-237.1993.

Abstract

At least three stages in the intrathymic development of pre-T cells are demarcated by differences in the competence to express the interleukin-2 (IL-2) gene as an acute response to stimulation. IL-2 inducibility appears to be acquired relatively early, prior to T-cell receptor (TcR) gene rearrangement. It is then abrogated during the stage when cells are subject to positive and negative selection, i.e., the fate determination processes that select cells for maturation or death. IL-2 inducibility finally reappears in mature classes of thymocytes that have undergone positive selection. To provide a basis for a molecular explanation of these developmental transitions, we have examined the representation in different thymocyte subsets of a set of DNA-binding proteins implicated in IL-2 gene regulation. As the DNA-binding activities of many factors are elicited only by inductive stimuli, the cells were cultured in the presence or absence of the calcium ionophore A23187 and phorbol ester. Our results separate these factors into four regulatory classes: (i) constitutive factors, such as Oct-1 and probably Sp1, that are expressed in thymocytes at all stages; (ii) inducible factors, such as NF-kappa B and complexes binding to the region of a CD28 response element, that can be activated in all thymocytes, including those cells (CD4+ CD8+ TcRlow) that can undergo selection; (iii) inducible factors, such as NF-AT and AP-1, that can be activated in mature (CD4+ CD8- TcRhigh) and immature (CD4- CD8- TcR-) thymocytes alike but not in the transitional stages when the cells (CD4+ CD8+ TcRlow) are subject to selection; and (iv) a factor containing CREB, which can be activated in thymocytes of all developmental stages by culture but does not require specific induction. These results verify that inducible transcription factors are targets of intrathymic developmental change. They also identify NF-AT and AP-1 as factors that are particularly sensitive to the mechanism altering thymocyte responses during the stages when thymocytes may undergo positive and negative selection.

摘要

前T细胞在胸腺内发育至少有三个阶段,这三个阶段可通过表达白细胞介素-2(IL-2)基因作为对刺激的急性反应的能力差异来区分。IL-2诱导能力似乎在相对早期获得,先于T细胞受体(TcR)基因重排。然后在细胞进行阳性和阴性选择的阶段,即选择细胞成熟或死亡的命运决定过程中,这种诱导能力被消除。IL-2诱导能力最终在经历了阳性选择的成熟胸腺细胞类别中重新出现。为了为这些发育转变提供分子解释的基础,我们研究了一组与IL-2基因调控有关的DNA结合蛋白在不同胸腺细胞亚群中的表现。由于许多因子的DNA结合活性仅由诱导刺激引发,因此细胞在存在或不存在钙离子载体A23187和佛波酯的情况下进行培养。我们的结果将这些因子分为四类调控因子:(i)组成型因子,如Oct-1以及可能的Sp1,它们在胸腺细胞的所有阶段都有表达;(ii)诱导型因子,如NF-κB和与CD28反应元件区域结合的复合物,它们可以在所有胸腺细胞中被激活,包括那些可以进行选择的细胞(CD4+ CD8+ TcRlow);(iii)诱导型因子,如NF-AT和AP-1,它们可以在成熟(CD4+ CD8- TcRhigh)和未成熟(CD4- CD8- TcR-)胸腺细胞中被激活,但在细胞(CD4+ CD8+ TcRlow)进行选择的过渡阶段则不能被激活;(iv)一种含有CREB的因子,它可以通过培养在所有发育阶段的胸腺细胞中被激活,但不需要特定诱导。这些结果证实诱导型转录因子是胸腺内发育变化的靶点。它们还确定NF-AT和AP-1是在胸腺细胞可能进行阳性和阴性选择的阶段对改变胸腺细胞反应的机制特别敏感的因子。

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