首页> 美国卫生研究院文献>The Journal of Experimental Medicine >A novel cysteine-rich sequence-specific DNA-binding protein interacts with the conserved X-box motif of the human major histocompatibility complex class II genes via a repeated Cys-His domain and functions as a transcriptional repressor
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A novel cysteine-rich sequence-specific DNA-binding protein interacts with the conserved X-box motif of the human major histocompatibility complex class II genes via a repeated Cys-His domain and functions as a transcriptional repressor

机译:一种新型的富含半胱氨酸的序列特异性DNA结合蛋白通过重复的Cys-His结构域与人类主要组织相容性复合体II类基因的保守X-box基序相互作用并起转录抑制因子的作用

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摘要

The class II major histocompatibility complex (MHC) molecules function in the presentation of processed peptides to helper T cells. As most mammalian cells can endocytose and process foreign antigen, the critical determinant of an antigen-presenting cell is its ability to express class II MHC molecules. Expression of these molecules is usually restricted to cells of the immune system and dysregulated expression is hypothesized to contribute to the pathogenesis of a severe combined immunodeficiency syndrome and certain autoimmune diseases. Human complementary DNA clones encoding a newly identified, cysteine-rich transcription factor, NF-X1, which binds to the conserved X-box motif of class II MHC genes, were obtained, and the primary amino acid sequence deduced. The major open reading frame encodes a polypeptide of 1,104 amino acids with a symmetrical organization. A central cysteine-rich portion encodes the DNA-binding domain, and is subdivided into seven repeated motifs. This motif is similar to but distinct from the LIM domain and the RING finger family, and is reminiscent of known metal-binding regions. The unique arrangement of cysteines indicates that the consensus sequence CX3CXL-XCGX1- 5HXCX3CHXGXC represents a novel cysteine-rich motif. Two lines of evidence indicate that the polypeptide encodes a potent and biologically relevant repressor of HLA-DRA transcription: (a) overexpression of NF-X1 from a retroviral construct strongly decreases transcription from the HLA-DRA promoter; and (b) the NF-X1 transcript is markedly induced late after induction with interferon gamma (IFN- gamma), coinciding with postinduction attenuation of HLA-DRA transcription. The NF-X1 protein may therefore play an important role in regulating the duration of an inflammatory response by limiting the period in which class II MHC molecules are induced by IFN-gamma.
机译:II类主要组织相容性复合物(MHC)分子在将加工后的肽呈递给辅助T细胞时发挥作用。由于大多数哺乳动物细胞都可以内吞并加工外源抗原,因此抗原呈递细胞的关键决定因素是其表达II类MHC分子的能力。这些分子的表达通常仅限于免疫系统的细胞,并且据推测表达失调会导致严重的联合免疫缺陷综合症和某些自身免疫性疾病的发病机理。获得了编码新鉴定的富含半胱氨酸的转录因子NF-X1的人互补DNA克隆,该因子与II类MHC基因的保守X-box基序结合,并推导了主要氨基酸序列。主要的开放阅读框编码具有对称结构的1,104个氨基酸的多肽。富含半胱氨酸的中央部分编码DNA结合结构域,并细分为七个重复的基序。该基序类似于但不同于LIM域和RING手指家族,并且使人联想到已知的金属结合区。半胱氨酸的独特排列表明共有序列CX3CXL-XCGX1-5HXCX3CHXGXC代表了一个富含半胱氨酸的新基序。有两条证据表明该多肽编码一种有效且与生物学相关的HLA-DRA转录阻遏物:(a)从逆转录病毒构建体中过表达NF-X1会强烈降低HLA-DRA启动子的转录; (b)干扰素γ(IFN-γ)诱导后晚期,NF-X1转录物被明显诱导,这与诱导后HLA-DRA转录的减弱相吻合。因此,NF-X1蛋白可能会通过限制IFN-γ诱导II类MHC分子的时间来在调节炎症反应的持续时间中发挥重要作用。

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