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首页> 外文期刊>Expert opinion on therapeutic targets >STAT nuclear translocation: potential for pharmacological intervention.
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STAT nuclear translocation: potential for pharmacological intervention.

机译:STAT核易位:药理干预的潜力。

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摘要

The signal transducer and activator of transcription (STAT) proteins are extracellular ligand-responsive transcription factors that mediate broadly diverse biological processes, including cell proliferation, transformation, apoptosis, differentiation, fetal development, inflammation and immune response. Stimulation with multiple cytokines or growth factors all result in the tyrosine phosphorylation of STAT proteins and the subsequent gene regulation via their direct binding to the promoters of responsive genes. Cytokine-regulated gene activation is dependent on the continuous nucleocytoplasmic cycling of STAT signal transducers. The STATs use intricately intertwined karyopherin-dependent and -independent translocation mechanisms to coordinate the activation step at the cell membrane and gene expression in the nucleus. In addition, STATs appear to have cytokine-independent gene regulatory functions that may also depend on their regulated nucleocytoplasmic transfer. Numerous studies have implicated aberrant STAT signalling in cancer, immune defects and inflammatory diseases. Given the central role of intracellular trafficking for the proper signal processing by STAT proteins, pharmacological targeting of STAT nucleocytoplasmic translocation appears to be an attractive strategy to interfere with dysregulated cytokine signalling. This review will discuss possible scenarios that would result from the use of novel modulators of STAT shuttling, which may both increase or decrease STAT activation and, hence, transcriptional activity.
机译:信号转导和转录激活(STAT)蛋白是细胞外配体响应转录因子,可介导广泛的生物学过程,包括细胞增殖,转化,凋亡,分化,胎儿发育,炎症和免疫反应。用多种细胞因子或生长因子刺激均会导致STAT蛋白的酪氨酸磷酸化,并通过直接结合响应基因的启动子来进行随后的基因调节。细胞因子调节的基因激活取决于STAT信号转导子的连续核质循环。 STAT使用错综复杂的核转运蛋白依赖性和非依赖性转运机制来协调细胞膜上的活化步骤和细胞核中的基因表达。此外,STATs似乎具有不依赖细胞因子的基因调节功能,这也可能取决于其调节的胞质转移。大量研究表明STAT信号转导异常可能与癌症,免疫缺陷和炎性疾病有关。鉴于细胞内运输对STAT蛋白进行适当信号处理的核心作用,针对STAT核质易位的药理靶向似乎是干扰失调的细胞因子信号传导的有吸引力的策略。这篇综述将讨论可能的情况,这些情况可能是由于使用了STAT穿梭的新型调节剂所致,该调节剂既可以增加也可以减少STAT的激活,进而增加转录活性。

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