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Juglone, an inhibitor of the peptidyl-prolyl isomerase Pin1, also directly blocks transcription

机译:肽基脯氨酰异构酶Pin1的抑制剂Juglone也直接阻止转录

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摘要

The C-terminal domain (CTD) of the large subunit of RNA polymerase II plays a role in transcription and RNA processing. Yeast ESS1, a peptidyl-prolyl cis/trans isomerase, is involved in RNA processing and can associate with the CTD. Using several types of assays we could not find any evidence of an effect of Pin1, the human homolog of ESS1, on transcription by RNA polymerase II in vitro or on the expression of a reporter gene in vivo. However, an inhibitor of Pin1, 5-hydroxy-1,4-naphthoquinone (juglone), blocked transcription by RNA polymerase II. Unlike N-ethylmaleimide, which inhibited all phases of transcription by RNA polymerase II, juglone disrupted the formation of functional preinitiation complexes by modifying sulfhydryl groups but did not have any significant effect on either initiation or elongation. Both RNA polymerases I and III, but not T7 RNA polymerase, were inhibited by juglone. The primary target of juglone has not been unambiguously identified, although a site on the polymerase itself is suggested by inhibition of RNA polymerase II during factor-independent transcription of single-stranded DNA. Because of its unique inhibitory properties juglone should prove useful in studying transcription in vitro.
机译:RNA聚合酶II大亚基的C末端结构域(CTD)在转录和RNA加工中起作用。酵母ESS1是一种肽基-脯氨酰顺/反异构酶,参与RNA加工,可与CTD结合。使用几种类型的测定,我们找不到任何证据表明Pin1(ESS1的人类同源物)对体外RNA聚合酶II转录或体内报道基因表达的影响。但是,Pin1的抑制剂5-hydroxy-1,4-naphthoquinone(juglone)阻止了RNA聚合酶II的转录。与抑制RNA聚合酶II转录的所有阶段的N-乙基马来酰亚胺不同,朱古龙通过修饰巯基破坏了功能性预起始复合物的形成,但对起始或延伸没有任何明显影响。 RNA聚合酶I和III均可抑制,但不能抑制T7 RNA聚合酶。尽管在单链DNA的因子非依赖性转录过程中通过抑制RNA聚合酶II暗示了聚合酶本身的位点,但尚未明确确定juglone的主要靶标。由于其具有独特的抑制特性,因此在研究体外转录方面,juglone应该被证明很有用。

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