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Selective Inhibition of NF-κB Activation by a Peptide That Blocks the Interaction of NEMO with the IκB Kinase Complex

机译:选择性抑制NF-κB活化的肽,该肽可阻止NEMO与IκB激酶复合物的相互作用。

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Activation of the transcription factor nuclear factor (NF)-κB by proinflamma-tory stimuli leads to increased expression of genes involved in inflammation. Activation of NF-κB requires the activity of an inhibitor of κB (IκB)-kinase (IKK) complex containing two kinases (IKKα and IKKβ) and the regulatory protein NEMO (NF-κB essential modifier). An amino-terminal α-helical region of NEMO associated with a carboxyl-terminal segment of IKKα and IKKβ that we term the NEMO-binding domain (NBD). A cell-permeable NBD peptide blocked association of NEMO with the IKK complex and inhibited cytokine-induced NF-κB activation and NF-κB-dependent gene expression. The peptide also ameliorated inflammatory responses in two experimental mouse models of acute inflammation. The NBD provides a target for the development of drugs that would block proinflammatory activation of the IKK complex without inhibiting basal NF-κB activity.
机译:促炎性刺激刺激转录因子核因子(NF)-κB的激活导致参与炎症的基因表达增加。 NF-κB的激活需要具有两种激酶(IKKα和IKKβ)和调节蛋白NEMO(NF-κB必需修饰剂)的κB(IκB)-激酶(IKK)复合物抑制剂的活性。 NEMO的氨基末端α螺旋区域与IKKα和IKKβ的羧基末端片段相关,我们称之为NEMO结合域(NBD)。细胞可渗透的NBD肽可阻止NEMO与IKK复合物的缔合,并抑制细胞因子诱导的NF-κB活化和NF-κB依赖性基因表达。该肽还改善了两种急性炎症实验小鼠模型的炎症反应。 NBD为药物开发提供了目标,该药物可在不抑制基础NF-κB活性的情况下阻断IKK复合物的促炎激活。

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