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1H-, 13C- and 15N-NMR assignment of the N-terminal domain of human cerebral dopamine neurotrophic factor (CDNF)

机译:人脑多巴胺神经营养因子(CDNF)N末端结构域的1H-,13C-和15N-NMR分配

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摘要

Parkinson’s disease (PD) is a neurodegenerative disorder that is caused by the death of midbrain dopaminergic neurons. Current therapies for PD do not halt the neurodegeneration nor repair the affected neurons. Therefore, search for novel neurotrophic factors (NTF) for midbrain dopaminergic neurons, which could be used in novel therapeutic approaches, is highly wanted. In 2007, a potent NTF for dopaminergic neurons was described as the conserved dopamine neurotrophic factor (CDNF). Single doses of this protein protect and restore dopaminergic neurons in experimental models of PD. CDNF has two domains; an N-terminal saposin-like domain, which may bind to membranes; and a presumably intrinsically unstructured C-terminal which contains an internal cysteine bridge in a CXXC motif similar to that of thiol/disulphide oxidoreductases and isomerases, and may thus reduce the endoplasmic reticulum stress caused by incorrectly folded proteins. We show for the first time the nuclear magnetic resonance assignment of N-terminal domain of recombinant CDNF (residues 1–105) by solution 2D and 3D NMR spectroscopy. We were able to obtain a nearly complete resonance assignment, which is the first step toward the solution structure determination of this neurotrophicfactor.
机译:帕金森氏病(PD)是由中脑多巴胺能神经元死亡引起的神经退行性疾病。目前用于PD的疗法不能阻止神经变性或修复受影响的神经元。因此,迫切需要寻找可用于新型治疗方法的中脑多巴胺能神经元的新型神经营养因子(NTF)。 2007年,一种有效的多巴胺能神经元NTF被描述为保守的多巴胺神经营养因子(CDNF)。在PD实验模型中,单剂量这种蛋白质可保护和恢复多巴胺能神经元。 CDNF具有两个域; N端的saposin样结构域,可以结合到膜上;推测是本质上无结构的C末端,在CXXC基序中包含一个内部半胱氨酸桥,类似于硫醇/二硫键氧化还原酶和异构酶,因此可以减少蛋白质折叠错误引起的内质网应激。我们首次通过溶液2D和3D NMR光谱显示了重组CDNF(残基1–105)的N端结构域的核磁共振分配。我们能够获得几乎完整的共振分配,这是确定该神经营养因子溶液结构的第一步。

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