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神经生长因子的无机方面:铜(II)和锌(II)影响包含TrkA受体识别域的N端肽的神经生长因子模拟信号传导。

The Inorganic Side of NGF: Copper(II) and Zinc(II) Affect the NGF Mimicking Signaling of the N-Terminus Peptides Encompassing the Recognition Domain of TrkA Receptor.

作者信息

Pandini Giuseppe, Satriano Cristina, Pietropaolo Adriana, Gianì Fiorenza, Travaglia Alessio, La Mendola Diego, Nicoletti Vincenzo G, Rizzarelli Enrico

机构信息

Endocrinology, Department of Clinical and Experimental Medicine, Garibaldi-Nesima Medical Center, University of CataniaCatania, Italy; Institute of Biostructures and Bioimages - Catania, National Research CouncilCatania, Italy.

Department of Chemical Sciences, University of CataniaCatania, Italy; Consorzio Interuniversitario di Ricerca in Chimica dei Metalli nei Sistemi BiologiciBari, Italy.

出版信息

Front Neurosci. 2016 Dec 20;10:569. doi: 10.3389/fnins.2016.00569. eCollection 2016.

Abstract

The nerve growth factor (NGF) N-terminus peptide, NGF(1-14), and its acetylated form, Ac-NGF(1-14), were investigated to scrutinize the ability of this neurotrophin domain to mimic the whole protein. Theoretical calculations demonstrated that non-covalent forces assist the molecular recognition of TrkA receptor by both peptides. Combined parallel tempering/docking simulations discriminated the effect of the N-terminal acetylation on the recognition of NGF(1-14) by the domain 5 of TrkA (TrkA-D5). Experimental findings demonstrated that both NGF(1-14) and Ac-NGF(1-14) activate TrkA signaling pathways essential for neuronal survival. The NGF-induced TrkA internalization was slightly inhibited in the presence of Cu and Zn ions, whereas the metal ions elicited the NGF(1-14)-induced internalization of TrkA and no significant differences were found in the weak Ac-NGF(1-14)-induced receptor internalization. The crucial role of the metals was confirmed by experiments with the metal-chelator bathocuproine disulfonic acid, which showed different inhibitory effects in the signaling cascade, due to different metal affinity of NGF, NGF(1-14) and Ac-NGF(1-14). The NGF signaling cascade, activated by the two peptides, induced CREB phosphorylation, but the copper addition further stimulated the Akt, ERK and CREB phosphorylation in the presence of NGF and NGF(1-14) only. A dynamic and quick influx of both peptides into PC12 cells was tracked by live cell imaging with confocal microscopy. A significant role of copper ions was found in the modulation of peptide sub-cellular localization, especially at the nuclear level. Furthermore, a strong copper ionophoric ability of NGF(1-14) was measured. The Ac-NGF(1-14) peptide, which binds copper ions with a lower stability constant than NGF(1-14), exhibited a lower nuclear localization with respect to the total cellular uptake. These findings were correlated to the metal-induced increase of CREB and BDNF expression caused by NGF(1-14) stimulation. In summary, we here validated NGF(1-14) and Ac-NGF(1-14) as first examples of monomer and linear peptides able to activate the NGF-TrkA signaling cascade. Metal ions modulated the activity of both NGF protein and the NGF-mimicking peptides. Such findings demonstrated that NGF(1-14) sequence can reproduce the signal transduction of whole protein, therefore representing a very promising drug candidate for further pre-clinical studies.

摘要

研究了神经生长因子(NGF)N端肽NGF(1 - 14)及其乙酰化形式Ac - NGF(1 - 14),以考察该神经营养因子结构域模拟完整蛋白的能力。理论计算表明,非共价力有助于两种肽对TrkA受体的分子识别。结合并行回火/对接模拟,区分了N端乙酰化对TrkA结构域5(TrkA - D5)识别NGF(1 - 14)的影响。实验结果表明,NGF(1 - 14)和Ac - NGF(1 - 14)均能激活神经元存活所必需的TrkA信号通路。在铜离子和锌离子存在的情况下,NGF诱导的TrkA内化略有抑制,而金属离子引发了NGF(1 - 14)诱导的TrkA内化,且在弱的Ac - NGF(1 - 14)诱导的受体内化中未发现显著差异。金属螯合剂 bathocuproine二磺酸的实验证实了金属的关键作用,由于NGF、NGF(1 - 14)和Ac - NGF(1 - 14)对金属的亲和力不同,其在信号级联反应中表现出不同的抑制作用。两种肽激活的NGF信号级联反应诱导了CREB磷酸化,但仅在NGF和NGF(1 - 14)存在的情况下,添加铜进一步刺激了Akt、ERK和CREB磷酸化。通过共聚焦显微镜活细胞成像追踪了两种肽快速动态流入PC12细胞的过程。发现铜离子在调节肽的亚细胞定位中起重要作用,尤其是在核水平。此外,还测定了NGF(1 - 14)具有很强的铜离子载体能力。与NGF(1 - 14)相比,Ac - NGF(1 - 14)肽与铜离子结合的稳定常数较低,相对于总细胞摄取量,其核定位较低。这些发现与NGF(1 - 14)刺激引起的金属诱导的CREB和BDNF表达增加相关。总之,我们在此验证了NGF(1 - 14)和Ac - NGF(1 - 14)作为能够激活NGF - TrkA信号级联反应的单体和线性肽的首个实例。金属离子调节了NGF蛋白和模拟NGF的肽的活性。这些发现表明,NGF(1 - 14)序列可以重现完整蛋白的信号转导,因此是进一步临床前研究中非常有前景的药物候选物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6737/5201159/7707c637ac61/fnins-10-00569-s0001.jpg

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