Publications by authors named "G Tabbi"

A low level of Neurotrophins (NTs), their Tyrosine Kinase Receptors (Trks), Vascular Endothelial Growth Factors (VEGFs) and their receptors, mainly VEGFR1 and VEGFR2, characterizes AD brains. The use of NTs and VEGFs as drugs presents different issues due to their low permeability of the blood-brain barrier, the poor pharmacokinetic profile, and the relevant side effects. To overcome these issues, different functional and structural NT mimics have been employed.

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Article Synopsis
  • Neurotrophins, important for the central nervous system development and functioning, face challenges in drug application due to instability and side effects.
  • This study focuses on a cyclic peptide, c-NGF(1-14), which mimics the neurotrophic growth factor and demonstrates a stable conformation that interacts effectively with the NGF receptor TrkA.
  • c-NGF(1-14) promotes PC12 cell differentiation and enhances biological activities when bound to copper, ultimately activating key signaling pathways that lead to the release of beneficial growth factors like BDNF and VEGF.
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A series of copper(II) complexes with the formula [CuHy()Car%] varying the molecular weight (MW) of Hyaluronic acid (Hy, = 200 or 700 kDa) conjugated with carnosine (Car) present at different loading were synthesized and characterized via different spectroscopic techniques. The metal complexes behaved as Cu, Zn-superoxide dismutase (SOD1) mimics and showed some of the most efficient reaction rate values produced using a synthetic and water-soluble copper(II)-based SOD mimic reported to date. The increase in the percentage of Car moieties parallels the enhancement of the I value determined via the indirect method of Fridovich.

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Ctr1 regulates copper uptake and its intracellular distribution. The first 14 amino acid sequence of the Ctr1 ectodomain Ctr1 encompasses the characteristic Amino Terminal Cu and Ni binding motif (ATCUN) as well as the bis-His binding motif (His5 and His6). We report a combined thermodynamic and spectroscopic (UV-vis, CD, EPR) study dealing with the formation of Cu homobinuclear complexes with Ctr1, the percentage of which is not negligible even in the presence of a small Cu excess and clearly prevails at a M/L ratio of 1.

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The angiogenin protein (ANG) is one of the most potent endogenous angiogenic factors. In this work we characterized by means of potentiometric, spectroscopic and voltammetric techniques, the copper complex species formed with peptide fragments derived from the N-terminal domain of the protein, encompassing the sequence 1-17 and having free amino, Ang1-17, or acetylated N-terminus group, AcAng1-17, so to explore the role of amino group in metal binding and cellular copper uptake. The obtained data show that amino group is the main copper anchoring site for Ang1-17.

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