Neuropilin-1 and Integrins as Receptors for Chromogranin A-Derived Peptides.
Angelo CortiGiulia AnderluzziFlavio CurnisPublished in: Pharmaceutics (2022)
Human chromogranin A (CgA), a 439 residue-long member of the " granin " secretory protein family, is the precursor of several peptides and polypeptides involved in the regulation of the innate immunity, cardiovascular system, metabolism, angiogenesis, tissue repair, and tumor growth. Despite the many biological activities observed in experimental and preclinical models for CgA and its most investigated fragments (vasostatin-I and catestatin), limited information is available on the receptor mechanisms underlying these effects. The interaction of vasostatin-1 with membrane phospholipids and the binding of catestatin to nicotinic and b2-adrenergic receptors have been proposed as important mechanisms for some of their effects on the cardiovascular and sympathoadrenal systems. Recent studies have shown that neuropilin-1 and certain integrins may also work as high-affinity receptors for CgA, vasostatin-1 and other fragments. In this case, we review the results of these studies and discuss the structural requirements for the interactions of CgA-related peptides with neuropilin-1 and integrins, their biological effects, their mechanisms, and the potential exploitation of compounds that target these ligand-receptor systems for cancer diagnosis and therapy. The results obtained so far suggest that integrins (particularly the integrin avb6) and neuropilin-1 are important receptors that mediate relevant pathophysiological functions of CgA and CgA fragments in angiogenesis, wound healing, and tumor growth, and that these interactions may represent important targets for cancer imaging and therapy.
Keyphrases
- endothelial cells
- wound healing
- papillary thyroid
- amino acid
- squamous cell
- vascular endothelial growth factor
- binding protein
- high resolution
- lymph node metastasis
- cell therapy
- healthcare
- squamous cell carcinoma
- fatty acid
- childhood cancer
- single molecule
- mass spectrometry
- protein protein
- social media
- climate change
- transcription factor
- induced pluripotent stem cells
- small molecule
- cell adhesion
- pluripotent stem cells
- replacement therapy