Nicotine and amyloid formation

beta-sheet or random, extended chain-->beta-sheet). In previous work, we and others established that nicotine, a major component of cigarette smoke, inhibits beta-amyloidosis of the Abeta(1-42), which may result from nicotine binding to the alpha-helical structure. These conclusions were based on solution nuclear magnetic resonance (NMR) spectroscopic studies with the nonnative 28-residue Abeta(1-28). This information suggests that, when administered therapeutically to AD patients, nicotine may not only affect cholinergic activation, but could also conceivably alter amyloid deposition. In this report, NMR studies were augmented with the naturally occurring Abeta(1-42), under conditions where the peptide folds into a predominantly alpha-helical or random, extended chain structure. The major result is that nicotine shows only modest binding to these conformations, indicating that the nicotine inhibition to beta-amyloidosis probably results from binding to a small, soluble beta-sheet aggregate that is NMR invisible. -->

ISSN:	0006-3223
Přístupová URL adresa:	https://explore.openaire.eu/search/publication?articleId=doi_dedup___::5541d920a790da5c3396f61afb0dac3b https://pubmed.ncbi.nlm.nih.gov/11230876
Rights:	OPEN
Přírůstkové číslo:	edsair.doi.dedup.....5541d920a790da5c3396f61afb0dac3b
Autor:	Nanda K. Menon, Robert P. Freidland, Li Jun Peng, Hong Zeng, Arthur R. Salomon, Michael G. Zagorski, Yongbo Zhang, Jing Yang, Haiyan Shao
Rok vydání:	2001
Předmět:	Nicotine Magnetic Resonance Spectroscopy Amyloid Protein Conformation Peptide Receptors Nicotinic Structure-Activity Relationship Protein structure Alzheimer Disease mental disorders medicine Humans Amino Acid Sequence Peptide sequence Biological Psychiatry chemistry.chemical_classification Amyloid beta-Peptides P3 peptide Brain Peptide Fragments Mechanism of action chemistry Biochemistry Cholinergic medicine.symptom medicine.drug
Zdroj:	Biological psychiatry. 49(3)
ISSN:	0006-3223
Popis:	The major protein constituents of amyloid deposits in Alzheimer's disease (AD) are the 40-residue beta-amyloid (Abeta) (1-40) peptide and the 42-residue Abeta(1-42) peptide. The Abeta(1-42) is more pathogenic and produced in greater quantities in familial forms of AD. A major goal of research is to uncover a suitable inhibitor that either slows down or inhibits Abeta formation (beta-amyloidosis). During beta-amyloidosis, structural changes associated with the conversion of monomeric Abeta peptide building blocks into the aggregated fibrillar beta-sheet structures occur (alpha-helix-->beta-sheet or random, extended chain-->beta-sheet). In previous work, we and others established that nicotine, a major component of cigarette smoke, inhibits beta-amyloidosis of the Abeta(1-42), which may result from nicotine binding to the alpha-helical structure. These conclusions were based on solution nuclear magnetic resonance (NMR) spectroscopic studies with the nonnative 28-residue Abeta(1-28). This information suggests that, when administered therapeutically to AD patients, nicotine may not only affect cholinergic activation, but could also conceivably alter amyloid deposition. In this report, NMR studies were augmented with the naturally occurring Abeta(1-42), under conditions where the peptide folds into a predominantly alpha-helical or random, extended chain structure. The major result is that nicotine shows only modest binding to these conformations, indicating that the nicotine inhibition to beta-amyloidosis probably results from binding to a small, soluble beta-sheet aggregate that is NMR invisible.
Databáze:	OpenAIRE
Externí odkaz:	https://explore.openaire.eu/search/publication?articleId=doi_dedup___::5541d920a790da5c3396f61afb0dac3b https://pubmed.ncbi.nlm.nih.gov/11230876 Zobrazit plný text záznamu Full Text from ScienceDirect