Bednar_2002_Mol.Cell.Neurosci_20_354

Reference

Title : Selective nicotinic receptor consequences in APP(SWE) transgenic mice - Bednar_2002_Mol.Cell.Neurosci_20_354
Author(s) : Bednar I , Paterson D , Marutle A , Pham TM , Svedberg M , Hellstrom-Lindahl E , Mousavi M , Court J , Morris C , Perry E , Mohammed A , Zhang X , Nordberg A
Ref : Molecular & Cellular Neurosciences , 20 :354 , 2002
Abstract :

The nicotinic (nAChRs) and muscarinic (mAChRs) acetylcholine receptors and acetylcholinesterase (AChE) activity were studied in the brains of APP(SWE) transgenic mice (Tg+) and age-matched nontransgenic controls (Tg-) that were between 4 and 19 months of age. A significant increase in the binding of 125I-labeled alpha-bungarotoxin (alpha7 nAChRs) was observed in most brain regions analyzed in 4-month-old Tg+ mice, preceding learning and memory impairments and amyloid-beta (Abeta) pathology. The enhanced alpha7 receptor binding was still detectable at 17-19 months of age. Increase in [3H]cytisine binding (alpha4beta2 nAChRs) was measured at 17-19 months of age in Tg+ mice, at the same age when the animals showed heavy Abeta pathology. No significant changes in [3H]pirenzepine (M1 mAChRs) or [3H]AFDX 384 (M2 mAChRs) binding sites were found at any age studied. The upregulation of the nAChRs probably reflects compensatory mechanisms in response to Abeta burden in the brains of Tg+ mice.

PubMedSearch : Bednar_2002_Mol.Cell.Neurosci_20_354
PubMedID: 12093166

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Citations formats

Bednar I, Paterson D, Marutle A, Pham TM, Svedberg M, Hellstrom-Lindahl E, Mousavi M, Court J, Morris C, Perry E, Mohammed A, Zhang X, Nordberg A (2002)
Selective nicotinic receptor consequences in APP(SWE) transgenic mice
Molecular & Cellular Neurosciences 20 :354

Bednar I, Paterson D, Marutle A, Pham TM, Svedberg M, Hellstrom-Lindahl E, Mousavi M, Court J, Morris C, Perry E, Mohammed A, Zhang X, Nordberg A (2002)
Molecular & Cellular Neurosciences 20 :354