RT Journal Article
SR Electronic
T1 Physiological and Biophysical Factors That Influence Alzheimer's Disease Amyloid Plaque Targeting of Native and Putrescine Modified Human Amyloid β40
JF Journal of Pharmacology and Experimental Therapeutics
JO J Pharmacol Exp Ther
FD American Society for Pharmacology and Experimental Therapeutics
SP 17
OP 25
DO 10.1124/jpet.105.095711
VO 318
IS 1
A1 Karunya K. Kandimalla
A1 Geoffry L. Curran
A1 Silvina S. Holasek
A1 Emily J. Gilles
A1 Thomas M. Wengenack
A1 Marina Ramirez-Alvarado
A1 Joseph F. Poduslo
YR 2006
UL http://jpet.aspetjournals.org/content/318/1/17.abstract
AB Amyloid β40 (Aβ40) and its derivatives are being developed as probes for the ante-mortem diagnosis of Alzheimer's disease. Putrescine-Aβ40 (PUT-Aβ40) showed better plaque targeting than the native Aβ40, which was not solely explained by the differences in their blood-brain-barrier (BBB) permeabilities. The objective of this study was to elucidate the physiological and biophysical factors influencing the differential targeting of Aβ40 and PUT-Aβ40. Despite better plaque-targeting ability 125I-PUT-Aβ40 was more rapidly cleared from the systemic circulation than amyloid β40 labeled with 125I (125I-Aβ40) after i.v. administration in mice. The BBB permeability of both compounds was inhibited by circulating peripheral Aβ40 levels. 125I-Aβ40 but not 125I-PUT-Aβ40 was actively taken up by the mouse brain slices in vitro. Only fluorescein-Aβ40, not fluorescein-PUT-Aβ40, was localized in the brain parenchymal cells in vitro. The metabolism of 125I-Aβ40 in the brain slices was twice as great as 125I-PUT-Aβ40. 125I-Aβ40 efflux from the brain slices was saturable and found to be 5 times greater than that of 125I-PUT-Aβ40. Thioflavin-T fibrillogenesis assay demonstrated that PUT-Aβ40 has a greater propensity to form insoluble fibrils compared with Aβ40, most likely due to the ability of PUT-Aβ40 to form β sheet structure more readily than Aβ40. These results demonstrate that the inadequate plaque targeting of Aβ40 is due to cellular uptake, metabolism, and efflux from the brain parenchyma. Despite better plaque targeting of PUTAβ40, its propensity to form fibrils may render it less suitable for human use and thus allow increased focus on the development of novel derivatives of Aβ with improved characteristics. The American Society for Pharmacology and Experimental Therapeutics