Protection from Alzheimer's-like disease in the mouse by genetic ablation of inducible nitric oxide synthase
C Nathan, N Calingasan, J Nezezon, A Ding… - The Journal of …, 2005 - rupress.org
The Journal of experimental medicine, 2005•rupress.org
Brains from subjects who have Alzheimer's disease (AD) express inducible nitric oxide
synthase (iNOS). We tested the hypothesis that iNOS contributes to AD pathogenesis.
Immunoreactive iNOS was detected in brains of mice with AD-like disease resulting from
transgenic expression of mutant human β-amyloid precursor protein (hAPP) and presenilin-
1 (hPS1). We bred hAPP-, hPS1-double transgenic mice to be iNOS+/+ or iNOS−/−, and
compared them with a congenic WT strain. Deficiency of iNOS substantially protected the AD …
synthase (iNOS). We tested the hypothesis that iNOS contributes to AD pathogenesis.
Immunoreactive iNOS was detected in brains of mice with AD-like disease resulting from
transgenic expression of mutant human β-amyloid precursor protein (hAPP) and presenilin-
1 (hPS1). We bred hAPP-, hPS1-double transgenic mice to be iNOS+/+ or iNOS−/−, and
compared them with a congenic WT strain. Deficiency of iNOS substantially protected the AD …
Brains from subjects who have Alzheimer's disease (AD) express inducible nitric oxide synthase (iNOS). We tested the hypothesis that iNOS contributes to AD pathogenesis. Immunoreactive iNOS was detected in brains of mice with AD-like disease resulting from transgenic expression of mutant human β-amyloid precursor protein (hAPP) and presenilin-1 (hPS1). We bred hAPP-, hPS1-double transgenic mice to be iNOS+/+ or iNOS−/−, and compared them with a congenic WT strain. Deficiency of iNOS substantially protected the AD-like mice from premature mortality, cerebral plaque formation, increased β-amyloid levels, protein tyrosine nitration, astrocytosis, and microgliosis. Thus, iNOS seems to be a major instigator of β-amyloid deposition and disease progression. Inhibition of iNOS may be a therapeutic option in AD.
rupress.org