Intranasal insulin improves cognition and modulates {beta}-amyloid in early AD

doi:10.1212/01.WNL.0000265401.62434.36

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Intranasal insulin improves cognition and modulates ${beta}$ -amyloid in early AD

M. A. Reger PhD, G. S. Watson PhD, P. S. Green PhD, C. W. Wilkinson PhD, L. D. Baker PhD, B. Cholerton PhD, M. A. Fishel MD, S. R. Plymate MD, J. C.S. Breitner MD, MPH, W. DeGroodt MS, P. Mehta PhD, and S. Craft PhD^*

From the Departments of Psychiatry and Behavioral Science (M.A.R., G.S.W., C.W.W., L.D.B., B.C., J.C.S.B., S.C.), Medicine (P.S.G., S.R.P.), and Neurology (M.A.F.), University of Washington School of Medicine, Seattle; Geriatric Research, Education, and Clinical Center (G.S.W., C.W.W., L.D.B., B.C., M.A.F., S.R.P., J.C.S.B., S.C.), Research and Development (P.S.G.), Veterans Affairs Puget Sound Health Care System, Seattle; Kurve Technology, Inc. (W.D.), Bothell, WA; and Department of Immunology (P.M.), Institute for Basic Research in Developmental Disabilities, Staten Island, NY.

^* To whom correspondence should be addressed. E-mail: scraft{at}u.washington.edu.

ABSTRACT

Background: Reduced brain insulin signaling and lowCSF-to-plasma insulin ratios have been observed in patientswith Alzheimer disease (AD). Furthermore, intracerebroventricularor IV insulin administration improve memory, alter evoked potentials,and modulate neurotransmitters, possibly by augmenting low brainlevels. After intranasal administration, insulin-like peptidesfollow extracellular pathways to the brain within 15 minutes.

Objective:We tested the hypothesis that daily intranasal insulin treatmentwould facilitate cognition in patients with early AD or itsprodrome, amnestic mild cognitive impairment (MCI). The proportionof verbal information retained after a delay period was theplanned primary outcome measure. Secondary outcome measuresincluded attention, caregiver rating of functional status, andplasma levels of insulin, glucose, ${beta}$ -amyloid, and cortisol.

Methods:Twenty-five participants were randomly assigned to receive eitherplacebo (n = 12) or 20 IU BID intranasal insulin treatment (n= 13) using an electronic atomizer, and 24 participants completedthe study. Participants, caregivers, and all clinical evaluatorswere blinded to treatment assignment. Cognitive measures andblood were obtained at baseline and after 21 days of treatment.

Results:Fasting plasma glucose and insulin were unchanged with treatment.The insulin-treated group retained more verbal information aftera delay compared with the placebo-assigned group (p = 0.0374).Insulin-treated subjects also showed improved attention (p =0.0108) and functional status (p = 0.0410). Insulin treatmentraised fasting plasma concentrations of the short form of the ${beta}$ -amyloid peptide (A ${beta}$ 40; p = 0.0471) without affecting the longerisoform (A ${beta}$ 42), resulting in an increased A ${beta}$ 40/42 ratio (p = 0.0207).

Conclusions:The results of this pilot study support further investigationof the benefits of intranasal insulin for patients with Alzheimerdisease, and suggest that intranasal peptide administrationmay be a novel approach to the treatment of neurodegenerativedisorders.

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