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Does Cognitive Stimulation Boost Effects of Neuropharmacology in Alzheimers

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Sandra Bond Chapman, PhD Audette Rackley,MS. Executive Director, Center for ... 2200 Mockingbird. Dallas, Texas 75235. 214.905.3007. Centerforbrainhealth.org ... – PowerPoint PPT presentation

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Title: Does Cognitive Stimulation Boost Effects of Neuropharmacology in Alzheimers


1
Does Cognitive Stimulation Boost Effects of
Neuropharmacology in Alzheimers?
Sandra Bond Chapman, PhD Audette Rackley,MS
Executive Director, Center for BrainHealth
Cognitive-Communication Specialist Professor,
Behavioral and Brain Science UTD Center for
BrainHealth Dee Wyly Distinguished Chair in Brain
Health 214.905.3007 This research was
supported by a grant from Pfizer, Inc. and Eisai,
Inc.
2
Objectives
  • Discuss approaches to mitigate loss of function
    in AD
  • Report findings of a randomized study in early
    stage AD
  • Explanation of findings and extension of work
  • Present implications for clinical practice

3
3 Approaches to Treatment in AD
  • Brain dysfunction Neurotransmitter deficit with
    Acetylcholinesterase inhibitors
  • Direct cognitive intervention to improve or
    maintain function
  • Caregiver training to reduce burden

4
1. Acetylcholinersterase Inhibitor Aricept
  • Well tolerated and easy to administer
  • Higher mean level of performance in cognitive and
    global function over placebo
  • Extended long-term potentiation decay times in
    hippocampus and neocortex in animal studies
  • (Rogers et al., 1998 Barnes et al., 2000)

5
One serious contender contributing to loss of
cognitive function in AD
  • Loss of basal forebrain cholinergic neurons in
    early stages of AD
  • Associated with decrease of choline-acetyltransfer
    ase
  • Cholinergic dysfunction plays an important role
    in memory loss in Alzheimers
  • Goal is to increase the acetycholine at synapse

6
2. Direct Cognitive Intervention
  • Improved cognitive functioning
  • Active Cognitive Stimulation
  • (Quayhagen et al., 1995)
  • Enhanced communication
  • Memory Wallets
  • (Bourgeois and Mason, 1996)
  • Long term maintenance of cognitive abilities
  • Exercise Stimulation
  • (Arkin 2001)
  • Improved retention of names of common objects,
    face-name and object-location associations
  • Spaced-Retrieval Interventions
  • (Camp et al., , 1990, 1993, 1996)

7
3. Caregiver Training
  • Increased use of facilitation strategies
  • Improved communication satisfaction
  • Increased knowledge
  • Altered caregiver attitudes
  • (Ripich, 1994 Ripich et al, 1995)

8
Expanding on Previous Studies
  • Small sample size (n lt10)
  • Few control groups
  • Not randomly assigned to conditions
  • Patients poorly characterized
  • Responses are time limited and task specific

9
Defining Effective Treatment in a Progressive
Brain Disease
  • Prevent premature loss of abilities
  • Delay the progression of the disease
  • Decrease cost to patient and family
  • Decrease cost to society
  • Improve quality of life for patient and care
    partner
  • Reveal a positive functional impact

10
A Randomized StudyEffects of
Cognitive-Communication Stimulation for
Alzheimers Disease Patients Treated with
DonepezilSandra Chapman, Myron Weiner, Audette
Rackley, Linda Hynan, Jennifer ZientzJournal
of Speech. Language, and Hearing Research,47,
1149-1163
11
Question Does cognitive-communication
intervention plus Aricept/ Donepezil impact
outcomes?
  • We hypothesized that Donepezil paired with
    cognitive-communication stimulation would show
    benefit in 5 domains
  • Relevance of verbalization
  • Performance of functional abilities
  • Emotional symptoms of irritability and apathy
  • Quality of life
  • Overall global function

12
Study Parameters
  • Random assignment
  • Intervention Group
  • (Aricept cognitive intervention)
  • Non-Intervention Group
  • (Aricept only)
  • Evaluation administration
  • Baseline (pre-test)
  • 4 months (post test)
  • 8 and 12 months (follow-up tests)

13
Subject Characteristics
  • Complete workup to indicate a diagnosis of
    probable Alzheimers disease
  • Taking Aricept for at least 3 months
  • MMSE of 14 or above
  • Involvement of family caregiver
  • Agreement to participate 1 year

14
Subject Characteristics
  • Acknowledgement of memory loss
  • Diagnosis conveyed to patient
  • Ability to converse
  • Ability to read enough to follow written handouts
  • Ability to sit for a period of 1 hour without
    problematic agitation
  • English speaking
  • Exclusion Criteria no head trauma, other
    neurologic disease, or psychiatric disease

15
Group Characteristics
16
Patient Measures
17
Intervention Program
  • Group Composition
  • Six individuals with AD
  • Project Coordinator (SLP)
  • 3 masters level students
  • Intervention (8 weekly sessions for 1 1/2 hours)
  • Relevant verbal content
  • Functional activities
  • Quality of life

18
Program Content
19
Analyses
  • I. All continuous variables were analyzed using
    ANCOVA
  • Baseline variable was used as the covariate
  • Between group factor was the group intervention
    vs. non-intervention
  • Repeated measurements were the measures at 4, 8
    and 12 months
  • II. Change scores (12-month measurements minus
    baseline) for continuous variables were
    calculated
  • One-sample t tests were conducted to determine if
    the change for each group was significantly
    different from zero

20
Relevant Verbal Content
  • No significant difference for group, time, and
    interaction of group and time.
  • However, average change from baseline showed
  • a nonsig change in Intervention group
  • A sig decline in Donepezil-only

21
Functional Abilities
  • No sig difference for group, time, and
    interaction
  • Both showed decline from baseline, but Donepezil
    plus stimulation declined less

22
Quality of Life IrritabilityNote A decrease
in NPI score signifies a positive change or
decrease in symptomatology
  • A significant interaction of group by time for
    rating severity of behavior in individual

23
Overall Global Function
24
Interpreting Findings
  • The most important findings from this study were
    positive outcomes when Donepezil paired with
    cognitive-communication stimulation
  • Relevant discourse
  • Functional abilities
  • Emotional Well-being
  • Global Function

25
Does Cognitive Stimulation Boost Effects of
Neuropharmacology in Alzheimers?
  • The intervention group showed slower rate of
    decline over time in discourse, functional
    abilities and psychiatric behaviors
  • These effects were found with relatively
    short-term intervention 8 sessions/12 hours.
  • The intervention showed effects that extended
    beyond the treatment and beyond the specific
    program

26
Generalized BenefitsInterprete with Caution
  • The intervention showed effects that
  • Extended beyond the treatment and
  • Generalized to areas outside the specific tasks
    of intervention, e.g.,
  • Emotional symptoms irritability, apathy
  • Functional Abilities
  • Caution Effects were modest and did not improve
    memory function

27
What is mechanism of cholinesterase inhibitor to
promote brain health?
  • In other studies, treatment with Cholinesterase
    Inhibitor revealed
  • Slower rate of decline in cerebral glucose
    metabolism on PET
  • Increased cerebral glucose metabolism in right
    frontal region
  • Positive correlation between changes in glucose
    metabolism and patients with higher doses
  • Cholinesterase Inhibitors increases cerebral
    metabolism and is assoc. with cognitive benefits
    in mild AD over 12 month period
  • Stefanova et al, Jr. of Neural Transmission, 2006

28
What is mechanism of cholinesterase inhibitors
to promote brain health?
  • Cognitive effects of treatment thought to be
    mediated by improvement in neuronal transmission
  • Increase cortical metabolic response to
    activation

29
How Could Cognitive Stimulation Boost Effects of
Neuropharmacology in Alzheimers?
  • Drug increases brain metabolism that could
    provide environment to enhance plasticity even in
    progressive brain disease.
  • Cognitive stimulation may be necessary to provide
    the necessary activation to maintain more intact
    and supporting brain networks.

30
Clinical Implications of Study
  • Intervention consisted of
  • Meaningful conversation as opposed to drills
  • Focus on preserved abilities rather than
    weaknesses
  • Weekly homework assignments to promote carryover
    and increase involvement.

31
Early Reframing of functionality may have Later
Benefits
  • Unexpectedly, no differences were present at 4
    months (end of active stimulation)
  • However, benefits were measured at 8 months after
    the active stimulation program ended.
  • The intervention showed effects that extended
    beyond the treatment and beyond the specific
    program

32
Factors that might enhance outcome
  • Increase the dose (frequency of treatment) and
    evaluate response
  • Add more Individualized treatment
  • More integrated caregiver-patient training
  • Intervene earlier
  • Ecological validation of training transfer

33
Limitations
  • Participants were not blinded to group
    assignments
  • Study may have attracted a select group of
    participants who had high hopes of benefit
  • Not possible to always blind test administrators
    to group assignments.

34
Using Functional Brain Imagingto study changes
in AD
  • Reveal how brain is working when thinking in AD
  • Indicate appropriate level of stimulation to
    engage brain
  • Measure response to treatments

35
  • Evidence suggests Cognitive Stimulation could
    boost effects of neuropharmacology in
    Alzheimers.
  • Dr. Sandra Bond Chapman
  • Executive Director, Center for BrainHealth
  • 2200 Mockingbird
  • Dallas, Texas 75235
  • 214.905.3007
  • Centerforbrainhealth.org
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