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Memantine restores impaired synaptic plasticity by reducing synaptic noise
s242
Poster
ANTI-AMYLOIDOGENIC VITRO STUDIES
111051
ACTIVITY
OF TETRACYCLINES:
IN
Presentation:
WITH ALZHEIMER’S
Alzheimer’s
of olanzapine
Aims A multicenter
tangles and cortical
atrophy.
deposited in cortical
Beta-amyloid
and meningeal
characterized
(bA)
is the major component
of bA peptide
in AD
genetic,
studies pointing
of bA
aggregates
approach
anthracycline
numerous
with
or their
to the disesase.
chemical
anti-tumoral
the possibility
analogies
the antibiotic derivatives
activity,
inhibited
with anthracyclines,
tetracycline,
(i.e. doxycycline)
formed
fluorescent
co-incubated formation. trypsin
with
T
digestion.
with a well-known
clinical
microscopy
not
profile,
tetracycline
in dose-dependent
only
including
the
fib&.
amyloid
Alzheimer‘s
years)
study was conducted
in treating psychotic
with
disease. Methods
dementia
study entered
(dose range:
Agifation/A,~gression, as the primary olanzapine.
Elderly
(n= 137) who
an open-label 5,
patients
mensure
(Core
SCOTCSimproved
p<.oOl),
Total
(mean,
p<.OOl).
included There
changed.
double-blind
which
change
they received
in the sum of the
wtal
(26W),
treatment
on the Core
scores
Total
improved
Simpson Angw
with
(meaw7.55:
injury
symptoms
wow
in patient
ECGs,
including symptom!,
and rash (22%).
generally
from
were not
Treatment-emergent
(2X%),
is an effective,
significantly
and AIMS
changes occurred
sign or in weight.
accidental
war used
treatment
p<.OOl), and IO of the 13 Owupational Disruptivmrss (mean,
Akathisia
for psychotic
Alzheimer’y
Following
SD=23.72;
including
No significant
nor in any
somnolence
long-term
(mean age: 83.1
a 6-week
during
Results
significantly
p=.C02).
data suggest that olanzapine
patients with
aaaociatrd
home patients
Mean
Total).
17.85;
Barner
haaehne (mean, 0.22; SD=O.SO; interval,
and safety
completed
15 mglday).
item score5 of the NPVNH,
significantly
successfully
10, or
individual
QTc
nursing
efficacy
disturbances
Delusions, and Hallucinations items of the NPVNH
efficacy
SD=3.24;
long-term
and behaworal
phase of up to 18 weeks
SD=8.53: 2.84;
to determine
symptoms
Beth E. Juliur. Peter D.
Conclusion?
safe, and well-tolerated
and behaworal
disturbances
in elderly
dementw
and quantified doxycycline the amyloid
amyloid
fibrils
beta-amylold
in CNS,
fibrils
nmnner
The rewlts
activity
We investi-
and
of beta l-42
inhibited
of
whose
depoaits and ha\
by electron
the pre-formed
capacity
using beta l-42
Beta l-42
also the resistance
Tetracyclines
but also diaawzmbled
Based on some
in the CNS.
in AD amyloid
Both
aggre-
profile.
formation.
assay.
an
barrier pasaagr
and doxycycline
represented
for amyloid
reduduced
The drugs attenuated
formation
of amyloid
toxicological
distribution
of tetracycline
binding
the peptide
is a potential
iodo-doxorubucin,
the formation
a safer
in vitro were analyzed
thioflavine with
that
and low blood-brain
have a favorable capacity
peptide, this peptide is highly
spontaneously
Thus. prevention
we tested the anti-amyloidogenic
a molecule
been proposed as a seed molecule
by
toxicity
of AD.
with
olanzapine
and neuropathological
once formed,
have found
of
is an early event
of a direct we of this drug m AD therapy.
gated the anti-amyloidogenic synthetic
and l-42,
biochemical
elimination
We
gates in vitro and in viva. The intrmsic has inhibited
l-40
to a causal role of bA in the pathogenesis
the formation therapeutic
are now
of SP and i\
blood vessels of the AD brain. The formation
bA deposits, which are insoluble fibrils and there
by senile plaques (SP)
II
DEMENTIA
Jarnie S. Street, W. Scott Clurk. Eli Lilly and Cornpam: Feldmun, Deborah L. Kadam, Alan Breier
is neuropathologically
Studies
LONG-TERM EFFICACY OF OLANZAPINE IN THE CONTROL 111071 OF PSYCHOTIC AND BEHAVlORAL SYMPTOMS IN PATIENTS
Gianluigi Forlnm. Laura Colombo, Lam Girola, lnsr di Ricerchr Farrnacologiche Mano Negri, Milano Italy; Fabririo Taglinvini, lnst Nazionalr Neurologico Carlo Bwtu, Milano Italy; Mm-w Salmona, lnst di Ricerche Farmacologichr Mario Negri. Milano ltul, disease (AD)
IIrug
MEMANTINE RESTORES IMPAIRED BY REDUCING SYNAPTIC NOISE
to
SYNAPTIC
PLASTICITY
aggregate?
indicate that drug\
are potentially
useful
for AD therapy. In the accompanying wxcral
MEMANTINE 111061 MODELS AT
PROVIDES NEUROPROTECTION IN ANIMAL THERAPEUTICALLY RELEVANT DOSES
models
abstracts we have shown that memantine
of
lneuroprotectlve
chronic
agent in dementia.
symptomatological contrast
with
neurodegenerative
effects
the effects
expected
function
of these receptors
indicate that memantine
of NMDA
disease.
has been suggested to be involved Hence,
NMDA
disease progression. actwity
receptor
However,
can be achwed
therapeutically therapeutic
relevant dose in animals
either
NMDA
relevent.
receptor
to the brain (i.c.v.)
for cognition.
Memantine
animals ally.
doses of NMDA
In the wne
quinolinic
acid
minipump
previously
microinjection NBM
infused
while
to the clinical
acid (3.NP)
different
nucleus
protection
by Memantine.
factors contributing
role m the neurodegeneration
NMDA
are preclinical
basah\
of Meynert
lesion
receptors
(NBM
of this structure
qyntheaising
2.8 @kg. toxin
might
to the neuronill insult and memantine diseae
studies
provided
the high
kinetics
&es
activation
propertie?
synaptic
NMDA
and MgZt
increased synaptic cholinesterase
where energy deficit5
inhibitors.
Again
synaptic noise.
receptor
data provide
antagonist kinetics
upport
for our
supporting
it’s promising
the physiological
in blocking
isn t quite
to act like a somewhat
noise. Memantine
strategy to treat Al/heimrr’s
by lowering noise.
slow unblocking
in determining allow
is more effective
memantine
Mg’ ’ under condition,
These
(I OpM)
and associated rapid strongly voltage-dependent
as its voltage-dependency
allow
in (25
of memantine
also be induced
increasing
uncompetitive
are important
memantine
function learning
by NMDA
concentration
could
thereby
voltage-dependency.
receptors but memantine
receptor The%
affinity
of memantine
Both
preclinical
dose\ of NMDA
reversed this deficit by reducing
that the moderate affinity
profile.
recent
their combined
of
tonic low level NMDA
so pronounced
as Mg”.
more potent surrogate for
cause tonic relief
shows no negative
thera-
activation
’block
of Mg’
interactions
and
with reversible
use as a potential.
rynergiatic
disease.
enzyme,
given i.p. before NMDA
with an EDSOof
blocking
a decrease in chohne
addition-
model,
wzem to
(2.5 and 5 mg/kp i.p.). Similarly,
slices was impaired
was unable to restore LTP due to its extremely
hypothesis peutic
Memantme
m hippocampal
completely
and far less pronounced
S.C. with
In all cases, no side-effects
of Allheimer’s
acid alone
for learning and affected in
of mitochondrial
NMDA
weeks
was seen in the cortex of
NMDA-induced
injection
doses. Hence,
to slow down the progression
quinolinic
Similarly,
in target cortical areas. Memantine
was inhiblted
at the neuroprotective
with
decrease in levels of the acetylcholine
by a direct
two
those infused in parallel
use of’Memantine
in rats).
for
a second pump delivered
acid but not in those recewing
produced a clear-cut
lesion produced
was infused
while
such as the cholinergic
caused a considerable
(I to IO bM)
dizocilpine
Alzheimer’s
choline acetyltransferase
memantme
may
as the normal
synaptic noise. Thus, passive avoidance
(I FM). Deficit? in LTP in hippocampal Mg* ’ concentration (to IOIJ.M) and
of this agent, the
the task normally.
magnocellularls
A
in rats maximum
in structures known to be impofiant
diseae
antagonists.
This
antagonist
of low, non-toxic
in
use as a
shows clear positive
However.
and this effect was reversed by a therapeutically-relevant
Hence,
of the density of ACh terminals)
treated with quinolinic
baaalla
down
activity
on neurodegeneration
nucleus
slow
p,M for Memantine).
Animals
relevance
should
To test neuroprotective
agonist
were able to acquire
Of particular
relevant
deficits in the T-maze
uptake sites (an indicator
Memantine)
(LTP)
it’s
is also able to restore normal physiological
by systemic administration
long term potentmtion
IS one that leads to plasma levels close to the
via an ALZET
saline or Memantine.
showed clear learning
(like
of Alrheimer’s
one of the major concerns is, whether neuroprotective
range in humans (0.2-1.0
endogenous directly
antagonista
at therapeutically
5 mg/kg is therapeutically
m the pathomechanism
al\o
patients.
receptor
mglkg i.p.) and this deficit was reversed memantine Glutamate
is neuroprotective
supporting
memantine
in demented
for a NMDA
ia essential
receptors by reducing
rats was impaired
However,
on cognition
findings
diseases
Similarly.
3-nitropropionic
12 MONTH DECLINE IN COGNITIVE AND DAILY FUNCTION 11109(IN PATIENTS WITH MILD-TO-MODERATE ALZHEIMER’S DISEASE: STUDIES
were observed
be a link
TWO
RANDOMIZED,
PLACEBO-CONTROLLED
between
should be expected
that glutamate
plays a
in this disorder. Background: cognitive of decline
dwase
and activities
in these domains
Objectives: data from
Alzheimer’s
function
(AD)
is characterized
of daily living (ADL).
is ersential
to the evaluation
To measure the rate? of change in cognitive two
double-blind.
12.month
AD
placebo-controlled
clinlcal
trial‘;.
ctudia
by a progressive
Characterizing
Methods:
of sabelurole
decline
long-term
of treatment
and functional Two
12.month,
were
undertaken
in
rates
intervention. ability,
using
randomixd. in wbjcct?
Poster
ANTI-AMYLOIDOGENIC VITRO STUDIES
111051
ACTIVITY
OF TETRACYCLINES:
IN
Presentation:
WITH ALZHEIMER’S
Alzheimer’s
of olanzapine
Aims A multicenter
tangles and cortical
atrophy.
deposited in cortical
Beta-amyloid
and meningeal
characterized
(bA)
is the major component
of bA peptide
in AD
genetic,
studies pointing
of bA
aggregates
approach
anthracycline
numerous
with
or their
to the disesase.
chemical
anti-tumoral
the possibility
analogies
the antibiotic derivatives
activity,
inhibited
with anthracyclines,
tetracycline,
(i.e. doxycycline)
formed
fluorescent
co-incubated formation. trypsin
with
T
digestion.
with a well-known
clinical
microscopy
not
profile,
tetracycline
in dose-dependent
only
including
the
fib&.
amyloid
Alzheimer‘s
years)
study was conducted
in treating psychotic
with
disease. Methods
dementia
study entered
(dose range:
Agifation/A,~gression, as the primary olanzapine.
Elderly
(n= 137) who
an open-label 5,
patients
mensure
(Core
SCOTCSimproved
p<.oOl),
Total
(mean,
p<.OOl).
included There
changed.
double-blind
which
change
they received
in the sum of the
wtal
(26W),
treatment
on the Core
scores
Total
improved
Simpson Angw
with
(meaw7.55:
injury
symptoms
wow
in patient
ECGs,
including symptom!,
and rash (22%).
generally
from
were not
Treatment-emergent
(2X%),
is an effective,
significantly
and AIMS
changes occurred
sign or in weight.
accidental
war used
treatment
p<.OOl), and IO of the 13 Owupational Disruptivmrss (mean,
Akathisia
for psychotic
Alzheimer’y
Following
SD=23.72;
including
No significant
nor in any
somnolence
long-term
(mean age: 83.1
a 6-week
during
Results
significantly
p=.C02).
data suggest that olanzapine
patients with
aaaociatrd
home patients
Mean
Total).
17.85;
Barner
haaehne (mean, 0.22; SD=O.SO; interval,
and safety
completed
15 mglday).
item score5 of the NPVNH,
significantly
successfully
10, or
individual
QTc
nursing
efficacy
disturbances
Delusions, and Hallucinations items of the NPVNH
efficacy
SD=3.24;
long-term
and behaworal
phase of up to 18 weeks
SD=8.53: 2.84;
to determine
symptoms
Beth E. Juliur. Peter D.
Conclusion?
safe, and well-tolerated
and behaworal
disturbances
in elderly
dementw
and quantified doxycycline the amyloid
amyloid
fibrils
beta-amylold
in CNS,
fibrils
nmnner
The rewlts
activity
We investi-
and
of beta l-42
inhibited
of
whose
depoaits and ha\
by electron
the pre-formed
capacity
using beta l-42
Beta l-42
also the resistance
Tetracyclines
but also diaawzmbled
Based on some
in the CNS.
in AD amyloid
Both
aggre-
profile.
formation.
assay.
an
barrier pasaagr
and doxycycline
represented
for amyloid
reduduced
The drugs attenuated
formation
of amyloid
toxicological
distribution
of tetracycline
binding
the peptide
is a potential
iodo-doxorubucin,
the formation
a safer
in vitro were analyzed
thioflavine with
that
and low blood-brain
have a favorable capacity
peptide, this peptide is highly
spontaneously
Thus. prevention
we tested the anti-amyloidogenic
a molecule
been proposed as a seed molecule
by
toxicity
of AD.
with
olanzapine
and neuropathological
once formed,
have found
of
is an early event
of a direct we of this drug m AD therapy.
gated the anti-amyloidogenic synthetic
and l-42,
biochemical
elimination
We
gates in vitro and in viva. The intrmsic has inhibited
l-40
to a causal role of bA in the pathogenesis
the formation therapeutic
are now
of SP and i\
blood vessels of the AD brain. The formation
bA deposits, which are insoluble fibrils and there
by senile plaques (SP)
II
DEMENTIA
Jarnie S. Street, W. Scott Clurk. Eli Lilly and Cornpam: Feldmun, Deborah L. Kadam, Alan Breier
is neuropathologically
Studies
LONG-TERM EFFICACY OF OLANZAPINE IN THE CONTROL 111071 OF PSYCHOTIC AND BEHAVlORAL SYMPTOMS IN PATIENTS
Gianluigi Forlnm. Laura Colombo, Lam Girola, lnsr di Ricerchr Farrnacologiche Mano Negri, Milano Italy; Fabririo Taglinvini, lnst Nazionalr Neurologico Carlo Bwtu, Milano Italy; Mm-w Salmona, lnst di Ricerche Farmacologichr Mario Negri. Milano ltul, disease (AD)
IIrug
MEMANTINE RESTORES IMPAIRED BY REDUCING SYNAPTIC NOISE
to
SYNAPTIC
PLASTICITY
aggregate?
indicate that drug\
are potentially
useful
for AD therapy. In the accompanying wxcral
MEMANTINE 111061 MODELS AT
PROVIDES NEUROPROTECTION IN ANIMAL THERAPEUTICALLY RELEVANT DOSES
models
abstracts we have shown that memantine
of
lneuroprotectlve
chronic
agent in dementia.
symptomatological contrast
with
neurodegenerative
effects
the effects
expected
function
of these receptors
indicate that memantine
of NMDA
disease.
has been suggested to be involved Hence,
NMDA
disease progression. actwity
receptor
However,
can be achwed
therapeutically therapeutic
relevant dose in animals
either
NMDA
relevent.
receptor
to the brain (i.c.v.)
for cognition.
Memantine
animals ally.
doses of NMDA
In the wne
quinolinic
acid
minipump
previously
microinjection NBM
infused
while
to the clinical
acid (3.NP)
different
nucleus
protection
by Memantine.
factors contributing
role m the neurodegeneration
NMDA
are preclinical
basah\
of Meynert
lesion
receptors
(NBM
of this structure
qyntheaising
2.8 @kg. toxin
might
to the neuronill insult and memantine diseae
studies
provided
the high
kinetics
&es
activation
propertie?
synaptic
NMDA
and MgZt
increased synaptic cholinesterase
where energy deficit5
inhibitors.
Again
synaptic noise.
receptor
data provide
antagonist kinetics
upport
for our
supporting
it’s promising
the physiological
in blocking
isn t quite
to act like a somewhat
noise. Memantine
strategy to treat Al/heimrr’s
by lowering noise.
slow unblocking
in determining allow
is more effective
memantine
Mg’ ’ under condition,
These
(I OpM)
and associated rapid strongly voltage-dependent
as its voltage-dependency
allow
in (25
of memantine
also be induced
increasing
uncompetitive
are important
memantine
function learning
by NMDA
concentration
could
thereby
voltage-dependency.
receptors but memantine
receptor The%
affinity
of memantine
Both
preclinical
dose\ of NMDA
reversed this deficit by reducing
that the moderate affinity
profile.
recent
their combined
of
tonic low level NMDA
so pronounced
as Mg”.
more potent surrogate for
cause tonic relief
shows no negative
thera-
activation
’block
of Mg’
interactions
and
with reversible
use as a potential.
rynergiatic
disease.
enzyme,
given i.p. before NMDA
with an EDSOof
blocking
a decrease in chohne
addition-
model,
wzem to
(2.5 and 5 mg/kp i.p.). Similarly,
slices was impaired
was unable to restore LTP due to its extremely
hypothesis peutic
Memantme
m hippocampal
completely
and far less pronounced
S.C. with
In all cases, no side-effects
of Allheimer’s
acid alone
for learning and affected in
of mitochondrial
NMDA
weeks
was seen in the cortex of
NMDA-induced
injection
doses. Hence,
to slow down the progression
quinolinic
Similarly,
in target cortical areas. Memantine
was inhiblted
at the neuroprotective
with
decrease in levels of the acetylcholine
by a direct
two
those infused in parallel
use of’Memantine
in rats).
for
a second pump delivered
acid but not in those recewing
produced a clear-cut
lesion produced
was infused
while
such as the cholinergic
caused a considerable
(I to IO bM)
dizocilpine
Alzheimer’s
choline acetyltransferase
memantme
may
as the normal
synaptic noise. Thus, passive avoidance
(I FM). Deficit? in LTP in hippocampal Mg* ’ concentration (to IOIJ.M) and
of this agent, the
the task normally.
magnocellularls
A
in rats maximum
in structures known to be impofiant
diseae
antagonists.
This
antagonist
of low, non-toxic
in
use as a
shows clear positive
However.
and this effect was reversed by a therapeutically-relevant
Hence,
of the density of ACh terminals)
treated with quinolinic
baaalla
down
activity
on neurodegeneration
nucleus
slow
p,M for Memantine).
Animals
relevance
should
To test neuroprotective
agonist
were able to acquire
Of particular
relevant
deficits in the T-maze
uptake sites (an indicator
Memantine)
(LTP)
it’s
is also able to restore normal physiological
by systemic administration
long term potentmtion
IS one that leads to plasma levels close to the
via an ALZET
saline or Memantine.
showed clear learning
(like
of Alrheimer’s
one of the major concerns is, whether neuroprotective
range in humans (0.2-1.0
endogenous directly
antagonista
at therapeutically
5 mg/kg is therapeutically
m the pathomechanism
al\o
patients.
receptor
mglkg i.p.) and this deficit was reversed memantine Glutamate
is neuroprotective
supporting
memantine
in demented
for a NMDA
ia essential
receptors by reducing
rats was impaired
However,
on cognition
findings
diseases
Similarly.
3-nitropropionic
12 MONTH DECLINE IN COGNITIVE AND DAILY FUNCTION 11109(IN PATIENTS WITH MILD-TO-MODERATE ALZHEIMER’S DISEASE: STUDIES
were observed
be a link
TWO
RANDOMIZED,
PLACEBO-CONTROLLED
between
should be expected
that glutamate
plays a
in this disorder. Background: cognitive of decline
dwase
and activities
in these domains
Objectives: data from
Alzheimer’s
function
(AD)
is characterized
of daily living (ADL).
is ersential
to the evaluation
To measure the rate? of change in cognitive two
double-blind.
12.month
AD
placebo-controlled
clinlcal
trial‘;.
ctudia
by a progressive
Characterizing
Methods:
of sabelurole
decline
long-term
of treatment
and functional Two
12.month,
were
undertaken
in
rates
intervention. ability,
using
randomixd. in wbjcct?