Title: Alzheimer
1Alzheimers Disease and Amyloid ß-peptide
polymerization Structures and Strategies
Karolinska Institutet, KASPAC
2Outline of the talk
A. Amyloid B. Amyloid ß-peptide (Aß) as a target
in Alzheimers disease C. Inhibition of Aß
polymerization D. A novel screen for Aß
polymerization inhibitors
3Amyloid
- The term amyloid was first used in the 1850s to
describe deposits that were stained with iodine - Thought to be composed of starch
- Main component is protein
- Thought to be amorphous
- 1920s Stains with Congo red gt
- ordered structure
4Congo Red stains amyloid
- Stain tissue with Congo red
- View under polarized light
- Turn polarizer red becomes green and vice versa
- This phenomena is called birefringence
- Indicates an ordered structure
Plaque core stained with Congo Red
5Amyloid is composed of protein fibrils
- Amyloid fibrils
- can be observed by electron microscopy (EM)
- are 8nm wide
- can be isolated from tissue
- can form from synthetic peptides
- are resistant to proteolysis
EM by Johan Thyberg, KI
6Amyloid fibrils show a cross-ß fibre diffraction
pattern
Peptide chain
4.8Å
Fibril direction
7Amyloid proteins
- Protein Disease .
- Amyloid b-peptide Alzheimers disease
- Gelsolin Finnish-type fam. amyloidosis
- Islet amyloid polypep. Type II diabetes
- Immunoglobulin l.c. Light-chain amyloidosis
- Lysozyme Heriditary syst. amyloidosis
- Medin Aortic medial amyloid
- Serum amyloid A Secondary syst. amyloidosis
- Transthyretin Senile syst. amyloidosis
- Fam. Amyloid polyneuropathy
8The amyloid plaque in Alzheimers disease
- Core of Amyloid b-peptide (arrows)
- Neurofibrillary tangles (Tau)
- Dystrophic neurites
- Activated microglia and astrocytes
D. Selkoe, Nature, 399, A23-31 (1999)
9The Amyloid b-peptide, Ab
Lumen/ extracellular
1.
- Derived from the b-amyloid precursor protein
(APP, 700 residues transmembrane protein) - First cleavage by BACE
- Second cleavage by ?-secretase (protein complex
containing presenilin) - 40-42 residue peptide
- Especially the longer variant (Aß42) has a strong
tendency to polymerize - Identified in1984 (Glenner Wong)
- Main component of the AD-plaque
Membrane
Cytosol
2.
Cytosol
10Amyloid plaque cores
Are composed of fibrils formed from the amyloid
ß-peptide (Aß)
A
Several lines of evidence indicate that the
polymerization process could be a drug target in
Alzheimers disease
11Aß is of importance in AD
- Aß plaques are always present in AD brain
- Brain Aß correlates with degree of dementia
- Aß becomes neurotoxic upon polymerization
- All familial AD mutations gt elevated levels of
Aß42 - Extra copy of APP (Downs syndrome) gt early
onset AD - Transgenic mice overexpressing Aß develop
AD-like - lesions and show impaired memory
12The amyloid cascade
FAD mutations APP, PS12, other
Aß-42
13Aß polymerization
Monomer Di/Trimer Oligomer Protofibril
Fibril
14Toxic Ab species
- Ab-fibrils are toxic
- Lorenzo et al. PNAS 91 12243-12247 (1994)
- Protofibrils are toxic
- C. Nilsberth et al. Nat. Neurosci. 4 887-893
(2001)
- Diffusable aggregates are toxic
- M. P. Lambert et al. PNAS 95 6448-6453 (1998)
15Amyloid ß-peptide as a target in AD Aß becomes
neurotoxic upon polymerizationPossible regimes
for pharmacological intervention
- Inhibit production of Aß ß- and ?-secretase
inhibitors - Increase clearance Vaccination
- Inhibit Aß aggregation Small Aß-binding
compounds capable of interfering with Aß-Aß
interactions
16Anti-amyloid strategies
- b-secretase
- No severe phenotype in knock-out mice
- - Difficult to develop inhibtors due to large
active site - g-secretase
- Several examples of efficient inhibitors
- Many different substrates besides APP i.e. Notch
- - Knock-out lethal in mice
- Vaccination
- Vaccination can reduce amyloid burden
- Clinical trials stopped due to side effects
- Aggregation inhibitors
- Aß aggregation has no physiological function
17Crystal structure of BACE with inhibitor
Eight residue transition state inhibitor Ki 1.6
nM Hong Science 2000
KO mice viable - Large binding pocket,
difficult to find good inhibitors
18?-Secretase
- Is composed of (at least) four transmembrane
proteins - Mediates the final catalytic step in the
processing of APP (C99) into Aß - Is a potential drug target in Alzheimers
disease - Has other substrates, e.g. Notch
Specific inhibition of APP processing is
necessary!
19Nonsteroidal anti-inflammatory drugs (NSAIDs)
- There is an inflammatory component in AD
- Large studies have shown that some none steroid
anti-inflammatory drugs (NSAIDs) decrease the
incidence of AD - The mechanism behind this effect is unknown, but
might be due to lower levels of Aß-42 - Ibuprofen-treated APP mice show reduced Aß-42 in
brain - Clinical trials ongoing
S. WEGGEN et al. Nature 414, 212 - 216 (2001)
20?-Secretase inhibitors in Clinical trials
- Ibuprofen in phase III
- Flurizan in Phase III
- Selective amyloid lowering agent
- Reduced insoluble Aß in Tg mice and improved
memory - Well tolerated
- May decrease cognitive decline
21Antibodies against Aß slow cognitive decline in
Alzheimers disease
30 AD patients were injected with aggregated
Aß-42 20 of them generated antibodies Patients
who generated antibodies showed less decline of
cognitive functions and activities of daily
living Trial stopped since several patients got
meningoencephalitis C. Hock et al. Neuron 38,
547-554 (2003) Clears amyloid Patients still
produce antibodies
New trials ongoing
22Aß immunotherapy for treatment of AD
- There are several trials ongoing
- Both passive and active immunization are
evaluated - Passive immunization might increase cerebral
amyloid angiopathy (CAA) - The antigen can be full length Aß or short
fragments - The peptide can be conjugated to a carrier
protein or micro-beads
23Inhibition of Aß polymerization
- Aß polymerization is thought to be
nucleation-dependent - Several different Aß species may be toxic
- Inhibit as early as possible
- No high resolution structure
24An important region for Aß-Aß bindingDAEFRHDSGY
EVHHQKLVFF AEDVGSNKGA IIGLMVGGVV IA
Tjernberg et al. J. Biol. Chem. 2718545-8
25 Aß 16-20 (KLVFF) is important for Aß-Aß binding
Truncated variants of the central binding
decapeptide were synthesized and incubated with
radio-labeled Aß. Peptides containing the KLVFF
sequence were found to bind Aß.
Biacore study The peptide AcKLVFFAAC was
immobilized on the sensorchip and Ab was
injected. Lower trace Cys
26Aß fibril formation can be inhibited by short
peptides
Synthetic Aß was incubated in buffer in the
absence (A) or in the presence (B) of a short
peptide (QKLVFFA). Tjernberg et al. J. Biol.
Chem. 2718545-8
27Pentapeptides composed of D-amino acids can
inhibit Aß fibril formation
Pentapeptides were synthesized on a membrane and
incubated w. radio-labelled KLVFF
Tjernberg et al. J. Biol. Chem. 27212601-5.
28Short Aß-fibril inhibitors have effect in vivo
- iAß5 blocks Aß-42 neurotoxicity in cell culture
and fibril formation in rat brain - iAß5 dissasembles fibrillar deposits in rat brain
and prevents/reverses neuronal shrinkage - E.M. Sigurdsson et al. Nat. Med. 4822-826 and J.
Neuropathol. Exp. Neurol. 5911-17 - Modified molecule crosses BBB
Clinical trials Phase I gt no toxicity
29Curcumin, a small organic compound can affect
amyloid in vivo
Curcumin crosses the BBB and binds to plaques
Yang, et al. J. Biol. Chem. (2005)2805892-5901
30Curcumin suppresses amyloid accumulation in aged
APP transgenic mice
Tg2576 mice were placed on chow supplemented w.
curcumin at 17 months of age and brains were
removed after 22 months A-C control D-F
Curcumin
G. Image analysis of plaque burden H. ELISA
measurement of guanidine- soluble Aß
Yang, F. et al. J. Biol. Chem. 20052805892-5901
31Curcumin inhibits formation of Ab oligomers
Yang, F. et al. J. Biol. Chem. 20052805892-5901
32A small organic Aß-polymerization inhibitor in
clinical trials
- Glycosaminoglycans (GAGs) bind to Aß, promote
fibril formation and are present in amyloid
deposits - Low molecular weight GAG mimetics bind to Ab and
inhibits fibril formation - APP tg mice treated with 3-amino-1-propanesulfonic
acid (3APS) show reduced amyloid burden - Phase II 3APS is safe, tolerated and reduces CSF
Aß - Phase III studies ongoing
P. Aisen et al. Neurology 2006 671757-1763
33Assays for Aß polymerization
ThT-binding is the most frequently used assay
34The ThT assay
A
35The ThT assay
36CD and FCS
Wanted A simple, rapid and sensitive assay
37Ab oligomers can be detected by specific antibody
A-B Single neuron labeled with oligomerspecific
antibody Fluorescent (A) or peroxidase-conjugated
(B) secondary antibody C Dot blot analysis of
soluble Ab in AD and control brain.
38HTS-Assay for Aß polymerization inhibitors
39Constrained peptides containing the HQKLVFFAED
motif form fibrils
40Amyloid fibril formation from a tetrapeptide, KFFE
EM
Congo Red
Model of a beta-sheet composed of four
antiparallel KFFE peptides
Tjernberg, L. et al. J. Biol. Chem.
200227743243-43246
41The turn-motif is of importance for the secondary
structure
CD-spectra
- KFFEYNGKKFFE gt ß-sheet
- KFFEAAAKKFFE gt random
42The peptide KFFEYNGKKFFE forms a ß-hairpin in
solution
B. Persson
Molecular modeling in agreement with NMR data
43HTS-Assay for Aß polymerization inhibitors
44FRET
F
lmax Donor
lmax Acceptor
l
Far away no transfer
45Urea denaturation of inhibitor probes
The acceptor and donor fluorescence was measured
at different urea concentrations and the ratio
calculated
These probes could be useful for screening!
46Curcumin gives dose dependent changes in
fluorescence spectrum
The probe was incubated 2h in the presence of 0,
1, 3 or 10 uM curcumin
47The probe shows decreased acceptor fluorescence
in the presence of curcumin
The probe (0.5 uM) was incubated in the presence
of curcumin (0, 0.25, 0.5, 0.75, 1.0, 1.5 or 2uM)
The inhibitor interacts with the probe
48Curcumin does not absorb the light emitted from
the acceptor
A solution of curcumin (2.5 uM) was placed in the
emission path, probe concentration 0.5 uM.
49CD-spectroscopy The probe shows decreased ß-sheet
in the presence of curcumin
The probe (10 µM) was incubated in the absence
(blue trace) or in the presence (green trace, t
0, red trace, t 30 min) of 36 µM curcumin
50SEC - fluorescence detection
The probe was dissolved in 50 acetonitrile and
injected onto a SEC column. The signal at 520 nm
was recorded (acceptor emission).
Broken line direct excitation of acceptor (350
nm) Full line excitation of donor (290 nm)
Conclusion The probe is a monomer and shows
intramolecular FRET
51Acknowledgements
- Karolinska Institutet
- Lars Terenius Rudolf Rigler Johan Thyberg
- The Picower Institute for Medical Research
- David Callaway
- Swedish University of Agricultural Sciences
- Jan Johansson
- Dainippon Sumitomo Pharma
52Conclusions
- Amyloid is bad
- The amyloid b-peptide is important in AD
- The amyloid b-peptide can be a therapeutic
target in AD - There are drugs aimed at lowering Ab-levels in
clinical trials - Still more to learn