Alzheimers Disease

Question 1

what is dementia?

Answer 1

an irreversible, progressive brain disease that slowly destroys memory and cognitive skills

Question 2

What may dementia affect?

Answer 2

comprehension, calculation, learning, language, judgement and potentially also personality, mood, behaviour and motivation

Question 3

what is the mean survival following AD diagnosis?

Answer 3

7 years

Question 4

What is the commonality in 80+ year olds?

Answer 4

1 in 5

Question 5

How common is AD in terms of dementias?

Answer 5

55%

Question 6

Where are signs of AD first noticed in the brain?

Answer 6

Enterohinal cortex

Question 7

Where does AD progress to from the enterohinal cortex?

Answer 7

hippocampus

Question 8

What is the enterohinal cortex a part of ?

Answer 8

the temporal lobe

Question 9

how long before symptoms appear can the neuropathology occur?

Answer 9

10-20 years

Question 10

What is the temporal lobe important for?

Answer 10

processing of semantics in speech and vision and key role in LTM

Question 11

What is the first sign of AD?

Answer 11

memory loss

Question 12

What can be seen in an MRI of an AD brain?

Answer 12

• enlargement of the ventricles
• hippocampal and cortical shrinkage
• lesions on occipital lobe (visual hallucinations)
• lesions on frontal lobe (decision making issues)

Question 13

What further issues may become apparent in severe AD?

Answer 13

gait, incontinence, motor disturbances, bedridden and long term care needed

Question 14

Where are b-amyloid plaques found?

Answer 14

outside the neurons

Question 15

What are b-amyloid plaques?

Answer 15

insoluble aggregates of b-amyloid proteins

Question 16

where are NFTs found?

Answer 16

inside the neurons

Question 17

What are NFTs?

Answer 17

insoluble aggregates of hyperphosphorylated Tau

Question 18

when can a confident diagnosis of AD be made?

Answer 18

at autopsy

Question 19

How well can clinical criteria hope to identify AD?

Answer 19

sensitivity -80%

specificity - 70%

Question 20

How is AD diagnosed?

Answer 20

Mini-mental status exam
History from family/friends
MRI and PET scans - rear brain inactivity
CSF markers - 300% increase in tau, Ab increase 50%

Question 21

What can be found in APP null mice?

Answer 21

normalish - underweight and decreased activity

Question 22

What can be found in APLP2 null mice?

Answer 22

normal

Question 23

What can be found in APP/APLP2 null mice?

Answer 23

80% die within a week, deficits in balance and strength

Question 24

What is the major pathway of b-amyloid production?

Answer 24

using a-secretase

Question 25

What are the minor pathways of Ab production?

Answer 25

b/y secretases -> Ab peptide and APPb, P7

Question 26

What is the y-secretase complex?

Answer 26

presenilin, nicastrin, presenilin enhancer

Question 27

What can be seen with Ab 42 and Ab43?

Answer 27

preferentially form networks of salt linkages and strong hydrogen bonds between ionised side chains of opposite charge which form plaques

Question 28

What form of Ab is increase in AD?

Answer 28

Ab1-42

Question 29

How much does Ab1-42 normally make up in healthy individuals?

Answer 29

5-20%

Question 30

What are some features of Ab1-42?

Answer 30

more hydrophobic
more prone to fibril formation
facilitated by Zn/Cu

Question 31

Why are plaques not a definitive marker of AD?

Answer 31

healthy patients have them too

not all mice with AD have plaques

Question 32

What is the evidence for Ab as a cause of AD?

Answer 32

• increased no. of plaques in patients
• genetic mutations in EOAD cause increased production of Ab peptides
• Ab plaques appear in Down Syndrome that carry extra copy of APP gene
• APOE4 increase risk of sporadic AD

Question 33

Why is b-amyloid toxic?

Answer 33

• can induce apoptosis in cultured cells
• induces production of ROS -> apoptosis
• may directly insert into and disrupt cellular membranes
• may promote aggregation of tau to form NFTs

Question 34

What is the b-amyloid hypothesis?

Answer 34

the accumulation of a fragment of APP or Ab1-42 leading to the formation of plaques that kill neurons

Question 35

What is the tau hypothesis?

Answer 35

abnormal phosphorylation of tau proteins making them sticky and leading to the break up of microtubules
loss of axonal transport leads to cell death

Question 36

What are the genetic mutations associated with EOAD?

Answer 36

PS1, PS2 and APP - increased production of Ab-peptide

Question 37

Why are Down Syndrome patients at increased risk of AD?

Answer 37

carry an extra copy of the APP gene which is on Chromosome 21

Question 38

Where does Tau bind?

Answer 38

microtubules, predominantly in the axons of neurons

Question 39

What does tau co-purify with?

Answer 39

tubulin and microtubules

Question 40

What does the co-existence of tau with tubulin and microtubules do?

Answer 40

stabilises MT integrity, promoting MT assembly which is responsible for transport of molecules within neurons

Question 41

What is the function of microtubules?

Answer 41

transport of molecules within neurons

Question 42

What are NFTs?

Answer 42

aggregated Tau

Question 43

Where is Tau redistributed in AD?

Answer 43

cell bodies and dendritesw

Question 44

What question does the redistribution of tau raise?

Answer 44

is it tau that is toxic or loss of MT function

Question 45

What happens in Tau KO mice?

Answer 45

normal and show no obvious developmental, cognitive or neuronal polarity deficits

Question 46

What other form of dementia is caused by mutations in Tau?

Answer 46

Frontotemporal Dementia with Parkinsonism (FTDP-17)

Question 47

What can be concluded from the genetic studies into tau?

Answer 47

it is the presence of abnormal tau/NFTs rather than loss of function that contributes to AD development

Question 48

Where have Tau mutations not been found?

Answer 48

AD

Question 49

What shows a high correlation with the development of AD?

Answer 49

the number and location of NFTs

Question 50

Which Tau mutations have increased tendency to aggregate and form NFTs?

Answer 50

FTDP-17

Question 51

Why is Tau not necessarily the answer to NFTs and neurodegeneration in AD?

Answer 51

some AD can have neuronal loss in absence of NFTs and some FTDP-17 can have extensive degeneration with few NFTs

Question 52

What proteins aid Tau hyperphosphorylation in AD?

Answer 52

GSK3, CdK5, MAPK

Question 53

What does tau hyper-phosphorylation do?

Answer 53

• affects its ability to bind MTs
• promotes aggregation
• forms NFTs

Question 54

What suggests that NFTs over plaques are the correct hypothesis?

Answer 54

• it is never just plaques that appear

- show higher correlation with AD progression than plaques

Question 55

What is the difference between familial AD and FTDP17?

Answer 55

AD - mutations in APP processing molecules and have high levels of plaques and tangles
FTDP17 - never has plaques, only tangles

Question 56

What backs up that plaques are the issue in AD?

Answer 56

transgenic mice that express mutant APP develop plaques but not tangles however have cognitive deficits

Question 57

What does Ab injection into transgenic mutant Tau mice do?

Answer 57

accelerates tangle formation

Question 58

What does accumulation of phosphate on Tau proteins do?

Answer 58

causes “Paired Helical Filaments” that accumulate and lead to NFTs - PHFs are the main component in NFTs

Question 59

What is the probable cause of cell death with the Tau hypothesis?

Answer 59

the impaired axonal transport

Question 60

What is the process of plaque accumulation according to the amyloid hypothesis?

Answer 60

non-soluble fragment of APP accumulates and is deposited outside the cell
insoluble nature of Ab-42 helps to gather other protein fragments i.e. ApoE into plaques

Question 61

What are the potential mechanisms of cell death in the amyloid hypothesis?

Answer 61

the plaques or possible migration of Ab-42 out of the cell

Question 62

What genes are the subunits of y-secretase?

Answer 62

PSEN1 and PSEN2

Question 63

What is the Serial model?

Answer 63

when Ab -> p-tau -> synaptic loss -> cell loss

Question 64

What is the dual pathway model?

Answer 64

Ab + p-tau -> synaptic loss -> cell loss

Question 65

What is the leading perception in AD ?

Answer 65

AD is initiated by the primary amyloidosis which causes secondary tauopathies -> neurodegeneration. Tau causes the neurodegeneration but the process is initiated by Ab

Question 66

What is the Current theory in AD?

Answer 66

it is a multifactorial pathway

• protein accumulation -> plaques and tangles
• inflammation -> glial activation
• lipid distribution - lipid membrane site of APP cleavage

Question 67

What is the size of ApoE?

Answer 67

34kDa, 299aa

Question 68

where is ApoE highly produced?

Answer 68

liver and brian

Question 69

What cells in the brain produce ApoE?

Answer 69

glial cells - astrocytes

Question 70

What are the common isoforms of ApoE?

Answer 70

E2 - cys 112, cys 158
E3 - cys 112, arg 158
E4 - arg 112, arg 158

Question 71

Which form of ApoE is a risk factor?

Answer 71

E4

Question 72

What form of ApoE is neuroprotective?

Answer 72

E2

Question 73

How does Ab cross the BBB?

Answer 73

LRP transporters

Question 74

How does ApoE influence Ab clearance?

Answer 74

Ab has an affinity for ApoE

Question 75

What is the proposed mechanisms of Ab removal via various ApoE?

Answer 75

Ab may have lower affinity for lipid bound ApoE4 than ApoE3 - reduced clearance

Question 76

What are areas containing a-secretase low in?

Answer 76

cholesterol

Question 77

What are areas containing b/y secretase high in?

Answer 77

cholesterol and sphingolipids

Question 78

What mediates Ab influx across the BBB?

Answer 78

RAGE

Question 79

What are the two major proteases involved in Ab degradation?

Answer 79

IDE and NEP

Question 80

Where are IDE and NEP found?

Answer 80

IDE in the cytoplasm

NEP - transmembrane with active site on EC domain

Question 81

What happens in mutations on IDE and NEP?

Answer 81

increased Ab accumulation

Question 82

What are the varying hypotheses in AD?

Answer 82

• Ab-amyloid hypothesis - plaques due to overproduction/clearance
• Ab-oligomer - soluble oligomers block induction of LTP
• Presenilin - impaired presenilin functions due to mutations or Ab
• Ca dysregulation - due to ageing, oxidative stress, Ab
• lysosome hypothesis - lysosome/autophagy dysfunction
• Tau hypothesis - aggregated hyperphosphorylated tau

Question 83

What are the mutations associated with EOAD?

Answer 83

mutations in APP, PS1, PS2 -> increase Ab 1-42 production

Question 84

What are the mutations associated with LOAD?

Answer 84

ApoE causing increase accumulation/decreased clearance of Ab1-42
IDE/NEP mutations

Question 85

What is the mulitfactorial threshold model?

Answer 85

many common alleles with low penetrance
most people have several risk factor
risk alleles are additive and environment additive factors
disease process begins when certain threshold is reached

Question 86

What are the features of APP mutations?

Answer 86

on chromosome 21
around 50yrs onset
5% families

Question 87

What are the features of the PS1 mutations?

Answer 87

chromosome 14
40 years onset
50% of families

Question 88

What are the features of PS2 mutations?

Answer 88

chromosome 1
40 years onset
rare

Question 89

What are the features of ApoE isoforms?

Answer 89

E4 decreases age of onset

chromosome 19

Question 90

What are the features of A2M?

Answer 90

a-macroglobulin
A2M-2 increased risk of AD
Chromosome 12

Question 91

What are the other risk factors of AD?

Answer 91

age, diabetes/obesity, brain activity, physical exercise

Question 92

What are the treatment goals in AD?

Answer 92

improve memory, functional status and behavioural symptoms
slow progression
delay or prevent onset

Question 93

Why are AChEIs given?

Answer 93

Acetylcholine transferases are lost early in AD progression in the cortex and hippocampus -> used to increase ACh in synapse

Question 94

What drugs may be given as AChEIs?

Answer 94

rivastigmine, donezepril, galantamine

Question 95

What are the effects seen with AChEI treatment?

Answer 95

modest improvement in memory and thinking in 50% AD patients
delays neurodegeneration by about 6 months
temporarily mitigates some of the symptoms

Question 96

What is used to target excitotoxicity in moderate-severe AD?

Answer 96

Memantine, glutamate receptor antagonist (NMDARs)

Question 97

What are considered the potential targets of future therapeutic needs in AD?

Answer 97

amyloid at the point of production, plaque build up or clearance

Question 98

What have NSAIDs been shown to do?

Answer 98

favour production of 1-40 over 1-42 via altered y-secretase activity

Question 99

Why is y-secretase a more difficult target?

Answer 99

has multiple essential substrates

Question 100

What enhances a-secretase activity and via what mechanisms?

Answer 100

bryostatin via PKC inhibition

Question 101

What other potential mechanisms could be targeted?

Answer 101

b-secretase - lacks other substrates
preventing aggregation - cluoquinol
immunotherapy for removal of Ab peptides/plaques

Question 102

What is cluoquinol?

Answer 102

an antibiotic and Cu/Zn chelator

Question 103

why did the AD vaccine fail?

Answer 103

due to encephalitis

Question 104

What are the research handicaps in developing AD therapies?

Answer 104

inconsistent results
inappropriate tools
inappropriate conclusions

Question 105

What does a good AD model need to show?

Answer 105

face validity - plaques/tangles/degeneration/cognitive loss
Reliability/reproducibility - consistent results between animals
Construct validity - observed in different environments w. different tests in the same species measuring the same things
Predictive validity - temporal relevance to the disease and treatment aimed at the insult