L42 patho and pharm of PD

Question 1

T or F: The ratio for PD is 2:1 female:male

Answer 1

F, males twice as likely

Question 2

PD results from a neurological deficit in the ___________ system.

Answer 2

extrapyramidal, (noncortical voluntary motor control)

Question 3

PD sxs acronym

Answer 3

TRAP
- resting Tremor
- Rigidity
- Akinesia/bradykinesia
- Postural instability

Question 4

other sxs of PD not related to motor fxn (3)

Answer 4

speech difficulties, cognitive deficits, depression

Question 5

PD is characterized by a loss of _______ ________ in the _______ ________

Answer 5

dopaminergic neurons, substantia nigra

Question 6

Some studies suggest that __% of the nigral dopamine neurons, or -% of the nerve terminals in the striatum, are lost before patients present with motor symptoms.

Answer 6

50, 70-80

Question 7

In PD, ther loss of neurotransmission is through what system?

Answer 7

nigrostriatal

Question 8

Lewy bodies are enriched with fibrillar forms of what protein?

Answer 8

protein a-synuclein

Question 9

surviving neurons in PD pts have dense, spherical protein deposits called?

Answer 9

lewy bodies

Question 10

T or F: Lewy bodies are found intracellularly

Answer 10

True

Question 11

If you see braak stages what should you think of?

Answer 11

A-synuclein

Question 12

At which Braak stage are there lewy bodies in the SN?

Answer 12

Stage 3

Question 13

lewy bodies move from where to where as the braak stages go up?

Answer 13

lower structures and move up towards cortex

Question 14

what structure in the brain undergoes neurodegeneration?

Answer 14

SN pars compacta

Question 15

what structure do the caudate nucleus and putamen make up?

Answer 15

striatum

Question 16

direct pathway (simple pathway)
A. D1 striatal neurons receptor pathway
B. D2 striatal neurons receptor pathway

Answer 16

A. D1 striatal neurons receptor pathway

Question 17

Indirect pathway (complicated pathway)
A. D1 striatal neurons receptor pathway
B. D2 striatal neurons receptor pathway

Answer 17

B. D2 striatal neurons receptor pathway

Question 18

SNpc ->striatum -> Gpi/SNpr -> thalamus -> cortex

Answer 18

simple pathway, D1 pathway

Question 19

SNpc -> striatum -> Gpe -> STN -> Gpi/SNpr -> thalamus -> cortex

Answer 19

imdirect/complicated pathway, D2 pathway

Question 20

what is the result of SNpc releasing dopamine to either pathway?

Answer 20

increased signaling from thalamus to the cortex -> increased proper motor function

Question 21

what signaling is favored in the signaling from the SNpc to D1 or D2 receptors?

Answer 21

thalamocortical signaling, this effect is disrupted in PD

Question 22

what is globus pallidus?

Answer 22

two versions, internal and external, both are downstream of striatum

Question 23

what do antimuscarinics treat in PD?

Answer 23

adjunct therapy for tremor and motor symptoms

Question 24

T or F: Antimuscarinics are used only in high doses to ensure treatment of motor symptoms

Answer 24

False, they are used in low doses because of side effects

Question 25

in the control of motor movement _______ is excitatory while _______ is inhibitory

Answer 25

ACh, Dopamine (IN THE INDIRECT PATHWAY (D2)

Question 26

the loss of dopamine results in relative _____ of activity in _______ pathways

Answer 26

excess, cholinergic

Question 27

what can partially compensate for the overactive activity of cholinergic pathways in the loss of dopamine?

Answer 27

a cholinergic antagonist

Question 28

what is the antimuscarinic drug in the slide for the tx of motor symptoms in PD?

Answer 28

Benztropine (Cogentin)

Question 29

What happens to cholinergic signaling when dopamine signaling is overactive?

Answer 29

it would go down

Question 30

what is the “gold standard” for PD therapy?

Answer 30

L-Dopa

Question 31

T or F: L-dopa is a precursor of dopamine

Answer 31

true

Question 32

T or F: L-DOPA is orally active and can enter the CNS

Answer 32

tru

Question 33

why is there a difference in bioavailability between L-DOPA and dopamine

Answer 33

because DA (?) has a net positive charge at PH 7

Question 34

at high doses L-DOPA produces what 3 side effects?

Answer 34

nausea, hypertension (weird), and psychosis

Question 35

the dose of L-DOPA can be lowered (4x) by doing what?

Answer 35

co-administering with carbidopa

Question 36

a peripherally-acting DOPA decarboxylase inhibitor

Answer 36

carbidopa

Question 37

what is the combo drug called with L-DOPA and carbidopa?

Answer 37

sinemet

Question 38

T or F: dopamine can go across the BBB with ease

Answer 38

False, it cant cross at all (which is super weird)

Question 39

where must L-DOPA be converted to dopamine?

Answer 39

in the SN, not in the periphery

Question 40

what structural feature keeps dopamine from crossing the BBB?

Answer 40

carboxyl group

Question 41

what happens physiologically that leads to us increasing the dose of DOPA?

Answer 41

LDOPA is converted in a decarboxylation reaction in the periphery, this leads to a loss of LDOPA that is supposed to go into the CNS leading to more dopamine in the periphery that we do not want

Question 42

T or F: carbidopa passes the BBB

Answer 42

False, meaning it cannot inhibit DDC in the SN

Question 43

what can happen after several years of L-DOPA treatment? (highlighted red)

Answer 43

on/off oscillations

Question 44

adding carbidopa to L-DOPA accomplishes what main goal?

Answer 44

keeps L-DOPA from converting dopamine in the periphery

Question 45

______ and _____ are major problems in long term L-DOPA tx

Answer 45

dyskinesias and on/off effects

Question 46

how can the dyskinesias and on/off effects cause by LTT of L-DOPA be alleviated? (red text)

Answer 46

administering L-DOPA in a continuous manner (new liquid-based subq infusion)

Question 47

T or F: Dyskinesias are caused by Parkinsons

Answer 47

false, its the drugs

Question 48

another key limitation in L-DOPA therapy is?

Answer 48

prodrug conversion

Question 49

How do you address the challenge of prodrug conversion in L-DOPA tx?

Answer 49

use dopamine receptor agonists- this is reasonable bc the postsynaptic dopamine receptors are still present in the striatum (this was red so read it twice)

Question 50

what drug is a mixed D1 and D2 agonist?

Answer 50

apomorphine

Question 51

what can be found in the apomorphine structure?

Answer 51

dopamine with catechol and aminoethyl groups

Question 52

Apomorphine administration

Answer 52

subq in late stage PD to provide rapid relief

Question 53

Why is the usefulness of Apomorphine limited?

Answer 53

potent emetic effects (puking)

Question 54

what are the 3 non-ergoline DA receptor agonists?

Answer 54

Ropinirole (requip), pramipexole (Mirapex), and rotigotine (neuropro)

Question 55

what kind of agonists are the non-ergoline DA agonist?

Answer 55

D2 and D3

Question 56

T or F: Ergolines have less side effects than non-ergolines

Answer 56

False, ergolines have more side effects

Question 57

How are the non-ergoline drugs generally used?

Answer 57

as monotherapies for early-stage PD

Question 58

Which one of the following is a transdermal patch?
A. Ropinirole (requip)
B. pramipexole (Mirapex), C. rotigotine (neuropro)

Answer 58

C. rotigotine (neuropro)

Question 59

what drug class inhibits dopamine metabolism?

Answer 59

MAO-B inhibitors

Question 60

what are the two propargylamine MAO-B inhibitors?

Answer 60

Selegiline (deprenyl) and rasagiline (azilect)

Question 61

what structural significance do the propargylamines have? (-giline drugs)

Answer 61

triple bond

Question 62

how are MAO-B inhibitors generally used?

Answer 62

monotherapies to delay first use of L-DOPA BUT they can also be adjunct with L-DOPA

Question 63

what do MAO-B inhibitors inhibit?

Answer 63

oxidation of dopamine to DOPAL by monoamine oxidase-B (MAO-B)

Question 64

what is the reversible MAO-B inhibitor?

Answer 64

Safinamide (xadago)

Question 65

what makes Safinamide (xadago) reversible?

Answer 65

no propargylamine group

Question 66

how is Safinamide (xadago) generally used?

Answer 66

as adjunct to L-DOPA/Carbidopa (particularly during off episodes)

Question 67

what drug class ALSO inhibits dopamine metabolism that isnt the MAO-Bi’s?

Answer 67

COMT inhibitors

Question 68

what are the 3 COMT inhibitors?

Answer 68

entacapone (comtan)
Tolcapone (tasmar)
Opicapone (Ongentys)

Question 69

what do the COMTi’s inhibit?

Answer 69

the methylation of the 3-OH group of DA or L-DOPA by catechol-O-methyl transferase (COMT)

Question 70

Inhibition of COMT by which of the following decreases metabolism of L-DOPA in the periphery
A. Entacapone (comtan)
B. Tolcapone (tasmar)
C. Opicapone (Ongentys)

Answer 70

A. Entacapone (comtan)
C. Opicapone (Ongentys)

Question 71

inhibition of COMT by which of the following in the CNS allows levels of CNS dopamine to remain higher and increased the dopamine elimination time by 30-50%
A. Entacapone (comtan)
B. Tolcapone (tasmar)
C. Opicapone (Ongentys)

Answer 71

B. Tolcapone (tasmar)

Question 72

T or F: COMT inhibitors increase the potency and duration of sinemet action

Answer 72

F, potency doesn’t change and it prolongs the duration

Question 73

the mixture of L-DOPA, carbidopa, and entacapone is called what

Answer 73

Stalevo