09 10 2014 Movement disorder drugs

Question 1

Parkinson’s Disease -what is it? -age of onset? -characteristics?

Answer 1

A progressive disorder of movement that occurs most commonly in the elderly. Age of onset = 55 years old. - Resting tremor -muscle rigidity -Bradykinesai (slowness of movement) -Impairment of postural balance leading to disturbance of gait and falling.

Question 2

What are the neurons affected by parkinson’s disease

Answer 2

loss of dopaminergic (DA) neurons in substantial nigra pars compact (SNpc) in the basal ganglia. -up to 70-80% of DA loss occurs before disease is clinically recognizable. -decrease in dopaminergic terminals in the striatum

parkinson’s disease is diagnosed at an advanced stage of cell loss

Question 3

What happens with the loss of DA in the corpus striatum

Answer 3

DA loss = effect of acetylcholine is relatively increased.

Loss of neurons in substancia nigra = decrease signaling to striatum.

Net effect results in decreased stimulation of the motor cortex by the basal ganglia

Question 4

Proposed cause of PD

Answer 4

1. Genetic
2. Environmental
3. Oxidative stress
4. Energy metaoblism and aging

Question 5

Genetic Factors?

Answer 5

Mostly genes invovled in protein degradation, mitochondrial function, and response to oxidative stress.

* alpha- synuclein –> Lewy bodies

* Parkin, DJ-1, PINK 1, LRRK2

* contribution of genetic factors is rather low

MOST PD IS IDIOPATHIC

Question 6

Environmental Factors

Answer 6

MPTP (contaminator of synthetic heronin) is metabolized to free radical MPP+ which produces oxidative stress and cell death.

MPP+ is actively transported to neurone via a dopamine transpoert.

Things that increase risk factor for Parkinson’s disease

1. Pesticides/Herbicides
2. hemolytic exposure

Things that decrease chance of PD

1. coffee drinking
2. use of anti-inflammatory

Question 7

Where does Oxidative Stress come from?

Answer 7

Metabolism of dopamine.

-Dopamine – MAO–> DOPAC + H2O2 —Glutathione–> 2 H2O

If system is not working properly, then it can lead to the formation of radicals.

Question 8

Energy metabolism and aging

Answer 8

Aging decreases the capacity of neurons to undergo oxidative metabolism

• function of complex 1 in mitochondria is reduced in patients with PD

Question 9

What are the mechanisms of treating PD

Answer 9

1. exogenous dopamine precursor
2. increase relase of endogenous dopamine
3. Direct dopamine agonist
4. Inhibitors of dopamine metabolism

Question 10

Levodopa

Answer 10

Synthesized from tyrosine – exogenous deopmain precursor

Decarboxylation (L-amino acid decarboxylase) converts to Dopamine.

Less than 1% penetrates CNS is administered alone.

Question 11

Absorption rate of Levadopa

Answer 11

Depends on gastric emptying, pH of gastric juice and time of exposure to degradative enzymes.

Absorbed rapidly from small intestine by active transport system.

• competes with aromatic amino acids
• high protein meal will delay absorption and reduce peak plasma concentration

Question 12

Levadoopa transport to brain?

Answer 12

Levadopa–> dopamine via decarboxylase

—COMT–> 3-O Methyldopa

COMT (Catechol-O- methyltransferse) makes compoudn that is actively transported to Brain

-substrate competes with dietray protein

Question 13

Carbidopa

Answer 13

L-aromatic amino acid inhibitor

• does not penetrate BBB
• increase fraction of unmetabolized levodopa
• increases half-life of Levodopa
• Increases plasma concentration of Levodopa
• Allows a reduction in levodopa dosage – decrease peripheral side effects

Question 14

Sinemet and Sinement CR

Answer 14

Levodopa + carbidopa - fixed concentration

1:4 and 1:10 where 1 = 25mg

Sustained release formulation (Sinemet CR)

* increase among of drug going into brain

Question 15

What are the types of adverse effects associated with Levodopa Therapy?

Answer 15

1. GI effects
2. Cardiovascular effects
3. CNS effects
4. Long term effects

Question 16

What are the GI effects associated with Levodopa treatment?

Answer 16

when given alone 80% of patients suffer the following:

• Anorexia, Nausea, Vomitting
• stimulation of emetic center located in brain stem outside of blood-brain barrier
• combination with carbidopa reduces GI effects of only 20% of patients.

Question 17

What are the GI effects associated with Levodopa treatment?

Answer 17

• Arrhythmias
• Postural hypotension (activation of vascular dopamine receptors)

Question 18

What is the danger of prescribing Levodopa with nonspecific MAO inhibitor?

Answer 18

Accentuates levodopa actions and may precipitate a lifethreatening hypertensive crisis

Question 19

What are the CNS adverse effects of Levodopa?

Answer 19

Desired:

-decrease tremor, rigidity, and bradykinesia

Undesired:

• Pshycological distubances
  
  • hallucinations, confusion, anxiety

Question 20

What is the conventional anti-psychotic agent that are effect for psychological disease but actually make parkinson’s worse?

Answer 20

Phenothiazines

Question 21

What is another anti-psychotic medication that can be used and does not worsen parkinson’s?

Answer 21

Clozapine

“atypical” anti-psychotic

Question 22

What are the long term effects of Levodopa therapy?

Answer 22

1. Response fluctuations

• Endo of dose
• On-off phenomena

2. increase side effects

• Dyskinesias
• Psychiatric disturbances

3. May require adjuctive therapy.

Question 23

What is End-of Dose Deterioration?

Answer 23

Early PD: nigrostriatal dopamine system retains some capaciy to store and relase dopamine (“ buffering effect”).

After long-term use of Levodopa: “buffering effect” is lost. Patients motor state may fluctuate drmatically with each dose of levodopa –> “wearing-off- phenomena”

-dose of levodopa may improve symptoms for 1 or 2 hours before wearing off.

Question 24

On-Off phenomena with Levodopa therapy

Answer 24

Patients fluctuate rapidly between having no apparent effects of medication (off) and having effects of medication (on).

Off periods are marked with akinesia (state of being without movement) –> improved mobililty but often marked dyskinesia.

this is probably due to the brain adapting to variations in levodopa levels (alterations in function of dopamine receptors)

Question 25

what is drug that can be used if Levodopa has caused sever off-periods and person is not responding to other measures?

Answer 25

Apomorphine

Question 26

Drug interactions with Levodopa Therapy

Answer 26

MAO -A- inhibitors : life-threatening hypertensive crisis

Pyridoxine (vit B enhances extracerebral metabolism of levodopa)

Question 27

Contraindications with Levodopa Therapy

Answer 27

Psychotic patients

Angle-closure glaucoma

Active peptic ulcer

Use with caution if history of melanoma (Levodopa is a precursor for melanin)

Question 28

What are the two types of dopamine agonists?

Answer 28

Exictatory (D1 receptor family)

Inhibitory (D2 receptor family)

-do not require to be enzymatically metabolized– elimits production of toxic metabolites ( levodopa was made outside of the CNS and had toxic effects)

Question 29

Bromocriptine

Answer 29

Ergot derivative

D2 agonist

• well absorbed orally
• half life of 2-3 hours
• used in combination with levodopa/carbidopa for advanced disease to smooth on/off response fluctuations.

Question 30

Adverse Effects of Bromocriptine?

Answer 30

-Same as Levodopa

Ergot adverse effects: (vasoconstriction)

• Pleuropulmonary fibrosis
• retroperitoneal fibrosis
• erythromelalgia (blockage and inflammation of blood vessels)
• Digital vasospasm (constriction of small arteries of the finger)

Question 31

Ropinirole

Answer 31

Non-ergot derivative.

D2 agonist

Metabolized by CYP1A2 – drugs metabolized by liver will significantly reduce clearance of drug.

Question 32

Pramipexole

Answer 32

Non-ergot derivative

D3 agonist

Excreted largely unchanged in urine.

Question 33

Ropinirole and Pramipexole benefits/usage

Answer 33

• Effective as monotherapy in patients with mild disease
• Effective as measn of smoothing response fluctuations in patients on levodopa therapy with more advanced disease.

Question 34

Adverse effects of ropinirole and pramipexole

Answer 34

Similar to Levodopa:

• GI effects
• Dyskinesia
• Orthostatic Hypotension, arrhythmias
• hallucinations and confusion

Ergot side effects:

-uncontrollabe tendency to fall asleep at inappropriate times; requires discontinuation of medication.

Question 35

Apomorphine

Answer 35

dopamine agonist

D4 receptors

Subcutaneous injection to treat “off” episodes in patients with advanced PD.

Question 36

Apomorphine Adverse Effects

Answer 36

-Emesis (vomitting/nausea) and requires pretreatment with ANTIEMETIC TRIMETHOBENZAMIDE 3 days before itital treatment and continued for at least two months.

Question 37

Apomorphine is contradicted with what drug?

Answer 37

Antimetics of the 5HT3 receptor class –> causes severe hypotension and loss of conciousness

Question 38

MAO-B inhibitors

Answer 38

metabolize dopamine selectively

Question 39

MAO-A inhibitors

Answer 39

metabolizes norepinephrine, serotonin, and dopamine; also found in liver and GI tract

Question 40

Selegiline

Answer 40

Irriversible MAO-B inhibitor

• retards breakdown of dopamine in the striatum without inhibiting peripheral metabolism of catecholamines
• modest beneficial effect when used alone.
• also used in combination with levodopa/carbidopa to decrease response fluctuations in late PD patients.

Question 41

Adverse effects of Selegiline?

Answer 41

• accentuate motor and cognitive effects of levodopa therapy
• Insominia, anxiety

Question 42

Selegiline should not be taken with which drugs?

Answer 42

1. analgesic meperidine – stupor, rigidity, agitation, and hyperthermia, tramadol, methadone, cyclobenzaprine, St. John’s wort.
2. tricyclic antidepressants OR Serotonin-reuptake inhibitors – risk of acute serotonin syndrome!

Question 43

Rasagiline

Answer 43

more selective MAO-B inhibitor

• does not produce amphetamine metabolites
• may prevent progression of PD in early PD.
• use in combination with levodopa/carbidopa to decrese respone fluctuations in late PD patients.
• Monotherapy in mild disease.

Question 44

Adverse effects of Rasagiline

Answer 44

-Accentuate adverse motor and cognitive effects of levodopa therapy

Question 45

What are drugs that should not be taken with Rasagiline?

Answer 45

1. Analgesic meperidine – stupor, rigidity, agitation
2. tricyclic antidepressants or serotonin reuptake inhibitors

Question 46

Rasagiline Treatment of early PD – Neuroprotective effect

Answer 46

1. decrese synthesis of toxic metabolites
2. neuroprotection by reducing oxidation of dopamine

Question 47

What are the 3 drugs in the Catechol-O-methyl Transferase Inhibitors

Answer 47

1. Tolcapone (central and peripheral effects)
2. entacapone (peripheral effects)
3. Stalevo – levodopa/carbidopa/entacapone

Question 48

Benefits of Tolcapone and entacapone

Answer 48

• Inhibition of COMT prolongs plasma half-life of levodopa and increases availability of levodopa in brain.
• adjunct to levodopa/carbidopa = reduction of levodopa dose
• approved for patients with late PD who have developed response fluctuations.

Question 49

Adverse effects of tolcapone and entacapone

Answer 49

Levodopa related dopaminergic effects

-Diarrhea, abdominal pain, sleep disturbances

Question 50

What drugs should you be aware of when using tolcapone and entacapone?

Answer 50

• Drug interactiosn with drugs notmally metabolzied by COMT
• concurrent with non-specific MAO inhibitor could severely limit metabolism of levodopa.

Question 51

Tolcapone

Answer 51

More potent

Half-life 2-3 hrs

ADVERSE EFFECT:

Hepatotoxicity

• can increase aminotransferase and transaminase activity – indicator of liver damage.

Question 52

Entacapone

Answer 52

Less potent that Tolcapone

Half life= 1-2 hrs

NO incidence of hepatotoxicity and is therefore, generally prefered.

Question 53

Anti-cholinergics drugs (5):

Answer 53

1. trihexyphenidyl
2. benzotropine mesylate
3. biperiden
4. orphenadrine
5. procyclidine

Question 54

Anti-cholinergics benefits

Answer 54

• May improve tremor and rigidity
• Little effect on bradykinesia
• If fail to respond to one drug, try others.

Question 55

Adverse effects of Anti-cholinergics

Answer 55

CNS effects: drowsiness, restlessness, inattention, confusion, delusions, hallucinations, mood changers..etc.

other adverse effects:

-Dry mouth, constipation, nausea vomiting, tachycardia, increased IOP, palpitation, blurring of vision, mydriasis…etc.

Question 56

Amatadine

Answer 56

Antiviral agent

• mechanism is unclear: increase dopamine release, blocks dopamine uptake, stimulates dopamine receptors.
• short lived but favorably influences bradykinesia, rigidity and tremor; it also ha antidyskinetic properties.
• used as initial therapy of mild PD and as adjunct therapy in patients on levodopa with dose-dependent fulctuations and dyskinesias.

Question 57

Adverse effects of amatadine

Answer 57

• restlessness, hallucinations, confusion, sleep disturbance, nausea
• overdose may cause acute toxic psychosis
• Livedo reticularis (swelling of small veins)

Question 58

When should you be hesitant of prescribing amatadine?

Answer 58

-patients with history of seizure or heart failure