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pr3153 > ic7 - antiseizure medicines (ASM) > Flashcards

ic7 - antiseizure medicines (ASM) Flashcards

1
Q

classify the ASM into its different generations

A

first gen: CBZ, PHT, PB, VPA
second gen: GBP, TPM, LEV, LTG, pregabalin

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2
Q

what drugs can we use for focal, GTC, tonic, atonic, absence, myoclonic

A

[focal] CBZ, VPA, LEV, LTG (TPM, GBP, PHT)
(refractory: pregabalin)

[GTC]
new: CBZ, VPA, LTG (TPM)
(refractory: LEV)

[tonic/ atonic] VPA first line, LTG adjunctive

[absence] LTG and VPA first line or adjunctive

[myoclonic] LEV and VPA and TPM first line or adjunctive

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3
Q

compare the PK of the various ASM (A, F, protein binding, E, half life, ddi, enzyme type)

A

[CBZ] F 80%, protein binding 75-85%, E 100% H (autoinduction), half life 6-15h, ddi yes, enzyme inducer 1A2, 2C, 3A4, UGT, P-gp

[PB] F 100%, protein binding 50%, E 75% H, half life 72-124h, ddi yes, enzyme inducer 1A2, 2A6, 2B, 3A, UGT

[PHT] slow but complete A (slower at higher doses >400mg and with enteral feeds thus space 2hr apart), F 90%, protein binding 95%, E 100% H (non linear), half life 12-60h, ddi yes, enzyme inducer 2C, 3A, UGT, P-gp

[VPA] F 100%, protein binding 75-95%, E 100% H, half life 6-18h, ddi yes, enzyme inhibitor 2C9, UGT

[GBP] <60% A, no protein binding, E 100% R, half life 5-9h, no ddi

[LTG] 100% A, protein binding 55%, E 100% H, half life 18-30h, few ddi

[LEV] 100% A, protein binding <10%, E 66% R, half life 4-8h, no ddi

[TPM] >80% A, protein binding 15%, E 30-55% R, half life 20-30h, ddi dose dependent, enzyme moderate inducer 3A and moderate inhibitor 2C19

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4
Q

what are the common ddi for ASMs

A

antidepressants and antipsychotics, immunosuppressive tx, antiretroviral tx, chemotx agents

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5
Q

which ASMs are enzyme inducers

A

CBZ, PB, PHT

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6
Q

what are the issues with enzyme inducing ASMs

A

reproductive hormones, sexual functions, OC in women (enzyme inducers act on liver enzymes and are not selective on whether it is a drug or hormone)

sexual func and fertility in men

bone health (can incr risk of osteopenia or osteoperosis if vitD and Ca not supplemented appropriately)

vascular risk

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7
Q

what are the available dosage forms, indication, moa, F, A, Vd, protein binding, E, half life, enzyme, s/e, labs and monitoring of PHT

A

[dosage forms] PO suspension phenytoin acid (125mg/5mL, 100%), capsules (30, 100mg), IV phenytoin sodium (92%)

[indication] focal and GTC

[moa] blockade of Na channels

[F] 100%

[A] slow but complete (reduced at higher doses of >400mg and if given with enteral feeds thus space 2hr apart)

non linear PK (zero order kinetics and capacity limited CL aka CL dependent on conc and CL will decr with incr conc thus conc increment not proportional to dose increment)

[Vd] 0.7L/kg

[protein binding] 95% highly albumin bound (if low albumin will incr free PHT)

[E] 100% H (non linear)

[half life] 12-60h

[enzyme] inducer 3A4, 2C9, 2C19, UGT, P-gp

[s/e] gingival hyperplasia, hirsutism, osteopenia/ osteoperosis, arryhthmia, SJS, CNS (nystagmus, dizziness, HA, blurred vision, ataxia, incoordination), GI (N/V)

[labs] total (bound and unbound) PHT level, must adjust for corrected PHT estimate if hypoalbuminemia

[monitoring] osteopenia/ osteoperosis, lipid profile (LDL and cholesterol)

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8
Q

what are the dosage forms, indication, moa, F, Vd, protein binding, E, half life, enzyme, s/e and monitoring for VPA

A

[dosage forms] inj (400mg/vial), enteric coated tablets 200mg), sustained release tablets aka chrono (200, 300, 500mg), syrup (200mg/5ml)

[indication] focal, GTC, myoclonic, absence

[moa] blockade of Na channels and GABA potentiation

[F] 100%

[protein binding] 90-95% (highly albumin bound, displacement by endogenous substances like in uremia and hyperbilirubinemia, competitive binding with PHT warfarin and NSAIDs, saturable protein binding)

[E] 100% H

[half life] 6-18h

[enzyme] inhibitor of 2C9, 2C19, UGT

[s/e] osteoperosis/ osteopenia, pancreatitis, weight gain, thrombocytopenia/ neutropenia, GI (N/V), CNS (ataxia)

[monitoring] osteopenia/ osteoperosis, PLT count, LFTs

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9
Q

what should you do if there is hypoalbuminemia and PHT is to be used

A

if albumin <40g/L

C corrected = C observed/ [X(alb/10)+0.1]

where X is albumin coeff (X = 0.275 if CrCl 10, X = 0.2 if CrCl <10 *note 0.2 and 0.1 respectively if original winter-tozer)

units of alb in g/L and C in mg/L

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10
Q

what are the dosage forms, indication, moa, F, protein binding, Vd, M, E, half life, enzyme, s/e and monitoring for CBZ

A

[dosage forms] immediate release tablets (200mg), controlled release tablets (200, 400mg)

[indication] focal, GTC

[moa] blockade of Na channel

[F] 80%

[protein binding] 75-85% (highly bound to albumin and alpha1 acid glycoprotein)

[M] >99% metabolised into active metabolite carbamazepine 10,11-epoxide by 3A4, autoinduction

[E] 100% H

[half life] 6-15h

[enzyme] inducer of 1A2, 2c9, 2C19, 3A, UGT, P-gp

[s/e] osteopenia/ osteoperosis, hypoNa, neutropenia, SJS, GI (N/V), CNS (nystagmus, dizziness, blurred vision, ataxia, incoordination)

[monitoring] osteoperosis/ osteopenia, LFTs, serum Na

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11
Q

what is “autoinduction” and which ASM experiences this and how does it affect its dosing

A

induction of own metabolism -> causes CL to incr and half life to decr until conc decline and stabilise in accord with new CL and half life

CBZ has autoinduction and maximal autoinduction occurs 2-3w after initiation -> do not start with desired MD but start lower and titrate up slowly to ensure better tolerability

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12
Q

what is “saturable protein binding” and which ASM experiences this

A

decr protein binding at higher conc of ASM and higher free frac of drug with low albumin (or other protein of interest)

VPA experiences this

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13
Q

what is the indication, moa, A, protein binding, E, half life, enzyme and s/e of GBP

A

[indication] focal and GTC

[moa] P/Q type Ca channel blockade

[A] 60% or less

[protein binding] none

[E] 100% R

[half life] 5-9h

[enzyme] NA

[s/e] weight gain, peripheral edema, dizziness, ataxia

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14
Q

what is the indication, moa, A, protein binding, E, half life, enzyme, s/e of LTG

A

[indication] focal, GTC

[moa] Na channel blockade and some effects on GABA potentiation

[A] 100%

[protein binding] 55%

[E] 100% H

[half life] 18-30h

[enzyme] inducer of UGT, inhibitor of 2C19 and UGT

[s/e] HA, insomnia, tremor, SJS, rash, GI (N/V)

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15
Q

what are the indications, moa, A, protein binding, E, half life, enzymes, s/e and monitoring for TPM

A

[indications] focal, GTC

[moa] Na channel blockade and some effects on GABA potentiation

[A] 80% and above

[protein binding] 15%

[E] 30-55% R

[half life] 20-30h

[enzyme] moderate inducer of 3A4, moderate inhibitor of 2C19 (ddi is dose dependent)

[s/e] weight loss, memory problems, difficulty finding words, nephrolithiasis (kidney stones), CNS (somnolence, ataxia, fatigue)

[monitoring] metabolic acidosis

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16
Q

what are the indications, moa, A, protein binding, E, half life, enzyme and s/e of LEV

A

[indications] focal, GTC

[moa] binding to SV2a protein

[A] 100%

[protein binding] <10%

[E] 66% R

[half life] 4-6h

[enzyme] NA

[s/e] psychiatric sx (behavioral disturbances)

17
Q

what are the types of s/e of ASM

A

dose/ plasma conc related, hypersensitivity related, chronic systemic, neurological, metabolic, endocrine, suicidal ideation

[dose/ plasma conc related] CNS (somnolence, fatigue, dizziness, visual disturbances, nystagmus, ataxia) GI (N/V) psychiatric (behavioural disturbances) cognition (speech fluency)

[neurological] peripheral neuropathy

[metabolic] weight gain, weight loss

[endocrine] osteomalacia

[suicidal ideation] FDA black box warning

[hypersensitivity] SJS/ TEN, exfoliative dermatitis, lupus like rxn, blood dyscrasia (aplastic anemia, agranulocytosis), pancreatitis, hepatotoxicity

[chronic systemic] gingival hyperplasia aka growth of gums, alopecia, hirsutism

18
Q

how to mitigate dose related s/e for ASMs

A

initiate at low dose and titrate slowly, avoid large dose changes, restrict tx to one drug only if possible, adjust administration schedule (largest dose at bedtime, divide daily dose into smaller doses given more freq, sustained release, reduce total daily dose)

19
Q

what are the drugs that can cause SJS and how can we risk manage

A

PHT, CBZ, LTG

PGx testing for CBZ, dosing guidance for LTG, identify potential cross sensitivity rxn for ASMs with aromatic rings

[PGx testing] HLAB*1502 for Han Chinese and other Asian ethnic groups -> conduct prior to starting and if positive avoid CBZ and PHT

[dosing guidance for LTG] risk of srs cutaneous rxn higher with high starting doses, rapid escalation and concom VPA

[cross sensitivity] ASMs with aromatic ring hypothesised to be able to form arene-oxide intermediate and become immunogenic through interactions with proteins or cellular macromolecules

20
Q

what is the dosing guidance for LTG

A

[if taking VPA] 25mg EOD weeks 1-2, 25mg QD weeks 3-4, incr by 25-50mg/d q1-2w weeks 5 until at MD, MD is 100-200mg/d w VPA alone, 100-400mg/d w VPA and other drugs that induce glucoronidation

[if NOT CBZ/PHT/VPA] 25mg QD weeks 1-2, 50mg QD weeks 3-4, incr by 50mg/d q1-2w weeks 5 until at MD, MD is 225-375mg/d

[if on CBZ/PHT but NOT VPA] 50mg QD weeks 1-2, 100mg/d weeks 3-4, incr by 100mg/d weeks 5 until at MD, MD is 300-500mg/d

21
Q

which ASMs are aromatic

A

CBZ, PHT, PB, LTG, oxycarbazine

22
Q

what is “nystagmus”

A

involuntary rhythmic side to side, up and down or circular motion of the eyes

23
Q

what is “ataxia”

A

poor muscle control that causes clumsy voluntary movements

24
Q

what is “dyskinesia”

A

involuntary, erratic, writhing movements of face, arms, legs or trunk

25
Q

what is “asthenia”

A

lack of energy/ strength

26
Q

what are the factors to consider and key determinants when choosing appropriate ASM for tx of epilepsy

A

[factors to consider] efficacy, tolerability, PK, personal preferences, nation specific factors

[key determinants] seizure type, epilepsy syndrome, drug profile effects on comorbs and other meds and tolerability in special populations, ddi and hormonal effects and renal/ hepatic impairment, formulation and dosing freq, guidelines and availability and costs

27
Q

what are the key components in the tx algorithm of epilepsy

A

after starting ASM, determine if seizure free -> determine if issue with intolerable s/e -> determine if optimal QoL -> determine if seizure free for >2 yrs

28
Q

when might ASM be discontinued

A

may be considered after a min of 2 yrs w/o seizure

but in pts with incr risk of seizure recurrence, advisable to wait longer than 2 yrs before considering discontinuation

decision to stop ASM involves balance of the risks of continuation (chronic toxicity, teratogenicity) with the implications of relapse

discussed with pts and carers/ family members and discussion details should be documented

tapering schedule should be individualised, taking into account risk factors for seizure recurrence, seizure freq, number of meds

29
Q

what are the details that should be documented when discussing discontinuation of ASM

A

when discussing discontinuation of ASM with pts and carers/ family members, should document

(i) reasons for discontinuation
(ii) taper schedule
(iii) plans for monitoring pts during and after taper
(iv) pts motivation for, attitude towards and understanding of the potential risks and benefits of discontinuation vs continuing tx

30
Q

what is the criteria to be met for epilepsy to be considered resolved

A

resolved for individuals who had an age dependent epilepsy syndrome but are now past the applicable age or those who have remained seizure free for last 10yrs with no seizure meds for past 5yrs

31
Q

why is there a need for TDM for ASM

A

difficult to identify optimal dose on clinical grounds alone bc

(i) plasma ASM conc correlate much better than dose with clinical effects
(ii) assessment of therapeutic response on clinical grounds alone is difficult in most cases (ASM tx is prophylactic, seizures occur at irregular intervals)
(iii) not always easy to recognise signs of toxicity purely on clinical grounds
(iv) ASMs subject to substantial PK variability and thus large differences in dosage are req in diff pts
(v) no lab markers for clinical efficacy or toxicity of ASM

32
Q

what are the indications for ASM TDM

A

(i) to establish individual’s therapeutic range -> ref range may not be effective for all, once stable document effective level which controls seizures while minimising s/e

(ii) to assess lack of efficacy -> fast metabolisers, lack of adherence

(iii) to assess potential toxicity -> changing physiology, slow metabolisers, changes in disease or drugs or renal/ liver or new drugs and interactions

(iv) to assess loss of efficacy (breakthrough seizures) -> changes in physiology (age, pregnancy), changes in pathology, changed formulation, drug interactions

33
Q

what are the information required in order to conduct ASM TDM

A

(i) indication for ASM (diagnosis)
(ii) dose (when, how long, how much)
(iii) sample and when was sample taken and what type of sample taken (if short half life, take trough to look at MD adequacy)
(iv) clinical condition (seizure control at baseline vs currently, comorbs)
(v) other lab values
(vi) other drugs (when, how long, how much)

34
Q

what are the ref ranges for the various ASM

A

PHT 10-20mg/L
VPA 50-100mg/L
CBZ 4-12mg/L
PB 15-40mg/L

35
Q

what are the special populations to consider for ASM

A

women of childbearing potential, pregnancy, lactation

[women of childbearing potential] referred to specialist care to (i) discuss fertility, contraception, family planning issues (ii) early discussion on family planning

use of OC may become ineffective due to ASM being potent enzyme inducers thus need alternative methods, OC may lower LTG conc resulting in breakthrough seizures, potential risk to fetus due to uncontrolled seizures and teratogenic potential of ASM

[pregnancy] LEV and LTG safer options, VPA should not be used bc high risk of serious developmental disorders and congenital malformations (CBZ, PB, PHT, TPM can cause major congenital malformations – all except PHT have dose dependent risk) (PB, PHT, TPM have neurodevelopmental risk)

[lactation] all breastfeeding women on ASM should be encouraged to breastfeed and encouraged to receive support from relevant HCPs

36
Q

what are the alternative contraception options for women of childbearing potential and wants to start on ASM

A
  1. levonorgestrel or copper IUD
  2. medroxyprogesterone depot inj q10-12w along with barrier method
  3. continuous cycle COC (E and P) with at least 50mcg of E taken every day with 4d break q3m along with barrier method
37
Q

what is “status epilepticus”

A

it is when seizures continue or have different episodes that come and go and last >5mins

38
Q

what is the tx algorithm for status epilepticus (interventions for the different phases along the timeline)

A

stabilisation phase (0-5min), initial therapy phase (5-20min), second therapy phase (20-40min), third therapy phase (40-60min)

[stabilisation phase]
(i) stabilise pt (airway, breathing, circulation, disability -> neurologic exam)
(ii) time seizure from its onset and monitor vital signs
(iii) assess oxygenation, give O2 via cannula or mask and consider intubation if resp assistance needed
(iv) initiate ECG monitoring
(v) collect finger stick BG
(vi) attempt IV access and collect electrolytes, hematology, toxicology screen, ASM drug levels if appropriate

[initial therapy phase]
(i) if seizure continues, first line benzodiazepine
(ii) if not IM midazolam (10mg for >40kg, 5mg for 13-40kg single dose) or IV lorazepam (0.1mg/kg/dose max 4mg, may repeat dose once) or IV diazepam (0.15-0.2mg/kg/dose max 10mg, may repeat dose once)
(iii) if none above IV PB (15mg/kg/dose single dose) or rectal diazepam (0.2-0.5mg/kg max 20mg single dose) or intranasal midazolam or buccal midazolam
(iv) if seizure does not continue and pt at baseline then symptomatic medical care

[second therapy phase]
(i) if seizure continues, either IV fosphenytoin or IV VPA or IV LEV
(ii) if none above, IV PB
(iii) if seizure does not continue and pt at baseline then symptomatic medical care

[third therapy phase]
(i) if seizure continues, either repeat second therapy phase or anesthetic doses of either thiopental, midazolam, PB or propofol (all with continuous EEG monitoring)
(ii) if seizure does not continue and pt at baseline then symptomatic medical care

39
Q

what is the tx algorithm for status epilepticus (interventions for the different phases along the timeline)

A

stabilisation phase (0-5min), initial therapy phase (5-20min), second therapy phase (20-40min), third therapy phase (40-60min)

[stabilisation phase]
(i) stabilise pt (airway, breathing, circulation, disability -> neurologic exam)
(ii) time seizure from its onset and monitor vital signs
(iii) assess oxygenation, give O2 via cannula or mask and consider intubation if resp assistance needed
(iv) initiate ECG monitoring
(v) collect finger stick BG
(vi) attempt IV access and collect electrolytes, hematology, toxicology screen, ASM drug levels if appropriate

[initial therapy phase]
(i) if seizure continues, first line benzodiazepine
(ii) if not IM midazolam (10mg for >40kg, 5mg for 13-40kg single dose) or IV lorazepam (0.1mg/kg/dose max 4mg, may repeat dose once) or IV diazepam (0.15-0.2mg/kg/dose max 10mg, may repeat dose once)
(iii) if none above IV PB (15mg/kg/dose single dose) or rectal diazepam (0.2-0.5mg/kg max 20mg single dose) or intranasal midazolam or buccal midazolam
(iv) if seizure does not continue and pt at baseline then symptomatic medical care

[second therapy phase]
(i) if seizure continues, either IV fosphenytoin or IV VPA or IV LEV
(ii) if none above, IV PB
(iii) if seizure does not continue and pt at baseline then symptomatic medical care

[third therapy phase]
(i) if seizure continues, either repeat second therapy phase or anesthetic doses of either thiopental, midazolam, PB or propofol (all with continuous EEG monitoring)
(ii) if seizure does not continue and pt at baseline then symptomatic medical care

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