CK E3 Word Scramble

Embed Code - If you would like this activity on your web page, copy the script below and paste it into your web page.

Normal Size Small Size show me how

Question	Answer
digoxin has ___ compartment model	2
are digoxin loading doses recommended in HF?	NO
what is digoxin used for?	controlling ventricular rate in AFib
are Digoxin loading doses given all at once and why?	because 2 compartment model, long distribution phase a large Vd
what is the initial Digoxin loading dose and the following doses?	0.25-0.5 then 0.25 q6h for total of 0.75-1.5
what is the absolute max loading dose?	1.5
does obesity have impact on Digoxin?	no, because it distributes into lean tissues
what weight is used for digoxin?	IBW, unless Actual is less than IBW then use TBW
what happens to the loading dose if pt has impaired renal function?	decrease total LD by 50%
what are lab abnormalities that make pt more sensitive to Digoxin and what should you do?	Hypokalemia, hypomagnesemia, hypercalcemia. lower doses used
what is the oral maintenance dose for adults with normal renal function?	0.125-0.25 mg po qd
what are the steps for determining dose in HF pts?	CrCl--> IBW --> Daily dose
safety monitoring for Digoxin?	BMP: Scr, K, Ca, Mg
when to get digoxin levels?	-initially starting, annually for stable pts, acute illness, concern for toxicity, change in renal function, drug interactions
what is the digoxin half life and when is steady state reached?	half life is 36hr, Steady state is reached in 3-5 t1/2= 108-180 hrs -5-7 days for normal renal function pts -2-3 wks for significant renal dysfunction
what happens if level is draw before SS?	falsely low
what happens if level is draw before the distributions phase had ended?	falsely high, wait at least 8 hours until after dose is given
what is digoxin's therapeutic range for HF	0.5-0.9
what is digoxin's therapeutic range for Afib	0.5-2 (1.2 is ideal because higher than that has been associated with increased mortality)
s/sx of digoxin toxicity	GI: N/V CNS: confusion, vertigo, dizziness Vision: yellow/ green halos Cardio: Vent Tachy Electrolytes: hyperkalemia
digoxin toxicity can occur in pts with____	normal therapeutic range usually in those with low K, Mg
risk factors for D tox	elderly, impaired renal function, hypokalemia, hypomagnesemia
digoxin toxicity antidote	DigiFab , Digoxin immune Fab
what are two types of D toxicity	acute, chronic
what are two DigiFab indications?	D conc above 10 after distribution phase OR >15 at any time Acute ingestion >10mg for adults
should digifab bw given to pt without s/sx of acute toxicity?	no, unless there is confirmed acute ingestion
DDI: NDH-CCB	V & D increases digoxin
DDI: amiodarone	increase D 2-3x above baseline--> decrease D dose by 20-50% if adding amiodarone
DDI: erythromycin, clarithromycin, tetracycline	increase D conc
DDI: Al containing products	decrease D absorption --> separate by 2 hours
DDI: cholestyramine	decrease D absorption
DDI: NSAIDs	increase D conc
DDI: Loop diuretics	increase risk for D toxicity
is amiodarone therapeutic monitoring routinely recommended?	no
amiodarone is the DOC in ___ pts	HF
consider d/c Amio	if hepatic enzymes are >3x UNL
is amio renally adjusted	NO
amiodarone organ system toxicity	pulmonary, hepatic, cardiac, renal
amiodarone is contraindicated in which population	***iodine allergy 2/3rd degree heart block bradycardia causing syncope cariogenic shock
amiodarone monitoring	LFT, PFT, CxR, eye exam, TSH, EKG
amiodarone is a common _____ inhibitor	CYP
PD interactions with amiodarone	other drugs that decrease HR, prolong QTc
amiodarone DDI: digoxin	increase D, decrease D by 25-50%
amiodarone DDI: warfarin	increase W, decrease W dose by 30-50%
amiodarone DDI: simvastatin and lovastatin	increase statin, max simvastatin dose is 20, max love is 40
amiodarone DDI: GFJ	increase Amio conc, avoid use together
Lithium shares properties of	physiological cations (Na/K)
changes in fluids and Na balance	can effect PK and drug interactions
what is lithium half life	~5 days
is lithium renally dose adjusted ?	yes
what is the acute mania lithium levels?	0.8-1.5
what is the maintenance lithium levels?	0.6-1
when do you obtain trough conc for lithuim	right before the next dose after SS has been reached
Lithium SE	GI upset N/D, cogwheel rigidity, fine hand tremor, weight gain, hypothyroidism
what are lithium levels for mod toxicity	1.5-2.5
what are lithium levels for severe toxicity	>2.5
Lithium DDI: thiazide	increase L conc --> inc risk of L toxicity
Lithium DDI: loop diuretics	may inc or dec L conc
Lithium DDI: ACE/ARB/ARNI	increases L conc --> inc risk of L toxicity
Lithium DDI: decreased salt intake/ dehydration	increase L conc --> inc risk of L toxicity
Lithium DDI: NSAID	increase L conc --> inc risk of L toxicity (only NSAID that can be used with L is sulindac)
Lithium DDI: theophylline	dec L conc
Lithium DDI: increased salt or caffeine intake	dec L conc
theophylline is structurally similar to what	caffeine
is theophylline distributed into fatty tissues	no! (IBW is used unless TBW is less, then TBW is used)
is theophylline renally eliminated	no
how long is the half life for theophylline	1-2 days
ciprofloxacin (strong cyp inhibitor) does what to theophylline	increase T conc
strong cyp inducers does what to theophylline	decrease T conc
what is the conversion factor when converting from aminophylline to theophylline	multiply A by 0.8
theophylline levels	5-15
do you measure peak levels with theophylline	yes, after SS, typically wait at least 2 days
theophylline toxicity symptoms	N/V, tachycardia/ palpitations, tremors
what is phenytoin loading dose	20mg/kg
can phenytoin IV/PO doses be given all at once	IV can be given at once, oral not all at once because it is rate-limited GI absorption or oral phenytoin
what is the max phenytoin oral dose to be administered at once	400 mg, given in multiple doses separated by 2 hours
what is the total phenytoin therapeutic conc	10-20 (both bound and unbound)
what is the total free phenytoin therapeutic conc	1-2 mg measures only FREE drug
when to draw phenytoin levels	-after loading dose (IV-wait at least 2 hr after end of infusion) (PO- wait at least 24 hours after last dose-Loading dose is administer over 6-8hrs) -after mtn dose initiation (trough q3-4 days until stable) -when there is a chance in status of pt
when to draw phenytoin trough levels for stable pts	3-12 months
what are some factors that can alter phenytoin protein binding	-hypoalbuminemia (liver disease, burn,trauma,malnourishment, elderly) -displacement by endogenous cmpds(hyperbilirubinemia, ESRD) -displacement by exogenous cmpd (warfarin, valproic acid)
what happens to phenytoin in altered conditions	conc increase in the extravascular space
who should FREE phenytoin levels be recommended for?	-when the pt has altered protein binding (especially when change is first noted--> after can obtain total level is acceptable) -total P levels don't correlate with clinical status -critically ill with suspected PB
what is the serum albumin for hypoalbuminemia	<3.5
phenytoin toxic conc	->20 nystagmus ->30 ataxia, N/V ->40 mental status change and CNS depression
phenytoin DDI: valproate	increases P conc
phenytoin DDI: oral contraceptive	dec oral contraceptive conc, recommend alternative contraception method
phenytoin DDI: carbamazepine	can inc or dec P conc dec carb conc
phenytoin DDI: warfarin	inc or dec anticoagulant effect, inc P conc
phenytoin DDI: lamotrigine	dec lamotrigine conc
what gene do we test for carbamazepine?	HLAB *1502
if the pt is postive for HLAB *1502, what do you do	AVOID carbamazepine
what is unique about carbamazepine weekly doses	increase dose every week
what is carb therapeutic levels	4-12 mg/L
when to draw carbamazepine levels	-w/i 3-5 days after starting drug -again after auto induction is complete (3-5 wk) -change in status (DDI, pt status, or dosing)
when to draw carbamazepine levels in stable pt	3-12 m
carbamazepine DDI: valproate	increases carb active metabolite conc
carbamazepine DDI: oral contraceptive	dec oral contraceptive effectiveness
carbamazepine DDI: phenytoin	inc or dec phenytoin conc dec carb conc
carbamazepine DDI: warfarin	dec anticoagulant effect (dec INR)
carbamazepine DDI: lamotrigine	dec lamotrigine conc
when calculating dose for valproate what body weight is used	actual body weight
how do you titrate dose for valproate	increase dose weekly
how long until the mtn dose is reached	4-6 weeks after initiation
in what pt population do we avoid valproate	severe liver disease
what is valproate therapuetic level	50-100
when to draw valproate levels	-pt is at SS on mtn dose (reached in about 2-4d after mtn dose is achieved) -morning levels drawn right before next dose (level fluctuation AM/PM) -when there is a change in pt status
when to draw valproate levels in stable ambulatory pts	3-12 m
what are factors that affect valproate protein binding	-hypoalbuminemia (liver disease, burn,trauma,malnourishment, elderly) -displacement by endogenous cmpds(hyperbilirubinemia, ESRD) -displacement by exogenous cmpd (warfarin, phenytoin)
pt with altered protein binding on VA would be expected to have ___ and be at risk ____	higher free conc ; for toxicity even with normal total conc
valproate toxicity	75-100 ataxia, sedation 100-175 tremor >175 stupor, coma
valproate DDI: lamotrigine	inc lamotrigine conc
valproate DDI: estrogen- containing contraceptive	dec in VPA conc
beta-lactam pk/pd parameters	% time over MIC
what is aminoglycosides PK/PD	Cmax/MIC
what is vancomycin PK/PD	AUC/MIC
what is BL PK/PD	time /MIC
what is PK/PD target for cefepime	60% >MIC
what is PK/PD target for ertapenem	40%> MIC
what is PK/PD target for ampicillin-sulbactam	50%>MIC
for BL free drug conc must remain ___ MIC to effectively kill pathogens	above
what two infusion methods are recommended for BL	extended and continuous
for example: zosyn is primarily adminstered through the	extended infusion
what happens when you inc dose of BL	higher risk for ADR which are peak dependent
what happens when you give BL more frequently	increases efficacy with lowest risk for ADR
which BL require NO renal dose adjustment	ceftriaxone, oxacillin

Created by: reynaaltayawi