Term
| what are COX1 and 2 known for |
|
Definition
NSAIDs inhibit these prostoglandin synthase enzymes. the synthesis takes place by converting arachadonic acid
inhibition of COX2 is thought to be responsible for antipyretic, analgesic, and antinflammatory effects achieved by NSAIDs
inhibition of COX1 is thought to be linked to unwanted side effects of the GI tract. COX1 is the dominant prostanoid producer and synthesizes housekeeping molecules |
|
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Term
| what are all eicosanoid receptors? |
|
Definition
| G protein coupled receptors that interact in the cell to modulate the activites of adenylyl cylcase and PLC |
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Term
| regions that prostanoids effect |
|
Definition
vasculature, airways, and gastrointestinal and reproductive tracts; platelets and monocytes; kidneys; the central nervous system, autonomic presynap-tic nerve terminals, and sensory nerve endings; endocrine organs; adi-pose tissue; and the eye (the effects on the eye may involve smooth muscle). |
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Term
|
Definition
they are the metabolized product of arachadonic acid by lipxoygenase, speccifically 5-LOX, and they play an important role in proloning the inflammatory response
lipoxygenases cannot be inhibited by NSAIDs |
|
|
Term
| general class properities of NSAIDs |
|
Definition
- most are organic acids (except nabumetone)
- most are racemic
- most absorb rapidly and completely in GI
- fast acting, not very affected by food
- often extensively plasma protein bound (usually albumin)
- they can accumulate in synovial fluid with repeated dosing
- heavily hepatically metabolized and renally excreted (therefore, not recommended for patients with impairments of either of these)
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Term
|
Definition
| a drug intended for only COX2 inhibition |
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Term
| MOA: aspirin and non-aspirin NSAIDs |
|
Definition
aspirin binds irreversably to allosteric site on COX1 and 2 by acetylating a serine (mostly 1)
all other NSAIDs are reversible and can exhibit selectivity
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|
|
Term
| what is one risk of aspirin hypersensitivity? |
|
Definition
| shunting of AA to lipoxygenases and increased sythesis of leukotrienes |
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Term
|
Definition
| very effective because they can alter the gene expression of COX-2 and inhibit the activation of PKA which liberates AA, however, they are associated with widespread adverse effects and therefore should not be used for simple maladies |
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|
Term
| why wont the ductus arteriosus close? what closes it? |
|
Definition
prostoglandins are responsible for maintaining the DA which would usually close when breathing initiates
intravenous injections of NSAIDs (i.e. indomethacin and ibuprogen) facilitate closure |
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Term
|
Definition
small to large ulcers, usually caused by COX-1 inhibition, a systemic effect
patients with infections with helicobacter pylori, mucosal injury, excess alcohol use, or anticoagulent or glucocorticoid use are most suseptible
mech is that COX-1 inhib leads to down reg of PGI2 and PGE3 muscosal cytoprotectives, decreased bicarbonate production, increased acid production |
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|
Term
|
Definition
tNSAIDs are associated with increased risk of MI and stroke, especially selective COX2 inhibs like celecoxib, diclofenac, and meoxicam
thromboxin (Tx) causes vasoconstriction and platelet aggregation and is a product of COX-1. It is inhibited by PGI2
PGI2 is produced by COX2. Stop COX2, like many tNSAIDs do, and you stop that inhibition, and promote platelet aggregation, vasoconstriction
HOWEVER, aspirin is mostly specific to COX1, which will cut off this pathway at the production of Tx, therefore, it can have CV protective features while other tSAIDs increase risks for MIs and ischemia
------------------------------------
salicylates also carry adverse CV effects bc they instigate retention of water and salt and decreased renal fxn. the result is increased circulating plasma volume |
|
|
Term
| how to nSAIDs contribute to renal toxicity? |
|
Definition
the medulla and cortex produce prostanoids which help modulate BP and salt excretion
COX2 prostoglandins typically increase blood flow and inhibit sodium reabsorption
COX 1 prostoglandins increase water excretion, salt excretion
the kidney also releases thromboxin and prostoglandins also increase renin (which will result in raising BP)
messing with COX messes with all these things and in an impaired individual, this is risky |
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|
Term
| how can you arrive at analgesic nephropathy |
|
Definition
| acetam + aspirin + caffeine or codeine increase the risk of kidney damage |
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|
Term
|
Definition
if the patient has aspirin hypersensitivity, do not give any other nSAIDs
cross-sensitivity has been linked to life threatening conditions
it's been associated with broncial constriction |
|
|
Term
|
Definition
besides AV closure, NSAIDs can prolong pregancy bc they inhibit prostoglandins which facilitate contractions
oligohydramnios (too little amino fluid)
NSAIDs can be detected in breast milk |
|
|
Term
| tested NSAIDs for juvenile arthritis |
|
Definition
| naproxen, indomethacin, tolmetin, meloxicam, celecoxib |
|
|
Term
|
Definition
some herbal drugs lke motherwort and gink biloba, garil and hawthorn can decrease coagulation
displacement of previously plasma bound anticoagulants by aspirin is a concern. do not want to release methotrexate (bone marrow suppression, GI toxicity, renal toxicity), warfarin |
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|
Term
| how are NSAIDs typically metabolized? |
|
Definition
through glucuronidation and by CYP3A, CYP2C families
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|
|
Term
| some other unintended interactions of NSAIDs? |
|
Definition
Selective serotonin receptor inhibitors= seretonin stimulates platelet aggregation and vasodialation, inhibitors can cause bleeding (somehow this includes NSAIDs)
NSAIDs can increase the reabsorption of Lithium, which is dangerous bc it has such a narrow therapeutic index |
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|
Term
| configuration wise, what makes aspirin effective? |
|
Definition
| its ability to acetylate and it's hydroxyl group in the ortho position |
|
|
Term
| what is a risky characteristic of salicylate? |
|
Definition
it is saturatable , therefore, there comes a point when a small increase in the conc of salicylate can lead to toxicity
salicylate metalism occures primarily in the hepatic ER and mitochondria by glucouronide conjugation. this metabolism is what is saturable |
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|
Term
| what is synthesized with COX-2 is acetylated? |
|
Definition
15(R)-HETE which can be metabolized by 5-LOX to yield 15-epilipoxin A4
this has potent anti-inflammatory properties through the inhibition of leukocyte activation
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|
Term
| why is salicylic acid a competitive inhibitor of arachadonic acid? |
|
Definition
| because it doesn't have an acetyl group |
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|
Term
|
Definition
the effects achieved depend on the dose given.
effects from pain and fever reduction -> anti-inflamation -> anti-inflammation caused by rheumatic disease requires increasing doses |
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|
Term
| aspirin and children with viral diseases |
|
Definition
| there is a concern that encephalopathy can take place or severe hepatic injury (as in reyes syndrome) |
|
|
Term
|
Definition
a disease of children with acute vasculitis
since aspirin can reduce inflammation and can help neutralize circulating myelin Abs which can downregulate proinflmmatory cytokines, it is considered a viable therapy |
|
|
Term
| how does aspirin affect skin flushing |
|
Definition
it prevents the leases of PGD from the skin
PGD release is caused by naicin sensitivity |
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|
Term
| salicylates and respiration |
|
Definition
they are capable of uncoupling Ox Phos which will cause an increase in CO2 production and a need to deeper, more frequent breathing
-liver and muscle glycogen can be depleted, excessive heat generation
-primary respiratory alkalosis can ensure of the partial pressure of CO2 falls too low due to increased respiratory rate and depth |
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|
Term
| why avoid aspirin treatment for the gout? |
|
Definition
| low doses can inhibit urate excretion and high doses can increase the risk of renal calculi by increasing urate excretion |
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|
Term
| what features of the aspirin triad contraindicate its use? |
|
Definition
asthma, rhinitis, and nasal polyps. if a patient has these things, 10-25% of them will have aspirin hypersensitivity leading to production of leukotrienes
aso, laryngeal edema, angioedema, urticaria, and hypotension |
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|
Term
| some symptoms of salicylate toxicity: |
|
Definition
nausea, vomiting, diaphoresis, tinnitus
vertigo, hyperventilation, tachycardia, hyperactivity
delirium, hallucinations, convulsions, stupor |
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|
Term
| acetaminophen (not really an NSAID) |
|
Definition
oral, rectal, IV, rapid onset, low plasma binding, almost totally metabolized in liver by CYP ox,
slight use for anti-inflam but not considered one,
does not affect platelets
MOA: inhibits COX in CNS
reduced-glutathione sequesters a metabolite form of acetam., NAPQI which is reactive and needs to be neutralized, but this takes it out of circulation. this contributes to the hepato-toxicity
also, chronic abuse is associated with renal papillary necrosis |
|
|
Term
| what is an antidote for acetaminophen toxicity? |
|
Definition
| acetylecysteine. maybe through detoxicifying the metabolites or by regenerating GSH |
|
|
Term
| CYP induction by acetaminophen |
|
Definition
| inducers, such as carbamazepine and phenytoin, and ethanol (CYP2E1) increase the metabolism of APAP which increases NAPQ1 concentrations which we know is an unwanted reactive metabolite of the drug |
|
|
Term
| warfarin and acetaminophen |
|
Definition
there is not a large effect of acetaminophen on the anticoagulation effects of warfarin.
unless there is a better alternative, acetaminophen is the anti-inflammatory analgesic drug of choice for patients who are taking warfarin
warfarin is usually heavily protein bound and some NSAIDs |
|
|
Term
|
Definition
Constitutively expressed in most cells
Responsible for “housekeeping” forms of processes:
›Vascular homeostasis
›Maintenance of renal and gastrointestinal blood flow
›Renal function
›Intestinal mucosal proliferation
›Antithrombogenesis |
|
|
Term
|
Definition
Inducible enzyme
Responsible for “as needed” processes
Up-regulated when stimulated by:
› cytokines and growth factors during inflammation or pain transduction
›Mitogenesis required in the GI epithelium
›Renal adaptation to stress
›Deposition of trabecular bone
›Ovulation
›Placentation
›Uterine contractions of labor |
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|
Term
| some drugs which show COX-2 selectivity, but are not necessarily classified as COX-2 selective drugs |
|
Definition
Meloxicam, Diclofenac, and Etodolac. |
|
|
Term
| what are the only two drugs that should be used to close the ductus arteriosus? |
|
Definition
indomethacin
and
ibuprofen
|
|
|
Term
| what does the increased lipophilicity of NSAIDs result in? |
|
Definition
| increased CNS penetration |
|
|
Term
| primary metabolism of NSAIDS |
|
Definition
›Hepatic biotransformation
P450 à CYP3A or CYP2C |
|
|
Term
| Two drug interactions of NSAIDs that risk GI complications? |
|
Definition
žCorticosteroids use and žSerotonin Selective Reuptake Inhibitors (SSRIs) |
|
|
Term
|
Definition
acetic acid derivative
20x more potent than aspirin, therefore, too strong for analgesic effects, better for fever if nothing else works
sometimes severe side effects, many of which are CNS |
|
|
Term
|
Definition
acetic acid derivative
potent analgesic/poor anti-inflammatory
not for use if there is an ASPIRIN ALLERGY
good for topical allergy conjunctivitis
potentially dangerous GI, renal, and bleeding complications
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|
|
Term
|
Definition
acetic acid deriviative
COX-2 selective (however, still some GI side-effects)
available in many forms (oral, dermal, rectal)
hepatic transaminase levels MUST be monitored because they are elevated
black box warning for CV side effects
NOT for the pregnant or nursing |
|
|
Term
| propionic acid derivatives |
|
Definition
naproxen and ibuprofen
naproxen is aleve. it is popular because it has a relatively long half life
ibuprofen is an effective anaglesic, is injectable, can close the ductus arteriosus
effects of both are similar to aspirin, but generally better tolerated |
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|
Term
why are COX2 selective drugs selective?
name one |
|
Definition
celecoxib (celebrex) all COX-2 selectives end with "coxib"
- it has a sulfamide group, therefore, people with sulfa allergies cannot take
- the elderly develop a higher peak conc. therefore cannot give yound and old same dose
the coxibs have a hydrophobic AA side chain that fits into the allosteric site of COX-2 which is bigger than the site on COX-1, therefore, it cannot fit in COX1's
not proven to be more effacious than other NSAIDs, but fewer GI problems |
|
|
Term
|
Definition
Meclofenamate
›Diarrhea associated with steatorrhea and inflammation of bowel (common)
›elevation of hepatic transaminases (but reversible)
›Autoimmune hemolytic anemia can occur but very rare |
|
|
Term
what is the goal of enolic acid derivates?
name one |
|
Definition
to try and decrease GI side effects
to have a longer half life so they are one-a-days
meloxicam |
|
|
Term
| how does aspirin evoke CNS effects? |
|
Definition
The CNS triggers hyperventilation
hyperventilation will decrease the partial pressure of CO2 leading to an increase in bicarbonate conc and increased pH
along with this is metabolic acidosis caused by interference with the kreb cycle and increases in lactic acid
these effects of hyperventiliation are the most common acid/base distuburbances seen in ill pts. |
|
|
Term
| how is aspirin activated? |
|
Definition
| it is hydrolyzed to salicyclic acid by plasma esterases |
|
|
Term
| what can 40 mg of ASA do? |
|
Definition
| inhibit the COX for 8-11 days of the lifespan of platelets |
|
|
Term
| why can ASA toxicity cause fever? |
|
Definition
due to an uncoupling of the ETC (causing non-shivering thermogenesis)
there will be deceased CO2 production, increased O2 consumption, depletion of liver glycogen
fever is often a PREMORBID sign |
|
|
Term
| how can respiratory alkylosis present in children or infants suffering from salicyclism? |
|
Definition
| it may present very subtly or not at all. it may occur quickly and with a short duration so it may have already passed by the time of evaulation |
|
|
Term
| chronic ASA toxicity in the elderly |
|
Definition
•Some overlap of symptoms with slow appearance and less severe appearance
*Frequent misdiagnosed is the elderly |
|
|
Term
|
Definition
| it's a non-specific symptom seen in ASA toxicity in which a patient hear's ringing in their ear |
|
|
Term
| significance of tachycardia experienced by patients with high ASA doses |
|
Definition
| not very clinical signifcant, but a sign effect of doses that are too high |
|
|
Term
|
Definition
it is a lower than normal amount of potassium in the blood and this can be a complication in patients whose ASA toxicity is being treated with alkalation of the urine if enough potassium is not provided
this lack of potassium will cause the tubules to reabsorb it in exchange for H+ ions. this prevents the excretion of alkaline urine
a single bolus of sodium carbonate with a steady infusion of KCl is recommended |
|
|
Term
| what is the active ingredient in bengay? |
|
Definition
methyl salicylic acid. it can be highly toxic too. one tablespoon could kill a small child.
usually used topically, much safer this way |
|
|
Term
| what are toxic levels of salicylates often seen? |
|
Definition
after 6 hours.
despite the early onset of effects, peak plasma conc may not be seen for 18-24 hours.
all the therapeutic effects of salicylates take place under first order kinetics, but it turn to zero-order kinetics once it is in toxic range |
|
|
Term
| what does alkalyzing urine do? |
|
Definition
| shifts the equilibrium of salicylic acid to the ionized form where charge exists. renal excretion will be the primary method of drug removal in an OD |
|
|
Term
| ingestion limits for aspirin |
|
Definition
no more than 650/4hrs, except initially dose can be up to 1000
goal is to reach 15-30 mg/dl |
|
|
Term
| what are the limits of the Done nomogram? |
|
Definition
assumes the drug conc is based on a single high dose, not chronic use
monitoring of toxicity must take place >6 hrs. after ingestion
above 50 mg/dl is mild tox, >110 is severe
the test is NOT the gold standard, has many flaw, but may serve use
time-release drugs can throw off the conc readings |
|
|
Term
| a quick way to test for salicylate use? |
|
Definition
| a ferric chloride test and phenistix test, only tests for presence of, not toxicity |
|
|
Term
| induction of vomitting in the ER? |
|
Definition
| charcoal has been shown to be superior to ipecac |
|
|
Term
| servicing the dehydration of a patient with an OD |
|
Definition
| forced diauresis is not recommended bc it will make urine harder to alkalyze and will just dilute the urine without affecting absportion of the ASA |
|
|
Term
| when might hemodialysis be necessary in an ASA OD? |
|
Definition
when the acidosis is refractory
when the there is severe manifestation of toxicity |
|
|
Term
| important note about APAP and pregnancy |
|
Definition
|
|
Term
|
Definition
| when the normal metabolism which converts APAP to gluconoride and sulfate is overwhelmed, the only channel left is the NAPQI channel |
|
|
Term
| phase 1 of APAP toxicity? |
|
Definition
Phase 1 of acute acetaminophen toxicity begins within 30 minutes of ingestion and may last for 12-24 hours.
•Anorexia, nausea, and vomiting are the most common symptoms and are due to local effects of acetaminophen on the gastrointestinal tract.** Diaphoresis and pallor
•Clinicians should be aware that some patients can be completely asymptomatic during the first phase of acetaminophen toxicity, even following ingestion of significant amounts of the drug. *** |
|
|
Term
|
Definition
•assymptomatic
Phase 2 of acute acetaminophen toxicity occurs 24-72 hours following ingestion and is a relatively asymptomatic period. Most of the gastrointestinal symptoms observed during Phase 1 will have subsided, but the patient may complain of right upper quadrant abdominal pain as a result of early hepatic necrosis.
•Laboratory evidence of abnormal hepatic function may appear, including increased levels of liver enzymes and bilirubin and prolonged prothrombin time. |
|
|
Term
|
Definition
•Phase 3 of acute acetaminophen toxicity occurs at 72-96 hours after ingestion and represents the manifestation of hepatic necrosis. Patients with extensive hepatic necrosis develop nausea, vomiting, jaundice, and hepatomegaly, and hepatic encephalopathy and coagulopathy may ensue. Laboratory findings include marked elevations of liver enzymes and bilirubin, and prolonged prothrombin time.
•Patients with irreversible liver damage secondary to acetaminophen toxicity may develop progressive clinical deterioration and a variety of severe complications, including hypotension, renal failure, lactic acidosis, hemorrhage, hypoglycemia, and markedly prolonged prothrombin time. Mortality usually is related to fulminant hepatic failure and increased intracranial pressure. |
|
|
Term
|
Definition
•Phase 4. Patients surviving Phase 3 of acute acetaminophen toxicity enter Phase 4 (the recovery phase) which occurs from day four to two weeks following acute ingestion. For patients with reversible hepatic necrosis, complete resolution of liver damage and hepatic dysfunction occurs during this time frame. |
|
|
Term
| explain the 4, 75, 150 rule |
|
Definition
obtain serum level 4 hours after ingestion
7.5 gm is toxic dose in adults
150 mg/kg is toxic dose in kids
serum levels above 150 ug/ml is toxic range
no need to keep repeating levels after initial
liver damage in hepatic zone III |
|
|
Term
| how does acetylcystine work? |
|
Definition
it works as a GSH substitute and increases the GSH supply
does not affect NAPQI production however
use w/n first 24 hours |
|
|
Term
| what is mandatory during a gastrointestinal exam when NSAID related symptoms are suspected? |
|
Definition
|
|
