Paracetamol
Paracetamol (INN)
or acetaminophen (USAN), is a common analgesic and antipyretic drug that is
used for the relief of fever, headaches, and other minor aches and pains.
Paracetamol is also useful in managing more severe pain, allowing lower dosages
of additional NSAID or opioid analgesics to be used, so minimizing overall
side-effects. It is a major ingredient in numerous cold and flu medications and
many prescription analgesics. It is remarkably safe in recommended doses, but
because of its wide availability, deliberate or accidental overdoses are fairly
common.
Common brand names for the drug include Herron in Australia,
Tylenol in Canada, South Korea and the US, Paralen in the Czech Republic and
Slovakia, Panadol in Australia, New Zealand, Malaysia, Hong Kong, the UK,
Portugal and Singapore, Doliprane, Dafalgan, and Efferalgan in France,
Tachipirina and Efferalgan in Italy, Crocin in India, Gelocatil in Spain,
Alvedon in Sweden, Panodil and Pinex in Denmark and Iceland, Pinex and Paracet
in Norway and Depon in Greece.
The words acetaminophen and paracetamol both come from the
chemical names for the compound: N-acetyl-para-aminophenol and
para-acetyl-amino-phenol. In some contexts, it is shortened to apap, for
N-acetyl-para-aminophenol.
Available forms
Panadol, which is marketed in Europe, Asia, Central America,
and Australasia, is the most widely available
brand, sold in over 80 countries. In North America,
paracetamol is sold in generic form (usually labelled as acetaminophen) or
under a number of trade names: for instance Tylenol (McNeil-PPC, Inc),
Anacin-3, Tempra, and Datril.
In some formulations paracetamol is combined with the opioid
codeine, sometimes referred to as co-codamol (BAN). In the United States and Canada,
this is marketed under the name of Tylenol #1/2/3/4 and in the US is only available by prescription, while the
lowest strength is over-the-counter in Canada. In the UK and in many
other countries, this combination is marketed under the names of Tylex CD and
Panadeine. Other names include Captin, Disprol, Dymadon, Fensum, Hedex,
Mexalen, Nofedol, Paralen, Pediapirin, Perfalgan, and Solpadeine. Paracetamol
is also combined with other opioids such as dihydrocodeine, referred to as
co-dydramol (BAN), oxycodone or hydrocodone, marketed in the U.S. as
Percocet and Vicodin, respectively. Another very commonly used analgesic
combination includes acetaminophen in combination with propoxyphene napsylate,
sold under the brand name Darvocet. A combination of paracetamol, codeine, and
the calmative doxylamine succinate is marketed as Syndol or Mersyndol.
Acetaminophen is commonly used in multi-ingredient
preparations for migraine headache, typically including butalbital and
acetaminophen with or without caffeine, and sometimes containing codeine. In
the US,
these anti-migraine products are marketed under the brand name Fioricet.
500 mg Panadol
suppositoriesIt is commonly administered in tablet, liquid suspension,
suppository or intravenous form. The common adult dose is 500 mg to 1000 mg.
The recommended maximum daily dose, for adults, is 4 grams. In recommended
doses paracetamol is safe for children and infants as well as for adults.
The effectiveness of paracetamol is often underestimated
because of its widespread availability.
Mechanism of action
Tablets are the most
common form of paracetamol.Paracetamol has long been suspected of having a
similar mechanism of action to aspirin because of the similarity in structure.
That is, it has been assumed that paracetamol acts by reducing production of
prostaglandins, which are involved in the pain and fever processes, by
inhibiting the cyclooxygenase (COX) enzyme.
However, there are important differences between the effects
of aspirin and those of paracetamol. Prostaglandins participate in the
inflammatory response which is why it has been known to trigger symptoms in
asthmatics, but paracetamol has no appreciable anti-inflammatory action and
hence does not have this side-effect. Furthermore, COX also produces
thromboxanes, which aid in blood clotting - aspirin reduces blood clotting, but
paracetamol does not. Finally, aspirin and the other NSAIDs commonly have
detrimental effects on the stomach lining, where prostaglandins serve a
protective role, but paracetamol is safe.
Indeed, while aspirin acts as an irreversible inhibitor of
COX and directly blocks the enzyme's active site, paracetamol indirectly blocks
COX, and that this blockade is ineffective in the presence of peroxides.
This might explain why paracetamol is effective in the central nervous system
and in endothelial cells but not in platelets and immune cells which have high
levels of peroxides.
In 2002 it was reported that paracetamol selectively blocks
a variant of the COX enzyme that was different from the then known variants
COX-1 and COX-2. This enzyme, which is only expressed in the brain and the
spinal cord, is now referred to as COX-3. Its exact mechanism of action is
still poorly understood, but future research may provide further insight into
how it works.
A single study has shown that administration of paracetamol
increases the bioavailability of serotonin (5-HT) in rats, but the mechanism
is unknown and untested in humans.
Metabolism
Paracetamol is metabolized primarily in the liver, where
most of it (60-90% of a therapeutic dose) is converted to inactive compounds by
conjugation with sulfate and glucuronide, and then excreted by the kidneys.
Only a small portion (5-10% of a therapeutic dose) is metabolized via the
hepatic cytochrome P450 enzyme system (specifically CYP2E1); the toxic effects
of paracetamol are due to a minor alkylating metabolite
(N-acetyl-p-benzo-quinone imine, abbreviated as NAPQI) that is produced through
this enzyme, not paracetamol itself or any of the major metabolites. The
metabolism of paracetamol is an excellent example of toxication, because the
metabolite NAPQI is primarily responsible for toxicity rather than paracetamol
itself.
At usual doses, the toxic metabolite NAPQI is quickly
detoxified by combining irreversibly with the sulfhydryl groups of glutathione
to produce a non-toxic conjugate that is eventually excreted by the kidneys.
Comparison with
NSAIDs
Paracetamol, unlike other common analgesics such as aspirin
and ibuprofen, has no anti-inflammatory properties, and so it is not a member
of the class of drugs known as non-steroidal anti-inflammatory drugs (NSAIDs).
In recommended doses, paracetamol does not irritate the lining of the stomach,
affect blood coagulation as much as NSAIDs, or affect function of the kidneys.
Paracetamol is safe in pregnancy, and does not affect the
closure of the foetal ductus arteriosus (as NSAIDs can). Unlike aspirin, it is
safe in children as paracetamol is not associated with a risk of Reye's
syndrome in children with viral illnesses.
Like NSAIDs and unlike opioid analgesics, paracetamol has
not been found to cause euphoria or alter mood in any way. Paracetamol and
NSAIDs have the benefit of bearing a low risk of addiction, dependence,
tolerance and withdrawal.
Paracetamol, particularly in combination with weak opioids,
is more likely than NSAIDs to cause rebound headache (medication overuse
headache), although less of a risk than ergotamine or triptans used for
migraines.
Toxicity
Paracetamol has a narrow therapeutic index - the therapeutic
dose is close to the toxic dose. Additionally, paracetamol is contained in many
preparations (both over-the-counter and prescription only medications). This
means that, despite being one of the safest analgesics available at recommended
doses, there is a large potential for overdose and toxicity. Without timely
treatment, paracetamol overdose can lead to liver failure and death within
days. Because of the wide over-the-counter availability of the drug, it is
sometimes used in suicide attempts by those unaware of the prolonged
timecourse, and high morbidity (incidence rate or prevalence rate?) associated
with paracetamol-induced toxicity.
In the UK,
sales of over-the-counter Paracetamol in pharmacies are restricted to packs of
32 tablets per customer per occasion (only 16 tablets in non-pharmacy stores).
In Ireland,
the limits are 24 and 12 tablets respectively.
Mechanism of toxicity
As discussed above in the section regarding metabolism,
paracetamol is mostly converted to inactive compounds via Phase II metabolism
by conjugation with sulfate and glucuronide, with a small portion being
oxidized via the cytochrome P450 enzyme system. Cytochrome P450 2E1 (CYP2E1)
converts paracetamol to a highly reactive intermediary metabolite,
N-acetyl-p-benzo-quinone imine (NAPQI).
Under normal conditions, NAPQI is detoxified by conjugation
with glutathione. In cases of paracetamol toxicity, the sulfate and glucuronide
pathways become saturated, and more paracetamol is shunted to the cytochrome
P450 system to produce NAPQI. As a result, hepatocellular supplies of
glutathione become exhausted and NAPQI is free to react with cellular membrane
molecules, resulting in widespread hepatocyte damage and death, clinically
leading to acute hepatic necrosis. In animal studies, 70% of hepatic
glutathione must be depleted before hepatotoxicity occurs.
Toxic dose
The toxic dose of paracetamol is highly variable. In adults,
single doses above 10 grams or 150 mg/kg have a reasonable likelihood of
causing toxicity. Toxicity can also occur when multiple smaller doses within
24 hours exceeds these levels, or even with chronic ingestion of doses as low
as 4 g/day, and death with as little as 6 g/day.
In children acute doses above 200 mg/kg could potentially
cause toxicity. This higher threshold is largely due to children having
relatively larger kidneys and livers than adults and hence being more tolerant
of paracetamol overdose than adults. Acute paracetamol overdose in children
rarely causes illness or death with chronic supratherapeutic doses being the
major cause of toxicity in children.
Since paracetamol is often included in combination with
other drugs, it is important to include all sources of paracetamol when
checking a person's dose for toxicity. In addition to being sold by itself,
paracetamol may be included in the formulations of various analgesics and
cold/flu remedies as a way to increase the pain-relieving properties of the
medication. To prevent overdoses, one should read medication labels carefully
for the presence of paracetamol and check with a pharmacist before using
over-the-counter medications.
Risk factors for
toxicity
Chronic excessive ethanol (alcohol) consumption can induce
CYP2E1, thus increasing the potential toxicity of paracetamol. For this
reason, other analgesics such as aspirin or ibuprofen are sometimes recommended
for hangovers.
Fasting is a risk factor, possibly because of depletion of
hepatic glutathione reserves.
It is well documented that concomitant use of the CYP2E1
inducer isoniazid increases the risk of hepatotoxicity, though whether CYP2E1
induction is related to the hepatotoxicity in this case is unclear.
Concomitant use of other drugs which induce CYP enzymes such as antiepileptics
(including carbamazepine, phenytoin, barbituates, etc) have also been reported
as risk factors.
Natural history
Individuals who have overdosed on paracetamol generally have
no specific symptoms for the first 24 hours. Although nausea, vomiting, and
diaphoresis may occur initially, these symptoms generally resolve after several
hours. After resolution of these symptoms, individuals tend to feel better, and
may believe that the worst is over. If a toxic dose was absorbed, after this
brief feeling of relative wellness, the individual develops overt hepatic
failure. In massive overdoses, coma and metabolic acidosis may occur prior to
hepatic failure.
Damage generally occurs in hepatocytes as they metabolize
the paracetamol. Rarely, acute renal failure also may occur. This is usually
caused by either hepatorenal syndrome or Multiple organ dysfunction syndrome.
Acute renal failure may also be the primary clinical manifestation of toxicity.
In these cases, it has been suggested that the toxic metabolite is produced
more in the kidneys than in the liver.
The prognosis of paracetamol varies depending on the dose
and the appropriate treatment. In some cases, massive hepatic necrosis leads to
fulminant hepatic failure with complications of bleeding, hypoglycaemia, renal
failure, hepatic encephalopathy, cerebral oedema, sepsis, multiple organ
failure, and death within days. In many cases, the hepatic necrosis may run its
course, hepatic function may return, and the patient may survive with liver
function returning to normal in a few weeks.
Diagnosis
Evidence of liver toxicity may develop in 1 to 4 days,
although in severe cases it may be evident in 12 hours. Right upper quadrant
tenderness may be present. Laboratory studies may show evidence of massive
hepatic necrosis with elevated AST, ALT, bilirubin, and prolonged coagulation
times (particularly, elevated prothrombin time). After paracetamol overdose,
when AST and ALT exceed 1000 IU/L, paracetamol-induced hepatotoxicity can be
diagnosed. However, the AST and ALT levels can exceed 10,000 IU/L. Generally
the AST is somewhat higher than the ALT in paracetamol-induced hepatotoxicity.
A drug nomogram was developed in 1975 which estimated the
risk of toxicity based on the serum concentration of paracetamol at a given
number of hours after ingestion. To determine the risk of potential
hepatotoxicity, the paracetamol level is traced along the standard nomogram. A
paracetamol level drawn in the first four hours after ingestion may
underestimate the amount in the system because paracetamol may still be in the
process of being absorbed from the gastrointestinal tract. Delay of the initial
draw for the paracetamol level to account for this is not recommended since the
history in these cases is often poor and a toxic level at any time is a reason
to give the antidote.
Treatment
Initial measures
The initial treatment for uncomplicated paracetamol
overdose, similar to any other overdose, is gastrointestinal decontamination.
In addition, the antidote, acetylcysteine plays an important role. Paracetamol
absorption from the gastrointestinal tract is complete within 2 hours under
normal circumstances, so decontamination is most helpful if performed within
this timeframe. Absorption may be somewhat slowed when it is ingested with
food. There is considerable room for physician judgement regarding
gastrointestinal decontamination, activated carbon administration is the most
commonly used procedure, however, gastric lavage may also be considered if the
amount ingested is potentially life threatening and the procedure can be
performed within 60 minutes of ingestion. Syrup of ipecac has no role in paracetamol
overdose because the vomiting it induces delays the effective administration of
activated carbon and oral acetylcysteine.
Activated carbon adsorbs paracetamol, reducing its
gastrointestinal absorption. Administering activated carbon also poses less
risk of aspiration than gastric lavage. Previously there was reluctance to give
activated carbon in paracetamol overdose, because of concern that it may also
absorb acetylcysteine. Studies have shown that no more than 39% of an oral
acetylcysteine is absorbed when they are administered together. Other
studies have shown that activated carbon seems to be beneficial to the clinical
outcome. It appears the most benefit from activated carbon is gained if it is
given with 2 hours of ingestion. However, administering activated carbon
later than this can be considered in patients who may have delayed gastric
emptying due to co-ingested drugs or following ingestion of sustained or
delayed release paracetamol preparations. Activated carbon should also be administered
if co-ingested drugs warrant decontamination. There are conflicting
recommendations regarding whether to change the dosing of oral
acetylcysteine after the administration of activated carbon, and even whether
the dosing of acetylcysteine needs to be altered at all.
Acetylcysteine
Acetylcysteine works to reduce paracetamol toxicity by
supplying sulfhydryl groups (mainly in the form of glutathione, of which it is
a precursor) to react with the toxic NAPQI metabolite so that it does not damage
cells and can be safely excreted.
If the patient presents less than 8 hours after paracetamol
overdose, then acetylcysteine significantly reduces the risk of serious
hepatotoxicity. If NAC is started more than 8 hours after ingestion, there is a
sharp decline in its effectiveness because the cascade of toxic events in the
liver has already begun and the risk of acute hepatic necrosis and death
increases dramatically. Although acetylcysteine is most effective if given
early, it still has beneficial effects if given as late as 48 hours after
ingestion. In clinical practice, if the patient presents more than 8 hours
after the paracetamol overdose, then activated charcoal is probably not useful,
and acetylcysteine is started immediately. In earlier presentations the doctor
can give charcoal as soon as the patient arrives, start giving acetylcysteine,
and wait for the paracetamol level from the laboratory.
In United
States practice, intravenous (IV) and oral
administration are considered to be equally effective. However, IV is the only
recommended route in Australasian and British practice.
Oral acetylcysteine is given as a 140 mg/kg loading dose
followed by 70 mg/kg every 4 hours for 17 more doses. Oral acetylcysteine may
be poorly tolerated due to its unpleasant taste, odour, and its tendency to
cause nausea and vomiting. It can be diluted to a 5% solution, from its
marketed 10% or 20% solutions, to improve palatability. Where oral
acetylcysteine is required, the inhalation formulation of acetylcysteine
(Mucomyst) is often given orally. The respiratory formulation can also be
diluted and filter sterilized by a hospital pharmacist for IV use, however this
is an uncommon practice. If repeat doses of charcoal are indicated because of
another ingested drug, then subsequent doses of carbon and acetylcysteine
should be staggered every two hours.
Intravenous acetylcysteine (Parvolex/Acetadote) is used as a
continuous intravenous infusion over 20 hours (total dose 300 mg/kg).
Recommended administration involves infusion of a 150 mg/kg loading dose over
15 minutes, followed by 50 mg/kg infusion over 4 hours; the last 100 mg/kg are
infused over the remaining 16 hours of the protocol. Intravenous acetylcysteine
has the advantage of shortening hospital stay, increasing both doctor and
patient convenience, and it allows administration of activated carbon to reduce
absorption of both the paracetamol and any co-ingested drugs without concerns
about interference with oral acetylcystine.
Baseline laboratory studies include bilirubin, AST, ALT, and
prothrombin time (with INR). Studies are repeated at least daily. Once it has
been determined that a potentially toxic overdose has occurred, acetylcysteine
is continued for the entire regimen, even after the paracetamol level becomes
undetectable in the blood. If hepatic failure develops, acetylcysteine should
be continued beyond the standard doses until hepatic function improves or until
the patient has a liver transplant.
Prognosis
The mortality rate from paracetamol overdose increases 2
days after the ingestion, reaches a maximum on day 4, and then gradually
decreases. Patients with a poor prognosis are usually identified for likely
liver transplantation. Acidemia is the most important single indicator of
probable mortality and the need for transplantation. A mortality rate of 95%
without transplant was reported in patients who had a documented pH of <
7.30. Other indicators of poor prognosis include renal insufficiency, grade 3
or worse hepatic encephalopathy, a markedly elevated prothrombin time, or a
rise in prothrombin time from day 3 to day 4. One study has shown that a factor
V level less than 10% of normal indicated a poor prognosis (91% mortality)
while a ratio of factor VIII to factor V of less than 30 indicated a good
prognosis (100% survival).
Source: wikipedia GFDL
