ection administration to lessen the risk of bradycardia [ see dosage and administration ( 2.4 ) ]. 5.2 cardiovascular complications cardiac arrhythmias, nonspecific electrocardiogram changes, cardiac arrest, syncope and hypotension have been reported with neostigmine methylsulfate. in patients with certain cardiovascular conditions such as coronary artery disease, cardiac arrhythmias or recent acute coronary syndrome, the risk of blood pressure and heart rate complications may be increased. risk of these complications may also be increased in patients with myasthenia gravis. standard antagonism with anticholinergics (e.g., atropine) is generally successful to mitigate the risk of cardiovascular complications. 5.3 hypersensitivity (anaphylaxis) hypersensitivity reactions including anaphylaxis have been reported with neostigmine. ensure that appropriate medical support measures, including atropine, cardiopulmonary resuscitation equipment, and medications to treat anaphylaxis are readily available. 5.4 neuromuscular dysfunction neuromuscular dysfunction has been associated with administration of large doses of neostigmine when neuromuscular blockade is minimal. to mitigate the risk of neuromuscular dysfunction, consider reducing the dose of neostigmine if recovery from neuromuscular blockade is nearly complete. 5.5 cholinergic crisis overdosage of neostigmine may cause cholinesterase inhibitor toxicity or cholinergic crisis which may be difficult to differentiate from myasthenia crisis since both conditions present with similar symptoms. both conditions result in extreme muscle weakness but require radically different treatments. cholinergic crisis requires immediate withdrawal of all anticholinergic medication and immediate use of atropine [ see overdosage ( 10 ) ].

to or concomitantly with neostigmine methylsulfate ( 2.4 ) dose of anticholinergic agent (atropine or glycopyrrolate) administer atropine sulfate (~15 mcg/kg) or glycopyrrolate (~10 mcg/kg) intravenously either several minutes before or concomitantly with neostigmine methylsulfate (using separate syringes) ( 2.4 ) 2.1 important dosage and administration instructions neostigmine should be administered by trained healthcare providers familiar with the use, actions, characteristics, and complications of neuromuscular blocking agents (nmba) and neuromuscular block reversal agents. prior to neostigmine methylsulfate injection administration and up until complete recovery of normal ventilation, the patient should be well ventilated and a patent airway maintained. use a peripheral nerve stimulator capable of delivering a train-of-four (tof) stimulus to evaluate the extent of recovery of neuromuscular function, and to determine the time of the first dose and the need for additional doses of neostigmine methylsulfate injection. prior to the administration of neostigmine methylsulfate injection, there must be a twitch response to the first stimulus in the tof of at least 10% of its baseline level (i.e., the response prior to nmba administration). dose selection should be based on the extent of spontaneous recovery at time of injection, half-life of the neuromuscular blocking agent (nmba) to be reversed, and need for rapid nmba reversal. patients should continue to be monitored for adequacy of reversal of the effect of nmbas for a period of time that would assure full recovery based on the patient’s medical condition and the pharmacokinetics of neostigmine and the nmba used. neostigmine methylsulfate injection is administered by intravenous bolus injection. additional, carefully adjusted bolus doses are administered according to the patient’s response. an anticholinergic agent (e.g., atropine or glycopyrrolate) should be administered prior to or concomitantly with neostigmine methylsulfate injection [ see dosage and administration ( 2.4 ), warnings and precautions ( 5.5 ) ]. tof monitoring alone should not be relied upon to determine the adequacy of reversal of neuromuscular blockade. satisfactory recovery should be judged by the patient’s ability to maintain a patent airway, adequacy of ventilation, and skeletal muscle tone. 2.2 recommended dosage in adults the recommended dose range of neostigmine methylsulfate injection is 0.03 mg/kg to 0.07 mg/kg administered as an intravenous bolus. a dose less than 0.04 mg/kg is recommended for reversal of the effect of nmbas with shorter half-lives (e.g., rocuronium), or when the first twitch response to the tof stimulus is substantially greater than 10% of baseline, or when a second twitch is present. a dose of 0.07 mg/kg is recommended for the reversal of the effect of nmbas with longer half-lives (e.g., vecuronium or pancuronium), or when first twitch response is not substantially greater than 10% of baseline, or if there is need for more rapid recovery. additional doses may be required. the recommended maximum total dose is 0.07 mg/kg or up to a total of 5 mg, whichever is less. 2.3 recommended dosage in pediatric patients including neonates adult guidelines should be followed when neostigmine methylsulfate injection is administered to pediatric patients. pediatric patients require neostigmine methylsulfate injection doses similar to those for adult patients. 2.4 concomitant or pre-administration of anticholinergic agents an anticholinergic agent (e.g., atropine sulfate or glycopyrrolate) should be administered intravenously several minutes prior to or with neostigmine methylsulfate injection administration using separate syringes. for bradycardic patients, the anticholinergic agent should be administered prior to neostigmine methylsulfate injection.

recovery at time of injection, half-life of the neuromuscular blocking agent (nmba) to be reversed, and need for rapid nmba reversal. patients should continue to be monitored for adequacy of reversal of the effect of nmbas for a period of time that would assure full recovery based on the patient’s medical condition and the pharmacokinetics of neostigmine and the nmba used. neostigmine methylsulfate injection is administered by intravenous bolus injection. additional, carefully adjusted bolus doses are administered according to the patient’s response. an anticholinergic agent (e.g., atropine or glycopyrrolate) should be administered prior to or concomitantly with neostigmine methylsulfate injection [ see dosage and administration ( 2.4 ), warnings and precautions ( 5.5 ) ]. tof monitoring alone should not be relied upon to determine the adequacy of reversal of neuromuscular blockade. satisfactory recovery should be judged by the patient’s ability to maintain a patent airway, adequacy of ventilation, and skeletal muscle tone.

nticholinergic agent, e.g., atropine sulfate or glycopyrrolate, may prevent or mitigate these reactions. quantitative adverse event data are available from trials of neostigmine methylsulfate in which 200 adult patients were exposed to the product. adverse reactions that occurred with an overall frequency of 1% or greater included the following: allergic: allergic reactions and anaphylaxis. neurological: dizziness, syncope, weakness, convulsions, loss of consciousness, drowsiness, headache, dysarthria, miosis and visual changes. cardiovascular: cardiac arrhythmias including bradycardia, tachycardia, atrioventricular block and nodal rhythm, as well as cardiac arrest, and hypotension. respiratory: increased oral, pharyngeal and bronchial secretions, dyspnea, respiratory depression, oxygen desaturation, respiratory arrest and bronchospasm. dermatologic: diaphoresis, flushing, rash, pruritus, and urticaria. gastrointestinal: dry mouth, nausea, emesis, flatulence and increased peristalsis. genitourinary: increased urinary frequency. musculoskeletal: muscle cramps and spasm, arthralgia. psychiatric: insomnia general: incision site complication, pharyngolaryngeal pain, procedural complication, procedural pain 6.2 post-marketing experience the following adverse reactions have been identified during parenteral use of neostigmine methylsulfate. because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to drug exposure. allergic disorders: allergic reactions, anaphylaxis nervous system disorders: convulsions, drowsiness, dysarthria, fasciculation, loss of consciousness, miosis, visual changes cardiovascular disorders: cardiac arrest, cardiac arrhythmias (a-v block, nodal rhythm), hypotension, nonspecific ekg changes, syncope respiratory, thoracic and mediastinal disorders: bronchospasm; increased oral, pharyngeal and bronchial secretions; respiratory arrest; respiratory depression skin and subcutaneous tissue disorders: rash, urticaria diaphoresis, flushing gastrointestinal disorders: bowel cramps, diarrhea, flatulence, increased peristalsis renal and urinary disorders: urinary frequency musculoskeletal and connective tissue disorders: arthralgia, muscle cramps, spasms, weakness

tigmine may cause uterine irritability and induce premature labor when administered to pregnant women near term. neostigmine methylsulfate injection should be given to a pregnant woman only if clearly needed. data animal data in embryofetal development studies, rats and rabbits were administered neostigmine methylsulfate at human equivalent doses (hed, on a mg/m 2 basis) of 1.6, 4 and 8.1 mcg/kg/day 3.2, 8.1, and 13 mcg/kg/day, respectively, during the period of organogenesis (gestation days 6 through 17 for rats and gestation days 6 through 18 for rabbits). there was no evidence for a teratogenic effect in rats and rabbits up to hed 8.1 and 13 mcg/kg/day, which are approximately 0.097-times and 0.16-times the mrhd of 5 mg/60 kg, respectively in the presence of minimal maternal toxicity (tremors, ataxia, and prostration). the studies resulted in exposures in the animals well below predicted exposures in humans. in a pre- and postnatal development study in rats, neostigmine methylsulfate was administered to pregnant female rats at human equivalent doses (hed) of 1.6, 4 and 8.1 mcg/kg/day from day 6 of gestation through day 20 of lactation, with weaning on day 21. there were no adverse effects on physical development, behavior, learning ability, or fertility in the offspring occurred at hed doses up 8.1 mcg/kg/day which is 0.097-times the mrhd of 5 mg/60 kg on a mg/m 2 basis in the presence of minimal maternal toxicity (tremors, ataxia, and prostration). the studies resulted in exposures in the animals well below predicted exposures in humans. 8.2 lactation it is not known whether neostigmine methylsulfate injection is excreted in human milk. because many drugs are excreted in human milk and because of the potential for serious adverse reactions from neostigmine methylsulfate injection in nursing infants, a decision should be made whether to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother. 8.4 pediatric use data from published literature support the intravenous use of neostigmine methylsulfate for reversal of nondepolarizing neuromuscular blocking agents in all pediatric age groups. recovery of neuromuscular activity occurs more rapidly with smaller doses of cholinesterase inhibitors in infants and children than in adults. however, infants and small children may be at greater risk of complications from incomplete reversal of neuromuscular blockade due to decreased respiratory reserve. the risks associated with incomplete reversal outweigh any risk from giving higher doses of neostigmine methylsulfate (up to 0.07 mg/kg or up to a total of 5 mg, whichever is lower). the dose of neostigmine methylsulfate required to reverse neuromuscular blockade in children varies between 0.03 mg to 0.07 mg/kg, the same dose range shown to be effective in adults, and should be selected using the same criteria as used for adult patients [see clinical pharmacology ( 12.3 )]. since the blood pressure in pediatric patients, particularly infants and neonates is sensitive to changes in heart rate, the effects of an anticholinergic agent (e.g., atropine) should be observed prior to administration of neostigmine to lessen the probability of bradycardia and hypotension. 8.5 geriatric use elderly patients are likely to have decreased renal function, which may prolong the duration of action of neostigmine methylsulfate. however, elderly patients also experience slower spontaneous recovery from neuromuscular blocking agents. therefore, dosage adjustments are generally not needed in geriatric patients; however, they should be monitored for longer periods than younger adults to assure additional doses of neostigmine methylsulfate injection are not required. the duration of monitoring should be predicated on the anticipated duration of action for the neuromuscular blocking agents used on the patient. 8.6 renal impairment elimination half-life of neostigmine was prolonged in anephric patients compared to normal subjects, so neostigmine concentration may increase in patients with impaired renal functions. although no adjustments to neostigmine methylsulfate injection dosing appear to be warranted in patients with impaired renal function, they should be closely monitored for a longer period of time. to assure the effects of the neuromuscular blocking agent, particularly one cleared by the kidneys, do not persist beyond those of neostigmine methylsulfate injection, the interval for re‐dosing the neuromuscular blocking agent during the surgical procedure may be useful in determining whether, and to what extent, post‐operative monitoring needs to be extended. 8.7 hepatic impairment the pharmacokinetics of neostigmine methylsulfate in patients with hepatic impairment have not been studied. neostigmine is metabolized by microsomal enzymes in the liver so neostigmine concentration may increase in patients with impaired hepatic functions. although no adjustments to the dosing of neostigmine methylsulfate injection appear to be warranted in patients with hepatic insufficiency, patients should be carefully monitored for a longer period of time. if hepatically cleared neuromuscular blocking agents were used during the surgical procedure, their duration of action may also be prolonged by hepatic insufficiency. this could result in the effects of the neuromuscular blocking agent outlasting those of neostigmine methylsulfate injection. in this regard, the interval for re-dosing the neuromuscular blocking agent during the surgical procedure may be useful in determining whether, and to what extent, post-operative monitoring needs to be extended.

rm. neostigmine methylsulfate injection should be given to a pregnant woman only if clearly needed. data animal data in embryofetal development studies, rats and rabbits were administered neostigmine methylsulfate at human equivalent doses (hed, on a mg/m 2 basis) of 1.6, 4 and 8.1 mcg/kg/day 3.2, 8.1, and 13 mcg/kg/day, respectively, during the period of organogenesis (gestation days 6 through 17 for rats and gestation days 6 through 18 for rabbits). there was no evidence for a teratogenic effect in rats and rabbits up to hed 8.1 and 13 mcg/kg/day, which are approximately 0.097-times and 0.16-times the mrhd of 5 mg/60 kg, respectively in the presence of minimal maternal toxicity (tremors, ataxia, and prostration). the studies resulted in exposures in the animals well below predicted exposures in humans. in a pre- and postnatal development study in rats, neostigmine methylsulfate was administered to pregnant female rats at human equivalent doses (hed) of 1.6, 4 and 8.1 mcg/kg/day from day 6 of gestation through day 20 of lactation, with weaning on day 21. there were no adverse effects on physical development, behavior, learning ability, or fertility in the offspring occurred at hed doses up 8.1 mcg/kg/day which is 0.097-times the mrhd of 5 mg/60 kg on a mg/m 2 basis in the presence of minimal maternal toxicity (tremors, ataxia, and prostration). the studies resulted in exposures in the animals well below predicted exposures in humans.

pressure in pediatric patients, particularly infants and neonates is sensitive to changes in heart rate, the effects of an anticholinergic agent (e.g., atropine) should be observed prior to administration of neostigmine to lessen the probability of bradycardia and hypotension.

and 1.4 l/kg following intravenous injection. elimination neostigmine is metabolized by microsomal enzymes in the liver and the observed elimination half-life reported is between 24 and 113 minutes. metabolism neostigmine is metabolized by microsomal enzymes in the liver. excretion the observed elimination half-life reported is between 24 and 113 minutes following intravenous injection. specific populations pediatric population: after intravenous administration as a 2-minute infusion (infants 2 to 10 months old: 100 mcg/kg; children 1 to 6 years old: 70 mcg/kg), the elimination half-life for infants and children were 39 ± 5 min and 48 ± 16 min (mean ± sd), respectively. clearance for infants and children were 13.6 ± 2.8 and 11.1 ± 2.7 ml/min/kg (mean ± sd), respectively. renal impairment elimination half-life was prolonged in anephric patients compared to normal subjects; elimination half-life for normal, transplant and anephric patients were 79.8 ± 48.6, 104.7 ± 64 and 181 ± 54 min (mean ± sd), respectively. hepatic impairment the pharmacokinetics of neostigmine in patients with hepatic impairment has not been studied. neostigmine is metabolized by microsomal enzymes in the liver and its concentration may increase in patients with impaired hepatic functions. drug interactions the pharmacokinetic interaction between neostigmine and other drugs has not been studied. neostigmine concentration may increase or decrease if concomitantly used drugs inhibit or induce the activity of metabolizing enzymes or transporters, respectively.

fe was prolonged in anephric patients compared to normal subjects; elimination half-life for normal, transplant and anephric patients were 79.8 ± 48.6, 104.7 ± 64 and 181 ± 54 min (mean ± sd), respectively. hepatic impairment the pharmacokinetics of neostigmine in patients with hepatic impairment has not been studied. neostigmine is metabolized by microsomal enzymes in the liver and its concentration may increase in patients with impaired hepatic functions. drug interactions the pharmacokinetic interaction between neostigmine and other drugs has not been studied. neostigmine concentration may increase or decrease if concomitantly used drugs inhibit or induce the activity of metabolizing enzymes or transporters, respectively.