may occur. this possibility must be considered when administering anticholinesterase agents to antagonize neuromuscular blockade induced by nondepolarizing muscle relaxants. electrolyte imbalance and diseases which lead to electrolyte imbalance, such as adrenal cortical insufficiency, have been shown to alter neuromuscular blockade. depending on the nature of the imbalance, either enhancement or inhibition may be expected. magnesium salts, administered for the management of toxemia of pregnancy, may enhance the neuromuscular blockade. the possibility that such circumstances may interfere with the restoration of neuromuscular function should be considered when administering regonol ® .

f skeletal muscle tone, respiratory measurements, and by observation of the response to peripheral nerve stimulation. a patent airway should be maintained and manual or mechanical ventilation should be continued until complete recovery of normal respiration is assured. exposure to excessive amounts of benzyl alcohol has been associated with toxicity (hypotension, metabolic acidosis), particularly in neonates, and an increased incidence of kernicterus, particularly in small preterm infants. there have been rare reports of deaths, primarily in preterm infants, associated with exposure to excessive amounts of benzyl alcohol. the amount of benzyl alcohol from medications is usually considered negligible compared to that received in flush solutions containing benzyl alcohol. administration of high dosages of medications containing this preservative must take into account the total amount of benzyl alcohol administered. the amount of benzyl alcohol at which toxicity may occur is not known. if the patient requires more than the recommended dosages or other medications containing this preservative, the practitioner must consider the daily metabolic load of benzyl alcohol from these combined sources (see precautions: pediatric use ).

12 at lower doses, full recovery usually occurs within 15 minutes in most patients, although others may require a half-hour or more. when regonol ® is given intravenously to reverse the action of muscle relaxant drugs, it is recommended that atropine sulfate (0.6 to 1.2 mg) or an equipotent dose of glycopyrrolate be given immediately prior to or simultaneously with the administration of regonol ® . side effects, notably excessive secretions and bradycardia are thereby minimized. please refer to the appropriate prescribing information prior to the use of glycopyrrolate or atropine sulfate. to obtain maximum clinical benefits of regonol ® and to minimize the possibility of overdosage, the monitoring of muscle twitch response to peripheral nerve stimulation is advised. regonol ® should be administered after spontaneous recovery of neuromuscular function has begun. satisfactory reversal can be evident by adequate voluntary respiration, respiratory measurements and use of a peripheral nerve stimulator device. it is recommended that the patient be well-ventilated and a patent airway maintained until complete recovery of normal respiration is assured. once satisfactory reversal has been attained following administration of regonol ® , recurrence of paralysis is unlikely to occur. inadequate reversal of neuromuscular blockade by anticholinesterase drugs is possible with all curariform drugs, and is managed by manual or mechanical ventilation until recovery is judged adequate. the administration of additional doses of anticholinesterase reversal agents is not recommended since excessive dosages of such drugs may produce depolarizing block through their own pharmacological actions. use in pediatrics the safety and efficacy of regonol ® (pyridostigmine bromide injection, usp) in pediatric patients have not been established, therefore no dosing recommendations can be made (see precautions ).

may occur. this possibility must be considered when administering anticholinesterase agents to antagonize neuromuscular blockade induced by nondepolarizing muscle relaxants. electrolyte imbalance and diseases which lead to electrolyte imbalance, such as adrenal cortical insufficiency, have been shown to alter neuromuscular blockade. depending on the nature of the imbalance, either enhancement or inhibition may be expected. magnesium salts, administered for the management of toxemia of pregnancy, may enhance the neuromuscular blockade. the possibility that such circumstances may interfere with the restoration of neuromuscular function should be considered when administering regonol ® .

which toxicity may occur is not known. premature and low-birth-weight infants, as well as patients receiving high dosages, may be more likely to develop toxicity. practitioners administering this and other medications containing benzyl alcohol should consider the combined daily metabolic load of benzyl alcohol from all sources.

ose to blocking dose) is approximately 1:6 (see overdosage ). 3 the antagonism of neuromuscular blockade by anticholinesterase agents may be influenced by the degree of spontaneous recovery achieved when the reversal agent is administered, by the particular relaxant administered, acid-base balance, body temperature, electrolyte imbalance, concomitant medications such as potent inhalational anesthetics, antibiotics or other drugs which enhance or antagonize the action of nondepolarizing muscle relaxants. 4 the use of peripheral nerve stimulation to determine the degree of neuromuscular blockade is recommended in evaluating the effects of the reversal agents. failure of anticholinesterase agents to produce prompt (within 30 minutes) reversal of neuromuscular blockade may occur in the presence of extreme debilitation, carcinomatosis, and with concomitant use of certain broad-spectrum antibiotics, or anesthetic agents and other drugs which enhance neuromuscular blockade or cause respiratory depression through their own pharmacologic actions. as with other anticholinesterase agents, the administration of regonol® may be associated with muscarinic and nicotinic side effects, notably bradycardia and excessive bronchial secretions; the use of glycopyrrolate or atropine sulfate simultaneously with or prior to administration of regonol® is recommended to counteract these side effects (see dosage and administration ). 5 pharmacokinetics it has been postulated that the clearance of pyridostigmine is almost equally dependent on metabolism and on urinary elimination of the unchanged drug. 6 other studies in man indicated that approximately 75 percent of the plasma clearance of pyridostigmine is dependent on renal excretion and the remainder on nonrenal mechanisms. 7