ADReCS

Pharmaceutical Information

Drug Name	Pyridostigmine
Drug ID	BADD_D01881
Description	Myasthenia gravis is an autoimmune disease involving dysfunction at the neuromuscular junction, most commonly due to autoantibodies directed against the acetylcholine receptor (AChR), which results in muscle tone loss, muscle weakness, and fatigue.[A231004] Acetylcholinesterase inhibitors have been the symptomatic treatment of choice in myasthenia gravis since the 1930s with the early use of [physostigmine] and [neostigmine]. By inhibiting the breakdown of acetylcholine in the neuromuscular junction, they increase signalling and relieve symptoms.[A231004, L32408, L32413] Pyridostigmine is the current drug of choice, with superior pharmacokinetics and reduced side effects compared to [neostigmine].[L32408, L32413] In addition to treating myasthenia gravis, pyridostigmine is used to reverse neuromuscular blocks, relieve symptoms in congenital myasthenic syndromes, and protect against certain nerve agents, notably during the Gulf War.[A231009, A231014, L32413, L32418] Pyridostigmine was granted initial FDA approval on April 6, 1955, as an oral tablet. Possible dose forms have been expanded to include extended-release tablets, syrups, and injections, marketed under various brand and generic names.[L32408, L32413]
Indications and Usage	Pyridostigmine is indicated for the treatment of myasthenia gravis.[L32408] When administered intravenously, it is indicated for the reversal or antagonism of the neuromuscular blocking effects of nondepolarizing muscle relaxants.[L32413] Pyridostigmine has also been used as a prophylactic agent against irreversible organophosphorus acetylcholinesterase inhibitors, primarily in a military capacity.[L32418]
Marketing Status	approved; investigational
ATC Code	N07AA02
DrugBank ID	DB00545
KEGG ID	D00487
MeSH ID	D011729
PubChem ID	4991
TTD Drug ID	D0O2WB
NDC Product Code	Not Available
UNII	19QM69HH21
Synonyms	Pyridostigmine Bromide \| Bromide, Pyridostigmine \| Pyridostigmine \| Mestinon

Chemical Information

Molecular Formula	C9H13N2O2+
CAS Registry Number	155-97-5
SMILES	C[N+]1=CC=CC(=C1)OC(=O)N(C)C
Chemical Structure

ADRs Induced by Drug

*The priority for ADR severity classification is based on FAERS assessment, followed by the most severe level in CTCAE rating. If neither is available, it will be displayed as 'Not available'.
**The 'Not Available' level is hidden by default and can be restored by clicking on the legend twice.

ADR Term	ADReCS ID	ADR Frequency (FAERS)	ADR Severity Grade (FAERS)	ADR Severity Grade (CTCAE)
Abdominal distension	07.01.04.001	-	-
Abdominal pain	07.01.05.002	-	-
Acute respiratory distress syndrome	10.02.01.067; 22.01.03.001; 24.03.02.034	0.002125%
Acute respiratory failure	14.01.04.004; 22.02.06.001	0.004250%		-
Aggression	19.05.01.001	0.002125%		-
Agitation	17.02.05.012; 19.06.02.001	-	-
Alopecia	23.02.02.001	-	-
Amblyopia	06.02.01.001	-	-	-
Anxiety	19.06.02.002	0.003188%
Arteriospasm coronary	02.02.02.005; 12.02.01.031; 24.04.04.005	0.003188%		-
Asthenia	08.01.01.001	0.023588%		-
Asthma	10.01.03.010; 22.03.01.002	0.005313%		-
Ataxia	08.01.02.004; 17.02.02.001	0.002125%
Atrioventricular block complete	02.03.01.003	0.002125%
Blood pressure increased	13.14.03.005	-	-	-
Bradycardia	02.03.02.002	0.010625%		-
Breast enlargement	21.05.04.001	0.002125%		-
Bronchitis	11.01.09.001; 22.07.01.001	-	-
Cardiac arrest	02.03.04.001	0.003188%
Chest discomfort	02.02.02.009; 08.01.08.019; 22.12.02.002	-	-	-
Chills	08.01.09.001; 15.05.03.016	0.002125%
Cholinergic syndrome	17.05.01.002	0.006375%		-
Condition aggravated	08.01.03.004	0.014875%		-
Confusional state	17.02.03.005; 19.13.01.001	-	-
Delusion	19.10.01.001	-	-
Dementia Alzheimer's type	17.03.06.001; 19.20.03.001	0.002125%		-
Depressed level of consciousness	17.02.04.002	0.005313%
Depressed mood	19.15.02.001	-	-	-
Dermatitis	23.03.04.002	-	-	-
Diarrhoea	07.02.01.001	0.032301%

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