Difference between revisions of "Atropine"

Atropine
	Clinical data
Drug class	Anticholinergic
Uses	Treatment of bradycardia, Antidote for acetylcholinesterase inhibitor toxicity
Contraindications	Known hypersensitivity
Routes of administration	IV, IM, PO, oral or endotracheal inhalation, ophthalmic solution
Dosage	Treatment of bradycardia: 1 mg every 3 to 5 minutes (3mg max), repeat until obtaining desired heart rate Treatment of acetylcholinesterase inhibitor toxicity: 2 to 3 mg every 20 to 30 min Antisialagogue/anti-vagal: 0.5 to 1mg every 1 to 2 hours Pediatric: 0.01 mg/kg to 0.03 mg/kg every 3 to 5 minutes. Minimum dose is 0.1 mg. Maximum dose is 0.5mg (child) or 1 mg (adolescent).
	Dosage
	Pharmacodynamics
Mechanism of action	Muscarinic acetylcholine antagonism
	Pharmacokinetics
Metabolism	Enzymatic hydrolysis in the liver
Protein binding	14-22%
	Physical and chemical data
Formula	C17H23NO3
Molar mass	289.369 g/mol
	Article quality
Editor rating	Comprehensive
User likes	0

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Revision as of 18:10, 10 January 2024

Atropine is a tertiary amine extracted from belladonna alkaloid as a racemic mixture of d and l-hyoscyamine, which vary in their potency as anticholinergic agents. It reversibly binds to peripheral muscarinic acetylcholine receptors where it acts a competitive inhibitor. Its primary uses include treatment of bradycardia or bradycardia-induced cardiac arrest, treatment of cholinergic effects of organophosphate, nerve agent, or insecticide toxicity, or in ophthalmic surgery to produce mydriasis and cycloplegia. It can also be utilized in conjunction with cholinesterase inhibitors for reversal of neuromuscular blockade in order to reduce their muscarinic effects.

Uses

Treatment of bradycardia (vasovagal response, AV block, bradyarrhythmias)
Treatment of acetylcholinesterase inhibitor toxicity (chemical nerve agents, carbamate, organophosphates)
Perioperatively for reduction of secretions and vagal responses
Perioperatively for prophylaxis against muscarinic effects when anticholinesterase agents (neostigmine, physostigmine, pyridostigmine) are used to reverse neuromuscular blockade
For ophthalmic surgery, to induce mydriasis or cycloplegia
Treatment of amblyopia

Contraindications

Absolute contraindications

Atropine or belladonna alkaloids hypersensitivity. Note: IM/IV administration of atropine can cause flushing of face and trunk, which is not associated with a hypersensitivity response.^[1]

Precautions

Coronary artery disease, acute myocardial infarct, congestive heart failure, tachycardia, or hypertension
Chronic lung disease
Obstructive gastrointestinal disease, including toxic megacolon, paralytic ileus, pyloric stenosis
Obstructive urinary disease, including uropathy and prostatic hypertrophy
Acute-angle glaucoma
Myasthenia gravis
Insufficient data regarding atropine use during pregnancy to determine risk of adverse developmental outcomes

Pharmacology

Pharmacodynamics

Mechanism of action

Atropine is a competitive inhibitor at autonomic postganglionic cholinergic receptors.^[2] Atropine’s activity is primarily due to the l-hyoscyamine enantiomer. Atropine binds receptors found in GI and pulmonary smooth muscle, exocrine glands, heart and eye; it does not block acetylcholine’s action at the NMJ. It does not inhibit nicotinic cholinergic receptors at typical doses. Atropine’s primary clinical effects include changes in heart rate, reduction in salivary, bronchial, and sweat gland secretions, bronchodilation, mydriasis and cycloplegia, decreased GI motility and gastric secretions, and contraction of the bladder detrusor muscle.

Adverse effects

Dry mouth (xerostomia)

Blurred vision, including photophobia and loss of visual acuity
GI symptoms: dysphagia, constipation, nausea, vomiting
Bradycardia (at doses of 0.4-0.6mg)
Tachycardia (at doses of 1-2mg)
Palpitations, arrhythmias, asystole
Flushing
Urinary retention
Delirium and coma at high doses

Pharmacokinetics

IV administration has a distribution half life of about 1 minute, with rapid decline in concentration within the first 8-10 minutes.^[2]
Crosses the blood-brain barrier and the placenta^[3]
Undergoes enzymatic hydrolysis in the liver into active metabolites^[3]
Atropine and its metabolites are primarily exreted renally, with small contributions from pulmonary and fecal routes of excretion. 13-57% of atropine is excreted unchanged in the urine.^[3]

Chemistry and formulation

History

References

↑ "Atropine Injection, 2mg" (PDF). FDA Drug Safety Data. 07/2018. Retrieved 01/05/2024. Check date values in: |access-date= and |date= (help)
↑ ^2.0 ^2.1 McLendon, Kevin; Preuss, Charles V. (2023), "Atropine", StatPearls, Treasure Island (FL): StatPearls Publishing, PMID 29262018, retrieved 2024-01-11
↑ ^3.0 ^3.1 ^3.2 Ali–Melkkilä, T.; Kanto, J.; Iisalo, E. (1993-10). "Pharmacokinetics and related pharmacodynamics of anticholinergic drugs". Acta Anaesthesiologica Scandinavica. 37 (7): 633–642. doi:10.1111/j.1399-6576.1993.tb03780.x. ISSN 0001-5172. Check date values in: |date= (help)

Top contributors: Anna McCarter, Olivia Sutton and Chris Rishel

[1] "Atropine Injection, 2mg" (PDF). FDA Drug Safety Data. 07/2018. Retrieved 01/05/2024. Check date values in: |access-date= and |date= (help)

[:0-2] 2.0 ^2.1 McLendon, Kevin; Preuss, Charles V. (2023), "Atropine", StatPearls, Treasure Island (FL): StatPearls Publishing, PMID 29262018, retrieved 2024-01-11

[:1-3] 3.0 ^3.1 ^3.2 Ali–Melkkilä, T.; Kanto, J.; Iisalo, E. (1993-10). "Pharmacokinetics and related pharmacodynamics of anticholinergic drugs". Acta Anaesthesiologica Scandinavica. 37 (7): 633–642. doi:10.1111/j.1399-6576.1993.tb03780.x. ISSN 0001-5172. Check date values in: |date= (help)

[1]

[2]

[3]

@@ Line 36: / Line 36: @@
 ==Uses<!-- Describe uses of the drug. If appropriate, add subsections for each indication. -->==
-- Treatment of bradycardia (vasovagal response, AV block, bradyarrhythmias)
+* Treatment of bradycardia (vasovagal response, AV block, bradyarrhythmias)
+*Treatment of acetylcholinesterase inhibitor toxicity (chemical nerve agents, carbamate, organophosphates)
-- Treatment of acetylcholinesterase inhibitor toxicity (chemical nerve agents, carbamate, organophosphates)
+*Perioperatively for reduction of secretions and vagal responses
+*Perioperatively for prophylaxis against muscarinic effects when anticholinesterase agents (neostigmine, physostigmine, pyridostigmine) are used to reverse neuromuscular blockade
-- Perioperatively for reduction of secretions and vagal responses
+*For ophthalmic surgery, to induce mydriasis or cycloplegia
+*Treatment of amblyopia
-- Perioperatively for prophylaxis against muscarinic effects when anticholinesterase agents (neostigmine, physostigmine, pyridostigmine) are used to reverse neuromuscular blockade
-- For ophthalmic surgery, to induce mydriasis or cycloplegia
-- Treatment of amblyopia
 ==Contraindications<!-- List contraindications and precautions for use of the drug. -->==
 ===Absolute contraindications<!-- List absolute contraindications for use of the drug. If none, this section may be removed. -->===
-- Atropine or belladonna alkaloids hypersensitivity. Note: IM/IV administration of atropine can cause flushing of face and trunk, which is not associated with a hypersensitivity response.<ref>{{Cite web|date=07/2018|title=Atropine Injection, 2mg|url=https://www.accessdata.fda.gov/drugsatfda_docs/label/2018/212319s000lbl.pdf|url-status=live|access-date=01/05/2024|website=FDA Drug Safety Data}}</ref>
+*Atropine or belladonna alkaloids hypersensitivity. Note: IM/IV administration of atropine can cause flushing of face and trunk, which is not associated with a hypersensitivity response.<ref>{{Cite web|date=07/2018|title=Atropine Injection, 2mg|url=https://www.accessdata.fda.gov/drugsatfda_docs/label/2018/212319s000lbl.pdf|url-status=live|access-date=01/05/2024|website=FDA Drug Safety Data}}</ref>
 ===Precautions<!-- List precautions for use of the drug. If none, this section may be removed. -->===
-- Coronary artery disease, acute myocardial infarct, congestive heart failure, tachycardia, or hypertension
+*Coronary artery disease, acute myocardial infarct, congestive heart failure, tachycardia, or hypertension
+*Chronic lung disease
-- Chronic lung disease
+*Obstructive gastrointestinal disease, including toxic megacolon, paralytic ileus, pyloric stenosis
+*Obstructive urinary disease, including uropathy and prostatic hypertrophy
-- Obstructive gastrointestinal disease, including toxic megacolon, paralytic ileus, pyloric stenosis
+* Acute-angle glaucoma
+*[[Myasthenia gravis]]
-- Obstructive urinary disease, including uropathy and prostatic hypertrophy
+*Insufficient data regarding atropine use during pregnancy to determine risk of adverse developmental outcomes
-- Acute-angle glaucoma
-- Myasthenia gravis
-- Insufficient data regarding atropine use during pregnancy to determine risk of adverse developmental outcomes
 ==Pharmacology==
@@ Line 73: / Line 61: @@
 ====Mechanism of action<!-- Describe the mechanism of action for the primary uses of the drug. -->====
-Atropine is a competitive inhibitor at autonomic postganglionic cholinergic receptors<ref name=":0">{{Cite web|title=Atropine|url=https://www-clinicalkey-com.laneproxy.stanford.edu/#!/topic/atropine?topic=atropine|url-status=live|access-date=1/5/2024|website=Elsevier Drug Information}}</ref>. Atropine’s activity is primarily due to the l-hyoscyamine enantiomer.  Atropine binds receptors found in GI and pulmonary smooth muscle, exocrine glands, heart and eye; it does not block acetylcholine’s action at the NMJ. It does not inhibit nicotonic cholingeric receptors at typical doses. Atropine’s primary clinical effects include changes in heart rate, reduction in salivary, bronchial, and sweat gland secretions, bronchodilation, mydriasis and cycloplegia, decreased GI motility and gastric secretions, and contraction of the bladder detrusor muscle.
+Atropine is a competitive inhibitor at autonomic postganglionic cholinergic receptors.<ref name=":0">{{Citation|last=McLendon|first=Kevin|title=Atropine|date=2023|url=http://www.ncbi.nlm.nih.gov/books/NBK470551/|work=StatPearls|place=Treasure Island (FL)|publisher=StatPearls Publishing|pmid=29262018|access-date=2024-01-11|last2=Preuss|first2=Charles V.}}</ref> Atropine’s activity is primarily due to the l-hyoscyamine enantiomer.  Atropine binds receptors found in GI and pulmonary smooth muscle, exocrine glands, heart and eye; it does not block acetylcholine’s action at the NMJ. It does not inhibit nicotinic cholinergic receptors at typical doses. Atropine’s primary clinical effects include changes in heart rate, reduction in salivary, bronchial, and sweat gland secretions, bronchodilation, mydriasis and cycloplegia, decreased GI motility and gastric secretions, and contraction of the bladder detrusor muscle.
 ====Adverse effects<!-- Describe any potential adverse effects of the drug. -->====
-- Dry mouth (xerostomia)
+*Dry mouth (xerostomia)
-- Blurred vision, including photophobia and loss of visual acuity
-- GI symptoms: dysphagia, constipation, nausea, vomiting
-- Bradycardia (at doses of 0.4-0.6mg)
-- Tachycardia (at doses of 1-2mg)
-- Palpitations, arrhythmias, aystole
-- Flushing
+*Blurred vision, including photophobia and loss of visual acuity
+*GI symptoms: dysphagia, constipation, nausea, vomiting
-- Urinary retention
+*Bradycardia (at doses of 0.4-0.6mg)
+*Tachycardia (at doses of 1-2mg)
-- Delirium and coma at high doses
+*Palpitations, arrhythmias, asystole
+*Flushing
+*Urinary retention
+*Delirium and coma at high doses
 ===Pharmacokinetics<!-- Describe the pharmacokinetics of the drug. -->===
-- IV administration has a distribution half life of about 1 minute, with rapid decline in concentration within the first 8-10 minutes.  <ref name=":0" />
-- Crosses the blood-brain barrier and the placenta<ref name=":1">{{Cite journal|last=Ali–Melkkilä|first=T.|last2=Kanto|first2=J.|last3=Iisalo|first3=E.|date=1993-10|title=Pharmacokinetics and related pharmacodynamics of anticholinergic drugs|url=https://onlinelibrary.wiley.com/doi/10.1111/j.1399-6576.1993.tb03780.x|journal=Acta Anaesthesiologica Scandinavica|language=en|volume=37|issue=7|pages=633–642|doi=10.1111/j.1399-6576.1993.tb03780.x|issn=0001-5172}}</ref>
-- Undergoes enzymatic hydrolysis in the liver into active metabolites<ref name=":1" />
-- Atropine and its metabolites are primarily exreted renally, with small contributions from  pulmonary and fecal routes of excretion. 13-57% of atropine is excreted unchanged in the urine.<ref name=":1" />
+* IV administration has a distribution half life of about 1 minute, with rapid decline in concentration within the first 8-10 minutes.<ref name=":0" />
+* Crosses the blood-brain barrier and the placenta<ref name=":1">{{Cite journal|last=Ali–Melkkilä|first=T.|last2=Kanto|first2=J.|last3=Iisalo|first3=E.|date=1993-10|title=Pharmacokinetics and related pharmacodynamics of anticholinergic drugs|url=https://onlinelibrary.wiley.com/doi/10.1111/j.1399-6576.1993.tb03780.x|journal=Acta Anaesthesiologica Scandinavica|language=en|volume=37|issue=7|pages=633–642|doi=10.1111/j.1399-6576.1993.tb03780.x|issn=0001-5172}}</ref>
+* Undergoes enzymatic hydrolysis in the liver into active metabolites<ref name=":1" />
+* Atropine and its metabolites are primarily exreted renally, with small contributions from  pulmonary and fecal routes of excretion. 13-57% of atropine is excreted unchanged in the urine.<ref name=":1" />
 ==Chemistry and formulation<!-- Describe the chemistry and formulation of the drug. -->==
-==History<!-- Describe the historical development of the drug. -->==
+== History<!-- Describe the historical development of the drug. -->==
-==References==
+== References==
 [[Category:Drug reference]]