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Pharmacology
Systemic Pharmacotherapeutics of the Respiratory System
Antitussive Drugs
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Chapters in Pharmacology
  • Pharmacology Introduction
  • Systemic Pharmacotherapeutics of the Cardiovascular System
  • Systemic Pharmacotherapeutics of the Digestive System
  • Systemic Pharmacotherapeutics of the Eye
  • Systemic Pharmacotherapeutics of the Integumentary System
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  • Systemic Pharmacotherapeutics of the Nervous System
  • Systemic Pharmacotherapeutics of the Reproductive System
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  • Systemic Pharmacotherapeutics of the Urinary System
  • Chemotherapeutics Introduction
  • Anthelmintics
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Topics in Systemic Pharmacotherapeutics of the Respiratory System
  • Overview of Systemic Pharmacotherapeutics of the Respiratory System
  • Antitussive Drugs
  • Systemic Therapy of Airway Disease
  • Inhalation Therapy of Airway Disease
  • Expectorants and Mucolytic Drugs
  • Decongestants
  • Respiratory Stimulants
 
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Antitussive Drugs

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The afferent arc of the cough reflex receives input from sensory nerves in the bronchial and tracheal airways. Airway irritation and inflammation stimulate the afferent nerves, which in turn activate the cough center located in the medulla oblongata. Most of the antitussive drugs are opiates or opioids that directly suppress the cough center in the medulla oblongata (see Systemic Pharmacotherapeutics of the Respiratory System: Antitussive DrugsTables). The antitussive effect does not appear to be related to the binding of traditional opiate receptors.

Table 1

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Antitussive Drugs

Drug

Dosage

Morphine

Dogs: 0.1 mg/kg, IM, tid-qid

Codeine

Dogs: 1–2 mg/kg, PO, bid-qid

Hydrocodone

Dogs: 0.25 mg/kg, PO, bid-qid

Butorphanol

Dogs: 0.055–0.11 mg/kg, SC, bid-qid or 0.055–1.1 mg/kg, PO, bid-qid

Morphine is an effective antitussive at doses lower than the doses that produce analgesia and sedation. It is not commonly used for antitussive activity due to adverse effects and the potential for abuse and addiction. Morphine has poor oral bioavailability due to a significant first-pass effect by the liver.

Codeine is methylmorphine; methylation of morphine significantly improves the oral bioavailability by reducing the first-pass effect. Codeine phosphate and codeine sulfate are found in many preparations, including tablets, liquids, and syrups. Codeine has analgesic effects that are about one-tenth that of morphine, but its antitussive potency is about equal to that of morphine. The adverse effects of codeine are significantly less than those seen with morphine at antitussive doses. Toxicity (especially in cats) is exhibited as excitement, muscular spasms, convulsions, respiratory depression, sedation, and constipation. Codeine should not be used after GI tract surgery. The potential for addiction and abuse of codeine is considerably lower than that for morphine.

Hydrocodone is chemically and pharmacologically similar to codeine but more potent. It is combined with an anticholinergic drug (homatropine) to discourage abuse by people. It can be prescribed for small animals but should be used with caution in cats.

Dextromethorphan is technically not considered an opiate because it does not bind to traditional opiate receptors and is not addictive or analgesic. It is the d-isomer of levorphanol. The l-isomer of levorphanol has addictive and analgesic properties. While recommended anecdotally for the treatment of cough, a pharmacokinetic study in dogs demonstrated a short elimination half-life, rapid clearance, and poor oral bioavailability, making its use as an orally administered cough suppressant in dogs questionable.

Butorphanol, an opioid agonist-antagonist, is used as an analgesic and antitussive in dogs. It is more potent than morphine as an analgesic and more potent than codeine as an antitussive. It may produce considerable sedation. Because butorphanol has poor bioavailability, the oral dose in dogs is 10 times the SC dose. Its use in cats is controversial.

Last full review/revision March 2012 by Patricia M. Dowling, DVM,MSc, DACVIM, DACVCP

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