Otenabant: Difference between revisions

Latest revision as of 03:29, 13 February 2025

Otenabant[edit]

Otenabant is a pharmaceutical drug that was developed as a cannabinoid receptor antagonist. It was primarily investigated for its potential use in the treatment of obesity and related metabolic disorders. Otenabant acts by blocking the CB1 receptor, which is part of the endocannabinoid system.

Mechanism of Action[edit]

Otenabant functions as a selective antagonist of the CB1 receptor, which is predominantly found in the central nervous system and peripheral tissues. By inhibiting the action of endogenous cannabinoids at this receptor, Otenabant reduces appetite and food intake, which can lead to weight loss. The blockade of CB1 receptors also affects lipid metabolism and glucose homeostasis, contributing to its potential benefits in treating metabolic syndrome.

Development and Clinical Trials[edit]

Otenabant was developed by Pfizer, a major pharmaceutical company. During its development, Otenabant underwent several clinical trials to assess its efficacy and safety in humans. These trials aimed to determine the drug's impact on body weight, metabolic parameters, and potential side effects.

Side Effects[edit]

Like other CB1 receptor antagonists, Otenabant was associated with several side effects. Common adverse effects included nausea, dizziness, and anxiety. More serious concerns were raised about the potential for psychiatric disorders, such as depression and suicidal ideation, which ultimately led to the discontinuation of its development.

Discontinuation[edit]

The development of Otenabant was halted due to safety concerns, particularly the risk of psychiatric side effects. This decision was influenced by the withdrawal of similar drugs from the market, such as Rimonabant, which faced similar issues. As a result, Otenabant did not receive regulatory approval and was never marketed.

Related Pages[edit]

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-'''Otenabant''' is a drug that was under development by [[Pfizer]] for the treatment of [[obesity]]. It acts as a [[CB1]] receptor antagonist.
+== Otenabant ==
-== History ==
+[[File:Otenabant.svg|thumb|right|Chemical structure of Otenabant]]
-Otenabant was developed by Pfizer in the early 2000s as a potential treatment for obesity. The drug works by blocking the CB1 receptor, which is involved in the regulation of appetite and energy balance in the body. However, the development of Otenabant was discontinued in 2008 due to concerns about side effects.
-== Mechanism of Action ==
+'''Otenabant''' is a [[pharmaceutical drug]] that was developed as a [[cannabinoid receptor]] antagonist. It was primarily investigated for its potential use in the treatment of [[obesity]] and related metabolic disorders. Otenabant acts by blocking the [[CB1 receptor]], which is part of the [[endocannabinoid system]].
-Otenabant is a CB1 receptor antagonist. The CB1 receptor is found primarily in the brain and is involved in a variety of physiological processes, including appetite regulation and energy balance. By blocking this receptor, Otenabant is thought to reduce appetite and increase energy expenditure, thereby helping to reduce body weight.
-== Clinical Trials ==
+=== Mechanism of Action ===
-Several clinical trials were conducted to evaluate the safety and efficacy of Otenabant in the treatment of obesity. However, the results of these trials were mixed, and the development of the drug was ultimately discontinued due to concerns about side effects.
-== Side Effects ==
+Otenabant functions as a selective antagonist of the [[CB1 receptor]], which is predominantly found in the [[central nervous system]] and [[peripheral tissues]]. By inhibiting the action of endogenous cannabinoids at this receptor, Otenabant reduces appetite and food intake, which can lead to weight loss. The blockade of CB1 receptors also affects [[lipid metabolism]] and [[glucose homeostasis]], contributing to its potential benefits in treating [[metabolic syndrome]].
-The most common side effects reported in clinical trials of Otenabant included nausea, vomiting, and dizziness. There were also concerns about the potential for psychiatric side effects, including depression and suicidal thoughts.
-== Discontinuation ==
+=== Development and Clinical Trials ===
-The development of Otenabant was discontinued in 2008. This decision was made due to concerns about the safety profile of the drug, particularly the potential for psychiatric side effects.
-== See Also ==
+Otenabant was developed by [[Pfizer]], a major [[pharmaceutical company]]. During its development, Otenabant underwent several [[clinical trials]] to assess its efficacy and safety in humans. These trials aimed to determine the drug's impact on body weight, metabolic parameters, and potential side effects.
-* [[Cannabinoid receptor antagonist]]
+=== Side Effects ===
+Like other CB1 receptor antagonists, Otenabant was associated with several side effects. Common adverse effects included [[nausea]], [[dizziness]], and [[anxiety]]. More serious concerns were raised about the potential for [[psychiatric disorders]], such as [[depression]] and [[suicidal ideation]], which ultimately led to the discontinuation of its development.
+=== Discontinuation ===
+The development of Otenabant was halted due to safety concerns, particularly the risk of psychiatric side effects. This decision was influenced by the withdrawal of similar drugs from the market, such as [[Rimonabant]], which faced similar issues. As a result, Otenabant did not receive regulatory approval and was never marketed.
+== Related Pages ==
+* [[Cannabinoid receptor]]
+* [[Endocannabinoid system]]
 * [[Obesity]]
-* [[Pfizer]]
+* [[Metabolic syndrome]]
+* [[Rimonabant]]
-[[Category:Drugs]]
-[[Category:Obesity]]
-[[Category:Pfizer]]
-{{stub}}
+[[Category:Pharmaceutical drugs]]
+[[Category:Cannabinoid receptor antagonists]]