sub:assertion {
drugbank:DB01175 a biolink:Drug ;
rdfs:label "Escitalopram" ;
biolink:category biolink:Drug .
mondo:0005689 a biolink:Disease ;
rdfs:label "Cannabis dependence" ;
biolink:category biolink:Disease .
sub:association rdf:object mondo:0005689 ;
rdf:predicate biolink:treats ;
rdf:subject drugbank:DB01175 ;
a biolink:ChemicalToDiseaseOrPhenotypicFeatureAssociation ;
rdfs:label "Currently, there are no FDA-approved pharmacotherapies available for CUD, though a number (eg, cannabinoids, antidepressants, anxiolytics, and glutamatergic modulators) have been proposed for off-label use. We identified 12 trials examining psychopharmacological interventions for the treatment of cannabis use disorder. Trials examined antidepressants (ie, escitalopram, fluoxetine, bupropion, nefazodone, venlafaxine, vilazodone), antipsychotics (ie, clozapine, ziprasidone), buspirone, mood stabilizers (ie, divalproex, lithium), and atomoxetine. Overall, studies found that antidepressants as a class were less effective than placebo for the achievement of abstinence (moderate SOE). There was no difference between antidepressants (moderate SOE) or buspirone (low SOE) and placebo in reducing overall cannabis use or retention in treatment. We found low strength evidence of no difference from placebo for antidepressants or buspirone on harms. Antidepressant medications did not impact secondary outcomes (low SOE). Findings for all other psychopharmacotherapies and drug/outcome combinations were either insufficient or were not identified in the current literature." ;
biolink:aggregator_knowledge_source infores:knowledge-collaboratory ;
biolink:category biolink:ChemicalToDiseaseOrPhenotypicFeatureAssociation ;
biolink:has_population_context sub:context ;
biolink:publications pmid:32227801 ;
biolink:relation ncit:C94303 .
sub:context a biolink:Cohort ;
rdfs:label "Adults" ;
biolink:category biolink:Cohort .
}