Journal article
Dose-Specific Adverse Drug Reaction Identification in Electronic Patient Records: Temporal Data Mining in an Inpatient Psychiatric Population
Department of Systems Biology, Technical University of Denmark1
Center for Biological Sequence Analysis, Department of Systems Biology, Technical University of Denmark2
Copenhagen University Hospital Herlev and Gentofte3
Functional Human Variation, Center for Biological Sequence Analysis, Department of Systems Biology, Technical University of Denmark4
Integrative Systems Biology, Center for Biological Sequence Analysis, Department of Systems Biology, Technical University of Denmark5
Data collected for medical, filing and administrative purposes in electronic patient records (EPRs) represent a rich source of individualised clinical data, which has great potential for improved detection of patients experiencing adverse drug reactions (ADRs), across all approved drugs and across all indication areas.The aim of this study was to take advantage of techniques for temporal data mining of EPRs in order to detect ADRs in a patient- and dose-specific manner.We used a psychiatric hospital’s EPR system to investigate undesired drug effects.
Within one workflow the method identified patient-specific adverse events (AEs) and links these to specific drugs and dosages in a temporal manner, based on integration of text mining results and structured data. The structured data contained precise information on drug identity, dosage and strength.When applying the method to the 3,394 patients in the cohort, we identified AEs linked with a drug in 2,402 patients (70.8 %).
Of the 43,528 patient-specific drug substances prescribed, 14,736 (33.9 %) were linked with AEs. From these links we identified multiple ADRs (p <0.05) and found them to occur at similar frequencies, as stated by the manufacturer and in the literature. We showed that drugs displaying similar ADR profiles share targets, and we compared submitted spontaneous AE reports with our findings.
For nine of the ten most prescribed antipsychotics in the patient population, larger doses were prescribed to sedated patients than non-sedated patients; five patients exhibited a significant difference (p <0.05). Finally, we present two cases (p <0.05) identified by the workflow. The method identified the potentially fatal AE QT prolongation caused by methadone, and a non-described likely ADR between levomepromazine and nightmares found among the hundreds of identified novel links between drugs and AEs (p <0.05).The developed method can be used to extract dose-dependent ADR information from already collected EPR data.
Large-scale AE extraction from EPRs may complement or even replace current drug safety monitoring methods in the future, reducing or eliminating manual reporting and enabling much faster ADR detection.
| Language: | English |
|---|---|
| Publisher: | Springer International Publishing |
| Year: | 2014 |
| Pages: | 237-247 |
| ISSN: | 11791942 and 01145916 |
| Types: | Journal article |
| DOI: | 10.1007/s40264-014-0145-z |
| ORCIDs: | 0000-0001-7885-715X and 0000-0003-0316-5866 |
Adolescent Adverse Drug Reaction Reporting Systems Aged Aged, 80 and over Antipsychotic Agents Data Collection Data Mining Drug Safety and Pharmacovigilance Drug-Related Side Effects and Adverse Reactions Electronic Health Records Female Humans Inpatients Male Medicine Medicine & Public Health Mental Disorders Middle Aged Pharmacology/Toxicology Young Adult
