Historique
Article de Périodique
Mortality related to novel psychoactive substances in Scotland, 2012: An exploratory study (2015)
Auteur(s) :
McAULEY, A. ;
HECHT, G. ;
BARNSDALE, L. ;
THOMSON, C. S. ;
GRAHAM, L. ;
PRIYADARSHI, S. ;
ROBERTSON, J. R.
Année
2015
Page(s) :
461-467
Langue(s) :
Anglais
Domaine :
Autres substances / Other substances ; Drogues illicites / Illicit drugs
Discipline :
EPI (Epidémiologie / Epidemiology)
Thésaurus géographique
ROYAUME-UNI
;
ECOSSE
Thésaurus mots-clés
DROGUES DE SYNTHESE
;
MORTALITE
;
SURDOSE
;
TOXICOLOGIE
;
BENZODIAZEPINES
;
STIMULANTS
;
PROFIL SOCIO-DEMOGRAPHIQUE
Résumé :
Background: The growth of novel psychoactive substances (NPS) over the last decade, both in terms of availability and consumption, is of increasing public health concern. Despite recent increases in related mortality, the circumstances surrounding and characteristics of individuals involved in NPS deaths at a population level remain relatively unknown.
Methods: The Scottish National Drug Related Death Database (NDRDD) collects a wide-range of data relating to the nature and circumstances of individuals who have died a drug-related death (DRD). We conducted exploratory descriptive analysis of DRDs involving NPS recorded by the NDRDD in 2012. Statistical testing of differences between sub-groups was also conducted where appropriate.
Results: In 2012, we found 36 DRDs in Scotland to have NPS recorded within post-mortem toxicology. However, in only 23 of these cases were NPS deemed by the reporting pathologist to be implicated in the actual cause of death. The majority of NPS-implicated DRDs involved Benzodiazepine-type drugs (13), mainly Phenazepam (12). The remaining 10 NPS-implicated deaths featured a range of different Stimulant-type drugs. The majority of these NPS-implicated deaths involved males and consumption of more than one drug was recorded by toxicology in all except one case.
NPS-implicated deaths involving Benzodiazepine-type NPS drugs appeared to involve older individuals known to be using drugs for a considerable period of time, many of whom had been in prison at some point in their lives. They also typically involved combinations of opioids and benzodiazepines; no stimulant drugs were co-implicated.
Deaths where stimulant-type NPS drugs were implicated appeared to be a younger group in comparison, all consuming two or more Stimulant-type drugs in combination.
Conclusion: This exploratory study provides an important insight into the circumstances surrounding and characteristics of individuals involved in NPS deaths at a population level. It identifies important issues for policy and practice, not least the prominent role of unlicensed benzodiazepines in drug-related mortality, but also the need for a range of harm reduction strategies to prevent future deaths.
Highlights:
Deaths involving novel psychoactive substances (NPS) affect small numbers at population level.
High incidence of NPS is noteworthy when considering DRDs within known drug user populations.
Deaths rarely involve NPS alone and typically involve a range of other substances.
The majority of deaths involved Benzodiazepine-type NPS drugs, mainly Phenazepam.
Differences in the profile of deaths involving Benzodiazepine and Stimulant-type NPS emerged.
Methods: The Scottish National Drug Related Death Database (NDRDD) collects a wide-range of data relating to the nature and circumstances of individuals who have died a drug-related death (DRD). We conducted exploratory descriptive analysis of DRDs involving NPS recorded by the NDRDD in 2012. Statistical testing of differences between sub-groups was also conducted where appropriate.
Results: In 2012, we found 36 DRDs in Scotland to have NPS recorded within post-mortem toxicology. However, in only 23 of these cases were NPS deemed by the reporting pathologist to be implicated in the actual cause of death. The majority of NPS-implicated DRDs involved Benzodiazepine-type drugs (13), mainly Phenazepam (12). The remaining 10 NPS-implicated deaths featured a range of different Stimulant-type drugs. The majority of these NPS-implicated deaths involved males and consumption of more than one drug was recorded by toxicology in all except one case.
NPS-implicated deaths involving Benzodiazepine-type NPS drugs appeared to involve older individuals known to be using drugs for a considerable period of time, many of whom had been in prison at some point in their lives. They also typically involved combinations of opioids and benzodiazepines; no stimulant drugs were co-implicated.
Deaths where stimulant-type NPS drugs were implicated appeared to be a younger group in comparison, all consuming two or more Stimulant-type drugs in combination.
Conclusion: This exploratory study provides an important insight into the circumstances surrounding and characteristics of individuals involved in NPS deaths at a population level. It identifies important issues for policy and practice, not least the prominent role of unlicensed benzodiazepines in drug-related mortality, but also the need for a range of harm reduction strategies to prevent future deaths.
Highlights:
Deaths involving novel psychoactive substances (NPS) affect small numbers at population level.
High incidence of NPS is noteworthy when considering DRDs within known drug user populations.
Deaths rarely involve NPS alone and typically involve a range of other substances.
The majority of deaths involved Benzodiazepine-type NPS drugs, mainly Phenazepam.
Differences in the profile of deaths involving Benzodiazepine and Stimulant-type NPS emerged.
Affiliation :
NHS Health Scotland, Public Health Science Directorate, Glasgow, Scotland, UK
Cote :
Abonnement