Weight gain and comorbidities associated with oral second-generation antipsychotics: analysis of real-world data for patients with schizophrenia or bipolar I disorder.
Cardiometabolic burden
Claims data
Electronic medical record
Treatment patterns
Journal
BMC psychiatry
ISSN: 1471-244X
Titre abrégé: BMC Psychiatry
Pays: England
ID NLM: 100968559
Informations de publication
Date de publication:
14 02 2022
14 02 2022
Historique:
received:
20
08
2021
accepted:
31
01
2022
entrez:
15
2
2022
pubmed:
16
2
2022
medline:
12
4
2022
Statut:
epublish
Résumé
Many second-generation antipsychotics (SGAs) are associated with weight gain and cardiometabolic effects. Antipsychotic-associated weight gain is linked to treatment interruptions, potentially increasing risk of relapse and hospitalization. This retrospective study assessed clinically significant weight gain (CSWG), treatment interruptions, and development of cardiometabolic conditions in patients with schizophrenia (SZ) or bipolar I disorder (BD-I) following initiation of oral SGAs with moderate to high weight gain risk. Patients with no prior use of moderate to high weight gain risk oral SGAs were identified from patient-level medical/pharmacy claims and electronic medical records (January 2013-February 2020; OM1 Real-World Data Cloud). Those with ≥ 1 weight measurement in both the 12 months preceding and 3 months after SGA initiation (index date) were analyzed for continuous changes in weight, CSWG (≥ 7% and ≥ 10% increases from baseline), treatment interruptions (switches/discontinuations), and development of cardiometabolic conditions. Median follow-up times in the SZ (n = 8174) and BD-I (n = 9142) cohorts were 153.4 and 159.4 weeks, respectively; 45.5% and 50.7% were obese at baseline. Mean (SD) percent weight increase during treatment was 3.3% (7.2) and 3.7% (7.0) for patients with SZ and BD-I, respectively, and was highest for underweight/normal weight patients (SZ: 4.8% [8.1]; BD-I: 5.5% [8.7]). More than 96% had treatment interruptions during follow-up, primarily discontinuations. CSWG and treatment interruptions occurred within a median of 13 and 14 weeks after treatment initiation, respectively. Of patients with CSWG and treatment interruptions, approximately 75% did not return to baseline weight during follow-up. Among those without baseline cardiometabolic conditions, 14.7% and 11.3% of patients with SZ or BD-I, respectively, developed ≥ 1 condition over 12 months post-index. Incidence was generally highest among those who were overweight/obese at baseline and those who experienced CSWG. In this analysis of real-world data, both weight gain and treatment interruptions occurred early in treatment for patients with SZ or BD-I. Treatment-associated weight gain persisted despite switching or discontinuing index treatment. Additionally, cardiometabolic morbidity increased within 12 months of treatment initiation. Patients with SZ or BD-I are at greater risk than the general population for cardiometabolic conditions; weight gain associated with SGAs may exacerbate these health risks.
Sections du résumé
BACKGROUND
Many second-generation antipsychotics (SGAs) are associated with weight gain and cardiometabolic effects. Antipsychotic-associated weight gain is linked to treatment interruptions, potentially increasing risk of relapse and hospitalization. This retrospective study assessed clinically significant weight gain (CSWG), treatment interruptions, and development of cardiometabolic conditions in patients with schizophrenia (SZ) or bipolar I disorder (BD-I) following initiation of oral SGAs with moderate to high weight gain risk.
METHODS
Patients with no prior use of moderate to high weight gain risk oral SGAs were identified from patient-level medical/pharmacy claims and electronic medical records (January 2013-February 2020; OM1 Real-World Data Cloud). Those with ≥ 1 weight measurement in both the 12 months preceding and 3 months after SGA initiation (index date) were analyzed for continuous changes in weight, CSWG (≥ 7% and ≥ 10% increases from baseline), treatment interruptions (switches/discontinuations), and development of cardiometabolic conditions.
RESULTS
Median follow-up times in the SZ (n = 8174) and BD-I (n = 9142) cohorts were 153.4 and 159.4 weeks, respectively; 45.5% and 50.7% were obese at baseline. Mean (SD) percent weight increase during treatment was 3.3% (7.2) and 3.7% (7.0) for patients with SZ and BD-I, respectively, and was highest for underweight/normal weight patients (SZ: 4.8% [8.1]; BD-I: 5.5% [8.7]). More than 96% had treatment interruptions during follow-up, primarily discontinuations. CSWG and treatment interruptions occurred within a median of 13 and 14 weeks after treatment initiation, respectively. Of patients with CSWG and treatment interruptions, approximately 75% did not return to baseline weight during follow-up. Among those without baseline cardiometabolic conditions, 14.7% and 11.3% of patients with SZ or BD-I, respectively, developed ≥ 1 condition over 12 months post-index. Incidence was generally highest among those who were overweight/obese at baseline and those who experienced CSWG.
CONCLUSIONS
In this analysis of real-world data, both weight gain and treatment interruptions occurred early in treatment for patients with SZ or BD-I. Treatment-associated weight gain persisted despite switching or discontinuing index treatment. Additionally, cardiometabolic morbidity increased within 12 months of treatment initiation. Patients with SZ or BD-I are at greater risk than the general population for cardiometabolic conditions; weight gain associated with SGAs may exacerbate these health risks.
Identifiants
pubmed: 35164737
doi: 10.1186/s12888-022-03758-w
pii: 10.1186/s12888-022-03758-w
pmc: PMC8842889
doi:
Substances chimiques
Antipsychotic Agents
0
Types de publication
Journal Article
Research Support, Non-U.S. Gov't
Langues
eng
Sous-ensembles de citation
IM
Pagination
114Informations de copyright
© 2022. The Author(s).
Références
J Psychiatr Res. 2013 Feb;47(2):197-207
pubmed: 23153955
Psychiatr Serv. 2004 Aug;55(8):886-91
pubmed: 15292538
BMC Psychiatry. 2020 Jul 6;20(1):354
pubmed: 32631362
Psychiatry Res. 2009 Dec 30;170(2-3):172-6
pubmed: 19897253
J Psychiatr Res. 2009 Mar;43(6):620-6
pubmed: 19110264
CNS Drugs. 2005;19 Suppl 1:1-93
pubmed: 15998156
J Psychopharmacol. 2013 Apr;27(4):358-65
pubmed: 23343595
CNS Drugs. 2007;21(11):911-36
pubmed: 17927296
Can J Psychiatry. 2001 Aug;46(6):549-55
pubmed: 11526812
Psychopharmacol Bull. 2009;42(4):23-39
pubmed: 20581791
PLoS One. 2014 Apr 24;9(4):e94112
pubmed: 24763306
N Engl J Med. 2005 Sep 22;353(12):1209-23
pubmed: 16172203
Eur Psychiatry. 2010 Jun;25 Suppl 2:S6-11
pubmed: 20620888
Bipolar Disord. 2011 Jun;13(4):387-95
pubmed: 21843278
World Psychiatry. 2011 Feb;10(1):52-77
pubmed: 21379357
Bipolar Disord. 2018 Mar;20(2):97-170
pubmed: 29536616
Eur Psychiatry. 2009 Sep;24(6):412-24
pubmed: 19682863
Neuropsychiatr Dis Treat. 2017 Aug 22;13:2231-2241
pubmed: 28883731
Psychiatr Serv. 2010 Aug;61(8):830-4
pubmed: 20675843
Epidemiol Rev. 2008;30:67-76
pubmed: 18480098
Front Psychiatry. 2014 Sep 26;5:137
pubmed: 25309466
Front Psychiatry. 2020 Apr 22;11:314
pubmed: 32390884
PLoS One. 2012;7(3):e31660
pubmed: 22457710
Clin Schizophr Relat Psychoses. 2011 Oct;5(3):135-41
pubmed: 21983497
Patient Prefer Adherence. 2020 Oct 28;14:2043-2054
pubmed: 33149559
J Clin Psychiatry. 2005 Oct;66(10):1205-15
pubmed: 16259532
Ther Clin Risk Manag. 2017 Jun 29;13:757-777
pubmed: 28721057
Curr Med Res Opin. 2007 Oct;23(10):2305-12
pubmed: 17697454
Schizophr Res. 2003 Jul 1;62(1-2):73-6
pubmed: 12765746
Arch Gen Psychiatry. 2006 Jul;63(7):824-30
pubmed: 16818872
Am J Public Health. 2016 Sep;106(9):1656-62
pubmed: 27459460
J Med Econ. 2018 Feb;21(2):127-134
pubmed: 28895758
Ann Clin Psychiatry. 2006 Oct-Dec;18(4):239-41
pubmed: 17162623
Schizophr Res. 2004 Jan 1;66(1):51-7
pubmed: 14693352
Schizophr Res Treatment. 2012;2012:916198
pubmed: 22966451
JAMA Cardiol. 2018 Apr 1;3(4):280-287
pubmed: 29490333
J Manag Care Pharm. 2013 Jul-Aug;19(6):468-77
pubmed: 23806061