Use of antidepressant medication and risk of type 2 diabetes: results from three cohorts of US adults

A Pan; Q Sun; O I Okereke; K M Rexrode; R R Rubin; M Lucas; W C Willett; J E Manson; F B Hu

doi:10.1007/s00125-011-2268-4

. Author manuscript; available in PMC: 2013 Jan 1.

Published in final edited form as: Diabetologia. 2011 Aug 3;55(1):63–72. doi: 10.1007/s00125-011-2268-4

Use of antidepressant medication and risk of type 2 diabetes: results from three cohorts of US adults

A Pan ¹, Q Sun ^1,², O I Okereke ^2,^3,⁴, K M Rexrode ⁵, R R Rubin ⁶, M Lucas ¹, W C Willett ^1,^2,³, J E Manson ^3,⁵, F B Hu ^1,^2,³

PMCID: PMC3229672 NIHMSID: NIHMS319485 PMID: 21811871

Abstract

Aims/hypothesis

Several studies suggested a potential positive association between antidepressant medication (ADM) use and incident type 2 diabetes mellitus. We examined this association in three cohorts of US adults.

Methods

We followed 29,776 men in the Health Professionals Follow-up Study (HPFS, 1990–2006), 61,791 women in the Nurses’ Health Study I (NHS I, 1996–2008) and 76,868 women in NHS II (1993–2005), who were free of diabetes mellitus, cardiovascular disease, or cancer at baseline. The mean baseline ages for HPFS, NHS I and II were 56.4, 61.3 and 38.1 years old, respectively. ADM use and other covariates were assessed at baseline and updated every 2 years. Time-dependent Cox proportional hazards model was used, and HRs were pooled together across the three cohorts.

Results

During 1,644,679 person-years of follow-up, we documented 6,641 new cases of type 2 diabetes. ADM use was associated with an increased risk of diabetes in all three cohorts in age-adjusted models (pooled HR 1.68 [95% CI 1.27, 2.23]). The association was attenuated after adjustment for diabetes risk factors and histories of high cholesterol and hypertension (1.30; 1.14, 1.49), and further attenuated by controlling for updated BMI (1.17; 1.09, 1.25). Uses of selective serotonin reuptake inhibitors and other antidepressants (mainly tricyclic antidepressants) were both associated with an elevated risk of diabetes, with pooled multivariate-adjusted HRs of 1.10 (1.00, 1.22) and 1.26 (1.11, 1.42), respectively.

Conclusions/interpretation

The results suggest that ADM users had a moderately elevated risk of type 2 diabetes mellitus compared to non-users, even after adjustment for BMI.

Keywords: antidepressant, depression, diabetes mellitus, prospective cohort study

INTRODUCTION

Antidepressant medication (ADM) use has substantially increased in the past decade in the US [1], becoming one of the most commonly prescribed classes of medications in outpatient medical practices [2, 3]. Antidepressants have been reported to cause considerable weight gain [4, 5] and impaired glucose homeostasis [6, 7]. Several studies have linked antidepressant medication use (ADM) and risk of type 2 diabetes, but the data are limited and inconsistent [8–13]. Previous studies are limited by the case-control study design [9, 10], or being restricted to high risk populations [8], or small sample sizes [11, 12]. Therefore, we investigated the association between ADM use (and types) and risk of developing type 2 diabetes mellitus in three large well-established cohorts: the Health Professionals Follow-up Study (HPFS), the Nurses’ Health Study (NHS) I and II.

METHODS

Study population

We used data from three prospective cohort studies: HPFS (initiated in 1986, n=51,529, age range 40–75), NHS I (started from 1976, n=121,704, age range 30–55), and NHS II (established in 1989, n=116,671, age range 25–42). Detailed descriptions of the three cohorts were introduced elsewhere [14–16]. In all three cohorts, questionnaires were administered at baseline and biennially thereafter, to collect and update information on lifestyle practice and occurrence of chronic diseases. The follow-up rates of the participants in these cohorts all exceeded 90%.

In the current analysis, we excluded participants who had diabetes (including type 1 and 2 diabetes mellitus and gestational diabetes), cardiovascular disease, or cancer at baseline (1990 for HPFS, 1996 for NHS I, and 1993 for NHS II). In addition, we excluded participants without baseline information on ADM use or BMI. Finally, data from 29,776 HPFS, 61,791 NHS I, and 76,868 NHS II participants were available for the analysis. The study protocol was approved by the institutional review boards of Brigham and Women’s Hospital and Harvard School of Public Health. All participants provided informed consents.

ADM measurement

Regular ADM use during the past two years was first assessed in 1990 for HPFS, 1996 for NHS I, and 1993 for NHS II. This information was updated biennially in each cohort, except for NHS II in 1995. Therefore, data from 1993 was carried forward to 1995. The types of ADM use were first inquired about in 1996 for HPFS, 2000 for NHS I, and 1993 for NHS II. In HPFS, men were specifically asked to report their regular use during the past two years of selective serotonin reuptake inhibitors (SSRIs, e.g., fluoxetine, sertraline, paroxetine, citalopram), tricyclic antidepressants (TCAs, e.g., amitriptyline, imipramine, and nortriptyline), and other antidepressants biennially since 1996. In NHS I, women provided information of SSRIs and other antidepressants, of which the TCAs were provided as examples. In NHS II, women were asked about their regular use of SSRIs and TCAs in 1993, 1997 and 1999, SSRIs and other types (TCAs as examples) biennially since 2001.

Depressive symptoms were assessed using the five-item Mental Health Index (MHI-5), a subscale of the Short-Form 36 Health Status Survey. The MHI-5 score has been shown to have high sensitivity and specificity for detection of major depressive disorder with the area under the receiver operating characteristic curve ranged from 0.89–0.94 [17,18]. The MHI-5 score was considered a dichotomous indicator of presence (MHI-5 score ≤52) or absence (MHI-5 score >52) of severe depressive symptoms (SDS). Using score value of 52 as the cut-off point, Yamazaki et al. [18] reported a sensitivity of 91.8% and specificity of 84.6%. However, MHI-5 was only available in 1992, 1996, and 2000 for NHS I, 1993, 1997, and 2001 for NHS II. No information on depressive symptoms was available for men. Women in NHS II in 2001 and men in HPFS in 2002 reported their lifetime history of depression by the following two questions: (1) In your lifetime, have you ever had 2 weeks or more when nearly everyday you felt sad, blue, or depressed for most of the day (0, no; 1, yes)? (2) Did you ever tell a doctor or mental health specialist that you were feeling depressed (0, no; 1, yes)? The study flow is shown in ESM Figure 1.

Assessment of diabetes

In all three cohorts, a supplementary questionnaire regarding symptoms, diagnostic tests, and hypoglycemic therapy was mailed to participants who reported a diagnosis of diabetes mellitus. A case of type 2 diabetes mellitus was considered confirmed if at least one of the following was reported on the supplementary questionnaire according to the National Diabetes Data Group criteria [19]: (1) one or more classic symptoms (excessive thirst, polyuria, weight loss, hunger) plus fasting plasma glucose levels of at least 7.8 mmol/l or random plasma glucose levels of at least 11.1 mmol/l; (2) at least two elevated plasma glucose concentrations on different occasions (fasting levels of at least 7.8 mmol/l, random plasma glucose levels of at least 11.1 mmol/l, and/or concentrations of at least 11.1 mmol/l after two hours or more shown by oral glucose tolerance testing) in the absence of symptoms; or (3) treatment with hypoglycemic medication (insulin or oral hypoglycemic agent). The diagnostic criteria changed in June 1998, and a fasting plasma glucose of 7.0 mmol/l was considered the threshold for the diagnosis of diabetes [20]. Self-reported type 2 diabetes diagnosis through supplemental questionnaire confirmation has been demonstrated to be highly accurate as compared to medical record reviews in validation studies [14, 21]. Out of a random sample of 62 NHS I participants who reported type 2 diabetes and were confirmed by the supplementary questionnaire, 61 (98%) of them were re-confirmed after their medical records were reviewed by an endocrinologist blinded to the supplementary questionnaire [21]. We conducted a similar validation study in the HPFS: of 59 type 2 diabetes cases who were confirmed by the supplementary questionnaire, 57 (97%) were re-confirmed by medical records [14]. In addition, in another substudy to assess the prevalence of undiagnosed diabetes in NHS I, fasting plasma glucose and plasma fructosamine were measured in a random sample of participants who did not report a previous diagnosis of diabetes. Only 1 (0.5%) of the women had an elevated fasting plasma glucose or plasma fructosamine level in the diabetic range, and her levels were barely above the diagnostic cutoffs [22]. By confirming all self-reported cases of diabetes, we exclude false-positive results, and the NHS I results suggest that the false-negative rate is low. We only included cases confirmed by the supplemental questionnaires in the current analysis.

Covariates

In the biennial follow-up questionnaires, we inquired about and updated information on risk factors for chronic diseases, such as body weight, cigarette smoking, physical activity, and a family history of diabetes mellitus, as well as a history of chronic diseases, including hypertension and hypercholesterolemia (and their medication treatments). Marital status and living status were updated every four years. Dietary information (including alcohol intake) was assessed using a validated semi-quantitative food frequency questionnaire every four years. A low-risk diet score was defined as a diet low in trans-fat and glycemic load, and high in cereal fiber and high ratio of polyunsaturated to saturated fat [15]. The dietary score summed the quintile values of the four nutrients with five representing the lowest-risk quintile in each dietary factor [15]. Among NHS I and II participants, we ascertained menopausal status, menopausal hormone use and oral contraceptive use.

Statistical analysis

Person-years for each participant was calculated from the date of return of the baseline questionnaire to the date of diagnosis of type 2 diabetes mellitus, death, the end of the follow-up (January 31, 2006 for HPFS, June 30, 2008 for NHS I, or June 30, 2007 for NHS II), or the date of return of their last questionnaire, whichever came first. Participants with missing information on ADM use during the follow-up were censored. Time-dependent Cox proportional hazards models were used to estimate age- and multivariable-adjusted HRs. In multivariable analysis, we adjusted for age, ethnicity, marital and living status, smoking status, alcohol intake, physical activity, current multivitamin and aspirin use, a family history of diabetes, quintile of dietary score, and major comorbidities (hypertension, hypercholesterolemia, and their treatments). Among nurses, we also adjusted for menopausal status and hormone use, and oral contraceptive use (NHS II participants only). Finally, we further adjusted for BMI. All the covariates were chosen by prior knowledge of their potential associations with diabetes or depression. ADM use and all the covariates were updated every 2–4 years and were treated as time-dependent variables, except for ethnicity and a family history of diabetes mellitus. Because ADM use may contribute to diabetes through weight gain, baseline BMI and subsequent weight gain in each 2-year interval were adjusted in a sensitivity analysis.

We investigated the association between different types of ADM and diabetes risk by categorizing the participants into four groups: non-users, only SSRIs users, only TCAs/others users, and multiple ADM users. Furthermore, we evaluated the association between ADM use and diabetes risk in participants with or without severe depressive symptoms in NHS I and II.

We also summarized the estimates of association across the three studies via a meta-analysis. Heterogeneity of HRs across studies was evaluated by the Cochrane Q statistic (p <0.10 was considered indicative of statistically significant heterogeneity). The HRs were pooled using the random-effects model if significant heterogeneity was detected, or the fixed-effect model otherwise. All p values were two-sided, and 95% CIs were calculated for HRs. Data were analyzed with the Statistical Analysis Systems software package, version 9.1 (SAS Institute Inc., Cary, North Carolina, USA).

RESULTS

We documented 1,287 incident cases of type 2 diabetes mellitus during 16 years of follow-up in HPFS (300,084 person-years), 3,514 cases during 12 years in NHS I (566,746 person-years), and 1,840 cases during 14 years in NHS II (777,930 person-years). Table 1 describes the distribution of baseline characteristics according to current ADM use status. The mean age was 56.4 years old in HPFS (range 43–80), 61.3 in NHS I (range 50–79), and 38.1 in NHS II (range 29–46). The baseline prevalence of current ADM use in the three cohorts (HPFS, NHS I and NHS II) was 1.2% in 1990, 6.7% in 1996, and 11.2% in 1993, respectively. There was a substantial increase in the prevalence of ADM use in all three cohorts over time (7.1% in 2004 for HPFS, 12.3% in 2006 for NHS I, and 22.2% in 2005 for NHS II, respectively). Current ADM users were less likely to be physically active, more likely to be smokers, to use multivitamin supplements, and to live alone and be unmarried. The prevalence of hypertension and hypercholesterolemia was higher in current ADM users. Current ADM users tended to have a higher BMI than non-users in women, but not in men. In addition, current ADM use was associated with a worse MHI-5 score in women.

Table 1.

Age-standardized Baseline Characteristics According to Antidepressant Medication Use Status in Three Cohorts.

Characteristics	HPFS (1990)		NHS I (1996)		NHS II (1993)

	No ADM	ADM	No ADM	ADM	No ADM	ADM
n	29411	365	57655	4136	68257	8611
Age (year)	56.4	56.3	61.4	59.8	37.9	39.3
Race (white, %)	95.6	95.5	97.5	98.7	96.4	97.5
Family history of diabetes (%)	20.3	22.6	26.3	26.8	33.8	36.3
BMI (kg/m²)	25.5	25.6	26.2	27.2	25.0	26.5
Physical activity (MET-hrs/wk)	38.3	27.3	18.4	14.5	21.6	19.4
Smoking status (%)
Current smoker	7.5	10.8	12.6	13.8	10.4	17.4
Past smoker	41.7	46.0	42.1	46.7	22.8	26.1
Never smoked	50.8	43.2	45.3	39.5	66.8	56.5
Marital status (with spouse, %)	89.3	81.8	78.7	74.2	81.3	69.9
Living status (alone, %)	6.7	11.8	14.5	17.5	8.4	14.0
Dietary score^a	12.0	11.4	12.0	11.9	12.0	11.9
Alcohol (g/day)	10.3	9.1	5.3	4.7	3.2	3.2
Current aspirin user (%)	31.0	32.0	52.8	47.9	9.5	14.4
Multivitamin supplement user (%)	36.9	42.5	52.0	57.3	43.6	48.0
Menopausal status (premenopausal, %)	NA	NA	12.1	13.2	95.4	90.9
Ever menopause hormone use (%)^b	NA	NA	57.9	71.2	14.8	26.3
Ever oral contraceptive use (%)^b	NA	NA	NA	NA	84.2	90.2
Hypertension (%)	23.8	29.5	36.4	43.8	6.8	12.2
Hypercholesterolemia (%)	28.4	40.5	50.3	60.0	16.0	25.4
MHI-5 Score	NA	NA	80.2	68.5	72.7	62.2
Severe depressive symptoms (%)^c	NA	NA	4.6	20.9	11.1	30.8

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Abbreviations: MET-hrs/wk, metabolic equivalent-hours/week; MHI-5, five-item Mental Health Index; HPFS, Health Professional Follow-up Study; NA, not available; NHS: Nurses’ Health Study.

Dietary score was defined as sum of quintiles of cereal fiber, glycemic load (reverse), polyunsaturated to saturated fat ratio, and trans fat (reverse) consumptions.

Current plus past users.

Severe depressive symptoms were defined as MHI-5 score 0–52.

In age-adjusted models, ADM users had an elevated risk of developing type 2 diabetes mellitus across the three cohorts (Table 2). The average absolute risk differences between ADM users and non-users were 2.87 per 1000 person-years. Adjustment for updated BMI attenuated the associations in women, but not in men. The final multivariable-adjusted HRs (95% CIs) were 1.37 (1.07, 1.76) for HPFS, 1.10 (1.00, 1.21) for NHS I, and 1.23 (1.11, 1.37) for NHS II. The HRs were slightly attenuated with further adjustment for MHI-5 scores in NHS I and II, and became non-significant for NHS I (HR 1.08 [0.97, 1.19]). After pooling the estimates across the three studies, the HR for developing type 2 diabetes associated with current ADM use was 1.17 (1.09, 1.25).

Table 2.

Antidepressant medication (ADM) use and risk of type 2 diabetes in the three cohorts.

	HPFS (1990–2006)		NHS I (1996–2008)		NHS II (1993–2007)		Pooled (Random effects model)

	No ADM	ADM	No ADM	ADM	No ADM	ADM	No ADM	ADM
Cases/person-years	1219/290794	68/9290	3040/511713	474/55033	1337/672931	503/104999	5596/1475438	1045/169241
Crude incidence, per 1000 person-years	4.19	7.32	5.94	8.61	1.99	4.79	3.79	6.17
Age-adjusted model	1.00	1.66 (1.30–2.12)	1.00	1.40 (1.27–1.54)	1.00	2.05 (1.84–2.27)	1.00	1.68 (1.27–2.23)
Multivariable-adjusted model^a	1.00	1.34 (1.04–1.72)	1.00	1.19 (1.08–1.31)	1.00	1.42 (1.28–1.58)	1.00	1.30 (1.14–1.49)
Further adjusted for BMI^b	1.00	1.37 (1.07–1.76)	1.00	1.10 (1.00–1.21)	1.00	1.23 (1.11–1.37)	1.00	1.17 (1.09–1.25)^d
Further adjusted for MHI-5 score^c	NA	NA	1.00	1.08 (0.97–1.19)	1.00	1.21 (1.08–1.35)	NA	NA

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Abbreviations: MHI-5, five-item Mental Health Index; HPFS, Health Professional Follow-up Study; NA, not available; NHS: Nurses’ Health Study.

Hazard ratios were adjusted for age (continuous), ethnicity (whites, non-whites), marital status (having spouse or not), living status (alone, with others), smoking status (never smoked, past smoker, current smoker), alcohol intake (0, 0.1–4.9, 5.0–14.9, ≥15.0 g/d in women, 0, 0.1–4.9, 5.0–29.9, ≥30.0 g/d in men), multivitamin and aspirin use (yes, no), physical activity (<3.0, 3.0–8.9, 9.0–17.9, 18.0–26.9, and ≥27.0 metabolic equivalent-hours/week), family history of diabetes, major comorbidities (history of hypertension, hypercholesterolemia, and their treatments), and quintile of dietary score. Among women, we also adjusted for menopausal status and hormone use, and oral contraceptive use (NHS II participants only).

Hazard ratios were further adjusted for BMI (<23.0, 23.0–24.9, 25.0–29.9, 30.0–34.9, and ≥35.0 kg/m²).

Hazard ratios were further adjusted for five-item Mental Health Index (0–52, 53–75, 76–85, 86–100).

Fixed effect model was chosen due to non-significant heterogeneity statistic (p >0.10).

We further analyzed the association between different types of ADM and diabetes risk (Table 3). Neither type of ADM was associated with diabetes risk in NHS I and HPFS. Both SSRIs and TCAs/others were associated with increased risks in NHS II, which were not substantially attenuated after adjustment for MHI-5 score. In HPFS, HR of diabetes for TCAs/others use was 1.50 (95% CI 0.96, 1.35), while HR for only TCAs use was 2.67 (95% CI 1.66, 4.29). The pooled HRs (95% CIs) for SSRIs, TCAs/others, and multiple types uses were 1.10 (1.00, 1.22), 1.26 (1.11, 1.42), and 1.09 (0.74, 1.61), respectively.

Table 3.

Different types of antidepressant medication (ADM) use and diabetes risk in three cohorts.

	Cases /person-years	Crude incidence, per 1000 person-years	Age-adjusted model	Multivariable-adjusted model^a	Further adjusted for BMI^b	Further adjusted for MHI-5 score^c
HPFS (1996–2006)
No ADM	827/172521	4.79	1.00	1.00	1.00	NA
SSRIs	33/4988	6.62	1.45 (1.02–2.06)	1.17 (0.82–1.67)	1.13 (0.79–1.60)	NA
TCAs, others	20/2614	7.65	1.69 (1.08–2.63)	1.37 (0.88–2.14)	1.50 (0.96–2.35)	NA
Multiple	3/346	8.67	2.07 (0.67–6.46)	1.39 (0.45–4.33)	1.22 (0.39–3.84)	NA
NHS I (2000–2008)
No ADM	1890/303466	6.23	1.00	1.00	1.00	1.00
SSRIs	206/25728	8.01	1.28 (1.10–1.47)	1.11 (0.96–1.28)	1.01 (0.87–1.17)	0.99 (0.85–1.15)
TCAs, others	109/12619	8.64	1.38 (1.14–1.68)	1.19 (0.98–1.44)	1.14 (0.93–1.38)	1.12 (0.92–1.36)
Multiple	26/3253	7.99	1.26 (0.85–1.86)	0.98 (0.66–1.44)	0.87 (0.59–1.29)	0.84 (0.57–1.25)
NHS II (1993–2007)
No ADM	1337/672931	1.99	1.00	1.00	1.00	1.00
SSRIs	306/59796	5.12	2.01 (1.78–2.28)	1.44 (1.27–1.64)	1.18 (1.04–1.34)	1.16 (1.02–1.32)
TCAs, others	137/33788	4.05	1.91 (1.60–2.28)	1.35 (1.12–1.61)	1.33 (1.11–1.59)	1.31 (1.09–1.57)
Multiple	60/11415	5.26	2.70 (2.08–3.51)	1.52 (1.17–1.98)	1.30 (1.00–1.69)	1.26 (0.96–1.65)
Pooled results (random effects model)
No ADM	4054/1148918	3.53	1.00	1.00	1.00	NA
SSRIs	545/90512	6.02	1.56 (1.11–2.20)	1.25 (1.02–1.52)	1.10 (1.00–1.22)^d	NA
TCAs, others	266/49021	5.43	1.64 (1.29–2.08)	1.28 (1.13–1.45)^d	1.26 (1.11–1.42)^d	NA
Multiple	89/15014	5.93	1.91 (1.04–3.35)	1.25 (0.81–1.92)	1.09 (0.74–1.61)	NA

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Abbreviations: BMI, body-mass index; MHI-5, five-item Mental Health Index; HPFS, Health Professional Follow-up Study; NA, not available; NHS: Nurses’ Health Study.

Hazard ratios were adjusted for age (continuous), ethnicity (whites, non-whites), marital status (having spouse or not), living status (alone, with others), smoking status (never smoked, past smoker, current smoker), alcohol intake (0, 0.1–4.9, 5.0–14.9, ≥15.0 g/d in women, 0, 0.1–4.9, 5.0–29.9, ≥30.0 g/d in men), multivitamin and aspirin use (yes, no), physical activity (<3.0, 3.0–8.9, 9.0–17.9, 18.0–26.9, and ≥27.0 Metabolic Equivalent-hours/week), family history of diabetes, major comorbidities (history of hypertension, hypercholesterolemia, and their treatments), and quintile of dietary score. Among women, we also adjusted for menopausal status and hormone use, and oral contraceptive use (NHS II participants only).

Hazard ratios were further adjusted for BMI (<23.0, 23.0–24.9, 25.0–29.9, 30.0–34.9, and ≥35.0 kg/m²).

Hazard ratios were further adjusted for five-item Mental Health Index (0–52, 53–75, 76–85, 86–100).

Fixed effect model was chosen due to non-significant heterogeneity statistic (p >0.10).

We also investigated the joint association of current ADM use and SDS with diabetes risk in women (Table 4). In the old-age cohort (NHS I), participants with both SDS and ADM use had an increased risk, while those with only SDS or ADM use had no increased risk. In the young-age cohort (NHS II), SDS and ADM use was individually and jointly associated with increased risk. However, no significant interaction was found in either NHS I (p for interaction = 0.60) or NHS II (p for interaction = 0.20). After pooling results from the two cohorts, compared with women without SDS and ADM use, ADM use alone and SDS alone was associated with a 15% (6%, 24%) and 14% (1%, 28%) increased risk of type 2 diabetes, respectively, while the combination of SDS and ADM use was associated with a 25% (9%, 44%) increased risk.

Table 4.

Risk of type 2 diabetes according to severe depressive symptoms (SDS) and antidepressant medication (ADM) use in the Nurses Health Studies (NHS). ^a

	No SDS		SDS

	No ADM use	ADM use	No ADM use	ADM use
NHS I (1996–2008)
Cases/person-years	2810/478455	376/44980	128/18707	90/8520
Crude incidence, per 1000 person-years	5.87	8.36	6.84	10.56
Age-adjusted model	1.00	1.37 (1.23–1.52)	1.20 (1.01–1.43)	1.77 (1.43–2.18)
Multivariable-adjusted model^b	1.00	1.18 (1.05–1.31)	1.05 (0.88–1.26)	1.38 (1.12–1.71)
Further adjusted for BMI^c	1.00	1.09 (0.97–1.21)	1.10 (0.92–1.31)	1.30 (1.05–1.61)

NHS II (1993–2007)
Cases/person-years	1107/573190	342/74137	162/61832	131/25689
Crude incidence, per 1000 person-years	1.93	4.61	2.62	5.10
Age-adjusted model	1.00	1.98 (1.75–2.24)	1.48 (1.25–1.75)	2.42 (2.02–2.90)
Multivariable-adjusted model^b	1.00	1.44 (1.27–1.63)	1.20 (1.02–1.42)	1.37 (1.14–1.65)
Further adjusted for BMI^c	1.00	1.23 (1.08–1.39)	1.17 (0.99–1.38)	1.22 (1.01–1.47)
Pooled results^d
Final multivariate adjusted model	1.00	1.15 (1.06–1.24)	1.14 (1.01–1.28)	1.25 (1.09–1.44)

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Abbreviations: BMI, body-mass index.

Severe depressive symptoms were defined as five-item Mental Health Index score 0–52.

Hazard ratios were further adjusted for BMI (<23.0, 23.0–24.9, 25.0–29.9, 30.0–34.9, and ≥35.0 kg/m²).

Results were pooled by fixed-effect models due to non-significant heterogeneity statistic (p for heterogeneity all >0.10).

In a sensitivity analysis of controlling for baseline BMI along with weight change in each interval instead of updated BMI, the results were similar (HR 1.20 [95% CI 1.12, 1.28]). The results were also similar for adjustment of updated BMI as a continuous variable (HR 1.16 [95% CI 1.08, 1.25]). Analyses stratified by age, overweight, significant weight gain (defined as weight gain of more than 5%), history of hypertension or hypercholesterolemia revealed similar risk estimates and no indications of interactions (Supplemental Table 1). Only baseline ADM use was not a predictor for incident type 2 diabetes (pooled HR 1.07 [95% CI 0.94, 1.22]), while the incident ADM use (excluding the baseline prevalent ADM users from the analysis) was associated with a significantly increased risk of type 2 diabetes (pooled HR 1.27 [95% CI 1.08, 1.48]), suggesting that recent ADM use might be more relevant to the elevated risk.

DISCUSSION

In the three cohorts of more than 160,000 US men and women with 12–16 years of follow-up, ADM users were at a moderately increased risk of developing type 2 diabetes mellitus after adjusting for diabetes risk factors. The increased risk did not appear to differ by types of ADM (SSRIs or others). The association was in part but not completely explained by BMI

The relationship between depression and diabetes is of particular interest, since both conditions are major contributors to the global burden of chronic diseases. Several epidemiological studies have documented a bidirectional association between depression and diabetes: depression increases the risk of developing diabetes, and vice verse, diabetes is also associated with an increased risk of being depressed [23, 24]. However, whether antidepressant treatment could elevate diabetes risk remains controversial. Rubin et al.[8] found in the Diabetes Prevention Program (DPP) study that ADM use (78% were SSRIs) was associated with a more than two-fold increased risk of type 2 diabetes among participants with impaired glucose tolerance who were assigned to lifestyle or placebo diabetes prevention interventions, even after controlling for depressive symptoms. However, the increased risk was not detected in participants in metformin intervention arm [8]. Recently, two large nested case-control studies using medical record database in the UK [9] and Finland [10] both found an increased diabetes risk associated with long-term ADM use of moderate and/or high daily doses for depression treatment, and the association was independent of depression severity. The associations were found for both SSRIs and TCAs in these two studies [9, 10]. A cohort study among 1000 older Australians found that ADM use was associated with an 80% (95% CI −9%, 257%) non-significant increased risk [12]. Campayo et al. [13] found in a Spanish community sample of adults aged ≥55 years (n=3,521) that the HR for ADM use was 1.26 (95% CI 0.63, 2.50). Knol et al. [11] used prescription data from the PHARMO database and did not find an increased risk in antidepressant users. However, this study lacked information on BMI and lifestyle factors, and included only patients with anti-diabetic treatment as diabetes cases. We also found that only baseline ADM use did not predict risk of type 2 diabetes, suggesting that recent ADM use might be more relevant to the elevated risk. The results concurred with Andersohn’s findings [9] that recent ADM use was positively associated with the risk of type 2 diabetes, but not past use or former use of antidepressants.

To the best of our knowledge, the current analysis is the largest prospective cohort study investigating the association between ADM use and diabetes risk. Despite heterogeneity in study design, population characteristics and risk estimates, our findings are largely consistent with those from previous studies. The results from NHS I were somewhat weaker than those from NHS II and HPFS. Despite homogeneity in study design and target population (health professionals or nurses, mostly whites), the cohorts have considerable heterogeneity. First, the age ranges are different. The NHS I encompasses middle-aged and elderly women (50–79 years old at baseline), while NHS II consists of a group of younger women (29–46 years old at baseline). One potential reason for the null association in NHS I was that the early-onset diabetes had been excluded, and participants with severe depression were more likely to withdraw from the study during the early follow-up of the entire cohort before 1996 (1976–1996), and thus, the remaining participants in NHS I were relatively less depressed. Whether the increased risk found in NHS II but not in NHS I reflects an age-specific effects of ADM on diabetes risk remains unclear and deserves further investigation. Second, the prevalence of ADM use was substantially lower in men compared to women. This might reflect the gender difference of depression prevalence [25], as well as the reluctance of men to seek [26] or receive treatment [27] compared to women. In the current study, the baseline ADM use prevalence in HPFS was 1.2% in 1990, which was consistent with the National Comorbidity Survey 1990–1992 where 1.4% of male participants reported ADM use [28]. This prevalence climbed to 2.9% in 1996 and 7.1% in 2004 in HPFS. The prevalence of ADM use over time in our studies was consistent with several national data [1, 28]. Finally, the results of specific types of ADM use should be interpreted cautiously because the reasons for prescribing the specific types of ADM may be different. The prevalence of SSRIs use has increased in all three cohorts over time, which was coincident with the practice that SSRIs have became the first-line treatment for depression during the follow-up [29]. Individuals using TCAs or multiple types were more likely to be non-responsive to the initial medication [29].

Antidepressants might be associated with an increased diabetes risk through a variety of mechanisms. First, ADM use may primarily be a marker of depression severity and/or chronicity, and depression has been shown to increase risk of subsequent diabetes [23, 24]. ADM users might have been more severely depressed or have a history of chronic or recurrent depression. Second, ADM use was associated with poor health behaviors (i.e., smoking and physical inactivity) and high prevalence of major comorbidities in this study. Although we controlled for a large number of health behavior factors and other medical conditions, residual confounding is still possible. Furthermore, weight gain is a common side effect in short- and long-term treatment with TCAs [4]. There is evidence of an initial stable weight or even weight loss with the use of SSRIs, followed by weight gain in the long-term phase [5]. Kivimaki et al. [10] found that ADM use (and different types) was associated with significantly more weight gain compared to non-users in a nested case-control study. The association between ADM use and diabetes was largely attenuated but remained significant even after controlling for updated BMI or weight gain in our study, which is consistent with the DPP results [8], suggesting that other mechanisms beyond weight gain may have a role. Moreover, a mechanistic study found that some SSRIs could act as inhibitors of insulin signaling and as potential inducers of cellular insulin resistance [6]. Different ADMs have varied binding affinities to various receptors, which may be involved in different effects on insulin secretion and action [30]. The associations with different types of ADM, even within a certain type, have been suggested by a recent report [9]. Therefore, future studies need to be more specific on types of ADM, beyond those of SSRIs and TCAs, and should examine more recent forms of ADM, such as serotonin-norepinephrine reuptake inhibitors.

Strengths, limitations and implications

Strengths of the current study include the large sample size, long-term follow-up, and biennially updated information on medication use, disease onset and lifestyle risk factors. Time-dependent Cox models were performed to incorporate these repeated measures, which minimized the possibility of residual and time-dependent confounding.

This study also has several limitations and the results should be interpreted with caution. First, our study populations primarily consisted of health professionals with European ancestry. Although their concern about health status and better understanding of health-related issues enhanced the reliability and validity of our questionnaire data, the generalizability to other populations may be limited. Nevertheless, it appears unlikely that the fundamental biology underlying a relation of ADM to diabetes would be different between our cohorts and the general population.

Second, the diabetes cases were self-reported, but we only included cases confirmed by the supplemental questionnaires. Moreover, information on ADM use was self-reported, and we could not assess the association between specific agents, doses and duration of drug use with diabetes risk. Furthermore, we lacked clinical data on participants’ depression history, severity and chronicity. Notably, ADM use may be a marker of depression severity and/or chronicity, and it is possible that the underlying more severe depressive disorder rather than ADM use increases risk of diabetes. We attempted to account for this by adjusting for a depressive score in women, but residual confounding may remain since this score could not capture the history and chronicity of depression, and we did not have depressive symptoms information in men. Aspecific depression symptoms measure (such as the Diagnostic Interview Schedule, Center for Epidemiologic Studies Depression Scale) may better capture the severity of depression.

Another limitation is that ADMs can be used for conditions other than depression, such as anxiety disorders, insomnia, neuropathic pain, and premenstrual syndrome and hot flushes in women. We could not distinguish different indications for ADMs in our cohorts. In a secondary analysis, we found that 79% of ADM users in HPFS reported a lifetime history of depression in 2002, and the proportion was 91% in NHS II in 2001, when questions about lifetime history of depression were asked. These data indicate that the majority of participants used ADM for treating depression or related symptoms.

In addition, surveillance bias due to the disease diagnosis is also possible in our analyses, although our participants had regular physical examinations and ready access to health care system. Finally, our results cannot prove causality, like any other observational data. Studies with post-intervention follow-up of existing randomized placebo-controlled antidepressant trials can be used to evaluate the effects on glucose homeostasis, insulin sensitivity and diabetes risk.

In conclusion, the results from the three large long-term cohort studies suggest that individuals with antidepressant treatment had a moderately increased risk of developing type 2 diabetes. This association appeared to be partly mediated through BMI, particularly in women. However, this study cannot determine whether ADM use is a causal risk factor for type 2 diabetes, or serves as a marker of depression severity/chronicity. Additional research is needed to confirm these results with more detailed information on dose and duration of treatment, and other clinical parameters. Mechanistic studies are also required to better understand the influence of antidepressants on glucose tolerance and carbohydrate metabolism. Before conclusive evidence on this relationship is obtained, patients with depression are recommended to adhere to their treatment strategies with careful attention of their body weights and blood glucose levels.

Supplementary Material

ESM Figure 1

NIHMS319485-supplement-ESM_Figure_1.pdf^{(24.3KB, pdf)}

ESM Table 1

NIHMS319485-supplement-ESM_Table_1.pdf^{(81.2KB, pdf)}

Acknowledgments

We are indebted to the participants in the Health Professional Follow-up Study, Nurses’ Health Study I and II for their continuing outstanding support and colleagues working in these studies for their valuable help. We also want to thank Dr. Alberto Ascherio of Department of Nutrition, Harvard School of Public Health for his suggestions on the statistical analysis and results interpretation.

Funding/Support

The study was supported by the National Institutes of Health grant (DK58845, CA55075, CA87969, CA50385). Q. Sun was supported by a career development award K99HL098459 from the National Heart, Lung, and Blood Institute. M. Lucas received a postdoctoral fellowship from the Fonds de recherche en santé du Québec (FRSQ). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.

Abbreviations

ADM: Antidepressant medication
DPP: Diabetes Prevention Program
HPFS: Health Professionals Follow-up Study
MHI-5: five-item Mental Health Index
NHS: Nurses’ Health Study
SDS: Severe Depressive Symptoms
SSRI: selective serotonin reuptake inhibitor
TCA: tricyclic antidepressant

Footnotes

Conflict of Interest

The authors declare that there is no duality of interest associated with this manuscript.

Author Contributions

A.P. contributed to conception and design, analysis and interpretation of data and manuscript drafting. Q.S., O.I.O., K.M.R., R.R.R., M.L. contributed to conception and design, manuscript revision. W.C.W., J.E.M. contributed to conception and design, acquisition of funding and manuscript revision. F.B.H. contributed to conception and design, analysis and interpretation of data, acquisition of funding and manuscript revision. All authors have approved the final version of the manuscript to be published.

References

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22.Field AE, Coakley EH, Must A, et al. Impact of overweight on the risk of developing common chronic diseases during a 10-year period. Arch Intern Med. 2001;161:1581–1586. doi: 10.1001/archinte.161.13.1581. [DOI] [PubMed] [Google Scholar]
23.Mezuk B, Eaton WW, Albrecht S, et al. Depression and type 2 diabetes over the lifespan: a meta-analysis. Diabetes Care. 2008;31:2383–2390. doi: 10.2337/dc08-0985. [DOI] [PMC free article] [PubMed] [Google Scholar]
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25.Belmaker RH, Agam G. Major depressive disorder. N Engl J Med. 2008;358:55–68. doi: 10.1056/NEJMra073096. [DOI] [PubMed] [Google Scholar]
26.Mojtabai R. Americans’ attitudes toward mental health treatment seeking: 1990–2003. Psychiatr Serv. 2007;58:642–651. doi: 10.1176/ps.2007.58.5.642. [DOI] [PubMed] [Google Scholar]
27.Wang PS, Lane M, Olfson M, et al. Twelve-month use of mental health services in the United States: results from the National Comorbidity Survey Replication. Arch Gen Psychiatry. 2005;62:629–640. doi: 10.1001/archpsyc.62.6.629. [DOI] [PubMed] [Google Scholar]
28.Mojtabai R. Increase in antidepressant medication in the US adult population between 1990 and 2003. Psychother Psychosom. 2008;77:83–92. doi: 10.1159/000112885. [DOI] [PubMed] [Google Scholar]
29.American Psychiatric Association. Practice guideline for the treatment of patients with major depressive disorder. 3. Arlington, Virginia, USA: 2010. [PubMed] [Google Scholar]
30.McIntyre RS, Soczynska JK, Konarski JZ, et al. The effect of antidepressants on glucose homeostasis and insulin sensitivity: synthesis and mechanisms. Expert Opin Drug Saf. 2006;5:157–168. doi: 10.1517/14740338.5.1.157. [DOI] [PubMed] [Google Scholar]

Associated Data

This section collects any data citations, data availability statements, or supplementary materials included in this article.

Supplementary Materials

ESM Figure 1

NIHMS319485-supplement-ESM_Figure_1.pdf^{(24.3KB, pdf)}

ESM Table 1

NIHMS319485-supplement-ESM_Table_1.pdf^{(81.2KB, pdf)}

[R1] 1.Olfson M, Marcus SC. National patterns in antidepressant medication treatment. Arch Gen Psychiatry. 2009;66:848–856. doi: 10.1001/archgenpsychiatry.2009.81. [DOI] [PubMed] [Google Scholar]

[R2] 2.Cherry DK, Woodwell DA, Rechtsteiner EA. National Ambulatory Medical Care Survey: 2005 summary. Adv Data. 2007;387:1–39. [PubMed] [Google Scholar]

[R3] 3.Middleton K, Hing E, Xu J. National Hospital Ambulatory Medical Care Survey: 2005 outpatient department summary. Adv Data. 2007;389:1–34. [PubMed] [Google Scholar]

[R4] 4.Zimmermann U, Kraus T, Himmerich H, et al. Epidemiology, implications and mechanisms underlying drug-induced weight gain in psychiatric patients. J Psychiatr Res. 2003;37:193–220. doi: 10.1016/s0022-3956(03)00018-9. [DOI] [PubMed] [Google Scholar]

[R5] 5.Sussman N, Ginsberg DL, Bikoff J. Effects of nefazodone on body weight: a pooled analysis of selective serotonin reuptake inhibitor- and imipramine-controlled trials. J Clin Psychiatry. 2001;62:256–260. [PubMed] [Google Scholar]

[R6] 6.Levkovitz Y, Ben-Shushan G, Hershkovitz A, et al. Antidepressants induce cellular insulin resistance by activation of IRS-1 kinases. Mol Cell Neurosci. 2007;36:305–312. doi: 10.1016/j.mcn.2007.05.009. [DOI] [PubMed] [Google Scholar]

[R7] 7.Derijks HJ, Meyboom RH, Heerdink ER, et al. The association between antidepressant use and disturbances in glucose homeostasis: evidence from spontaneous reports. Eur J Clin Pharmacol. 2008;64:531–538. doi: 10.1007/s00228-007-0441-y. [DOI] [PMC free article] [PubMed] [Google Scholar]

[R8] 8.Rubin RR, Ma Y, Peyrot M, et al. Antidepressant medicine use and risk of developing diabetes during the Diabetes Prevention Program and Diabetes Prevention Program Outcomes Study. Diabetes Care. 2010;33:2549–2551. doi: 10.2337/dc10-1033. [DOI] [PMC free article] [PubMed] [Google Scholar]

[R9] 9.Andersohn F, Schade R, Suissa S, et al. Long-term use of antidepressants for depressive disorders and the risk of diabetes mellitus. Am J Psychiatry. 2009;66:591–598. doi: 10.1176/appi.ajp.2008.08071065. [DOI] [PubMed] [Google Scholar]

[R10] 10.Kivimaki M, Hamer M, Batty GD, et al. Antidepressant medication use, weight gain and risk of type 2 diabetes: a population-based study. Diabetes Care. 2010;33:2611–2616. doi: 10.2337/dc10-1187. [DOI] [PMC free article] [PubMed] [Google Scholar]

[R11] 11.Knol MJ, Geerlings MI, Egberts AC, et al. No increased incidence of diabetes in antidepressant users. Int Clin Psychopharmacol. 2007;22:382–386. doi: 10.1097/YIC.0b013e3282202c0e. [DOI] [PubMed] [Google Scholar]

[R12] 12.Atlantis E, Browning C, Sims J, et al. Diabetes incidence associated with depression and antidepressants in the Melbourne Longitudinal Studies on Healthy Ageing (MELSHA) Int J Geriatr Psychiatry. 2010;25:688–696. doi: 10.1002/gps.2409. [DOI] [PubMed] [Google Scholar]

[R13] 13.Campayo A, de Jonge P, Roy JF, et al. Depressive disorder and incident diabetes mellitus: the effect of characteristics of depression. Am J Psychiatry. 2010;167:580–588. doi: 10.1176/appi.ajp.2009.09010038. [DOI] [PubMed] [Google Scholar]

[R14] 14.Hu FB, Leitzmann MF, Stampfer MJ, Colditz GA, Willett WC, Rimm EB. Physical activity and television watching in relation to risk for type 2 diabetes mellitus in men. Arch Intern Med. 2001;161:1542–1548. doi: 10.1001/archinte.161.12.1542. [DOI] [PubMed] [Google Scholar]

[R15] 15.Hu FB, Manson JE, Stampfer MJ, et al. Diet, lifestyle, and the risk of type 2 diabetes mellitus in women. N Engl J Med. 2001;345:790–797. doi: 10.1056/NEJMoa010492. [DOI] [PubMed] [Google Scholar]

[R16] 16.Schulze MB, Manson JE, Willett WC, Hu FB. Processed meat intake and incidence of type 2 diabetes in younger and middle-aged women. Diabetologia. 2003;46:1465–1473. doi: 10.1007/s00125-003-1220-7. [DOI] [PubMed] [Google Scholar]

[R17] 17.Berwick DM, Murphy JM, Goldman PA, et al. Performance of a five-item mental health screening test. Med Care. 1991;29:169–176. doi: 10.1097/00005650-199102000-00008. [DOI] [PubMed] [Google Scholar]

[R18] 18.Yamazaki S, Fukuhara S, Green J. Usefulness of five-item and three-item Mental Health Inventories to screen for depressive symptoms in the general population of Japan. Health Qual Life Outcomes. 2005;8:3–48. doi: 10.1186/1477-7525-3-48. [DOI] [PMC free article] [PubMed] [Google Scholar]

[R19] 19.American Diabetes Association. Classification and diagnosis of diabetes mellitus and other categories of glucose intolerance. National Diabetes Data Group. Diabetes. 1979;28:1039–1057. doi: 10.2337/diab.28.12.1039. [DOI] [PubMed] [Google Scholar]

[R20] 20.American Diabetes Association. Report of the expert committee on the diagnosis and classification of diabetes mellitus. Diabetes Care. 1997;20:1183–1197. doi: 10.2337/diacare.20.7.1183. [DOI] [PubMed] [Google Scholar]

[R21] 21.Manson JE, Rimm EB, Stampfer MJ, et al. Physical activity and incidence of non-insulin-dependent diabetes mellitus in women. Lancet. 1991;338:774–778. doi: 10.1016/0140-6736(91)90664-b. [DOI] [PubMed] [Google Scholar]

[R22] 22.Field AE, Coakley EH, Must A, et al. Impact of overweight on the risk of developing common chronic diseases during a 10-year period. Arch Intern Med. 2001;161:1581–1586. doi: 10.1001/archinte.161.13.1581. [DOI] [PubMed] [Google Scholar]

[R23] 23.Mezuk B, Eaton WW, Albrecht S, et al. Depression and type 2 diabetes over the lifespan: a meta-analysis. Diabetes Care. 2008;31:2383–2390. doi: 10.2337/dc08-0985. [DOI] [PMC free article] [PubMed] [Google Scholar]

[R24] 24.Pan A, Lucas M, Sun Q, et al. Bidirectional association between depression and type 2 diabetes in women. Arch Intern Med. 2010;170:1884–1891. doi: 10.1001/archinternmed.2010.356. [DOI] [PMC free article] [PubMed] [Google Scholar]

[R25] 25.Belmaker RH, Agam G. Major depressive disorder. N Engl J Med. 2008;358:55–68. doi: 10.1056/NEJMra073096. [DOI] [PubMed] [Google Scholar]

[R26] 26.Mojtabai R. Americans’ attitudes toward mental health treatment seeking: 1990–2003. Psychiatr Serv. 2007;58:642–651. doi: 10.1176/ps.2007.58.5.642. [DOI] [PubMed] [Google Scholar]

[R27] 27.Wang PS, Lane M, Olfson M, et al. Twelve-month use of mental health services in the United States: results from the National Comorbidity Survey Replication. Arch Gen Psychiatry. 2005;62:629–640. doi: 10.1001/archpsyc.62.6.629. [DOI] [PubMed] [Google Scholar]

[R28] 28.Mojtabai R. Increase in antidepressant medication in the US adult population between 1990 and 2003. Psychother Psychosom. 2008;77:83–92. doi: 10.1159/000112885. [DOI] [PubMed] [Google Scholar]

[R29] 29.American Psychiatric Association. Practice guideline for the treatment of patients with major depressive disorder. 3. Arlington, Virginia, USA: 2010. [PubMed] [Google Scholar]

[R30] 30.McIntyre RS, Soczynska JK, Konarski JZ, et al. The effect of antidepressants on glucose homeostasis and insulin sensitivity: synthesis and mechanisms. Expert Opin Drug Saf. 2006;5:157–168. doi: 10.1517/14740338.5.1.157. [DOI] [PubMed] [Google Scholar]

PERMALINK

Use of antidepressant medication and risk of type 2 diabetes: results from three cohorts of US adults

A Pan

Q Sun

O I Okereke

K M Rexrode

R R Rubin

M Lucas

W C Willett

J E Manson

F B Hu

Abstract

Aims/hypothesis

Methods

Results

Conclusions/interpretation

INTRODUCTION

METHODS

Study population

ADM measurement

Assessment of diabetes

Covariates

Statistical analysis

RESULTS

Table 1.

Table 2.

Table 3.

Table 4.

DISCUSSION

Strengths, limitations and implications

Supplementary Material

Acknowledgments

Abbreviations

Footnotes

References

Associated Data

Supplementary Materials

ACTIONS

PERMALINK

RESOURCES

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