OBJECTIVE

Studies in type 2 diabetes report both increased mortality for normal weight and no evidence of an obesity paradox. We aimed to examine whether adipose tissue, muscle size, and physical function, which are known to vary by weight, mediate associations between BMI and mortality.

RESEARCH DESIGN AND METHODS

The AGES-Reykjavik cohort comprised participants aged 66–96 years with diabetes defined by fasting glucose, medications, or self-report. BMI was determined from measured height and weight and classified as normal (18.5–24.9 kg/m2, n = 117), overweight (25.0–29.9 kg/m2, n = 293, referent group) or obese (≥30.0 kg/m2, n = 227). Thigh muscle area and intermuscular, visceral, and subcutaneous adipose tissues were assessed with computed tomography. Function was assessed from gait speed and knee extensor strength. Hazard ratios (HRs) and 95% CIs were estimated by Cox proportional hazards regression adjusted for demographics and diabetes-related risk factors.

RESULTS

The median follow-up was 6.66 years, and there were 85, 59, and 44 deaths among normal weight, overweight, and obese participants, respectively. There was no mortality risk for obese participants and an increased risk among normal weight compared with overweight participants (HR 1.72 [95% CI 1.12–2.64]). Associations remained with adjustment for adipose tissues and knee extensor strength; however, mortality risk for normal weight was attenuated following adjustment for thigh muscle (HR 1.36 [95% CI 0.87–2.11]) and gait speed (HR 1.44 [95% CI 0.91–2.27]). Linear regression confirmed with bootstrapping indicated that thigh muscle size mediated 46% of the relationship between normal weight and mortality.

CONCLUSIONS

Normal weight participants had elevated mortality risk compared with overweight participants. This paradoxical association was mediated in part by muscle size.

The negative health outcomes of obesity, including elevated mortality risk, are widely documented and accepted (13). However, numerous studies in free-living populations (4) and individuals with chronic disease, including chronic kidney disease (5), heart failure (6), and cancer (7), reported that obese individuals have a lower mortality risk than normal weight individuals, a phenomenon termed the “obesity paradox.”

Although type 2 diabetes is typically associated with excess weight, the prevalence among normal weight individuals has increased over the past decade (8) to ∼10–20% of individuals with diabetes (8,9). A number of studies suggested that normal weight individuals have increased mortality risk compared with overweight or obese individuals with diabetes (911). Conversely, Tobias et al. (12) did not find evidence of an obesity paradox. As a result, the relationship between BMI and mortality is controversial. Questions remain regarding potential confounding of relationships by inflammation, kidney function, physical function, and hypertension (1315). Also suggested but not tested is that physical function, low muscle, and differences in adipose tissue distribution may mediate the obesity paradox (9) because these factors are related to both BMI and mortality.

Our objective was to provide a deeper understanding of factors underlying associations between BMI and mortality among individuals with type 2 diabetes by investigating mortality risk factors known to vary by weight: adipose tissue, muscle size, and physical function. We hypothesized that normal weight individuals would have a more advanced disease profile, including less muscle, different adipose distribution, and poorer physical function, compared with overweight or obese individuals. Therefore, after comprehensively adjusting for comorbid conditions, adipose tissue, muscle size, and physical function, we hypothesized that risk differences among BMI categories would be minimal and that this conclusion would be supported by mediation analysis.

Study Population

The Age, Gene/Environment Susceptibility Study-Reykjavik Study (AGES-Reykjavik) is a random sample of 5,764 men and women nested in the Reykjavik Study, a single-center population-based cohort begun in 1967 to study heart disease. At study baseline (2002–2006), participants were aged 66–96 years. All variables with the exception of midlife BMI were assessed at baseline. Details of the study design are provided in Harris et al. (16). All participants provided written informed consent, and the study was approved by the institutional review board (VSN: 00-063).

Diabetes

Type 2 diabetes was determined from self-reported diabetes, diabetes medication use, or fasting plasma glucose ≥7 mmol/L based on American Diabetes Association diagnosis recommendations (17).

Assessment of Body Composition and Physical Function

BMI from measured height and weight (kg/m2) and waist circumference (cm) were determined using standardized protocols (16). Midlife BMI was available from height and weight measured in the Reykjavik Study (16,18,19). BMI categories of normal weight (18.5–24.9 kg/m2), overweight (25.0–29.9 kg/m2), and obese (≥30.0 kg/m2) were used to classify participants.

Computed tomography imaging of the midthigh and abdomen at the L4/L5 vertebrae was performed with a four-row detector system (Sensation; Siemens Medical Systems, Erlangen, Germany). Visceral adipose tissue (VAT) and subcutaneous adipose tissue (SAT) were estimated from a single 10-mm-thick transaxial section. VAT was distinguished from SAT by tracing along the facial plane defining the internal abdominal wall. Adipose areas (cm2) were calculated by multiplying the number of pixels by the pixel area using specialized software (University of California, San Francisco). Total thigh muscle cross-sectional area was determined from a single 10-mm-thick transaxial section in the left and right legs as described previously (20). Thigh muscle attenuation (Hounsfield units), an indicator of fat infiltration, was recorded.

Physical function was assessed using baseline measures of gait speed and muscle strength. Usual gait speed was determined over 6 m. Knee extensor strength was assessed as the maximal isometric strength from three trials of the dominant leg (20).

Mortality

Mortality was ascertained through 31 May 2011 from the Icelandic National Roster (33), an adjudicated registry of deaths. Cause-specific mortality was collected from National Health System Records through 31 December 2009. Participants who were not identified as deceased were censored at the date through which vital records were complete.

Diabetes-Related Covariates

Diabetes duration was calculated as the difference between self-reported age of diabetes diagnosis and age at baseline examination. Medication use was determined from medications brought to the clinic and self-report questionnaire. Blood pressure was assessed in a recumbent position using a mercury sphygmomanometer and large cuff on the right arm after participants had rested for 5 min. Hypertension was determined from self-report, use of hypertensive medication, systolic blood pressure ≥140 mmHg, or diastolic blood pressure ≥90 mmHg. Microalbuminuria was defined as urinary albumin/creatinine ratio between 30 and 300 mg/g (21). Total cholesterol, HDL cholesterol, triglycerides, C-reactive protein (CRP), glucose, and HbA1c were analyzed from fasting blood samples using reagents from Roche Diagnostics (Mannheim, Germany) on a Hitachi 912 analyzer according to manufacturer instructions. LDL cholesterol was calculated using the Friedewald equation. The coefficients of variation for the entire AGES-Reykjavik study were 1.8% for plasma glucose, 1.4% for total cholesterol, 2.3% for HDL, 4.8% for urinary albumin, and 1.3% for CRP.

Analytical Cohort

Participants with type 1 diabetes (diabetes before age 25 [n = 2]) and incomplete data on diabetes history (n = 66) were excluded, leaving 749 participants with diabetes. Participants missing BMI (n = 18) and thigh muscle area (n = 90) data or with a BMI <18.5 kg/m2 (n = 4) were also excluded. Thus, 637 participants (117 normal weight, 293 overweight, and 227 obese) were included. All data presented are from individuals with diabetes except for a comparison of the analytic cohort and the AGES-Reykjavik cohort.

Statistical Analysis

Differences between groups were assessed using the Kruskal-Wallis test for continuous variables due to nonnormal distributions or χ2 test for categorical variables. Cox proportional hazards models were used to estimate hazard ratios (HRs) and 95% CIs for mortality risk. Overweight was the referent group due to potential positive relationships between obesity and mortality. Proportional hazards were confirmed from examination of Kaplan-Meier curves and Schoenfeld residuals. Model 1 was unadjusted. Model 2 was adjusted for age, sex, education (less than high school, high school graduate, or more than high school), and duration of diabetes. Model 3 was additionally adjusted for midlife BMI, waist circumference, total cholesterol, HDL-cholesterol, systolic blood pressure, smoking status (never, current, or former), hypertension, statin use, diabetes medication use, microalbuminuria, and CRP. The effect of VAT, SAT, thigh muscle attenuation, thigh muscle area, and physical function on risk estimates was assessed by adjusting for each variable in model 3. Measures that attenuated risk estimates were assessed with mediation models that progress through four steps/models (22). The models tested whether a variable was a significant mediator of the association between an independent variable (BMI category) and a dependent variable (mortality) and quantified the direct, indirect, and total effect of relationships. The proportion of the effect of BMI category and mortality mediated was then determined. Bootstrapping was used to estimate the 95% CIs of mediators (23).

We conducted multiple sensitivity analyses to assess the strength of risk relationships. Analyses were conducted using an alternative definition of diabetes from self-report, medication use, and HbA1c ≥6.5% (≥48 mmol/mol), which has been suggested as a redefinition of diabetes by an International Expert Committee (24). BMI was analyzed as a continuous value (risk per SD increment in BMI). Analyses excluding participants who died within 2 years of study baseline were conducted to exclude potentially undetected subclinical disease. To minimize confounding of BMI and mortality due to smoking, we restricted analyses to never smokers, although this resulted in only 54 normal weight, 109 overweight, and 84 obese participants. All tests were two-sided, with significance set at P < 0.05. Analyses were performed with Stata 12.1 (StataCorp, College Station, TX) and SPSS version 22.0 (IBM Corporation, Chicago, IL).

Compared with the AGES-Reykjavik population, participants with diabetes were more likely to be men (54.6 vs. 40.5%, P < 0.001), older (77.4 vs. 76.9 years, P = 0.03), and heavier (BMI 28.8 vs. 26.8 kg/m2, P < 0.001). The distribution of thigh muscle area in the analytic sample of participants with diabetes is similar to the distribution in the AGES-Reykjavik population (Supplementary Fig. 1). When adjusted for BMI, men but not women with diabetes had lower thigh muscle area than the AGES-Reykjavik population (P < 0.001 vs. P = 0.29, respectively).

Characteristics of participants according to BMI categories are shown in Table 1. Age, HDL cholesterol, CRP, triglycerides, midlife BMI, waist circumference, VAT, SAT, thigh muscle area, muscle strength, and thigh muscle attenuation increased in a graded manner across BMI categories from normal weight to obese. Conversely, duration of diabetes, current smoking, and HDL cholesterol decreased across BMI categories from normal weight to obese. Self-reported illness-related weight loss of ≥5 kg in the prior year was present in 7.97% of normal weight, 4.18% of overweight, and 3.52% of obese participants.

Table 1

Baseline characteristics of participants with diabetes according to BMI

Normal weight
(n = 117)Overweight
(n = 293)Obese
(n = 227)P value
Women 51 (43.6) 113 (38.6) 121 (53.3) 0.003 
Age (years) 78 (75–81) 76 (72–81) 75 (72–79) <0.001 
Duration of diabetes (years) 10.0 (1.0–20.0) 3.0 (0–14.0) 3.0 (0–10.0) <0.001 
Less than high school education 19 (16.2) 67 (22.9) 52 (22.9) 0.34 
Current smoker 20 (17.1) 33 (11.3) 20 (8.81) 0.02 
Systolic BP (mmHg) 143 (130–163) 145 (132–159) 143 (131–159) 0.71 
Diastolic BP (mmHg) 73.0 (67.0–79.0) 73.0 (67.0–80.0) 74.0 (67.0–80.0) 0.66 
Hypertension 104 (88.9) 262 (89.4) 214 (94.3) 0.10 
Fasting glucose (mmol/L) 7.40 (6.00–8.90) 7.40 (6.70–8.40) 7.30 (6.60–8.50) 0.80 
Hemoglobin A1c (%) 6.30 (5.90–7.20) 6.20 (5.80–6.80) 6.20 (5.90–6.60) 0.20 
Hemoglobin A1c (mmol/mol) 45.4 (41.0–55.2) 44.3 (39.9–50.8) 44.3 (41.0–48.6)  
Insulin medication 8 (7.08) 12 (4.24) 9 (4.04) 0.41 
Hypoglycemia medication 62 (54.9) 149 (52.7) 109 (48.9) 0.53 
Total cholesterol (mg/dL) 197 (162–230) 197 (170–232) 201 (166–232) 0.88 
HDL cholesterol (mg/dL) 57.9 (45.2–72.4) 49.4 (42.9–59.9) 47.9 (41.3–57.5) <0.001 
LDL cholesterol (mg/dL) 114 (87.1–139) 119 (91.5–149) 118 (85.7–147) 0.50 
Triglycerides (mg/dL) 91.2 (65.9–137) 114 (83.2–159) 136 (104–177) <0.001 
CRP (mg/L) 1.55 (0.75–3.40) 2.00 (1.00–4.40) 2.60 (1.30–5.00) <0.001 
Cancer 20 (17.1) 40 (13.8) 32 (14.2) 0.68 
Coronary heart disease 38 (32.5) 76 (25.9) 64 (28.2) 0.41 
Microalbuminuria 16 (13.7) 38 (13.0) 36 (15.9) 0.64 
BMI (kg/m223.8 (22.4–24.5) 27.4 (26.4–28.6) 32.8 (31.2–35.1) <0.001 
Midlife BMI (kg/m224.3 (22.2–26.5) 26.1 (23.8–27.8) 28.6 (26.7–31.4) <0.001 
Waist circumference (cm) 93.0 (87.0–97.0) 104 (99.0–107) 116 (110–123) <0.001 
VAT (cm2253 (223–299) 325 (280–376) 405 (338–461) <0.001 
SAT (cm2281 (241–320) 354 (316–410) 465 (411–532) <0.001 
Thigh muscle (cm2226 (208–239) 238 (222–256) 242 (227–270) <0.001 
Thigh muscle attenuation (HU) 168 (165–171) 167 (163–171) 165 (161–169) <0.001 
Gait speed (m/s) 0.95 (0.80–1.05) 0.94 (0.81–1.07) 0.88 (0.76–1.01) 0.004 
Muscle strength (N · m) 112 (88.7–155) 134 (96.8–184) 120 (90.5–168) 0.006 
Normal weight
(n = 117)Overweight
(n = 293)Obese
(n = 227)P value
Women 51 (43.6) 113 (38.6) 121 (53.3) 0.003 
Age (years) 78 (75–81) 76 (72–81) 75 (72–79) <0.001 
Duration of diabetes (years) 10.0 (1.0–20.0) 3.0 (0–14.0) 3.0 (0–10.0) <0.001 
Less than high school education 19 (16.2) 67 (22.9) 52 (22.9) 0.34 
Current smoker 20 (17.1) 33 (11.3) 20 (8.81) 0.02 
Systolic BP (mmHg) 143 (130–163) 145 (132–159) 143 (131–159) 0.71 
Diastolic BP (mmHg) 73.0 (67.0–79.0) 73.0 (67.0–80.0) 74.0 (67.0–80.0) 0.66 
Hypertension 104 (88.9) 262 (89.4) 214 (94.3) 0.10 
Fasting glucose (mmol/L) 7.40 (6.00–8.90) 7.40 (6.70–8.40) 7.30 (6.60–8.50) 0.80 
Hemoglobin A1c (%) 6.30 (5.90–7.20) 6.20 (5.80–6.80) 6.20 (5.90–6.60) 0.20 
Hemoglobin A1c (mmol/mol) 45.4 (41.0–55.2) 44.3 (39.9–50.8) 44.3 (41.0–48.6)  
Insulin medication 8 (7.08) 12 (4.24) 9 (4.04) 0.41 
Hypoglycemia medication 62 (54.9) 149 (52.7) 109 (48.9) 0.53 
Total cholesterol (mg/dL) 197 (162–230) 197 (170–232) 201 (166–232) 0.88 
HDL cholesterol (mg/dL) 57.9 (45.2–72.4) 49.4 (42.9–59.9) 47.9 (41.3–57.5) <0.001 
LDL cholesterol (mg/dL) 114 (87.1–139) 119 (91.5–149) 118 (85.7–147) 0.50 
Triglycerides (mg/dL) 91.2 (65.9–137) 114 (83.2–159) 136 (104–177) <0.001 
CRP (mg/L) 1.55 (0.75–3.40) 2.00 (1.00–4.40) 2.60 (1.30–5.00) <0.001 
Cancer 20 (17.1) 40 (13.8) 32 (14.2) 0.68 
Coronary heart disease 38 (32.5) 76 (25.9) 64 (28.2) 0.41 
Microalbuminuria 16 (13.7) 38 (13.0) 36 (15.9) 0.64 
BMI (kg/m223.8 (22.4–24.5) 27.4 (26.4–28.6) 32.8 (31.2–35.1) <0.001 
Midlife BMI (kg/m224.3 (22.2–26.5) 26.1 (23.8–27.8) 28.6 (26.7–31.4) <0.001 
Waist circumference (cm) 93.0 (87.0–97.0) 104 (99.0–107) 116 (110–123) <0.001 
VAT (cm2253 (223–299) 325 (280–376) 405 (338–461) <0.001 
SAT (cm2281 (241–320) 354 (316–410) 465 (411–532) <0.001 
Thigh muscle (cm2226 (208–239) 238 (222–256) 242 (227–270) <0.001 
Thigh muscle attenuation (HU) 168 (165–171) 167 (163–171) 165 (161–169) <0.001 
Gait speed (m/s) 0.95 (0.80–1.05) 0.94 (0.81–1.07) 0.88 (0.76–1.01) 0.004 
Muscle strength (N · m) 112 (88.7–155) 134 (96.8–184) 120 (90.5–168) 0.006 

Data are median (interquartile range) or n (%). BP, blood pressure; HU, Hounsfield unit; N · m, newton meter.

Median follow-up was 6.66 years (interquartile range 5.72–7.63 years), during which 188 participants died (46.8 per 1,000 person-years). The number of deaths by smoking status did not differ (nonsmokers 68 [36.4%], former smokers 90 [48.1%], current smokers 29 [15.5%], P = 0.12). Among participants with cause-specific mortality (n = 143), the main causes of death were cardiovascular disease (n = 68 [47.6%]) and cancer (n = 40 [28.0%]). Eight deaths (5.59%) were attributed to diabetes.

Compared with overweight, normal weight tended to be associated with increased mortality risk in unadjusted models (Supplementary Fig. 2 and Table 2). Associations strengthened after full adjustment for risk factors (model 3, HR 1.72 [95% CI 1.12–2.64]) (Table 2). Within model 3, covariates positively associated with mortality were age, female sex, current smoking, midlife BMI, and microalbuminuria. When body composition and physical function variables were added to model 3, only thigh muscle area and gait speed attenuated the mortality risk in normal weight participants (HR 1.36 [95% CI 0.87–2.11] and 1.44 [95% CI 0.91–2.27], respectively). When gait speed and thigh muscle area were included in the same model, the risk estimate was attenuated further (HR 1.27 [95% CI 0.80–2.01]). Interactions between BMI and thigh muscle area, BMI and gait speed, and BMI and muscle strength were significant (P < 0.05) in the fully adjusted model (model 3).

Table 2

BMI and mortality risk in participants with diabetes

No. participantsNo. eventsEvent rateModel 1Model 2Model 3
Overweight 293 85 45.5 1.00 1.00 1.00 
Obese 227 59 40.8 0.90 (0.65–1.26) 1.13 (0.81–1.60) 0.89 (0.58–1.38) 
Normal weight 117 44 62.5 1.39 (0.97–2.01) 1.34 (0.93–1.95) 1.72 (1.12–2.64) 
Adjustment for adipose tissue, muscle tissue, and/or function in model 3    
 Normal weight + thigh muscle area   1.36 (0.87–2.11) 
 Normal weight + gait speed   1.44 (0.91–2.27) 
 Normal weight + gait speed + thigh muscle area   1.27 (0.80–2.01) 
 Normal weight + muscle strength   1.59 (1.00–2.52) 
 Normal weight + thigh muscle attenuation   1.93 (1.25–2.99) 
 Normal weight + VAT and SATa   1.60 (1.03–2.49) 
No. participantsNo. eventsEvent rateModel 1Model 2Model 3
Overweight 293 85 45.5 1.00 1.00 1.00 
Obese 227 59 40.8 0.90 (0.65–1.26) 1.13 (0.81–1.60) 0.89 (0.58–1.38) 
Normal weight 117 44 62.5 1.39 (0.97–2.01) 1.34 (0.93–1.95) 1.72 (1.12–2.64) 
Adjustment for adipose tissue, muscle tissue, and/or function in model 3    
 Normal weight + thigh muscle area   1.36 (0.87–2.11) 
 Normal weight + gait speed   1.44 (0.91–2.27) 
 Normal weight + gait speed + thigh muscle area   1.27 (0.80–2.01) 
 Normal weight + muscle strength   1.59 (1.00–2.52) 
 Normal weight + thigh muscle attenuation   1.93 (1.25–2.99) 
 Normal weight + VAT and SATa   1.60 (1.03–2.49) 

Data are HR (95% CI) unless otherwise indicated. Events per 1,000 person-years. Model 1 unadjusted. Model 2 adjusted for age, sex, education, and duration of diabetes. Model 3 adjusted for model 2 covariates plus midlife BMI, waist circumference, total cholesterol, HDL cholesterol, systolic blood pressure, smoking status, hypertension, statin use, diabetes medication type, microalbuminuria, and CRP. HRs are shown only for covariates that were significant in the fully adjusted model.

aModel excluded waist circumference due to collinearity with VAT.

Sensitivity analyses are shown in Table 3. An alternative diabetes definition similarly showed no mortality risk for obese participants and increased mortality risk for normal weight participants (model 3, HR 1.49 [95% CI 1.06–2.09]), which was attenuated with adjustment for thigh muscle and gait speed. BMI per SD increase was not associated with mortality risk, suggesting a nonlinear relationship. Excluding participants who died within 2 years of baseline to account for undiagnosed underlying chronic disease did not alter associations. Despite losing statistical power, the results from never smokers were consistent with the main analysis in Table 2.

Table 3

BMI and mortality risk in participants with diabetes: sensitivity analysis

No. participantsNo. eventsEvent rateModel 1Model 2Model 3
Diabetes from self-report, medications, and HbA1c ≥6.5%       
 Overweight 408 115 40.7 1.00 1.00 1.00 
 Obese 247 63 37.6 0.94 (0.69–1.28) 1.23 (0.90–1.69) 0.95 (0.64–1.42) 
 Normal weight 263 84 45.6 1.12 (0.85–1.48) 1.8 (0.82–1.44) 1.49 (1.06–2.09) 
 Normal weight + thigh muscle      1.21 (0.86–1.71) 
 Normal weight + gait speed      1.39 (0.98–1.96) 
 BMI per SD increment 637 188 46.8 0.95 (0.83–1.09) 1.09 (0.94–1.27) 0.98 (0.71–1.36) 
Excluding participants who died within first 2 years       
 Overweight 278 70 37.8 1.00 1.00 1.00 
 Obese 108 52 36.2 1.04 (0.91–1.18) 1.29 (0.89–1.88) 0.99 (0.62–1.59) 
 Normal weight 108 35 50.5 1.35 (1.21–1.50) 1.38 (0.91–2.08) 1.63 (1.02–2.62) 
 Normal weight + thigh muscle      1.33 (0.81–2.17) 
 Normal weight + gait speed      1.39 (0.85–2.27) 
Excluding participants reporting current or former smoking       
 Overweight 109 32 45.1 1.00 1.00 1.00 
 Obese 85 19 33.9 0.75 (0.43–1.32) 1.08 (0.60–1.95) 0.73 (0.36–1.51) 
 Normal 54 17 51.0 1.15 (0.64–2.07) 1.28 (0.70–2.33) 1.83 (0.90–3.70) 
No. participantsNo. eventsEvent rateModel 1Model 2Model 3
Diabetes from self-report, medications, and HbA1c ≥6.5%       
 Overweight 408 115 40.7 1.00 1.00 1.00 
 Obese 247 63 37.6 0.94 (0.69–1.28) 1.23 (0.90–1.69) 0.95 (0.64–1.42) 
 Normal weight 263 84 45.6 1.12 (0.85–1.48) 1.8 (0.82–1.44) 1.49 (1.06–2.09) 
 Normal weight + thigh muscle      1.21 (0.86–1.71) 
 Normal weight + gait speed      1.39 (0.98–1.96) 
 BMI per SD increment 637 188 46.8 0.95 (0.83–1.09) 1.09 (0.94–1.27) 0.98 (0.71–1.36) 
Excluding participants who died within first 2 years       
 Overweight 278 70 37.8 1.00 1.00 1.00 
 Obese 108 52 36.2 1.04 (0.91–1.18) 1.29 (0.89–1.88) 0.99 (0.62–1.59) 
 Normal weight 108 35 50.5 1.35 (1.21–1.50) 1.38 (0.91–2.08) 1.63 (1.02–2.62) 
 Normal weight + thigh muscle      1.33 (0.81–2.17) 
 Normal weight + gait speed      1.39 (0.85–2.27) 
Excluding participants reporting current or former smoking       
 Overweight 109 32 45.1 1.00 1.00 1.00 
 Obese 85 19 33.9 0.75 (0.43–1.32) 1.08 (0.60–1.95) 0.73 (0.36–1.51) 
 Normal 54 17 51.0 1.15 (0.64–2.07) 1.28 (0.70–2.33) 1.83 (0.90–3.70) 

Data are HR (95% CI) unless otherwise indicated. Events per 1,000 person-years. Model 1 unadjusted. Model 2 adjusted for age, sex, education, and duration of diabetes. Model 3 adjusted for model 2 covariates plus midlife BMI, waist circumference, total cholesterol, HDL cholesterol, systolic blood pressure, smoking status, hypertension, statin use, diabetes medication type, microalbuminuria, and CRP.

Thigh muscle area met all four criteria for mediation (22), as shown in models 1–4 (Table 4). In the adjusted mediation model, muscle was significantly associated with mortality (model 4, β = 0.25, P < 0.001). However, normal weight BMI no longer significantly accounted for any unique variance (model 4, β = −0.05, P = 0.29), indicating a significant mediating effect of thigh muscle whereby thigh muscle mediated 46% of the effect of normal weight on mortality. This was confirmed by bootstrapping (95% CI 0.01–0.02). Although normal weight was no longer significant in the adjusted mediation model of gait speed (model 4, β = −0.07, P = 0.13), the 95% CI (−0.03 to 0.06) indicated a nonsignificant mediating effect. Thigh muscle in relation to BMI and mortality was also explored in post hoc analyses. The median thigh muscle for men and women was defined within normal weight and overweight participants, resulting in four groups: 1) normal weight, low muscle (below the respective sex-specific median); 2) normal weight, high muscle; 3) overweight, low muscle; and 4) overweight, high muscle. The first three groups had increased mortality risk relative to overweight, high muscle (Supplementary Fig. 3). Risk appeared to increase in a graded manner related to muscle, whereas normal weight, low muscle, and overweight, low muscle, had the highest risks of mortality.

Table 4

Mediating effects of muscle and function on the association of normal weight BMI and mortality

EffectβP value
Model 1 Normal weight on mortality risk −0.10 0.04 
Thigh muscle area as mediator    
 Model 2 Normal weight on muscle −0.18 <0.001 
 Model 3 Muscle on mortality 0.25 <0.001 
 Model 4 Normal weight and muscle on mortality  
Muscle on mortality 0.25 <0.001 
Normal weight on mortality −0.05 0.29 
Gait speed as mediator    
 Model 2 Normal weight on gait speed −0.03 0.58 
 Model 3 Gait speed on mortality 0.21 <0.001 
 Model 4 Normal weight and gait speed on mortality  
Gait speed on mortality 0.21 <0.001 
Normal weight on mortality −0.07 0.13 
EffectβP value
Model 1 Normal weight on mortality risk −0.10 0.04 
Thigh muscle area as mediator    
 Model 2 Normal weight on muscle −0.18 <0.001 
 Model 3 Muscle on mortality 0.25 <0.001 
 Model 4 Normal weight and muscle on mortality  
Muscle on mortality 0.25 <0.001 
Normal weight on mortality −0.05 0.29 
Gait speed as mediator    
 Model 2 Normal weight on gait speed −0.03 0.58 
 Model 3 Gait speed on mortality 0.21 <0.001 
 Model 4 Normal weight and gait speed on mortality  
Gait speed on mortality 0.21 <0.001 
Normal weight on mortality −0.07 0.13 

Overweight BMI as referent group vs. normal weight, standardized β. Models adjusted for age, sex, education, duration of diabetes, midlife BMI, waist circumference, total cholesterol, HDL cholesterol, systolic blood pressure, smoking status, hypertension, statin use, diabetes medication type, microalbuminuria, and CRP. The four models tested whether muscle size and gait speed mediate/drive increased mortality risk in normal weight individuals. Model 1 shows that normal weight participants have 0.10 units less of life. Model 2 shows that normal weight participants have 0.18 units less muscle but not significantly different gait speed than overweight participants. Model 3 shows that for a 1-unit increase in muscle, survival increases by 0.25 units (0.21-unit increase for each 1-unit increase in gait speed). When thigh muscle and normal weight are included in a model, the effect of normal weight on mortality is no longer significant, suggesting that the effect is explained in part by thigh muscle (model 4). The 95% CI for thigh muscle was (0.01–0.02) as estimated by the bootstrapping method–confirmed significant mediation (23). When gait speed and normal weight on mortality are included in a model, the effect of normal weight on mortality is no longer significant, but the 95% CI (−0.03 to 0.06) indicated nonsignificant mediation.

In this study of older adults with type 2 diabetes, normal weight participants had elevated mortality risk compared with overweight participants, whereas obese participants had no mortality risk relative to overweight participants. The results are consistent with previous studies (911) and suggest that increased risk of mortality in normal weight participants is not attenuated, even with adjustment for risk factors, including inflammation and adipose tissue distribution. The results further suggest that the obesity paradox is related to differences in muscle size, whereby muscle size mediates 46% of the effect of normal weight on mortality risk, which is a novel contribution.

Contrary to our hypothesis, adipose tissue distribution did not attenuate mortality risk for normal weight participants, aligning with a study reporting that the obesity paradox in diabetes persists with adjustment for waist circumference, an indirect measure of VAT (9). Physical function and frailty have been hypothesized to mediate relationships between BMI and mortality whereby both lead to weight loss and increased risk of death (9,25). The present results do not support this notion because muscle strength did not attenuate risk estimates and mediation analysis did not indicate a significant mediating effect of gait speed. However, we did not assess frailty directly because the study population was not characterized by overt frailty; >60% met gait speed thresholds for poor performance, but the prevalence of illness-related weight loss and weakness (grip strength) was low (data not shown). Further studies that address frailty directly in older populations with a wider range of physical functioning are warranted.

The finding of muscle as a mediating factor of relationships between BMI and mortality in diabetes is a step forward in our understanding of risk factors. However, potential mechanisms need to be investigated, particularly because the effect of muscle does not seem to reflect muscle function or quality (no attenuating effect of intermuscular fat). Muscle mass is inversely associated with insulin resistance (26). Because insulin resistance is an etiologic factor for cardiovascular disease (27) and cancer (28), this may help to explain the elevated mortality risk among normal weight participants who had less muscle than overweight or obese participants. However, the results provide conflicting support that overweight or obese participants have more-favorable metabolic profiles than normal weight participants. Fasting glucose, HbA1c, and type of diabetes medication did not differ, but the duration of diabetes was longer among normal weight participants.

An alternative explanation for the obesity paradox in diabetes is that of selection bias (29,30). It has been suggested that conditioning on a variable (diabetes) that is affected by exposure (BMI) may induce associations with mortality (31). However, the notion that restricting analyses to populations with diabetes results in normal weight individuals with more risk factors for mortality than overweight or obese individuals is not supported by the present data. The distribution of baseline factors suggests differences that would be expected to be both risk and protective factors. For example, relative to overweight or obese participants, normal weight participants were older and had longer duration of diabetes and higher prevalence of current smoking but had higher HDL cholesterol, lower triglycerides, lower CRP, and similar HbA1c. Furthermore, although current smoking was more prevalent among normal weight individuals, the positive direction of the association between normal weight and mortality persisted when the analysis was restricted to never smokers.

Strengths of this study are the measures of physical function and body composition from radiographic imaging, which enabled novel examination of factors known to vary by BMI. Another strength is the availability of measured midlife BMI. A criticism of previous studies has been that BMI often is assessed up to several decades after diabetes diagnosis, thereby increasing the risk of reverse causation (12). In the present analysis, normal weight participants had lost weight since midlife, but adjustment for midlife BMI did not attenuate mortality risk. Excluding deaths within 2 years of study baseline also did not attenuate risk, suggesting that the results were not driven by early mortality from undetected subclinical disease at baseline. We were also able to address the possibility of survival bias by referencing a comparative analysis by Olafsdottir et al. (32) of type 2 diabetes in the Reykjavik Study and the AGES-Reykjavik study (survivors from the Reykjavik Study) who were examined 11 years apart. The rate for all-cause and cardiovascular mortality was lower in the AGES-Reykjavik study, but the decline in mortality was similar to that in the general Icelandic population over that time period (33). Thus, it does not appear that individuals with type 2 diabetes in the present cohort had a survival bias relative to the general type 2 diabetes population.

The main limitation of this study is the small sample size, which did not permit us to restrict the study population to those with incident diabetes. Thus, we were unable to avoid reverse causation or possible differences in mortality that reflect complications from longer diabetes duration in normal weight participants. The study was undertaken with the aim of examining the effects of weight-related measures from imaging and clinical tests, which are typically not available in large samples, rather than providing a definitive answer regarding the presence or absence of an obesity paradox in type 2 diabetes. Although we adjusted for diabetes duration, we cannot rule out possible residual confounding from self-reported age at diabetes diagnosis. It is noteworthy that the prevalence of diabetes complications, such as cardiovascular disease and peripheral neuropathy, in old age is similar for individuals diagnosed with diabetes in midlife versus old age (34), and chronic diseases did not differ by BMI despite differences in diabetes duration. Also possible is that we had residual bias from adjusting for smoking status rather than stratifying by smoking status, but the number of deaths did not vary by smoking status, and analyses restricted to never smokers indicated increased mortality risk for normal weight participants, although the sample size was limited. The finding of muscle as a mediating factor was tested in a statistical model that provides insight into causal relationships but is not a substitute for clinical studies. It is also important to test the possible mediating effect of muscle in younger populations that may have a different body composition from older adults (35).

In conclusion, the results illustrate the importance of identifying type 2 diabetes among normal weight individuals and suggest that muscle size may help to explain relationships between BMI and mortality in type 2 diabetes. The divergence of muscle size and muscle function as mediators of relationships is likely to spur additional debate on the importance of muscle size versus physical function in old age (3638), and further studies in this area are warranted.

Funding. This study was funded by National Institutes of Health contract N01-AG-012100, the National Institute on Aging Intramural Research Program, Hjartavernd (the Icelandic Heart Association), and the Althingi (the Icelandic Parliament). R.A.M. holds a Banting Postdoctoral Fellowship.

Duality of Interest. No potential conflicts of interest relevant to this article were reported.

Author Contributions. R.A.M. contributed to the study concept and design, data analysis and interpretation, statistical analysis, and drafting of the manuscript. I.R. contributed to the drafting of the manuscript. M.E.G. contributed to the data acquisition. G.E. contributed to the data acquisition and critical revision of the manuscript and provided administrative, technical, and material support. L.J.L. contributed to obtaining funding. R.B. contributed to the critical revision of the manuscript. V.G. and T.B.H. contributed to the study concept and design, obtaining funding, and the critical revision of the manuscript. P.V.J. contributed to the study concept and design and obtaining funding. R.A.M. is the guarantor of this work and, as such, had full access to all the data in the study and takes responsibility for the integrity of the data and the accuracy of the data analysis.

Prior Presentation. This work was presented in abstract form at Experimental Biology, San Diego, CA, 26–30 April 2014.

1.
Calle
EE
,
Thun
MJ
,
Petrelli
JM
,
Rodriguez
C
,
Heath
CW
 Jr
.
Body-mass index and mortality in a prospective cohort of U.S. adults
.
N Engl J Med
1999
;
341
:
1097
1105
[PubMed]
2.
McGee
DL
Diverse Populations Collaboration
.
Body mass index and mortality: a meta-analysis based on person-level data from twenty-six observational studies
.
Ann Epidemiol
2005
;
15
:
87
97
[PubMed]
3.
Flegal
KM
,
Graubard
BI
,
Williamson
DF
,
Gail
MH
.
Excess deaths associated with underweight, overweight, and obesity
.
JAMA
2005
;
293
:
1861
1867
[PubMed]
4.
Hong
NS
,
Kim
KS
,
Lee
IK
, et al
.
The association between obesity and mortality in the elderly differs by serum concentrations of persistent organic pollutants: a possible explanation for the obesity paradox
.
Int J Obes (Lond)
2012
;
36
:
1170
1175
[PubMed]
5.
Kalantar-Zadeh
K
,
Abbott
KC
,
Salahudeen
AK
,
Kilpatrick
RD
,
Horwich
TB
.
Survival advantages of obesity in dialysis patients
.
Am J Clin Nutr
2005
;
81
:
543
554
[PubMed]
6.
Oreopoulos
A
,
Padwal
R
,
Kalantar-Zadeh
K
,
Fonarow
GC
,
Norris
CM
,
McAlister
FA
.
Body mass index and mortality in heart failure: a meta-analysis
.
Am Heart J
2008
;
156
:
13
22
[PubMed]
7.
Halabi
S
,
Small
EJ
,
Vogelzang
NJ
.
Elevated body mass index predicts for longer overall survival duration in men with metastatic hormone-refractory prostate cancer
.
J Clin Oncol
2005
;
23
:
2434
2435; author reply 2435
[PubMed]
8.
Gregg
EW
,
Cadwell
BL
,
Cheng
YJ
, et al
.
Trends in the prevalence and ratio of diagnosed to undiagnosed diabetes according to obesity levels in the U.S
.
Diabetes Care
2004
;
27
:
2806
2812
[PubMed]
9.
Carnethon
MR
,
De Chavez
PJ
,
Biggs
ML
, et al
.
Association of weight status with mortality in adults with incident diabetes
.
JAMA
2012
;
308
:
581
590
[PubMed]
10.
McEwen
LN
,
Kim
C
,
Karter
AJ
, et al
.
Risk factors for mortality among patients with diabetes: the Translating Research Into Action for Diabetes (TRIAD) Study
.
Diabetes Care
2007
;
30
:
1736
1741
[PubMed]
11.
Doehner
W
,
Erdmann
E
,
Cairns
R
, et al
.
Inverse relation of body weight and weight change with mortality and morbidity in patients with type 2 diabetes and cardiovascular co-morbidity: an analysis of the PROactive study population
.
Int J Cardiol
2012
;
162
:
20
26
[PubMed]
12.
Tobias
DK
,
Pan
A
,
Jackson
CL
, et al
.
Body-mass index and mortality among adults with incident type 2 diabetes
.
N Engl J Med
2014
;
370
:
233
244
[PubMed]
13.
Yano
Y
,
Ishikawa
S
,
Kario
K
.
Weight and mortality in adults with diabetes
.
JAMA
2012
;
308
:
2079
2080; author reply 2080–2081
[PubMed]
14.
Jornayvaz FR. Weight and mortality in adults with diabetes. JAMA 2012;308:2080; author reply 2080–2081
15.
Zeng
Q
,
Dong
SY
.
Weight and mortality in adults with diabetes
.
JAMA
2012
;
308
:
2079
; author reply 2080–2081
[PubMed]
16.
Harris
TB
,
Launer
LJ
,
Eiriksdottir
G
, et al
.
Age, Gene/Environment Susceptibility-Reykjavik Study: multidisciplinary applied phenomics
.
Am J Epidemiol
2007
;
165
:
1076
1087
[PubMed]
17.
American Diabetes Association
.
Diagnosis and classification of diabetes mellitus
.
Diabetes Care
2013
;
36
(
Suppl. 1
):
S67
S74
[PubMed]
18.
Jonasson
F
,
Arnarsson
A
,
Eiríksdottir
G
, et al
.
Prevalence of age-related macular degeneration in old persons: Age, Gene/environment Susceptibility Reykjavik Study
.
Ophthalmology
2011
;
118
:
825
830
[PubMed]
19.
Qiu
C
,
Cotch
MF
,
Sigurdsson
S
, et al
.
Microvascular lesions in the brain and retina: the Age, Gene/Environment Susceptibility-Reykjavik Study
.
Ann Neurol
2009
;
65
:
569
576
[PubMed]
20.
Johannesdottir
F
,
Aspelund
T
,
Siggeirsdottir
K
, et al
.
Mid-thigh cortical bone structural parameters, muscle mass and strength, and association with lower limb fractures in older men and women (AGES-Reykjavik Study)
.
Calcif Tissue Int
2012
;
90
:
354
364
[PubMed]
21.
National Kidney Foundation-Kidney Disease Outcomes Quality Initiative. KDOQI clinical practice guidelines and clinical practice recommendations for diabetes and chronic kidney disease. Am J Kidney Dis 2007;49(Suppl. 2):S12-S154
22.
Baron
RM
,
Kenny
DA
.
The moderator-mediator variable distinction in social psychological research: conceptual, strategic, and statistical considerations
.
J Pers Soc Psychol
1986
;
51
:
1173
1182
[PubMed]
23.
Preacher
KJ
,
Hayes
AF
.
SPSS and SAS procedures for estimating indirect effects in simple mediation models
.
Behav Res Methods Instrum Comput
2004
;
36
:
717
731
[PubMed]
24.
Gillett
MJ
.
International expert committee report on the role of the A1C assay in the diagnosis of diabetes: Diabetes Care 2009; 32(7): 1327-1334
.
Clin Biochem Rev
2009
;
30
:
197
200
[PubMed]
25.
Florez
H
,
Castillo-Florez
S
.
Beyond the obesity paradox in diabetes: fitness, fatness, and mortality
.
JAMA
2012
;
308
:
619
620
[PubMed]
26.
Srikanthan
P
,
Karlamangla
AS
.
Relative muscle mass is inversely associated with insulin resistance and prediabetes. Findings from the third National Health and Nutrition Examination Survey
.
J Clin Endocrinol Metab
2011
;
96
:
2898
2903
[PubMed]
27.
DeFronzo
RA
,
Ferrannini
E
.
Insulin resistance. A multifaceted syndrome responsible for NIDDM, obesity, hypertension, dyslipidemia, and atherosclerotic cardiovascular disease
.
Diabetes Care
1991
;
14
:
173
194
[PubMed]
28.
Donohoe
CL
,
Doyle
SL
,
Reynolds
JV
.
Visceral adiposity, insulin resistance and cancer risk
.
Diabetol Metab Syndr
2011
;
3
:
12
[PubMed]
29.
Banack
HR
,
Kaufman
JS
.
The “obesity paradox” explained
.
Epidemiology
2013
;
24
:
461
462
[PubMed]
30.
Ferreira
I
,
Stehouwer
CD
.
Obesity paradox or inappropriate study designs? Time for life-course epidemiology
.
J Hypertens
2012
;
30
:
2271
2275
[PubMed]
31.
Lajous
M
,
Bijon
A
,
Fagherazzi
G
, et al
.
Body mass index, diabetes, and mortality in French women: explaining away a “paradox”
.
Epidemiology
2014
;
25
:
10
14
[PubMed]
32.
Olafsdottir
E
,
Aspelund
T
,
Sigurdsson
G
, et al
.
Similar decline in mortality rate of older persons with and without type 2 diabetes between 1993 and 2004 the Icelandic population-based Reykjavik and AGES-Reykjavik cohort studies
.
BMC Public Health
2013
;
13
:
36
[PubMed]
33.
Statistics Iceland. 2010. Births and deaths [article online]. Available from http://www.statice.is/Statistics/Population/Births-and-deaths. Accessed 7 October 2013
34.
Selvin
E
,
Coresh
J
,
Brancati
FL
.
The burden and treatment of diabetes in elderly individuals in the U.S
.
Diabetes Care
2006
;
29
:
2415
2419
[PubMed]
35.
Visser
M
,
Pahor
M
,
Tylavsky
F
, et al
.
One- and two-year change in body composition as measured by DXA in a population-based cohort of older men and women
.
J Appl Physiol (1985)
2003
;
94
:
2368
2374
[PubMed]
36.
Newman
AB
,
Kupelian
V
,
Visser
M
, et al
.
Strength, but not muscle mass, is associated with mortality in the health, aging and body composition study cohort
.
J Gerontol A Biol Sci Med Sci
2006
;
61
:
72
77
[PubMed]
37.
Metter
EJ
,
Talbot
LA
,
Schrager
M
,
Conwit
R
.
Skeletal muscle strength as a predictor of all-cause mortality in healthy men
.
J Gerontol A Biol Sci Med Sci
2002
;
57
:
B359
B365
[PubMed]
38.
Cesari
M
,
Pahor
M
,
Lauretani
F
, et al
.
Skeletal muscle and mortality results from the InCHIANTI Study
.
J Gerontol A Biol Sci Med Sci
2009
;
64
:
377
384
[PubMed]

Supplementary data