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. 2018 Sep 3;5:23. doi: 10.1186/s40608-018-0201-9

Association of Metabolic Markers with self-reported osteoarthritis among middle-aged BMI-defined non-obese individuals: a cross-sectional study

Kelsey H Collins 1,✉,#, Behnam Sharif 2,✉,#, Raylene A Reimer 3, Claudia Sanmartin 4, Walter Herzog 1, Rick Chin 5, Deborah A Marshall 2
PMCID: PMC6120068  PMID: 30186613

Abstract

Background

Osteoarthritis (OA) is a chronic degenerative joint disease. While it is well-established that obesity affects OA through increased axial loading on the joint cartilage, the indirect effect of obesity through metabolic processes among the body mass index (BMI)-defined non-obese population, i.e., BMI < 30 kg/m2, is less known. Our goal was to evaluate the association of metabolic markers including body fat percentage (BF%), waist circumference, maximum weight gain during adulthood and serum creatinine with self-reported OA to establish if such measures offer additional information over BMI among the non-obese population between 40 and 65 years of age.

Methods

Cross-sectional data from two cycles of the Canadian Health Measures Survey (CHMS) in 2007–2009 and 2009–2011 were analyzed. Sex-specific logistic regression models were developed to evaluate the association of self-reported OA with metabolic markers. Models were separately adjusted for age, BMI categories and serum creatinine, and a stratified analysis across BM categories was performed. In a secondary analysis, we evaluated the association of self-reported OA, cardiovascular diseases and hypertension across BF% categories.

Results

Of 2462 individuals, 217 (8.8%) self-reported OA. After adjusting for age and BMI, those within BF%-defined overweight/obese category had 2.67 (95% CI: 1.32–3.51) and 2.11(95% CI: 1.38–3.21) times higher odds of reporting self-reported OA compared to those within BF%-defined athletic/acceptable category for females and males, respectively. BF% was also significantly associated with self-reported OA after adjusting for age and serum creatinine only among females (OR: 1.47, 95%CI: 1.12–1.84). Furthermore, among the BMI-defined overweight group, the age-adjusted odds of self-reported OA was significantly higher for overweight/obese BF% compared to athletic/acceptable BF% in both females and males. In a secondary analysis, we showed that the association of self-reported OA and hypertension/cardiovascular diseases is significantly higher among BF% overweight/obese (OR: 1.37, 95%CI: 1.19–3.09) compared to BF% athletic/acceptable (OR: 1.13, 95%CI: 0.87–2.82).

Conclusion

Our results provide corroborating evidence for a relationship between body fat and OA in a population-based study, while no significant independent correlates were found between other metabolic markers and OA prevalence. Future investigation on the longitudinal relationship between BF and OA among this sub-population may inform targeted prevention opportunities.

Electronic supplementary material

The online version of this article (10.1186/s40608-018-0201-9) contains supplementary material, which is available to authorized users.

Keywords: Osteoarthritis, Obesity, Adipose tissue, Metabolic markers, Body fat, Population-based survey

Introduction

Osteoarthritis (OA) is a multifactorial degenerative joint disease affecting more than 1 in 8 individuals worldwide [1]. OA is among the fastest growing causes of loss in Disability Adjusted Life Years (DALYs) [2] mainly because of the aging population and increasing incidence of obesity [1, 2]. Obesity is conventionally measured using body mass index (BMI), and several studies have shown that individuals with obesity according to a BMI ≥ 30 are at higher risk for developing radiographic and symptomatic OA [1, 3]. Previous studies have shown that measurements of body composition and fat distribution may offer no advantage over BMI in assessment of risk for severe radiographic knee OA among the obese population [4, 5]. However, there is a paucity of research evaluating the independent association of metabolic markers and OA prevalence among a non-obese population [6].

Previous studies suggested that the initiation and progression of OA results from a complex interaction between mechanical axial loading on joints and various lipid, metabolic, and humoral risk factors [710]. Furthermore, recent findings on the significant association of body fat distribution with OA in non-weight bearing joints suggests that obesity-associated systemic factors could play an important role in the development and progression of OA [1115]. Brasnjevic et al. [16] showed that abdominal obesity was associated with radiographic progression of knee OA, and in a large Japanese cohort study, accumulation of metabolic syndrome components was related to the incidence and progression of knee OA components [17]. Preclinical models in rats also suggested a role of chronic inflammation, likely from metabolic stress, in OA onset and progression [1822].

Muscle weakness has also been identified as a key factor affecting OA onset and progression that further emphasizes the role for body composition, body fat distribution and OA development [2327]. In a population-based study, Ding et al. [24] noted a link between muscle weakness and body fat with OA, and found that the additive effects of muscle weakness and body fat increase the relative risk of OA compared to age and sex matched controls. Serum creatinine levels have been used as a surrogate measure for muscle mass in patients with chronic diseases [28, 29] and are also associated with lean mass in healthy individuals [30].

Several studies have also demonstrated that overweight (BMI between 25 to 30 kg/m2) during middle adulthood may play an important role in OA’s initiation and progression [31, 32]. Furthermore, OA management strategies and obesity prevention interventions [33] are most effective in the long-run when they are targeted to patients with overweight (BMI-defined non-obese) at early stages of the disease process [34]. As such, Manninen et al. [35] highlights the need to identify candidates for OA prevention and management strategies in the middle-aged and the non-obese.

The purpose of this study was to investigate the independent association between metabolic markers and self-reported OA among middle-aged BMI-defined non-obese individuals (40 to 65 years of age and BMI < 30 kg/m2). As such, we focus on measurements that are low-cost, ready to be implemented, and widely used in large population-based study cohorts including skinfold measured body fat, waist circumference and weight gained since adulthood. As the study population may not be assessed for OA prevalence at this time, the use of such metrics may be a feasible approach to support data collection and potential screening for adiposity and OA prevalence in this population who may not otherwise be assessed [35].

Methods

Data source and population

The Canadian Health Measures Survey (CHMS) is a bi-annual survey of Canadians health and health habits [36]. In the CHMS, Statistics Canada collects data from a nationally representative sample of the Canadian population aged 6–79 years living in private households in which approximately 96% of Canadians were represented [37]. CHMS is the first comprehensive and representative direct health measures study in Canada since the 1978–1979 Canada Health Survey [37].

The survey involved two components: an interview in the respondent’s home and a visit to a mobile examination center for a series of physical and clinical measurements. In all cycles of CHMS, data were collected at 15 sites across Canada. The interview included questions from respondents about a range of chronic conditions, defined as a condition diagnosed by a health professional and lasting, or expected to last, more than 6 months including OA, type 2 diabetes, and heart disease. Clinical and physical measures at an examination center included anthropometry, blood pressure, oral health examination, and blood and urine specimens [37]. Ethics approval to conduct the CHMS was obtained from Health Canada’s Research Ethics Board. Informed written consent was obtained from all adult respondents.

Sample selection

In this study, we used two cycles of the CHMS: 2007–2009, and 2009–2011. Health measures were included from both cycles. As our aim was to evaluate the relationship between body composition measurements and OA in non-obese middle-aged individuals, we included individuals between ages 40 to 65 years with BMI < 30 kg/m2. Individuals were not included if data were missing due to invalid BMI measurement, invalid skinfold measurements or if there were no body fat data collected. Figure 1 depicts the diagram of the sample selection from two cycles of CHMS included in this study.

Fig. 1.

Fig. 1

Flow chart of the study sample selection

Primary outcome

Osteoarthritis was determined from a patient reported response to the survey question about the physician-diagnosed arthritis: what kind of arthritis do you have? 1. Rheumatoid arthritis, 2. Osteoarthritis, 3. Rheumatism, or 4. Other. As a result, self-reported physician diagnosed OA was used as the outcome.

Metabolic markers

The measures used in this study were selected according to the metrics used in the literature for OA patients [47], which are low-cost, readily available and have been validated in population-based studies. Height was measured to the nearest 0.1 cm and weight was measured to the nearest 0.1 kg by standard devices on each mobile examination center [36]. BMI was calculated and classified according to standardized thresholds: normal (18.5 to 24.9 kg/m2), overweight (25.0 to 29.9 kg/m2) [36]. To determine the body fat, body density was first calculated using the summation of skinfold measures at four sites (triceps, biceps, subscapula, and iliac crest). Once body density was determined, body fat was calculated using a general sex-specific equation previously derived and validated by Durnin et al. [38]. Individual body fat percentages (BF%) were grouped into two body fat categories according to their distributions: athletic/acceptable (males: ≤20% females ≤30%), or overweight/obese (male > 20% females > 30%). This skinfold caliper technique is only validated for use in a population with BMI < 30 kg/m2, and as such, evaluating it excludes individuals who are obese by BMI [7].

Waist circumference was measured between the last rib and the top of the iliac crest after an expiration to the nearest 0.1 cm [36]. Waist circumference categories was defined according to standard thresholds used for females (> 88 cm and < 88 cm) and those for males (> 102 cm and < 102 cm) [39]. Maximum weight gain during adulthood was derived by subtracting “most adult weight ever” from the “weight at 18 years of age”. Previous studies have also examined maximum weight gain during adulthood in assessing risk of chronic diseases [40]. Laboratory Serum creatinine measures (μmol/L) were used as a surrogate for muscle mass [41]. Threshold for definition of high and low value of serum creatinine was used from [41] in which high values were defined as those with ≥65 μmol/L among males and ≥ 73 μmol/L among females.

Comorbidity assessments

We also extracted data on cardiovascular (CVD)-related comorbidities which included self-reported measures on history of heart disease, heart attack or high blood pressure. These were assessed using a response to three CHMS household questionnaire: (i) CCC_Q61: Do you have heart disease (1) Yes (0) No or (ii)CCC_Q63: Have you had a heart attack? (1) Yes (0) No, or (iii) CCC_Q64: Do you have high blood pressure?, (1) Yes (0) No. Clinical measurement for blood creatinine was also included as an indirect assessment of muscle mass (μmol/L). The sample size for responses to other chronic conditions including diabetes was small, and violated the minimal cell count prescribed by Statistics Canada, and therefore they were not included in the analysis.

Statistical analysis

All variables were assessed to ensure similarities in questions and responses. Cycles 1 and 2 were combined using methods described in the Statistics Canada documentation for combining the two CHMS datasets [36]. Quality assurance and quality control measures were previously performed independently on both CHMS datasets to minimize systematic bias [37]. Categorical variables were examined using frequency tables, and continuous variables were evaluated using summary statistics. If laboratory values were missing for blood creatinine, they were imputed using the level of detection limit divided by 2 [36]. Univariate analyses were conducted to investigate crude associations between the covariates and self-reported OA. In univariate analysis, p-values were based on an adjusted Pearson chi-squared test for independence (categorical variables), or a Bonferroni-adjusted Wald F-test (continuous variables). All results are weighted and standard errors are estimated using bootstrapping to account for the survey design effects of the CHMS. Kolmogorov–Smirnov tests were also performed to assess the normality of data for metabolic markers (p < 0.05). Multicollinearity diagnostics were performed by calculating variance inflation factor (VIF), which quantifies the severity of multicollinearity in an ordinary least squares regression analysis. VIF of BMI in all models were less than 2.6, which is below the threshold of 4 to represent multicollinearity.

Sex-stratified logistic regression models were developed to evaluate the association of self-reported OA with the five metabolic markers in this study. Models were separately adjusted for age, age and BMI, and age and blood creatinine levels in order to detect additional correlations that may exist between metabolic markers and self-reported OA. We further performed a stratified analysis across BMI groups to evaluate the independent association of BF% and self-reported OA among the BMI-defined overweight group and assess the additional information BF% could potentially provide other than those gained from BMI. In a secondary analysis, we developed logistic regression models to assess the association between OA and hypertension/CVD across BF% categories to identify the possible mediating role of the body fat on the association of OA and hypertension/CVD. Due to the small sample size within each cell for logistic regression modelling, and the limited age range in this sample of interest, no interactions with age or sex were included. All results were weighted according to the survey weights to represent the population-based sampling scheme of the CHMS. To account for survey design effects of the CHMS, standard errors, coefficients of variation, and 95% confidence intervals were estimated using the bootstrap technique (500 replications) provided in the CHMS documentation[36].

Results

A total of 2462 individuals between 40 to 65 years of age with BMI < 30 were selected for the final analysis, of which 217 (8.8%) reported OA (Fig. 1). Kolmogorov–Smirnov tests revealed that BMI, BF%, waist circumference and maximum weight gain data were normally distributed (p > 0.05). As shown in Table 1, the proportion of females was significantly higher among the individuals with self-reported OA (77%, SE: 3.5) compared to the non-OA (49.5%, SE: 0.94). The average BF% of individuals with self-reported OA was also higher than those of the non-OA group among both men [28.1%, SE:0.5) vs. (23.2%, SE:0.3), p < 0.01] and women [30.2%, SE: 0.3) vs. 33.9%, SE:0.2, p < 0.01], while waist circumference was significantly higher only among men [89.0 cm (SE:0.5) vs. 93.0 cm (SE:1.1), p < 0.01]. Furthermore, higher proportion of the self-reported OA indicated at least one CVD-related comorbidity compared to that of the non-OA sample among males [12.4%, SE: 2. vs. 4.9%, SE: 0.6, p < 0.01] and females [9.1% (SE: 2.1) vs. 3.8% (SE:0.5)] and had lower blood creatinine among males [78.1 μmol/L (SE: 1.0) vs. 82.4 μmol/L (SE: 0.5), p = < 0.01] and females [67.3 μmol/L (SE:1.0) vs. 72.8 μmol/L (SE:0.5), p = < 0.01]. The detailed results for the count of individuals within each BF%, BMI and sex groups are provided in Additional file 1: Table S1.

Table 1.

Characteristics of individuals with self-reported osteoarthritis (OA) compared to individuals without self-reported OAa

Characteristics b Overall sample No Self-Reported OA Self-Reported OA p-valued
n = 2462 n = 2245 n = 217
Demographics
 Age (years), mean (SEc) 52.6 (0.3) 52.2 (0.2) 57.3 (0.6) < 0.001
 Females, % (SE) 51 (1.2) 49.0 (0.9) 77.0 (3.5) < 0.001
Metabolic Markers
Females (n = 1267)
 Body Fat Percentage, mean (SE) 30.58 (0.3) 30.20 (0.2) 33.90 (0.3) < 0.01
 Body Mass Index (kg/m2), mean (SE) 26.33 (0.5) 26.20(0.4) 27.25(1.0) 0.112
 Waist Circumference (cm), mean (SE) 78.49(0.4) 78.23(0.4) 80.31(0.9) 0.08
 Maximum Weight Change (kg), mean (SE) 19.06(0.4) 18.90(0.5) 20.70 (0.9) 0.12
 Serum Creatinine (μmol/L), mean (SE) 71.6 (0.6) 72.8 (0.5) 67.3 (1.0) < 0.01
 Hypertension/CVDe, % (SE) 3.9 (0.6) 3.8 (0.5) 9.1 (2.1) < 0.01
Males (n = 1195)
 Body Fat Percentage, mean (SE) 23.67 (0.4) 23.2(0.3) 28.12(0.5) < 0.01
 Body Mass Index (kg/m2), mean (SE) 27.47 (0.6) 27.10 (0.5) 28.90 (1.2) 0.318
 Waist Circumference (cm), mean (SE) 89.53 (0.6) 89.00 (0.5) 93.00 (1.0) < 0.05
 Maximum Weight Change (kg), mean (SE) 16.46 (0.6) 16.30 (0.5) 18.10 (1.1) 0.231
 Serum Creatinine (μmol/L), mean (SE) 80.3 (0.5) 82.4 (0.5) 78.1 (1.0) < 0.01
 Hypertension/CVDe, % (SE) 5.1 (0.7) 4.9 (0.6) 12.4 (2.0) < 0.01

a All results are weighted according to the sample weights of the Canadian Health Measure Survey (CHMS); b Anthropometric, laboratory values, and percentage with comorbidity for patients with and without self-reported OA. c Standard error estimates were generated using 500 bootstrap replications. All statistics were evaluated at α = 0.05. d P-values are used for comparing measures across self-reported OA and non-OA; for categorical variables, p-values were based on an adjusted Pearson chi-squared test for independence, and p-values for continuous variables were based on an adjusted Wald F test. e Maximum Weight Change as an adult from 18-years-old; fHypertension/CVD: Self-reported hypertension or Cardiovascular Disease

As shown in Table 2 for the result of the multivariate analysis, higher BF% and waist circumference categories were significantly associated with self-reported OA, independent of age, for both males and females (p < 0.05). Those within the BF%-defined obese/overweight category had higher odds of self-reported OA compared to those within the BF%-defined athletic/acceptable category for females (OR: 3.2, 95% CI: 1.25–4.4) and males (OR: 1.82, 95% CI: 1.15–3.58) after adjusting for age. Similarly, those in the high waist circumference category had significantly higher odds of self-reported OA compared to those in the low category for both females (OR: 2.62, 95% CI: 1.51–3.01) and males (OR: 2.21, 95% CI:1.3–3.81) after adjusting for age. Furthermore, among males, each kilogram of maximum weight gained was associated with 3% higher odds of self-reported OA independent of the current age (OR: 1.04, 95% CI: 1.02–1.76).

Table 2.

Odds ratios (and 95% confidence intervals) from logistic regressions for associations of metabolic markers with self-reported OAa

Models Categories Adjusted models (by age) Adjusted models (by age, BMI) Adjusted models (by age, serum creatinine)
Female (n = 1267) Model 1. BMI categories Underweight/normal (< 25 kg/m2) Ref Ref
Overweight (25–30 kg/m2) 1.53 (0.65, 2.13) 1.32 (0.87,2.21)
Model 2. BF%b categories Athletic/ Acceptable Ref Ref Ref
Overweight/obese 3.12 (1.25,4.4)* 2.67 (1.32,3.51)* 1.47 (1.12,1.84)*
Model 3. Waist circumference (cm) < 88 cm Ref Ref Ref
> 88 cm 2.62 (1.51,3.01)* 0.91 (0.80,2.64) 1.27 (0.91,2.14)
Model 4. Maximum Weight change (kg)c 1.03 (0.91,1.43) 1.07 (0.96,2.46) 1.03 (0.82,2.68)
Model 5. Serum Creatinine ≥65 μmol/L Ref Ref
< 65 μmol/L 1.21 (0.87,2.45) 0.87 (0.45,1.97)
Male (n = 1195) Model 1. BMI categories Underweight/normal (< 25 kg/m2) Ref Ref
Overweight (25–30 kg/m2) 0.92 (0.75,1.91) 1.43 (0.93,2.45)
Model 2. BF%b categories Athletic/ acceptable Ref Ref Ref
Overweight/obese 1.82 (1.15,3.58)* 2.11 (1.38,3.21)* 1.12 (0.78,1.93)
Model 3. Waist circumference (cm) < 102 cm Ref Ref Ref
> 102 cm 2.21 (1.3,3.81)* 0.91(0.83,1.54) 1.08 (0.91,1.72)
Model 4. Maximum Weight change c(kg) 1.04 (1.02,1.76)* 1.05 (0.87,2.32) 0.29 (0.12,2.16)
Model 5. Serum Creatinine ≥73 μmol/L Ref Ref
< 73 μmol/L 1.97 (0.91,2.89) 0.91 (0.35,2.1)

a All results are weighted according to the sample weights of the Canadian Health Measure Survey (CHMS); b Body Fat percentage (BF%);c Individual body fat percentages were grouped into three body fat categories: athletic/good (males: < 14% females < 23%), acceptable (males 15–20%, females 24–30%), or overweight/obese (male > 21% females > 31%).; d Maximum Weight change as an adult from 18-years-old (kg); * p-value< 0.05

As shown in Table 2, only the BF%-defined obese/overweight category was associated with self-reported OA independent of BMI and age. The adjusted odds of self-reported OA was higher among overweight/obese BF% compared to athletic/acceptable category among females (OR: 2.67, 95%CI:1.32–3.51) and males (OR:2.11, 95%CI:1.38–3.21) after adjusting for age and BMI. Furthermore, BF% was significantly associated with self-reported OA after adjusting for age and serum creatinine only among females (OR: 1.47, 95%CI: 1.12–1.84).

BMI-stratified analysis in Table 3 revealed that among the BMI-defined overweight group, the age-adjusted odds of self-reported OA was significantly higher for overweight/obese BF% compared to athletic/acceptable BF% in both females (OR:1.84, 95% CI:1.18–3.19) and males (OR:1.32,95% CI:1.12–2.79). The association between OA and BF% categories was not significant among the BMI-defined underweight/normal group.

Table 3.

Age-adjusted odds ratio (and 95% confidence intervals) for self-reported OA across BF% categories stratified by BMI groups and sex

BMI Underweight/Normal Overweight
Body Fat Percentage (BMI < 25 kg/m2) (BMI 25–29.99 kg/m2)
Female Athletic/Acceptable Reference Reference
Overweight/Obese 1.92 (0.81,2.87) 1.84 (1.18,3.19)*
(n = 711) (n = 556)
Male Athletic/Acceptable Reference Reference
Overweight/Obese 1.41 (0.61,2.39) 1.32 (1.12,2.79)*
(n = 394) (n = 801)

All four models were adjusted for age; Individual body fat percentages were grouped into three body fat categories: athletic/good (males: < 14% females < 23%), acceptable (males 15–20%, females 24–30%), or overweight/obese (male > 21% females > 31%).;* p-value< 0.05

According to our secondary analysis for association of OA and CVD across BF% categories, the age and sex–adjusted odds of self-reported OA was 37% (OR:1.37, 95%CI: 1.19–3.09) higher in those with CVD compared to those without CVD among the overweight/obese BF% category, while the OA and CVD association was not significant among those with athletic/acceptable BF% (OR: 1.13, 95% CI:0.87–2.82).

Discussion

In this study, BF% measured by skinfold calipers provides important information with respect to self-reported OA among a Canadian sample of middle-aged BMI-defined non-obese individuals (40 to 65 years of age and BMI < 30 kg/m2) that is not necessarily captured by BMI alone. According to these results, BF% categories are independently associated with self-reported OA while adjusting for BMI and age, and there is a significant difference between the odds of OA across body fat categories for those within the BMI-defined overweight category (BMI between 25 and 30 kg/m2) in both male and female models. No independent correlates were found between other metabolic markers used in this study and self-reported OA among the study population.

Our results, however, demonstrate a univariate relationship between decreased serum creatinine, an indirect measurement of muscle mass [29] with increased OA. Furthermore, in the female-specific model, the odds of self-reported OA was significantly higher among obese/overweight BF% compared to athletic/acceptable BF% when adjusting for age and blood creatinine. This suggests that body fat may provide independent information other than that gained from serum creatinine regarding the relations between body composition and OA. Our findings suggest that both increased body fat and decreased lean mass may be characteristic of OA, but the causal contribution of these metabolic abnormalities to OA have yet to be directly tested and explored [29]. In a previous study, the combined effects of reduced lean mass with increased fat mass were shown to be associated with elevated risk of OA compared to obesity alone [42]. Results from the present study provide cross-sectional evidence for an association between obesity and OA among the middle-aged non-obese population. Longitudinal studies are needed to confirm these associations.

We further showed that the age and sex-adjusted association of self-reported OA and CVD was significantly higher in the obese/overweight BF% group compared to the association observed in athletic/acceptable BF% group. This highlights the importance of BF% in identifying those with multi-morbidity among OA population. Similar results were reported in a recent large Japanese cohort study [17] where accumulation of metabolic syndrome components were shown to be related to the incidence and progression of knee OA components. OA individuals with overweight or obesity have shown to demonstrate higher abdominal adiposity (waist circumference) [25], increased waist-to-height ratio, increased rates of high blood pressure, high cholesterol, and higher body fat compared to OA patients with athletic/acceptable BF% [43]. A recent study evaluated the cross-sectional association between metabolic markers and OA among the BMI-defined non-obese and showed that skinfold BF% is associated with higher OA prevalence [44] which corresponds to our results. Brasnjevic et al. [16] showed that abdominal obesity was associated with radiographic progression of knee OA.

While several studies showed that body fat distribution does not provide additional information other than those gained through BMI among individuals with severe knee OA [4, 5], there is a scarcity of research that individually assesses the non-obese population in this context. Our study demonstrates that measuring body fat may provide additional information that is supplementary to, or independent of, BMI with regards to OA prevalence among the middle-aged non-obese OA patients. Understanding the association of BF% and other metabolic markers with OA within a non-obese population may help improve the development of screening policies for prevention and management strategies in OA [33]. For instance, the discordance between BMI and body fat is predominantly observed in women with “healthy” BMIs (BMI ≤24.99) but who are overweight or obese based on metabolic markers such as levels of body fat (BF% ≥ 31%) [21, 23, 24] or abdominal obesity measured by waist circumference [8, 9]. Given that these metabolic markers have shown to be significantly associated with OA progression [16] and health outcomes [17], such women would traditionally be medically managed as healthy, and as such, and may miss OA prevention opportunities even though they may be at increased risk.

As our data are representative of the Canadian population, they are likely generalizable to other countries with population characteristics similar to that of Canada. There are known differences in body fat and body composition across races and ethnicities [45], and the predictability of body fat by the equations used by the CHMS dataset. The data presented in this study reflects the ethnic diversity of Canadians. OA affects more than 4.6 million Canadians [46], and it is estimated that 1 in 4 Canadians will have OA by 2040 due to aging, increased longevity of the population and the obesity epidemic [46]. Countries with a homogeneous racial or ethnic population should validate these findings in their given population, as differences in fat storage between races have been previously reported [47].

A body fat classification system from Durnin et al. [38] was used in this study that divided individuals into categories based on BF% and sex. Other body fat categorization schemes have been developed, but include age [48]. Specifically, the World Health Organization criteria incorporates increased BF% in the “acceptable” category for each increasing age group, which makes isolating the individual effect of body fat on OA challenging [49]. As the goal of this study was to evaluate the effects of discrete BF% values on OA, a fixed sex-specific classification of BF% was used. Body fat changes with age [50], and both age and sex are strongly associated with OA [1]. To compensate for this, our models were adjusted for age and stratified by sex.

There are several limitations to this work. One significant limitation of the CMHS dataset is that it does not include data on previous injury or family history of OA. However, as previously mentioned, there are several accepted primary risk factors calling for sub classification, or subtypes of OA to define a “profile” that describes each of these subtypes [25]. Therefore, we speculate that the trend toward an increased odds ratio of athletic/acceptable BF% individuals for OA demonstrated here may be related to these factors that were not measured. As all individuals included in this study had a BMI < 30 kg/m2, it is possible that they demonstrate a “pre-metabolic syndrome” phenotype but may still have metabolic abnormalities contributing to their OA. Here, we were unable to evaluate all metabolic parameters of interest in the logistic regression models because of weighting limitations associated with combining fasted lab values from the CHMS Statistics Canada dataset. Due to the limited sample size of our study, we also did not adjust for a variety of risk factors that are known to be related to OA (socioeconomic status, ethnicity, smoking), but that would be useful to consider in future investigations. Additionally, the limited age group evaluated did not allow for us to evaluate these relations across the weight or age spectrum. There are also limitations associated with the use of skinfold anthropometry; it may underestimate BF% when compared to other methods such as dual energy x-ray absorptiometry as the former does not account for intra-abdominal or visceral adipose tissue stores [51]. Consequently, skinfold anthropometry lacks appropriate population-specific cut-off values to identify health risks among individuals with obesity [51]. Lastly, a substantial limitation of this work was the binary and self-reported nature of the primary outcome measure, OA. This analysis is based on an outcome variable acquired from self-report data. However, we suggest that the preliminary context of this study and information gained from this analysis justifies the use of this outcome.

Future work should longitudinally evaluate the association of body fat, lean mass, muscle strength, pain and structural graded MRI Osteoarthritis Knee Score [4] or radiographic Kellgren-Lawrence outcomes [4] to better understand implications of metabolic risk factors, adiposity, and osteoarthritis severity among the non-obese population. Clinically, better measures of body fat or body composition (e.g., DXA [47]) could be used to understand risk of developing OA according to body fat measurements in patients across the spectrum of body composition. The presence of an OA subtype may be supported by a relationship between increased body fat, indirect measures of body composition, elevated CVD risk, and OA.

Conclusion

This study demonstrates that measuring body fat may provide additional information over and above BMI with regards to OA prevalence among the middle-aged non-obese population. However, no independent correlate was found between other metabolic markers used in this study and the self-reported OA among the study population. Given the rise in prevalence of OA among the middle-aged population [46] and the increased effectiveness of prevention interventions among the BMI-defined non-obese population [34], this study highlights the need to better understand the interrelation of body fat and risk of OA among the BMI-defined non-obese population. Our results pave the way to further explore the use of low-cost, readily available, population-based metrics for metabolic markers as a primary care screening tool among younger non-obese individuals, who may not otherwise be assessed for OA risk or musculoskeletal compromise.

Additional file

Additional file 1: (14.2KB, docx)

BMI and body fat percentage classification. The supplementary data provides a summary of the sample data for BMI and body fat percentage classification across males and females. (DOCX 14 kb)

Acknowledgements

We wish to acknowledge the assistance of the Prairie Regional Research Data Centre, Statistics Canada, Dr. Cyril Frank, Sarah L. Lacny, and thoughtful conversations about data interpretation with fellow members and trainees from the Alberta Innovates Health Solutions Team in Osteoarthritis.

Funding

Alberta Innovates Health Solutions Team in Osteoarthritis. DM is supported by a Canada Research Chair in Health Systems and Services Research, and Arthur J.E. Child Chair in Rheumatology. KH is supported by an Izaak Walton Killam pre-doctoral scholarship. WH is supported by a Canada Research Chair in Applied Cellular and Molecular Biomechanics and a Killam Memorial Research Chair. The funding agencies listed here had no role in the project design, execution, analysis, or manuscript drafting.

Availability of data and materials

The data that support the findings of this study are available from Statistics Canada, health Analysis Division, but restrictions apply to the availability of these data, which were used under license for the current study, and so are not publicly available. Data are however available from the authors upon reasonable request and with permission of Statistics Canada.

Abbreviations

BF

Body Fat

BMI

Body Mass Index

CHMS

Canadian Health Measures Survey

CVD

Cardiovascular diseases

OA

Osteoarthritis

SE

Standard Error

Authors’ contributions

Study concept and design: BS, KC, DM, CS, RR, RC, WH; Acquisition of data: CS,KC, RC, DM,CS; Analysis and interpretation of data: BS, KC, DM, RR, CS, WH; Statistical analysis: RC, BS; Drafting of the manuscript: KC, BS, DM, CS, RR, RC, WH; Critical revision of the manuscript for important intellectual content: BS, KC, RC, RR, CS, WH, DM. All authors read and approved the final manuscript.

Ethics approval and consent to participate

Ethics approval to conduct the survey used for this study was obtained from Health Canada’s Research Ethics Board. Informed written consent was obtained from all adult respondents.

Competing interests

The views expressed in this paper are solely those of the authors and do not reflect those of Statistics Canada. We thank Claudia Sanmartin for her contributions related to data access and analysis

Publisher’s Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Contributor Information

Kelsey H. Collins, Email: Khmcolli@ucalgary.ca

Behnam Sharif, Phone: 587-703-8474, Email: behnam.sharif@ucalgary.ca.

Raylene A. Reimer, Email: reimer@ucalgary.ca

Claudia Sanmartin, Email: claudia.sanmartin@canada.ca.

Walter Herzog, Email: wherzog@ucalgary.ca.

Rick Chin, Email: rchin@ucalgary.ca.

Deborah A. Marshall, Email: damarsha@ucalgary.ca

References

  • 1.Oliveria SA, Felson DT, Cirillo PA, Reed JI, Walker AM. Body weight, body mass index, and incident symptomatic osteoarthritis of the hand, hip, and knee. Epidemiology. 1999;10(2):161–166. doi: 10.1097/00001648-199903000-00013. [DOI] [PubMed] [Google Scholar]
  • 2.Cross M, Smith E, Hoy D, Nolte S, Ackerman I, Fransen M, Bridgett L, Williams S, Guillemin F, Hill CL, Laslett LL. The global burden of hip and knee osteoarthritis: estimates from the global burden of disease 2010 study. Ann Rheum Dis 2014 Feb 19. [DOI] [PubMed]
  • 3.Blagojevic M, Jinks C, Jeffery A, Jordan KP. Risk factors for onset of osteoarthritis of the knee in older adults: a systematic review and meta-analysis. Osteoarthr Cartil. 2010;18(1):24–33. doi: 10.1016/j.joca.2009.08.010. [DOI] [PubMed] [Google Scholar]
  • 4.Abbate LM, Stevens J, Schwartz TA, Renner JB, Helmick CG, Jordan JM. Anthropometric measures, body composition, body fat distribution, and knee osteoarthritis in women. Obesity. 2006;14(7):1274–1281. doi: 10.1038/oby.2006.145. [DOI] [PubMed] [Google Scholar]
  • 5.Lohmander LS, de Verdier MG, Rollof J, Nilsson PM, Engström G. Incidence of severe knee and hip osteoarthritis in relation to different measures of body mass: a population-based prospective cohort study. Ann Rheum Dis. 2009;68(4):490–496. doi: 10.1136/ard.2008.089748. [DOI] [PubMed] [Google Scholar]
  • 6.Sowers MR, Karvonen-Gutierrez CA. The evolving role of obesity in knee osteoarthritis. Curr Opin Rheumatol. 2010;22(5):533. doi: 10.1097/BOR.0b013e32833b4682. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 7.Velasquez MT, Katz JD. Osteoarthritis: another component of metabolic syndrome? Metab Syndr Relat Disord. 2010;8:295–305. doi: 10.1089/met.2009.0110. [DOI] [PubMed] [Google Scholar]
  • 8.Wang Y, Simpson JA, Wluka AE, Teichtahl AJ, English DR, Giles GG, Graves S, Cicuttini FM. Relationship between body adiposity measures and risk of primary knee and hip replacement for osteoarthritis: a prospective cohort study. Arthritis research & therapy. 2009;11(2):R31. doi: 10.1186/ar2636. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 9.Hart DJ, Doyle DV, Spector TD. Association between metabolic factors and knee osteoarthritis in women: the Chingford study. J Rheumatol. 1995;22:1118–1123. [PubMed] [Google Scholar]
  • 10.Conaghan PG, Kloppenburg M, Schett G, Bijlsma JW. Osteoarthritis research priorities: a report from a EULAR ad hoc expert committee. Ann Rheum Dis. 2014;73(8):1442–1445. doi: 10.1136/annrheumdis-2013-204660. [DOI] [PubMed] [Google Scholar]
  • 11.Berenbaum F, Griffin TM, Liu-Bryan R. Metabolic regulation of inflammation in osteoarthritis. Arthritis & rheumatology. 2017;69(1):9–21. doi: 10.1002/art.39842. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 12.Bliddal H, Leeds AR, Christensen R. Osteoarthritis, obesity and weight loss: evidence, hypotheses and horizons–a scoping review. Obes Rev. 2014;15(7):578–586. doi: 10.1111/obr.12173. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 13.Gregor MF, Hotamisligil GS. Inflammatory mechanisms in obesity. Annu Rev Immunol. 2011;29:415–445. doi: 10.1146/annurev-immunol-031210-101322. [DOI] [PubMed] [Google Scholar]
  • 14.Hotamisligil GS. Inflammation and metabolic disorders. Nature. 2006;444(7121):860–867. doi: 10.1038/nature05485. [DOI] [PubMed] [Google Scholar]
  • 15.Visser AW, Ioan-Facsinay A, de Mutsert R, Widya RL, Loef M, de Roos A, le Cessie S, den Heijer M, Rosendaal FR, Kloppenburg M. Adiposity and hand osteoarthritis: the Netherlands epidemiology of obesity study. Arthritis research & therapy. 2014;16(1):1. doi: 10.1186/ar4447. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 16.Vasilic-Brasnjevic S, Marinkovic J, Vlajinac H, Vasiljevic N, Jakovljevic B, Nikic M, Maksimovic M. Association of body mass index and waist circumference with severity of knee osteoarthritis. Acta reumatologica portuguesa. 2016;41(3):226–231. [PubMed] [Google Scholar]
  • 17.Yoshimura N, Muraki S, Oka H, Tanaka S, Kawaguchi H, Nakamura K, et al. Accumulation of metabolic risk factors such as overweight, hypertension, dyslipidaemia, and impaired glucose tolerance raises the risk of occurrence and progression of knee osteoarthritis: a 3-year follow-up of the ROAD study. Osteoarthr Cartil. 2012;20:1217–1226. doi: 10.1016/j.joca.2012.06.006. [DOI] [PubMed] [Google Scholar]
  • 18.Gierman LM, van der Ham F, Koudijs A, Wielinga PY, Kleemann R, Kooistra T, Stoop R, Kloppenburg M, van Osch GJ, Stojanovic-Susulic V, Huizinga TW. Metabolic stress–induced inflammation plays a major role in the development of osteoarthritis in mice. Arthritis & Rheumatism. 2012;64(4):1172–1181. doi: 10.1002/art.33443. [DOI] [PubMed] [Google Scholar]
  • 19.Griffin TM, Huebner JL, Kraus VB, Yan Z, Guilak F. Induction of osteoarthritis and metabolic inflammation by a very high-fat diet in mice: effects of short-term exercise. Arthritis & Rheumatism. 2012;64(2):443–453. doi: 10.1002/art.33332. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 20.Brunner AM, Henn CM, Drewniak EI, Lesieur-Brooks A, Machan J, Crisco JJ, Ehrlich MG. High dietary fat and the development of osteoarthritis in a rabbit model. Osteoarthr Cartil. 2012;20(6):584–592. doi: 10.1016/j.joca.2012.02.007. [DOI] [PubMed] [Google Scholar]
  • 21.Louer CR, Furman BD, Huebner JL, Kraus VB, Olson SA, Guilak F. Diet-induced obesity significantly increases the severity of posttraumatic arthritis in mice. Arthritis & Rheumatism. 2012;64(10):3220–3230. doi: 10.1002/art.34533. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 22.Collins KH, Herzog W, MacDonald GZ, Reimer RA, Rios JL, Smith IC, Zernicke RF, Hart DA. Obesity, metabolic syndrome, and musculoskeletal disease: common inflammatory pathways suggest a central role for loss of muscle integrity. Front Physiol. 2018;9:112. https://www.frontiersin.org/article/10.3389/fphys.2018.00112. [DOI] [PMC free article] [PubMed]
  • 23.Lee R, Kean WF. Obesity and knee osteoarthritis. Inflammopharmacology. 2012;20(2):53–58. doi: 10.1007/s10787-011-0118-0. [DOI] [PubMed] [Google Scholar]
  • 24.Ding C, Stannus O, Cicuttini F, Antony B, Jones G. Body fat is associated with increased and lean mass with decreased knee cartilage loss in older adults: a prospective cohort study. Int J Obes. 2013;37(6):822–827. doi: 10.1038/ijo.2012.136. [DOI] [PubMed] [Google Scholar]
  • 25.Karlsson MK, Magnusson H, Cöster M, Karlsson C, Rosengren BE. Patients with knee osteoarthritis have a phenotype with higher bone mass, higher fat mass, and lower lean body mass. Clin Orthop Relat Res. 2015;473(1):258–264. doi: 10.1007/s11999-014-3973-3. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 26.World Health Organization. Obesity: Preventing and Managing the Global Epidemic [Internet]. Report of a WHO consultation on obesity. 1998 [cited 2016 June 18]. Available from: http://www.who.int/nutrition/publications/obesity/WHO_TRS_894/en/ [PubMed]
  • 27.Mokdad AH, Ford ES, Bowman BA, Dietz WH, Vinicor F, bales VS, et al. prevalence of obesity, diabetes, and obesity-related health risk factors, 2001. JAMA 2003 Jan 1;289(1):76–79. [DOI] [PubMed]
  • 28.Patel SS, Molnar MZ, Tayek JA, Ix JH, Noori N, Benner D, Heymsfield S, Kopple JD, Kovesdy CP, Kalantar-Zadeh K. Serum creatinine as a marker of muscle mass in chronic kidney disease: results of a cross-sectional study and review of literature. J Cachexia Sarcopenia Muscle. 2013;4(1):19–29. doi: 10.1007/s13539-012-0079-1. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 29.Heymsfield S, Arteaga C, McManus C, Smith J, Moffitt S. Measurement of muscle mass in humans: validity of the 24-hour urinary creatinine method. Am J Clin Nutr. 1983;37(3):478–494. doi: 10.1093/ajcn/37.3.478. [DOI] [PubMed] [Google Scholar]
  • 30.Kim SW, Jung HW, Kim CH, Kim KI, Chin HJ, Lee H. A new equation to estimate muscle mass from creatinine and cystatin C. PLoS One. 2016;11(2):e0148495. doi: 10.1371/journal.pone.0148495. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 31.Holliday KL, McWilliams DF, Maciewicz RA, Muir KR, Zhang W, Doherty M. Lifetime body mass index, other anthropometric measures of obesity and risk of knee or hip osteoarthritis in the GOAL case-control study. Osteoarthr Cartil. 2011;19:37–43. doi: 10.1016/j.joca.2010.10.014. [DOI] [PubMed] [Google Scholar]
  • 32.Liu B, Balkwill A, Banks E, Cooper C, Green J, Beral V. Relationship of height, weight and body mass index to the risk of hip and knee replacements in middle-aged women. Rheumatology (Oxford) 2007;46:861–867. doi: 10.1093/rheumatology/kel434. [DOI] [PubMed] [Google Scholar]
  • 33.Chan RS, Woo J. Prevention of overweight and obesity: how effective is the current public health approach. Int J Environ Res Public Health. 2010;7(3):765–783. doi: 10.3390/ijerph7030765. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 34.Collins KH. Association of body mass index (BMI) and percent body fat among BMI-defined non-obese middle-aged individuals: insights from a population-based Canadian sample. Canadian Journal of Public Health. 2016;107(6):E520. doi: 10.17269/cjph.107.5652. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 35.Manninen P, Riihimaki H, Heliövaara M, Suomalainen O. Weight changes and the risk of knee osteoarthritis requiring arthroplasty. Ann Rheum Dis. 2004;63(11):1434–1437. doi: 10.1136/ard.2003.011833. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 36.Statistics Canada. Canadian Health Measures Survey (CHMS) Data User Guide: Cycle 1 [Internet]. 2011 [cited 2016 June 18]. Available from: http://www23.statcan.gc.ca/imdb-bmdi/pub/document/5071_D2_T1_V1-eng.htm.
  • 37.Tremblay M, Wolfson M, Connor Gorber S. Canadian Health Measures Survey: rationale, background, and overview. Stat Canada Heal Reports. 2007;18 Supp:7–20. [PubMed]
  • 38.Durnin JVG a, Womersley J. Body fat assessed from total body density and its estimation from skinfold thickness: measurements on 481 men and women aged from 16 to 72 years. Br J Nutr. 2007;32(01):77–97. doi: 10.1079/BJN19740060. [DOI] [PubMed] [Google Scholar]
  • 39.US Department of Health and Human Services. Clinical Guidelines on the Identification, Evaluation, and Treatment of Overweight and Obesity in Adults: An Evidence Report [Internet]. US DHHS. 1998. p.98–4083 [cited 2016 June 18]. Available from: https://www.ncbi.nlm.nih.gov/books/NBK2003/.
  • 40.Lim S, Kim KM, Kim MJ, Woo SJ, Choi SH, Park KS, Jang HC, Meigs JB, Wexler DJ. The association of maximum body weight on the development of type 2 diabetes and microvascular complications: MAXWEL study. PLoS One. 2013;8(12):e80525. doi: 10.1371/journal.pone.0080525. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 41.Hjelmesæth J, Røislien J, Nordstrand N, Hofsø D, Hager H, Hartmann A. Low serum creatinine is associated with type 2 diabetes in morbidly obese women and men: a cross-sectional study. BMC Endocr Disord. 2010;10(1):6. doi: 10.1186/1472-6823-10-6. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 42.Patel SS, Molnar MZ, Tayek JA, Ix JH, Noori N, Benner D, et al. Serum creatinine as a marker of muscle mass in chronic kidney disease: results of a cross-sectional study and review of literature. J Cachexia Sarcopenia Muscle. 2013;4(1):19–29. doi: 10.1007/s13539-012-0079-1. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 43.Lee S, Kim T-N, Kim S-H. Sarcopenic obesity is more closely associated with knee osteoarthritis than is nonsarcopenic obesity: a cross-sectional study. Arthritis Rheum. 2012;64(12):3947–3954. doi: 10.1002/art.37696. [DOI] [PubMed] [Google Scholar]
  • 44.Sanghi D, Srivastava RN, Singh A, Kumari R, Mishra R, Mishra A. The association of anthropometric measures and osteoarthritis knee in non-obese subjects: a cross sectional study. Clinics. 2011;66(2):275–279. doi: 10.1590/S1807-59322011000200016. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 45.Topp R, RN PD, Malkani AL. Self-reported chair-rise ability relates to stair-climbing readiness of total knee arthroplasty patients: a pilot study. J Rehabil Res Dev. 2007;44(5):751. doi: 10.1682/JRRD.2006.11.0146. [DOI] [PubMed] [Google Scholar]
  • 46.Arthrtiis Alliance of Canda. The Impact of Arthritis in Canada: Today and Over the Next 30 Years [internet]. 2011[cited 2016 June 18]. Available from: http://www.arthritisalliance.ca/images/PDF/eng/Initiatives/20111022_2200_impact_of_arthritis.pdf.
  • 47.Davidson LE, Wang J, Thornton JC, Kaleem Z, Silva-Palacios F, Pierson RN, et al. Predicting fat percent by skinfolds in racial groups: Durnin and Womersley revisited. Med Sci Sports Exerc. 2011;43(3):542–549. doi: 10.1249/MSS.0b013e3181ef3f07. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 48.Gallagher D, Heymsfield SB, Heo M, Jebb SA, Murgatroyd PR, Sakamoto Y. Healthy percentage body fat ranges: an approach for developing guidelines based on body mass index. Am J Clin Nutr. 2000;72(3):694–701. doi: 10.1093/ajcn/72.3.694. [DOI] [PubMed] [Google Scholar]
  • 49.Woolf AD, Pfleger B. Burden of major musculoskeletal conditions. Bull World Health Organ. 2003;81(9):646–656. [PMC free article] [PubMed] [Google Scholar]
  • 50.Kuk JL, Saunders TJ, Davidson LE, Ross R. Age-related changes in total and regional fat distribution. Ageing Res Rev. 2009;8(4):339–348. doi: 10.1016/j.arr.2009.06.001. [DOI] [PubMed] [Google Scholar]
  • 51.Garcia AL, Wagner K, Hothorn T, Koebnick C, Zunft H-JF, Trippo U. Improved prediction of body fat by measuring skinfold thickness, circumferences, and bone breadths. Obes Res. 2005;13(3):626–634. doi: 10.1038/oby.2005.67. [DOI] [PubMed] [Google Scholar]

Associated Data

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

Supplementary Materials

Additional file 1: (14.2KB, docx)

BMI and body fat percentage classification. The supplementary data provides a summary of the sample data for BMI and body fat percentage classification across males and females. (DOCX 14 kb)

Data Availability Statement

The data that support the findings of this study are available from Statistics Canada, health Analysis Division, but restrictions apply to the availability of these data, which were used under license for the current study, and so are not publicly available. Data are however available from the authors upon reasonable request and with permission of Statistics Canada.


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