Hostname: page-component-586b7cd67f-gb8f7 Total loading time: 0 Render date: 2024-11-22T00:40:50.223Z Has data issue: false hasContentIssue false

Assessing the causal relationship of birth weight and childhood obesity on osteoarthritis: a Mendelian randomization study

Published online by Cambridge University Press:  03 June 2024

Zengfeng Xin
Affiliation:
Department of Orthopaedics, The Second Affiliated Hospital, Zhejiang University School of Medicine, Hangzhou, China Orthopedics Research Institute of Zhejiang University, Hangzhou, China Key Laboratory of Motor System Disease Research and Precision Therapy of Zhejiang Province, Hangzhou, China Clinical Research Center of Motor System Disease of Zhejiang Province, Hangzhou, China
Lingxiao Xu
Affiliation:
Department of Orthopaedics, The Second Affiliated Hospital, Zhejiang University School of Medicine, Hangzhou, China Orthopedics Research Institute of Zhejiang University, Hangzhou, China Key Laboratory of Motor System Disease Research and Precision Therapy of Zhejiang Province, Hangzhou, China Clinical Research Center of Motor System Disease of Zhejiang Province, Hangzhou, China
Lingling Sun*
Affiliation:
Department of Orthopaedics, The Second Affiliated Hospital, Zhejiang University School of Medicine, Hangzhou, China Orthopedics Research Institute of Zhejiang University, Hangzhou, China Key Laboratory of Motor System Disease Research and Precision Therapy of Zhejiang Province, Hangzhou, China Clinical Research Center of Motor System Disease of Zhejiang Province, Hangzhou, China
*
Corresponding author: L. Sun; Email: [email protected]
Rights & Permissions [Opens in a new window]

Abstract

Obesity is associated with osteoarthritis (OA), but few studies have used fetal origin to explore the association. Our study aims to disentangle the causality between birth weight, childhood obesity, and adult OA using Mendelian randomization (MR). We identified single nucleotide polymorphisms (SNPs) related to birth weight (n = 298,142) and childhood obesity (n = 24,160) from two genome-wide association studies contributed by the Early Growth Genetics Consortium. Summary statistics of OA and its phenotypes (knee, hip, spine, hand, thumb, and finger OA) from the Genetics of Osteoarthritis Consortium (n = 826,690) were used to estimate the effects of SNPs on OA. Multivariable MR (MVMR) was conducted to investigate the independent effects of exposures. It turned out that genetically predicted standard deviation increase in birth weight was not associated with OA. In contrast, there was a marginally positive effect of childhood obesity on total [odds ratio (OR) = 1.07, 95% confidence interval (CI) = 1.00, 1.15 using IVW], knee (OR = 1.13, 95% CI = 1.05, 1.22 using weighted median), hip (OR = 1.13, 95% CI = 1.04, 1.24 using IVW), and spine OA (OR = 1.12, 95% CI = 1.03, 1.22 using IVW), but not hand, thumb, or finger OA. MVMR indicated a potential adulthood body mass index-dependent causal pathway between childhood obesity and OA. In conclusion, no association of birth weight with OA was suggested. Childhood obesity, however, showed a causality with OA in weight-bearing joints, which seems to be a general association of obesity with OA.

Type
Original Article
Copyright
© The Author(s), 2024. Published by Cambridge University Press in association with The International Society for Developmental Origins of Health and Disease (DOHaD)

Introduction

Obesity and osteoarthritis (OA) are two major public healthcare problems due to their high prevalence among adults worldwide. Reference Peat and Thomas1,2 There is evidence for a higher risk of developing OA among overweight adults than those with normal weight. Reference Litwic, Edwards, Dennison and Cooper3Reference Blagojevic, Jinks, Jeffery and Jordan5 More recently, the effects of childhood obesity and even birth weight on developing OA in adulthood were also recognized, Reference Antony, Jones and Venn6Reference Hussain, Ackerman, Wang, Zomer and Cicuttini10 suggesting the fetal origins hypothesis. Reference Barker11,Reference Lucas, Fewtrell and Cole12 The hypothesis indicates that adverse intrauterine environment may influence fetal growth and development, consequently, resulting in a long-term influence on later health status. Such idea is helpful to broaden the potential mechanisms for many chronic diseases in humans. Many observational studies have reported an increased risk of OA in individuals with early abnormal weight, such as lower birth weight as well as childhood obesity. Reference Antony, Jones and Venn6,Reference Hussain, Ackerman, Wang, Zomer and Cicuttini10 However, no significant effect of intra-pair birth weight differences on OA was observed in a prospective cohort study of female twins. Reference Antoniades, MacGregor, Andrew and Spector13 A British birth cohort study found that the association between body mass index (BMI) and later knee OA was not detectable until age 15 in women and 20 in men. Reference Wills, Black and Cooper14 Thus, the association between birth weight, childhood obesity, and OA is still ambiguous.

On the other hand, the above controversial evidence may be since observational studies are likely to be affected by uncontrollable factors and reverse causality. Mendelian randomization (MR) provides a way to determine if the observed correlation between a risk factor and an outcome is actually indicative of a causal relationship. It utilizes genetic variations as instrumental variables (IVs) and takes advantage of genetic variants randomly, independently, and uniformly distributed during meiosis. Reference Emdin, Khera and Kathiresan15 Three assumptions of MR must be met in order to obtain impartial results: (a) genetic IVs should be closely associated with exposure; (b) genetic IVs are not affected by any confounding factors related to the chosen exposure and outcome; and (c) genetic IVs affect outcome only through exposure and not through any other biological pathways. Reference Emdin, Khera and Kathiresan15 Since the determination of genotype occurs at conception and before the onset of medically relevant trait or disease, this method largely avoids unmeasured confounding and reverse causality. Reference Davey Smith and Hemani16

The purpose of our study is to investigate the potential links between birth weight, childhood obesity, and the development of OA in adulthood using both univariable MR and multivariable MR (MVMR) methods. In addition, we sought to elucidate the origin of the association between birth weight and adult OA by examining the potential maternal and/or fetal effects on birth weight. A two-sample MR framework was used to disentangle the causality.

Material and methods

Study design

The design of two-sample MR study is overviewed in Figure 1. In the MR study, IVs are determined based on the following three core assumptions. Reference Davies, Holmes and Davey Smith17 First, genetic IVs are highly correlated with exposure. Second, genetic IVs have no shared confounding factors with outcome (e.g., adulthood BMI, waist-to-hip ratio, and height). Finally, genetic IVs cannot be directly involved in outcome except through the exposure pathway. We further performed MR analysis using summary statistic datasets from large-scale genome-wide association studies (GWASs) of birth weight, childhood obesity, and OA.

Figure 1. The design of two-sample MR study. The solid lines are significant; dashed lines should not exist based on MR assumptions. SNP: single nucleotide polymorphism; IVW, inverse-variance-weighted; WM, weighted median; MR-PRESSO, Mendelian randomization pleiotropy residual sum and outlier.

Data sources

Summary association data of birth weight-related single nucleotide polymorphisms (SNPs) were publicly available from a recent GWAS of birth weight contributed by the Early Growth Genetics (EGG) Consortium. Reference Warrington, Beaumont and Horikoshi18 The effects of each SNP on own (n = 298,142) and offspring (n = 210,267) birth weights were analyzed after adjusting for covariates (e.g., gestational age) in the GWAS. Besides, it used structural equation modeling to classify the genetic effects as maternal (n = 264,498) or fetal (n = 179,360) effects. Notably, the maternal effects adjusted for offspring genotype-specific effects and were therefore independent of offspring, representing the effects of intrauterine environment. The fetal effects were independent of maternal, representing the own inherited effect after adjustment of maternal genotype-specific effects. This partition approach thus facilitates the differentiation between the direct fetal effects and the indirect maternal effects of SNPs on birth weight, which is measured in grams as the weight of a newborn. We obtained SNPs associated with childhood obesity from another GWAS on EGG Consortium participants of European ancestry (n = 24,160). Reference Bradfield, Vogelezang and Felix19 EGG defined childhood obesity as having a BMI equal to or exceeding the 95th percentile for individuals aged 2–18 years old.

We extracted summary statistics of OA and its phenotypes from the Genetics of Osteoarthritis (GO) Consortium, including a total of 826,690 (177,517 cases and 649,173 controls) participants of mainly European ancestry. Reference Boer, Hatzikotoulas and Southam20 The GWAS defined patients with OA who met criteria such as self-reported status, the hospital diagnosed, ICD10 codes, or radiography defined by the TREAT-OA consortium.

Detailed information on the study population can be found in Supplementary Table S1. As the present study involved only a secondary analysis of existing published data, ethical approval was not required.

SNP selection

We selected 209 SNPs associated with birth weight at genome-wide significance (p < 6.6 × 10−9), as reported by GWAS, to serve as IVs for our analysis. The association effect sizes for each SNP were divided into uncorrected, corrected fetal- and maternal-independent effect estimates. To assess the influence of inherited and environmental factors on the association between birth weight and OA, we conducted MR analyses of the three distinct effect sizes. We identified 19 SNPs that showed significant associations with childhood obesity (p < 5 × 10−8) in the GWAS analysis.

We searched all of the obtained SNPs in the GWAS catalog (https://www.ebi.ac.uk/gwas) and removed those associated with confounding factors or outcome at high significance (p < 1 × 10−5). Thus, potential horizontal pleiotropy that violated assumptions 2 and 3 of the MR method was avoided. Meanwhile, we performed linkage disequilibrium (LD) tests for these SNPs. The parameters (kb = 10,000 and r 2 = 0.001) were set to select independent SNPs. Next, we matched the SNPs in the summary statistic datasets of SNP–outcome (OA) association estimates and removed SNPs that were not obtained in the OA GWAS. Furthermore, to guarantee the strength of IVs, R 2 and the F-statistics were calculated. Characteristics of instrument SNPs for birth weight and childhood obesity were summarized in Supplementary Table S2-S3.

MR analysis

To investigate the causal impact of genetically predicted exposure on outcome, we primarily employed the inverse-variance-weighted (IVW) method for our analysis. Reference Hemani, Zheng and Elsworth21 In addition, we employed the weighted median (WM) method for additional MR analysis. Reference Burgess, Bowden, Fall, Ingelsson and Thompson22 IVW estimates assume that all genetic variants are valid IVs, while WM estimates can provide consistent estimates of causality when up to 50% of the weight is attributed to valid IVs. Therefore, the WM estimator has lower type 1 error rates than the IVW method, especially when directional pleiotropy exists and InSIDE (instrument strength independent of direct effect) assumption is not satisfied. Reference Bowden, Davey Smith, Haycock and Burgess23

The MR-Egger regression and MR-PRESSO method were conducted as sensitivity analyses to guarantee the robustness of results. Among them, MR-Egger method may give a reliable estimate of causal effects, though no genetic variants are valid IVs. Reference Bowden, Davey Smith and Burgess24 And it could robustly detect the presence of pleiotropy. MR-PRESSO is a method that can be employed to identify and correct outliers in IVW linear regression. Reference Verbanck, Chen, Neale and Do25 Heterogeneity was detected by Cochran’s Q test (P < 0.05 suggesting heterogeneity). Additionally, to investigate the impact of potential outlying and pleiotropic SNPs, we performed a “leave-one-out analysis” by systematically removing each SNP from the analysis in turn. We calculated statistical power for a type 1 error of 5% using an online tool (http://cnsgenomics.com/shiny/mRnd/). The power estimates for the MR were showed in Supplementary Table S4.

What’s more, we performed a two-sample MVMR analysis to investigate the independent effects of correlated exposures. We extracted SNPs which were genome-wide significant in either the EGG GWAS of childhood obesity or the Genetic Investigation of ANthropometric Traits GWAS of adulthood BMI. Reference Yengo, Sidorenko and Kemper26 After LD test, 498 SNPs with r 2<0.001 were used in the analysis. Both the IVW and MR-Egger method were conducted to ascertain the independent effects in MVMR analysis.

All of the effect estimates of exposure on OA outcome were reported by odds ratios (OR). Notably, the OR of birth weight was in terms of per standard deviation (SD) increasing in birth weight, where the SD of birth weight was 539 g. Univariable MR analyses were performed using “TwoSampleMR” and “MR-PRESSO” packages with R software, Reference Verbanck, Chen, Neale and Do25,Reference Yavorska and Burgess27 and MVMR analyses were performed using “MVMR” and “Mendelian Randomization” packages with R software. Reference Yavorska and Burgess27Reference Burgess and Thompson29 P value was corrected by Bonferroni based upon the number of tests performed in all analyses. The statistical analyses had statistically significant evidence at P-values < 0.004 (0.05/14) and had marginal significance at P-values between 0.004 and 0.05.

Results

Causal effect of birth weight on OA and its phenotypes

We excluded 35 SNPs associated with confounding factors or outcome and 75 SNPs with LD through GWAS catalog search and LD test. Lastly, 99 SNPs were selected in the MR analysis. We find no evidence for the causal association of birth weight with OA and its phenotypes as shown in Table 1. Using the IVW method, genetically predicted 1-SD increase in birth weight was not found to be associated with total OA [1.01, 95% confidence interval (CI) = 0.94, 1.07, P = 0.834] or other site-specific OA. Other MR estimates provided consistent findings. Substantial heterogeneity was indicated by Cochran’s Q test except for spine OA. The MR-Egger method did not find any evidence of directional pleiotropy.

Table 1. MR results of the causal association between birth weight and OA

MR, Mendelian randomization; OA, osteoarthritis; SNPs, single nucleotide polymorphisms; OR, odds ratio; CI, confidence interval; IVW, inverse-variance-weighted; WM, weighted median; MR-PRESSO, MR-pleiotropy residual sum and outlier.

a Bolded P represents heterogeneity.

The absence of a causality between birth weight and OA was likely due to the diverse effects of fetal and maternal genomes in the direction and size. Therefore, we further used genetic data on fetal- or maternal-independent effects of birth weight for validation. Finally, 104 and 97 LD-independent SNPs were taken as IVs for fetal and maternal effect of birth weight, respectively. Note that, after matching the SNPs of maternal effect in the spine and thumb OA GWAS, the number of final IVs used in the MR analysis was different (Supplementary Table S5). The IVW results did not show a causal impact of fetal effect of birth weight on total OA (OR = 1.01, 95% CI = 0.95, 1.08, P = 0.728) or other site-specific OA (Supplementary Table S6). In addition, the maternal effect of birth weight was not found to have causal effect on the risk of total OA (OR = 0.97, 95% CI = 0.90, 1.05, P = 0.501) or other site-specific OA using the IVW method (Supplementary Table S7). Other MR estimates provided consistent findings.

Causal effect of childhood obesity on OA and its phenotypes

For childhood obesity traits, 19 SNPs were taken as genetic variants, of which 9 SNPs were excluded due to association with confounders and 6 SNPs were ruled out due to LD. Lastly, a total of 4 SNPs were taken as IVs for childhood obesity. As shown in the Table 2, childhood obesity had marginally causal association with total OA (IVW OR = 1.07, 95% CI = 1.00, 1.15, P = 0.036). Childhood obesity was also marginally associated with hip OA (IVW OR = 1.13, 95% CI = 1.04, 1.24, P = 0.005) and spine OA (IVW OR = 1.12, 95% CI = 1.03, 1.22, P = 0.008) and was suggestively associated with knee OA (WM OR = 1.13, 95% CI = 1.05, 1.22, P = 8E-04). However, we discovered that childhood obesity had no causal effect on hand, thumb, and finger OA. Heterogeneity was only detected for total, knee, and thumb OA by Cochran’s Q test. The MR-Egger method found no evidence of directional pleiotropy. The results of funnel plots and “leave-one-out analysis” demonstrated that no single SNP has a significant effect on the pooled results, verifying the stability of our results in Supplementary Fig. S1-S7.

Table 2. MR results of the causal association between childhood obesity and OA

MR, Mendelian randomization; OA, osteoarthritis; SNPs, single nucleotide polymorphisms; OR, odds ratio; CI, confidence interval; IVW, inverse-variance-weighted; WM, weighted median; MR-PRESSO, MR-pleiotropy residual sum and outlier.

a Bolded P value represents statistical significance.

b Bolded P represents heterogeneity.

Multivariable MR analyses

The MVMR analysis indicated that after controlling for adulthood BMI, the causal effect of childhood obesity on total (IVW OR = 0.99, 95% CI = 0.97, 1.02, P = 0.612) and knee (IVW OR = 1.00, 95% CI = 0.96, 1.03, P = 0.859) OA was not statistically significant (Table 3). The childhood obesity-hip OA (OR = 1.06, 95% CI = 1.01, 1.11, P = 0.025) and -spine OA (OR = 1.06, 95% CI = 1.00, 1.11, P = 0.044) associations were marginally significant using MR-Egger method, but attenuated completely using IVW method. The results on hand, thumb, and finger OA were consistent in the adjusted model.

Table 3. Multivariable MR associations of childhood obesity with OA adjusted for adulthood BMI

MR, Mendelian randomization; OA, osteoarthritis; BMI, body mass index; OR, odds ratio; CI, confidence interval; IVW, inverse-variance-weighted.

a Bolded P value represents statistical significance.

Discussion

To the best of our knowledge, this is the first two-sample MR analysis of the association between birth weight, childhood obesity, and OA risk in adulthood by using large genetic datasets. The MR results supported the association between childhood obesity and total, knee, hip, and spine OA, but not hand, thumb, and finger OA. It is worth noting that the causal effect of childhood obesity on OA was weakened after adjusting for adult BMI. Besides, we observed no evidence for the association between birth weight and OA. Indeed, when distinguish fetal- or maternal-independent effects of birth weight in additional analysis, we also observed a null association.

Previous observational results on the association between birth weight with total as well as site-specific OA remain inconclusive. Sultana et al. conducted a retrospective cohort study in 3,604 participants from Australian Diabetes, Obesity and Lifestyle Study and found that low birth weight was associated with a multivariable-adjusted HR of 2.04 for increased incidence of hip arthroplasty when compared to those with normal birth weight. Reference Hussain, Wang and Wluka9 Several other cohort studies found that low birth weight was associated with the development of OA in men, but not in women. Reference Antoniades, MacGregor, Andrew and Spector13,Reference Jordan, Syddall, Dennison, Cooper and Arden30 On the contrary, the results from the Hertfordshire Cohort Study indicated that lower birth weight was not associated with increased risk of clinical knee, hip, and hand OA. Reference Clynes, Parsons and Edwards31 Indeed, these studies may suggest the fetal origins hypothesis, which indicate the development of adult OA may due to early life factors, such as vitamin D receptor gene. Reference Jordan, Syddall, Dennison, Cooper and Arden30 In our MR study, we found no evidence of a causal association between birth weight and OA using both the IVW and WM methods. MR Egger’s result did not present any bias by directional pleiotropy. In contrast to previous MR study, Reference Zengini, Hatzikotoulas and Tachmazidou32 our study further distinguished fetal or maternal factors of effects on birth weight by taking advantage of the recent GWAS. By analyzing the fetal- or maternal-independent effects of birth weight, we found no association between birth weight and OA, suggesting that factors related to fetal development and intrauterine exposure are unlikely to confound the observed relationship.

Our findings of a positive relationship between childhood obesity and OA are consistent with the results of observational studies. Widhalm et al. found higher knee OA risk in morbidly obese children compared to controls. Reference Widhalm, Seemann and Hamboeck33 A cohort study by Andrew et al. showed that increased BMI in childhood was associated with a higher risk of knee OA. Reference Wills, Black and Cooper14 Other studies reported that obese children were at increased risk of many predisposing traits of OA, such as slipped capital femoral epiphysis, idiopathic genu valgum, and so on. Reference Wabitsch, Horn and Esch34,Reference Walker, Hosseinzadeh and White35 However, findings from a longitudinal study indicated that childhood obesity had no effect on the risk of hand OA. Reference Sayer, Poole and Cox36 The association between obesity and specific OA phenotype is well established. Higher force transmission on weight-bearing joints activates chondrocytes and advances cartilage degeneration. Reference Sokolove and Lepus37 Some adipokines secreted by adipose tissue and some joint cells have proinflammatory and prodegenerative effects on OA, including hand OA. Reference Malemud38,Reference Berenbaum, Eymard and Houard39 Previous MR study had found that increased BMI in childhood and adulthood was all associated with a higher risk of OA at weight-bearing joints. Reference Funck-Brentano, Nethander, Movérare-Skrtic, Richette and Ohlsson40,Reference Cao, Wu, Li, Li and Wu41 Therefore, the present study performed a multivariable analysis to investigated the robustness of the relationship of childhood obesity with OA after adjusting for adulthood BMI. The causal effect of childhood obesity on hip and spine OA was attenuated and marginally significant and can be explained by a more general causal effect of adulthood obesity on OA. The findings of the study reveal that obesity contributes to OA at weight-bearing joints through a separate pathway different from that of fetal origins.

There are several limitations in our study. First, the number of SNPs for childhood obesity included in the study is relatively small. Thus, a GWAS with a greater number of SNP is required to replicate MR study to strengthen power of estimate causal effect. Second, the study only involves in participants of European descent, so it is unknown whether our findings can be transferable to non-European populations. Third, constrained by summary data, we are unable to stratify the causality between birth weight and childhood obesity and OA by sex or weight. Furthermore, we are unable to know whether the null results of the MR analysis are due to misclassification of OA participants at baseline. This limitation may lead to our underestimation of cases of hand OA. Finally, the sources of three samples have overlapping, so we mostly used powerful tools (i.e., the F-statistic > 10) to minimize its bias. Reference Hemani, Zheng and Elsworth21

It was worth noting that the study had some strengths. First, this is the first MR analysis to investigate the causal association between birth weight, childhood obesity and OA at the same time. The MR study further confirmed neither indirect maternal effects nor direct fetal effect have indirect long-term effects on the risk of OA. Besides, we included seven specific OA phenotypes obtained from the largest GWAS, enhancing the comprehensiveness of our analysis. By utilizing IVs extracted from the latest GWAS data for birth weight and childhood obesity, we ensure the relevance and accuracy of our findings. The large sample size employed in our study adds to the reliability and generalizability of our results. What’s more, the statistical power for the causality between childhood obesity and total OA and OA at weight-bearing joints is highly enough, which improve the reliability of the results. Finally, we are more able to remove the bias due to adult BMI by using MVMR than using univariable MR.

Conclusion

Our study provided support for a suggestive association between genetically predicted childhood obesity and OA at weight-bearing joints. However, we did not find a significant association between childhood obesity and hand OA. Although evidence for the association between birth weight and OA is lacking, it is important to note that birth weight is considered a significant risk factor for the development of OA, mainly due to its impact on various other diseases.

Supplementary material

The supplementary material for this article can be found at https://doi.org/10.1017/S2040174424000114.

Data availability statement

All data included in this study is commercially available.

Acknowledgments

None.

Author contribution

Zengfeng Xin and Lingxiao Xu contributed equally to this work.

All authors participated in the study. LS and LX contributed to the conception or design of the work. ZX and LS contributed to the acquisition of data. ZX and LX contributed to the analysis and interpretation of data and the preparation of the manuscript. All authors read and approved the final manuscript.

Financial support

This work was supported by National Natural Science Foundation of China, Grant Number 81702118.

Competing interests

None.

Footnotes

Zengfeng Xin and Lingxiao Xu contributed equally to this work and co-first authors.

References

Peat, G, Thomas, MJ. Osteoarthritis year in review 2020: epidemiology & therapy. Osteoarthr Cartilage. 2021; 29(2), 180189.CrossRefGoogle ScholarPubMed
World HO. World Heath Organization. 2021; Available from: https://www.who.int/news-room/fact-sheets/detail/obesity-and-overweight. Accessed June 3, 2023.Google Scholar
Litwic, A, Edwards, MH, Dennison, EM, Cooper, C. Epidemiology and burden of osteoarthritis. Brit Med Bull. 2013; 105(1), 185199.CrossRefGoogle ScholarPubMed
Reyes, C, Leyland, KM, Peat, G, Cooper, C, Arden, NK, Prieto-Alhambra, D. Association Between Overweight and Obesity and Risk of Clinically Diagnosed Knee, Hip, and hand osteoarthritis: a population-based cohort study. Arthritis Rheumatol. 2016; 68(8), 18691875.CrossRefGoogle ScholarPubMed
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 Cartilage. 2010; 18(1), 2433.CrossRefGoogle ScholarPubMed
Antony, B, Jones, G, Venn, A, et al. Association between childhood overweight measures and adulthood knee pain, stiffness and dysfunction: a 25-year cohort study. Ann Rheum Dis. 2015; 74(4), 711717.CrossRefGoogle ScholarPubMed
Molina-Garcia, P, Migueles, JH, Cadenas-Sanchez, C, et al. A systematic review on biomechanical characteristics of walking in children and adolescents with overweight/obesity:Possible implications for the development of musculoskeletal disorders. Obes Rev. 2019; 20(7), 10331044.CrossRefGoogle ScholarPubMed
Poole, J, Sayer, AA, Cox, V, et al. Birth weight, osteoarthritis of the hand, and cardiovascular disease in men. Ann Rheum Dis. 2003; 62(10), 10291029.CrossRefGoogle ScholarPubMed
Hussain, SM, Wang, Y, Wluka, AE, et al. Association of low birth weight and preterm birth with the incidence of knee and hip arthroplasty for osteoarthritis. Arthrit Care Res. 2015; 67(4), 502508.CrossRefGoogle ScholarPubMed
Hussain, SM, Ackerman, IN, Wang, Y, Zomer, E, Cicuttini, FM. Could low birth weight and preterm birth be associated with significant burden of hip osteoarthritis? A systematic review. Arthritis Res Ther. 2018; 20(1), 121.CrossRefGoogle ScholarPubMed
Barker, DJ. The fetal and infant origins of adult disease. BMJ (Clinical research ed). 1990; 301(6761), 1111.CrossRefGoogle ScholarPubMed
Lucas, A, Fewtrell, MS, Cole, TJ. Fetal origins of adult disease-the hypothesis revisited. BMJ (Clinical research ed). 1999; 319(7204), 245249.CrossRefGoogle ScholarPubMed
Antoniades, L, MacGregor, AJ, Andrew, T, Spector, TD. Association of birth weight with osteoporosis and osteoarthritis in adult twins. Rheumatology (Oxford, England). 2003; 42(6), 791796.CrossRefGoogle ScholarPubMed
Wills, AK, Black, S, Cooper, R, et al. Life course body mass index and risk of knee osteoarthritis at the age of 53 years: evidence from the 1946 British birth cohort study. Ann Rheum Dis. 2012; 71(5), 655660.CrossRefGoogle ScholarPubMed
Emdin, CA, Khera, AV, Kathiresan, S. Mendelian randomization. JAMA. 2017; 318(19), 19251926.CrossRefGoogle ScholarPubMed
Davey Smith, G, Hemani, G. Mendelian randomization: genetic anchors for causal inference in epidemiological studies. Hum Mol Genet. 2014; 23(1), R8998.CrossRefGoogle ScholarPubMed
Davies, NM, Holmes, MV, Davey Smith, G. Reading Mendelian randomisation studies: a guide, glossary, and checklist for clinicians. BMJ. 2018;362:k601.CrossRefGoogle ScholarPubMed
Warrington, NM, Beaumont, RN, Horikoshi, M, et al. Maternal and fetal genetic effects on birth weight and their relevance to cardio-metabolic risk factors. Nat Genet. 2019; 51(5), 804814.CrossRefGoogle ScholarPubMed
Bradfield, JP, Vogelezang, S, Felix, JF, et al. A trans-ancestral meta-analysis of genome-wide association studies reveals loci associated with childhood obesity. Hum Mol Genet. 2019; 28(19), 33273338.CrossRefGoogle ScholarPubMed
Boer, CG, Hatzikotoulas, K, Southam, L, et al. Deciphering osteoarthritis genetics across 826,690 individuals from 9 populations. Cell. 2021; 184(18), 47844818.e17.CrossRefGoogle ScholarPubMed
Hemani, G, Zheng, J, Elsworth, B, et al. The MR-base platform supports systematic causal inference across the human phenome. eLife. 2018; 7, 34408.CrossRefGoogle ScholarPubMed
Burgess, S, Bowden, J, Fall, T, Ingelsson, E, Thompson, SG. Sensitivity analyses for robust Causal inference from Mendelian randomization analyses with multiple genetic variants. Epidemiology (Cambridge, Mass). 2017; 28(1), 3042.CrossRefGoogle ScholarPubMed
Bowden, J, Davey Smith, G, Haycock, PC, Burgess, S. Consistent estimation in Mendelian randomization with some invalid instruments using a weighted median estimator. Genet Epidemiol. 2016; 40(4), 304314.CrossRefGoogle ScholarPubMed
Bowden, J, Davey Smith, G, Burgess, S. Mendelian randomization with invalid instruments: effect estimation and bias detection through Egger regression. Int J Epidemiol. 2015; 44(2), 512525.CrossRefGoogle ScholarPubMed
Verbanck, M, Chen, CY, Neale, B, Do, R. Detection of widespread horizontal pleiotropy in causal relationships inferred from Mendelian randomization between complex traits and diseases. Nat Genet. 2018; 50(5), 693698.CrossRefGoogle ScholarPubMed
Yengo, L, Sidorenko, J, Kemper, KE, et al. Meta-analysis of genome-wide association studies for height and body mass index in ∼700000 individuals of European ancestry. Hum Mol Genet. 2018; 27(20), 36413649.CrossRefGoogle ScholarPubMed
Yavorska, OO, Burgess, S. MendelianRandomization: an R package for performing Mendelian randomization analyses using summarized data. Int J Epidemiol. 2017; 46(6), 17341739.CrossRefGoogle Scholar
Rees, JMB, Wood, AM, Burgess, S. Extending the MR-Egger method for multivariable Mendelian randomization to correct for both measured and unmeasured pleiotropy. Stat Med. 2017; 36(29), 47054718.CrossRefGoogle ScholarPubMed
Burgess, S, Thompson, SG. Multivariable Mendelian randomization: the use of pleiotropic genetic variants to estimate causal effects. Am J Epidemiol. 2015; 181(4), 251260.CrossRefGoogle ScholarPubMed
Jordan, KM, Syddall, H, Dennison, EM, Cooper, C, Arden, NK. Birthweight, vitamin D receptor gene polymorphism, and risk of lumbar spine osteoarthritis. The Journal of rheumatology. 2005; 32(4), 678683.Google ScholarPubMed
Clynes, MA, Parsons, C, Edwards, MH, et al. Further evidence of the developmental origins of osteoarthritis: results from the hertfordshire cohort study. J Dev Orig Hlth Dis. 2014; 5(6), 453458.CrossRefGoogle ScholarPubMed
Zengini, E, Hatzikotoulas, K, Tachmazidou, I, et al. Genome-wide analyses using UK biobank data provide insights into the genetic architecture of osteoarthritis. Nat Genet. 2018; 50(4), 549558.CrossRefGoogle ScholarPubMed
Widhalm, HK, Seemann, R, Hamboeck, M, et al. Osteoarthritis in morbidly obese children and adolescents, an age-matched controlled study. Knee Surg Sports Traumatol Arthrosc. 2016; 24(3), 644652.CrossRefGoogle ScholarPubMed
Wabitsch, M, Horn, M, Esch, U, et al. Silent slipped capital femoral epiphysis in overweight and obese children and adolescents. Eur J Pediatr. 2012; 171(10), 14611465.CrossRefGoogle ScholarPubMed
Walker, JL, Hosseinzadeh, P, White, H, et al. Idiopathic Genu Valgum and its association with obesity in children and adolescents. J Pediatr Orthoped. 2019; 39(7), 347352.CrossRefGoogle ScholarPubMed
Sayer, AA, Poole, J, Cox, V, et al. Weight from birth to 53 years: a longitudinal study of the influence on clinical hand osteoarthritis. Arthritis Rheum. 2003; 48(4), 10301033.CrossRefGoogle Scholar
Sokolove, J, Lepus, CM. Role of inflammation in the pathogenesis of osteoarthritis: latest findings and interpretations. Ther Adv Musculoskel Dis. 2013; 5(2), 7794.CrossRefGoogle Scholar
Malemud, CJ. Biologic basis of osteoarthritis: state of the evidence. Curr Opin Rheumatol. 2015; 27(3), 289294.CrossRefGoogle ScholarPubMed
Berenbaum, F, Eymard, F, Houard, X. Osteoarthritis, inflammation and obesity. Curr Opin Rheumatol. 2013; 25(1), 114118.CrossRefGoogle ScholarPubMed
Funck-Brentano, T, Nethander, M, Movérare-Skrtic, S, Richette, P, Ohlsson, C. Causal factors for knee, hip, and hand osteoarthritis: a mendelian randomization study in the UK biobank. Arthritis Rheumatol. 2019; 71(10), 16341641.CrossRefGoogle ScholarPubMed
Cao, Z, Wu, Y, Li, Q, Li, Y, Wu, J. A causal relationship between childhood obesity and risk of osteoarthritis: results from a two-sample Mendelian randomization analysis. Ann Med. 2022; 54(1), 16361645.CrossRefGoogle ScholarPubMed
Figure 0

Figure 1. The design of two-sample MR study. The solid lines are significant; dashed lines should not exist based on MR assumptions. SNP: single nucleotide polymorphism; IVW, inverse-variance-weighted; WM, weighted median; MR-PRESSO, Mendelian randomization pleiotropy residual sum and outlier.

Figure 1

Table 1. MR results of the causal association between birth weight and OA

Figure 2

Table 2. MR results of the causal association between childhood obesity and OA

Figure 3

Table 3. Multivariable MR associations of childhood obesity with OA adjusted for adulthood BMI

Supplementary material: File

Xin et al. supplementary material

Xin et al. supplementary material
Download Xin et al. supplementary material(File)
File 121.2 KB