Gout is not associated with the risk of fracture: a meta-analysis

Gout affected 2.4% of adults in the UK [1] and more than eight million Americans [2], which was one of the most common rheumatic diseases [3]. The growing recognition indicated that gout did not just occur in men, but also in women, and caused a substantial disease burden with the significantly higher cost, morbidities, and mortality [4‐8]. Additionally, hyperuricemia, a characteristic in gout, was reported to be an independent risk factor for cardiovascular diseases, diabetes, and even death [9‐12]. In recent decades, concern has mounted regarding the association between gout and bone health. It was generally believed that chronic inflammation had a negative effect on the bones due to the stimulation of the inflammatory cascade and production of pro-inflammatory cytokines, so gout, a type of inflammatory arthritis, has been hypothesized to be associated with a high risk of fractures [13, 14]. However, the increased serum level of uric acid (UA) in gout [15], which is the degradation production of purine compounds [16], made the relationship inconsistent. UA may affect bone health, including resorption and formation, through its two-way control of oxidative stress due to its antioxidant or pro-oxidant properties [17], and several prior studies on the association between hyperuricemia and bone mineral density (BMD) also demonstrated conflicting results [18‐22]. Meanwhile, the urate-lowering therapy faced a dilemma when considering the relationship with fracture. Therefore, the indistinct interaction of these factors made it challenging to determine whether gout was protective or detrimental to bone health.

Numerous quantitatively based studies debating the association between gout and the risk of fractures remain inconclusive. Tzeng et al. [23] reported that gout history increased the fracture risk, which was consistent with the results of a Chinese adult-based research conducted by Wang et al. [24]. However, the relationship became variable when focus on different fracture sites in the study performed by Paik et al. [17], in which the risk of fractures raised in the hip but not in the wrist. Kim et al. [25] conducted a large-scale epidemiological study and demonstrated the neutral association between gout and bone health, and Sultan et al. [1] reported the similar results in a nationally representative cohort research. Additionally, a population-based study in Taiwan demonstrated a lower fracture risk among gout patients prescribed urate-lowering therapy [23], while a 9% higher risk was found in a Denmark registry-based study [26]. Hence, it was difficult to clarify the associations of gout and its related treatment with the risk of fractures based on these published observational studies.

The aim of this study was to assess precisely the risk of fractures among patients with gout and estimate the potential effect of urate-lowering therapy on the risk. Furthermore, several subgroup analyses based on the gender, fracture sites, and etc. were performed to reveal more influencing factors.

The checklist of the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) statement was followed in the conduction of this investigation (Additional file 1). Electronic searches, reference lists screening, study selection, data extraction, assessment of the risk of bias, and pooling of outcome estimates were performed by two investigators (LFX and XF) independently. Any disagreement was resolved by consensus or judgment of an arbitrator (DJL). Informed consent or ethics approval was not needed because all required data were retrieved from published articles.

This meta-analysis aimed to address the fracture risk of patients with gout and demonstrated that gout was not associated with an increased risk of fractures for any site, such as the humerus, wrist, vertebral, and hip fracture. In addition, urate-lowering drugs prescribed early during the course of disease had neither adverse nor beneficial effect on the long-term risk of fractures.

As a typical feature of gout, high UA levels were demonstrated an inconsistent relationship with BMD and fracture, because the diverse properties of UA depend on the specific conditions. The protective effects of UA on BMD are mainly because of the antioxidant function or via vitamin D/parathyroid hormone pathway [29‐31]. The pro-oxidant properties are dominant when UA exists at supersaturated concentrations, such as in gout, and results in oxidative stress [32, 33]. Numerous cross-sectional analyses demonstrated the positive or inverse association between UA and BMD [18‐21]. The more recent one based on the National Health and Nutrition Examination Survey (NHANES) reported the neutral results which were also supported by animal data [22]; however, a prospective Rotterdam Study revealed that a higher UA level led to a higher BMD [34]. In terms of the association between UA and fracture risk, the results also remained inconsistent, which may be partly related to the age and sex distribution in different studies. A prospective Osteoporotic Fractures in Men (MrOS) study recruiting 5994 men aged 65 years or old showed a higher UA level had a negative impact on the risk of non-spine fracture, but not applied in hip fracture [35]. A more recent prospective study included 1963 men and 2729 women and found a significant positive association between high UA level and an increased risk of hip fractures, but only in men [36].

Hyperuricemia is a necessary but not sufficient predisposing factor for gout [23], which is also characterized by uric acid crystals and inflammatory. Importantly, the uric acid crystals can activate the NOD-like receptor protein-3 (NLRP3) [37, 38], which act as a diver of pro-inflammatory cytokines. Additionally, interleukin-1 beta (IL-1β), a strong stimulator of bone resorption, can be produced in the inflammatory cascades during gout [39‐41]. These effects further promote osteoclastogenesis and osteoclast differentiation and may be related to the changes in BMD, thereby potentially increasing fracture risk [42‐46]. Therefore, the complex pathophysiology made the relationship between gout and fracture varied.

Our research based on the analysis of seven studies including 151,002 gout patients and 533,962 participants in the control group revealed that there was no significant association between gout and fracture risk. Three of these articles demonstrated different conclusions from ours. Although Tzeng et al. [23] found that gout increased the overall fracture risks, the absent detailed information regarding important lifestyle-related factors (body mass index, smoking status, and alcohol habit) in the National Health Insurance research database (NHIRD) may confound their conclusions. The large prospective cohort study performed by Paik and colleagues showed that a history of gout modestly increased the risk of hip fracture in women but was not associated with wrist fracture [17]. However, the population in this study was female, so their findings should be carefully generalizable to men, while our subgroup analysis based on gender did not show significant a significant increase in the risk of fractures. Wang et al. [24] demonstrated that, in Chinese adults, gout significantly increased the risk of osteoporotic fractures in women. Because of its cross-sectional design, some biases were inherent, and the causal relationship between gout, fractures, and osteoporosis cannot be established; therefore, the results required cautious interpretation. Notably, a subgroup analysis based on the site of fractures was conducted in our research; the results showed that gout increased the risk of upper limb fractures, but a more detailed location analysis (humerus, wrist, and etc.) made the relationship disappear. Therefore, more prospective studies focusing on different factors should be performed to identify the association between gout and high fracture incidence under specific conditions.

We found that gout-related medication had a neutral effect on the risk of fractures, although previous literature on this topic was conflicting. Dennison et al. [26] reported that 9% excess risk of osteoporotic fractures was associated with gouty arthritis requiring allopurinol; however, the significant differences of characteristics between the exposed group and nonusers, and the control group involving non-gout participants may affect their observation. The opposite conclusion was raised by Tzeng et al. [23], in which urate-lowering therapy decreased a 28% risk of fractures among gout patients, while this study ignored the exclusion of the patients in the exposed group who underwent other events before the first prescription of urate-lowering therapy. A cohort study conducted by Sultan et al. demonstrated that urate-lowering therapy had a neutral effect on the long-term risk of fractures [1]. Although the use of 1- and 3-year landmarks to some extent limited the generalization of the population, the nationally representative data recording enables us to understand better the causal relationship between therapy and fractures with minimum bias.

The strength of this study compared with previous investigations lies in the large quantity of included data, reliable statistical methods, and comprehensive evaluation indexes. This meta-analysis included eight datasets by exhaustive database searching and reference screening, among which there were seven datasets from national or regional register databases. The large participant base made the results of this study well represented. Moreover, outcomes of interests were compared using a pairwise meta-analysis method and analyzed from multi-dimension to fully elucidate the association between gout and the risk of fractures and discuss the underlying mechanism. Findings of this meta-analysis provide the currently most comprehensive evidence about this issue, which will help gout patients and their clinicians to determine whether or not to make an appropriate therapeutic regimen to propose the fracture. Hence, the conclusions based on these articles were not fairly reliable.

Nevertheless, this investigation was not without limitations. First, we only demonstrated an overall effect of gout on fracture but were not able to analyze the influence of some clinical and demographical factors (e.g., age and comorbidities). Second, there were only two prospective studies, and no randomized controlled trials were included. However, given the properties of gout and source of data, large scale RCT is currently inaccessible. Third, several studies did not present all characteristics of participants, and these missing data affect and weaken the strength of conclusions.

This meta-analysis confirmed that gout was not associated with an increased risk of fractures. Urate-lowering drugs prescribed early during the course of disease had neither adverse nor beneficial effect on the long-term risk of fractures.