Trabecular bone scores in young HIV-infected men: a matched case-control study

Advances in antiretroviral therapy (ART) have improved life expectancy dramatically among people living with HIV. However, this improvement gives to rise to concerns about non-AIDS-related comorbidities that may be related to ART and age, such as cardiovascular, renal, metabolic, and bone disease. A meta-analysis showed that the prevalence of osteopenia or osteoporosis is higher in HIV-infected patients than in controls [1]. The pathogenesis of bone loss in HIV-infected individuals is a complex and multifactorial process, with HIV itself, the use of antiretroviral agents, hypogonadism in men, menopause in women, low body mass index (BMI), aging, malnutrition, steroid use, and smoking all associated with bone disease [2]. Hormonal changes in postmenopausal women or in elderly people are associated changes in the bone remodeling cycle, which leads to bone fragility and an increased risk of bone fracture [3, 4].

Bone mineral density (BMD) is determined by the peak bone mass and amount of bone loss and is the standard measure used for the diagnosis of osteoporosis. BMD evaluates bone quantity, rather than bone microarchitecture or composition [5]. Recently, the trabecular bone score (TBS) has been introduced as a novel tool for assessing bone microarchitecture. TBS values are obtained from dual-energy X-ray absorptiometry (DXA) scans of the lumbar spine using a proprietary software program; TBS is a noninvasive, indirect measurement calculated from the projection of the three-dimensional bone structure onto a two-dimensional plane [6]. TBS has been validated as a good prognostic tool for assessing trabecular microstructure independent of BMD and has been reported to increase the accuracy of fracture prediction in patients with BMD above the osteoporotic threshold [7, 8]. However, few studies have evaluated TBS in HIV-infected individuals, especially young male patients. We calculated TBS values from DXA images of the lumbar spine taken from HIV-infected male patients under 50 years of age. The etiology of osteoporosis in HIV-infected patients is multifactorial; therefore this descriptive study included only male HIV infected patients aged less than 50 years to minimize the influence of traditional risk factors associated with low BMD, such as age and postmenopausal status in women. We compared TBS values obtained from HIV-infected young male patients with those from matched healthy controls and investigated the associations between TBS and demographic parameters, clinical parameters, and BMD scores for the lumbar spine and femoral neck.

In this cross-sectional study, TBS values were significantly lower in HIV-infected young male patients than in age- and sex-matched controls. Furthermore, TBS values were positively correlated with BMD at the lumbar spine, femoral neck, and total hip and negatively correlated with the duration of TDF exposure.

The difference in TBS values between individuals with and without HIV is consistent with prior results from the Women’s Interagency HIV Study [14]. It is well known that age, postmenopausal status, smoking, and low BMI are risk factors for osteoporosis in the general population, and that HIV-related factors such as the direct action of the virus, chronic immune activation, and antiviral toxicity can also affect bone structure [2, 12, 15, 16]. A strength of the present study is that we included only HIV-infected male patients aged between 18 and 50 years to minimize the effects of the general risk factors.

TDF, an acyclic nucleotide analog of adenosine monophosphate, is widely used as a core component of many ART regimens, and several longitudinal studies have reported an association between TDF treatment and significantly reduced BMD [17, 18]. Thus, long-term use of TDF may lead to clinically relevant changes in BMD. One study reported a significant decrease in BMD and TBS after 1 year of TDF therapy [19]. We found that TBS, a measure of bone microarchitecture, was negatively correlated with TDF exposure, suggesting that TDF can affect not only the quantity of bone, but also its microarchitecture. We did not analyze the factors associated with low TBS because of the small number of patients with low TBS values; however, creatinine levels differed between the low-TBS and normal-TBS patient groups. Although the mechanism by which TDF causes bone toxicity is still unclear, TDF has both direct and indirect effects on bone via renal and endocrine systems [18, 20]. Subclinical tubulopathy may be a key factor in TDF-driven reductions in BMD, and our results support the hypothesis that renal function may affect bone microarchitecture in HIV-infected patients. This study also shows that TBS was marginally negatively correlated with the duration of HIV diagnosis, and uncorrelated with serum markers of bone turnover. CTX levels were slightly lower in the low-TBS patient group. HIV infection decreases bone formation and increases bone loss through direct effects related to the virus as well as through indirect effects related to pro-inflammatory cytokines, resulting in an increase in bone resorption and loss. However, the pathophysiology of bone fragility with HIV infection remains incompletely understood [2, 21]. Our results support the hypothesis that virus-associated factors, in addition to a patient’s clinical risk factors, contribute to bone turnover in young HIV-infected male patients despite suppression of the virus by ART. Animal experiments have shown that low BMI leads to osteoclast activation through enhanced production of the receptor activator of nuclear factor kappa-B (RANK) ligand by B-cells, accompanied by downregulation of the antagonist osteoprotegerin [22]. In the present study, the HIV-infected patients had lower BMI scores than the control subjects, which may have affected the bone. Further studies with larger patient groups are warranted to assess the risk factors and bone turnover markers associated with low TBS.

This study found that 21.3% of young male HIV-infected patients had a low BMD for their age (Z-score ≤ − 2.0). Currently, screening for osteoporosis with DXA is recommended in male HIV patients aged ≥50 years [12, 23]. A previous meta-analysis found that 67% of 884 HIV-infected patients had reduced BMD, of whom 15% had osteoporosis, yielding pooled odds ratios of 6.4 and 3.7, respectively, compared with non-HIV-infected controls [24], similar to our results for HIV-infected men aged 50 years and younger. Therefore, our results question the current guidelines for DXA screening in young HIV-infected men, although further studies will be needed to confirm our results. In this study, 7.5% of young HIV-infected men were deemed at high risk of fracture according to the TBS value, although a similar percentage was found for the control group. TBS, a texture index derived from DXA of the lumbar spine, is a widely available and endorsed technique and is included in the World Health Organization (WHO) Fracture Risk Assessment Tool [25, 26]. The correlation coefficient between TBS and BMD varies depending on the study. Some studies have shown that TBS correlates with lumbar BMD; however other studies reported that TBS correlates poorly with BMD [8, 27, 28]. This may be due to the diversity in the underlying diseases and differences in the demographic characteristics of the participants. Studies on the role of TBS as a complement to BMD and as a means of identifying cut-off values to predict fracture risk in HIV-infected populations are limited. Thus, additional studies are warranted to clarify the role that TBS may play in this patient population.

In this study, BMD values of the lumbar spine were not statistically significant between the two groups, although BMD results in HIV-infected patients were lower than in controls. A meta-analysis showed that the prevalence of osteopenia/osteoporosis of the lumbar spine [OR = 2.4 (95% Cl: 2.0–2.8)] and hip [OR = 2.6 (95%Cl: 2.2–3.0)] was significantly higher in HIV-infected groups than in controls [1]. This is probably due to sampling bias or the small number of patients. The pathogenesis of bone loss in HIV-infected patients is a complex and has not been established. Therefore, there exists a possibility that unknown processes are involved in bone turnover in HIV-infected patients.

This study has several limitations. First, laboratory markers related to bone metabolism, such as vitamin D and osteocalcin, were not examined in the control group so we could not compare these parameters between the two groups. Second, we did not obtain long-term follow-up TBS data, and were therefore unable to assess the extent to which TBS predicts fractures. Third, sampling bias could have occurred in the HIV-infected patients group and the control group.

We have presented a cross-sectional study of HIV-infected men aged 50 years and younger, and assessed bone microarchitecture via TBS in this patient population. We observed lower TBS and BMD values in HIV-infected young men than in the control group and found that TBS values were positively correlated with BMD at the lumbar spine, femoral neck, and total hip, and negatively correlated with the duration of TDF exposure.