Latent metabolic bone disease, skeletal dysplasia and other conditions related to low bone formation among 38 patients with subtrochanteric femoral fractures: a retrospective observational study

AtypicalPlease femoral fracture (AFF) is a type of fracture that develops with weak external forces or without trauma in the subtrochanteric area or shaft of the femur [1]. More than three cases per 1000 patient-years of treatment involve AFF in osteoporotic women who have taken antiresorptive agents continuously for more than 8 years. The risk of AFF among antiresorptive agent users with osteoporosis is approximately eightfold greater in Asian women than in Caucasian women [2‐4]. Bisphosphonate use is a historically well-recognized risk factor for AFF, and there are now multiple recent case reports regarding AFF after denosumab in bisphosphonate-naive patients [5‐9]. Glucocorticoids are also a candidate risk factor for AFF in osteoporotic women who take antiresorptives [10, 11]. There are reports of the development of AFF after romosozumab treatment, although it is still unclear whether this treatment is associated with the development of AFF [12]. The incidence of AFF in people who have taken antiresorptive agents for skeletal metastasis for more than 1 year is more than 2%, perhaps because the cumulative annual absorbed dose of an antiresorptive agent in patients with cancer is about ten times greater than the cumulative annual absorbed osteoporosis dose [13‐15].

More than one-third of patients with one AFF eventually develop contralateral AFF. The union of the AFF is often delayed, which places patients in adverse situations and suggests a slow healing response due to antiresorptive-based inhibition of Haversian remodeling, an underlying bone disease, or perhaps even a combination of the two [10, 16].

Several metabolic bone diseases, such as hypophosphatemic osteomalacia, including X-linked hypophosphatemic rickets/osteomalacia (XLH), tumor-induced osteomalacia (TIO), Fanconi syndrome, and vitamin D-dependent rickets (VDDR), and several skeletal dysplasias, including hypophosphatasia (HPP) and osteopetrosis, are recognized to cause fractures that are morphologically identical to the AFF [17‐21]. Several reports indicating that morphologic AFF is sometimes associated with monogenic bone diseases have been reported, and several genes, including ALPL, GGPS1, COL1A2, and CYP1A1, have been identified as disease susceptibility genes by candidate-gene association studies and genome-wide association studies (GWASs) [17‐32].

The updated epidemiology of AFF and the high frequency of bilateral fracture and delayed union in AFF suggest the possible existence of conditions and unidentified bone disorders that are associated with low bone formation, including the disorders mentioned above. Thus far, few studies have explored latent metabolic bone disease and skeletal dysplasia comprehensively in patients with atypical femoral fractures in a single cohort. In the current study, we retrospectively collected and analyzed the clinical characteristics of 38 patients with subtrochanteric fractures to reveal the presence of known risk factors such as bisphosphonate and glucocorticoid use, along with latent bone metabolic disorders and skeletal dysplasia associated with low bone formation.

AFF is a fracture that occurs on the subtrochanteric femur or shaft of the femur with minor external force or without trauma, and the detailed 2nd definition of AFF was introduced by ASBMR in 2013 [1]. A systematic review of 14 studies reported that the incidence of AFF was as low as 3.0 to 9.8 cases per 100,000 person-years [35], although the incidence of AFF in osteoporotic women who are treated with antiresorptive agents continuously for more than 8 years is more than three cases per 1000 patient-years of treatment [3, 4].

Similar to the purpose of our current study, Nguyen et al. [17] conducted a literature review to determine the presence of monogenic disorders among patients with AFF. In this article, 2566 relevant citations were searched, and reports of 23 individuals with seven monogenic bone disorders (osteogenesis imperfecta, pycnodysostosis, HPP, X-linked osteoporosis, osteopetrosis, XLH, and osteoporosis pseudoglioma syndrome) were identified. In eight patients, monogenic disorders were uncovered after the development of morphologic AFF [17]. Similarly, in a literature review by Zhou et al., AFF was reported in 57 patients with monogenic bone diseases; 17.5% of those patients were diagnosed after the development of AFF and 56.1% had no history of antiresorptive treatment [36]. These studies not only point out that both antiresorptive agent and particular metabolic bone diseases/skeletal dysplasia are independently associated with morphologic AFF, but also raise the possibility that when both antiresorptive treatment and monogenetic bone diseases exist simultaneously in the same individual, their effects on AFF may be additive. In one report, 14 of 16 untreated osteoporosis patients with persistently low serum ALP levels had loss-of-function mutations in the ALPL gene [37]. The serum ALP level is a serological marker of overt osteomalacia, especially when it is persistently elevated; therefore, clinicians should consider serum ALP levels to help exclude typical metabolic bone disease/skeletal dysplasia before initiating antiresorptive agents for osteoporotic patients [37, 38]. Based on serum ALP levels, two patients with metabolic bone disease/skeletal dysplasia were identified among four patients in the current cohort. However, in addition to serum ALP levels, detailed clinical examinations such as bone mineral density (BMD), past medical history, and medication history are necessary to thoroughly identify metabolic bone disease/skeletal dysplasia. The current study revealed that four out of 38 of the patients with morphologic AFF were suffering from definite and suspected bone diseases, and, notably, bone diseases were diagnosed or suspected only after the first morphologic AFF in three of them.

In this study, 16 out of 38 patients (42%) had a history of past bisphosphonate treatment. Bisphosphonate use is the most recognized risk factor for the development of AFF and the occurrence of AFF in osteoporotic women who have used antiresorptive drugs for more than 8 years is not uncommon [3, 4]. The development of AFF has also been reported in patients treated with denosumab [5‐9, 39]. Although there is no definite evidence that anticancer drugs increase AFF, it has been reported that cyclophosphamide decreases osteoblasts and osteoclasts in mice, suggesting that particular anticancer drugs may suppress bone turnover in humans [40]. All 38 patients included in the current study were Japanese. Regarding racial differences, it has long been suggested that Asian race is a risk factor for AFF, and recently, Lo et al. reported that Asians were eight times more likely to develop AFF than non-Asians in a cohort in the USA, Nguyen et al. reported that Asians were 3.4 times more likely to develop AFF than non-Asians in a cohort in an Australian hospital, and Dhanekula et al. reported that Asian ethnicity increased the risk of developing AFF by sevenfold in an Australian multicenter cohort [2, 41, 42]. AFF risk is significantly greater in patients over age 65 than in those younger than age 65. In previous reports, the incidence rates were higher in the 65–74 and 75–84 age groups than in the 50–64 age group (2.24, 2.35, and 0.83 per 10,000 person-years, respectively) [11].

Patients younger than 79 years with morphologic AFF are more likely to have any risk factor other than age, such as bone metabolic disorders and skeletal dysplasia, should be excluded, especially when a patient is not treated with antiresorptive agents or glucocorticoids. In contrast, only one of the ten patients who used glucocorticoids had no other risk factors, thereby providing no evidence concerning the relationship between glucocorticoid use alone and AFF. Previously, Takahashi et al. reported that “antiresorptive treatment (> 3.5 years)” and “prior zoledronic acid treatment” were risk factors for developing AFF among bone metastatic patients with antiresorptive treatment [13]. The two denosumab cases with antiresorptive treatment in the current study suffered from breast cancer, and the durations of treatment (5 and 2 years) were shorter compared to the previous report (Supplementary Table 1).

Antiresorptive agents increase BMD by inhibiting bone resorption; nevertheless, long-term use increases the risk of AFF. It has been proposed that in the bones of antiresorptive agent users who develop AFF, the natural mechanism of dissipating energy and slowing crack propagation is impaired [43]. The main cause of AFF could be that microdamage in the lateral femoral cortex of the subtrochanteric region is not repaired in a timely fashion, due to the suppression of cortical bone remodeling by antiresorptive agents or the low rate of cortical bone remodeling in patients with metabolic bone diseases/skeletal dysplasia. Although the characteristic lateral periosteal callus forms normally, the gradual accumulation of unrepaired microdamage in the lateral femoral cortex leads first to unicortical fracture of the lateral femoral cortex and often thereafter to complete fracture through the medial cortex, at that point comprising a complete AFF. AFF occurs in patients with long-term antiresorptive agent use, pycnodysostosis, HPP, heterozygous loss-of-function variant with ALPL, and hypophosphatemic osteomalacia. On the other hand, although osteoblastic function could largely be low in patients with long-term antiresorptive agent use and pycnodysostosis, compensatory activation of osteoblasts with an increase in osteoid is seen in HPP, heterozygous loss-of-function variants with ALPL, and hypophosphatemic osteomalacia, and also seen is an elevated ALP in hypophosphatemic osteomalacia. Therefore, although remodeling of bone hard tissue is low, remodeling of bone matrix protein is activated in these disorders [19, 44, 45].

Usually, serum ALP level is low among the disorders and conditions with low bone turnover, such as the patients using glucocorticoid and antiresorptive drugs, HPP, and patients with heterozygous loss-of-function variants in ALPL, while high serum ALP levels are typically observed in the patients with hypophosphatemic osteomalacia due to compensatory activation of osteoblasts. Therefore, paying attention to serum ALP levels might facilitate the detection of latent causative bone metabolic disorders and skeletal dysplasia among some patients with morphologic AFF, although ALP is not a perfect indicator because its level varies depending on several other factors. A recent study by Ng et al. reported that among 1839 patients visiting an osteoporosis clinic, seven (0.4%) had persistently low serum ALP levels. Five patients were genetically diagnosed with HPP, including four patients with persistently low ALP levels [46]. Similarly, Alonso et al. reported that out of 3285 patients in the osteoporotic clinic, 16 had low serum ALP and 14 of the 16 had ALPL gene variants [37]. HPP is a skeletal dysplasia caused by heterozygous, compound heterozygous, or homozygous variants in ALPL encoding ALP. Symptoms of HPP show a wide range and mild cases only present low serum ALP, arthrosis, and musculoskeletal pain. Such cases are mainly associated with loss of heterozygous function of ALPL, which has been shown to be dominantly inherited and relatively frequent (one in 187) [47‐50]. In 2012, Sutton et al. reported a case of bilateral subtrochanteric fracture after 4 years of bisphosphonate use for osteoporosis with mildly low serum ALP and later demonstrated a heterozygous variant in the ALPL gene (c.212G > A, p. Arg71His). Based on this result, it was suggested that administration of antiresorptive agents to osteoporotic patients with even heterozygous loss-of-function variants of ALPL should be carefully considered to avoid the development of subtrochanteric fractures [51]. In the present case with low serum ALP (patient #19), a heterozygous variant of ALPL is suspected, given the previous tibial fracture. However, even if serum ALP was decreased by other causes, low ALP itself could be associated with the risk of morphologic AFF. In 30 patients with ALP within the reference range, 19 (63%) had lower levels of ALP than the middle of the reference range, where elevation of ALP levels was expected due to active fractures. Given that ALP is usually supposed to elevate after a fracture due to enhanced bone remodeling at the fracture site, which may reflect low bone remodeling in all bone areas except the fracture site due to antiresorptive therapy [52].

The median serum Alb concentration in this cohort was relatively low (3.4 g/dL) compared with the reference value. Decreased food intake or absorption, decreased muscle mass, proinflammatory cytokines, acute illness, and comorbidities are common causes of hypoalbuminemia [53]. Considering that more than half of the patients in this study were older than 75 years, it is possible that low muscle mass and a greater complication rate of chronic inflammatory diseases contributed to low albumin levels.

To our knowledge, this is the first attempt to evaluate latent bone metabolic diseases and skeletal dysplasia associated with low bone formation comprehensively among patients with morphologic AFF in a single-center cohort. However, the sample size of this study was too small to predict the actual frequency of these bone diseases in morphologic AFF. Moreover, the genuine number of patients with these disorders in the current cohort was uncertain because it was a retrospective study, and some participants lacked pivotal data to conduct the differential diagnosis. For example, three, nine, and one patients were missing serum cCa, Pi, and ALP data, respectively.

Because of the retrospective nature of the current study, there were several analytical limitations. One of the limitations is a lack of information about the laboratory data relating to bone metabolism. For example, lack of measurement of 25-hydroxyvitamin D, which meant we could not evaluate the involvement of vitamin D deficiency in the development of AFF, which was reported elsewhere [54]. Inappropriately low BMD for age and sex without derangement of the bone metabolism-related laboratory measurements might suggest the possibility of mild osteogenesis imperfecta and related skeletal dysplasia [55]. Thus, in combination with genetic tests, screening for BMD might help evaluate the involvement of other skeletal dysplasia, including mild cases of osteogenesis imperfecta, in the development of morphologic AFF. In addition, since data collection was conducted on the electronic medical record in our hospital, past medical history, including past fractures, might be inaccurate. In the future, to clarify the genuine prevalence of bone disorders among patients with morphologic AFF, the execution of a comprehensive study with a large number of patients with morphologic AFF equipped with a completed laboratory dataset for all participants, and genetic testing if needed, is warranted.

When clinicians encounter patients with AFF, the careful exclusion of bone metabolic diseases and skeletal dysplasia associated with low bone formation should be conducted, since, in the cases of these disorders, appropriate treatment or elimination of the causative factor will reduce the risk of delayed union and recurrent fracture as those were observed in cases 1 and 2 in the current study. Furthermore, given that two out of the six patients with recurrent subtrochanteric fractures and two out of the five patients with subtrochanteric fractures on both sides had underlying bone metabolic disorders or skeletal dysplasia, in cases with these conditions, metabolic bone disease/skeletal dysplasia should be carefully differentiated. In addition, it is also desirable to exclude these bone diseases in advance before initiating long-term use of antiresorptive agents in osteoporotic patients to reduce the risk of the development of morphologic AFF. To determine the subjects who require a screening for metabolic bone disease/skeletal dysplasia, it might be adequate to select subsets of patients with high or low fasting, antiresorptive-free, measurement of serum ALP [37]. It is also important to confirm that the change in ALP levels is persistent and not transient because only the long-term suppression of bone formation serves as a risk factor for developing morphologic AFF.