A randomized, controlled trial of once-weekly teriparatide injection versus alendronate in patients at high risk of osteoporotic fracture: primary results of the Japanese Osteoporosis Intervention Trial-05

Pharmacologic treatment is an important component of the management of osteoporosis. According to the recommendations of current guidelines, bone resorption inhibitors such as bisphosphonates and selective estrogen receptor modulators are commonly used as initial treatment in the majority of patients with osteoporosis [1, 2]. At the same time, once-daily subcutaneous injection of teriparatide (recombinant human parathyroid hormone [1-34]) is recommended for patients at high risk of fracture [1, 2].

Teriparatide possesses a potent anti-fracture effect by stimulating bone formation. Results of a network meta-analysis of randomized, controlled trials have shown that teriparatide may be the most effective anti-osteoporosis agent in reducing the risk of fractures [3]. However, its use for more than 2 years is not recommended [4]. Therefore, teriparatide must be switched to another medication once patients have received it for the approved period because of the possibility that bone mineral density (BMD) may decrease after the termination of teriparatide treatment [5, 6].

Recently, once-weekly subcutaneous injection of teriparatide (Teribone, Asahi Kasei Pharma Corporation, Tokyo, Japan) has been approved in Japan. Several non-clinical studies have suggested that the frequency of teriparatide administration may affect the histological pattern of bone formation and that a once-weekly regimen may not increase cortical porosity, in contrast to the once-daily regimen [7‐10]. In a randomized, placebo-controlled trial, once-weekly injections of teriparatide significantly reduced the risk of new vertebral fractures [11]. These results indicate that a once-weekly regimen is a promising treatment option, because once-weekly administration is generally more convenient than once-daily administration. However, its use is also restricted to 2 years. Furthermore, no head-to-head clinical trial has compared the anti-fracture efficacy of a once-weekly regimen with that of another anti-osteoporosis agent.

In a follow-up observational study of the placebo-controlled trial mentioned above, patients who received bisphosphonate following once-weekly injections of teriparatide achieved a further gain in BMD [12]. A previous randomized, controlled trial also showed that the sequential therapy with full-length parathyroid hormone (1-84) followed by alendronate significantly increased areal BMD at the lumbar spine compared with parathyroid hormone therapy followed by placebo or monotherapy with alendronate alone [13]. These results suggest that alendronate may be a suitable successor to teriparatide.

Accordingly, the Adequate Treatment of Osteoporosis (A-TOP) research group conducted the Japanese Osteoporosis Intervention Trial-05 (JOINT-05), which compared the efficacy and safety of sequential therapy (once-weekly injection of teriparatide for 72 weeks followed by alendronate for 48 weeks) and monotherapy (alendronate for 120 weeks) in patients at high risk of fracture. This study consisted of 2 parts. In the first part covering the treatment period up to 72 weeks, the efficacy and safety of teriparatide and alendronate were compared, and the hypothesis that teriparatide is superior to alendronate in reducing the incidence of morphometric vertebral fracture was tested. This was the primary objective. In the second part, during the treatment period of 73 to 120 weeks, the plan was to determine whether the efficacy of sequential therapy is superior to that of monotherapy, and this was the secondary objective. The primary results of the study are now reported.

Between October 2014 and December 2017, 1011 patients (505 in the teriparatide group and 506 in the alendronate group) were enrolled (Fig. 1). Of these, 26 patients (16 and 10, respectively) were excluded from the analysis, and the remaining 985 patients (489 and 496, respectively) were included in the full analysis set. In the alendronate group, 222 patients took the 35 mg/week tablet, 179 patients received 900 μg/4 weeks administration, 79 patients took 35 mg/week oral jelly formulation, 3 patients took the 5 mg/day tablet, and the administration routes of 13 patients were unknown. Data on morphometric vertebral fractures were obtained from 778 patients (351 and 427, respectively) and were included in the primary analysis.

During the study, 238 patients in the teriparatide group and 139 in the alendronate group discontinued the study. Of these, 142 and 70 patients in the teriparatide and alendronate groups did not wish to continue the study treatment, respectively. Furthermore, 42 and 18 patients in the teriparatide and alendronate groups, respectively, discontinued the study treatment because of safety reasons. However, most of the adverse events leading to treatment discontinuation were mild or moderate in intensity and resolved after treatment discontinuation.

By the end of 72 weeks, 5 and 7 patients in the teriparatide and alendronate groups, respectively, died. Of these, 3 deaths (2 in the teriparatide group and 1 in the alendronate group) were considered possibly related to the treatment (Online Resource Supplementary Table S1). The mean (SD) percentage adherence throughout the 72 weeks was 29.0% (45.2) in the teriparatide group and 64.2% (44.6) in the alendronate group, which was calculated under the assumption that patients not reporting adherence did not receive the study medication at all.

Baseline characteristics were well balanced between the treatment groups (Table 1). The mean (SD) age was 81.4 (4.5) years in the teriparatide group and 81.5 (4.7) years in the alendronate group. Approximately 40% of the patients in each treatment group had at least 2 prevalent vertebral fractures and grade 3 prevalent vertebral fractures. Baseline characteristics were also similar between patients with and without radiographs at 72 weeks (Online Resource Supplementary Table S2).

In the analysis of the primary endpoint (Table 2), the incidence of morphometric vertebral fracture was significantly lower in the teriparatide group (56 per 419.9 person-years, annual incidence rate 0.1334) than in the alendronate group (96 per 553.6 person-years, annual incidence rate 0.1734) with a rate ratio of 0.78 (95% CI 0.61 to 0.99, P = 0.04). The results of the sensitivity analyses also showed the superiority of teriparatide over alendronate (Online Resource Supplementary Table S3).

Mean lumbar spine BMD (T-score) was similarly elevated up to 72 weeks in both treatment groups (Fig. 2). Similar trends in BMD were observed at the second lumbar vertebra (L2) to L4, total hip, femoral neck, and forearm (Online Resource Supplementary Table S4). Serum levels of osteocalcin and P1NP rose in the teriparatide group and reached peak values at 12 weeks, whereas they constantly decreased in the alendronate group. As a result, the increases in osteocalcin and P1NP levels were significantly larger in the teriparatide group at 72 weeks (P < 0.01). Serum levels of TRACP-5b decreased in both groups, but the amount of reduction was significantly greater in the alendronate group at 72 weeks (P < 0.01).

The treatment effects of teriparatide on the incidence of morphometric vertebral fractures were generally consistent across various subgroups (Fig. 3). In the subgroups stratified by SQ grade of prevalent vertebral fracture, however, teriparatide showed a good effect in patients with grade 3 fractures, whereas alendronate showed it in those with grades 1–2 fractures (P = 0.08 for interaction). Teriparatide also showed a good effect in patients with T-scores of less than −3.3, whereas alendronate showed it in those with T-scores of at least −3.3 (P = 0.61 for interaction).

In both treatment groups, adverse events were most frequently reported in the following system organ classes: infections and infestations, gastrointestinal disorders, and musculoskeletal and connective tissue disorders (Table 3). During the treatment, 6 patients (2 in the teriparatide group and 4 in the alendronate group) experienced severe adverse events that were considered possibly related to the treatment (Online Resource Supplementary Table S1). In the teriparatide group, nausea and pancreatic carcinoma were reported. In the alendronate group, gastric ulcer, herpes zoster, acute heart failure, and death due to unknown cause were reported.

In the primary analysis of this study, the incidence of morphometric vertebral fractures was significantly lower in the teriparatide group than in the alendronate group. Moreover, the secondary analysis showed the non-inferiority of teriparatide to alendronate in reducing the risk of non-vertebral fractures. Although the vertebral fracture treatment comparisons in osteoporotic women (VERO) study showed the superiority of once-daily injection of teriparatide over risedronate in reducing new radiographic vertebral fractures [18], no randomized, controlled trial has compared the anti-fracture efficacy of a once-weekly regimen and another anti-osteoporosis agent. To the best of our knowledge, this is the first head-to-head comparison trial.

The rate ratio for the incidence of morphometric vertebral fractures was 0.78, which was relatively smaller than that obtained from the VERO study (risk ratio 0.44 vs. risedronate) or a network meta-analysis (hazard ratio 0.46 vs. alendronate) [18, 19]. This smaller effect size may simply imply that the once-daily regimen is more efficacious than the once-weekly regimen, or it may have been derived from the patients’ characteristics in the present study. For example, patients enrolled in this study were older than those in the VERO study by an average of 10 years. Another possibility is the poor treatment adherence. In the present study, the mean percentage adherence in the teriparatide group was 29%, and approximately 30% of the patients did not wish to continue teriparatide treatment. Once-weekly injection of teriparatide, as well as the once-daily regimen, is much more expensive than other therapies. It is notable that this was a pragmatic trial in which study drugs were not provided by the researchers and were open-label. In other words, patients in the present study paid the cost of the study medication. This payment might have led to the poor adherence, although most of the cost was covered by insurance. The cost is an important limitation of teriparatide [2], and effective strategies to improve adherence are needed.

Patients aged at least 75 years were enrolled, and their mean age exceeded 80 years. Because clinical trials usually do not include patients aged 80 years or older, the present findings are important when considering the treatment strategy for such an elderly population. In the subgroup analysis stratified by age (<85 vs. ≥85 years), treatment effects were consistent regardless of age group. This result means that the anti-fracture efficacy of teriparatide is superior to that of alendronate even in elderly persons.

Other subgroup analyses have suggested the superiority of teriparatide in patients with grade 3 prevalent vertebral fractures and those with T-scores less than −3.3. Currently, teriparatide is recommended for patients with severe osteoporosis or those at high risk of fracture worldwide [1, 2, 20]. However, there are no universally accepted criteria for identifying such a population [1]. For example, the European guidance strongly recommends teriparatide for patients with vertebral fractures [1], whereas the Endocrine Society Clinical Practice Guideline recommends it for those with severe or multiple vertebral fractures [2]. Furthermore, the Japanese guideline recommends a once-weekly regimen for those with low BMD, prevalent fractures, older age, or a family history of hip fracture [20]. The results of the subgroup analyses, as well as the inclusion criteria, support the recommendations of the Japanese guideline.

Despite the significant difference in the incidence of vertebral fracture between the treatment groups, the mean BMD increased similarly in both groups. In the post hoc analysis of the Fracture Prevention Trial, teriparatide-mediated increases in spine BMD accounted for approximately one-third of the vertebral fracture risk reduction, and the majority of the risk reduction resulted from improvements in non-BMD determinants of bone strength [21]. In another study, total bone mineral content, total and cortical bone areas, periosteal circumference, and polar cross-sectional moment of inertia were significantly higher in patients treated with teriparatide than in those treated with placebo [22]. These results indicate that the anti-fracture efficacy of teriparatide is mainly derived from its effects on bone strength and bone geometry.

As for the changes in bone turnover markers, once-weekly injection of teriparatide increased the serum levels of osteocalcin and P1NP and decreased the levels of TRACP-5b, which indicates that it increases bone formation while decreasing bone resorption. This result is inconsistent with those obtained from the once-daily regimen, which increased bone-resorption markers after increasing bone-formation markers [23, 24]. This may be a unique action of the once-weekly regimen because previous clinical studies have also shown that once-weekly injection of teriparatide induced bone formation without promoting bone resorption [11, 25]. In a non-clinical study in mice, a low frequency of administration of teriparatide induced bone formation by both remodeling and mini-modeling, whereas high-frequency administration induced it predominantly by remodeling [7]. This result may explain its unique action, because bone formation by modeling involves little increase in bone resorption [25].

In the safety assessments, adverse events were frequently reported in both groups because elderly patients were enrolled in the study. However, only 4 severe adverse events were considered possibly related to teriparatide. In addition, similar proportions of patients in both groups died by the end of 72 weeks in the present study, whereas more patients died in the teriparatide group than in the risedronate group in the VERO study [18]. These safety results, as well as the efficacy results, suggest that a once-weekly regimen could be a promising treatment option.

Some limitations should be mentioned. First, the sample size was not large enough to detect the difference between the treatment groups in the incidence of any fracture, the incidence of clinical vertebral fracture, and vertebral fracture progression. We plan to assess the effects of the sequential therapy on these outcomes at 120 weeks. Second, the mean percentage adherence differed between the treatment groups. However, regarding the primary endpoint, the robustness of the findings was examined through three sensitivity analyses, and the results were similar to those of the planned primary analysis, although multiple imputation was not performed. Third, since BMD was measured at the lumbar spine, proximal femur, radius, and second metacarpal bone in each institution, the precise analytical methods might have differed among the institutions. Therefore, changes in T-scores were analyzed in this study.

In conclusion, treatment with once-weekly subcutaneous injection of teriparatide for 72 weeks was associated with a significant reduction in the incidence of morphometric vertebral fractures compared with that with alendronate in women with primary osteoporosis who were at high risk of fracture. However, teriparatide must be switched to another medication once patients have received it for the approved period. Therefore, a suitable successor to teriparatide must be identified. In the second part of this study, we will determine whether the efficacy of sequential therapy with teriparatide followed by alendronate is superior to that of monotherapy with alendronate alone.