Charcot neuroosteoarthropathy (CNO) can lead to disruption of the bone architecture of the foot (1). Increased osteoclastic activity is believed to be responsible for the bone destruction in CNO (2). Previous studies showed COOH-terminal telopeptide region of type 1 collagen (1CTP) and bone-specific alkaline phosphatase (BALP) as useful markers of bone turnover in patients with CNO (3–5).
Presently, only bisphosphonates have been demonstrated to have some benefit in patients with CNO (6). However, bisphosphonates may have potential disadvantages in that they decrease bone remodeling and are contraindicated in patients with renal insufficiency (7).
Our previous study (8) showed positive effects of calcitonin on bone resorption in patients with acute CNO. In this study, we set out to assess the effect of calcitonin on bone metabolism and disease activity during a 6-month treatment with intranasal calcitonin in acute CNO.
REASERCH DESIGN AND METHODS
Thirty-two consecutive patients with acute CNO were entered into the study. Subjects were recruited from our diabetic foot clinic during a 17-month period and were followed up for 6 months. The study was approved by the local ethics committee, and all participants gave written informed consent.
Acute CNO was defined by clinical signs: warm, swollen foot and skin temperatures ≥2°C at the site of maximum deformity of the affected foot compared with a similar site on the contralateral foot (infrared thermometer) and confirmed by plain X-ray and three-phase technetium bone scan (9). The presence of diabetic neuropathy was determined by measurement of vibration perception threshold >25 V on the tip of the hallux, using a biothesiometer (10). Osteomyelitis was excluded by the absence of clinical and laboratory signs of acute inflammation. Two patients in each group ulcerated during the study period. The midfoot was the most commonly affected site (n = 26) with no difference between groups.
Participants were randomized to receive salmon calcitonin nasal spray 200 IU daily with calcium supplementation (study group) or calcium supplementation only (control group) using a computer-generated randomization list. All patients also had standard treatment of the CNO, including off-loading by removable contact cast or cast walkers (11).
Disease activity was monitored by skin temperature measurement and markers of bone turnover: 1CTP (Orion Diagnostica, Espoo, Finland) and BALP (Tandem-R Ostase; Beckman Coulter, Fullerton, CA) were measured at each visit (monthly for the first 3 months and then at 6 months). Renal insufficiency was defined as an increased serum creatinine of >120 μmol/l, and five study patients and four control subjects had renal failures.
The sample size required for the study was 32 patients, which gave a power of 80% to detect a difference of 15% between the intervention and control groups with a two-sided α of 0.05. Data were analyzed by means of Wilcoxon rank test and Mann-Whitney two-sample test, and P < 0.05 was considered significant.
RESULTS
There was no difference in age (52.18 ± 10.3 and 54.93 ± 9.9 years; study versus control groups, respectively), type of diabetes, or sex between the two groups (type 2 diabetes and male sex: 11 patients per group) and no difference in severity of neuropathy (vibration perception threshold 42.9 ± 10.1 vs. 40.1 ± 8.9 V). In addition, there were no differences in disease activity as assessed by skin temperature difference (3.5 ± 0.9 vs. 3.6 ± 0.8°C), 1CTP (9.82 ± 2.17 vs. 9.73 ± 2.02 μg/l), and BALP (15.39 ± 6.25 vs. 15.44 ± 4.99 μg/l) between groups at the beginning of the study.
The study group had significantly greater reduction in 1CTP in comparison with the control group during the first 3 months (1st month 8.12 ± 1.39 vs. 9.48 ± 0.93 μg/l, 2nd month 7.96 ± 1.11 vs. 8.97 ± 0.75 μg/l, and 3rd month 7.63 ± 0.87 vs. 8.74 ± 0.74 μg/l; all P < 0.01); similarly, 1CTP reduction was seen in the subgroup of nine patients with renal insufficiency. Significant reduction of BALP was seen in the study group at 3 months in comparison with the control group (12.06 ± 4.02 vs. 13.72 ± 2.11 μg/l; P < 0.05); however, no difference in BALP was seen at 6 months between groups. Skin temperature of the affected foot significantly decreased in both groups; maximum reduction seen at 3 months (1.4 ± 0.4 and 1.5 ± 0.5°C vs. baseline; study and control groups, respectively; P < 0.001) with no significant differences between groups (Fig. 1).
CONCLUSIONS
We have shown that intranasal calcitonin treatment in patients with acute CNO significantly reduced bone turnover compared with standard therapy during the first 3 months of follow-up. In contrast to previous studies with bisphosphonates, our study included patients with renal insufficiency, who comprised 28% of the group.
The current standard treatment recommended for CNO includes off-loading and decreased weight bearing of the affected foot (12). Recent work has shown that bisphosphonates might be useful in the acute phase of CNO (3,13,14). However, one experimental study demonstrated that bone remodeling is strongly suppressed by high doses of bisphosphonates (15).
Calcitonin may have some advantageous effects in comparison with bisphosphonates. Bisphosphonates inhibit the action of osteoclasts, although not by impacting directly on the osteoprotegerin/receptor-activator nuclear factor κB ligand system (16) in contrast to calcitonin, which impacts directly on this signaling pathway. Bisphosphonates can cause total inhibition of calcifying colony-forming units (17) contrary to the cessation of the osteoclast bone resorption by calcitonin, which was not accompanied by a decreased activity of osteoblasts (18). For these reasons, it might be logical to consider treating patients with calcitonin rather than bisphosphonates (16).
Reduction of bone resorption markers has been demonstrated in patients treated with bisphosphonates (3,13) as well as bone formation markers (3). In our study, 1CTP and BALP significantly decreased in both groups in comparison with baseline values. In addition, a significantly greater reduction in the study group was seen. Calcitonin reduced 1CTP in comparison with baseline values throughout follow-up, whereas in the control group, a significant reduction in 1CTP was seen only at the end of the study. Similar to the Pamidronate Study (3), we also demonstrated skin temperature reduction in both groups with no differences between groups, probably due to the fact that all patients received off-loading measures (3). Although no study has previously been done in acute CNO, the effect of intranasal calcitonin on bone remodeling in postmenopausal osteoporosis is proven (19).
In conclusion, this study suggests that intranasal calcitonin treatment of acute CNO, including patients with renal insufficiency, could be an effective modality to prevent bone resorption and progression of this condition, although larger clinical trials are needed to assess the role of calcitonin in patients with acute CNO.
Effect of calcitonin on 1CTP (A), BALP (B), and skin temperature differences (C) in the control (dashed line) and calcitonin-treated (solid line) groups. Data are means ± SE. Study group vs. control group: *P < 0.05, **P < 0.01; study group and control group vs. baseline : †P < 0.05, ††P < 0.01, †††P < 0.001.
Effect of calcitonin on 1CTP (A), BALP (B), and skin temperature differences (C) in the control (dashed line) and calcitonin-treated (solid line) groups. Data are means ± SE. Study group vs. control group: *P < 0.05, **P < 0.01; study group and control group vs. baseline : †P < 0.05, ††P < 0.01, †††P < 0.001.
Article Information
This study was supported by grant MZO 00023001.
References
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