Background
Charcot neuroarthropathy (Charcot foot) is a highly destructive joint disease characterised by progressive multiple bone fractures, dislocations and severe deformity of the foot and ankle [
1‐
3]. There are a number of medical conditions with neuropathic manifestations that are linked to the development of Charcot foot [
4], although diabetes has become the leading cause in the Western world [
3‐
6]. The estimated prevalence of Charcot foot in the general diabetes population is 0.08%, but can rise to 13% in high-risk foot populations [
3,
4]. Acute Charcot neuroarthropathy typically presents as a warm, erythematous and oedematous foot [
7,
8]. As such, this condition is often masked by, or is clinically indistinguishable from deep vein thrombosis, inflammatory arthritis (e.g. gout) or infection (e.g. cellulitis, osteomyelitis). Consequently, this often leads to delayed or missed diagnosis in its early stages [
4,
7,
9].
Delayed diagnosis can result in devastating complications such as gross deformity, instability, recurrent ulceration and/or amputation [
2,
3,
6,
9]. Structural damage to the foot and ankle can be limited, however, if acute Charcot foot is identified and managed early [
2,
7,
9]. Total contact casting (TCC) is a treatment used to offload and immobilise the affected foot and ankle to prevent trauma, further fractures and destruction, and preserve the foot structure during the inflammatory phase [
10,
11]. The TCC slows the progression of the Charcot foot by controlling the cycle of inflammation and the degree of lower limb oedema [
3,
5,
8,
11,
12].
It is widely accepted that TCC is the preferred method of immobilisation for an acute Charcot foot, as it is customised and non-removable [
3,
10,
12]. However, a common question from patients being treated with TCC is “
this cast is hot and heavy; how long do I have to use it?” Duration of TCC treatment will depend upon the patient’s response, but it is recommended that casting is continued until the temperature differential is less than 2 °C between the affected and non-affected Charcot foot for 4–6 consecutive weeks, and there are radiographic signs of healing [
3,
8,
13‐
16].
Globally, population-based studies have found significant discrepancies regarding the duration of TCC treatment for resolution of acute Charcot foot. In the United Kingdom (UK), studies have reported treatment times of 9 to 12 months [
2,
17,
18], while data from the United States (US) [
10,
11,
19,
20], Europe [
21‐
28] and other Asia Pacific countries [
29,
30] have reported shorter treatment times of 3 to 9 months. Unfortunately, none of the above-mentioned studies included Australian subjects. To date, there has only been one Australian study that has reported on TCC duration times for acute Charcot foot resolution. This study reported an average treatment time of approximately 10 months [
31]. Therefore, there is limited data regarding the duration of TCC treatment for resolution of acute Charcot foot in the Australian population. To address this deficiency, this study conducted a retrospective analysis of cases presenting to a high-risk foot service (HRFS) with acute Charcot foot over a three-year period. This study specifically aimed to investigate the time to resolution of acute Charcot foot with TCC treatment, and to explore patient and clinical factors affecting its duration.
Results
Of the 46 patient records screened, 27 adults with acute Charcot foot attending the HRFS between January 2012 and January 2015 were eligible for inclusion. Table
1 provides the participant characteristics. The mean age (SD) was 57.9 (12.6) years, 66.7% were male, and 29.6% had a smoking history (i.e. past or current smoker). The majority of participants had diabetes (88.9%) with an average duration of 24.0 (SD, 13.3) years and glycated haemoglobin of 8.6% (SD, 2.0). Overall, there was a high prevalence of previous foot complications including foot ulceration (66.7%), infection (63.0%) and amputation (14.8%). Peripheral neuropathy and peripheral arterial disease were present in 96.3 and 33.3%, respectively (Table
2).
Table 1
Participant characteristics
Mean age (SD), years | 57.9 (12.6) | 56.3 (13.7) | 59.1 (12.0) | 2.81 (−7.40 to 13.02)† | 0.576 |
Male sex, n (%) | 18 (66.7) | 8 (66.7) | 10 (66.7) | 1.00 (0.20 to 5.00) | > 0.99 |
Known ethanol abuse, n (%) | 6 (22.2) | 4 (33.3) | 2 (13.3) | 0.31 (0.05 to 2.08) | 0.357 |
Smoking history, n (%)a | 8 (29.6) | 2 (16.7) | 6 (40.0) | 3.33 (0.53 to 20.91) | 0.236 |
Diabetes, n (%) | 24 (88.9) | 10 (83.3) | 14 (93.3) | 2.80 (0.22 to 35.29) | 0.569 |
Type 1, n (%) | 8 (33.3) | 4 (40.0) | 4 (28.6) | 0.60 (0.11 to 3.34) | 0.673 |
Type 2, n (%) | 16 (66.7) | 6 (60.0) | 10 (71.4) | 1.67 (0.30 to 9.27) | 0.673 |
Mean duration (SD), years | 24.0 (13.3) | 22.4 (13.5) | 25.1 (13.6) | 2.74 (−8.87 to 14.36)† | 0.629 |
Mean HbA1c (SD), %b | 8.6 (2.0) | 8.1 (2.5) | 8.9 (1.7) | 0.82 (−0.99 to 2.63)† | 0.358 |
Dyslipidaemia, n (%) | 16 (59.3) | 6 (50.0) | 10 (66.7) | 2.00 (0.42 to 9.52) | 0.452 |
Hypertension, n (%) | 13 (48.1) | 4 (33.3) | 9 (60.0) | 3.00 (0.62 to 14.62) | 0.168 |
Ischaemic heart disease, n (%) | 3 (11.1) | 1 (8.3) | 2 (13.3) | 1.69 (0.14 to 21.27) | > 0.99 |
Congestive cardiac failure, n (%) | 0 (0) | 0 (0) | 0 (0) | N/A | N/A |
Cerebrovascular disease, n (%) | 2 (7.4) | 0 (0) | 2 (13.3) | 1.92 (1.32 to 2.80) | 0.487 |
Chronic kidney disease, n (%) | 4 (14.8) | 1 (8.3) | 3 (20.0) | 2.75 (0.25 to 30.51) | 0.605 |
Osteoarthritis, n (%) | 13 (48.1) | 3 (25.0) | 10 (66.7) | 6.00 (1.11 to 32.55) | 0.031* |
Previous foot ulceration, n (%) | 18 (66.7) | 7 (58.3) | 11 (73.3) | 1.96 (0.39 to 9.93) | 0.448 |
Previous foot infection, n (%) | 17 (63.0) | 7 (58.3) | 10 (66.7) | 1.43 (0.30 to 6.88) | 0.706 |
Previous amputation, n (%) | 4 (14.8) | 3 (25.0) | 1 (6.7) | 0.21 (0.02 to 2.39) | 0.294 |
Table 2
Neurovascular foot assessments
Peripheral neuropathya | 26 (96.3) | 11 (91.7) | 15 (100.0) | 0.42 (0.27 to 0.66) | 0.444 |
Left | | | | | |
0/3, n (%) | 24 (88.9) | 11 (84.6) | 13 (92.9) |
1/3, n (%) | 1 (3.7) | 0 (0) | 1 (7.1) |
2/3, n (%) | 1 (3.7) | 1 (7.7) | 0 (0) |
3/3, n (%) | 1 (3.7) | 1 (7.7) | 0 (0) |
Right | | | |
0/3, n (%) | 24 (88.9) | 11 (84.6) | 13 (92.9) |
1/3, n (%) | 1 (3.7) | 1 (7.7) | 0 (0) |
2/3, n (%) | 0 (0) | 0 (0) | 0 (0) |
3/3, n (%) | 2 (7.4) | 1 (7.7) | 1 (7.1) |
Peripheral arterial diseaseb | 9 (33.3) | 4 (33.3) | 5 (33.3) | 1.00 (0.20 to 5.00) | > 0.99 |
Pedal pulses† | | | | | |
0/4, n (%) | 1 (3.7) | 1 (7.7) | 0 (0) |
1/4, n (%) | 1 (3.7) | 0 (0) | 1 (7.1) |
2/4, n (%) | 4 (14.8) | 2 (15.4) | 2 (14.3) |
3/4, n (%) | 1 (3.7) | 0 (0) | 1 (7.1) |
4/4, n (%) | 19 (70.4) | 10 (76.9) | 9 (64.3) |
Mean ABPI (SD) | | | |
Left† | 1.15 (0.20) | 1.11 (0.21) | 1.20 (0.20) |
Right† | 1.11 (0.23) | 1.08 (0.15) | 1.16 (0.33) |
Mean TBPI (SD) | | | |
Left† | 0.82 (0.15) | 0.79c | 0.83 (0.21) |
Right† | 0.66 (0.17) | 0.78c | 0.53c |
Mean systolic toe pressure (SD) | | | |
Left† | 105.4 (11.6) | 118c | 102.3 (10.6) |
Right† | 99.0 (13.9) | 109c | 95.7 (15.0) |
Charcot misdiagnosis occurred in 63.0% of participants, and signs and symptoms consistent with acute Charcot foot were present for a median of 2.0 (IQR, 1.0 to 6.0) months prior to presenting or being referred to the HRFS. The affected foot was most commonly misdiagnosed as cellulitis (47.1%). All participants presented with a stage 1 Charcot foot. Of these, the majority were located in the tarsometatarsal joints (44.4%) or midfoot (40.7%) and were triggered by an ulcer or traumatic injury (85.2%). All participants received x-ray imaging to establish diagnosis at initial presentation to the HRFS, while 14.8% also had a bone scan and/or magnetic resonance imaging (Table
3).
Table 3
Charcot foot history
Charcot foot |
Left, n (%) | 14 (51.9) | 4 (33.3) | 10 (66.7) | 4.00 (0.80 to 20.02) | 0.085 |
Right, n (%) | 13 (48.1) | 8 (66.7) | 5 (33.3) | 0.25 (0.05 to 1.25) | 0.085 |
Stage of Charcot |
Stage 0, n (%) | 0 (0) | 0 (0) | 0 (0) | N/A | N/A |
Stage 1, n (%) | 27 (100.0) | 12 (100.0) | 15 (100.0) | N/A | N/A |
Median Charcot duration (IQR), monthsa,b | 2.0 (1.0 to 6.0) | 2.5 (1.0 to 6.0) | 1.8 (0.9 to 6.8) | N/A | 0.709† |
Charcot trigger |
Ulceration, n (%) | 9 (33.3) | 5 (41.7) | 4 (26.7) | 0.51 (0.10 to 2.57) | 0.448 |
Injury/trauma, n (%) | 14 (51.9) | 5 (41.7) | 9 (60.0) | 2.10 (0.45 to 9.84) | 0.343 |
Amputation, n (%) | 2 (7.4) | 2 (16.7) | 0 (0) | 1.20 (0.93 to 1.55) | 0.188 |
Lymphoedema, n (%) | 1 (3.7) | 0 (0) | 1 (6.7) | 0.93 (0.82 to 1.07) | > 0.99 |
Unknown, n (%) | 1 (3.7) | 0 (0) | 1 (6.7) | 0.93 (0.82 to 1.07) | > 0.99 |
Charcot misdiagnosis, n (%) | 17 (63.0) | 7 (58.3) | 10 (66.7) | 1.43 (0.30 to 6.88) | 0.706 |
Charcot pattern |
Tarsometatarsal joints, n (%) | 12 (44.4) | 5 (41.7) | 7 (46.7) | 1.23 (0.27 to 5.67) | 0.795 |
NC, TN, CC joints, n (%) | 11 (40.7) | 6 (50.0) | 5 (33.3) | 0.50 (0.11 to 2.38) | 0.452 |
Ankle and subtalar joints, n (%) | 1 (3.7) | 0 (0) | 1 (6.7) | 0.93 (0.82 to 1.07) | > 0.99 |
Combination, n (%)c | 3 (11.1) | 1 (8.3) | 2 (13.3) | 1.69 (0.14 to 21.3) | > 0.99 |
Imaging received |
X-ray, n (%) | 27 (100.0) | 12 (100.0) | 15 (100.0) | N/A | N/A |
Bone scan, n (%) | 4 (14.8) | 0 (0) | 4 (26.7) | 0.73 (0.54 to 1.00) | 0.106 |
MRI, n (%) | 4 (14.8) | 2 (16.7) | 2 (13.3) | 0.77 (0.09 to 6.45) | > 0.99 |
Throughout the study period, there were a total of 421 TCCs applied (average of 15 TCCs per participant). The median TCC duration for resolution of acute Charcot foot was 4.3 (IQR, 2.7 to 7.8) months. A large proportion of participants (77.8%) were able to weightbear as tolerated using a post-operative shoe over the TCC. Overall, there were 21 complications/adverse events related to the TCC treatment, the majority being minor and reversible. Skin rubbing/irritation (40.7%) and asymmetry pain (22.2%) were the most common. The overall complication rate was 5% per cast (calculated from the total number of complications divided by the total number of TCCs i.e. 21/421). Post TCC treatment, almost half of the participants (48.1%) transitioned into specialised or off-the-shelf footwear with custom foot orthoses, 25.9% used a life-long CROW, and 22.2% underwent soft tissue or bone reconstructive surgery. The median follow-up time from ceasing TCC treatment (due to Charcot resolution) to the end of the study period was 11.9 (IQR, 2.8 to 14.6) months. During this time, there were no recurrent Charcot feet recorded, however, contralateral Charcot foot occurred in 3 (11.1%) participants (Table
4).
Table 4
Total contact casting treatment
TCC applications |
Total number | 421 | 101 | 320 | N/A | N/A |
Mean (SD), per participant | 15.6 (9.2) | 8.4 (2.3) | 21.3 (8.5) | N/A | N/A |
TCC duration |
Median (IQR), months | 4.3 (2.7 to 7.8) | 2.6 (2.1 to 3.4) | 6.0 (4.4 to 8.9) | N/A | N/A |
Ambulation status |
Walking with post-operative shoe, n (%) | 21 (77.8) | 10 (83.3) | 11 (73.3) | 0.55 (0.08 to 3.68) | 0.662 |
Wheelchair bound, n (%) | 2 (7.4) | 1 (8.3) | 1 (6.7) | 0.79 (0.04 to 14.03) | > 0.99 |
Crutches, n (%) | 3 (11.1) | 1 (8.3) | 2 (13.3) | 1.69 (0.14 to 21.27) | > 0.99 |
Scooter, n (%) | 1 (3.7) | 0 (0) | 1 (6.7) | 0.93 (0.82 to 1.07) | > 0.99 |
Total number of complications/adverse events | 21 | 7 | 14 | N/A | N/A |
Complications/adverse events, n (%) | 16 (59.3) | 6 (50.0) | 10 (66.7) | 2.00 (0.42 to 9.52) | 0.452 |
Ulceration, n (%) | 2 (7.4) | 0 (0) | 2 (13.3) | 0.87 (0.71 to 1.06) | 0.487 |
Amputation, n (%) | 0 (0) | 0 (0) | 0 (0) | N/A | N/A |
Infection, n (%) | 0 (0) | 0 (0) | 0 (0) | N/A | N/A |
Deep vein thrombosis, n (%) | 0 (0) | 0 (0) | 0 (0) | N/A | N/A |
Falls, n (%) | 0 (0) | 0 (0) | 0 (0) | N/A | N/A |
Asymmetry pain, n (%) | 6 (22.2) | 2 (16.7) | 4 (26.7) | 1.82 (0.27 to 12.17) | 0.662 |
Rubbing/irritation, n (%) | 11 (40.7) | 5 (41.7) | 6 (40.0) | 0.93 (0.20 to 4.37) | > 0.99 |
Self-inflicted, n (%) | 0 (0) | 0 (0) | 0 (0) | N/A | N/A |
Other, n (%)a | 2 (7.4) | 0 (0) | 2 (13.3) | 0.87 (0.71 to 1.06) | 0.487 |
None, n (%) | 11 (40.7) | 6 (50.0) | 5 (33.3) | 1.00 (0.20 to 5.00) | > 0.99 |
Treatment after TCC |
Specialised footwear and custom foot orthoses, n (%) | 13 (48.1) | 4 (33.3) | 9 (60.0) | 3.00 (0.62 to 14.62) | 0.168 |
Life-long CROW, n (%) | 7 (25.9) | 5 (41.7) | 2 (13.3) | 0.22 (0.03 to 1.41) | 0.185 |
Reconstructive/bone surgery, n (%) | 4 (14.8) | 1 (8.3) | 3 (20.0) | 2.75 (0.25 to 30.51) | 0.605 |
Soft tissue surgery, n (%) | 2 (7.4) | 1 (8.3) | 1 (6.7) | 0.79 (0.04 to 14.03) | > 0.99 |
CAM walker, n (%) | 1 (3.7) | 1 (8.3) | 0 (0) | 1.09 (0.92 to 1.29) | 0.444 |
Recurrent Charcot foot, n (%) | 0 (0) | 0 (0) | 0 (0) | N/A | N/A |
Contralateral Charcot foot, n (%) | 3 (11.1) | 1 (8.3) | 2 (13.3) | 1.69 (0.14 to 21.27) | > 0.99 |
Charcot pattern | | | | | |
Tarsometatarsal joints, n (%) | 1 (33.3) | 0 (0) | 1 (50.0) | N/A | N/A |
NC, TN, CC joints, n (%) | 1 (33.3) | 0 (0) | 1 (50.0) | N/A | N/A |
Ankle and subtalar joints, n (%) | 0 (0) | 0 (0) | 0 (0) | N/A | N/A |
Combination, n (%)b | 1 (33.3) | 1 (100.0) | 0 (0) | N/A | N/A |
On comparison of participants with more or less than 4 months duration of TCC treatment, only osteoarthritis was significantly associated with a longer TCC duration (OR, 6.00; 95% CI, 1.11 to 32.55;
p = 0.031). All other patient and clinical factors were non-significant (Tables
1 to
4).
From acute Charcot diagnosis to resolution, the greatest reduction in dermal temperature differential was seen at the medial aspect of the navicular (− 1.7 °C), followed closely by the dorsal aspect of the base of the 3rd metatarsal, the medial aspect of the base of the 1st metatarsal, and the medial malleolus (− 1.5 °C) (Table
5).
Table 5
Dermal temperatures
1 | Plantar 1st metatarsal head | 2.5 (2.2) | 1.3 (1.6) | 1.2 |
2 | Plantar 3rd metatarsal head | 2.8 (2.0) | 1.4 (2.2) | 1.4 |
3 | Plantar 5th metatarsal head | 2.6 (2.2) | 1.2 (1.8) | 1.4 |
4 | Plantar aspect of the base of the 5th metatarsal (styloid process) | 2.4 (1.3) | 1.1 (1.3) | 1.3 |
5 | Dorsal aspect of the base of the 3rd metatarsal | 2.9 (2.2) | 1.4 (1.5) | 1.5 |
6 | Medial aspect of the base of the 1st metatarsal | 3.0 (2.1) | 1.5 (1.8) | 1.5 |
7 | Medial aspect of the navicular | 3.0 (1.7) | 1.3 (1.3) | 1.7 |
8 | Plantar medial tubercle of the calcaneus | 1.6 (1.4) | 0.7 (1.1) | 0.9 |
9 | Medial malleolus | 2.6 (1.7) | 1.1 (1.3) | 1.5 |
10 | Lateral malleolus | 2.9 (1.5) | 1.7 (1.3) | 1.2 |
Discussion
This is one of the first studies to investigate duration of TCC treatment for resolution of acute Charcot foot in Australian subjects. Overall, this study found that the median duration of TCC treatment was 4.3 (IQR, 2.7 to 7.8) months. This finding is observed to be shorter than reports from studies in the UK (median, 9 to 12 months) [
2,
17,
18], but is mostly comparable to studies conducted in the US (mean, 3 to 5 months) [
10,
11,
19,
20], Europe (mean, 3 to 9 months) [
21‐
27], and other Asia Pacific countries, including Thailand (median, 5 months) [
30] and New Zealand (mean, 5 months) [
29]. Interestingly, this finding was lower than an earlier Australian study conducted in Perth, where the average TCC duration was approximately 10 months [
31]. This global (and local) variation may be explained by differing participant characteristics, Charcot characteristics (e.g. pattern and stage), techniques and protocols for monitoring Charcot progression, definition of Charcot resolution, the type of offloading used and their respective protocols (e.g. initial treatment with TCC and then transitioning to removable walker) [
10,
25,
26], reduced access to services, staff capacity and experience in applying the TCCs, and study design [
2,
20,
21,
43‐
46].
That being said, the available data on TCC duration are largely derived from retrospective and observational studies with small sample sizes, therefore, there is limited ability to determine temporal relationships with the reported clinical outcomes. The two largest studies in the literature includes a web-based observational study [
2] with 288 acute Charcot cases from 76 centres in the UK and Ireland (although data on resolution were only available in 219 participants). The median duration of TCC treatment was 9 months [
2]. Another study [
28] that conducted a retrospective analysis on 164 participants with acute Charcot found the average TCC treatment time was 6 months [
28]. Given that these two studies have the largest cohorts, and are likely to be the most clinically relevant, these figures may perhaps act as a benchmark for TCC duration more broadly.
There were five additional important findings from our study. First, those with osteoarthritis were 6-fold more likely to have a TCC duration of more than 4 months for acute Charcot foot resolution, compared to those without osteoarthritis (OR, 6.00; 95% CI, 1.11 to 32.55;
p = 0.031). While there is some evidence to suggest a relationship between rheumatoid arthritis and Charcot neuroarthropathy [
47], to the authors’ knowledge, no publications have reported Charcot neuroarthropathy in association with osteoarthritis. Our finding that osteoarthritis may be associated with longer TCC duration (i.e. longer time to Charcot resolution) may be explained by the biomechanical (e.g. foot structure and function) and/or biochemical factors (e.g. chemokines, cytokines, growth factors) associated with osteoarthritis [
48], which may be further exacerbated by the Charcot process. This finding, however, should be interpreted with caution due to the wide confidence interval. There were no other significant patient or clinical factors that affected TCC treatment time (i.e. when comparing those < 4 or > 4 months TCC duration), which is consistent with a previous study [
15]. Due to the small sample size (
n = 27) and retrospective nature of this study, high-quality prospective studies with large sample sizes are needed to confirm these findings.
Second, our findings relating to Charcot foot characteristics, including Charcot pattern and history of misdiagnosis, are similar to reports from previous studies [
21,
31]. In the current study, Charcot foot most commonly affected the tarsometatarsal joints (44.4%) or midfoot (40.7%). Overall, 85.2% were triggered by an ulcer or traumatic injury and were present for a median of 2.0 (IQR, 1.0 to 6.0) months prior to attending the HRFS. Charcot misdiagnosis occurred in 63.0% of participants prior to attending the HRFS, most commonly confused with cellulitis (47.1%). Despite increased awareness, the acknowledged importance of Charcot-related patient education [
49], and the publication of an evidence-based pathway [
3], disparity still remains for early diagnosis [
31]. Our findings support close monitoring for signs of Charcot foot in those with ulceration or reported traumatic injury to the foot. Furthermore, in those presenting with a warm, erythematous and/or oedematous foot, Charcot diagnosis should be considered, and the foot treated as such, until proven otherwise [
8]. This is particularly important for high-risk patients with long-standing diabetes and neuropathy [
3,
21].
Third, of the 421 TCCs applied, there were 21 complications in total. This equates to an overall complication rate of 5% per cast, which is consistent with a previous study [
50]. Overall, 59.3% of participants experienced a complication or adverse event, the majority being minor and reversible. The most common complications were skin rubbing/irritation (61.1%) and asymmetry pain (33.3%). Previous studies have shown that the duration of non-removable (e.g. TCC) versus removable offloading devices (e.g. Aircast, CAM walker) for Charcot resolution is significantly less [
2,
31]. Given that the use of non-removable offloading can shorten the median time to resolution by approximately 3 months [
2], this option may appeal to patients with Charcot foot due to the known physical, mental and social consequences of prolonged offloading (e.g. muscle atrophy, reduced activity levels and fitness, weight gain, poor glycaemic control, risk of falls, loss of work or income, offloading-related stigma, reduced health-related quality of life, inability to participate in certain family activities) [
1,
5]. Our findings and those of a previous study [
50] support that TCC is a relatively safe modality for offloading and immobilising neuropathic feet, despite some expected minor and reversible complications [
50]. However, it is still essential when considering TCC treatment that the risks and benefits are carefully considered, and that patients are fully informed of these risks prior to their first TCC application.
Fourth, a large proportion of participants experienced good clinical outcomes post TCC treatment. Almost half were able to return to specialised or off-the-shelf footwear and custom foot orthoses (48.1%), while the other half with more severe cases of Charcot foot chose to wear a life-long CROW (25.9%) or had soft tissue or bone reconstructive surgery (22.2%). Fortunately, there were no recurrent Charcot feet recorded, which is consistent with other studies [
15,
26]. Contralateral Charcot foot occurred in 3 (11.1%) participants. Therefore, to reduce the risk of bilateral Charcot, it is essential to ensure contralateral footwear is appropriate and an offloading foot orthotic is fitted [
3]. As this study only collected data over a three-year period, longitudinal, prospective studies are needed to evaluate these clinical outcomes further.
Fifth, from acute Charcot diagnosis to resolution, the greatest reduction in temperature differential (i.e. when performing dermal temperature measurements at 10 commonly used anatomical sites) was seen at the medial aspect of the navicular (− 1.7 °C), followed closely by the dorsal aspect of the base of the 3rd metatarsal, the medial aspect of the base of the 1st metatarsal, and the medial malleolus (− 1.5 °C). This reduction in temperature differential is supported by a previous study [
14]. Considering that the highest dermal temperatures often correlate with the joints affected by Charcot [
3,
51,
52], this may explain why a greater temperature reduction was seen at these anatomical sites (i.e. as the majority of Charcot feet in this study affected the tarsometatarsal and midfoot joints). This finding provides valuable information regarding the expected reduction in temperature differential for each specific anatomical testing site at Charcot resolution, which may assist clinicians in monitoring Charcot progression.
This study has the limitations of a retrospective design and small sample size. To address the potential for selection bias, all participants that met the strict study eligibility criteria within the available sample were included. Therefore, the risk of selection bias was negligible or essentially non-existent. Due to the small sample size (n = 27), there is an increased likelihood of the study being underpowered, which may have increased the risk for type II statistical errors. For example, the ability to detect differences between the TCC groups (i.e. < 4 months and > 4 months duration). However, as all eligible participants were exhausted from the available sample, the maximum sample size was reached. Therefore, it was not possible to increase the sample size of the current study. Another limitation relates to having no data or measurements pertaining to the degree of adherence to the TCC treatment. However, as this was a non-removable device, poor adherence to treatment was unlikely. Regarding external validity, our findings are mostly generalisable to patients presenting with modified Eichenholtz stage 1 Charcot foot and those with diabetes (88.9% of the cohort). In addition, as this study only included participants from a single metropolitan health service, this may affect the applicability of the findings to the broader Australian context. Finally, in cases of unexpected removal (e.g. patient request, work/travel requirements), the time spent out of the TCC was included in the participant’s overall TCC treatment time. As a result, this may have slightly increased the study’s calculated median TCC duration. However, to ensure this study remained pragmatic and clinically relevant, the authors’ decision to include time spent out of the TCC was relevant.
Despite these limitations, this is one of the first studies to investigate duration of TCC treatment for resolution of acute Charcot foot in Australian subjects. This study had a rigorous inclusion and exclusion criteria, sound HRFS protocols using objective measurements (e.g. dermal temperatures and medical imaging findings) for monitoring the progression and resolution of acute Charcot, and expert TCC plaster technicians who used the same application technique for each cast (Fig.
1).
Large, high-quality, prospective studies are required to confirm the findings of this study and those reported in previous literature [
2,
10,
11,
17‐
31]. Future research may be directed towards investigating TCC duration for:
(i)
removable (e.g. CROW, CAM walker) versus non-removable (e.g. TCC, iTCC) offloading devices for Charcot treatment, including an evaluation of treatment adherence (e.g. installing an accelerometer into a removable offloading device, as per a previous study [
53]);
(ii)
non diabetes-related Charcot neuroarthropathy;
(iii)
patients with/without diabetes or with varying diabetes duration and/or;
(iv)
different stages of Charcot foot.
There is also a need for longitudinal studies to evaluate adverse clinical outcomes, such as Charcot recurrence rates, development of contralateral Charcot, and rates of Charcot-related foot ulcers, infections and amputations.
Importantly, this study provides insight into the duration of TCC treatment for resolution of acute Charcot foot in Australian subjects, with comparisons made to the global body of evidence. Patient characteristics, Charcot foot presentations, TCC complications, factors affecting TCC duration, and post-TCC clinical outcomes have also been explored. The findings may provide recommendations and assist clinicians in relaying evidenced-based education for patients newly diagnosed with Charcot foot. Further, the findings may also assist Australian metropolitan settings (i.e. that follow a similar treatment protocol to the one described in this study) by developing HRFS patient pathways and expected resource requirements, clinical decision making for offloading treatment plans, managing patient expectations and goals, developing risk reduction plans, and improving overall adherence to TCC treatment for acute Charcot neuroarthropathy cases in HRFS throughout Australia. However, it is important to consider these findings and possible applications in the context of the study’s limitations, the variation of TCC treatment times between the current study and an existing Australian study [
31], and the broad TCC duration found in this study (IQR, 2.7 to 7.8 months).