Cavovarus With a Twist: Midfoot Coronal and Axial Plane Rotational Deformity in Charcot-Marie-Tooth Disease

Background: The cavovarus deformity of Charcot-Marie-Tooth (CMT) disease is often characterized by a paradoxical relationship of hindfoot varus and forefoot valgus. The configuration of the midfoot, which links these deformities, is poorly understood. Accurate assessment of 3-dimensional alignment under physiologic loadbearing conditions is possible using weightbearing computed tomography (WBCT). This is the first study to examine the rotational deformity in the midfoot of CMT patients and, thus, provide key insights to successful correction of CMT cavovarus foot. Methods: A total of 27 WBCT scans from 21 CMT patients were compared to control WBCTs from 20 healthy unmatched adults. CMT patients with a history of bony surgery, severe degenerative joint disease, or open physes in the foot were excluded. Scans were analyzed using 3-dimensional software. Anatomic alignment of the tarsal bones was calculated relative to the anterior-posterior axis of the tibial plafond in the axial plane, and weightbearing surface in the coronal plane. Results: Maximal rotational deformity in CMT patients occurred at the transverse tarsal joints, averaging 61 degrees of external rotation (supination), compared to 34 degrees among controls ( P < .01). The talonavicular joint was also the site of peak adduction deformity in the midfoot, with an average talonavicular coverage angle measuring 12 degrees compared with −11 degrees in controls ( P < .01). Conclusion: This 3-dimensional WBCT analysis is the first to isolate and quantify the multiplanar rotational deformity in the midfoot of CMT patients. Compared with healthy unmatched control cases, CMT patients demonstrated increased axial plane adduction and coronal plane rotation at the talonavicular (TN) joint. These findings support performing soft tissue release at the TN joint to abduct and derotate the midfoot as a first step for targeted deformity correction. Level of Evidence: Level III, retrospective case-control study.

Bilateral Multiple Tarsal Coalitions (Talonavicular and Talocalcaneal Coalitions) with Recurrent Ankle Sprain in an Adolescent

Tarsal coalition is defined as an abnormal bony, cartilaginous, or fibrous union of two or more tarsal bones. The incidence of tarsal coalition is approximately 2% in the general population. Talocalcaneal and calcaneonavicular coalitions are the most common. The talonavicular coalition is a rare entity with an incidence of approximately 1.3% among patients with tarsal coalitions. We present a case of a 12-year-old girl who had talonavicular and talocalcaneal coalitions associated with a recurrent ankle sprain. The talonavicular coalition was asymptomatic, and the talocalcaneal coalition was the cause of ankle pain and recurrent sprain. Surgical resection of the talocalcaneal coalition led to successful clinical and functional outcomes. In conclusion, the possibility of multiple tarsal coalitions should be considered in tarsal coalition patients, and the talocalcaneal coalition should be considered as a differential diagnosis in an adolescent patient with a recurrent ankle sprain.

Morphometric Measurements of Talus in South Keralites

BACKGROUND The posterior half of the foot is made of seven tarsal bones. Talus is seen above calcaneus. It has a head, neck and body. There are three facets anterior, middle and posterior facets that articulate with corresponding facets of the calcaneus. The middle and posterior facets are separated by a groove sulcus tali. We wanted to know the morphometric measurements of talus in South Keralites in this study. METHODS The study was done on 68 dry human tali of unknown age and sex in the Department of Anatomy, Government medical college, Trivandrum. The measurements were taken i.e., length, width and height of talus using vernier calipers. The length, width and height of sulcus tali were also measured. The range and mean of measurements were estimated. The calcaneal facets were studied and classified to find the most common and least common types. Data analysis was performed using SPSS ver 16.0. RESULTS The mean anteroposterior length of the talus was 4.84 ± 0.44 cm. The mean transverse length was 3.46 ± 0.47 cm. The mean height of the talus was 2.56 ± 0.31 cm. Anteroposterior length ranged from 3.84 to 6.07. The transverse length of the talus ranged from 2.81- 5 cm. Height of talus ranged from 2 - 3.2 cm. The mean anteroposterior length of sulcus tali was 2.09 ± 0.45 cm. The mean height of sulcus tali was 0.55 ± 0.09 cm. The mean width of sulcus tali was 0.62 ± 0.30 cm. Anteroposterior length of sulcus tali ranged from 1.4 - 3.8 cm. The transverse length of sulcus tali ranged from 0.34 to 1.6 cm. Height of sulcus tali ranged from 0.2 to 0.7 cm, regarding the type of facets, type 2 was most common and type 4 was found to be absent. CONCLUSIONS The adequate knowledge of the anatomy of the talus is significant not only to the anatomists but also to the orthopaedic surgeons as fractures of the talus are quite common and lead to avascular necrosis, arthritis and when unrecognized, chronic pain and non-union 3. Talectomy has been described as a limb-saving procedure for the treatment of neglected talipes equinovarus deformity. KEY WORDS Talus, Sulcus Tali, Calcaneal Facet Morphometric Measurements of Talus in South Keralites.

Multicentric Carpo-Tarsal Osteolysis Syndrome Mimicking Juvenile Idiopathic Arthritis: Two Case Reports and Review of the Literature

Multicentric carpo-tarsal osteolysis syndrome (MCTO) is a rare skeletal disorder commonly caused by MAF bZIP transcription factor B (MAFB) mutation. Clinically, it is characterized by aggressive osteolysis, which mainly affects the carpal tarsal bones, and is frequently associated with progressive nephropathy. Since the painful swelling and motion limitation on the wrists and/or ankles of MCTO mimics those of juvenile idiopathic arthritis (JIA), very often, MCTO is misdiagnosed as JIA. Here, we report two MCTO patients initially diagnosed with JIA but showed no response to treatment: P1, with a medical history of more than 10 years, was presented with a typical triad of arthritis-osteolysis-nephropathy; while P2 showed oligoarthritis. Gene tests were then taken and revealed a novel mutation, p.P63Q, and a previously reported conversion, p.S54L, in the MAFB gene. We also summarized the clinical and genetic features of a cohort containing 49 genetically confirmed MCTO patients. All 51 gene-confirmed MCTO cases (49 identified from the literature plus two patients identified herein) developed the disease during childhood. The median delay in diagnosis was 3.83 years (0–35 years). All cases presented bony lesions, and two-thirds had secondary renal lesions (32/48; three unknown), half of which (16/32) progressed into renal failure. Almost two-thirds (34/51), 75% (38/51), and 71% (36/51) of patients had no record of eye problems, facial abnormalities, and other manifestations. Most were misdiagnosed as JIA but didn't respond to treatment. Based on our experience, we suggest that clinicians should comprehensively evaluate the involvement of multiple systems in JIA patients, especially the kidney and eyes. And for JIA patients who underwent more than 3-month treatment with Bio-DMARD, genetic tests are recommended when they show little/no clinical and imaging changes, their high disease activity remains, and their disease activity remission is &lt;50%, especially when combined with a triad of arthritis-osteolysis-nephropathy.

O18 When joints vanish

Case report - Introduction Paediatric rheumatology is an interesting speciality. Exact characterisation of juvenile idiopathic arthritis (JIA) and other autoinflammatory conditions still remains a grey area in rheumatology. To add to the confusion, a horde of heritable and acquired conditions can mimic these diseases, making diagnosis a real challenge. Idiopathic multicentric carpotarsal osteolysis syndrome (MCTO) is a rare skeletal disorder characterised by aggressive osteolysis, predominantly carpal and tarsal bones. The early clinical presentation is joint pain, and can mimic polyarticular JIA. Progressive nephropathy in latter stages is a known association. Genetic tests helps in early diagnosis of MCTO. Case report - Case description A 17-year-old male was managed as polyarticular JIA since the age of 1.5 years. He was the first child of healthy nonconsanguinous Sri Lankan parents. His prenatal and perinatal periods were uncomplicated. His development was unremarkable until joint symptoms evolved. The family history was insignificant for any bone disorder. He was on long-term methotrexate and approximately 15 monthly tocilizumab infusions but to no avail. His distinctive facial features included cloudy cornea and subtle facial dysmorphism such as maxillary hypoplasia. Upper limb deformities included shortening of arms and forearms, fixed flexion deformity of the left elbow joint and distorted and grossly swollen wrists. Deformities of the lower extremities included short thighs and short bowed legs. A painful limp on the right was observed. His inflammatory markers were persistently normal. His initial investigations revealed moderate proteinuria without renal impairment. Serum electrolytes, bone profile, ALP and PTH was unremarkable. This clinical case was revised due to the apparent resistance to treatment and uncharacteristic limb deformities. A skeletal survey was performed. Radiographic examination revealed disappearing carpal and tarsal bones as well as disappearing long bone ends, compatible with a diagnosis of idiopathic multicentric osteolysis. The characteristic 'sucked candy' apperance of metacarpals was appreciated. In addition, severe cortical thinning of all bones indicating osteopenia was observed. He was also noted to have proteinuria and was referred to the nephrologists for further evaluation. The adolescent was taken off all immunosuppressive therapy without any clinical worsening. Given the limited evidence for treatment strategies, he was initiated on a trial of oral bisphosphonates. He responded well to treatment symptomatically, as pain gradually subsided. He was further referred for rehabilitation. Genetic test for MAFB seqeuencing (V-maf musculoaponeurotic fibrosarcoma oncogene homolog B) was not performed due to unavailability. This clinical case further directed us to diagnose multicentric carpo-tarsal osteolysis in two more children who were initially managed for JIA and had poorly responded to immunosuppressive therapies. Case report - Discussion We report the challenges in diagnosing a mimicker of JIA, where awareness of the rare syndrome and high index of suspicion plays a pivotal role in the diagnosis of the condition, especially in the absence of genetic testing due to resource-poor settings. MCTO, is a rare osteolytic condition largely of unknown etiology. The syndrome manifests with progressive loss of carpal and tarsal bones in childhood. Affected children have arthritic-like episodes, followed by progressive deformities, radiographic osteolytic changes, and variable degrees of disability. There are many different types of osteolytic syndromes with overlapping features and it may have a familial inheritance. Clinical symptoms and signs occur early in childhood. They present with multiple bone and joint pains, and bony 'dysplasia' associated with reduced range of joint movements and functions. Our patient initially presented at the age of 2 years with features mimicking polyarticular JIA and these deformities developed gradually and were not noticed until adolescent stage. Fragmentation, lysis and eventual disappearance of the distal ends of long bones, carpal and tarsal bones, is the hallmark feature. Studies demonstrate the presence of localised osteoclastic activity adjacent to osteolytic areas. Radiological investigations help aid in diagnosis. The findings include characteristic osteolytic changes. Serological and histological investigations are always negative for classical inflammatory or autoimmune causes. Described associations include protein losing nephropathy due to underlying focal segmental glomerulosclerosis, cloudy cornea and subtle facial dysmorphisms such as triangular face, maxillary hypoplasia and micrognathia. Genetic testing has revealed possible MAFB mutations associated in MCTO. Treatment with traditional anti-inflammatory drugs, conventional DMARDS, and biological therapies do not have any effect on the pain, progression of the diseases or the deformities caused. Bisphosphonates are beneficial in improving acute pain, and bone mineral density in MCTO. This clinical case teaches us to think outside the box and to revisit diagnosis for better patient outcome. Case report - Key learning points JIA is a clinical diagnosis with a wide spectrum of differential diagnosis. Accurate diagnosis relies on clinical judgement. JIA mimics constitute a pitfall to even the most experienced clinician. Atypical features such as persistently normal inflammatory markers, relative lack of pain or activity limitation despite swollen joints, should alert the physician to alternative diagnosis such as multicentric carpo-tarsal osteolysis. Having a good knowledge about potential JIA mimics would help avoid unnecessary immunosuppression. MCTO is a rare skeletal dysplasia which needs a high index of suspicion for diagnosis. Many questions still remain unanswered in this condition. Further research is needed to understand whether a high bone turnover is specific to MAFB gene mutation and if MCTO may represent a form of idiopathic juvenile osteoporosis in which short bones are more severely affected than long bones.

Multicentric Carpotarsal Osteolysis Syndrome in a Mother and Daughter with a MAFB Missense Variant and Natural History of the Disease

Multicentric carpotarsal osteolysis syndrome (MCTO; MIM #166300) is a rare skeletal disorder characterized by osteolysis affecting particularly the carpal, metacarpal, and tarsal bones, although other bones might be involved. MCTO is an autosomal dominant disease caused by heterozygous variants in the <i>MAFB</i> gene, frequently misdiagnosed as juvenile rheumatoid arthritis due to similar clinical manifestations. This study reports the first Brazilian family diagnosed with MCTO with progressive osteolysis of the carpal and tarsal bones, presenting a c.161C&#x3e;T (p.Ser54Leu) heterozygous variant in the <i>MAFB</i> gene, describing the clinical, radiological, and molecular findings, compared with literature data, and discussing the different clinical and molecular diagnosis, as well as the natural history of the disease. Since MCTO is a disorder with progressive symptoms, an early diagnosis is important to avoid unnecessary investigations and treatments and to provide the proper follow-up.

Treatment of Cleft Foot Deformity using Fish Mouth Incision and Suture-Button in Paediatric Foot

Cleft foot is a congenital anomaly characterized by absence of the metatarsal bones and phalanges. It is commonly seen in children with Ectrodactyly-ectrodermal dysplasia and clefting syndrome (EEC) ranging from a median cleft up to the mid metatarsals to a deep cleft up to the tarsal bones. Surgical treatment in the form of cleft closure, excision of the rudimentary metatarsal bone and cross K-wire fixation of metatarsal bones have been tried for the management of such cases. Here, we report a case of one year old child with Type III cleft foot having four metatarsals, who was treated with suture-endobutton system using three transverse tunnels in the 2nd and 3rd metatarsal bones in order to bring them closer. We were able to achieve a satisfactory outcome with a normal fitting shoe wear. Keywords: Cleft foot; suture-button; fish mouth incision.

Finite element analysis of the kinematic coupling effect of the joints around talus when Ponseti manipulation

Background Little information was obtained from the published papers about the kinematic coupling effect between tarsal bones during Ponseti manipulation. The aim was to explore the kinematic coupling effect of the joints around talus, to investigate the kinematic rhythm and coupling relationship of tarsal joints; to clarify the pulling effect on medial ligament of the ankle during the process of Ponseti manipulation. Methods The model of foot and ankle was reconstructed from the Chinese digital human girl No.1 (CDH-G1) image database. Finite element analysis was applied to explore the kinematic coupling effect of the joints around talus. The distal tibia and fibula bone and the head of talus were fixed in all six degrees of freedom; outward pressure was added to the first metatarsal head to simulate the Ponseti manipulation. Kinematic coupling of each tarsal joint was investigated using the method of whole model splitting, and medial ligament pulling of the ankle was studied by designing the model of medial ligament deletion during the Ponseti manipulation. Results All the tarsal joints produced significant displacement in kinematic coupling effect, and the talus itself produced great displacement in the joint of ankle. Quantitative analysis revealed that the maximum displacement was found in the joints of talonavicular (12.01mm), cuneonavicular (10.50mm), calcaneocuboid (7.97mm), and subtalar(6.99mm).The kinematic coupling rhythm between talus and navicular, talus and calcaneus, calcaneus and cuboid, navicular and cuneiform 1 were 1:12, 1:7, 1:2 and 1:1.6. The results of ligaments pulling showed that the maximum displacement was presented in the ligaments of tibionavicular (mean 27.99mm), talonavicular (21.03mm), and calcaneonavicular (19.18 mm). Conclusions All the tarsal joints around talus were involved in the process of Ponseti manipulation, and the strongest kinematic coupling effect was found in the joints of talonavicular, subtalar, calcaneocuboid, and cuneonavicular. The ligaments of tibionavicular, talonavicular, and calcaneonavicular were stretched greatly. It was suggested that the method of Ponseti management was a complex deformity correction processes involved all the tarsal joints. The present study contributed to better understanding the principle of Ponseti manipulation and the pathoanatomy of clubfoot. Also, the importance of cuneonavicular joint should be stressed in clinical practice.