Fibrosplasia Ossificans Progressiva
Fibrodysplasia ossificans progressiva is a genetic disorder that affects connective tissue. The main consequence of this disorder is heterotopic, the development of bony tissue in locations where bone is not present in a healthy body.
Such locations include the muscles,. The first symptoms of fibrodysplasia ossificans progressiva usually develop in childhood, and the disease progresses throughout the life of the individual. This is an extremely rare disorder with a global frequency of one person out of 2 million. Children who are born with fibrodysplasia ossificans progressiva appear normal in almost all respects. The single abnormality present in almost all cases is a deformity of the big toes, in which the toes are much shorter than normal and have a -like bony lump near the base of the toe. The presence of this toe abnormality at birth is considered a defining diagnostic characteristic of the disorder. Generally, progressive symptoms begin to appear as the child approaches adolescence.
The first symptoms are painful swellings that are exacerbated by injury or viral illnesses. Over time, swellings become more numerous, and existing swellings become harder as soft tissues gradually transform into bone. Joints stiffen, and movement becomes difficult and painful.
People with this condition gradually lose mobility as the disease progresses, and most require a wheelchair or other mobility aids by the third decade of life. Loss of mobility is not necessarily the most debilitating consequence of this disorder, because of the involvement of soft tissue in all parts of the body in addition to those involved in movement. For example, muscles and connective tissue in the chest wall can be disrupted as a result of bony growths. This can lead to acute or chronic.
The underlying cause of fibrodysplasia ossificans progressiva is a mutation in a gene called ACVR1, which codes for a protein known as receptor type-1. This mutation changes the shape of the receptor and causes it to malfunction.
As a result, injury to soft tissue causes bone to be deposited during the body’s repair process. This is why injury can not only cause the formation of new swellings but also exacerbate existing ones. Viral illness plays a role in the development of abnormal because the immune system causes inflammatory reactions that also can cause tissue damage. Fibrodysplasia ossificans progressiva is an incurable disorder, but certain medications can help reduce the rate of bone deposition in the body. The main medication used to achieve this is corticosteroids. A short course of high-dose corticosteroids can be administered when symptoms of the disorder flare up. By reducing in the body, this treatment can reduce the amount of bone deposition that occurs.
Other medications that might be used include painkillers and muscle relaxants, to reduce pain and muscle spasms. Could this condition be caused by a TBI or head injury (24 yrs old)? The doctors say that there is no pituitary damage after many tests.
Thyroid levels are a bit low, but not excessively low. Very low metabolism; sleep apnea. Foot growth 9.5 to 14 size shoe. Neck, wrists, hands, etc. Overall body/muscle growth; no fat tissue, total muscle. Not able to exercise.
Backs of legs/calf muscles extremely sore. Approximate weight 300 pounds from 190 lbs prior to accident. We have been to an excessive number of doctors and surgeons (neurologists, endocrinologists, orthopedic surgeons, etc. Over the last eight years.
Many forms of therapy and surgeries. We are very frustrated and discouraged.
Fibrodysplasia ossificans progressiva (FOP), a rare and disabling genetic condition of congenital skeletal malformations and progressive heterotopic ossification (HO), is the most catastrophic disorder of HO in humans. Episodic disease flare-ups are precipitated by soft tissue injury, and immobility is cumulative. Recently, a recurrent mutation in activin receptor IA/activin-like kinase 2 (ACVR1/ALK2), a bone morphogenetic protein (BMP) type I receptor, was reported in all sporadic and familial cases of classic FOP, making this one of the most highly specific disease-causing mutations in the human genome. The discovery of the FOP gene establishes a critical milestone in understanding FOP, reveals a highly conserved target for drug development in the TGF-β/BMP signalling pathway, and compels therapeutic approaches for the development of small molecule signal transduction inhibitors for ACVR1/ALK2.
Present management involves early diagnosis, assiduous avoidance of iatrogenic harm, and symptomatic amelioration of painful flare-ups. Effective therapies for FOP, and possibly for other common conditions of HO, may potentially be based on future interventions that block ACVR1/ALK2 signalling.
HISTORICAL DESCRIPTIONS OF FOP Possible cases of FOP date back to antiquity. FOP, known by many names throughout history, was first described in detail more than 250 years ago by a London physician. In a letter to The Royal Society of Medicine, dated 14 April 1736 (published in 1740), John Freke of Saint Bartholomew’s Hospital, London wrote: ‘There came a boy of healthy look, and about 14 years of age, to ask of us at the hospital, what should be done to cure him of many large swellings on his back, which began about 3 years since, and have continued to grow as large on many parts as a penny loaf particularly on the left side. They arise from all the vertebrae of the neck and reach down to the os sacrum; they likewise arise from every rib of his body, and joining together in all parts of his back, as the ramifications of coral do, they make as it were, a fixed bony pair of bodice’.
Nearly 200 years later in 1918, Jules Rosenstirn from Mount Zion Hospital in San Francisco, USA wrote: ‘One does not wonder that a disease, so baffling in its course from the first causes to its ultimate state, should invite the speculative as well as the patiently investigating observer to lift the obscuring veil and solve this embarrassing puzzle’. FOP was, until recently, one of medicine’s most elusive mysteries.
To patients who suffer from FOP, it is a painful metamorphosis into progressive immobility and a lifelong obstacle to physical freedom. While definitive treatments and cures are not yet available, the goals of FOP research are well articulated: to establish the genetic, molecular and cellular basis of FOP; and to use that knowledge to establish effective prevention, treatment and eventually cure. CLASSIC CLINICAL FEATURES OF FOP Two clinical features define classic FOP: malformation of the great toes; and progressive HO in specific spatial patterns. Individuals with FOP appear normal at birth except for the characteristic malformations of the great toes which are present in all classically affected individuals. During the first decade of life, children with FOP develop painful and highly inflammatory soft tissue swellings (or flare-ups) that transform soft connective tissues, including aponeuroses, fascia, ligaments, tendons and skeletal muscles, into an armament-like encasement of bone., Ribbons, sheets and plates of heterotopic bone replace skeletal muscles and connective tissues through a process of endochondral ossification that leads to permanent immobility.
– Minor trauma such as intramuscular immunizations, mandibular blocks for dental work, muscle fatigue and blunt muscle trauma from bumps, bruises, falls or influenza-like illnesses can trigger painful new flare-ups of FOP leading to progressive HO. – Surgical attempts to remove heterotopic bone commonly lead to episodes of explosive and painful new bone growth., HO in FOP progresses in characteristic anatomical and temporal patterns that mimic the patterns of normal embryonic skeletal formation.
FOP involvement is typically seen first in the dorsal, axial, cranial and proximal regions of the body and later in the ventral, appendicular, caudal and distal regions., Several skeletal muscles including the diaphragm, tongue and extra-ocular muscles are enigmatically spared from FOP. Cardiac muscle and smooth muscle are not involved in the FOP process. Characteristic clinical features of fibrodysplasia ossificans progressive (FOP).
(a) Extensive heterotopic bone formation typical of FOP is seen by three-dimensional reconstructed computed tomography scan of the back of a 12-year-old child. (b) Anteroposterior radiograph of the feet of a 3-year-old child shows symmetrical great toe malformations. Source: Shore et al. Nature Genet 2006; 38: 525–527. Copyright held by the authors. The clinical features of early lesional involvement in the axial regions are often different from those seen in the appendicular regions. Axial lesions may appear very rapidly, more rapidly than almost any neoplasm.
In the axial regions, swelling is often mistaken for tumours, as large bulbous lesions may appear on the neck and back, whereas in the limbs, the swelling is often diffuse and may be mistaken for acute thrombophlebitis; a complication that can occur in patients with FOP due to generalized immobility and associated venous stasis. The qualitative differences in swelling in the axial versus the appendicular regions in patients with FOP may reflect regional differences in the anatomy of the subaponeurotic spaces, as well as differences in the anatomy of the fascial compartments.
Bone formation in FOP is episodic, but disability is cumulative. Most patients with FOP are confined to a wheelchair by the third decade of life, and require lifelong assistance in performing activities of daily living. – Severe weight loss may result following ankylosis of the jaw, and pneumonia or right-sided heart failure may complicate rigid fixation of the chest wall. The severe disability of FOP results in low reproductive fitness, and fewer than 10 multigenerational families are known worldwide. The median age of survival is approximately 45 years, and death often results from complications of thoracic insufficiency syndrome (TIS). MISDIAGNOSIS OF FOP FOP is commonly misdiagnosed, as clinicians often fail to associate the rapidly developing soft tissue swellings that appear on the head, neck and upper back with the malformed great toes. The correct diagnosis of FOP can be made clinically even before radiographic evidence of HO is seen if rapidly waxing and waning soft tissue lesions are associated with symmetrical malformations of the great toes.
When such associations are not made, FOP is commonly misdiagnosed as aggressive juvenile fibromatosis (extra-abdominal desmoid tumours), lymphoedema or soft tissue sarcomas. Children often undergo unnecessary and harmful diagnostic biopsies that exacerbate progression of the condition. This can be particularly dangerous at any anatomical site, but especially so in the neck or back where asymmetric HO can lead to rapidly progressive spinal deformity and exacerbation of TIS.
CERVICAL SPINE ANOMALIES IN FOP In addition to malformations of great toes and thumbs, early developmental anomalies are frequently observed in the cervical spine. Stiffness of the neck is an early finding in most patients and can precede the appearance of HO at that site.
Characteristic anomalies of the cervical spine include large posterior elements, tall narrow vertebral bodies, and fusion of the facet joints between C2 and C7; findings that are strikingly similar to those seen in mice with homozygous deletions of the gene encoding noggin, a secreted bone morphogenetic protein antagonist. CARDIOPULMONARY FUNCTION IN FOP Patients with FOP develop TIS that can lead to life-threatening complications. Features contributing to TIS in patients with FOP include: costovertebral malformations with orthotopic ankylosis of the costovertebral joints; ossification of intercostal muscles, paravertebral muscles and aponeuroses; and progressive spinal deformity including kyphoscoliosis or thoracic lordosis.
Pneumonia and right-sided heart failure are the major life-threatening hazards that result from TIS in patients with FOP. Prophylactic measures to maximize pulmonary function, minimize respiratory compromise, and prevent influenza and pneumonia are helpful in decreasing the morbidity and mortality from TIS in patients with FOP., Assiduous attention should be directed towards the prevention and therapy of intercurrent chest infections. Such measures should include prophylactic pneumococcal pneumonia and influenza vaccinations (given subcutaneously), chest physiotherapy and prompt antibiotic treatment of early chest infection.
Upper abdominal surgery should be avoided if possible, as it interferes with diaphragmatic respiration. Sleep studies to assess sleep apnoea may be helpful, and positive pressure assisted breathing devices such as bipap masks without the use of supplemental oxygen may also be helpful. Patients with FOP who have advanced TIS and who use unmonitored oxygen have a high risk of sudden death. Sudden correction of oxygen tension in the presence of chronic carbon dioxide retention suppresses respiratory drive. Patients who have FOP and severe TIS should not use supplemental oxygen in an unmonitored setting.
Additional understanding of the complex chest wall dynamics in a true genetic model of FOP should greatly enhance understanding of the pathophysiology of these dreaded complications. RADIOGRAPHIC FEATURES OF FOP Joint malformations and soft tissue ossification are the characteristic radiographic features of FOP. Malformation of the great toes, thumbs, cervical spine and proximal femurs, along with the presence of proximal medial tibial osteochondromas, can make the diagnosis more certain. –, Radiographic and bone scan findings suggest normal modelling and remodelling of heterotopic bone., The incidence of fractures is not increased in patients with FOP, although fracture healing is characteristically accelerated in heterotopic bone. Bone scans are abnormal before HO can be detected by conventional radiographs. Computerized tomography and magnetic resonance imaging of early lesions have been described, but are superfluous., The definitive diagnosis of FOP can be made by simple clinical evaluation that associates progressively ossifying soft tissue lesions with malformations of the great toes., Clinical diagnosis of FOP can be confirmed by DNA diagnostic testing of the ACVR1 gene (see below). LABORATORY FINDINGS IN FOP Routine biochemical evaluations of bone mineral metabolism are usually normal, although serum alkaline phosphatase activity may be increased, especially during disease flare-ups., Urinary basic fibroblast growth factor levels may be elevated during disease flare-ups coinciding with the pre-osseous angiogenic phase of fibroproliferative lesions.
Fibrodysplasia Ossificans Progressive Imaging Center
Nephrolithiasis is more common in older patients with FOP, and may be due to increased immobilization and dehydration in the setting of generalized increased bone remodelling and mineral turnover. HISTOPATHOLOGY OF FOP LESIONS The histological stages of FOP lesions have been well described. – Early FOP lesions contain an intense perivascular B-cell and T-cell lymphocytic infiltrate. Subsequent migration of mononuclear inflammatory cells into affected muscle precedes widespread myonecrosis. Following a brief inflammatory stage, an intense fibroproliferative reaction associated with robust angiogenesis and neovascularity is noted., These early- to intermediate-stage lesions are microscopically indistinguishable from aggressive juvenile fibromatosis.
As the lesion matures, fibroproliferative tissue undergoes an avascular condensation into cartilage followed by a revascularization stage and osteogenesis in a characteristic process of endochondral ossification. The resultant HO is normal, histologically mature lamellar bone with marrow elements. – Mast cells have been identified at every histological stage, and are found in much greater abundance compared with normal skeletal muscle and non-lesional FOP muscle. In fact, during the intense fibroproliferative stage of the lesion, mast cells are found at a density much higher than in any other inflammatory myopathy. All stages of histological development are present in an active FOP lesion, indicating that different regions within the lesion mature at different rates.
Although heterotopic bone formation in FOP is similar in some respects to bone formation in embryonic skeletal development and postnatal fracture healing, important differences are the lack of inflammation in embryonic skeletal induction and the relative absence of lymphocytic inflammatory cells in early fracture healing. EPIDEMIOLOGIC, GENETIC AND ENVIRONMENTAL FACTORS IN FOP FOP is extremely rare with a worldwide prevalence of approximately one in two million. There appears to be no ethnic, racial, gender or geographic predisposition., Most cases arise as a result of a spontaneous new mutation. When observed, genetic transmission is autosomal dominant and can be inherited from either mothers or fathers., Both genetic and environmental factors affect the phenotype of FOP.
A study of three pairs of monozygotic twins with FOP found that within each pair, congenital toe malformations were identical. However, postnatal HO varied greatly depending on life history and environmental exposure. This study indicated that genetic determinants strongly influence disease phenotype during prenatal development, and that environmental factors strongly influence postnatal progression of HO. DISCOVERY OF THE FOP GENE In order to identify the chromosomal locus for the FOP gene, a conservative genome-wide linkage analysis was conducted using a subset of five families with the most stringent and unambiguous features of FOP. This approach identified linkage of FOP to 2q23–24. The gene encoding activin receptor IA (ACVR1) also known as activin-like kinase 2 (ALK2), a BMP type I receptor, was identified in the linkage interval. DNA sequencing of the ACVR1 gene determined that the same heterozygous mis-sense mutation in the glycine–serine (GS) activation domain (c.617GA;R206H) occurs in all classically affected individuals examined.
The discovery of the FOP gene was the culmination of a monumental 15-year search. PROTEIN MODELLING OF THE FOP MUTATION ACVR1/ALK2 is a BMP type I receptor, and protein structure homology modelling of the recurrent mutation predicts destabilization of the GS domain, consistent with an overactive BMP signalling pathway as the underlying cause of the ectopic chondrogenesis, osteogenesis and joint fusion seen in FOP. This mutation is consistent with a wealth of previous findings of an overactive BMP signalling pathway in FOP cells, and provides a rational basis for understanding both the postnatal HO and the congenital skeletal malformations that are ignominious signatures of this devastating disease. Hypothetical protein structure models are being developed to understand both inter-and intramolecular interactions of the mutant receptor. The GS domain of all TGF-β/BMP type I receptors is a critical site for binding and activation of pathway-specific Smad signalling proteins, and is a binding site of FKBP12, an inhibitory protein that prevents leaky activation of the type I receptor in the absence of ligand., FKBP12 also recruits a Smad7-Smurf1 ubiquitin ligase that functions normally to regulate the abundance of the receptor at the membrane. Both leaky activation of BMP signalling and accumulation of BMP type I receptors at the cell membrane are seen in FOP cells, suggesting possible aberrant association with FKBP12 in FOP. The most likely possibility is that FKBP12 interactions with the GS domain become altered, leading to promiscuous ACVR1/ALK2 activity.
However, exactly how the R206H mutation in ACVR1/ALK2 specifically perturbs BMP signalling in FOP remains undetermined but could involve dysregulation of BMP receptor oligomerization, internalization, degradation and/or activation of downstream signalling. This is presentlythe subject of intense investigation. Hypothetical schema of bone morphogenetic protein (BMP) signalling in fibrodysplasia ossificans progressiva (FOP) cells. In control cells (A), in the absence of ligand, the Smad/Smurf-FKBP12 (SM-FKBP12) complex binds activin receptor IA (ACVR1; a BMP type I receptor) and prevents its promiscuous phosphorylation by the constitutively active type II BMP receptor (not shown). SM-FKBP12 also promotes ubiquitin-associated degradation of ACVR1 in the absence of ligand, thus maintaining low steady-state levels of ACVR1 at the cell membrane. Following ligand binding in control cells (B), SM-FKBP12 dissociates from ACVR1, thus allowing the constitutively active BMP type II receptor (not shown) to phosphorylate ACVR1, and promote Smad 1, 5 and8 phosphorylation and downstream BMP signalling. In FOP cells, SM-FKBP12 does not appear to bind appropriately to the mutant receptor ACVR1 (R206H).
Thus, inhibition of BMP signalling is impaired in the absence of ligand, and basal leakiness of BMP signalling occurs (C). Additionally, it is suspected that since the SM-FKBP12 complex cannot properly target the mutant ACVR1 (R206H) receptor for ubiquitin-associated degradation, ACVR1 may be expected to accumulate at the cell surface. Thus, in the presence of ligand (D), hyper-responsive BMP signalling may be predicted to occur. Arrows, signalling promoted; blunt-end lines, signalling inhibited; lock, SM-FKBP12 binding to ACVR1; dashed lines, SM-FKBP12 binding to ACVR1 impaired; open cups, extracellular ligand-binding domain of ACVR1; filled-in circles, BMP ligand; filled-in circles inside open cups, BMP ligand binding to ACVR1. ACVR1/ALK2: A DRUGGABLE TARGET FOR THE SECOND SKELETON The ultimate goal of FOP research is the development of treatments that will prevent, halt or even reverse progression of the condition. The prevention and treatment of HO in FOP, as for any of the more common forms of HO, will be based on at least one of four principles: disrupting the relevant inductive signalling pathways; suppressing the immunological and/or inflammatory triggers; altering the relevant osteoprogenitor cells in the target tissues; and/or modifying the tissue environment conducive to heterotopic osteogenesis. The discovery of the FOP gene identifies ACVR1/ALK2 as a specific druggable target for FOP.
The identification of the recurrent heterozygous mis-sense point mutation that causes FOP in all classically affected individuals provides a specific druggable target and a rational point of intervention in a critical signalling pathway. Plausible therapeutic approaches to inhibiting BMP signalling in FOP include inhibitory RNA technology, monoclonal antibodies directed against ACVR1/ALK2, and (most plausibly) orally available small molecule selective signal transduction inhibitors (STIs) of ACVR1/ALK2. Small molecule STIs have proven to be invaluable for investigating signal transduction pathways. Such molecules also have the potential for development into powerful therapeutic agents. The development of specific STIs for promiscuous ACVR1/ALK2 signalling in FOP have the potential to modify the natural history of the disease. Residues close to the ATP-binding site of ACVR1/ALK2 could be exploited to achieve selectivity, even among closely related receptor serine threonine kinases such as ALK3 (BMPRIA) and ALK6 (BMPRIB). Small soluble molecule inhibitors designed to specifically block ACVR1/ALK2 signalling intracellularly will need to be designed, screened and tested in cell and animal models of FOP.
ACVR1/ALK2 STIs will need to have sufficient efficacy, tolerance to resistance, and acceptable safety profiles. Selective inhibitors have been developed for the ALKs that signal through Smads 2 and 3 ALK4, 5 (TβRI) and 7. At the present time, there are no known selective inhibitors of ACVR1/ALK2 or the other three BMP pathway type I receptors (ALK 1, 3 and 6) that signal through the BMP-pathway-specific Smads 1, 5 and 8.
Such selective inhibitors are desperately needed. ANIMAL MODELS OF FOP Animal models of FOP will be important for understanding the pathophysiology of FOP and for testing possible therapies. Laboratory-generated animal models with some features of FOP have provided the opportunity to better understand the biology of HO and to study the effectiveness and safety of currently available and emerging therapies. Development of a knock-in mouse model carrying the specific FOP-disease-causing mutation in ACVR1/ALK2 will be necessary to establish specificity of treatment in FOP. Such a genetically engineered knock-in mouse is presently being developed. CURRENT MANAGEMENT OF FOP The rarity, variable severity and episodic clinical course of FOP pose substantial uncertainties when evaluating experimental therapies.
Accordingly, medical intervention is currently supportive. Surgical release of joint contractures is generally unsuccessful and risks new, trauma-induced HO.
Osteotomy of heterotopic bone or surgical removal of heterotopic bone to mobilize joints is generally counterproductive because additional HO develops at the operative site. Rarely, a joint may be repositioned surgically to improve the patient’s overall functional status. Spinal bracing is ineffective and surgical intervention is associated with numerous complications. Guidelines for symptomatic management of disease flare-ups have been published, and highlight the anecdotal utility of glucocorticoids in managing new flare-ups affecting the function of major joints in the appendicular skeleton. Non-steroidal anti-inflammatory medications, cyclo-oxygenase-2 inhibitors, leukotriene inhibitors and mast cell stabilizers are useful anecdotally in managing chronic discomfort and ongoing flare-ups, but to date there is no proven efficacy with any therapy in altering the natural history of the disease.
A recent report documented the failure of bone marrow transplantation to cure the condition, but suggested that chronic immunosuppression may have some utility, although its general use is not recommended. ANAESTHESIA IN PATIENTS WITH FOP General anaesthesia is particularly dangerous in patients with FOP. Guidelines for general anaesthesia have been reported. Overstretching of the jaw for intubation may cause additional trauma to the TMJs, and lead to disease flare-ups. In older patients whose TMJs are ankylosed, oral access for intubation may not be possible. General anaesthesia in FOP patients should be accomplished through an awake fibre-optic nasal intubation under light sedation so that the patient can control secretions.
This should be performed by well-trained anaesthesia teams who are familiar and experienced with this type of procedure. THE INTERNATIONAL FOP ASSOCIATION The International FOP Association (IFOPA) was founded in June 1988 to educate patients, doctors and the public about FOP; to support medical research into FOP; and to support patients with FOP and their families by providing a network of communication to help end the isolation that accompanies this rare and severely disabling condition. Additional information can be found on the IFOPA website. In recent years, many regional FOP organizations have arisen worldwide to support patient-related activities. RESEARCH AGENDA AND SUMMARY While the mutation that causes classic FOP has been discovered, much work remains to elucidate the molecular mechanism by which this mutation leads to the complex disease phenotype of skeletal malformations and episodic progression of HO.
It will be essential to fully understand the role of the inflammatory pathways in triggering flare-ups of the disease, and to better understand the interaction of the immune system with the as-yet-unidentified connective tissue progenitor cells that are mobilized by disease flare-ups. Additionally, the molecular micro-environment in which HO develops needs to be more fully understood in the context of the disease-causing mutation that underlies the pathophysiology of the episodic flare-ups.
The critical relationships between the mutant receptor, the environmental triggers, the responsive stem cells and the micro-environmental niches in which this renegade skeletal metamorphosis takes place will be vitally important to understand in order to design and develop the most effective treatment and prevention strategies. Accurate and clinically available premonitory markers of FOP flare-ups are desperately needed to assess potential therapies. All of these important goals, and of course the ultimate goal of using this knowledge to develop better treatments and eventually a cure, will require the development of relevant cell and animal models. Practice points This very brief guide will summarize the current symptomatic management of FOP. Activities: avoid soft tissue injuries, contact sports, overstretching of soft tissues and muscle fatigue.
Avoid biopsies, surgical removal of heterotopic bone and all non-emergent surgical procedures Anaesthesia: if general anaesthesia is required, perform awake intubation by nasotracheal fibre-optic technique Falls: locked upper limbs may accentuate head trauma from falls. Epidural haematomas are common (surgical emergency). Use protective headgear in children who have upper limb involvement Flare-up (back/chest): use non-steroidal anti-inflammatory medications with gastrointestinal precautions. Use analgesics and/or muscle relaxants, as needed Flare-up (limbs/throat): prednisone – 2 mg/kg PO once daily for 4 days; begin within first 24 h of flare-up. Keep medication on-hand for emergencies. Use analgesias and/or muscle relaxants, as needed, with gastrointestinal precautions Flare-ups (protection): most flare-ups result from over-use and soft tissue injuries.
Prednisone 2 mg/kg PO once daily for 3 days to prevent flare-up after severe soft tissue injury. Do not use after minor bumps or bruises Hearing: conductive hearing impairment is common. Perform periodic audiology evaluations. Hearing aids may improve conductive hearing loss Immunizations: avoid all intramuscular immunizations.
Subcutaneous immunizations are acceptable when FOP is quiescent. Avoid any immunizations during flare-ups Influenza: administer influenza vaccines subcutaneously, but never during flare-ups. Avoid live attenuated flu vaccine; it may cause flu-like symptoms and exacerbate FOP. Household contacts of FOP patients should be immunized annually. IVs: superficial IV access and venepuncture is acceptable.
Traumatic IVs and arterial punctures may cause HO Limb swelling: lymphoedema and transient neuropathy may occur with flare-ups of limbs. Elevate legs while sleeping and recumbent. Use support stockings.
Take one baby aspirin daily with food. Rule-out deep vein phlebitis with Doppler ultrasound Occupational therapy: perform periodic occupational therapy evaluations as activities of daily living change Physiotherapy: avoid passive range of motion. Warm water hydrotherapy may be helpful Pulmonary function: perform baseline pulmonary function tests and echocardiogram. Repeat periodically. Supplemental oxygen should not be used in an unmonitored setting School: use school aides to protect and assist children.
Request medical letter and preschool evaluation Surgery: avoid surgery, except in emergencies Teeth: avoid mandibular blocks, overstretching of the jaw and muscle fatigue. Contributor Information Frederick S. Kaplan, Departments of Orthopedic Surgery & Medicine, The University of Pennsylvania School of Medicine, c/o Hospital of The University of Pennsylvania, Philadelphia, PA, USA. Martine Le Merrer, U781 INSERM, Hopital Necker-Enfants Malades, Paris, France.
Glaser, Department of Orthopedic Surgery, The University of Pennsylvania School of Medicine, c/o Hospital of the University of Pennsylvania, Philadelphia, PA, USA. Pignolo, Department of Medicine, The University of Pennsylvania School of Medicine, Philadelphia, PA, USA. Robert Goldsby, Department of Pediatrics and Cardiovascular Research Institute, The University of California San Francisco, San Francisco, CA, USA. Kitterman, Department of Pediatrics and Cardiovascular Research Institute, The University of California San Francisco, San Francisco, CA, USA. Jay Groppe, Department of Biochemistry, University of Texas Health Science Center at San Antonio, San Antonio, TX, USA. Shore, Departments of Orthopedic Surgery and Genetics, The University of Pennsylvania School of Medicine, Philadelphia, PA, USA.