Camurati-Engelmann Disease
Summary
Clinical characteristics.
Camurati-Engelmann disease (CED) is characterized by hyperostosis of the long bones and the skull, proximal muscle weakness, limb pain, a wide-based, waddling gait, and joint contractures. Facial features such as macrocephaly, frontal bossing, enlargement of the mandible, proptosis, and cranial nerve impingement resulting in facial palsy are seen in severely affected individuals later in life.
Diagnosis/testing.
The diagnosis of CED is established in a proband with the characteristic radiographic findings or (if radiographic findings are inconclusive) on identification of a heterozygous pathogenic variant in TGFB1 by molecular genetic testing.
Management.
Treatment of manifestations: Corticosteroid therapy as needed to control symptoms; losartan may be a helpful adjuvant therapy to minimize the need for steroids to control pain. Pain is also managed with analgesics and non-pharmacologic methods. Craniectomy may be needed to reduce intracranial pressure and relieve symptoms in individuals with several cranial sclerosis. Bilateral myringotomy can improve conductive hearing loss resulting from serous otitis.
Prevention of secondary complications: Monitor blood pressure in individuals treated with corticosteroids and treat hypertension if necessary; individuals taking losartan also need regular blood pressure monitoring due to the increased risk for hypotension; taper corticosteroid dose as tolerated to reduce the risk of osteoporosis and compression fractures of the spine.
Surveillance: Following initiation of corticosteroid treatment, blood pressure should be monitored monthly; when maintenance steroid dose is achieved, yearly evaluation includes complete neurologic examination, CBC, blood pressure, audiology evaluation, ophthalmology evaluation, and bone density scan; routine monitoring of linear growth in children due to the possible side effect of delayed or stunted growth; individuals with cranial hyperostosis (including those treated surgically) should continue to be monitored for signs and symptoms of increased intracranial pressure.
Genetic counseling.
CED is inherited in an autosomal dominant manner. Penetrance is reduced. The incidence of de novo pathogenic variant is unknown. Each child of an individual with CED has a 50% chance of inheriting the TGFB1 pathogenic variant. Prenatal testing for a pregnancy at increased risk and preimplantation genetic testing are possible for families in which the pathogenic variant has been identified.
Diagnosis
There are no current published guidelines for the diagnosis of Camurati-Engelmann disease.
Suggestive Findings
Camurati-Engelmann disease (CED) should be suspected in individuals with the following clinical findings:
- Proximal muscle weakness
- Limb pain
- Waddling gait
Establishing the Diagnosis
The diagnosis of CED is established in a proband with the characteristic radiographic findings or, if radiographic findings are inconclusive, on identification of a heterozygous pathogenic variant in TGFB1 by molecular genetic testing (Table 1).
Radiographic findings
- Hyperostosis of one or more of the long bones:
- Begins with the diaphyses of the long bones
- Can progress to the metaphyses and (in rare cases) epiphyses
- Periosteal involvement with uneven cortical thickening and increased diameter
- Endosteal bony sclerosis that can lead to narrowed medullary canal
- Hyperostosis usually symmetric in the appendicular skeleton but in some cases asymmetricNote: Hyperostosis does not affect the spine.
- Other radiologic findings variably seen:
- Skull involvement beginning at the base of the anterior and middle fossae and often including the frontal bone [Wallace et al 2004]
- Mild osteosclerosis in the posterior neural arch of the spine and parts of the flat bones that correspond to the diaphysis
Molecular genetic testing approaches can include single-gene testing, use of a multigene panel, and more comprehensive genomic testing.
- Single-gene testing. Sequence analysis of TGFB1 is performed.Note: CED is postulated to occur through a gain-of-function mechanism. Large intragenic deletions or duplications have not been reported in individuals with CED; testing for intragenic deletions or duplication is not indicated.
- A multigene panel that includes TGFB1 and other genes of interest (see Differential Diagnosis) may be considered. Note: (1) The genes included in the panel and the diagnostic sensitivity of the testing used for each gene varies by laboratory and are likely to change over time. (2) Some multigene panels may include genes not associated with the condition discussed in this GeneReview; thus, clinicians need to determine which multigene panel is most likely to identify the genetic cause of the condition at the most reasonable cost while limiting identification of variants of uncertain significance and pathogenic variants in genes that do not explain the underlying phenotype. (3) In some laboratories, panel options may include a custom laboratory-designed panel and/or custom phenotype-focused exome analysis that includes genes specified by the clinician. (4) Methods used in a panel may include sequence analysis, deletion/duplication analysis, and/or other non-sequencing-based tests.For an introduction to multigene panels click here. More detailed information for clinicians ordering genetic tests can be found here.
- More comprehensive genomic testing (when available) including exome sequencing and genome sequencing may be considered. Such testing may provide or suggest a diagnosis not previously considered (e.g., mutation of a different gene or genes that results in a similar clinical presentation). For an introduction to comprehensive genomic testing click here. More detailed information for clinicians ordering genomic testing can be found here.
Table 1.
Gene 1 | Method | Proportion of Probands with a Pathogenic Variant 2 Detectable by Method |
---|---|---|
TGFB1 | Sequence analysis 3 | >90% 4 |
Gene-targeted deletion/duplication analysis 5 | Unknown 6 | |
Unknown 7 | NA |
- 1.
See Table A. Genes and Databases for chromosome locus and protein.
- 2.
See Molecular Genetics for information on allelic variants detected in this gene.
- 3.
Sequence analysis detects variants that are benign, likely benign, of uncertain significance, likely pathogenic, or pathogenic. Variants may include small intragenic deletions/insertions and missense, nonsense, and splice site variants; typically, exon or whole-gene deletions/duplications are not detected. For issues to consider in interpretation of sequence analysis results, click here.
- 4.
The majority are missense variants in exon 4 leading to single amino acid substitutions in the encoded protein [Janssens et al 2000, Kinoshita et al 2000, Campos-Xavier et al 2001, Hecht et al 2001, Mumm et al 2001, Janssens et al 2003, Kinoshita et al 2004, Wallace et al 2004, Janssens et al 2006].
- 5.
Gene-targeted deletion/duplication analysis detects intragenic deletions or duplications. Methods used may include quantitative PCR, long-range PCR, multiplex ligation-dependent probe amplification (MLPA), and a gene-targeted microarray designed to detect single-exon deletions or duplications.
- 6.
No data on detection rate of gene-targeted deletion/duplication analysis are available.
- 7.
The affected members of one family with CED did not share marker haplotypes at the TGFB1 locus and had no sequence alterations in TGFB1 exons 1 through 7; deletion/duplication analysis was not done on these individuals [Hecht et al 2001]. Several additional individuals with CED have not had TGFB1 pathogenic variants identified, implying genetic locus heterogeneity [Author, personal observation].
Clinical Characteristics
Clinical Description
Individuals with Camurati-Engelmann disease (CED) present with limb pain, proximal muscle weakness, poor muscular development, a wide-based, waddling gait, easy fatigability, and headaches. The average age of onset of symptoms in the 306 reported individuals is 13.4 years [Carlson et al 2010] with a range from birth to age 76 years [Wallace et al 2004].
Musculoskeletal. Decreased muscle mass and weakness are most apparent in the proximal lower limbs, resulting in difficulty when rising from a sitting position. A wide-based, waddling gait is found in 48%-64% of individuals. Joint contractures occur in 43% of individuals. Marfanoid body habitus is described in some affected individuals [Wallace et al 2004, Janssens et al 2006]. Musculoskeletal involvement can lead to varying degrees of lumbar lordosis, kyphosis, scoliosis, coxae valga, radial head dislocation, genua valga, hallux valgus, flat feet, and frontal bossing [Yuldashev et al 2017].
Bone pain is reported in 68%-90% of affected individuals [Wallace et al 2004, Janssens et al 2006]. The reported severity of bone pain ranged from mild (not requiring any treatment) to severe (requiring narcotic analgesics) [Yuldashev et al 2017]. The pain is described as constant, aching, and most intense in the lower limbs. Pain often increases with activity, stress, and cold weather. Many individuals have intermittent episodes of severe pain and incapacitation. Bone pain has resulted in limited ambulation in some individuals. The enlarged bone shafts can also be palpable and tender on examination; 52% of affected individuals report bone tenderness with palpation [Wallace et al 2004]. Intermittent limb swelling, erythema, and warmth also occur.
Although bone mineral density measured at the hip and femoral neck are increased in individuals with CED, bone strength measured by bone impact microindentation in three sibs with CED was below normal. Because of the small sample size, the difference in bone strength was not statistically significant. [Herrera et al 2017]. Increased susceptibility to fracture has not been reported. Healing of fractures, when they occur, may be delayed [Wallace et al 2004].
Neurologic. Sclerosis of the cranial nerve foramina can lead to direct nerve compression or neurovascular compromise. Cranial nerve deficits occur in 38% of affected individuals. The most common deficits are hearing loss, vision problems, and facial paralysis.
Approximately 19% of individuals with CED have conductive and/or sensorineural hearing loss [Carlson et al 2010]. Conductive loss can be caused by narrowing of the external auditory meatus, bony encroachment of the ossicles, or narrowing of the oval and round windows. Sensorineural hearing loss is caused by narrowing of the internal auditory canal and compression of the cochlear nerve and/or vasculature. Sensorineural hearing loss can also occur with attempted decompression of the facial nerves.
Involvement of the orbit has led to blurred vision, proptosis, papilledema, epiphora, glaucoma, and subluxation of the globe [Carlson et al 2010, Popiela & Austin 2015].
Rarely, clonus [Neuhauser et al 1948], sensory loss, slurred speech, dysphagia, cerebellar ataxia, and bowel and bladder incontinence are reported [Carlson et al 2010]. Calvarial hyperostosis can lead to increased intracranial pressure and headaches.
Recurrent cranial hyperostosis following surgical decompression can occur [Wong et al 2017].
Facial features. Children with CED do not typically have recognizable changes to their facial features. In older individuals who are severely affected, osteosclerosis of the skull can lead to macrocephaly, frontal bossing, enlargement of the mandible, proptosis, and cranial nerve impingement resulting in facial palsy.
Ribbing disease, an osteosclerotic disease of the long bones that is radiographically indistinguishable from CED and usually presents with bone pain after puberty [Makita et al 2000], is now known to be caused by pathogenic variants in TGFB1 [Janssens et al 2006]. Thus, CED and Ribbing disease represent phenotypic variations of the same disorder.
Other. Rare manifestations include anemia (hypothesized to be caused by a narrowed medullary cavity), anorexia, low body mass index, hepatosplenomegaly, decreased subcutaneous tissue, atrophic skin, hyperhidrosis of the hands and feet, delayed dentition, extensive caries, delayed puberty, and hypogonadism [Gupta & Cheikh 2005, Yuldashev et al 2017].
Pregnancy. One individual who experienced relief with steroids also experienced decreased bone pain and improved muscle strength while pregnant, which allowed discontinuation of her steroid therapy. Scintigraphic bone imaging with methylene diphosphate (MDP) a few hours after delivery of her second child showed decreased uptake compared to imaging prior to pregnancy and six weeks post partum.
Genotype-Phenotype Correlations
No known correlation exists between the nature of the TGFB1 pathogenic variants and the severity of the clinical or radiographic manifestations [Campos-Xavier et al 2001].
Penetrance
Some obligate heterozygotes with an identified TGFB1 pathogenic variant have had normal radiographs [Wallace et al 2004]; an exact penetrance figure is not known.
Anticipation
Earlier onset of symptoms and increased severity of symptoms and bone involvement in successive generations has been reported in several families [Wallace et al 2004, Janssens et al 2006]. If these findings represent anticipation rather than ascertainment bias (the latter being more likely), the mechanism of anticipation is unknown. Although multiple copies of the amino acid leucine can be encoded by one observed pathogenic variant in exon 1, the pathogenic variant was not found in these families.
Nomenclature
Engelmann described the second reported occurrence of CED in 1929 as "osteopathic hyperostotica (sclerotisans) multiplex infantilis."
The terms Engelmann disease and diaphyseal dysplasia were commonly used until Neuhauser et al [1948] coined the term progressive diaphyseal dysplasia.
Gulledge & White [1951] suggested the term progressive diaphyseal hyperostosis, which was not widely used.
Prevalence
The prevalence is unknown. More than 300 affected individuals have been reported.
The disorder is pan ethnic.
Differential Diagnosis
Few disorders share the clinical and radiographic findings of Camurati-Engelmann disease (CED). The correct diagnosis is made by physical examination and skeletal survey.
Table 2.
Differential Diagnosis Disorder | Gene | MOI | Clinical Features of This Disorder | |
---|---|---|---|---|
Overlapping w/CED | Distinguishing from CED | |||
Craniodiaphyseal dysplasia (CDD) (OMIM 218300) | Unknown | AR (suggested) | Diaphyseal sclerosis, cranial hyperostosis |
|
Kenny-Caffey syndrome type 2 (OMIM 127000) | FAM111A | AD | Sclerosis of long bones, cortical thickening, medullary stenosis | Hypocalcemia, hypoparathyroidism, delayed fontanelle closure |
Juvenile Paget disease (OMIM 239000) | TNFRSF11B | AR | Cranial hyperostosis, sensorineural hearing loss, sclerosis of long bones | Predisposition to fractures, bowing of the long bones |
Ghosal hematodiaphyseal dysplasia (OMIM 231095) | TBXAS1 | AR | Diaphyseal sclerosis | Severe anemia; leukopenia & thrombocytopenia |
Endosteal hyperostosis, AD (OMIM 144750) | LRP5 | AD | Diaphyseal sclerosis (endosteal), cranial nerve involvement in some | Wide deep mandible w/↑ gonial angle (distinct from the enlarged mandible found only occasionally in CED) |
SOST-related sclerosing bone dysplasias incl sclerosteosis & van Buchem disease | SOST | AR | Cranial hyperostosis, cranial nerve involvement, diaphyseal sclerosis | Syndactyly, dysplastic or absent nails |
AD = autosomal dominant; AR = autosomal recessive; MOI = mode of inheritance
Management
Evaluations Following Initial Diagnosis
To establish the extent of disease and needs in an individual diagnosed with Camurati-Engelmann disease (CED), the initial evaluation should include the following if they have not already been completed:
- Complete skeletal survey
- Assessment for cranial nerve deficits, including neurologic examination, audiology evaluation, and ophthalmologic evaluation
- Baseline blood pressure if considering treatment with losartan
- CBC to evaluate for anemia in individuals with significant endosteal involvement
- If acute bone pain is present, consideration of serum ESR and bone scan examination as baseline measures of disease activity
- In individuals with radiographic evidence of skull base sclerosis and neurologic symptoms, consideration of baseline CT examination of the head and neck to determine the extent of disease and allow consideration of surgical treatment options
- Consultation with a clinical geneticist and/or genetic counselor
Treatment of Manifestations
No consensus management guidelines have been developed to date.
Corticosteroids may relieve many of the symptoms of Camurati-Engelmann disease (CED). Several investigators report success with corticosteroid treatment in reducing pain and weakness; improving gait, exercise tolerance, and flexion contractures; and correcting anemia and hepatosplenomegaly [Lindstrom 1974, Baş et al 1999, Wallace et al 2004]. Unsuccessful steroid therapy was reported in one adult.
Individuals with severe symptoms can be treated with a bolus of prednisolone 1.0-2.0 mg/kg/day followed by rapid tapering to the lowest alternate-day dose tolerated. Less symptomatic individuals can be started on 0.5-1.0 mg/kg every other day. Some individuals may be able to discontinue steroid therapy during quiescent periods.
Higher-dose steroids may help with acute pain crises.
Note: Steroids may delay bone hyperostosis and prevent or delay the onset of skull involvement. Although histologic studies following steroid therapy showed increased bone resorption and secondary remodeling with increased osteoblast activity and decreased lamellar bone deposition, several authors reported no regression of sclerosis on radiographic evaluation [Verbruggen et al 1985] or on scintigraphic evaluation [Baş et al 1999]. Lindstrom [1974] and Baş et al [1999] reported diminished sclerosis on radiographs following steroid therapy. Verbruggen et al [1985] and Inaoka et al [2001] reported reduced radioactivity on bone scintigraphy. Long-term follow-up studies should be conducted to evaluate the success of corticosteroid therapy in preventing anemia, hepatosplenomegaly, headaches, and cranial nerve impingement.
Calcitonin. Pain relief from intranasal calcitonin was reported in one individual [Trombetti et al 2012].
Losartan. Reduced bone pain and increased physical activity were reported in two individuals treated with losartan [Ayyavoo et al 2014, Simsek-Kiper et al 2014]. Losartan has an anti-TGFβ effect and is being tested in individuals with Marfan syndrome. Treatment with losartan has not improved bone pain in some individuals [Yuldashev et al 2017]
Other analgesics and non-pharmacologic methods are frequently used for alleviation of pain.
Surgical treatment for persistent bone pain by intramedullary reaming was reported in a woman age 22 years diagnosed with Ribbing disease [Oztürkmen & Karamehmetoğlu 2011]. Pain in the tibia resolved completely following the surgery; the individual remained pain free at five-year follow up.
Craniectomy has relieved increased intracranial pressure and headaches in affected individuals [Carlson et al 2010]. Recurrent cranial hyperostosis with resultant increased intracranial pressure has been managed by radical craniectomy with titanium mesh cranioplasties [Wong et al 2017].
Hearing loss evaluation by an otolaryngologist should include a BAER and a CT with fine cuts through the inner ear. Reports of successful treatment of hearing loss in CED are rare. Surgical decompression of the internal auditory canals can improve hearing. However, the skull hyperostosis is progressive, and cranial nerve compression often recurs.
Corticosteroids may delay skull hyperostosis and cranial nerve impingement. Lindstrom [1974] reported no change in conductive hearing loss with steroid therapy. A woman age 30 years with a 75-dB neurosensory hearing loss on the right and a 65-dB neurosensory hearing loss of the left experienced some improvement in hearing with prednisone. Her hearing stabilized after decompression of the right internal auditory canal.
Bilateral myringotomy can improve conductive hearing loss resulting from serous otitis in individuals with CED.
A woman age 71 years with bilateral conductive hearing loss and patent internal auditory canals underwent a cochlear implantation, and speech detection improved from 75 dB to 45 dB [Friedland et al 2000]. General contraindications for cochlear implants include a narrowed internal auditory canal and absence of a functioning eighth nerve, both of which can be found in individuals with CED.
Carlson et al [2010] reported six individuals with CED and bilateral sensorineural hearing loss. Three underwent internal auditory canal decompression with mixed results. Conservative management was used in the other three individuals with no worsening of symptoms (see also Hereditary Deafness and Hearing Loss Overview).
Prevention of Primary Manifestations
Initiation of steroids prior to the onset of proximal muscle weakness and/or sclerotic bone changes has not been reported. Because of the variable symptomatology and decreased penetrance, treatment of asymptomatic individuals cannot be recommended.
Prevention of Secondary Complications
Monitor blood pressure in individuals treated with corticosteroids and treat hypertension if necessary.
Individuals taking losartan also need regular blood pressure monitoring due to the increased risk for hypotension.
Taper corticosteroid dose as tolerated to reduce the risk of osteoporosis and compression fractures of the spine.
Surveillance
After initiating corticosteroids, affected individuals should be followed monthly, with efforts to taper the steroids to the lowest tolerated dose. Blood pressure should be monitored at each visit, as hypertension can develop following the initiation of steroid therapy.
When a maintenance steroid dose is achieved, ongoing evaluations should include the following:
- Annual:
- Complete neurologic examination
- CBC
- Measurement of blood pressure
- Audiology evaluation
- Ophthalmology evaluation
- Evaluation of bone mineral densityNote: CED does not appear to cause an increase in spine density; therefore, steroid therapy could lead to osteoporosis of the spine [Author, personal observation].
- Routine monitoring of linear growth in children due to the possible side effect of delayed or stunted growth
- Individuals with cranial hyperostosis (including those treated surgically) should continue to be monitored for signs and symptoms of increased intracranial pressure, as cranial hyperostosis can recur.
The authors are aware of one affected teenage individual who died of a dilated ascending aorta dissection. Whether this is related to CED is unknown. Because the mechanism of CED involves increased TGFB1 signaling, also found in Marfan syndrome and Loeys-Dietz syndrome, this death is of some concern. The authors are unaware of any other similar cases. Note: No recommendations for routine evaluation of the aorta can be made at this time.
Agents/Circumstances to Avoid
Bisphosphonates. Pamidronate did not improve symptoms in four individuals [Inaoka et al 2001, Janssens et al 2006]. Clodronate infusion caused increased bone pain in one individual with CED and no improvement in another individual reported by Castro et al [2005].
Excess phosphate. Treatment with cellulose phosphate led to worsening hypocalcemia and proximal myopathy in another individual.
Evaluation of Relatives at Risk
It is appropriate to evaluate relatives at risk in order to identify the diagnosis as early as possible, avoid potential misdiagnosis, and provide appropriate treatment for extremity pain.
Evaluations can include:
- Molecular genetic testing if the pathogenic variant in the family is known;
- Radiographic evaluation for hyperostosis if the pathogenic variant in the family is not known.
See Genetic Counseling for issues related to testing of at-risk relatives for genetic counseling purposes.
Therapies Under Investigation
Search ClinicalTrials.gov in the US and EU Clinical Trials Register in Europe for access to information on clinical studies for a wide range of diseases and conditions. Note: There may not be clinical trials for this disorder.