Calvarial doughnut lesions-bone fragility syndrome, also known as familial calvarial doughnut lesions, is a rare autosomal dominant genetic disorder characterized by mild to moderate fragility of the bones accompanied with calvarial doughnut lesions.
Calvarial doughnut lesions-bone fragility syndrome | |
---|---|
X-ray of the skull of three familial CDL patients showing the multiple cranial lesions characteristic of this condition. All of these patients carried a c.148C>T (p.Arg50*) mutation in the SGMS2 gene. | |
Specialty | Medical genetics |
Causes | Genetic mutation |
Prevention | none |
Signs and symptoms
editThis condition consists of the presence of multiple lesions in bones of the cranium that resemble the shape of a doughnut, fragile bones that fracture easily starting from early childhood, and a lowered bone mineral density.[1][2]
Other features of this condition include dental caries, teeth hypoplasia, and an increased level of serum alkaline phosphatase levels.[2][3] Glaucoma is occasionally reported among patients.[4][5]
Individuals with severe cases of the condition show other symptoms such as cranial sclerosis, spondylometaphyseal dysplasia, very short stature, and a more early onset of bone fragility with recurrent bone fractures starting during the neonatal stage of life.[1]
Complications
editThis section is empty. You can help by adding to it. (October 2022) |
Genetics
editThis condition is caused by a mutation in the SGMS2 gene, located on the long arm of the 4th chromosome.[6] The mutations result in the production of a SGMS2 enzyme that has no function at all.[7]
Said mutation has an autosomal dominant mode of inheritance, which means that for a person to exhibit the disorder associated with the mutation, they need to have at least one copy of the mutation in one of their two SGMS2 genes, this mutation had to be inherited or it had to be the result of a spontaneous genetic error.
In rare cases, this disorder can be caused by a mutation (which is also autosomal dominant) in the IFITM5 gene. This mutation (c.143A>G (p.N48S)) has only been described in a single Japanese family with the condition.[8]
Diagnosis
editDiagnostic methods for familial doughnut calvarial lesions include the use of MRI technology, X-rays, bone biopsies, and next-generation genetic testing.
D Baumgartner et al. found abnormalities of the skull through MRIs and X-rays on a 16-year-old teenager with a sporadic case of the condition.[9]
Jaakkola et al. found skeletal anomalies in 3 generations of a single Finnish family through X-rays and bone biopsies, their findings included a compression fracture at spinal vertebrae T12, an abnormal, thin cortical bone and trabeculae, high osteoclast activity, and abnormal diffuse thickening of the skull.[5]
Pekkiken et al. found scoliosis and platyspondyly in a Dutch woman, her son, and a Hispanic boy through X-rays.[7]
Treatment
editThis section is empty. You can help by adding to it. (October 2022) |
Prevalence
editAs of 2009, there had been less than 50 cases of this condition in the medical literature.[5]
History
editThis condition was first described in 1976 by Bartlett et al. Their patients were a man and his 3 sons who had calvarial lesions in their skulls and frequent bone fractures resulting from bone fragility. All of the three sons were born from different biological mothers, and although the latter detail, combined with the fact that they all shared a common biological father with the disorder, was indicative of autosomal dominant inheritance, the researchers leading the study erroneously came to the conclusion that the disorder was inherited as a form of sex-linked trait. The man also had 4 other children which weren't affected with the condition.[1][10]
Pekkinen et al. discovered the causative gene and mutations for the disorder in the year 2019 in 6 families from Finland, the United States, the Netherlands, and Latin America. Three mutations were identified; two missense mutations (c.191T>G and c.185T>G) which occurred in 2 families, and a nonsense mutation (c.148C>T) in the other 4 families.[7]
Genotype-phenotype correlation with symptoms
editIn a 2019 study, Pekkinen et al. did next-generation sequencing on a subset of 13 patients from 6 families with various ethnic origins and found 3 different mutations in all of the patients, 2 in particular were predicted to cause severe symptoms, while the other 1 (shared by the other four families) was predicted to cause a milder phenotype.[7]
The mutations were as follows:[7]
- c.148C>T (p.Arg50*)
- c.185T>G (p. Ile62Ser)
- c.191T>G (p.Met64Arg)
Individuals from the first four families with the c.148C>T variant showed mild symptoms of the condition, which included cranial sclerosis and childhood onset bone fragility, while individuals with the c.185T>G or the c.191T>G variant showed bone fragility and fractures starting during neonatal years, spondylometaphyseal dysplasia, abnormally short stature, recurrent paresis affecting the peripheral facial nerve, and other neurological anomalies.[7]
See also
edit- Osteoporosis-pseudoglioma syndrome, genetic disorder which combines the association of osteoporosis and pseudoglioma.
- Osteogenesis imperfecta, also known as brittle bone disease, it is a similar type of genetic bone disease characterized by congenital bone fragility.
References
edit- ^ a b c "Entry – #126550 – CALVARIAL DOUGHNUT LESIONS WITH BONE FRAGILITY; CDL – OMIM". www.omim.org. Retrieved 11 October 2022.
- ^ a b "Orphanet: Calvarial doughnut lesions bone fragility syndrome". www.orpha.net. Retrieved 11 October 2022.
- ^ Neto A, Bell D. "Calvarial doughnut lesion". Radiopaedia. Retrieved 12 October 2022.
- ^ Collantes ER, Flores-Anotado JF, Guevarra MC, Dumdum A, Futolan J, de Guzman MH, et al. (June 2022). "SGMS2 mutation in a large Filipino family with calvarial doughnut lesions with bone fragility and juvenile-onset open angle glaucoma". Investigative Ophthalmology & Visual Science. 63 (7): 4019 – A0361–4019 – A0361. ISSN 1552-5783.
- ^ a b c Jaakkola E, Laine CM, Mäyränpää MK, Falck A, Ignatius J, Mäkitie O (November 2009). "Calvarial doughnut lesions and osteoporosis: a new three-generation family and review". American Journal of Medical Genetics. Part A. 149A (11): 2371–2377. doi:10.1002/ajmg.a.33040. PMID 19839042. S2CID 24858892.
- ^ "KEGG DISEASE: Calvarial doughnut lesions with bone fragility". www.genome.jp. Retrieved 11 October 2022.
- ^ a b c d e f Pekkinen M, Terhal PA, Botto LD, Henning P, Mäkitie RE, Roschger P, et al. (April 2019). "Osteoporosis and skeletal dysplasia caused by pathogenic variants in SGMS2". JCI Insight. 4 (7): 126180. doi:10.1172/jci.insight.126180. PMC 6483641. PMID 30779713.
- ^ Mäkitie RE, Pekkinen M, Morisada N, Kobayashi D, Yonezawa Y, Nishimura G, et al. (December 2021). "A Novel IFITM5 Variant Associated with Phenotype of Osteoporosis with Calvarial Doughnut Lesions: A Case Report". Calcified Tissue International. 109 (6): 626–632. doi:10.1007/s00223-021-00878-5. PMC 8531111. PMID 34156493.
- ^ Baumgartner D, Gassner I, Sperl W, Salzer-Kuntschik M, Judmaier W, Steinmann B (March 2001). "Calvarial "doughnut lesions": clinical spectrum of the syndrome, report on a case, and review of the literature". American Journal of Medical Genetics. 99 (3): 238–243. doi:10.1002/1096-8628(2001)9999:9999<::aid-ajmg1154>3.0.co;2-0. PMID 11241496.
- ^ Bartlett JE, Kishore PR (May 1976). "Familial "doughnut" lesions of the skull. A benign, hereditary dysplasia". Radiology. 119 (2): 385–387. doi:10.1148/119.2.385. PMID 1265267.