Spondylometaphyseal Dysplasia, Axial Clinical CharacteristicsOcular Features: Due to the small number of individuals reported, the ocular phenotype is variable and likely incompletely described. Optic atrophy and pigmentary retinopathy are the most consistent findings. The most completely studied individual had evidence of slight bilateral optic nerve atrophy on cerebral MRI imaging as well. There may be extensive RPE atrophy but the fundus pigmentation is usually described as resembling retinitis pigmentosa. The ERG in several patients during the second decade of life already shows severe dysfunction of the photoreceptors, with cones the most severely impacted. In spite of this Goldmann visual fields have been reported to be normal. The macula and OCT have been reported as normal. Telecanthus, nystagmus, hypertelorism, proptosis, and photophobia have been reported. Early onset and progressive visual impairment are characteristic. Systemic Features: Only 5 patients with this condition have been reported most of whom were short in stature. There may be frontal bossing and the chest is narrow and flattened. Moderate platyspondyly has been described with enlarged but shortened ribs and an irregular iliac crest. Rhizomelic shortening of the limbs is common. The femoral metaphyses are abnormal with their necks shortened and enlarged. The ribs are enlarged but shortened as well and are flared at the ends. Mental development and function are normal. GeneticsThis is an autosomal recessive condition due to homozygous or compound heterozygous mutations in C21orf2. TreatmentTreatment Options: No effective treatment is known. ReferencesArticle Title: Axial Spondylometaphyseal Dysplasia Is Caused by C21orf2 Mutations Wang Z, Iida A, Miyake N, Nishiguchi KM, Fujita K, Nakazawa T, Alswaid A, Albalwi MA, Kim OH, Cho TJ, Lim GY, Isidor B, David A, Rustad CF, Merckoll E, Westvik J, Stattin EL, Grigelioniene G, Kou I, Nakajima M, Ohashi H, Smithson S, Matsumoto N, Nishimura G, Ikegawa S. Axial Spondylometaphyseal Dysplasia Is Caused by C21orf2 Mutations. PLoS One. 2016 Mar 14;11(13). PubMed ID: 26974433 Axial spondylometaphyseal dysplasia: Confirmation and further delineation of a new SMD with retinal dystrophy Isidor B, Baron S, Khau van Kien P, Bertrand AM, David A, Le Merrer M. Axial spondylometaphyseal dysplasia: Confirmation and further delineation of a new SMD with retinal dystrophy. Am J Med Genet A. 2010 Jun;152A(6):1550-4. PubMed ID: 20503334 Axial spondylometaphysealdysplasia Ehara S, Kim OH, Maisawa S, Takasago Y, Nishimura G. Axial spondylometaphysealdysplasia. Eur J Pediatr. 1997 Aug;156(8):627-30. PubMed ID: 9266195 Read more about Spondylometaphyseal Dysplasia, Axial
Axial Spondylometaphyseal Dysplasia Is Caused by C21orf2 Mutations Wang Z, Iida A, Miyake N, Nishiguchi KM, Fujita K, Nakazawa T, Alswaid A, Albalwi MA, Kim OH, Cho TJ, Lim GY, Isidor B, David A, Rustad CF, Merckoll E, Westvik J, Stattin EL, Grigelioniene G, Kou I, Nakajima M, Ohashi H, Smithson S, Matsumoto N, Nishimura G, Ikegawa S. Axial Spondylometaphyseal Dysplasia Is Caused by C21orf2 Mutations. PLoS One. 2016 Mar 14;11(13). PubMed ID: 26974433
Axial spondylometaphyseal dysplasia: Confirmation and further delineation of a new SMD with retinal dystrophy Isidor B, Baron S, Khau van Kien P, Bertrand AM, David A, Le Merrer M. Axial spondylometaphyseal dysplasia: Confirmation and further delineation of a new SMD with retinal dystrophy. Am J Med Genet A. 2010 Jun;152A(6):1550-4. PubMed ID: 20503334
Axial spondylometaphysealdysplasia Ehara S, Kim OH, Maisawa S, Takasago Y, Nishimura G. Axial spondylometaphysealdysplasia. Eur J Pediatr. 1997 Aug;156(8):627-30. PubMed ID: 9266195
Gracile Bone Dysplasia Clinical CharacteristicsOcular Features: The eyes have been described as small. Aniridia may be present. Systemic Features: This is a usually fatal form of skeletal dysplasia with splenic and ocular features as well. In utero death is not uncommon while newborns may not survive the neonatal period. The face has been described as dysmorphic with a high forehead, flat nasal bridge, a cloverleaf-shaped skull, and hypoplastic cranial bones with premature suture closure. The long bones are dysplastic as well with thinned diaphyses (sometimes fractured in utero), growth plate disorganization, excessive remodeling, and signs of arrested growth. The ribs share in the dysplasia but pulmonary hypoplasia has also been described. Most individuals have short limbs. The spleen can be hypoplastic or aplastic and ascites has been noted in several infants. Failure to thrive is common and seizures have been reported. Males may have micropenis and hypospadias while females have been described with labial fusion. Low parathyroid hormone levels and hypocalcemia has been reported in most individuals. GeneticsHeterozygous mutations in the FAM111A gene (11q12.1) have been associated with this disorder. The functional role of FAM111A products is unknown but likely play a role in calcium metabolism, parathyroid hormone secretion, and osseous development. Mutations in the same gene can be responsible for the allelic autosomal dominant Kenny-Caffey syndrome (127000) with some similar features. Pedigree: Autosomal dominantTreatmentTreatment Options: No treatment has been reported. ReferencesArticle Title: Osteocraniostenosis-hypomineralized skull with gracile long bones and splenic hypoplasia. Four new cases with distinctive chondro-osseous morphology Elliott AM, Wilcox WR, Spear GS, Field FM, Steffensen TS, Friedman BD, Rimoin DL, Lachman RS. Osteocraniostenosis-hypomineralized skull with gracile long bones and splenic hypoplasia. Four new cases with distinctive chondro-osseous morphology. Am J Med Genet A. 2006 Jul 15;140(14):1553-63. PubMed ID: 16770805 FAM111A mutations result in hypoparathyroidism and impaired skeletal development Unger S, Gorna MW, Le Bechec A, Do Vale-Pereira S, Bedeschi MF, Geiberger S, Grigelioniene G, Horemuzova E, Lalatta F, Lausch E, Magnani C, Nampoothiri S, Nishimura G, Petrella D, Rojas-Ringeling F, Utsunomiya A, Zabel B, Pradervand S, Harshman K, Campos-Xavier B, Bonafe L, Superti-Furga G, Stevenson B, Superti-Furga A. FAM111A mutations result in hypoparathyroidism and impaired skeletal development. Am J Hum Genet. 2013 Jun 6;92(6):990-5. PubMed ID: 23684011 Read more about Gracile Bone Dysplasia
Osteocraniostenosis-hypomineralized skull with gracile long bones and splenic hypoplasia. Four new cases with distinctive chondro-osseous morphology Elliott AM, Wilcox WR, Spear GS, Field FM, Steffensen TS, Friedman BD, Rimoin DL, Lachman RS. Osteocraniostenosis-hypomineralized skull with gracile long bones and splenic hypoplasia. Four new cases with distinctive chondro-osseous morphology. Am J Med Genet A. 2006 Jul 15;140(14):1553-63. PubMed ID: 16770805
FAM111A mutations result in hypoparathyroidism and impaired skeletal development Unger S, Gorna MW, Le Bechec A, Do Vale-Pereira S, Bedeschi MF, Geiberger S, Grigelioniene G, Horemuzova E, Lalatta F, Lausch E, Magnani C, Nampoothiri S, Nishimura G, Petrella D, Rojas-Ringeling F, Utsunomiya A, Zabel B, Pradervand S, Harshman K, Campos-Xavier B, Bonafe L, Superti-Furga G, Stevenson B, Superti-Furga A. FAM111A mutations result in hypoparathyroidism and impaired skeletal development. Am J Hum Genet. 2013 Jun 6;92(6):990-5. PubMed ID: 23684011
CODAS Syndrome Clinical CharacteristicsOcular Features: Dense nuclear cataracts can be seen by six months of age. Some patients have ptosis. The fundi have been described as normal at one month of age in a single infant but vision was described at the 20/200 level at 2 years of age. Cataracts noted at 4 months had been removed. Systemic Features: Patients have multiple severe systemic abnormalities. There is generalized developmental delay along with mild microcephaly and hypotonia. The forehead is often broad while the face appears flattened with anteverted nares, a flat nasal bridge, a short philtrum, low-set and crumpled ears. Infants may have an inadequate upper respiratory apparatus with atrophic vocal cords and some die of laryngeal obstruction in the first days of life. Sialorrhea and difficulty swallowing have been noted. Mild to moderate neurosensory hearing loss is often present but there may also be a conduction component to this. Brain imaging has revealed large ventricles, with subcortical hypomyelination, a thin corpus callosum, and prominent cortical sulci. The vertebrae may have coronal clefts and scoliosis often develops. Generalized metaphyseal dysplasia and delayed bone age are usually present. The anus may be imperforate and a rectovaginal fistula and cryptorchidism have been reported. Long bones may be malformed as well and most patients are short in stature. Delayed dentition, enamel dysplasia, and abnormal cusp morphology are often present. Cardiac septal defects may be seen. GeneticsHomozygous mutations in LONF1 (19p13.3) segregate with the phenotype. Pedigree: Autosomal recessiveTreatmentTreatment Options: There is no general treatment available and infants sometimes die from laryngeal obstruction in the first days of life. Individual anomalies may be surgically correctable in selected individuals. Occasional infants are stillborn but one patient died an accidental death at 14 years of age. ReferencesArticle Title: CODAS syndrome is associated with mutations of LONP1, encoding mitochondrial AAA+ Lon protease Strauss KA, Jinks RN, Puffenberger EG, Venkatesh S, Singh K, Cheng I, Mikita N, Thilagavathi J, Lee J, Sarafianos S, Benkert A, Koehler A, Zhu A, Trovillion V, McGlincy M, Morlet T, Deardorff M, Innes AM, Prasad C, Chudley AE, Lee IN, Suzuki CK. CODAS syndrome is associated with mutations of LONP1, encoding mitochondrial AAA+ Lon protease. Am J Hum Genet. 2015 Jan 8;96(1):121-35. PubMed ID: 25574826 Newly recognized syndrome of cerebral, ocular, dental, auricular, skeletal anomalies: CODAS syndrome--a case report Shebib SM, Reed MH, Shuckett EP, Cross HG, Perry JB, Chudley AE. Newly recognized syndrome of cerebral, ocular, dental, auricular, skeletal anomalies: CODAS syndrome--a case report. Am J Med Genet. 1991 Jul 1;40(1):88-93. PubMed ID: 1887855 Read more about CODAS Syndrome
CODAS syndrome is associated with mutations of LONP1, encoding mitochondrial AAA+ Lon protease Strauss KA, Jinks RN, Puffenberger EG, Venkatesh S, Singh K, Cheng I, Mikita N, Thilagavathi J, Lee J, Sarafianos S, Benkert A, Koehler A, Zhu A, Trovillion V, McGlincy M, Morlet T, Deardorff M, Innes AM, Prasad C, Chudley AE, Lee IN, Suzuki CK. CODAS syndrome is associated with mutations of LONP1, encoding mitochondrial AAA+ Lon protease. Am J Hum Genet. 2015 Jan 8;96(1):121-35. PubMed ID: 25574826
Newly recognized syndrome of cerebral, ocular, dental, auricular, skeletal anomalies: CODAS syndrome--a case report Shebib SM, Reed MH, Shuckett EP, Cross HG, Perry JB, Chudley AE. Newly recognized syndrome of cerebral, ocular, dental, auricular, skeletal anomalies: CODAS syndrome--a case report. Am J Med Genet. 1991 Jul 1;40(1):88-93. PubMed ID: 1887855
Spherophakia and Metaphyseal Dysplasia Clinical CharacteristicsOcular Features: The corneas and anterior chambers were normal in the son but the lenses were small and spherical and had colobomatous defects. The father developed a retinal detachment in one eye and elevated intraocular pressure. The morphology of the lenses in the father is unknown. Systemic Features: The diaphyses of the long bones are thickened with relative sparing of the small bones in the extremities. The epiphyses become more irregular later in life. The vertebrae are deformed with flattening. The result is brachymelia and moderately severe dwarfism. Pigeon breast deformity can be present. GeneticsA father and son have been reported with this combination of findings suggesting autosomal dominant inheritance. No locus or mutation has been identified. Pedigree: Autosomal dominantTreatmentTreatment Options: Unknown. ReferencesArticle Title: Microspherophakia-metaphyseal dysplasia: a 'new' dominantly inherited bone dysplasia with severe eye involvement Verloes A, Van Maldergem L, de Marneffe P, Dufier JL, Maroteaux P. Microspherophakia-metaphyseal dysplasia: a 'new' dominantly inherited bone dysplasia with severe eye involvement. J Med Genet. 1990 Jul;27(7):467-71. PubMed ID: 2395168 Read more about Spherophakia and Metaphyseal Dysplasia
Microspherophakia-metaphyseal dysplasia: a 'new' dominantly inherited bone dysplasia with severe eye involvement Verloes A, Van Maldergem L, de Marneffe P, Dufier JL, Maroteaux P. Microspherophakia-metaphyseal dysplasia: a 'new' dominantly inherited bone dysplasia with severe eye involvement. J Med Genet. 1990 Jul;27(7):467-71. PubMed ID: 2395168
