cloverleaf skull

Gracile Bone Dysplasia

Clinical Characteristics

Ocular 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.

Genetics

Heterozygous 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 dominant

Treatment

Treatment Options:

No treatment has been reported.

References

Article 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

Pfeiffer Syndrome

Clinical Characteristics

Ocular Features:

Patients may have extreme proptosis (95%) secondary to shallow orbits and exposure keratitis (41%) is a risk. Hypertelorism, strabismus, and antimongoloid lid slants are common. More rare signs include anterior chamber anomalies and optic nerve hypoplasia.

Systemic Features:

Pfeiffer syndrome has been divided into 3 types, of which cases with types 2 and 3 often die young. Type 1 has the more typical features with midface hypoplasia, broad thumbs and toes, craniosynostosis, and often some degree of syndactyly. Adult patients with type 1 may be only mildly affected with some degree of midface hypoplasia and minor broadening of the first digits. Hearing loss secondary to bony defects is relatively common. Cleft palate is uncommon. Airway malformations especially in the trachea can cause respiratory problems.

Genetics

This is a genetically heterogeneous disorder resulting from mutations in at least 2 genes, FGFR1 (8p11.2-p11.1) and FGFR2 (10q26). The less common cases with the latter mutation are allelic to Apert (101200), Crouzon (123500), and Jackson-Weiss (123150) syndromes. Inheritance is autosomal dominant but some cases are only mildly affected. New mutations exhibit a paternal age effect.

Other forms of craniosynostosis in which mutations in FGFR2 have been found are: Beare-Stevenson Syndrome (123790), and Saethre-Chotzen Syndrome (101400).

Pedigree:

Autosomal dominant

Treatment

Treatment Options:

Exposure keratitis requires the usual treatment. Fronto-orbital advancement surgery for the midface underdevelopment is generally helpful for the complications of proptosis. Airway obstruction may require tracheostomy or surgical correction of the air passages.

References

Article Title:

The ophthalmic sequelae of Pfeiffer syndrome and the long-term visual outcomes after craniofacial surgery

Sharma N, Greenwell T, Hammerton M, David DJ, Selva D, Anderson PJ. The ophthalmic sequelae of Pfeiffer syndrome and the long-term visual outcomes after craniofacial surgery. J AAPOS. 2016 Jul 11. [Epub ahead of print].

PubMed ID:

27418250

Closing the Gap: Genetic and Genomic Continuum from Syndromic to Nonsyndromic Craniosynostoses

Heuze Y, Holmes G, Peter I, Richtsmeier JT, Jabs EW. Closing the Gap: Genetic and Genomic Continuum from Syndromic to Nonsyndromic Craniosynostoses. Curr Genet Med Rep. 2014 Sep 1;2(3):135-145.

PubMed ID:

16146596

Paternal origin of FGFR2 mutations in sporadic cases of Crouzon syndrome and Pfeiffer syndrome

Glaser RL, Jiang W, Boyadjiev SA, Tran AK, Zachary AA, Van Maldergem L, Johnson D, Walsh S, Oldridge M, Wall SA, Wilkie AO, Jabs EW. Paternal origin of FGFR2 mutations in sporadic cases of Crouzon syndrome and Pfeiffer syndrome. Am J Hum Genet. 2000 Mar;66(3):768-77.

PubMed ID:

10712195

Mutations in FGFR1 and FGFR2 cause familial and sporadic Pfeiffer syndrome

Schell U, Hehr A, Feldman GJ, Robin NH, Zackai EH, de Die-Smulders C, Viskochil DH, Stewart JM, Wolff G, Ohashi H, et al. Mutations in FGFR1 and FGFR2 cause familial and sporadic Pfeiffer syndrome. Hum Mol Genet. 1995 Mar;4(3):323-8.

PubMed ID:

7795583

FGFR2 mutations in Pfeiffer syndrome

Lajeunie E, Ma HW, Bonaventure J, Munnich A, Le Merrer M, Renier D. FGFR2 mutations in Pfeiffer syndrome. Nat Genet. 1995 Feb;9(2):108.

PubMed ID:

7719333

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