Entry - #106260 - ANKYLOBLEPHARON-ECTODERMAL DEFECTS-CLEFT LIP/PALATE; AEC - OMIM

 
ICD+
# 106260

ANKYLOBLEPHARON-ECTODERMAL DEFECTS-CLEFT LIP/PALATE; AEC


Alternative titles; symbols

AEC SYNDROME
HAY-WELLS SYNDROME


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
3q28 Hay-Wells syndrome 106260 AD 3 TP63 603273
Clinical Synopsis
 

INHERITANCE
- Autosomal dominant
HEAD & NECK
Head
- Scalp erosions
Face
- Oval face
- Maxillary hypoplasia
Ears
- Conductive hearing loss
- Atretic external auditory canal
- Cup-shaped auricles
Eyes
- Ankyloblepharon filiforme adnatum
- Lacrimal duct atresia
- Sparse to absent eyelashes
- Conjunctivitis
- Blepharitis
Nose
- Broadened nasal bridge
Mouth
- Cleft lip
- Cleft palate
Teeth
- Conical teeth
- Widely spaced teeth
- Hypodontia
- Selective tooth agenesis
CARDIOVASCULAR
Heart
- Ventricular septal defect
Vascular
- Patent ductus arteriosus
CHEST
Breasts
- Supernumerary nipples
GENITOURINARY
External Genitalia (Male)
- Hypospadias
- Micropenis
Internal Genitalia (Female)
- Vaginal dryness
SKELETAL
Feet
- 2-3 toe soft tissue syndactyly
SKIN, NAILS, & HAIR
Skin
- Red, cracking, peeling skin at birth
- Palmar and plantar keratoderma
- Hyperkeratosis
- Hyperpigmentation
- Partial anhidrosis
- Scalp erosions
Nails
- Absent nails
- Dystrophic nails
- Hyperconvex nails
Hair
- Wiry, sparse hair
- Patchy alopecia
- Sparse to absent eyelashes
- Sparse body hair
- Patchy alopecia
- Sparse to absent eyelashes
- Sparse body hair
NEUROLOGIC
Central Nervous System
- Normal intelligence
MISCELLANEOUS
- Allelic to EEC3 (604292), SHFM4 (605289), ADULT syndrome (103285), limb-mammary syndrome (603543), and Rapp-Hodgkin syndrome (129400)
MOLECULAR BASIS
- Caused by mutations in the tumor protein p63 gene (TP63, 603273.0009)
▲ Close

TEXT

A number sign (#) is used with this entry because of evidence that the AEC syndrome (ankyloblepharon-ectodermal defects-cleft lip/palate) is caused by heterozygous mutation in the TP63 gene (603273) on chromosome 3q27.

Allelic disorders with overlapping features include EEC3 (604292), limb-mammary syndrome (LMS; 603543), ADULT syndrome (103285), Rapp-Hodgkin syndrome (RHS; 129400), and SHFM4 (605289).

Description

Ankyloblepharon-ectodermal defects-cleft lip/palate syndrome (AEC) is an autosomal dominant disorder characterized by congenital ectodermal dysplasia, including alopecia, scalp infections, dystrophic nails, hypodontia, ankyloblepharon, and cleft lip and/or palate (summary by McGrath et al., 2001).


Clinical Features

Hay and Wells (1976) described 7 individuals from 4 families with an uncommon disorder characterized by congenital ectodermal dysplasia with coarse, wiry, and sparse hair, dystrophic nails, slight hypohidrosis, scalp infections, ankyloblepharon filiforme adnatum, hypodontia, maxillary hypoplasia, and cleft lip/palate.

Spiegel and Colton (1985) reported an affected mother and son who both had cleft lip and palate. The eyelashes were rudimentary, and in the son there was fusion of the right upper and lower eyelids at birth.

Greene et al. (1987) described 2 isolated cases. Weiss et al. (1992) described an isolated case. They reported 2 other patients with ankyloblepharon filiforme adnatum who had chromosomal abnormalities and 1 patient who had the abnormality as an isolated finding.

Seres-Santamaria et al. (1993) reported a family in which 2 sibs showed cleft palate, ankyloblepharon, and ectodermal defects and, in addition, had congenital adhesions between the upper and lower jaws (alveolar synechiae). Neither parent had any features of the syndrome, suggesting this is either a recessive form of Hay-Wells syndrome with additional features or should be viewed as a separate entity. It is possible, of course, that the family reported by Seres-Santamaria et al. (1993) represented an instance of germinal mosaicism for the dominant mutation in one of the normal parents.

Bertola et al. (2000) described a 5-year-old Brazilian boy with ectodermal dysplasia, ankyloblepharon, and bilateral choanal atresia but without cleft palate. The authors noted that choanal atresia was present in one of the patients reported by Hay and Wells (1976). The patient's nonconsanguineous parents had no ectodermal abnormality, and there was no family history of the disorder.

Fete et al. (2009) provided a conference report from the 2006 International Research Symposium on AEC Syndrome. They noted that features present in 100% of 12 AEC patients presented in a workshop included scalp/skin erosions, ankyloblepharon, dental abnormalities, recurrent otitis media, and nail abnormalities; in addition, 92% had cleft palate, and 83% had cleft lip. Nails were not characteristically 'hyperconvex' as previously described, but were more often thin, distorted, or absent. The most dramatic ophthalmologic abnormality was blepharitis. Scalp erosions were a major source of morbidity for affected infants, and tetracyclines, especially doxycycline, were recommended for dual antimicrobial and matrix metalloproteinase activity. Fete et al. (2009) noted that many children with AEC have nutritional issues, with a majority suffering failure to thrive that was out of proportion compared to other children with isolated cleft lip/palate; the reasons for this were not clear.

Cole et al. (2009) evaluated 18 patients with a diagnosis of AEC, who all had a history of otitis externa or otitis media; 14 of 15 subjects tested had conductive hearing loss, and 8 had hoarseness or voice problems. The authors suggested that many oroauditory problems in AEC are likely related to palatal clefting, as well as associated disorders such as feeding difficulty, recurrent middle ear infection, and speech disarticulation. Cole et al. (2009) noted that persistent feeding difficulties following cleft closure indicated that additional factors might be involved, and suggested that increased tissue vulnerability associated with absent epidermal appendages might also play a role.

Sutton et al. (2009) examined 17 AEC patients from 13 unrelated families and found that short stature and poor weight gain with preservation of head circumference were present in nearly all patients. Additional features included trismus in 35% and hypospadias in 85% of males. In contrast to previous reports of syndactyly limited to the soft tissue, 8 (47%) of 17 patients had bilateral complete 2-3 toe syndactyly, and 3 cases (18%) had 3-4 toe syndactyly that was noted to extend to the fifth toe in some cases. In 4 (24%) of 17 cases there was webbing and/or syndactyly of the hands involving the third and fourth digits. Other limb anomalies included hammertoe deformities in 8 (47%) of the 17 patients. Sutton et al. (2009) concluded that limb involvement in AEC is more significant than previously thought; they also noted that these patients confirmed the extreme clinical variability in AEC.

Dishop et al. (2009) used light microscopy to examine biopsies of normal and lesional skin from 19 AEC patients; in addition, hair samples from 18 patients were examined by light and scanning electron microscopy. Histopathologic changes identified within the skin biopsies from clinically unaffected skin included mild atrophy, focal orthokeratosis, and mild superficial perivascular lymphocytic dermatitis. Scattered melanophages in the superficial and deep dermis were believed to reflect postinflammatory changes. Examination of hair shafts revealed atrophy and loss of melanin pigment in some patients; structural abnormalities included pili torti, pili trianguli et canaliculi, and irregular indentation and shallow grooves. No pathognomonic findings of skin or hair were identified.


Inheritance

The transmission pattern of AEC in family A reported by Dianzani et al. (2003) was consistent with autosomal dominant inheritance.


Molecular Genetics

Some phenotypic overlap can be recognized with Hay-Wells syndrome and other ectodermal dysplasia syndromes, including ectrodactyly-ectodermal dysplasia-cleft lip/palate (EEC; 604292). Celli et al. (1999) demonstrated that heterozygous mutations in the TP63 gene are the major cause of EEC syndrome. McGrath et al. (2001) analyzed the TP63 gene in AEC syndrome patients and identified missense mutations in 8 families. All mutations gave rise to amino acid substitutions in the sterile alpha motif (SAM) domain, and were predicted to affect protein-protein interactions. In contrast, the vast majority of the mutations found in EEC syndrome are amino acid substitutions in the DNA-binding domain. The authors suggested that a distinct genotype-phenotype correlation can be recognized for EEC and AEC syndromes.

In 2 sibs and their mother who had been diagnosed with Rapp-Hodgkin syndrome (RHS; 129400), Dianzani et al. (2003) identified a 1-bp deletion in the TP63 gene (603273.0017). The mother had a slight ankyloblepharon on the right eye at birth which was surgically treated; Dianzani et al. (2003) suggested that AEC and RHS are the same clinical entity.

In a patient with AEC previously described by Bertola et al. (2000), Bertola et al. (2004) identified an ile510-to-thr mutation in the TP63 gene (603273.0018). They identified the same mutation in a patient with RHS and concluded that AEC and RHS represent variable expression of a single genetic disorder.

In an 11-year-old boy who displayed an overlapping phenotype with features of both AEC and RHS, Prontera et al. (2008) identified heterozygosity for an 11-bp duplication in the TP63 gene (603273.0027). The authors stated that their findings confirmed the hypothesis that AEC and RHS are variable expressions of a single genetic disorder, and suggested that intermediate phenotypes are possible.


Animal Model

Koster et al. (2009) generated mice with downregulated delta-N-p63-alpha, the predominantly expressed TP63 isoform in postnatal skin. The mutant mouse epidermis developed severe skin erosions resembling those of AEC patients and similarly characterized by suprabasal epidermal proliferation, delayed terminal differentiation, and basement membrane abnormalities. The authors suggested that by failing to provide structural stability to the epidermis, these defects likely contribute to the observed skin fragility.


REFERENCES

  1. Bertola, D. R., Kim, C. A., Albano, L. M. J., Scheffer, H., Meijer, R., van Bokhoven, H. Molecular evidence that AEC syndrome and Rapp-Hodgkin syndrome are variable expression of a single genetic disorder. (Letter) Clin. Genet. 66: 79-80, 2004. [PubMed: 15200513, related citations] [Full Text]

  2. Bertola, D. R., Kim, C. A., Sugayama, S. M. M., Albano, L. M. J., Utagawa, C. Y., Gonzalez, C. H. AEC syndrome and CHAND syndrome: further evidence of clinical overlapping in the ectodermal dysplasias. Pediat. Derm. 17: 218-221, 2000. [PubMed: 10886756, related citations] [Full Text]

  3. Celli, J., Duijf, P., Hamel, B. C. J., Bamshad, M., Kramer, B., Smits, A. P. T., Newbury-Ecob, R., Hennekam, R. C. M., Van Buggenhout, G., van Haeringen, A., Woods, C. G., van Essen, A. J., de Waal, R., Vriend, G., Haber, D. A., Yang, A., McKeon, F., Brunner, H. G., van Bokhoven, H. Heterozygous germline mutations in the p53 homolog p63 are the cause of EEC syndrome. Cell 99: 143-153, 1999. [PubMed: 10535733, related citations] [Full Text]

  4. Cole, P., Hatef, D. A., Kaufman, Y., Magruder, A., Bree, A., Friedman, E., Sindwani, R., Hollier, L. H., Jr. Facial clefting and oroauditory pathway manifestations in ankyloblepharon-ectodermal defects-cleft lip/palate (AEC) syndrome. Am. J. Med. Genet. 149A: 1910-1915, 2009. [PubMed: 19697430, related citations] [Full Text]

  5. Dianzani, I., Garelli, E., Gustavsson, P., Carando, A., Gustafsson, B., Dahl, N., Anneren, G. Rapp-Hodgkin and AEC syndromes due to a new frameshift mutation in the TP63 gene. J. Med. Genet. 40: e133, 2003. Note: Electronic Article. [PubMed: 14684701, related citations] [Full Text]

  6. Dishop, M. K., Bree, A. F., Hicks, M. J. Pathologic changes of skin and hair in ankyloblepharon-ectodermal defects-cleft lip/palate (AEC) syndrome. Am. J. Med. Genet. 149A: 1935-1941, 2009. [PubMed: 19697429, related citations] [Full Text]

  7. Fete, M., vanBokhoven, H., Clements, S. E., McKeon, F., Roop, D. R., Koster, M. I., Missero, C., Attardi, L. D., Lombillo, V. A., Ratovitski, E., Julapalli, M., Ruths, D., Sybert, V. P., Siegfried, E. C., Bree, A. F. International Research Symposium on ankyloblepharon-ectodermal defects-cleft lip/palate (AEC) syndrome. Am. J. Med. Genet. 149A: 1885-1893, 2009. [PubMed: 19353643, related citations] [Full Text]

  8. Greene, S. L., Michels, V. V., Doyle, J. A. Variable expression in ankyloblepharon-ectodermal defects-cleft lip and palate syndrome. Am. J. Med. Genet. 27: 207-212, 1987. [PubMed: 3605196, related citations] [Full Text]

  9. Hay, R. J., Wells, R. S. The syndrome of ankyloblepharon, ectodermal defects and cleft lip and palate: an autosomal dominant condition. Brit. J. Derm. 94: 277-289, 1976. [PubMed: 946410, related citations] [Full Text]

  10. Koster, M. I., Marinari, B., Payne, A. S., Kantaputra, P. N., Costanzo, A., Roop, D. R. Delta-Np63 knockdown mice: a mouse model for AEC syndrome. Am. J. Med. Genet. 149A: 1942-1947, 2009. [PubMed: 19681108, images, related citations] [Full Text]

  11. McGrath, J. A., Duijf, P. H. G., Doetsch, V., Irvine, A. D., de Waal, R., Vanmolkot, K. R. J., Wessagowit, V., Kelly, A., Atherton, D. J., Griffiths, W. A. D., Orlow, S. J., van Haeringen, A., Ausems, M. G. E. M., Yang, A., McKeon, F., Bamshad, M. A., Brunner, H. G., Hamel, B. C. J., van Bokhoven, H. Hay-Wells syndrome is caused by heterozygous missense mutations in the SAM domain of p63. Hum. Molec. Genet. 10: 221-229, 2001. [PubMed: 11159940, related citations] [Full Text]

  12. Prontera, P., Escande, F., Cocchi, G., Donti, E., Martini, A., Sensi, A. An intermediate phenotype between Hays-Wells and Rapp-Hodgkin syndromes in a patient with a novel p63 mutation: confirmation of a variable phenotypic spectrum with a common aetiology. Genet. Counsel. 19: 397-402, 2008. [PubMed: 19239083, related citations]

  13. Seres-Santamaria, A., Arimany, J. L., Muniz, F. Two sibs with cleft palate, ankyloblepharon, alveolar synechiae, and ectodermal defects: a new recessive syndrome? J. Med. Genet. 30: 793-795, 1993. [PubMed: 8411079, related citations] [Full Text]

  14. Spiegel, J., Colton, A. AEC syndrome: ankyloblepharon, ectodermal defects, and cleft lip and palate. J. Am. Acad. Derm. 12: 810-815, 1985. [PubMed: 3839246, related citations] [Full Text]

  15. Sutton, V. R., Plunkett, K., Dang, D. X., Lewis, R. A., Bree, A. F., Bacino, C. A. Craniofacial and anthropometric phenotype in ankyloblepharon-ectodermal defects-cleft lip/palate syndrome (Hay-Wells syndrome) in a cohort of 17 patients. Am. J. Med. Genet. 149A: 1916-1921, 2009. [PubMed: 19676059, related citations] [Full Text]

  16. Weiss, A. H., Riscile, G., Kousseff, B. G. Ankyloblepharon filiforme adnatum. Am. J. Med. Genet. 42: 369-373, 1992. [PubMed: 1536181, related citations] [Full Text]


Contributors:
Marla J. F. O'Neill - updated : 7/12/2011
Marla J. F. O'Neill - updated : 6/9/2010
Marla J. F. O'Neill - updated : 8/4/2005
George E. Tiller - updated : 4/17/2001
Creation Date:
Victor A. McKusick : 5/19/1987
Edit History:
alopez : 12/15/2022
alopez : 05/16/2022
carol : 06/11/2021
alopez : 06/10/2021
carol : 01/22/2020
carol : 10/09/2018
carol : 10/22/2013
wwang : 7/15/2011
terry : 7/12/2011
wwang : 6/10/2010
terry : 6/9/2010
wwang : 5/7/2009
wwang : 8/5/2005
terry : 8/4/2005
cwells : 4/26/2001
cwells : 4/20/2001
cwells : 4/17/2001
terry : 4/30/1999
mark : 11/1/1995
mimadm : 3/11/1994
carol : 11/3/1993
carol : 11/2/1993
carol : 10/29/1993
supermim : 3/16/1992

# 106260

ANKYLOBLEPHARON-ECTODERMAL DEFECTS-CLEFT LIP/PALATE; AEC


Alternative titles; symbols

AEC SYNDROME
HAY-WELLS SYNDROME


SNOMEDCT: 55821006;   ORPHA: 1071;   DO: 0090119;  


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
3q28 Hay-Wells syndrome 106260 Autosomal dominant 3 TP63 603273

TEXT

A number sign (#) is used with this entry because of evidence that the AEC syndrome (ankyloblepharon-ectodermal defects-cleft lip/palate) is caused by heterozygous mutation in the TP63 gene (603273) on chromosome 3q27.

Allelic disorders with overlapping features include EEC3 (604292), limb-mammary syndrome (LMS; 603543), ADULT syndrome (103285), Rapp-Hodgkin syndrome (RHS; 129400), and SHFM4 (605289).

Description

Ankyloblepharon-ectodermal defects-cleft lip/palate syndrome (AEC) is an autosomal dominant disorder characterized by congenital ectodermal dysplasia, including alopecia, scalp infections, dystrophic nails, hypodontia, ankyloblepharon, and cleft lip and/or palate (summary by McGrath et al., 2001).


Clinical Features

Hay and Wells (1976) described 7 individuals from 4 families with an uncommon disorder characterized by congenital ectodermal dysplasia with coarse, wiry, and sparse hair, dystrophic nails, slight hypohidrosis, scalp infections, ankyloblepharon filiforme adnatum, hypodontia, maxillary hypoplasia, and cleft lip/palate.

Spiegel and Colton (1985) reported an affected mother and son who both had cleft lip and palate. The eyelashes were rudimentary, and in the son there was fusion of the right upper and lower eyelids at birth.

Greene et al. (1987) described 2 isolated cases. Weiss et al. (1992) described an isolated case. They reported 2 other patients with ankyloblepharon filiforme adnatum who had chromosomal abnormalities and 1 patient who had the abnormality as an isolated finding.

Seres-Santamaria et al. (1993) reported a family in which 2 sibs showed cleft palate, ankyloblepharon, and ectodermal defects and, in addition, had congenital adhesions between the upper and lower jaws (alveolar synechiae). Neither parent had any features of the syndrome, suggesting this is either a recessive form of Hay-Wells syndrome with additional features or should be viewed as a separate entity. It is possible, of course, that the family reported by Seres-Santamaria et al. (1993) represented an instance of germinal mosaicism for the dominant mutation in one of the normal parents.

Bertola et al. (2000) described a 5-year-old Brazilian boy with ectodermal dysplasia, ankyloblepharon, and bilateral choanal atresia but without cleft palate. The authors noted that choanal atresia was present in one of the patients reported by Hay and Wells (1976). The patient's nonconsanguineous parents had no ectodermal abnormality, and there was no family history of the disorder.

Fete et al. (2009) provided a conference report from the 2006 International Research Symposium on AEC Syndrome. They noted that features present in 100% of 12 AEC patients presented in a workshop included scalp/skin erosions, ankyloblepharon, dental abnormalities, recurrent otitis media, and nail abnormalities; in addition, 92% had cleft palate, and 83% had cleft lip. Nails were not characteristically 'hyperconvex' as previously described, but were more often thin, distorted, or absent. The most dramatic ophthalmologic abnormality was blepharitis. Scalp erosions were a major source of morbidity for affected infants, and tetracyclines, especially doxycycline, were recommended for dual antimicrobial and matrix metalloproteinase activity. Fete et al. (2009) noted that many children with AEC have nutritional issues, with a majority suffering failure to thrive that was out of proportion compared to other children with isolated cleft lip/palate; the reasons for this were not clear.

Cole et al. (2009) evaluated 18 patients with a diagnosis of AEC, who all had a history of otitis externa or otitis media; 14 of 15 subjects tested had conductive hearing loss, and 8 had hoarseness or voice problems. The authors suggested that many oroauditory problems in AEC are likely related to palatal clefting, as well as associated disorders such as feeding difficulty, recurrent middle ear infection, and speech disarticulation. Cole et al. (2009) noted that persistent feeding difficulties following cleft closure indicated that additional factors might be involved, and suggested that increased tissue vulnerability associated with absent epidermal appendages might also play a role.

Sutton et al. (2009) examined 17 AEC patients from 13 unrelated families and found that short stature and poor weight gain with preservation of head circumference were present in nearly all patients. Additional features included trismus in 35% and hypospadias in 85% of males. In contrast to previous reports of syndactyly limited to the soft tissue, 8 (47%) of 17 patients had bilateral complete 2-3 toe syndactyly, and 3 cases (18%) had 3-4 toe syndactyly that was noted to extend to the fifth toe in some cases. In 4 (24%) of 17 cases there was webbing and/or syndactyly of the hands involving the third and fourth digits. Other limb anomalies included hammertoe deformities in 8 (47%) of the 17 patients. Sutton et al. (2009) concluded that limb involvement in AEC is more significant than previously thought; they also noted that these patients confirmed the extreme clinical variability in AEC.

Dishop et al. (2009) used light microscopy to examine biopsies of normal and lesional skin from 19 AEC patients; in addition, hair samples from 18 patients were examined by light and scanning electron microscopy. Histopathologic changes identified within the skin biopsies from clinically unaffected skin included mild atrophy, focal orthokeratosis, and mild superficial perivascular lymphocytic dermatitis. Scattered melanophages in the superficial and deep dermis were believed to reflect postinflammatory changes. Examination of hair shafts revealed atrophy and loss of melanin pigment in some patients; structural abnormalities included pili torti, pili trianguli et canaliculi, and irregular indentation and shallow grooves. No pathognomonic findings of skin or hair were identified.


Inheritance

The transmission pattern of AEC in family A reported by Dianzani et al. (2003) was consistent with autosomal dominant inheritance.


Molecular Genetics

Some phenotypic overlap can be recognized with Hay-Wells syndrome and other ectodermal dysplasia syndromes, including ectrodactyly-ectodermal dysplasia-cleft lip/palate (EEC; 604292). Celli et al. (1999) demonstrated that heterozygous mutations in the TP63 gene are the major cause of EEC syndrome. McGrath et al. (2001) analyzed the TP63 gene in AEC syndrome patients and identified missense mutations in 8 families. All mutations gave rise to amino acid substitutions in the sterile alpha motif (SAM) domain, and were predicted to affect protein-protein interactions. In contrast, the vast majority of the mutations found in EEC syndrome are amino acid substitutions in the DNA-binding domain. The authors suggested that a distinct genotype-phenotype correlation can be recognized for EEC and AEC syndromes.

In 2 sibs and their mother who had been diagnosed with Rapp-Hodgkin syndrome (RHS; 129400), Dianzani et al. (2003) identified a 1-bp deletion in the TP63 gene (603273.0017). The mother had a slight ankyloblepharon on the right eye at birth which was surgically treated; Dianzani et al. (2003) suggested that AEC and RHS are the same clinical entity.

In a patient with AEC previously described by Bertola et al. (2000), Bertola et al. (2004) identified an ile510-to-thr mutation in the TP63 gene (603273.0018). They identified the same mutation in a patient with RHS and concluded that AEC and RHS represent variable expression of a single genetic disorder.

In an 11-year-old boy who displayed an overlapping phenotype with features of both AEC and RHS, Prontera et al. (2008) identified heterozygosity for an 11-bp duplication in the TP63 gene (603273.0027). The authors stated that their findings confirmed the hypothesis that AEC and RHS are variable expressions of a single genetic disorder, and suggested that intermediate phenotypes are possible.


Animal Model

Koster et al. (2009) generated mice with downregulated delta-N-p63-alpha, the predominantly expressed TP63 isoform in postnatal skin. The mutant mouse epidermis developed severe skin erosions resembling those of AEC patients and similarly characterized by suprabasal epidermal proliferation, delayed terminal differentiation, and basement membrane abnormalities. The authors suggested that by failing to provide structural stability to the epidermis, these defects likely contribute to the observed skin fragility.


REFERENCES

  1. Bertola, D. R., Kim, C. A., Albano, L. M. J., Scheffer, H., Meijer, R., van Bokhoven, H. Molecular evidence that AEC syndrome and Rapp-Hodgkin syndrome are variable expression of a single genetic disorder. (Letter) Clin. Genet. 66: 79-80, 2004. [PubMed: 15200513] [Full Text: https://doi.org/10.1111/j.0009-9163.2004.00278.x]

  2. Bertola, D. R., Kim, C. A., Sugayama, S. M. M., Albano, L. M. J., Utagawa, C. Y., Gonzalez, C. H. AEC syndrome and CHAND syndrome: further evidence of clinical overlapping in the ectodermal dysplasias. Pediat. Derm. 17: 218-221, 2000. [PubMed: 10886756] [Full Text: https://doi.org/10.1046/j.1525-1470.2000.01756.x]

  3. Celli, J., Duijf, P., Hamel, B. C. J., Bamshad, M., Kramer, B., Smits, A. P. T., Newbury-Ecob, R., Hennekam, R. C. M., Van Buggenhout, G., van Haeringen, A., Woods, C. G., van Essen, A. J., de Waal, R., Vriend, G., Haber, D. A., Yang, A., McKeon, F., Brunner, H. G., van Bokhoven, H. Heterozygous germline mutations in the p53 homolog p63 are the cause of EEC syndrome. Cell 99: 143-153, 1999. [PubMed: 10535733] [Full Text: https://doi.org/10.1016/s0092-8674(00)81646-3]

  4. Cole, P., Hatef, D. A., Kaufman, Y., Magruder, A., Bree, A., Friedman, E., Sindwani, R., Hollier, L. H., Jr. Facial clefting and oroauditory pathway manifestations in ankyloblepharon-ectodermal defects-cleft lip/palate (AEC) syndrome. Am. J. Med. Genet. 149A: 1910-1915, 2009. [PubMed: 19697430] [Full Text: https://doi.org/10.1002/ajmg.a.32836]

  5. Dianzani, I., Garelli, E., Gustavsson, P., Carando, A., Gustafsson, B., Dahl, N., Anneren, G. Rapp-Hodgkin and AEC syndromes due to a new frameshift mutation in the TP63 gene. J. Med. Genet. 40: e133, 2003. Note: Electronic Article. [PubMed: 14684701] [Full Text: https://doi.org/10.1136/jmg.40.12.e133]

  6. Dishop, M. K., Bree, A. F., Hicks, M. J. Pathologic changes of skin and hair in ankyloblepharon-ectodermal defects-cleft lip/palate (AEC) syndrome. Am. J. Med. Genet. 149A: 1935-1941, 2009. [PubMed: 19697429] [Full Text: https://doi.org/10.1002/ajmg.a.32826]

  7. Fete, M., vanBokhoven, H., Clements, S. E., McKeon, F., Roop, D. R., Koster, M. I., Missero, C., Attardi, L. D., Lombillo, V. A., Ratovitski, E., Julapalli, M., Ruths, D., Sybert, V. P., Siegfried, E. C., Bree, A. F. International Research Symposium on ankyloblepharon-ectodermal defects-cleft lip/palate (AEC) syndrome. Am. J. Med. Genet. 149A: 1885-1893, 2009. [PubMed: 19353643] [Full Text: https://doi.org/10.1002/ajmg.a.32761]

  8. Greene, S. L., Michels, V. V., Doyle, J. A. Variable expression in ankyloblepharon-ectodermal defects-cleft lip and palate syndrome. Am. J. Med. Genet. 27: 207-212, 1987. [PubMed: 3605196] [Full Text: https://doi.org/10.1002/ajmg.1320270123]

  9. Hay, R. J., Wells, R. S. The syndrome of ankyloblepharon, ectodermal defects and cleft lip and palate: an autosomal dominant condition. Brit. J. Derm. 94: 277-289, 1976. [PubMed: 946410] [Full Text: https://doi.org/10.1111/j.1365-2133.1976.tb04384.x]

  10. Koster, M. I., Marinari, B., Payne, A. S., Kantaputra, P. N., Costanzo, A., Roop, D. R. Delta-Np63 knockdown mice: a mouse model for AEC syndrome. Am. J. Med. Genet. 149A: 1942-1947, 2009. [PubMed: 19681108] [Full Text: https://doi.org/10.1002/ajmg.a.32794]

  11. McGrath, J. A., Duijf, P. H. G., Doetsch, V., Irvine, A. D., de Waal, R., Vanmolkot, K. R. J., Wessagowit, V., Kelly, A., Atherton, D. J., Griffiths, W. A. D., Orlow, S. J., van Haeringen, A., Ausems, M. G. E. M., Yang, A., McKeon, F., Bamshad, M. A., Brunner, H. G., Hamel, B. C. J., van Bokhoven, H. Hay-Wells syndrome is caused by heterozygous missense mutations in the SAM domain of p63. Hum. Molec. Genet. 10: 221-229, 2001. [PubMed: 11159940] [Full Text: https://doi.org/10.1093/hmg/10.3.221]

  12. Prontera, P., Escande, F., Cocchi, G., Donti, E., Martini, A., Sensi, A. An intermediate phenotype between Hays-Wells and Rapp-Hodgkin syndromes in a patient with a novel p63 mutation: confirmation of a variable phenotypic spectrum with a common aetiology. Genet. Counsel. 19: 397-402, 2008. [PubMed: 19239083]

  13. Seres-Santamaria, A., Arimany, J. L., Muniz, F. Two sibs with cleft palate, ankyloblepharon, alveolar synechiae, and ectodermal defects: a new recessive syndrome? J. Med. Genet. 30: 793-795, 1993. [PubMed: 8411079] [Full Text: https://doi.org/10.1136/jmg.30.9.793]

  14. Spiegel, J., Colton, A. AEC syndrome: ankyloblepharon, ectodermal defects, and cleft lip and palate. J. Am. Acad. Derm. 12: 810-815, 1985. [PubMed: 3839246] [Full Text: https://doi.org/10.1016/s0190-9622(85)70100-4]

  15. Sutton, V. R., Plunkett, K., Dang, D. X., Lewis, R. A., Bree, A. F., Bacino, C. A. Craniofacial and anthropometric phenotype in ankyloblepharon-ectodermal defects-cleft lip/palate syndrome (Hay-Wells syndrome) in a cohort of 17 patients. Am. J. Med. Genet. 149A: 1916-1921, 2009. [PubMed: 19676059] [Full Text: https://doi.org/10.1002/ajmg.a.32791]

  16. Weiss, A. H., Riscile, G., Kousseff, B. G. Ankyloblepharon filiforme adnatum. Am. J. Med. Genet. 42: 369-373, 1992. [PubMed: 1536181] [Full Text: https://doi.org/10.1002/ajmg.1320420324]


Contributors:
Marla J. F. O'Neill - updated : 7/12/2011
Marla J. F. O'Neill - updated : 6/9/2010
Marla J. F. O'Neill - updated : 8/4/2005
George E. Tiller - updated : 4/17/2001

Creation Date:
Victor A. McKusick : 5/19/1987

Edit History:
alopez : 12/15/2022
alopez : 05/16/2022
carol : 06/11/2021
alopez : 06/10/2021
carol : 01/22/2020
carol : 10/09/2018
carol : 10/22/2013
wwang : 7/15/2011
terry : 7/12/2011
wwang : 6/10/2010
terry : 6/9/2010
wwang : 5/7/2009
wwang : 8/5/2005
terry : 8/4/2005
cwells : 4/26/2001
cwells : 4/20/2001
cwells : 4/17/2001
terry : 4/30/1999
mark : 11/1/1995
mimadm : 3/11/1994
carol : 11/3/1993
carol : 11/2/1993
carol : 10/29/1993
supermim : 3/16/1992



NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2025 Johns Hopkins University.

NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2025 Johns Hopkins University.
Printed: March 5, 2025