Rosselli–Gulienetti syndrome
(Redirected from Cleft lip palate oligodontia syndactyly pili torti)
Rosselli–Gulienetti syndrome | |
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Synonyms | Zlotogora–Ogur syndrome, Bowen–Armstrong syndrome |
Pronounce | |
Field | Medical genetics, Dermatology |
Symptoms | Cleft lip, cleft palate, intellectual disability, ectodermal dysplasia, ankyoblepharon, nail dysplasia, hypohidrosis, dry skin, delayed bone growth |
Complications | Feeding difficulties, speech problems, recurrent infections |
Onset | Congenital |
Duration | Lifelong |
Types | |
Causes | Mutations in the PVRL1 gene |
Risks | Parental consanguinity |
Diagnosis | Clinical evaluation, genetic testing |
Differential diagnosis | EEC syndrome, AEC syndrome, Rapp–Hodgkin syndrome, Hay–Wells syndrome |
Prevention | Genetic counseling |
Treatment | Supportive care, surgical correction of clefts |
Medication | Symptomatic treatment for skin and nail conditions |
Prognosis | Variable; depends on severity of symptoms |
Frequency | Very rare |
Deaths | Rare; may occur due to complications in severe cases |
Rosselli–Gulienetti syndrome, also known as Zlotogora–Ogur syndrome or Bowen–Armstrong syndrome, is a rare genetic disorder classified under the group of ectodermal dysplasia syndromes. It is characterized by a combination of craniofacial anomalies, intellectual disability, and ectodermal defects affecting the skin, nails, teeth, and hair.
Signs and symptoms
The clinical features vary among affected individuals but typically include:
- Cleft lip and/or cleft palate
- Intellectual disability
- Features of ectodermal dysplasia including:
- Sparse hair
- Dry skin (xerosis)
- Hypohidrosis (reduced sweating)
- Absent or malformed nails
- Tooth abnormalities
- Ankyoblepharon (fused eyelids)
- Delayed bone development
- Feeding and speech difficulties due to clefting
Cause
Rosselli–Gulienetti syndrome is caused by mutations in the PVRL1 gene, located on chromosome 11q23–q24. This gene encodes nectin-1, a cell adhesion molecule important in the development of epithelial tissue. Nectin-1 is also a receptor for certain alpha-herpesviruses, although viral susceptibility is not a clinical feature of the syndrome.
Mutations in PVRL1 disrupt nectin-dependent cell adhesion processes, particularly in keratinocytes, leading to defective development of ectoderm-derived tissues such as skin, nails, and craniofacial structures.
Inheritance
Rosselli–Gulienetti syndrome is inherited in an autosomal recessive pattern, meaning a child must inherit two defective copies of the PVRL1 gene (one from each parent) to be affected. Parents of affected children are typically asymptomatic carriers.
Diagnosis
Diagnosis is based on:
- Recognition of characteristic clinical features
- Family history and inheritance pattern
- Molecular genetic testing confirming mutations in the PVRL1 gene
Differential diagnosis includes other syndromes involving ectodermal dysplasia and clefting, such as AEC syndrome, EEC syndrome, and Rapp–Hodgkin syndrome.
Treatment
There is no specific cure for Rosselli–Gulienetti syndrome. Management focuses on treating individual symptoms:
- Surgical correction of cleft lip and cleft palate
- Supportive care for developmental delays
- Dental interventions for tooth abnormalities
- Skin and nail care with moisturizing agents or dermatologic treatment
- Speech therapy and feeding support
- Genetic counseling for families
Prognosis
The prognosis varies depending on the severity of symptoms. With appropriate supportive care, many individuals can lead stable lives, though developmental and functional impairments may persist.
See also
External links
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