Antley–Bixler syndrome
Editor-In-Chief: Prab R Tumpati, MD
Obesity, Sleep & Internal medicine
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Antley–Bixler syndrome | |
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Synonyms | Trapezoidocephaly-synostosis syndrome |
Pronounce | N/A |
Specialty | N/A |
Symptoms | Craniosynostosis, midface hypoplasia, radiohumeral synostosis, femoral bowing, joint contractures, genital abnormalities |
Complications | Respiratory distress, developmental delay |
Onset | Congenital |
Duration | Lifelong |
Types | N/A |
Causes | Mutations in the FGFR2 or POR genes |
Risks | Family history of the condition |
Diagnosis | Genetic testing, clinical evaluation |
Differential diagnosis | Crouzon syndrome, Apert syndrome, Pfeiffer syndrome |
Prevention | N/A |
Treatment | Surgical intervention, supportive care |
Medication | N/A |
Prognosis | Variable, depending on severity |
Frequency | Rare |
Deaths | N/A |
A rare genetic disorder affecting bone and cartilage development
Antley–Bixler syndrome is a rare genetic disorder characterized by skeletal malformations and other systemic abnormalities. It is primarily associated with autosomal recessive inheritance patterns, although some cases may arise from autosomal dominant mutations. The syndrome is named after Dr. Ray M. Antley and Dr. David Bixler, who first described the condition.
Clinical Features
Antley–Bixler syndrome presents with a variety of clinical features, which can vary in severity among affected individuals. Common characteristics include:
- Craniosynostosis: Premature fusion of the skull bones, leading to an abnormal head shape.
- Midface hypoplasia: Underdevelopment of the midfacial region, often resulting in a flattened appearance.
- Radiohumeral synostosis: Fusion of the radius and humerus bones in the arm, limiting movement.
- Femoral bowing: Abnormal curvature of the femur, or thigh bone.
- Joint contractures: Stiffness and limited range of motion in the joints.
- Genital abnormalities: Ambiguous genitalia or underdeveloped genital structures.
Genetics
Antley–Bixler syndrome is most commonly associated with mutations in the FGFR2 gene, which encodes the fibroblast growth factor receptor 2. This gene plays a crucial role in bone development and growth. Mutations in the POR gene, which is involved in steroidogenesis and drug metabolism, have also been implicated in some cases. The condition can be inherited in an autosomal recessive manner, meaning that an affected individual must inherit two copies of the mutated gene, one from each parent. In some cases, autosomal dominant inheritance has been observed, where a single copy of the mutated gene can cause the disorder.
Diagnosis
Diagnosis of Antley–Bixler syndrome is based on clinical evaluation, family history, and genetic testing. Imaging studies, such as X-rays and CT scans, are used to assess skeletal abnormalities. Genetic testing can confirm mutations in the FGFR2 or POR genes.
Management
Management of Antley–Bixler syndrome is multidisciplinary, involving specialists in orthopedics, genetics, endocrinology, and plastic surgery. Treatment focuses on addressing specific symptoms and may include:
- Surgical correction of craniosynostosis and other skeletal deformities.
- Hormonal therapy for endocrine abnormalities.
- Physical therapy to improve joint mobility and muscle strength.
Prognosis
The prognosis for individuals with Antley–Bixler syndrome varies depending on the severity of the symptoms and the presence of associated complications. Early intervention and comprehensive management can improve quality of life and functional outcomes.
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Contributors: Prab R. Tumpati, MD