National Center for Advancing and Translational Sciences Genetic and Rare Diseases Information Center, a program of the National Center for Advancing and Translational Sciences

Opitz G/BBB syndrome


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Other Names:
Hypospadias-dysphagia, syndrome; Opitz-Frias syndrome; G syndrome; Hypospadias-dysphagia, syndrome; Opitz-Frias syndrome; G syndrome; Opitz-G syndrome, type 2; Hypertelorism hypospadias syndrome; Hypertelorism with esophageal abnormality and hypospadias; BBB syndrome; Telecanthus with associated abnormalities; Opitz BBBG syndrome; GBBB syndrome See More

Opitz G/BBB syndrome is an inherited condition that affects several structures along the midline of the body. The most common features are wide-spaced eyes and defects of the larynx, trachea, and/or esophagus causing breathing problems and difficulty swallowing. Affected males usually have a urethra opening on the underside of the penis (hypospadias). Other features can include mild intellectual disability, cleft lip and/or a cleft palate, heart defects, an obstruction of the anal opening (imperforate anus), agenesis of the corpus callosum, and facial abnormalities. These features may vary, even among members of the same family.[1]

There are two forms of Opitz G/BBB syndrome, which are distinguished by their genetic causes and patterns of inheritance. The X-linked form is caused by mutations in the MID1 gene. Autosomal dominant Opitz G/BBB syndrome is caused by a deletion of 22q11.2, and is often referred to as 22q11.2 deletion syndrome.[1]

Treatment depends on the individual’s specific needs.[2]
Last updated: 11/14/2016

Opitz G/BBB syndrome mainly affects structures along the midline of the body. The most common features of the condition, knwon as major anomalies, are:[3]
  • Wide-spaced eyes (hypertelorism)
  • Defects of the larynx, trachea, and/or esophagus causing breathing problems and difficulty swallowing (dysphagia
  • Urethra opening on the underside of the penis (hypospadias). 
Other frequent findings (minor anomalies) include:[3510[3]
  • Mild intellectual disability and developmental delay occur in about 50 percent of people with Opitz G/BBB syndrome
  • Delays in motor skills, speech delays, and learning difficulties 
  • Features similar to autistic spectrum disorders, including impaired communication and socialization skills 
  • Cleft lip with or without a cleft palate. Some have cleft palate alone.
  • Heart defects
  • Obstruction of the anal opening (imperforate anus)
  • Brain defects such as an absence of the tissue connecting the left and right halves of the brain (agenesis of the corpus callosum) which occur in less than 50 percent of those affected
  • Facial dysmorphism such as a flat nasal bridge, thin upper lip, and low set ears.
These features vary among affected individuals, even within the same family.[1] 

The signs and symptoms of the autosomal dominant form of the condition are comparable to those seen in the X-linked form. However, the X-linked form of Opitz G/BBB syndrome tends to include cleft lip with or without cleft palate, while cleft palate alone is more common in the autosomal dominant form. Females with X-linked Opitz G/BBB syndrome are usually mildly affected, as hypertelorism may be the only sign of the disorder.[1]
Last updated: 11/14/2016

This table lists symptoms that people with this disease may have. For most diseases, symptoms will vary from person to person. People with the same disease may not have all the symptoms listed. This information comes from a database called the Human Phenotype Ontology (HPO) . The HPO collects information on symptoms that have been described in medical resources. The HPO is updated regularly. Use the HPO ID to access more in-depth information about a symptom.

Showing of 76 |
Medical Terms Other Names
Learn More:
HPO ID
80%-99% of people have these symptoms
Abnormality of the pharynx 0000600
Anteverted nares
Nasal tip, upturned
Upturned nasal tip
Upturned nose
Upturned nostrils
[ more ]
0000463
Epicanthus
Eye folds
Prominent eye folds
[ more ]
0000286
30%-79% of people have these symptoms
Abnormality of the voice
Voice abnormality
0001608
Intellectual disability
Mental deficiency
Mental retardation
Mental retardation, nonspecific
Mental-retardation
[ more ]
0001249
Respiratory insufficiency
Respiratory impairment
0002093
5%-29% of people have these symptoms
Cleft palate
Cleft roof of mouth
0000175
Craniosynostosis 0001363
Downslanted palpebral fissures
Downward slanting of the opening between the eyelids
0000494
Hypodontia
Failure of development of between one and six teeth
0000668
Increased number of teeth
Extra teeth
Increased tooth count
Supplemental teeth
[ more ]
0011069
Large fontanelles
Wide fontanelles
0000239
Low-set ears
Low set ears
Lowset ears
[ more ]
0000369
Pectus carinatum
Pigeon chest
0000768
Pectus excavatum
Funnel chest
0000767
Prominent metopic ridge 0005487
Sensorineural hearing impairment 0000407
Percent of people who have these symptoms is not available through HPO
Abnormal heart morphology
Abnormality of the heart
Abnormally shaped heart
Heart defect
[ more ]
0001627
Abnormality of cardiovascular system morphology 0030680
Abnormality of the kidney
Abnormal kidney
0000077
Abnormality of the nasopharynx 0001739
Abnormality of the ureter 0000069
Absent gallbladder 0011467
Agenesis of corpus callosum 0001274
Anal atresia
Absent anus
0002023
Anal stenosis
Narrowing of anal opening
0002025
Aplasia/Hypoplasia of the cerebellar vermis 0006817
Aspiration 0002835
Atrial septal defect
An opening in the wall separating the top two chambers of the heart
Hole in heart wall separating two upper heart chambers
[ more ]
0001631
Autosomal dominant inheritance 0000006
Bifid scrotum
Cleft of scrotum
0000048
Bifid uvula 0000193
Cavum septum pellucidum 0002389
Cerebellar vermis hypoplasia 0001320
Cerebral cortical atrophy
Decrease in size of the outer layer of the brain due to loss of brain cells
0002120
Cleft upper lip
Harelip
0000204
Coarctation of aorta
Narrowing of aorta
Narrowing of the aorta
[ more ]
0001680
Conductive hearing impairment
Conductive deafness
Conductive hearing loss
[ more ]
0000405
Cranial asymmetry 0000267
Cryptorchidism
Undescended testes
Undescended testis
[ more ]
0000028
Depressed nasal bridge
Depressed bridge of nose
Flat bridge of nose
Flat nasal bridge
Flat, nasal bridge
Flattened nasal bridge
Low nasal bridge
Low nasal root
[ more ]
0005280
Diastasis recti
Gap between large left and right abdominal muscles
0001540
Dysphagia
Poor swallowing
Swallowing difficulties
Swallowing difficulty
[ more ]
0002015
Frontal bossing 0002007
Gastroesophageal reflux
Acid reflux
Acid reflux disease
Heartburn
[ more ]
0002020
Generalized hypotonia
Decreased muscle tone
Low muscle tone
[ more ]
0001290
Global developmental delay 0001263
Hiatus hernia
Stomach hernia
0002036
High palate
Elevated palate
Increased palatal height
[ more ]
0000218
Hoarse cry 0001615
Hypertelorism
Wide-set eyes
Widely spaced eyes
[ more ]
0000316
Hypospadias 0000047
Infantile onset
Onset in first year of life
Onset in infancy
[ more ]
0003593
Inguinal hernia 0000023
Laryngeal cleft 0008751
Micrognathia
Little lower jaw
Small jaw
Small lower jaw
[ more ]
0000347
Muscular hypotonia
Low or weak muscle tone
0001252
Patent ductus arteriosus 0001643
Posterior pharyngeal cleft 0006783
Posteriorly rotated ears
Ears rotated toward back of head
0000358
Prominent forehead
Pronounced forehead
Protruding forehead
[ more ]
0011220
Pulmonary arterial hypertension
Increased blood pressure in blood vessels of lungs
0002092
Pulmonary hypoplasia
Small lung
Underdeveloped lung
[ more ]
0002089
Short lingual frenulum 0000200
Smooth philtrum 0000319
Strabismus
Cross-eyed
Squint
Squint eyes
[ more ]
0000486
Telecanthus
Corners of eye widely separated
0000506
Thin upper lip vermilion
Thin upper lip
0000219
Tracheoesophageal fistula 0002575
Umbilical hernia 0001537
Ventricular septal defect
Hole in heart wall separating two lower heart chambers
0001629
Ventriculomegaly 0002119
Weak cry 0001612
Wide nasal bridge
Broad nasal bridge
Broad nasal root
Broadened nasal bridge
Increased breadth of bridge of nose
Increased breadth of nasal bridge
Increased width of bridge of nose
Increased width of nasal bridge
Nasal bridge broad
Wide bridge of nose
Widened nasal bridge
[ more ]
0000431
Widow's peak
Hairline peak
Hairline point
Pointed hairline at front of head
V-shaped frontal hairline
[ more ]
0000349
X-linked recessive inheritance 0001419
Showing of 76 |
Last updated: 7/1/2020

The X-linked form of Opitz G/BBB syndrome is caused by mutations in the MID1 gene. The MID1 gene provides instructions for making a specific protein called midline-1. This protein helps regulate the function of microtubules, which are rigid, hollow fibers that make up the cell's structural framework (the cytoskeleton). Microtubules help cells maintain their shape, assist in the process of cell division, and are essential for the movement of cells (cell migration).[1] The MID1 gene is a member of a group of genes called the TRIM (tripartite motif) family. The proteins produced from this large family of genes are involved in many cellular activities. Primarily, TRIM proteins play a role in the cell machinery that breaks down (degrades) unwanted proteins. As part of its protein degrading function, midline-1 is responsible for recycling certain proteins, including phosphatase 2A (PP2A), integrin alpha-4 (ITGA4), and serine/threonine-protein kinase 36 (STK36). The recycling of these three proteins so they can be reused instead of broken down is essential because they are needed for normal cellular functioning. Mutations in the MID1 gene lead to a decrease in midline-1 function, which prevents this protein recycling. As a result, certain proteins are not recycled, and they buildup in cells. This buildup impairs microtubule function, resulting in problems with cell division and migration. Researchers speculate that the altered midline-1 protein affects how the cells divide and migrate along the midline of the body during development, resulting in the features of Opitz G/BBB syndrome.[4]

Some people who have a family history of X-linked Opitz G/BBB syndrome have no detectable MID1 mutation. The reason for this is not yet known, although some researchers have suggested the involvement of other unknown genes.[1]

The autosomal dominant form of Opitz G/BBB syndrome is caused by a deletion of a small piece of chromosome 22, specifically 22q11.2, which is why researchers consider this condition to be part of 22q11.2 deletion syndrome. It is not yet known which deleted gene(s) within this region of chromosome 22 specifically cause the signs and symptoms of Opitz G/BBB syndrome. In others with autosomal dominant Opitz G/BBB syndrome, the cause is related to a mutation in the SPECCIL gene.[1] 
Last updated: 11/14/2016

Opitz G/BBB syndrome often has an X-linked pattern of inheritance. A condition is considered X-linked if the mutated gene that causes the disorder is located on the X chromosome, one of the two sex chromosomes (the other sex chromosome is the Y chromosome). In most cases, males experience more severe symptoms of the disorder than females. This is because females have two different X chromosomes in each cell, and males have one X chromosome and one Y chromosome. A characteristic of X-linked inheritance is that fathers cannot pass X-linked traits to their sons, because fathers only pass a Y chromosome on to their sons (which is what makes them male). In some cases, an affected person inherits a mutation in the MID1 gene from an affected parent, while in other cases, it may result from a new mutation (de novo) in the affected individual. These cases occur in people with no history of the disorder in their family.[1]

A female who has the X-linked form of Opitz G/BBB syndrome has a 25% (1 in 4) chance to have a daughter with the mutation, a 25% chance to have a son with the mutation, a 25% chance to have an unaffected daughter, and a 25% chance to have an unaffected son. This also means that there is a 50% chance, with each pregnancy, for the child to inherit the mutation. A male with the X-linked dominant form of Opitz G/BBB syndrome will pass the mutation on to all of his daughters and none of his sons.

Researchers have also described an autosomal dominant form of Opitz G/BBB syndrome caused by a deletion in one copy of chromosome 22 in each cell. In some cases, an affected person inherits the chromosome with a deleted segment from a parent, while in other cases, the condition results from a new deletion in the affected individual. These cases occur in people with no history of the disorder in their family. Males and females with the autosomal dominant form of Opitz G/BBB syndrome usually have the same degree of severity of symptoms.[1] A male or female who has the autosomal dominant form of Opitz G/BBB syndrome has a 50% (1 in 2) chance with each pregnancy for the child (male or female) to inherit the genetic abnormality.
Last updated: 11/14/2016

The diagnosis of Opitz G/BBB syndrome is usually based on clinical findings. In order to differentiate the X-linked form from 22q11.2 deletion syndrome (the autosomal dominant form), the pattern of inheritance within the family may be assessed. Molecular genetic testing for mutations in the MID1 gene is available for confirmation. Between 15 and 45% of males with clinically diagnosed Opitz G/BBB syndrome are found to have a mutation in this gene.[3][5]
Last updated: 11/14/2016

Testing Resources

  • The Genetic Testing Registry (GTR) provides information about the genetic tests for this condition. The intended audience for the GTR is health care providers and researchers. Patients and consumers with specific questions about a genetic test should contact a health care provider or a genetics professional.

Because of the wide range of signs and symptoms that may be present in affected individuals, management of Opitz G/BBB syndrome typically incorporates a multidisciplinary team consisting of various specialists. Treatment for the condition may include surgery for significant abnormalities involving the larynx, trachea and/or esophagus; surgical intervention as needed for hypospadias, cleft lip and/or cleft palate, and imperforate anus; therapy for speech problems; surgical repair as needed for heart defects; neuropsychological support; and special education services.[3]
Last updated: 11/14/2016

If you need medical advice, you can look for doctors or other healthcare professionals who have experience with this disease. You may find these specialists through advocacy organizations, clinical trials, or articles published in medical journals. You may also want to contact a university or tertiary medical center in your area, because these centers tend to see more complex cases and have the latest technology and treatments.

If you can’t find a specialist in your local area, try contacting national or international specialists. They may be able to refer you to someone they know through conferences or research efforts. Some specialists may be willing to consult with you or your local doctors over the phone or by email if you can't travel to them for care.

You can find more tips in our guide, How to Find a Disease Specialist. We also encourage you to explore the rest of this page to find resources that can help you find specialists.

Healthcare Resources


Related diseases are conditions that have similar signs and symptoms. A health care provider may consider these conditions in the table below when making a diagnosis. Please note that the table may not include all the possible conditions related to this disease.

Conditions with similar signs and symptoms from Orphanet
XLOS and ADOS can be differentiated based on the mode of inheritance. Differential diagnoses include FG syndrome, craniofrontonasal dysplasia, and Mowat-Wilson syndrome (see these terms).
Visit the Orphanet disease page for more information.

Support and advocacy groups can help you connect with other patients and families, and they can provide valuable services. Many develop patient-centered information and are the driving force behind research for better treatments and possible cures. They can direct you to research, resources, and services. Many organizations also have experts who serve as medical advisors or provide lists of doctors/clinics. Visit the group’s website or contact them to learn about the services they offer. Inclusion on this list is not an endorsement by GARD.

Organizations Supporting this Disease


These resources provide more information about this condition or associated symptoms. The in-depth resources contain medical and scientific language that may be hard to understand. You may want to review these resources with a medical professional.

Where to Start

  • Genetics Home Reference (GHR) contains information on Opitz G/BBB syndrome. This website is maintained by the National Library of Medicine.
  • The National Organization for Rare Disorders (NORD) has a report for patients and families about this condition. NORD is a patient advocacy organization for individuals with rare diseases and the organizations that serve them.

In-Depth Information

  • GeneReviews provides current, expert-authored, peer-reviewed, full-text articles describing the application of genetic testing to the diagnosis, management, and genetic counseling of patients with specific inherited conditions.
  • The Monarch Initiative brings together data about this condition from humans and other species to help physicians and biomedical researchers. Monarch’s tools are designed to make it easier to compare the signs and symptoms (phenotypes) of different diseases and discover common features. This initiative is a collaboration between several academic institutions across the world and is funded by the National Institutes of Health. Visit the website to explore the biology of this condition.
  • Online Mendelian Inheritance in Man (OMIM) is a catalog of human genes and genetic disorders. Each entry has a summary of related medical articles. It is meant for health care professionals and researchers. OMIM is maintained by Johns Hopkins University School of Medicine. 
    X-linked Opitz G/BBB syndrome
    Autosomal dominant Opitz G/BBB syndrome
  • Orphanet is a European reference portal for information on rare diseases and orphan drugs. Access to this database is free of charge.
  • PubMed is a searchable database of medical literature and lists journal articles that discuss Opitz G/BBB syndrome. Click on the link to view a sample search on this topic.

Questions sent to GARD may be posted here if the information could be helpful to others. We remove all identifying information when posting a question to protect your privacy. If you do not want your question posted, please let us know. Submit a new question

  • We have been told that my son has Opitz G syndrome. The hospital did not do any tests, they just looked in a book. How can we be sure that he has this condition? Is there a cure? Can it be treated? See answer

  • My son was diagnosed with Opitz G/BBB syndrome and I was wondering if you can provide any information about this syndrome. I would like to have a full understanding of my son and his condition. See answer



  1. Opitz G/BBB syndrome. Genetics Home Reference. January 2015; http://ghr.nlm.nih.gov/condition/opitz-g-bbb-syndrome.
  2. McDonald-McGinn DM, Emanuel BS, Zackai EH. 22q11.2 deletion syndrome. GeneReviews. February 28, 2013; https://www.ncbi.nlm.nih.gov/books/NBK1523.
  3. Meroni G. X-Linked Opitz G/BBB Syndrome. GeneReviews. July 28, 2011; http://www.ncbi.nlm.nih.gov/books/NBK1327/.
  4. MID1. Genetics Home Reference. January 2015; http://ghr.nlm.nih.gov/gene/MID1.
  5. Germana Meroni. X-linked Opitz G/BBB syndrome. National Organization for Rare Disorders (NORD). 2015; http://rarediseases.org/rare-diseases/x-linked-opitz-gbbb-syndrome/.