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

Temtamy syndrome


Other Names:
Dysmorphism, corpus callosum agenesis and colobomas; Craniofacial dysmorphism with ocular coloboma absent corpus callosum and aortic dilatation
Categories:
Temtamy syndrome is a developmental neurological disorder, meaning that it affects the way the brain is formed and how well it functions. In most cases, the bundle of nerve fibers (the corpus callosum) that connects the two sides of the brain is partially or completely missing. Other symptoms may include seizures, changes in the size or function of the eyes, heart problems, intellectual disability, and developmental delay. The syndrome appears to be more common in people from the Middle East, especially Saudi Arabia.[1][2][3]

Temtamy syndrome is caused by genetic changes (pathogenic variants or mutations) in the C12orf57 gene. The syndrome is inherited in an autosomal recessive manner. Diagnosis is based on observing symptoms of the syndrome and the results of brain imaging. The diagnosis can be confirmed with genetic testing. Treatment for Temtamy syndrome may include medications to treat seizures, as well as therapies to help manage developmental delays.[1][2][3]
Last updated: 4/17/2018
Temtamy syndrome may affect the development of the brain, eyes, heart, and facial features. Children with Temtamy syndrome typically look different than other children. They may have a long face, widely-spaced eyes (hypertelorism), a large nose, and a small chin (micrognathia). Some children with Temtamy syndrome have relatively large heads (macrocephaly). These facial features may be present from birth. Other physical features of the syndrome may include having short fingers and toes (brachydactyly), bowed legs, or flat feet (pes planus).[1][2][3]

People with Temtamy syndrome may have differences in the brain that can be seen on brain imaging. The most common feature is having a part of the brain, called the corpus callosum, that is smaller than expected, completely absent, or may be unusually thick. The corpus callosum is the bundle of nerves fibers that allows information to easily and quickly travel from one side of the brain to the other (between the left and right hemisphere). Problems in the development of the white matter of the brain may also be present. The white matter is the part of the brain made up of nerve fibers and myelin. Myelin forms a fatty, protective layer around nerve fibers, insulating the fibers so nerve signals pass through quickly.[1][2][3] 

Other neurological symptoms of Temtamy syndrome can include seizures and intellectual disability. Children with Temtamy syndrome may have low muscle tone (hypotonia) and they may meet milestones such as sitting up or walking later than other children do (developmental delay). Some children with Temtamy syndrome have autism.[1][2][3]

Temtamy syndrome can also cause changes in the eyes, including changes in the tissues that form the eye (coloboma). Some people with Temtamy syndrome have one or both eyes that are smaller than expected (microphthalmia). These changes of the eyes may affect vision. Some people with Temtamy syndrome are born with heart problems because the heart did not form correctly.[1][2][3] 

The signs and symptoms of Temtamy syndrome can vary from person to person, even among members of the same family. This is a concept called variable expressivity.[2] 
Last updated: 4/17/2018

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.

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Medical Terms Other Names
Learn More:
HPO ID
80%-99% of people have these symptoms
Aplasia/Hypoplasia of the corpus callosum 0007370
Brachydactyly
Short fingers or toes
0001156
Chorioretinal coloboma
Birth defect that causes a hole in the innermost layer at the back of the eye
0000567
Global developmental delay 0001263
Hypertelorism
Wide-set eyes
Widely spaced eyes
[ more ] 		0000316
Intellectual disability
Mental deficiency
Mental retardation
Mental retardation, nonspecific
Mental-retardation
[ more ] 		0001249
Iris coloboma
Cat eye
0000612
Short toe
Short toes
Stubby toes
[ more ] 		0001831
30%-79% of people have these symptoms
Aortic aneurysm
Bulge in wall of large artery that carries blood away from heart
0004942
Coarse facial features
Coarse facial appearance
0000280
Convex nasal ridge
Beaked nose
Beaklike protrusion
Hooked nose
Polly beak nasal deformity
[ more ] 		0000444
Dolichocephaly
Long, narrow head
Tall and narrow skull
[ more ] 		0000268
Genu varum
Outward bow-leggedness
Outward bowing at knees
[ more ] 		0002970
Long face
Elongation of face
Increased height of face
Increased length of face
Vertical elongation of face
Vertical enlargement of face
Vertical overgrowth of face
[ more ] 		0000276
Low-set ears
Low set ears
Lowset ears
[ more ] 		0000369
Macrocephaly
Increased size of skull
Large head
Large head circumference
[ more ] 		0000256
Micrognathia
Little lower jaw
Small jaw
Small lower jaw
[ more ] 		0000347
Pes planus
Flat feet
Flat foot
[ more ] 		0001763
5%-29% of people have these symptoms
Abnormal palate morphology
Abnormality of the palate
Abnormality of the roof of the mouth
[ more ] 		0000174
Clinodactyly of the 5th finger
Permanent curving of the pinkie finger
0004209
Facial asymmetry
Asymmetry of face
Crooked face
Unsymmetrical face
[ more ] 		0000324
Joint hyperflexibility
Joints move beyond expected range of motion
0005692
Microphthalmia
Abnormally small eyeball
0000568
Telecanthus
Corners of eye widely separated
0000506
Thick lower lip vermilion
Increased volume of lower lip
Plump lower lip
Prominent lower lip
[ more ] 		0000179
Percent of people who have these symptoms is not available through HPO
Agenesis of corpus callosum 0001274
Aortic regurgitation 0001659
Autosomal recessive inheritance 0000007
Dental crowding
Crowded teeth
Dental overcrowding
Overcrowding of teeth
[ more ] 		0000678
Downslanted palpebral fissures
Downward slanting of the opening between the eyelids
0000494
Frontal bossing 0002007
Generalized hypotonia
Decreased muscle tone
Low muscle tone
[ more ] 		0001290
Highly arched eyebrow
Arched eyebrows
Broad, arched eyebrows
High, rounded eyebrows
High-arched eyebrows
Thick, flared eyebrows
[ more ] 		0002553
Hip dislocation
Dislocated hips
Dislocation of hip
[ more ] 		0002827
Hypoplasia of teeth 0000685
Infantile onset
Onset in first year of life
Onset in infancy
[ more ] 		0003593
Intellectual disability, mild
Mental retardation, borderline-mild
Mild and nonprogressive mental retardation
Mild mental retardation
[ more ] 		0001256
Lens luxation
Dislocated lens
0012019
Long philtrum 0000343
Lop ear 0000394
Myopia
Close sighted
Near sighted
Near sightedness
Nearsightedness
[ more ] 		0000545
Seizure 0001250
Short 2nd toe
Short second toe
0001885
Talipes equinovarus
Club feet
Club foot
Clubfeet
Clubfoot
[ more ] 		0001762
Ventriculomegaly 0002119
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Last updated: 7/1/2020
Temtamy syndrome is caused by genetic changes (pathogenic variants or mutations) in the C12orf57 gene. This gene provides each cell with instructions to make a protein that is thought to be important in the development of the brain, eyes, heart, and face. When there are pathogenic variants in both copies of the C12orf57 gene, not enough working protein is made, or possibly no working protein is made. Without enough of this protein the brain, eyes, heart, and face do not form properly. However, the exact function of the C12orf57 gene is not completely understood.[1][2] 
Last updated: 4/17/2018
Temtamy syndrome is inherited in an autosomal recessive manner.[1] Like most genes, the C12orf57 gene comes in a pair (two copies). One copy of the gene is inherited from each parent. When a syndrome is inherited in an autosomal recessive manner, a person must have a pathogenic variant in both copies of the gene to have the syndrome. People who have a change in only one copy of the C12orf57 gene are carriers of Temtamy syndrome. Carriers typically do not have signs or symptoms of the syndrome. 

When two carriers of Temtamy syndrome have children together, for each child there is a:
  • 25% chance to inherit both changed copies of the C12orf57 gene, meaning the child will have Temtamy syndrome
  • 50% chance to inherit one changed copy of the C12orf57 gene, meaning the child will be a carrier of Temtamy syndrome like each of the parents
  • 25% chance to inherit both working copies of the C12orf57 gene, meaning the child will not have Temtamy syndrome and will not be a carrier of the syndrome
Last updated: 4/17/2018
Temtamy syndrome may be suspected when a baby or child has symptoms of the syndrome including intellectual disabilitydevelopmental delay, problems with the eyes or heart, distinctive facial features, or seizures. Brain imaging such as an MRI may show changes in the way the corpus callosum or white matter of the brain developed.[3] Because Temtamy syndrome is so rare and many of its features are common to other syndromes, most children are diagnosed when they have a genetic test called whole exome sequencing. This test is used to look for genetic changes (mutations or pathogenic variants) in every gene of the body, including the C12orf57 gene.[2][3]
Last updated: 4/17/2018
Unfortunately, there is no cure for Temtamy syndrome. Treatment is aimed at managing the symptoms of the syndrome. These treatment options may include surgeries to treat heart and eye problems and medications to treat seizuresSpeechoccupational, and physical therapies may be important to allow children with Temtamy syndrome to reach their full potentials. Developmental delays may be helped by early intervention programs. Additional help in school may also be required, as most children with Temtamy syndrome have intellectual disability.[1][3]
Last updated: 4/17/2018
Many children who have Temtamy syndrome have seizures that are not managed well with medications. This can cause some children with the syndrome to lose skills that they once had (regress) or have worsening intellectual disability.[1][2] Eye abnormalities may cause problems with vision, and vision may continue to worsen throughout life.[4] In some cases, a baby or child may pass away due to complications such as complex heart problems. However, people with the syndrome can live into adulthood.[2][4] 
Last updated: 4/17/2018

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
Differential diagnoses include muscle-eye-brain disease, Peters-plus, Walker-Warburg, Aicardi, Donnai-Barrow, and Baraitser-Winter syndromes (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.

In-Depth Information

  • 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. 
  • 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 Temtamy 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.

  1. Sherr E. Temtamy syndrome. Orphanet. August 2014; http://www.orpha.net/consor/cgi-bin/OC_Exp.php?lng=en&Expert=1777.
  2. Temtamy Syndrome; TEMTYS. Online Mendelian Inheritance in Man. March 28, 2017; https://www.omim.org/entry/218340.
  3. Alrakaf L, Al-Owain MA, Busehail M, Alotaibi MA, Monies D, Aldhalaan HM, Alhashem A, Al-Hassnan ZN, Rahbeeni ZA, Murshedi FA, Ani NA, Al-Maawali A, Ibrahim NA, Abdulwahab FM, Alsagob M, Hashem MO, Ramadan W, Abouelhoda M, Meyer BF, Kaya N, Maddirevula S, and Alkuraya FS. Further delineation of Temtamy syndrome of corpus callosum and ocular abnormalities. American Journal of Medical Genetics. Part A. March 2018; 176(3):715-721. https://www.ncbi.nlm.nih.gov/pubmed/29383837.
  4. Temtamy Syndrome. Hereditary Ocular Disease Database. The University of Arizona Health Sciences; http://disorders.eyes.arizona.edu/handouts/temtamy-syndrome. Accessed 4/5/2018.