16p13.11 Duplication Syndrome
What is 16p13.11 Duplication Syndrome?
Pieces of genetic information copied and inserted into the wrong place can lead to a rare disease. 16p13.11 microduplication syndrome is caused by the duplication of a region of chromosome 16, located at a designated position called p13.11. The clinical manifestation of 16p13.11 microduplication syndrome varies widely. The diverse clinical picture may include behavioral abnormality, intellectual disability, developmental delay, congenital heart defects, and skeletal abnormalities. 16p13.11 microduplication syndrome is complementary to the 16p13.11 deletion syndrome, both of which share similar characteristics such as developmental delays and intellectual disability.
Synonyms
- Dup(16)(p13.11)
- Trisomy 16p13.11
Pieces of genetic information copied and inserted into the wrong place can lead to a rare disease. 16p13.11 microduplication syndrome is caused by the duplication of a region of chromosome 16, located at a designated position called p13.11. The clinical manifestation of 16p13.11 microduplication syndrome varies widely. The diverse clinical picture may include behavioral abnormality, intellectual disability, developmental delay, congenital heart defects, and skeletal abnormalities. 16p13.11 microduplication syndrome is complementary to the 16p13.11 deletion syndrome, both of which share similar characteristics such as developmental delays and intellectual disability.
The prevalence of this condition is unknown. It has been characterized in fewer than 100 patients.
| Name | Abbreviation |
|---|---|
| Dup(16)(p13.11) | Dup(16)(p13.11) |
| Trisomy 16p13.11 | Trisomy 16p13.11 |
The 16p13.11 microduplication syndrome is caused by a genetic swapping event between two highly similar DNA sequences at position p13.11 of chromosome 16. The duplications can appear de novo (new, and not inherited from either parent) or can be inherited. Patients only need to inherit the mutation from one parent for disease manifestation (also known as autosomal dominant inheritance pattern). Carriers of the 16p13.11 duplication may have mild symptoms or may be completely normal.
The duplicated region of chr16p13.11 encompasses approximately 15 genes. It is suggested that the gene copy number, aka the dosage of these genes, is essential for normal development. A complementary syndrome, where the exact region (16p13.11) is deleted increases people’s susceptibility to neurocognitive diseases. Therefore, too many or too few gene copies are both disruptive to brain development.
The structure of Chromosome 16. Red box labels chr16p13.11, the site of microduplications.
In general, children with 16p13.11 microduplication are healthy at birth. However, up to ~80% of children have behavioral and emotional disorders such as attention deficit hyperactivity disorder (ADHD), language impairment, global developmental delay, hand polydactyly (extra finger), intellectual disability, or joint hyper-flexibility. Some patients may also present aggressive behaviors, abnormal brain sizes, autism spectrum disorder (ASD), anxiety disorder, distinct facial features, congenital heart defects, and vertebral anomalies.
Genetic testing can be performed. Genomic testing methods such as chromosomal microarray (CMA) or targeted duplication analysis (Fluorescence in situ hybridization, FISH, or quantitative PCR) to detect recurrent duplications in the affected individual can help uncover the 16p13.11 microduplication.
Even though there is no treatment available, a diagnosis of behavioral impairments such as Autism or intellectual disability can be important to provide children with early and tailored access to educational and behavioral therapy.
Patients who are generally in good health should have a normal lifespan. Some adults with 16p13.11 microduplication syndrome are reported to develop adult-onset cardiovascular disorder including thoracic aortic aneurysm dissection (TAAD). However, this was reported only in a limited number of patients.
16p13.11 microduplication syndrome (GARD). (2011). Retrieved June 24, 2020, from https://rarediseases.info.nih.gov/diseases/13392/16p1311-microduplication-syndrome
Allach El Khattabi L, Heide S, Caberg JH, et al. 16p13.11 microduplication in 45 new patients: refined clinical significance and genotype-phenotype correlations. J Med Genet. 2020;57(5):301‐307. doi:10.1136/jmedgenet-2018-105389
Hannes, F. D., Sharp, A. J., Mefford, H. C., de Ravel, T., Ruivenkamp, C. A., Breuning, M. H., Fryns, J. P. et al. Recurrent reciprocal deletions and duplications of 16p13.11: the deletion is a risk factor for MR/MCA while the duplication may be a rare benign variant. J. Med. Genet. 46, 223–232 (2008).
Ramalingam, A., Zhou, X., Fiedler, S. et al. 16p13.11 duplication is a risk factor for a wide spectrum of neuropsychiatric disorders. J Hum Genet 56, 541–544 (2011). https://doi.org/10.1038/jhg.2011.42
Rarechromo.org. (n.d.). 16p13.11 microduplications. Retrieved May 20, 2020 from
https://www.rarechromo.org/media/information/Chromosome%2016/16p13.11%20microduplications%20FTNW.pdf
Ullmann, R., Turner, G., Kirchhoff, M., Chen, W., Tonge, B, Rosenberg, C. et al. Array CGH identifies reciprocal 16p13.1 duplications and deletions that predispose to autism and/or mental retardation. Hum. Mutat. 28, 674–682 (2007).
Last updated 14 Jul 2020, 11:09 PM
14 Jul 2020, 11:09 PM
Hi everyone,
The 16p13.11 microduplication syndrome community details have been updated. We added more information about the cause, prevalence, symptoms, diagnosis, and treatment. Hopefully, you find it helpful.
Best regards,
RareShare team
Last updated 19 Aug 2015, 02:45 PM
19 Aug 2015, 02:45 PM
Hello I have just recently found out my 7 yr old son has 16p13.11 diagnosis, I have information about him and would love to compare note, he also has a diagnosis of short stature and he is currently on growth hormones, he sees a child therapist he is very emotionally unstable, they are going to start testing him for other pycosocial disorders. he has two birth defects, Ventricular megaly and no primary teeth for his bottom two teeth, he is a very loving child he is just highly emotional.
19 Sep 2014, 04:25 PM
Hi! I'm Holly. Our daughter, Autumn,age 4 1/2, was diagnosed a couple of years ago. The lack of case studies is frustrating. We have very little information to help us know what to expect. So far, she has been seen by specialists for orthopedics, urology, cardiology, neuro, hearing & something else, but I can't remember. She was seen by genetics once, for diagnosis, but hasn't been seen by them since. She is very tiny. We celebrated this spring when she finally made it onto the growth chart for height. lol Until then, she was always -3 to -5% for height. :-) She is in special ed. & gets speech therapy, pt & ot. I wish I had more info on the actual genetics to give you an outlook, but her geneticist had only one other case study for comparison. There isn't much to go on.
18 Sep 2014, 07:09 PM
Hi, we have a 4 year old daughter Dollee who was diagnosed 2 years ago. We are really interested in comparing notes for want of a better word. We are really struggling with getting information about it and the effects both physically and mentally. I'm Toni and Simon is my other half. Dollee is the baby of 7, 5 girls and 2 boy's. We are really hoping to hear from you soon x
Last updated 19 Sep 2014, 07:20 AM
19 Sep 2014, 07:20 AM
hwagon and blazingcolty, I have a daughter and grandson with this disorder. I am also a member of a support group for this disorder. If you would like to contact me to learn more, you can email me at: diamondnthemaking@yahoo.com. For email topic, please type "16p" so I will know it is important in case it ends up in my spam.
23 Jan 2013, 08:11 PM
I just learned about this site from my son's doctor. We live on Long Island in NY. Would love to talk to someone else with this issue.
7 May 2012, 10:35 PM
Hi! I requested this community be started for those of us whose children have been diagnosed with 16p13.11 partial duplication. I have yet to connect with other parents & would love to chat about our incredible kids!
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