Clinical characteristics.

The 16p11.2 recurrent deletion phenotype is characterized by motor speech disorder, language disorder, motor coordination difficulties, psychiatric conditions, and autistic features. While most, if not all, individuals with the 16p11.2 recurrent deletion experience some degree of developmental delay, the severity varies significantly. Most affected individuals do not have intellectual disability (defined as an IQ of <70), but many have below average cognition and learning disabilities in both verbal and nonverbal domains. Obesity is a feature of this disorder and generally emerges in childhood; BMI in individuals with the 16p11.2 recurrent deletion is significantly higher than in the general population by age five years. Seizures are observed in approximately 25% of individuals with the recurrent deletion. Vertebral anomalies, hearing impairment, macrocephaly, and cardiovascular malformation have each been observed in some individuals. Clinical follow-up data from adults suggests that the greatest medical challenges are obesity and related comorbidities that can be exacerbated by medications used to treat behavioral and psychiatric problems.

Diagnosis/testing.

The diagnosis of 16p11.2 recurrent deletion is established by detection of a heterozygous ~593-kb recurrent deletion at the approximate position of chr16:29638676-30188531 in the reference genome (NCBI Build 38).

Management.

Treatment of manifestations: Treatment should be targeted to the specific deficits identified. Full developmental assessment, including neuropsychological testing by a clinical psychologist, is strongly suggested to establish neurodevelopmental needs and treatment recommendations. Standard treatment by a neurologist for seizures or movement disorders. Because of the high risk of obesity beginning in adolescence, encourage healthy eating habits with attention to portion size and an active lifestyle from a young age. Routine management of vertebral anomalies, hearing loss, and congenital heart defects.

Surveillance: Routine surveillance of growth parameters and calculation of BMI after age two years. Monitor developmental progress and educational needs and provide behavioral assessment at each visit. Monitor those with seizures as clinically indicated and monitor for any new neurologic changes, scoliosis, or hearing loss. For those with obesity, monitor blood pressure and fasting blood glucose.

Genetic counseling.

The 16p11.2 recurrent deletion is de novo in most probands. Less commonly, the deletion is transmitted from a parent to a child in an autosomal dominant manner.

Once a 16p11.2 recurrent deletion has been identified in a family member, prenatal and preimplantation genetic testing are possible. Interpretation of results from prenatal testing is challenging given the inherent difficulty in accurately predicting the phenotype.

Suggestive Findings

The 16p11.2 recurrent deletion should be considered in individuals with the following clinical findings:

• Motor speech disorder, especially childhood apraxia of speech
• Language disorder
• Learning difficulties / intellectual disability
• Social impairments with or without a diagnosis of autism spectrum disorder (ASD)
• Macrocephaly
• Chiari I malformation / cerebellar tonsillar ectopia
• Seizures/epilepsy
• Vertebral anomalies
• Obesity starting in adolescence, and in the setting of developmental delay

Family history. Because the 16p11.2 recurrent deletion is most often caused by a de novo pathogenic variant, most probands represent a simplex case (i.e., a single occurrence in a family). Rarely, the family history may be consistent with autosomal dominant inheritance (e.g., affected males and females in multiple generations).

Establishing the Diagnosis

The diagnosis of the 16p11.2 recurrent deletion is established by identification of a heterozygous ~593-kb deletion at the approximate position of chr16:29638676-30188531 in the reference genome (GRCh38) (sometimes referred to as between BP4 and BP5) (see Table 1 and Molecular Genetics).

Of note, an adjacent (distal) recurrent 16p11.2 deletion (GRCh38 chr16:28811314-29035178), which is also associated with variable features, is not discussed further, as this GeneReview addresses the more proximal chr16:29638676-30188531 recurrent deletion only.

Molecular methods that determine the copy number of sequences can include chromosomal microarray (CMA), exome/genome sequencing with copy number variant calling, or targeted deletion analysis. Note: The 16p11.2 deletion cannot be identified by routine analysis of G-banded chromosomes or other conventional cytogenetic banding techniques.

• Chromosomal microarray (CMA) using oligonucleotide arrays or SNP genotyping arrays can detect the recurrent deletion in a proband. The ability to size the deletion depends on the type of microarray used and the density of probes in the 16p11.2 region.
  Note: (1) Most individuals with the 16p11.2 recurrent deletion are identified by CMA performed in the context of evaluation of developmental delay, intellectual disability, or ASD. (2) Prior to 2008 many CMA platforms did not include coverage for this region and thus may not have detected this deletion.
• Exome and genome sequencing analyses are next-generation sequencing technologies that generate DNA sequence either for all coding regions (exome) or the entire genome. Copy number variant-calling algorithms need to be utilized to detect the 16p11.2 recurrent deletion.
• Targeted deletion analysis. Fluorescent in situ hybridization (FISH) analysis, quantitative PCR (qPCR), multiplex ligation-dependent probe amplification (MLPA), or other targeted quantitative methods may be used to test relatives of a proband known to have the 16p11.2 recurrent deletion.
  Note: (1) Targeted deletion testing is not appropriate for an individual in whom the 16p11.2 recurrent deletion was not detected by CMA designed to target this region. (2) It is not possible to size the deletion routinely by use of targeted methods.

Clinical Description

The 16p11.2 recurrent deletion is one of the most common known genetic causes of neurodevelopmental disorders [Männik et al 2015, Chung et al 2021]. Common clinical features include motor speech disorder, language disorder, motor coordination difficulties, psychiatric conditions, and autistic features. Clinical follow-up data from adults suggest that the greatest medical challenges are obesity and related comorbidities that can be exacerbated by medications used to treat behavioral and psychiatric problems.

Genotype-Phenotype Correlations

No genotype-phenotype correlations have been observed.

Prevalence

The most recent estimate is approximately 1:2,000 in the general population [Männik et al 2015, Chung et al 2021].

16p11.2 Recurrent Duplication

Reciprocal ~593-kb duplication of 16p11.2 is the copy number variant most frequently associated with autism spectrum disorder (ASD), schizophrenia, and decreased BMI [D'Angelo et al 2016]. Other conditions associated with the duplication include attention-deficit/hyperactivity disorder (ADHD), anxiety, intellectual disability, and motor delays [Green Snyder et al 2016]. The prevalence is estimated to be approximately 0.05%–0.09% of the population [Männik et al 2015]. Adults with the 16p11.2 recurrent duplication often have fewer intellectual impairments or psychiatric disorders compared to their children who have the 16p11.2 recurrent duplication [Green Snyder et al 2016]. The duplication has also been reported in at least two individuals with childhood-onset schizophrenia [Walsh et al 2008].

The phenotype of the 16p11.2 recurrent duplication shows more variability than the phenotype of the 16p11.2 recurrent deletion; however, most individuals with the 16p11.2 recurrent duplication are identified by CMA performed in the evaluation of developmental delay, intellectual disability, or ASD, conferring an ascertainment bias that makes the phenotype associated with the 16p11.2 recurrent duplication difficult to establish.

• In a study of 270 individuals with the 16p11.2 recurrent duplication, the mean full-scale IQ (FSIQ) was 78.8 with 30% meeting criteria for a diagnosis of intellectual disability. FSIQ measures were significantly lower than in relatives who did not have the 16p11.2 recurrent duplication [D'Angelo et al 2016]. Individuals with the 16p11.2 recurrent duplication with lower FSIQ often display other impairments in motor, language, and social skills [Green Snyder et al 2016].
• ASD has been found to be slightly more common in those with the 16p11.2 recurrent duplication (20%) than in those with the 16p11.2 recurrent deletion (16%), and individuals with the 16p11.2 recurrent duplication with ASD have lower cognition than those with the 16p11.2 recurrent deletion with ASD [D'Angelo et al 2016].
• Seizures are observed in approximately 20% of individuals with the 16p11.2 recurrent duplication [D'Angelo et al 2016, Green Snyder et al 2016].
• Head circumference tends to be smaller in individuals with the 16p11.2 recurrent duplication than in their relatives without the duplication [D'Angelo et al 2016].
• In addition, the 16p11.2 recurrent duplication is associated with underweight and a lower body mass index (BMI). The reciprocal impact of both the 16p11.2 recurrent deletion and duplication indicate that severe obesity (deletion) and being underweight (duplication) could have mirror etiologies, possibly through contrasting effects on energy balance [Jacquemont et al 2011, D'Angelo et al 2016].

Whereas 16p11.2 recurrent deletions are often de novo, a larger proportion of recurrent duplications are inherited. Parents with a 16p11.2 recurrent duplication may not have a history of developmental delay, ID, or ASD but may have more subtle neurobehavioral manifestations.

16p11.2-p12.2 Deletion

At least two individuals with much larger deletions that include the 16p11.2 recurrent deletion region have been described [Ballif et al 2007, Battaglia et al 2009]. In both individuals, the deletion was larger than 8 Mb, causing a more severe phenotype.

Evaluations Following Initial Diagnosis

To establish the extent of disease and needs in an individual diagnosed with the 16p11.2 recurrent deletion, the evaluations summarized in Table 3 (if not performed as part of the evaluation that led to diagnosis) are recommended.

Treatment of Manifestations

Surveillance

Agents/Circumstances to Avoid

Some medications used to treat behavioral problems (e.g., clozapine, olanzapine) may lead to excessive weight gain. When possible, use medications that are not associated with weight gain.

Evaluation of Relatives at Risk

See Genetic Counseling for issues related to testing of at-risk relatives for genetic counseling purposes.

Therapies Under Investigation

Search ClinicalTrials.gov in the US and EU Clinical Trials Register in Europe for access to information on clinical studies for a wide range of diseases and conditions. Note: There may not be clinical trials for this disorder.

Mode of Inheritance

The 16p11.2 recurrent deletion is de novo in most probands. Less commonly, the deletion is transmitted from a parent to a child in an autosomal dominant manner.

Risk to Family Members

Parents of a proband

• The 16p11.2 recurrent deletion is de novo in approximately 93% of reported probands whose parents have undergone genomic testing.
• Approximately 7% of probands inherited the 16p11.2 recurrent deletion from a parent. Parents with a 16p11.2 recurrent deletion typically do not have a history of ID or ASD but may have more subtle neurodevelopmental and behavioral manifestations.
• Genomic testing that will detect the 16p11.2 recurrent deletion present in the proband is recommended for the parents of the proband to evaluate their genetic status and inform recurrence risk assessment. The 16p11.2 recurrent deletion has been detected in mildly affected and unaffected parents.
• If the 16p11.2 recurrent deletion identified in the proband is not identified in either confirmed biological parent, the following possibilities should be considered:
  • The proband has a de novo deletion.
  • The proband inherited a deletion from a parent with germline (or somatic and germline) mosaicism [Kumar et al 2008, Weiss et al 2008, Steinman et al 2016].
    Note: Testing of parental leukocyte DNA may not detect all instances of somatic mosaicism and will not detect a genetic alteration that is present in the germ cells only.
• The 16p11.2 recurrent deletion has not been reported to have a parent-of-origin bias.

Sibs of a proband. The risk to the sibs of a proband depends on the genetic status of the parents:

• If one of the parents has the 16p11.2 recurrent deletion identified in the proband, the risk to each sib of inheriting the deletion is 50%. It is not possible to predict the phenotype in sibs who inherit a 16p11.2 recurrent deletion; family members with the deletion may be mildly affected or have features similar to those of the proband.
• If the 16p11.2 recurrent deletion identified in the proband cannot be detected in parental leukocyte, the recurrence risk to sibs is approximately 1% because of the possibility of parental germline mosaicism for the deletion [Kumar et al 2008, Weiss et al 2008].

Offspring of a proband. Each child of an individual with the 16p11.2 recurrent deletion has a 50% chance of inheriting the deletion; it is not possible to predict the phenotype in offspring who inherit the deletion.

Other family members. The risk to other family members depends on the genetic status of the proband's parents: if a parent has the 16p11.2 recurrent deletion, the parent's family members may also have the deletion.

Related Genetic Counseling Issues

Family planning

• The optimal time for determination of genetic risk and discussion of the availability of prenatal/preimplantation genetic testing is before pregnancy.
• It is appropriate to offer genetic counseling (including discussion of potential risks to offspring and reproductive options) to young adults who are at risk of having a child with the 16p11.2 recurrent deletion.

Prenatal Testing and Preimplantation Genetic Testing

Once a 16p11.2 recurrent deletion has been identified in a family member, prenatal and preimplantation genetic testing are possible.

Although the prenatal finding of a 16p11.2 recurrent deletion cannot be used to reliably predict the phenotype, the majority of individuals with the 16p11.2 recurrent deletion have language delay and cognitive disability.

Differences in perspective may exist among medical professionals and within families regarding the use of prenatal testing. While most centers would consider use of prenatal testing to be a personal decision, discussion of these issues may be helpful.

Molecular Pathogenesis

The 16p11.2 recurrent deletion is mediated by nonallelic homologous recombination (NAHR) between flanking 147-kb low-copy repeat sequences with 99.5% sequence identity [Ghebranious et al 2007, Sebat et al 2007, Kumar et al 2008, Marshall et al 2008, Weiss et al 2008]. The reciprocal duplication is also mediated by NAHR at the same site.

Mechanism of disease causation. Loss of function of some or all of the genes within the deleted region (See Notable genes typically included in this region.)

Laboratory technical considerations. The 16p11.2 recurrent deletion cannot be identified by routine analysis of G-banded chromosomes or other conventional cytogenetic banding techniques.

Notable genes typically included in this region. The 16p11.2 recurrent deletion involves the loss of one chromosome segment containing 25 annotated genes or transcripts [Kumar et al 2008, Marshall et al 2008, Weiss et al 2008]. The recurrent deletion is flanked by segmental duplications that contain four additional genes.

How deletion of these genes results in the clinical manifestations associated with the 16p11.2 recurrent deletion is largely unknown, but ongoing investigations have identified the roles of some key genes and their associated functional pathways as responsible for the phenotypic features.

While most of the genes at 16p11.2 exhibited dosage-dependent expression pattern [Migliavacca et al 2015], the pathogenic functions of each gene or their combinations require further examination.

• PRRT2. Heterozygous loss-of-function PRRT2 pathogenic variants are associated with autosomal dominant PRRT2-related disorder, which encompasses three allelic paroxysmal disorders: paroxysmal kinesigenic dyskinesia (38.7%); benign familial infantile epilepsy (41.7%); and infantile convulsions with choreoathetosis syndrome (14.3%) [Heron et al 2012, Schubert et al 2012, van Vliet et al 2012, Ebrahimi-Fakhari et al 2015]. These phenotypes have been reported in a small number of individuals with the 16p11.2 recurrent deletion.
• KCTD13. A smaller (~118-kb) deletion within 16p11.2 that segregated with ASD and other neurodevelopmental abnormalities has been identified [Crepel et al 2011]. One of the five genes at this interval, KCTD13, was identified as a major driver for the neuroanatomic phenotypes of the 16p11.2 recurrent deletion [Golzio et al 2012]. This gene is associated with ciliary function, which is thought to be significantly disrupted in individuals with the 16p11.2 recurrent deletion or duplication [Migliavacca et al 2015].
• TBX6. It has been determined that vertebral abnormalities and scoliosis observed in some individuals with the 16p11.2 recurrent deletion result from a combination of a TBX6 null allele (i.e., the recurrent deletion) and hypomorphic allele [Wu et al 2015].

Author History

Wendy Chung, MD, PhD, FACMG (2015-present)
Ellen Hanson, PhD; Boston Children's Hospital (2009-2021)
Rachel Hundley, PhD; Boston Children's Hospital (2009-2011)
Christopher Lehman, MS (2021-present)
David T Miller, MD, PhD, FACMG; Boston Children's Hospital (2009-2021)
Marissa Mitchel, MS, CCC-SLP (2021-present)
Ramzi Nasir, MD, MPH; Boston Children's Hospital (2009-2021)
Yiping Shen, PhD, FACMG; Boston Children's Hospital (2009-2021)
Kaitlyn Singer, MS (2021-present)
Magdi M Sobeih, MD, PhD; Boston Children's Hospital (2009-2015)
Kyle J Steinman, MD, MAS; Seattle Children's Hospital / University of Washington (2015-2021)
Rebecca Smith, MS, CGC (2021-present)
Cora M Taylor, PhD (2021-present)
W Curtis Weaver, BS (2021-present)
Bai-Lin Wu, MMed, PhD, FACMG; Boston Children's Hospital (2009-2021)

Revision History

• 28 October 2021 (ha) Comprehensive update posted live
• 10 December 2015 (me) Comprehensive update posted live
• 8 February 2011 (me) Comprehensive update posted live
• 22 September 2009 (et) Review posted live
• 6 March 2009 (dtm) Original submission

Literature Cited

• Ballif BC, Hornor SA, Jenkins E, Madan-Khetarpal S, Surti U, Jackson KE, Asamoah A, Brock PL, Gowans GC, Conway RL, Graham JM Jr, Medne L, Zackai EH, Shaikh TH, Geoghegan J, Selzer RR, Eis PS, Bejjani BA, Shaffer LG. Discovery of a previously unrecognized microdeletion syndrome of 16p11.2-p12.2. Nat Genet. 2007;39:1071–3. [PubMed: 17704777]
• Battaglia A, Novelli A, Bernardini L, Igliozzi R, Parrini B. Further characterization of the new microdeletion syndrome of 16p11.2-p12.2. Am J Med Genet A. 2009;149A:1200–4. [PubMed: 19449418]
• Chawner SJRA, Owen MJ, Holmans P, Raymond FL, Skuse D, Hall J, van den Bree MBM. Genotype-phenotype associations in children with copy number variants associated with high neuropsychiatric risk in the UK (IMAGINE-ID): a case-control cohort study. Lancet Psychiatry. 2019;6:493-505. [PubMed: 31056457]
• Chung WK, Roberts TPL, Sherr EH, Green Snyder LA, Spiro JE. 16p11.2 deletion syndrome. Curr Opin Genet Dev. 2021;68:49-56. [PMC free article: PMC10256135] [PubMed: 33667823]
• Crepel A, Steyaert J, De la Marche W, De Wolf V, Fryns JP, Noens I, Devriendt K, Peeters H. Narrowing the critical deletion region for autism spectrum disorders on 16p11.2. Am J Med Genet B Neuropsychiatr Genet. 2011;156:243-5. [PubMed: 21302354]
• D'Angelo D, Lebon S, Chen Q, Martin-Brevet S, Snyder LG, Hippolyte L, Hanson E, Maillard AM, Faucett WA, Macé A, Pain A, Bernier R, Chawner SJ, David A, Andrieux J, Aylward E, Baujat G, Caldeira I, Conus P, Ferrari C, Forzano F, Gérard M, Goin-Kochel RP, Grant E, Hunter JV, Isidor B, Jacquette A, Jønch AE, Keren B, Lacombe D, Le Caignec C, Martin CL, Männik K, Metspalu A, Mignot C, Mukherjee P, Owen MJ, Passeggeri M, Rooryck-Thambo C, Rosenfeld JA, Spence SJ, Steinman KJ, Tjernagel J, Van Haelst M, Shen Y, Draganski B, Sherr EH, Ledbetter DH, van den Bree MB, Beckmann JS, Spiro JE, Reymond A, Jacquemont S, Chung WK, et al. Defining the effect of the 16p11.2 duplication on cognition, behavior, and medical comorbidities. JAMA Psychiatry. 2016;73:20-30. [PMC free article: PMC5894477] [PubMed: 26629640]
• Demopoulos C, Kothare H, Mizuiri D, Henderson-Sabes J, Fregeau B, Tjernagel J, Houde JF, Sherr EH, Nagarajan SS. Abnormal speech motor control in individuals with 16p11.2 deletions. Sci Rep. 2018;8:1274. [PMC free article: PMC5775320] [PubMed: 29352208]
• Ebrahimi-Fakhari D, Saffari A, Westenberger A, Klein C. The evolving spectrum of PRRT2-associated paroxysmal diseases. Brain. 2015;138:3476-95. [PubMed: 26598493]
• Egolf LE, Vaksman Z, Lopez G, Germline 16p11.2 microdeletion predisposes to neuroblastoma. Germline 16p11.2 microdeletion predisposes to neuroblastoma. Am J Hum Genet. 2019;105:658-68. [PMC free article: PMC6731370] [PubMed: 31474320]
• Fedorenko E, Morgan A, Murray E, Cardinaux A, Mei C, Tager-Flusberg H, Fisher SE, Kanwisher. A highly penetrant form of childhood apraxia of speech due to deletion of 16p11.2. Eur J Hum Genet. 2016;24:302-6. [PMC free article: PMC4717199] [PubMed: 26173965]
• Fetit R, Price DJ, Lawrie SM, Johnstone M. Understanding the clinical manifestations of 16p11.2 deletion syndrome: a series of developmental case reports in children. Psychiatr Genet. 2020;30:136-40. [PMC free article: PMC7497286] [PubMed: 32732550]
• Garone G, Capuano A, Travaglini L, Graziola F, Stregapede F, Zanni G, Vigevano F, Bertini E, Nicita F. Clinical and genetic overview of paroxysmal movement disorders and episodic ataxias. Int J Mol Sci. 2020;21:3603. [PMC free article: PMC7279391] [PubMed: 32443735]
• Ghebranious N, Giampietro PF, Wesbrook FP, Rezkalla SH. A novel microdeletion at 16p11.2 harbors candidate genes for aortic valve development, seizure disorder, and mild mental retardation. Am J Med Genet A. 2007;143A:1462-71 [PubMed: 17568417]
• Gill R, Chen Q, D'Angelo D, Chung WK. Eating in the absence of hunger but not loss of control behaviors are associated with 16p11.2 deletions. Obesity (Silver Spring). 2014;22:2625-31. [PubMed: 25234362]
• Goldman S, McCullough AK, Young SD, Mueller C, Stahl A, Zoeller A, Abbruzzese LD, Rao AK, Montes J. Quantitative gait assessment in children with 16p11.2 syndrome. J Neurodev Disord. 2019;11:26. [PMC free article: PMC6816222] [PubMed: 31656164]
• Golzio C, Willer J, Talkowski ME, Oh EC, Taniguchi Y, Jacquemont S, Reymond A, Sun M, Sawa A, Gusella JF, Kamiya A, Beckmann JS, Katsanis N. KCTD13 is a major driver of mirrored neuroanatomical phenotypes of the 16p11.2 copy number variant. Nature. 2012;485:363-7. [PMC free article: PMC3366115] [PubMed: 22596160]
• Green Snyder L, D'Angelo D, Chen Q, Bernier R, Goin-Kochel RP, Wallace AS, Gerdts J, Kanne S, Berry L, Blaskey L, Kuschner E, Roberts T, Sherr E, Martin CL, Ledbetter DH, Spiro JE, Chung WK, Hanson E, et al. Autism spectrum disorder, developmental and psychiatric features in 16p11.2 duplication. J Autism Dev Disord. 2016;46:2734-48. [PubMed: 27207092]
• Hanson E, Bernier R, Porche K, Jackson FI, Goin-Kochel RP, Snyder LG, Snow AV, Wallace AS, Campe KL, Zhang Y, Chen Q, D'Angelo D, Moreno-De-Luca A, Orr PT, Boomer KB, Evans DW, Kanne S, Berry L, Miller FK, Olson J, Sherr E, Martin CL, Ledbetter DH, Spiro JE, Chung WK, et al. The cognitive and behavioral phenotype of the 16p11.2 deletion in a clinically ascertained population. Biol Psychiatry. 2015;77:785-93. [PMC free article: PMC5410712] [PubMed: 25064419]
• Heron SE, Grinton BE, Kivity S, Afawi Z, Zuberi SM, Hughes JN, Pridmore C, Hodgson BL, Iona X, Sadleir LG, Pelekanos J, Herlenius E, Goldberg-Stern H, Bassan H, Haan E, Korczyn AD, Gardner AE, Corbett MA, Gécz J, Thomas PQ, Mulley JC, Berkovic SF, Scheffer IE, Dibbens LM. PRRT2 mutations cause benign familial infantile epilepsy and infantile convulsions with choreoathetosis syndrome. Am J Hum Genet. 2012;90:152-60. [PMC free article: PMC3257886] [PubMed: 22243967]
• Hippolyte L, Maillard AM, Rodriguez-Herreros B, Pain A, Martin-Brevet S, Ferrari C, Conus P, Macé A, Hadjikhani N, Metspalu A, Reigo A, Kolk A, Männik K, Barker M, Isidor B, Le Caignec C, Mignot C, Schneider L, Mottron L, Keren B, David A, Doco-Fenzy M, Gérard M, Bernier R, Goin-Kochel RP, Hanson E, Green Snyder L; 16p11.2 European Consortium, Simons Variation in Individuals Project Consortium, Ramus F, Beckmann JS, Draganski B, Reymond A, Jacquemont S. The number of genomic copies at the 16p11.2 locus modulates language, verbal memory, and inhibition. Biol Psychiatry. 2016;80:129-39. [PubMed: 26742926]
• Jacquemont S, Reymond A, Zufferey F, Harewood L, Walters RG, Kutalik Z, Martinet D, Shen Y, Valsesia A, Beckmann ND, Thorleifsson G, Belfiore M, Bouquillon S, Campion D, de Leeuw N, de Vries BB, Esko T, Fernandez BA, Fernández-Aranda F, Fernández-Real JM, Gratacòs M, Guilmatre A, Hoyer J, Jarvelin MR, Kooy RF, Kurg A, Le Caignec C, Männik K, Platt OS, Sanlaville D, Van Haelst MM, Villatoro Gomez S, Walha F, Wu BL, Yu Y, Aboura A, Addor MC, Alembik Y, Antonarakis SE, Arveiler B, Barth M, Bednarek N, Béna F, Bergmann S, Beri M, Bernardini L, Blaumeiser B, Bonneau D, Bottani A, Boute O, Brunner HG, Cailley D, Callier P, Chiesa J, Chrast J, Coin L, Coutton C, Cuisset JM, Cuvellier JC, David A, de Freminville B, Delobel B, Delrue MA, Demeer B, Descamps D, Didelot G, Dieterich K, Disciglio V, Doco-Fenzy M, Drunat S, Duban-Bedu B, Dubourg C, El-Sayed Moustafa JS, Elliott P, Faas BH, Faivre L, Faudet A, Fellmann F, Ferrarini A, Fisher R, Flori E, Forer L, Gaillard D, Gerard M, Gieger C, Gimelli S, Gimelli G, Grabe HJ, Guichet A, Guillin O, Hartikainen AL, Heron D, Hippolyte L, Holder M, Homuth G, Isidor B, Jaillard S, Jaros Z, Jiménez-Murcia S, Helas GJ, Jonveaux P, Kaksonen S, Keren B, Kloss-Brandstätter A, Knoers NV, Koolen DA, Kroisel PM, Kronenberg F, Labalme A, Landais E, Lapi E, Layet V, Legallic S, Leheup B, Leube B, Lewis S, Lucas J, MacDermot KD, Magnusson P, Marshall C, Mathieu-Dramard M, McCarthy MI, Meitinger T, Mencarelli MA, Merla G, Moerman A, Mooser V, Morice-Picard F, Mucciolo M, Nauck M, Ndiaye NC, Nordgren A, Pasquier L, Petit F, Pfundt R, Plessis G, Rajcan-Separovic E, Ramelli GP, Rauch A, Ravazzolo R, Reis A, Renieri A, Richart C, Ried JS, Rieubland C, Roberts W, Roetzer KM, Rooryck C, Rossi M, Saemundsen E, Satre V, Schurmann C, Sigurdsson E, Stavropoulos DJ, Stefansson H, Tengström C, Thorsteinsdóttir U, Tinahones FJ, Touraine R, Vallée L, van Binsbergen E, Van der Aa N, Vincent-Delorme C, Visvikis-Siest S, Vollenweider P, Völzke H, Vulto-van Silfhout AT, Waeber G, Wallgren-Pettersson C, Witwicki RM, Zwolinksi S, Andrieux J, Estivill X, Gusella JF, Gustafsson O, Metspalu A, Scherer SW, Stefansson K, Blakemore AI, Beckmann JS, Froguel P. Mirror extreme BMI phenotypes associated with gene dosage at the chromosome 16p11.2 locus. Nature. 2011;478:97-102. [PMC free article: PMC3637175] [PubMed: 21881559]
• Kim SH, Green-Snyder L, Lord C, Bishop S, Steinman KJ, Bernier R, Hanson E, Goin-Kochel RP, Chung WK. Language characterization in 16p11.2 deletion and duplication syndromes. Am J Med Genet B Neuropsychiatr Genet. 2020;183:380-91. [PMC free article: PMC8939307] [PubMed: 32652891]
• Kostopoulou E, Dastamani A, Caiulo S, Antell H, Flanagan SE, Shah P. Hyperinsulinaemic hypoglycaemia: a new presentation of 16p11.2 deletion syndrome. Clin Endocrinol (Oxf). 2019;90:766-9. [PubMed: 30776145]
• Kumar RA, Karamohamed S, Sudi J, Conrad DF, Brune C, Badner JA, Gilliam TC, Nowak NJ, Cook EH Jr, Dobyns WB, Christian SL. Recurrent 16p11.2 microdeletions in autism. Hum Mol Genet. 2008;17:628-38 [PubMed: 18156158]
• Lee HY, Huang Y, Bruneau N, Roll P, Roberson ED, Hermann M, Quinn E, Maas J, Edwards R, Ashizawa T, Baykan B, Bhatia K, Bressman S, Bruno MK, Brunt ER, Caraballo R, Echenne B, Fejerman N, Frucht S, Gurnett CA, Hirsch E, Houlden H, Jankovic J, Lee WL, Lynch DR, Mohammed S, Müller U, Nespeca MP, Renner D, Rochette J, Rudolf G, Saiki S, Soong BW, Swoboda KJ, Tucker S, Wood N, Hanna M, Bowcock AM, Szepetowski P, Fu YH, and Ptáček LJ. Mutations in the gene PRRT2 cause paroxysmal kinesigenic dyskinesia with infantile convulsions. Cell Rep. 2012;1:2-12. [PMC free article: PMC3334308] [PubMed: 22832103]
• Li J, Zhu X, Wang X, Sun W, Feng B, Du T, Sun B, Niu F, Wei H, Wu X, Dong L, Li L, Cai X, Wang Y, and Liu Y. Targeted genomic sequencing identifies PRRT2 mutations as a cause of paroxysmal kinesigenic choreoathetosis. J Med Genet. 2012;49:76-8. [PMC free article: PMC3261727] [PubMed: 22131361]
• Männik K, Mägi R, Macé A, Cole B, Guyatt AL, Shihab HA, Maillard AM, Alavere H, Kolk A, Reigo A, Mihailov E, Leitsalu L, Ferreira AM, Nõukas M, Teumer A, Salvi E, Cusi D, McGue M, Iacono WG, Gaunt TR, Beckmann JS, Jacquemont S, Kutalik Z, Pankratz N, Timpson N, Metspalu A, Reymond A. Copy number variations and cognitive phenotypes in unselected populations. JAMA. 2015;313:2044-54. [PMC free article: PMC4684269] [PubMed: 26010633]
• Marshall CR, Noor A, Vincent JB, Lionel AC, Feuk L, Skaug J, Shago M, Moessner R, Pinto D, Ren Y, Thiruvahindrapduram B, Fiebig A, Schreiber S, Friedman J, Ketelaars CE, Vos YJ, Ficicioglu C, Kirkpatrick S, Nicolson R, Sloman L, Summers A, Gibbons CA, Teebi A, Chitayat D, Weksberg R, Thompson A, Vardy C, Crosbie V, Luscombe S, Baatjes R, Zwaigenbaum L, Roberts W, Fernandez B, Szatmari P, Scherer SW. Structural variation of chromosomes in autism spectrum disorder. Am J Hum Genet. 2008;82:477-88. [PMC free article: PMC2426913] [PubMed: 18252227]
• Mei C, Fedorenko E, Amor DJ, Boys A, Hoeflin C, Carew P, Burgess T, Fisher SE, Morgan AT. Deep phenotyping of speech and language skills in individuals with 16p11.2 deletion. Eur J Hum Genet. 2018;26:676-86. [PMC free article: PMC5945616] [PubMed: 29445122]
• Migliavacca E, Golzio C, Männik K, Blumenthal I, Oh EC, Harewood L, Kosmicki JA, Loviglio MN, Giannuzzi G, Hippolyte L, Maillard AM, Alfaiz AA, van Haelst MM, Andrieux J, Gusella JF, Daly MJ, Beckmann JS, Jacquemont S, Talkowski ME, Katsanis N, Reymond A, et al. A potential contributory role for ciliary dysfunction in the 16p11.2 600 kb BP4-BP5 pathology. Am J Hum Genet. 2015;96:784-96. [PMC free article: PMC4570289] [PubMed: 25937446]
• Moreno-De-Luca A, Evans DW, Boomer KB, Hanson E, Bernier R, Goin-Kochel RP, Myers SM, Challman TD, Moreno-De-Luca D, Slane MM, Hare AE, Chung WK, Spiro JE, Faucett WA, Martin CL, Ledbetter DH. The role of parental cognitive, behavioral, and motor profiles in clinical variability in individuals with chromosome 16p11.2 deletions. JAMA Psychiatry. 2015;72:119-26. [PubMed: 25493922]
• Niarchou M, Chawner SJRA, Doherty JL, Maillard AM, Jacquemont S, Chung WK, Green-Snyder L, Bernier RA, Goin-Kochel RP, Hanson E, Linden DEJ, Linden SC, Raymond FL, Skuse D, Hall J, Owen MJ, Bree MBMVD. Psychiatric disorders in children with 16p11.2 deletion and duplication. Transl Psychiatry. 2019;9:8. [PMC free article: PMC6341088] [PubMed: 30664628]
• Owen JP, Bukshpun P, Pojman N, Thieu T, Chen Q, Lee J, D'Angelo D, Glenn OA, Hunter JV, Berman JI, Roberts TP, Buckner R, Nagarajan SS, Mukherjee P, Sherr EH. Brain MR imaging findings and associated outcomes in carriers of the reciprocal copy number variation at 16p11.2. Radiology. 2018;286:217-26. [PubMed: 28786752]
• Qureshi AY, Mueller S, Snyder AZ, Mukherjee P, Berman JI, Roberts TP, Nagarajan SS, Spiro JE, Chung WK, Sherr EH, Buckner RL. Opposing brain differences in 16p11.2 deletion and duplication carriers. J Neurosci. 2014;34:11199-211. [PMC free article: PMC4138332] [PubMed: 25143601]
• Schaaf CP, Goin-Kochel RP, Nowell KP, Hunter JV, Aleck KA, Cox S, Patel A, Bacino CA, Shinawi M. Expanding the clinical spectrum of the 16p11.2 chromosomal rearrangements: three patients with syringomyelia. Eur J Hum Genet. 2011;19:152-6. [PMC free article: PMC3025795] [PubMed: 20959866]
• Schubert J, Paravidino R, Becker F, Berger A, Bebek N, Bianchi A, Brockmann K, Capovilla G, Dalla Bernardina B, Fukuyama Y, Hoffmann GF, Jurkat-Rott K, Anttonen AK, Kurlemann G, Lehesjoki AE, Lehmann-Horn F, Mastrangelo M, Mause U, Müller S, Neubauer B, Püst B, Rating D, Robbiano A, Ruf S, Schroeder C, Seidel A, Specchio N, Stephani U, Striano P, Teichler J, Turkdogan D, Vigevano F, Viri M, Bauer P, Zara F, Lerche H, Weber YG. PRRT2 mutations are the major cause of benign familial infantile seizures. Hum Mutat. 2012;33:1439-43. [PubMed: 22623405]
• Sebat J, Lakshmi B, Malhotra D, Troge J, Lese-Martin C, Walsh T, Yamrom B, Yoon S, Krasnitz A, Kendall J, Leotta A, Pai D, Zhang R, Lee YH, Hicks J, Spence SJ, Lee AT, Puura K, Lehtimäki T, Ledbetter D, Gregersen PK, Bregman J, Sutcliffe JS, Jobanputra V, Chung W, Warburton D, King MC, Skuse D, Geschwind DH, Gilliam TC, Ye K, Wigler M. Strong association of de novo copy number mutations with autism. Science. 2007;316:445-9 [PMC free article: PMC2993504] [PubMed: 17363630]
• Steinman KJ, Spence SJ, Ramocki MB, Proud MB, Kessler SK, Marco EJ, Green Snyder L, D'Angelo D, Chen Q, Chung WK, Sherr EH, et al. 16p11.2 deletion and duplication: characterizing neurologic phenotypes in a large clinically ascertained cohort. Am J Med Genet A. 2016;170:2943-55. [PubMed: 27410714]
• Stingl CS, Jackson-Cook C, Couser NL. Ocular findings in the 16p11.2 microdeletion syndrome: a case report and literature review. Case Rep Pediatr. 2020;2020:2031701. [PMC free article: PMC7189309] [PubMed: 32373379]
• Termsarasab P, Yang AC, Reiner J, Mei H, Scott SA, Frucht SJ. Paroxysmal kinesigenic dyskinesia caused by 16p11.2 microdeletion. Tremor Other Hyperkinet Mov (N Y). 2014;4:274. [PMC free article: PMC4303604] [PubMed: 25667815]
• van Vliet R, Breedveld G, de Rijk-van Andel J, Brilstra E, Verbeek N, Verschuuren-Bemelmans C, Boon M, Samijn J, Diderich K, van de Laar I, Oostra B, Bonifati V, Maat-Kievit A. PRRT2 phenotypes and penetrance of paroxysmal kinesigenic dyskinesia and infantile convulsions. Neurology. 2012;79:777-84. [PubMed: 22875091]
• Vlaskamp DRM, Callenbach PMC, Rump P, Giannini LAA, Brilstra EH, Dijkhuizen T, Vos YJ, van der Kevie-Kersemaekers AF, Knijnenburg J, de Leeuw N, van Minkelen R, Ruivenkamp CAL, Stegmann APA, Brouwer OF, van Ravenswaaij-Arts CMA. PRRT2-related phenotypes in patients with a 16p11.2 deletion. Eur J Med Genet. 2019;62:265-9. [PubMed: 30125676]
• Walsh T, McClellan JM, McCarthy SE, Addington AM, Pierce SB, Cooper GM, Nord AS, Kusenda M, Malhotra D, Bhandari A, Stray SM, Rippey CF, Roccanova P, Makarov V, Lakshmi B, Findling RL, Sikich L, Stromberg T, Merriman B, Gogtay N, Butler P, Eckstrand K, Noory L, Gochman P, Long R, Chen Z, Davis S, Baker C, Eichler EE, Meltzer PS, Nelson SF, Singleton AB, Lee MK, Rapoport JL, King MC, Sebat J. Rare structural variants disrupt multiple genes in neurodevelopmental pathways in schizophrenia. Science. 2008;320:539-43. [PubMed: 18369103]
• Wang JL, Cao L, Li XH, Hu ZM, Li JD, Zhang JG, Liang Y, San-A, Li N, Chen SQ, Guo JF, Jiang H, Shen L, Zheng L, Mao X, Yan WQ, Zhou Y, Shi YT, Ai SX, Dai MZ, Zhang P, Xia K, Chen SD, Tang BS. Identification of PRRT2 as the causative gene of paroxysmal kinesigenic dyskinesias. Brain. 2011;134:3493-501. [PMC free article: PMC3235563] [PubMed: 22120146]
• Weiss LA, Shen Y, Korn JM, Arking DE, Miller DT, Fossdal R, Saemundsen E, Stefansson H, Ferreira MA, Green T, Platt OS, Ruderfer DM, Walsh CA, Altshuler D, Chakravarti A, Tanzi RE, Stefansson K, Santangelo SL, Gusella JF, Sklar P, Wu BL, Daly MJ, et al. Association between microdeletion and microduplication at 16p11.2 and autism. N Engl J Med. 2008;358:667-75. [PubMed: 18184952]
• Wu N, Ming X, Xiao J, Wu Z, Chen X, Shinawi M, Shen Y, Yu G, Liu J, Xie H, Gucev ZS, Liu S, Yang N, Al-Kateb H, Chen J, Zhang J, Hauser N, Zhang T, Tasic V, Liu P, Su X, Pan X, Liu C, Wang L, Shen J, Shen J, Chen Y, Zhang T, Zhang J, Choy KW, Wang J, Wang Q, Li S, Zhou W, Guo J, Wang Y, Zhang C, Zhao H, An Y, Zhao Y, Wang J, Liu Z, Zuo Y, Tian Y, Weng X, Sutton VR, Wang H, Ming Y, Kulkarni S, Zhong TP, Giampietro PF, Dunwoodie SL, Cheung SW, Zhang X, Jin L, Lupski JR, Qiu G, Zhang F. TBX6 null variants and a common hypomorphic allele in congenital scoliosis. N Engl J Med. 2015;372:341-50. [PMC free article: PMC4326244] [PubMed: 25564734]
• Zufferey F, Sherr EH, Beckmann ND, Hanson E, Maillard AM, Hippolyte L, Macé A, Ferrari C, Kutalik Z, Andrieux J, Aylward E, Barker M, Bernier R, Bouquillon S, Conus P, Delobel B, Faucett WA, Goin-Kochel RP, Grant E, Harewood L, Hunter JV, Lebon S, Ledbetter DH, Martin CL, Mannik K, Martinet D, Mukherjee P, Ramocki MB, Spence SJ, Steinman K, Tjernagel J, Spiro JE, Reymond A, Beckmann JS, Chung WK, Jacquemont S, et al. A 600 kb deletion syndrome at 16p11.2 leads to energy imbalance and neuropsychiatric disorders. J Med Genet. 2012; 49:660-8 [PMC free article: PMC3494011] [PubMed: 23054248]