De novo and inherited TCF20 pathogenic variants are associated with intellectual disability, dysmorphic features, hypotonia, and neurological impairments with similarities to Smith-Magenis syndrome

Francesco Vetrini; Shane McKee; Jill A Rosenfeld; Mohnish Suri; Andrea M Lewis; Kimberly Margaret Nugent; Elizabeth Roeder; Rebecca O Littlejohn; Sue Holder; Wenmiao Zhu; Joseph T Alaimo; Brett Graham; Jill M Harris; James B Gibson; Matthew Pastore; Kim L McBride; Makanko Komara; Lihadh Al-Gazali; Aisha Al Shamsi; Elizabeth A Fanning; Klaas J Wierenga; Daryl A Scott; Ziva Ben-Neriah; Vardiella Meiner; Hanoch Cassuto; Orly Elpeleg; J Lloyd Holder Jr; Lindsay C Burrage; Laurie H Seaver; Lionel Van Maldergem; Sonal Mahida; Janet S Soul; Margaret Marlatt; Ludmila Matyakhina; Julie Vogt; June-Anne Gold; Soo-Mi Park; Vinod Varghese; Anne K Lampe; Ajith Kumar; Melissa Lees; Muriel Holder-Espinasse; Vivienne McConnell; Birgitta Bernhard; Ed Blair; Victoria Harrison; DDD study; Donna M Muzny; Richard A Gibbs; Sarah H Elsea; Jennifer E Posey; Weimin Bi; Seema Lalani; Fan Xia; Yaping Yang; Christine M Eng; James R Lupski; Pengfei Liu

doi:10.1186/s13073-019-0623-0

De novo and inherited TCF20 pathogenic variants are associated with intellectual disability, dysmorphic features, hypotonia, and neurological impairments with similarities to Smith-Magenis syndrome

Genome Med. 2019 Feb 28;11(1):12. doi: 10.1186/s13073-019-0623-0.

Authors

Francesco Vetrini^{1

2}, Shane McKee³, Jill A Rosenfeld⁴, Mohnish Suri⁵, Andrea M Lewis⁴, Kimberly Margaret Nugent^{4

6}, Elizabeth Roeder^{4

6}, Rebecca O Littlejohn^{4

6}, Sue Holder⁷, Wenmiao Zhu¹, Joseph T Alaimo⁴, Brett Graham^{4

2}, Jill M Harris⁸, James B Gibson⁸, Matthew Pastore⁹, Kim L McBride⁹, Makanko Komara¹⁰, Lihadh Al-Gazali¹⁰, Aisha Al Shamsi¹¹, Elizabeth A Fanning¹², Klaas J Wierenga^{12

13}, Daryl A Scott^{4

14}, Ziva Ben-Neriah¹⁵, Vardiella Meiner¹⁵, Hanoch Cassuto¹⁶, Orly Elpeleg¹⁷, J Lloyd Holder Jr¹⁸, Lindsay C Burrage⁴, Laurie H Seaver¹⁹, Lionel Van Maldergem²⁰, Sonal Mahida²¹, Janet S Soul²¹, Margaret Marlatt²¹, Ludmila Matyakhina²², Julie Vogt²³, June-Anne Gold²⁴, Soo-Mi Park²⁴, Vinod Varghese²⁵, Anne K Lampe²⁶, Ajith Kumar²⁷, Melissa Lees²⁷, Muriel Holder-Espinasse²⁸, Vivienne McConnell³, Birgitta Bernhard⁷, Ed Blair²⁹, Victoria Harrison³⁰; DDD study; Donna M Muzny^{4

31}, Richard A Gibbs^{4

31}, Sarah H Elsea^{1

4}, Jennifer E Posey⁴, Weimin Bi^{1

4}, Seema Lalani^{1

4

18}, Fan Xia^{1

4}, Yaping Yang^{1

4}, Christine M Eng^{1

4}, James R Lupski^{1

4

31

18}, Pengfei Liu^{32

33}

Affiliations

¹ Baylor Genetics, Houston, TX, 77021, USA.
² Present address: Department of Medical and Molecular Genetics, Indiana University School of Medicine, Indianapolis, IN, 46202, USA.
³ Northern Ireland Regional Genetics Service, Belfast City Hospital, Belfast, UK.
⁴ Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, TX, 77030, USA.
⁵ Nottingham Genetics Service, Nottingham City Hospital, Nottingham, UK.
⁶ Department of Pediatrics, Baylor College of Medicine, San Antonio, TX, 78207, USA.
⁷ North West Thames Regional Genetics Service, 759 Northwick Park Hospital, London, UK.
⁸ Dell Children's Medical Group, Austin, TX, 78723, USA.
⁹ Division of Genetic and Genomic Medicine, Nationwide Children's Hospital; and Department of Pediatrics, College of Medicine, Ohio State University, Columbus, OH, 43205, USA.
¹⁰ Department of Pediatrics, College of Medicine & Health Sciences, United Arab University, Al Ain, UAE.
¹¹ Department of Pediatrics, Tawam Hospital, Al-Ain, UAE.
¹² Department of Pediatrics, Section of Genetics, University of Oklahoma Health Sciences Center, Oklahoma City, OK, 73104, USA.
¹³ Present address: Mayo Clinic Florida, Department of Clinical Genomics, Jacksonville, FL, 32224, USA.
¹⁴ Department of Molecular Physiology and Biophysics, Baylor College of Medicine, Houston, TX, 77030, USA.
¹⁵ Department of Human Genetics and Metabolic Diseases, Hadassah-Hebrew University Medical Center, Jerusalem, Israel.
¹⁶ The Hebrew University of Jerusalem, Jerusalem, Israel.
¹⁷ Monique and Jacques Roboh Department of Genetic Research, Hadassah-Hebrew University Medical Center, 91120, Jerusalem, Israel.
¹⁸ Department of Pediatrics, Texas Children's Hospital, Houston, TX, 77030, USA.
¹⁹ Department of Pediatrics, University of Hawaii, Honolulu, HI, 96826, USA.
²⁰ Centre de Génétique Humaine, Université de Franche-Comté, Besançon, France.
²¹ Department of Neurology, Boston Children's Hospital, Boston, MA, 0211, USA.
²² Gene DX, Gaithersburg, MD, 20877, USA.
²³ West Midlands Regional Clinical Genetics Service and Birmingham Health Partners; and Women's and Children's Hospitals NHS Foundation Trust, Birmingham, UK.
²⁴ East Anglia Regional Genetics Service, Addenbrooke's Hospital, Cambridge, UK.
²⁵ All-Wales Medical Genetics Service, University Hospital of Wales, Cardiff, UK.
²⁶ South East of Scotland Clinical Genetic Service, Western General Hospital, Edinburgh, UK.
²⁷ North East Thames Regional Genetics Service, Great Ormond Street Hospital, London, UK.
²⁸ South East Thames Regional Genetics Service, Guy's Hospital, London, UK.
²⁹ Oxford Regional Genetics Service, Oxford University Hospitals, Oxford, UK.
³⁰ Wessex Clinical Genetics Service, Princess Anne Hospital, Southampton, UK.
³¹ Human Genome Sequencing Center, Baylor College of Medicine, Houston, TX, 77030, USA.
³² Baylor Genetics, Houston, TX, 77021, USA. pengfeil@bcm.edu.
³³ Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, TX, 77030, USA. pengfeil@bcm.edu.

Abstract

Background: Neurodevelopmental disorders are genetically and phenotypically heterogeneous encompassing developmental delay (DD), intellectual disability (ID), autism spectrum disorders (ASDs), structural brain abnormalities, and neurological manifestations with variants in a large number of genes (hundreds) associated. To date, a few de novo mutations potentially disrupting TCF20 function in patients with ID, ASD, and hypotonia have been reported. TCF20 encodes a transcriptional co-regulator structurally related to RAI1, the dosage-sensitive gene responsible for Smith-Magenis syndrome (deletion/haploinsufficiency) and Potocki-Lupski syndrome (duplication/triplosensitivity).

Methods: Genome-wide analyses by exome sequencing (ES) and chromosomal microarray analysis (CMA) identified individuals with heterozygous, likely damaging, loss-of-function alleles in TCF20. We implemented further molecular and clinical analyses to determine the inheritance of the pathogenic variant alleles and studied the spectrum of phenotypes.

Results: We report 25 unique inactivating single nucleotide variants/indels (1 missense, 1 canonical splice-site variant, 18 frameshift, and 5 nonsense) and 4 deletions of TCF20. The pathogenic variants were detected in 32 patients and 4 affected parents from 31 unrelated families. Among cases with available parental samples, the variants were de novo in 20 instances and inherited from 4 symptomatic parents in 5, including in one set of monozygotic twins. Two pathogenic loss-of-function variants were recurrent in unrelated families. Patients presented with a phenotype characterized by developmental delay, intellectual disability, hypotonia, variable dysmorphic features, movement disorders, and sleep disturbances.

Conclusions: TCF20 pathogenic variants are associated with a novel syndrome manifesting clinical characteristics similar to those observed in Smith-Magenis syndrome. Together with previously described cases, the clinical entity of TCF20-associated neurodevelopmental disorders (TAND) emerges from a genotype-driven perspective.

Keywords: 22q13; Deletions; Haploinsufficiency; Loss-of-function variants; Neurodevelopmental disorders; Smith–Magenis syndrome; TCF20.

Publication types

Case Reports
Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Child
Child, Preschool
Craniofacial Abnormalities / genetics*
Craniofacial Abnormalities / pathology
Developmental Disabilities / genetics*
Developmental Disabilities / pathology
Female
Humans
INDEL Mutation*
Infant
Intellectual Disability / genetics*
Intellectual Disability / pathology
Male
Muscle Hypotonia / genetics*
Muscle Hypotonia / pathology
Smith-Magenis Syndrome / genetics*
Smith-Magenis Syndrome / pathology
Transcription Factors / genetics*
Transcription Factors / metabolism
Young Adult

Substances

TCF20 protein, human
Transcription Factors

Abstract

Publication types

MeSH terms

Substances

Grants and funding