ECRD 2026

Knowledge on rare diseases and orphan drugs

COVID-19 & Rare diseases logo Rare Diseases Resources for Refugees/Displaced Persons
Homepage > Rare diseases > Search

Search for a rare disease

*
(*) mandatory field

17q11 microdeletion syndrome

Suggest an update
Your message has been sent Your message has not been sent. Please contact an administrator.
Disease definition

17q11 microdeletion syndrome is a rare severe form of neurofibromatosis type 1 (NF1) characterized by mild facial dysmorphism, developmental delay, intellectual disability, increased risk of malignancies, and a large number of neurofibromas.

ORPHA:97685

Classification level: Subtype of disorder

Synonym(s):
  • Del(17)(q11)
  • Monosomy 17q11
  • NF1 microdeletion syndrome
  • Neurofibromatosis type 1 microdeletion syndrome

Prevalence: Unknown

Inheritance: Not applicable

Age of onset: Antenatal, Infancy, Neonatal

ICD-10: Q85.0

ICD-11: LD44.H0

OMIM: 613675

UMLS: C5401456

MeSH: C563524

GARD: 5408

Summary
Epidemiology

The prevalence of 17q11 microdeletion syndrome is not known. About 5% of NF1 cases are reported to have deletions of the entire NF1 gene. More than 170 affected patients have been reported to date.

Clinical description

Affected individuals often have unusual body habitus and facial dysmorphism including facial coarsening, prominent forehead, ptosis, down-slanting palpebral fissures, hypertelorism, broad nose and nasal bridge, low set ears, and micrognathia. Patients develop a large number of neurofibromas, often with early onset, including multiple cutaneous neurofibromas, and less commonly plexiform neurofibromas. Other characteristic features include attention deficit/hyperactivity disorder (AD/HD), delayed cognitive development and intellectual disability. Some patients are reported to have microcephaly or macrocephaly, optic pathway glioma, iris coloboma, heart defects (mitral valve prolapse, aortic dilatation), large hands and feet, connective tissue dysplasia (joint hyperflexibility, soft palm skin), muscular hypotonia, scoliosis, pectus excavatum, and bone cysts. A higher risk of malignancy for NF1 and non-NF1 tumors is reported: malignant peripheral nerve sheath tumors (lifetime risk of 16-26%), retroperitoneal fibrosarcoma, and medulloblastoma with extensive nodularity.

Etiology

Germline and mosaic microdeletions of the NF1 gene and its flanking regions caused by non-allelic homologous recombination are reported in patients with this disorder. Most occur de novo.

Genetic counseling

As most cases are de novo, recurrence risk for offspring of unaffected parents is very low. Affected individuals have a 50% risk of transmitting the microdeletion, and prenatal and preimplantation genetic diagnosis is possible.

Last update: July 2014 - Expert reviewer(s): Pr Eric LEGIUS
A summary on this disease is available in Français, Español, Italiano, Nederlands, Polski Ελληνικά
Detailed information

Logo ERN: produced/endorsed by ERN(s) Logo FSMR: produced/endorsed by FSMR(s)

Guidelines
Emergency guidelines
Français (2019.pdf) - Orphanet Urgences
Clinical practice guidelines
Français (2021) - PNDS Logo FSMR
English (2023) - EClinicalMedicine
English (2021) - Genet Med
Disease review articles
Clinical genetics review
English (2007.pdf) - Eur J Hum Genet
English (2022) - GeneReviews
Additional information

Further information on this disease

Patient-centred resources for this disease

Research activities on this disease

Newborn screening

The documents contained in this website are presented for information purposes only. The material is in no way intended to replace professional medical care by a qualified specialist and should not be used as a basis for diagnosis or treatment.