Trisomy 18

(Edwards Syndrome; Trisomy E)

ByNina N. Powell-Hamilton, MD, Sidney Kimmel Medical College at Thomas Jefferson University
Reviewed/Revised Oct 2023
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Trisomy 18 is caused by an extra chromosome 18 and is usually associated with intellectual disability, small birth size, and various congenital anomalies, including severe microcephaly, heart defects, prominent occiput, low-set malformed ears, and a characteristic pinched facial appearance. Prenatal diagnosis is with cytogenetic testing; postnatal diagnosis is with peripheral blood testing. Treatment is supportive.

(See also Overview of Chromosomal Abnormalities.)

Trisomy 18 occurs in approximately 4.1/10,000 pregnancies (based on data from induced abortion for fetal anomalies, stillbirths, and live births) (1). More than 95% of affected children have complete trisomy 18 (2). The extra chromosome is almost always maternally derived, and advanced maternal age increases risk. The female:male ratio is 3:1.

General references

  1. 1. Goel N, Morris JK, Tucker D, et al: Trisomy 13 and 18-Prevalence and mortality-A multi-registry population based analysis. Am J Med Genet A 179(12):2382-2392, 2019. doi: 10.1002/ajmg.a.61365

  2. 2. Bugge M, Collins A, Petersen MB, et al: Non-disjunction of chromosome 18. Hum Mol Genet 7(4):661-669, 1998. doi: 10.1093/hmg/7.4.661

Symptoms and Signs of Trisomy 18

Typical findings on prenatal ultrasonography and other fetal testing include polyhydramnios, small placenta, a single umbilical artery, and fetal growth restriction.

Birth weight is low, and there is hypotonia and marked hypoplasia of skeletal muscle and subcutaneous fat.

The cry is weak, and response to sound is decreased. The orbital ridges are hypoplastic, the palpebral fissures are short, and the mouth and jaw are small; all of these characteristics give the face a pinched appearance. Microcephaly, prominent occiput, low-set malformed ears, narrow pelvis, and a short sternum are common.

A clenched fist with the index finger overlapping the 3rd and 4th fingers often occurs. The distal crease on the 5th finger is often absent. Redundant skinfolds, especially over the back of the neck, are common. The fingernails are hypoplastic, and the big toe is shortened and frequently dorsiflexed. Clubfeet and rocker-bottom feet are common.

Severe congenital heart disease is common, especially patent ductus arteriosus and ventricular septal defects. Anomalies of lungs, diaphragm, gastrointestinal tract, abdominal wall, kidneys, and ureters are frequent. Boys may have undescended testes.

Common muscular manifestations include hernias, separation of the rectus muscles of the abdominal wall, or both.

Characteristic Physical Features of Trisomy 18
Clenched Fist With Polydactyly
Clenched Fist With Polydactyly

This photo shows the hand of an infant with trisomy 18. Note the clenched fist and postaxial polydactyly.

Image courtesy of Nina Powell-Hamilton, MD, FAAP, FACMG.

Low-Set Ear and Clenched Fists in Trisomy 18
Low-Set Ear and Clenched Fists in Trisomy 18

Image courtesy of the Centers for Disease Control and Prevention Public Health Image Library.

Rocker-Bottom Feet in Trisomy 18
Rocker-Bottom Feet in Trisomy 18

Image courtesy of the Centers for Disease Control and Prevention Public Health Image Library.

Clenched Fist in Trisomy 18
Clenched Fist in Trisomy 18

Image courtesy of the Centers for Disease Control and Prevention Public Health Image Library.

Diagnosis of Trisomy 18

  • Prenatal chorionic villus sampling and/or amniocentesis with cytogenetic testing by karyotype analysis, fluorescent in situ hybridization (FISH), and/or chromosomal microarray analysis (CMA)

(See also Next-generation sequencing technologies.)

Diagnosis of trisomy 18 may be suspected postnatally by appearance, or prenatally on ultrasonography (eg, with abnormalities of extremities and fetal growth restriction), or by multiple marker screening or noninvasive prenatal screening (NIPS) using cell-free fetal DNA analysis on a maternal blood sample (1). The sensitivity and specificity of NIPS for trisomy 18 is relatively low, compared to trisomy 21. Management decisions, including termination of pregnancy, should not be made based on NIPS testing alone.

Confirmation prenatally is by cytogenetic testing (karyotyping, FISH analysis, and/or chromosomal microarray analysis ) of samples obtained by amniocentesis or chorionic villus sampling, or postnatally by testing peripheral blood for women who did not wish to have additional procedures during pregnancy. Trisomy 18 detected on chorionic villus sampling may warrant further investigation either by amniocentesis or postnatal testing because the trisomy may represent confined placental mosaicism, in which aneuploidy is present in the placenta but undetectable in the fetus.

Diagnosis reference

  1. 1. American College of Obstetricians and Gynecologists’ Committee on Practice Bulletins—Obstetrics; Committee on Genetics; Society for Maternal-Fetal Medicine: Screening for fetal chromosomal abnormalities: ACOG Practice Bulletin, Number 226. Obstet Gynecol 136(4):e48-e69, 2020. doi: 10.1097/AOG.0000000000004084

Treatment of Trisomy 18

  • Supportive care

The underlying genetic abnormality cannot be cured.

Children with trisomy 18 have marked developmental delay and disability, so there is controversy about doing multiple, invasive procedures to correct various associated anomalies.

Early referral for physical and speech therapy is important. Support for the family is critical.

Screening for complications of trisomy 18

Treatment of some of the associated anomalies has increased survival for certain people with trisomy 18, which has led to recognition of an increased risk of solid organ tumors (eg, hepatoblastoma, Wilms tumor). Because early recognition of these tumors and other anomalies is important for successful treatment (if desired), regular surveillance is recommended. Although the specifics are based mainly on expert opinion at one center, there is a published surveillance protocol for tumors and other complications that many specialists find reasonable (1).

If screening detects abnormalities, children should be referred to the appropriate specialists.

Table

Treatment reference

  1. 1. Kepple JW, Fishler KP, Peeples ES: Surveillance guidelines for children with trisomy 18. Am J Med Genet A 185(4):1294–1303, 2021. doi: 10.1002/ajmg.a.62097

Prognosis for Trisomy 18

More than 50% of children die within the first week; only 5 to 10% survive the first year (1), but there are now reports of adults with trisomy 18 (2).

Prognosis references

  1. 1. Rasmussen SA, Wong LY, Yang Q, et al: Population-based analyses of mortality in trisomy 13 and trisomy 18. Pediatrics 111(4 Pt 1):777-784, 2003. doi: 10.1542/peds.111.4.777

  2. 2. Alshami A, Douedi S, Guida M, et al: Unusual Longevity of Edwards Syndrome: A Case Report. Genes (Basel) 11(12):1466, 2020. doi: 10.3390/genes11121466

More Information

The following English-language resources may be useful. Please note that THE MANUAL is not responsible for the content of these resources.

  1. American College of Obstetricians and Gynecologists Committee on Practice Bulletins–Obstetrics, Committee of Genetics, and the Society for Maternal–Fetal Medicine: Screening for fetal chromosomal abnormalities: ACOG practice bulletin, number 226 (2020)

  2. SOFT (Support Organization for Trisomy 18, 13, and Related Disorders): An organization providing resources, research information, and community and support services to people caring for others who have trisomy 18, 13, or another related chromosome disorder

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