Trisomy 18 (Edwards syndrome) and major gastrointestinal malformations

Rosa, Rafael Fabiano Machado; Rosa, Rosana Cardoso Manique; Lorenzen, Marina Boff; Zen, Paulo Ricardo Gazzola; Oliveira, Ceres Andréia Vieira de; Graziadio, Carla; Paskulin, Giorgio Adriano

doi:10.1590/S1516-31802013000100025

Trisomy 18 or Edwards syndrome is a chromosomal disease characterized by involvement of many organs and systems, and limited survival.¹1. Rosa RF, Rosa RC, Lorenzen MB, et al. Trisomy 18: experience of a reference hospital from the south of Brazil. Am J Med Genet A. 2011;155A(7):1529-35. The aim of our study was to determine the frequency and types of major gastrointestinal abnormalities observed among patients with Edwards syndrome. The sample consisted of patients consecutively evaluated over the period between 1975 and 2008 in a clinical genetics service at a referral hospital in southern Brazil. Clinical data and karyotype results were gathered from this hospital's medical records. We use Fisher's exact test (two-tailed) to compare frequencies (P values < 0.05 were considered significant). Thus, our sample was composed of 50 patients, of whom 33 (66%) were female. Their ages at the first evaluation ranged from 1 day to 16 years (median 14 days). Eight of the patients (16%) were born in that hospital.

Presence of a single lineage with free trisomy of chromosome 18 was the main abnormality, observed in 90% of the cases. The remainder consisted of patients with mosaicism. Major gastrointestinal abnormalities were observed in eight patients (16%): two cases of esophageal atresia (4%), three of tracheoesophageal fistula (6%) (one associated with esophageal atresia), one of diaphragmatic hernia (2%) and three of omphalocele (6%). Among these eight patients, five (62%) were female. Their ages at the time of the initial evaluation ranged from one to 70 days (median 7.5 days). Only two patients (25%) presented a clinical suspicion of Edwards syndrome. Additional abnormalities, including minor and major anomalies, were observed in all cases. These included dysmorphic features like a clenched fist with overlapping fingers and major malformations like congenital heart defects. None had a chromosomal constitution with mosaicism. Three patients underwent surgical correction of their defects (one with esophageal atresia, one with tracheoesophageal fistula and one with omphalocele). In all cases, the diagnosis of Edwards syndrome was made only after surgery.

Gastrointestinal malformations are frequent among patients with Edwards syndrome. In the literature, the frequency of esophageal atresia among these patients ranges from 16 to 18%.²2. Kinoshita M, Nakamura Y, Nakano R, et al. Thirty-one autopsy cases of trisomy 18: clinical features and pathological findings. Pediatr Pathol. 1989;9(4):445-57.−⁴4. Lin HY, Lin SP, Chen YJ, et al. Clinical characteristics and survival of trisomy 18 in a medical center in Taipei, 1988-2004. Am J Med Genet A. 2006;140(9):945-51. Despite the frequency of 4% observed in our study, no statistically significant difference was seen using Fisher's exact test when we compared it with these studies. However, it is noteworthy that the samples in other studies (n = 24 to 39 patients) were smaller than in ours (n = 50). Patients with esophageal atresia usually present the associated finding of tracheoesophageal fistula,⁴4. Lin HY, Lin SP, Chen YJ, et al. Clinical characteristics and survival of trisomy 18 in a medical center in Taipei, 1988-2004. Am J Med Genet A. 2006;140(9):945-51.,⁵5. Moore CA, Harmon JP, Padilla LM, Castro VB, Weaver DD. Neural tube defects and omphalocele in trisomy 18. Clin Genet. 1988;34(2):98-103. as observed in one of our two patients. Omphalocele has been described in less than 10% of the patients,²2. Kinoshita M, Nakamura Y, Nakano R, et al. Thirty-one autopsy cases of trisomy 18: clinical features and pathological findings. Pediatr Pathol. 1989;9(4):445-57.−⁵5. Moore CA, Harmon JP, Padilla LM, Castro VB, Weaver DD. Neural tube defects and omphalocele in trisomy 18. Clin Genet. 1988;34(2):98-103. which is compatible with the rate in our study (6%). Despite the possible association described in the literature,⁵5. Moore CA, Harmon JP, Padilla LM, Castro VB, Weaver DD. Neural tube defects and omphalocele in trisomy 18. Clin Genet. 1988;34(2):98-103. none of our patients with omphalocele presented a neural tube defect. Diaphragmatic hernia is considered to be a less common abnormality, and has been described in less than 8% of the patients.²2. Kinoshita M, Nakamura Y, Nakano R, et al. Thirty-one autopsy cases of trisomy 18: clinical features and pathological findings. Pediatr Pathol. 1989;9(4):445-57.−⁴4. Lin HY, Lin SP, Chen YJ, et al. Clinical characteristics and survival of trisomy 18 in a medical center in Taipei, 1988-2004. Am J Med Genet A. 2006;140(9):945-51. This frequency was similar to our study (2%).

Thus, Edwards syndrome should always be considered among dysmorphic children presenting these major gastrointestinal malformations. Diagnosing it is important for proper management and for determining the prognosis for these patients.

REFERENCES

¹
Rosa RF, Rosa RC, Lorenzen MB, et al. Trisomy 18: experience of a reference hospital from the south of Brazil. Am J Med Genet A. 2011;155A(7):1529-35.
²
Kinoshita M, Nakamura Y, Nakano R, et al. Thirty-one autopsy cases of trisomy 18: clinical features and pathological findings. Pediatr Pathol. 1989;9(4):445-57.
³
Sugayama SMM, Kim CA, Utagawa CY, et al. Estudo genético-clínico de 24 pacientes com trissomia 18 (síndrome de Edwards) [Clinical and genetic study of 24 patients with trisomy 18 (Edwards' syndrome)]. Pediatria (São Paulo). 1999;21(2):133-43. Available from: http://pediatriasaopaulo.usp.br/upload/pdf/415.pdf Accessed in 2012 (Jun 14).
» http://pediatriasaopaulo.usp.br/upload/pdf/415.pdf
⁴
Lin HY, Lin SP, Chen YJ, et al. Clinical characteristics and survival of trisomy 18 in a medical center in Taipei, 1988-2004. Am J Med Genet A. 2006;140(9):945-51.
⁵
Moore CA, Harmon JP, Padilla LM, Castro VB, Weaver DD. Neural tube defects and omphalocele in trisomy 18. Clin Genet. 1988;34(2):98-103.

Publication Dates

Publication in this collection
Apr 2013

History

Reviewed
25 Apr 2012
Received
22 June 2012
Accepted
30 July 2012

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] ¹
Rosa RF, Rosa RC, Lorenzen MB, et al. Trisomy 18: experience of a reference hospital from the south of Brazil. Am J Med Genet A. 2011;155A(7):1529-35.

[2] ²
Kinoshita M, Nakamura Y, Nakano R, et al. Thirty-one autopsy cases of trisomy 18: clinical features and pathological findings. Pediatr Pathol. 1989;9(4):445-57.

[3] ³
Sugayama SMM, Kim CA, Utagawa CY, et al. Estudo genético-clínico de 24 pacientes com trissomia 18 (síndrome de Edwards) [Clinical and genetic study of 24 patients with trisomy 18 (Edwards' syndrome)]. Pediatria (São Paulo). 1999;21(2):133-43. Available from: http://pediatriasaopaulo.usp.br/upload/pdf/415.pdf Accessed in 2012 (Jun 14).
» http://pediatriasaopaulo.usp.br/upload/pdf/415.pdf

[4] ⁴
Lin HY, Lin SP, Chen YJ, et al. Clinical characteristics and survival of trisomy 18 in a medical center in Taipei, 1988-2004. Am J Med Genet A. 2006;140(9):945-51.

[5] ⁵
Moore CA, Harmon JP, Padilla LM, Castro VB, Weaver DD. Neural tube defects and omphalocele in trisomy 18. Clin Genet. 1988;34(2):98-103.

Brasil

Brasil

Trisomy 18 (Edwards syndrome) and major gastrointestinal malformations

Trissomia do cromossomo 18 (síndrome de Edwards) e malformações gastrointestinais maiores

REFERENCES

Publication Dates

History