TY - JOUR
T1 - Autosomal-dominant non-syndromic anal atresia
T2 - Sequencing of candidate genes, array-based molecular karyotyping, and review of the literature
AU - Schramm, Charlotte
AU - Draaken, Markus
AU - Tewes, Gabriel
AU - Bartels, Enrika
AU - Schmiedeke, Eberhard
AU - Märzheuser, Stefanie
AU - Grasshoff-Derr, Sabine
AU - Hosie, Stuart
AU - Holland-Cunz, Stefan
AU - Priebe, Lutz
AU - Kreiß-Nachtsheim, Martina
AU - Hoffmann, Per
AU - Aretz, Stefan
AU - Nöthen, Markus M.
AU - Reutter, Heiko
AU - Ludwig, Michael
PY - 2011/6
Y1 - 2011/6
N2 - Introduction: Anorectal malformations (ARM) range from mild anal to severe anorectal anomalies. Approximately 50% are estimated to be non-syndromic with multiple familial cases reported that suggest underlying genetic factors. These, however, still await identification. Materials and methods: We report a familial case of non-syndromic ARM with a mother and her two children being affected. Mother and daughter had mild ARM that had only been diagnosed after the index patient was born with a more severe form and ultrashort Hirschsprung's disease. To reveal the genetic cause in our family genome-wide array analysis was carried out to ascertain microaberrations characterized by loss or gain of genomic material. In addition, sequence analysis of four major Hirschsprung's disease genes (RET, EDNRB, EDN3, and GDNF) and the HLXB9 gene was performed to identify a mutation common to all three family members; however, these analyses did not reveal any causal genetic alteration. To demonstrate the frequency of familial non-syndromic cases, we performed a literature search revealing 59 families with at least two affected members. Sufficient description of ARM phenotype and affection status of relatives to surely classify them as familial non-syndromic forms was given for 22 families. Conclusion: The present family suggests that mild ARM may be overlooked in patients with non-specific clinical symptoms and that the incidence of ARM may thus be higher than previously estimated. With the new possibilities of whole exome sequencing, even small families hold the possibility to identify causal defects.
AB - Introduction: Anorectal malformations (ARM) range from mild anal to severe anorectal anomalies. Approximately 50% are estimated to be non-syndromic with multiple familial cases reported that suggest underlying genetic factors. These, however, still await identification. Materials and methods: We report a familial case of non-syndromic ARM with a mother and her two children being affected. Mother and daughter had mild ARM that had only been diagnosed after the index patient was born with a more severe form and ultrashort Hirschsprung's disease. To reveal the genetic cause in our family genome-wide array analysis was carried out to ascertain microaberrations characterized by loss or gain of genomic material. In addition, sequence analysis of four major Hirschsprung's disease genes (RET, EDNRB, EDN3, and GDNF) and the HLXB9 gene was performed to identify a mutation common to all three family members; however, these analyses did not reveal any causal genetic alteration. To demonstrate the frequency of familial non-syndromic cases, we performed a literature search revealing 59 families with at least two affected members. Sufficient description of ARM phenotype and affection status of relatives to surely classify them as familial non-syndromic forms was given for 22 families. Conclusion: The present family suggests that mild ARM may be overlooked in patients with non-specific clinical symptoms and that the incidence of ARM may thus be higher than previously estimated. With the new possibilities of whole exome sequencing, even small families hold the possibility to identify causal defects.
KW - Anal atresia
KW - Anorectal malformations
KW - Multiplex family
KW - Ultrashort Hirschsprung's disease
UR - http://www.scopus.com/inward/record.url?scp=79959731575&partnerID=8YFLogxK
U2 - 10.1007/s00431-010-1332-2
DO - 10.1007/s00431-010-1332-2
M3 - Article
C2 - 21042811
AN - SCOPUS:79959731575
SN - 0340-6199
VL - 170
SP - 741
EP - 746
JO - European Journal of Pediatrics
JF - European Journal of Pediatrics
IS - 6
ER -