We present a clinical case of a female infant with multiple anomalies and distinctive facial features, with an exceptionally severe clinical course of Hirschsprung disease. The girl was also diagnosed with Mowat-Wilson syndrome, confirmed by molecular analysis as a heterozygous deletion of the ZEB2 gene. Moreover, molecular karyotyping revealed a deletion involving further genes (KYNU, ARHGAP15, and GTDC1).Mowat-Wilson syndrome (MWS) is a recently delineated syndrome with multiple congenital anomalies and mental retardation (Amiel et al. 2001;Cacheux et al. 2001;Mowat et al. 1998;Wakamatsu et al. 2001;Zweier et al. 2002). MWS is characterized by distinctive facial features, short stature, and structural anomalies, including Hirschsprung disease (HD), genitourinary anomalies, congenital heart defects, agenesis or hypogenesis of the corpus callosum, and eye defects, as well as moderate to severe intellectual disability and severe speech impairment. We present a young female with a clinical diagnosis of MWS, confirmed by molecular analysis, presenting a severe course of HD.The proband was born to a G2,P1 healthy mother at 36 weeks of gestation. The parameters at birth were: weight 2600 g, length 52 cm, OFC 31 cm. Heart murmur, delayed meconium passage, and enterocolitis, were diagnosed after birth. Echocardiography showed a Fallot tetralogy. Radiographic barium enema studies suggested HD, which was confirmed by immunohistochemistry.During the operative procedure a short segment of aganglionosis was found and sigmoid colostomy was created. The postoperative course was complicated by multiple eventrations and severe sepsis. At the age of 18 months, the Duhamel procedure was planned. However, during the operation the Swenson procedure was performed, because of severe adhesions and difficult tissue preparation. The course of the disease was complicated again by leakage at the level of colorectal anastomosis, which required temporal protective ileostomy. Two days later the girl was reoperated because of severe haemorrhage from the rectum and through the peritoneal drain, but the source of bleeding was not found and she developed a sepsis. Ten days later ileal mechanical obstruction occurred. The ileostomy was closed 2 months later. The subsequent course was complicated by an incisional hernia. No congenital and acquired immunological defects were detected. However, hepatic cell lesion and a-1 antitrypsin deficiency (ATD) were revealed. The microscopic evaluation Abstract. We present a clinical case of a female infant with multiple anomalies and distinctive facial features, with an exceptionally severe clinical course of Hirschsprung disease. The girl was also diagnosed with Mowat-Wilson syndrome, confirmed by molecular analysis as a heterozygous deletion of the ZEB2 gene. Moreover, molecular karyotyping revealed a deletion involving further genes (KYNU, ARHGAP15, and GTDC1).
