库拉里诺综合征：基因异常的存在是否与更严重的表型相关？一项多中心研究。

Currarino syndrome: does the presence of a genetic anomaly correlate with a more severe phenotype? A multicentre study.

作者信息

Costanzo Sara, Spaccini Luigina, Pio Luca, Mattioli Girolamo, Virgone Calogero, Dall'Igna Patrizia, Iacobelli Barbara, Inserra Alessandro, Brisighelli Giulia, Fagnani Anna Maria, Leva Ernesto, Giannotti Giulia, Cheli Maurizio, Frumento Paolo, Riccipetitoni Giovanna

机构信息

Pediatric Surgery Unit, V. Buzzi Children's Hospital, Milan, Italy.

Genetic Service, V. Buzzi Children's Hospital, Milan, Italy.

出版信息

J Pediatr Surg. 2017 Oct;52(10):1591-1596. doi: 10.1016/j.jpedsurg.2017.06.012. Epub 2017 Jun 24.

DOI:10.1016/j.jpedsurg.2017.06.012

PMID:28689883

Abstract

BACKGROUND/PURPOSE: Currarino syndrome (CS) phenotype, initially described as the triad of hemisacrum, anorectal malformation (ARM) and presacral mass, can be extremely variable. The triad is often incomplete and 3 main CS phenotypical subtypes have been described: Complete, Mild and Minimal. Various associated malformations are often present. Mutations in the MNX1 gene are the main genetic background of CS, although they are not present in almost half of the cases. Aim of our study is to analyze the distribution of the 3 CS subtypes and the incidence of associated malformations in a large sample of patients and to add information about the role of the genetic testing in guiding the diagnostic and prognostic evaluation of CS patients.

METHODS

A multicentre retrospective data collection was performed. CS patients' phenotype was accurately analyzed according to a diagnostic-therapeutic standardized data collection sheet. The distribution of the three CS types and the frequency of each associated malformation were calculated. The phenotype of the patients with a known genetic anomaly was compared to the phenotype of the population with no genetic diagnosis, in order to determine whether the presence of a known genetic defect could correlate with a more severe CS phenotype.

RESULTS

Data from 45 patients were analyzed. Twenty patients (44.5%) presented a Complete CS type, 19 (42.2%) a Mild CS and 6 (13.3%) a Minimal CS. In addition to the classical triad elements, 38 (84.5%) patients showed associated anomalies. The group of patients who resulted positive for a MNX1 mutation comprised a higher number (56.5%) of Complete CS cases than the group of patients that did not carry any MNX1 mutation (13%) (p = 0.0085). We could not find any relationship between CS subtype and the number of associated anomalies (p = 0.5102).

CONCLUSIONS

The presence of a MNX1 mutation seems to correlate with a more severe CS phenotype. MNX1 seems the main responsible for the expression and the severity of the CS triad, while the associated anomalies appear to be prevalently determined by genes sited on different loci. A thorough multidisciplinary diagnostic overview of CS patients should always include genetic counseling and analysis, both in postnatal and prenatal settings.

TYPE OF STUDY

Retrospective Study.

LEVEL OF EVIDENCE

II.

摘要

背景/目的：库拉里诺综合征（CS）的表型最初被描述为半骶骨、肛门直肠畸形（ARM）和骶前肿块三联征，其表现可能极具多样性。该三联征往往并不完整，已描述了3种主要的CS表型亚型：完全型、轻度型和微小（或最小）型。常伴有各种相关畸形。MNX1基因突变是CS的主要遗传背景，尽管几乎半数病例中不存在该突变。本研究的目的是分析大量患者样本中3种CS亚型的分布情况及相关畸形的发生率，并补充有关基因检测在指导CS患者诊断和预后评估中作用的信息。

方法

进行了一项多中心回顾性数据收集。根据一份诊断 - 治疗标准化数据收集表对CS患者的表型进行了精确分析。计算了3种CS类型的分布情况以及每种相关畸形的发生频率。将已知存在基因异常的患者表型与未进行基因诊断的人群表型进行比较，以确定已知基因缺陷的存在是否与更严重的CS表型相关。

结果

分析了45例患者的数据。20例（44.5%）呈现完全型CS，19例（42.2%）为轻度型CS，6例（13.3%）为微小（或最小）型CS。除了经典的三联征要素外，38例（84.5%）患者还表现出相关异常。MNX1基因突变检测呈阳性的患者组中，完全型CS病例的数量（56.5%）高于未携带任何MNX1突变的患者组（13%）（p = 0.0085）。我们未发现CS亚型与相关异常数量之间存在任何关联（p = 0.5102）。