Gripp K W, Stolle C A, Celle L, McDonald-McGinn D M, Whitaker L A, Zackai E H
Division of Human Genetics and Molecular Biology, The Children's Hospital of Philadelphia, Pennsylvania 19104, USA.
Am J Med Genet. 1999 Jan 15;82(2):170-6. doi: 10.1002/(sici)1096-8628(19990115)82:2<170::aid-ajmg14>3.0.co;2-x.
The term Baller-Gerold syndrome was coined by Cohen [1979: Birth Defects 15(5B): 13-63] to designate the phenotype of craniosynostosis and radial aplasia. It is thought to be a rare autosomal recessive condition, which, in some patients, presents with additional abnormalities, such as polymicrogyria, mental retardation or anal atresia. A phenotypic overlap of Baller-Gerold and Roberts-SC phocomelia syndrome was noted when a patient with bicoronal synostosis and bilateral radial hypoplasia was found to have premature centromere separation, a finding characteristic of Roberts syndrome [Huson et al.,1990: J Med Genet 27:371-375]. Other cases of presumed Baller-Gerold syndrome were rediagnosed as Fanconi pancytopenia, Rothmund-Thomson syndrome or VACTERL association. These reports led to a narrowed redefinition of Baller-Gerold syndrome based on the exclusion of cytogenetic and hematopoetic abnormalities and the absence of additional malformations in patients with craniosynostosis and preaxial upper limb abnormalities. Here we report on a patient with unilateral radial aplasia and bicoronal synostosis without additional malformations and without chromosome breakage, who fits this narrow definition of Baller-Gerold syndrome. We identified a novel TWIST gene mutation in this patient, a Glu181Stop mutation predicting a premature termination of the protein carboxy-terminal to the helix 2 domain. This report provides further evidence that Baller-Gerold is of heterogeneous cause, and a thorough evaluation is indicated to identify a possibly more specific diagnosis, including Saethre-Chotzen syndrome. This differential diagnosis is of particular importance, as it is an autosomal dominant trait. Therefore, the recurrence risk for parents of an affected child can be 50% if one parent carries the mutation, as opposed to the 25% recurrence risk for autosomal recessive inheritance. Offspring of the affected patient also have a 50% risk to inherit the mutation, while the risk to bear an affected offspring for an autosomal recessive trait is very low.
“巴勒 - 杰罗尔德综合征”这一术语由科恩(1979年:《出生缺陷》15(5B):13 - 63)提出,用于指代颅缝早闭和桡骨发育不全的表型。它被认为是一种罕见的常染色体隐性疾病,在一些患者中还伴有其他异常,如多小脑回、智力发育迟缓或肛门闭锁。当一名患有双冠状缝早闭和双侧桡骨发育不全的患者被发现有过早的着丝粒分离现象(这是罗伯茨综合征的一个特征性表现)时,人们注意到巴勒 - 杰罗尔德综合征与罗伯茨 - SC短肢畸形综合征存在表型重叠[休森等人,1990年:《医学遗传学杂志》27:371 - 375]。其他疑似巴勒 - 杰罗尔德综合征的病例被重新诊断为范可尼全血细胞减少症、罗思蒙德 - 汤姆森综合征或VACTERL联合征。这些报告导致了对巴勒 - 杰罗尔德综合征的重新定义更加严格,即排除细胞遗传学和造血异常,且患有颅缝早闭和上肢轴前异常的患者不存在其他畸形。在此,我们报告一名患有单侧桡骨发育不全和双冠状缝早闭且无其他畸形及染色体断裂的患者,该患者符合巴勒 - 杰罗尔德综合征的这一狭义定义。我们在该患者中鉴定出一种新的TWIST基因突变,即Glu181Stop突变,该突变预测蛋白质在螺旋2结构域羧基末端会过早终止。本报告进一步证明巴勒 - 杰罗尔德综合征病因具有异质性,因此需要进行全面评估以确定可能更具体的诊断,包括塞特雷 - 乔岑综合征。这种鉴别诊断尤为重要,因为它是一种常染色体显性性状。所以,如果父母一方携带该突变,患病儿童父母的复发风险可能为50%,这与常染色体隐性遗传25%的复发风险不同。患病患者的后代继承该突变的风险也为50%,而对于常染色体隐性性状,生育患病后代的风险非常低。
