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致死性骨骼发育异常的产前诊断

Antenatal diagnosis of lethal skeletal dysplasias.

作者信息

Tretter A E, Saunders R C, Meyers C M, Dungan J S, Grumbach K, Sun C C, Campbell A B, Wulfsberg E A

机构信息

Department of Pediatrics, University of Maryland School of Medicine, Baltimore 21201-1595, USA.

出版信息

Am J Med Genet. 1998 Feb 17;75(5):518-22.

PMID:9489797
Abstract

Lethal skeletal dysplasias (LSD) are a heterogeneous group of rare but important genetic disorders characterized by abnormal growth and development of bone and cartilage. We describe the diagnosis and outcome of 29 cases of lethal skeletal dysplasias evaluated between January 1989 and December 1996 at the University of Maryland Medical Center and the Ultrasound Institute of Baltimore. Two cases presented at delivery with no prenatal care while the remaining 27 cases were identified by antenatal sonography. Final diagnoses included thanatophoric dysplasia (14), osteogenesis imperfecta, type II (6), achondrogenesis (2), short rib syndromes (3), campomelic syndrome (2), atelosteogenesis (1), and no evidence of a skeletal dysplasia (1). Twenty out of 27 pregnancies were terminated with an average at detection of 21.6 weeks. The other 7 pregnancies that went on to deliver had an average age at detection of 29.2 weeks. Fetal abnormalities in the terminated pregnancies were identified at a significantly earlier gestational age (P = 0.0016) than the pregnancies that continued. While the identification of LSD by sonography was excellent (26/27), only 13/27 (48%) were given an accurate specific antenatal diagnosis. In 8/14 (57%) cases with an inaccurate or nonspecific diagnosis there was a significant or crucial change in the genetic counseling. Thus, while antenatal sonography is an excellent method for discovering LSD, clinical examination, radiographs, and autopsy are mandatory for making a specific diagnosis.

摘要

致死性骨骼发育异常(LSD)是一组罕见但重要的遗传性疾病,其特征为骨骼和软骨的生长发育异常。我们描述了1989年1月至1996年12月间在马里兰大学医学中心和巴尔的摩超声研究所评估的29例致死性骨骼发育异常的诊断和结局。2例在分娩时就诊,未接受产前检查,其余27例通过产前超声检查确诊。最终诊断包括致死性侏儒症(14例)、II型成骨不全(6例)、软骨发育不全(2例)、短肋综合征(3例)、弯肢侏儒综合征(2例)、骨发育不全(1例),以及无骨骼发育异常证据(1例)。27例妊娠中有20例终止妊娠,平均检测孕周为21.6周。其余7例继续妊娠并分娩的孕妇,平均检测孕周为29.2周。终止妊娠的胎儿异常在孕龄显著早于继续妊娠的胎儿时被发现(P = 0.0016)。虽然超声检查对LSD的诊断效果良好(26/27),但只有13/27(48%)得到了准确的产前特异性诊断。在8/14(57%)诊断不准确或不特异的病例中,遗传咨询发生了重大或关键变化。因此,虽然产前超声检查是发现LSD的优秀方法,但进行特异性诊断必须进行临床检查、X线检查和尸检。

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1
Antenatal diagnosis of lethal skeletal dysplasias.致死性骨骼发育异常的产前诊断
Am J Med Genet. 1998 Feb 17;75(5):518-22.
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Skeletal dysplasias: 38 prenatal cases.骨骼发育异常:38例产前病例。
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Prenatal sonographic diagnosis of skeletal dysplasias.产前超声诊断骨骼发育不良。
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[Osteogenesis imperfecta - diagnostic challenges].[成骨不全症——诊断挑战]
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