Henneton Pierrick, Legrand Anne, Giunta Cecilia, Frank Michael
Médecine Interne et Vasculaire, Centre Hospitalier Regional Universitaire de Montpellier, Montpellier, France.
Service de Génétique, AP-HP, Hôpital Européen Georges Pompidou, Paris, France.
BMJ Case Rep. 2018 Jul 6;2018:bcr-2018-224423. doi: 10.1136/bcr-2018-224423.
Pathogenic variants in the lysyl-hydroxylase-1 gene (PLOD1) are responsible for the kyphoscoliotic type of Ehlers-Danlos syndrome (EDS). The disease is classically responsible for severe hypotonia at birth, progressive kyphoscoliosis, generalised joint hypermobility and scleral fragility. Arterial fragility is an important feature of the disease, but its characterisation remains limited. We report the clinical history of a 41-year-old woman who presented repeated arterial accidents, which occurred in previously normal medium size arteries within a limited time span of 2 years. Molecular investigations revealed compound heterozygosity for two PLOD1 gene deletions of exons 11-12 and 14-15. Arterial fragility is an important characteristic of kyphoscoliotic EDS. It manifests as spontaneous arterial rupture, dissections and dissecting aneurysms which may occur even during early childhood. This fragility is particularly likely to manifest during surgical intervention. Early medical management and surveillance may be indicated, but its modalities remain to be defined.
赖氨酰羟化酶-1基因(PLOD1)的致病性变异是脊柱后侧凸型埃勒斯-当洛综合征(EDS)的病因。该疾病通常导致出生时严重肌张力减退、进行性脊柱后侧凸、全身关节活动过度和巩膜脆弱。动脉脆弱是该疾病的一个重要特征,但其特征描述仍然有限。我们报告了一名41岁女性的临床病史,她在2年的有限时间内,在先前正常的中等大小动脉中反复发生动脉意外。分子研究显示该患者为PLOD1基因第11-12外显子和第14-15外显子两个缺失的复合杂合子。动脉脆弱是脊柱后侧凸型EDS的一个重要特征。它表现为自发性动脉破裂、夹层和夹层动脉瘤,甚至在儿童早期也可能发生。这种脆弱性在手术干预期间尤其可能表现出来。可能需要早期医疗管理和监测,但其方式仍有待确定。
