Background Musculocontractural Ehlers–Danlos Syndrome (mcEDS) is a rare connective tissue disorder caused by biallelic loss‐of‐function variants in CHST14 (mcEDS‐CHST14) or DSE (mcEDS‐DSE), both of which result in defective dermatan sulfate biosynthesis. Forty‐one patients with mcEDS‐CHST14 and three patients with mcEDS‐DSE have been described in the literature. Methods Clinical, molecular, and glycobiological findings in three additional patients with mcEDS‐DSE were investigated. Results Three patients from two families shared craniofacial characteristics (hypertelorism, blue sclera, midfacial hypoplasia), skeletal features (pectus and spinal deformities, characteristic finger shapes, progressive talipes deformities), skin features (fine or acrogeria‐like palmar creases), and ocular refractive errors. Homozygous pathogenic variants in DSE were found: c.960TA/p.Tyr320* in patient 1 and c.996dupT/p.Val333Cysfs*4 in patients 2 and 3. No dermatan sulfate was detected in the urine sample from patient 1, suggesting a complete depletion of DS. Conclusion McEDS‐DSE is a congenital multisystem disorder with progressive symptoms involving craniofacial, skeletal, cutaneous, and cardiovascular systems, similar to the symptoms of mcEDS‐CHST14. However, the burden of symptoms seems lower in patients with mcEDS‐DSE.
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机译:背景技术肌钙动脉瘤ehlers-danlos综合征(mceds)是CHST14(MCEDS-CHST14)或DSE(MCEDS-DSE)中的双腿式函数变体引起的罕见结缔组织障碍,这两者都会导致皮肤有缺陷的皮肤硫酸盐生物合成。在文献中描述了四十一名患有Mccs-Chst14和三名患有Mccs-DSE患者的患者。方法研究了三种额外的MCEDS-DSE患者的临床,分子和糖血管学发现。结果三名患者来自两个家庭共用颅面特征(超兴奋,蓝巩膜,中阶发育不全),骨骼特征(PECTUS和脊柱畸形,特征手指形状,渐进式纵向畸形),皮肤特征(良好或助理等棕榈折痕)和眼部屈光误差。发现DSE中的纯合致病变体:C.960t> A / P.Tyr320 *患者1和C.996dupt / p.Val333333333333333333333333333333333CYSFS * 4在患者1的尿液中未检测到皮肤硫酸盐,表明DS完全消耗。结论Mcceds-DSE是一种先天性多系统障碍,具有渐进症状,涉及颅面,骨骼,皮肤和心血管系统,类似于MCEDS-CHST14的症状。然而,McceS-DSE患者症状的负担似乎较低。
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