Coagulation abnormalities and vascular complications are common in PGM1-CDG

IF 3.7 2区 生物学 Q2 ENDOCRINOLOGY & METABOLISM Molecular genetics and metabolism Pub Date : 2024-07-02 DOI:10.1016/j.ymgme.2024.108530
Silvia Radenkovic , Sofie Bleukx , Nicole Engelhardt , Erik Eklund , Saadet Mercimek-Andrews , Andrew C. Edmondson , Eva Morava
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Abstract

Phosphoglucomutase-1-congenital disorder of glycosylation (PGM1-CDG) is a rare genetic disorder caused by biallelic variants in the PGM1 gene, leading to the deficiency of the PGM1 enzyme. The most common clinical presentations include muscle involvement, failure to thrive, cleft palate, and cardiac involvement. Abnormal serum N-glycosylation, hypoglycemia, and liver function abnormalities including coagulation abnormalities are the most common laboratory abnormalities. While PGM1-CDG has been extensively studied, little is known about the extent of the coagulation abnormalities in individuals with PGM1-CDG. Unlike most CDG, some symptoms of PGM1-CDG are treatable with D-galactose (D-gal) supplementation, though reliable clinical endpoints are necessary to appropriately evaluate the potential improvement with D-gal in PGM1-CDG. Here, we aimed to describe the incidence of coagulation abnormalities in PGM1-CDG and their evolution, their relation to clinical events, and the ability of D-gal treatment to improve them. A retrospective analysis was conducted on 73 reported individuals. All individuals had a molecularly confirmed PGM1-CDG diagnosis. All incidences of antithrombin (AT), aPTT, PT, factor (F) XI, FX, FIX, FVII, protein C and protein S data and major clinical events related to coagulation abnormalities, were collected. Coagulation information was available for only 58.9 % of the reported individuals, out of which 67.4 % of PGM1-CDG individuals were reported to have abnormalities. The most frequently observed abnormality was AT (mean: 30.8% R:80-120 %) deficiency. Four individuals had major thrombotic events. Coagulation status on D-gal treatment, were reported in 19 individuals. Several factors showed improvement including AT (mean: 64.5 %), indicating galactose is beneficial in treating coagulation abnormalities in PGM1-CDG. Due to the scarcity of the reported data on coagulation parameters, we also evaluated data collected in sixteen PGM1-CDG individuals enrolled in the FCDGC Natural History Study. Longitudinal data showed improvements in several coagulant parameters and disease severity improved for almost all patients of whom we had multiple datapoints on D-gal. AT showed significant improvement on D-gal. We conclude that coagulation abnormalities are frequently present in PGM1-CDG and show improvement on D-gal. We recommend coagulation parameters should be routinely checked in individuals with PGM1-CDG or suspected of having PGM1-CDG. Finally, AT may be used as a primary or secondary clinical endpoint for upcoming clinical trials in PGM1-CDG individuals.

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PGM1-CDG 常见凝血异常和血管并发症。
磷酸葡萄糖突变酶-1-先天性糖基化障碍(PGM1-CDG)是一种罕见的遗传性疾病,由PGM1基因的双倍变异引起,导致PGM1酶缺乏。最常见的临床表现包括肌肉受累、发育不良、腭裂和心脏受累。血清 N-糖基化异常、低血糖和肝功能异常(包括凝血功能异常)是最常见的实验室异常。虽然对 PGM1-CDG 进行了广泛的研究,但对 PGM1-CDG 患者的凝血异常程度却知之甚少。与大多数 CDG 不同的是,PGM1-CDG 的某些症状可以通过补充 D-半乳糖(D-gal)来治疗,但要适当评估 D-gal 对 PGM1-CDG 的潜在改善作用,还需要可靠的临床终点。在此,我们旨在描述 PGM1-CDG 中凝血异常的发生率及其演变、它们与临床事件的关系以及 D-gal 治疗改善这些异常的能力。我们对 73 例报告患者进行了回顾性分析。所有患者均经分子确诊为 PGM1-CDG。收集了所有抗凝血酶 (AT)、aPTT、PT、因子 (F) XI、FX、FIX、FVII、蛋白 C 和蛋白 S 数据的发生率以及与凝血异常有关的主要临床事件。仅有 58.9% 的报告者提供了凝血信息,其中 67.4% 的 PGM1-CDG 报告者有凝血异常。最常见的异常是 AT(平均:30.8% R:80-120%)缺乏。有 4 人发生了严重的血栓事件。据报告,19 人在接受 D-gal 治疗后出现了凝血状况。包括AT(平均:64.5%)在内的几种因素都有所改善,这表明半乳糖对治疗PGM1-CDG的凝血异常有益。由于有关凝血参数的报告数据很少,我们还评估了参加 FCDGC 自然史研究的 16 名 PGM1-CDG 患者的数据。纵向数据显示,几项凝血参数有所改善,几乎所有患者的疾病严重程度都有所改善,而且我们在 D-gal 上获得了多个数据点。 我们的结论是,PGM1-CDG 患者经常出现凝血异常,而且在 D-gal 上有所改善。 我们建议对 PGM1-CDG 患者或疑似 PGM1-CDG 患者进行常规凝血参数检查。最后,在即将对 PGM1-CDG 患者进行的临床试验中,可将 AT 作为主要或次要临床终点。
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来源期刊
Molecular genetics and metabolism
Molecular genetics and metabolism 生物-生化与分子生物学
CiteScore
5.90
自引率
7.90%
发文量
621
审稿时长
34 days
期刊介绍: Molecular Genetics and Metabolism contributes to the understanding of the metabolic and molecular basis of disease. This peer reviewed journal publishes articles describing investigations that use the tools of biochemical genetics and molecular genetics for studies of normal and disease states in humans and animal models.
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