Department of Genetics, University of Groningen, University Medical Center Groningen, Groningen, The Netherlands.
Department of Medical Genetics, Amsterdam UMC, University of Amsterdam, Amsterdam, The Netherlands.
Orphanet J Rare Dis. 2019 Dec 19;14(1):294. doi: 10.1186/s13023-019-1269-0.
Mandibuloacral Dysplasia with type B lipodystrophy (MADB) is a rare premature aging disorder with an autosomal recessive inheritance pattern. MADB is characterized by brittle hair, mottled, atrophic skin, generalized lipodystrophy, insulin resistance, metabolic complications and skeletal features like stunted growth, mandibular and clavicular hypoplasia and acro-osteolysis of the distal phalanges. MADB is caused by reduced activity of the enzyme zinc metalloprotease ZMPSTE24 resulting from compound heterozygous or homozygous mutations in ZMPSTE24.
In 2012, and again in 2018, eight related patients from the remote tropical rainforest of inland Suriname were analysed for dysmorphic features. DNA analysis was performed and clinical features were documented. We also analysed all previously reported genetically confirmed MADB patients from literature (n = 12) for their clinical features. Based on the features of all cases (n = 20) we defined major criteria as those present in 85-100% of all MADB patients and minor criteria as those present in 70-84% of patients.
All the Surinamese patients are of African descent and share the same homozygous c.1196A > G, p.(Tyr399Cys) missense variant in the ZMPSTE24 gene, confirming MADB. Major criteria were found to be: short stature, clavicular hypoplasia, delayed closure of cranial sutures, high palate, mandibular hypoplasia, dental crowding, acro-osteolysis of the distal phalanges, hypoplastic nails, brittle and/or sparse hair, mottled pigmentation, atrophic and sclerodermic skin, and calcified skin nodules. Minor criteria were (generalized or partial) lipoatrophy of the extremities, joint contractures and shortened phalanges. Based on our detailed clinical observations, and a review of previously described cases, we propose that the clinical diagnosis of MADB is highly likely if a patient exhibits ≥4 major clinical criteria OR ≥ 3 major clinical criteria and ≥ 2 minor clinical criteria.
We report on eight related Surinamese patients with MADB due to a homozygous founder mutation in ZMPSTE24. In low-income countries laboratory facilities for molecular genetic testing are scarce or lacking. However, because diagnosing MADB is essential for guiding clinical management and for family counselling, we defined clinical diagnostic criteria and suggest management guidelines.
B 型脂肪营养不良性下颌骨-肢端发育不良症(MADB)是一种罕见的早发性衰老障碍,呈常染色体隐性遗传模式。MADB 的特征是头发脆弱、斑驳、萎缩性皮肤、全身性脂肪营养不良、胰岛素抵抗、代谢并发症以及骨骼特征,如生长迟缓、下颌骨和锁骨发育不良以及远端指骨的肢端骨溶解。MADB 是由锌金属蛋白酶 ZMPSTE24 的活性降低引起的,这是由于 ZMPSTE24 的复合杂合或纯合突变所致。
2012 年和 2018 年,我们对来自苏里南内陆偏远热带雨林的 8 名相关患者进行了分析,以评估其畸形特征。进行了 DNA 分析并记录了临床特征。我们还分析了文献中所有先前报道的经基因证实的 MADB 患者(n=12)的临床特征。基于所有病例(n=20)的特征,我们将主要标准定义为 85-100%的 MADB 患者存在的标准,次要标准定义为 70-84%的患者存在的标准。
所有苏里南患者均为非洲裔,均携带 ZMPSTE24 基因中相同的纯合 c.1196A>G,p.(Tyr399Cys) 错义变异,证实了 MADB 的存在。主要标准为:身材矮小、锁骨发育不良、颅缝闭合延迟、高腭、下颌骨发育不良、牙齿拥挤、远端指骨肢端骨溶解、甲床发育不良、脆弱和/或稀疏的头发、斑驳的色素沉着、萎缩性和硬皮病样皮肤以及钙化性皮肤结节。次要标准为(四肢)局部或全身性脂肪萎缩、关节挛缩和指骨缩短。基于我们的详细临床观察以及对先前描述病例的回顾,我们提出如果患者出现≥4 项主要临床标准或≥3 项主要临床标准和≥2 项次要临床标准,则极有可能做出 MADB 的临床诊断。
我们报告了苏里南的 8 名相关 MADB 患者,这些患者均由于 ZMPSTE24 的纯合启动子突变所致。在低收入国家,实验室进行分子遗传学检测的设施稀缺或缺乏。然而,由于诊断 MADB 对于指导临床管理和家庭咨询至关重要,因此我们定义了临床诊断标准并提出了管理指南。
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