Service d'endocrinologie, diabétologie et médecine de la reproduction, hôpital de l'Archet 2, université Côte d'Azur, CHU de Nice, Nice, France.
Inserm, CNRS, IRCAN, Université Côte d'Azur, CHU de Nice, Nice, France.
Ann Endocrinol (Paris). 2020 Jun;81(2-3):68-77. doi: 10.1016/j.ando.2020.04.007. Epub 2020 Apr 28.
While the most frequent mutation responsible for mitochondrial diabetes is the point mutation m.3243 A>G of mitochondrial DNA (mtDNA), few data are available about the role of rare mtDNA mutations in the pathophysiology of diabetes. The main objective of our study was to describe the phenotypic characteristics of patients suffering from diabetes linked to rare mtDNA mutations.
We performed a post-hoc analysis of a prospective multicenter cohort of 743 patients with mitochondrial disorder (previously published by the French Network of Mitochondrial Diseases), associated to a literature review of the PubMed database from 1992 to May 2016. We extracted all reported patients with diabetes and identified rare mtDNA mutations and described their clinical and metabolic phenotypes.
The 50 identified patients (10 from the princeps study; 40 from the review of the literature) showed a heterogeneous metabolic phenotype in terms of age, symptoms prior to diagnosis, treatments, and associated clinical and biological signs. However, neurological symptoms were more frequent in case of rare mtDNA mutations compared to the classical m.3243 A>G mutation (P=0.024). In contrast, deafness (65% vs. 95%, P=3.7E-5), macular pattern dystrophy (20% vs. 86%, P=1.6E-10) and nephropathy (8% vs. 28%, P=0.018) were significantly less frequent than in case of the classical m.3243 A>G mutation.
Although no specific metabolic phenotype could be identified suggesting or eliminating implication of rare mtDNA mutations in diabetes, clinical phenotypes featured more frequent neurological signs.
虽然导致线粒体糖尿病的最常见突变是线粒体 DNA(mtDNA)的点突变 m.3243 A>G,但关于罕见 mtDNA 突变在糖尿病发病机制中的作用的数据很少。我们研究的主要目的是描述与罕见 mtDNA 突变相关的糖尿病患者的表型特征。
我们对先前由法国线粒体疾病网络发表的 743 例线粒体疾病患者的前瞻性多中心队列进行了事后分析,并对 1992 年至 2016 年 5 月期间 PubMed 数据库的文献进行了综述。我们提取了所有报道的糖尿病患者,并确定了罕见的 mtDNA 突变,并描述了他们的临床和代谢表型。
在 50 名确定的患者(10 名来自 princeps 研究;40 名来自文献综述)中,根据年龄、诊断前症状、治疗方法以及相关的临床和生物学特征,表现出代谢表型的异质性。然而,与经典 m.3243 A>G 突变相比,罕见的 mtDNA 突变患者更常出现神经系统症状(P=0.024)。相比之下,耳聋(65%比 95%,P=3.7E-5)、黄斑图案营养不良(20%比 86%,P=1.6E-10)和肾病(8%比 28%,P=0.018)的发生率显著低于经典 m.3243 A>G 突变。
尽管没有确定的代谢表型可以提示或排除罕见 mtDNA 突变与糖尿病的关系,但临床表型更常出现神经系统症状。
