Dr. John T. Macdonald Foundation, Department of Human Genetics, Miller School of Medicine, University of Miami, Miami, FL 33136, USA.
Magnetic Resonance Center, University of Florence, 50019 Florence, Italy.
Genes (Basel). 2022 Nov 6;13(11):2044. doi: 10.3390/genes13112044.
Multiple mitochondrial dysfunction syndrome type 3 (MMDS3) is a rare mitochondrial leukoencephalopathy caused by biallelic pathogenic variants in . Here, we describe a homozygous variant in , (NM_001010867.2): c.310G>T (p.Gly104Cys), in a 2-month-old infant of Cuban descent who presented with a one-month history of progressive hypotonia, weakness, and episodes of upgaze deviation. This is the first report of a patient homozygous for this variant and the first report of MMDS3 in a patient of Hispanic descent described to our knowledge. Using in silico tools, we found that the variant resides in a putative mutational hotspot located in the neighborhood of a key active ligand required for iron-sulfur cluster coordination. In addition, while previous case reports/series have reported the variable phenotypic features of the disease, the incidence of these features across the literature has not been well described. In order to construct a clearer global picture of the typical presentation of MMDS3, we reviewed 52 cases across the literature with respect to their clinical, biochemical, genotypic, and neuroradiographic features.
多系统线粒体功能障碍综合征 3 型(MMDS3)是一种罕见的线粒体脑肌病,由 基因的双等位致病性变异引起。在此,我们描述了一位 2 月龄、具有古巴血统的患儿,其携带 基因的纯合变异:c.310G>T(p.Gly104Cys)(NM_001010867.2),该患儿有进行性肌张力低下、无力和上视障碍的病史 1 个月。这是首例报道该变异纯合子的患者,也是我们所知的首例报道的西班牙裔患者的 MMDS3。使用计算机预测工具,我们发现该变异位于一个假定的突变热点区域,该区域位于一个关键的活性配体附近,这个配体对于铁硫簇的协调是必需的。此外,虽然之前的病例报告/系列已经报道了该疾病的可变表型特征,但这些特征在文献中的发生率尚未得到很好的描述。为了更清晰地构建 MMDS3 的典型表现的全球图景,我们回顾了文献中的 52 例病例,评估了其临床、生化、基因型和神经影像学特征。
