Akram Rabia, Baig Shahid Mahmood, Anwar Haseeb, Hussain Ghulam
Rabia Akram, M Phil. Department of Physiology, Neurochemicalbiology and Genetics Laboratory (NGL), Faculty of Life Sciences, Government College University, Faisalabad, Pakistan.
Shahid Mahmood Baig, PhD. Human Molecular Genetics Laboratory, Health Biotechnology Division, National Institute for Biotechnology and Genetic Engineering (NIBGE) College, Faisalabad, Pakistan. Department of Biological and Biomedical Sciences, Aga Khan University, Karachi, Pakistan.
Pak J Med Sci. 2024 Sep;40(8):1765-1769. doi: 10.12669/pjms.40.8.9246.
BACKGROUND & OBJECTIVES: Ataxia is usually caused by cerebellar pathology or a decrease in vestibular or proprioceptive afferent input to the cerebellum. It is characterized by uncoordinated walking, truncal instability, body or head tremors, uncontrolled coordination of the hands, dysarthria, and aberrant eye movements. The objective of the current investigation was to identify the underlying genetic cause of the hereditary ataxia that affects the Pakistani population.
We studied numerous consanguineous Pakistani families whose members had ataxia-related clinical symptoms to varying degrees. The families were chosen from the Punjab province, and the neurophysician conducted a clinical examination. Peripheral blood samples from both sick and healthy members of the family were taken after obtaining informed consent. Genomic DNA was used to find potential variations in probands using whole exome sequencing. The study was carried out at the University Hospital of Tübingen, Germany, and Government College University in Faisalabad, Pakistan, during 2018-2023.
The molecular analysis of these families identified different variants including : c.902C>T, c.668G>A, : c.6196_6197insGAA, : c.5769del, c.5525_5533del, and : c.7969A>T. A noteworthy mutation in and was observed among them, and its symptoms were shown to cause ataxia in these families.
The current study broadens the mutation spectrum of several hereditary ataxia types and suggests the next generation sequencing in conjunction with clinical research for a more accurate diagnosis of overlapping phenotypes of this disorder in the Pakistani population.
共济失调通常由小脑病变或小脑前庭或本体感觉传入输入减少引起。其特征为行走不协调、躯干不稳、身体或头部震颤、手部控制失调、构音障碍和异常眼动。本研究的目的是确定影响巴基斯坦人群的遗传性共济失调的潜在遗传原因。
我们研究了众多有血缘关系的巴基斯坦家庭,其成员有不同程度的共济失调相关临床症状。这些家庭来自旁遮普省,由神经科医生进行临床检查。在获得知情同意后,采集了患病和健康家庭成员的外周血样本。使用全外显子组测序,利用基因组DNA在先证者中寻找潜在变异。该研究于2018年至2023年在德国图宾根大学医院和巴基斯坦费萨拉巴德政府学院大学开展。
对这些家庭的分子分析确定了不同的变异,包括:c.902C>T、c.668G>A、c.6196_6197insGAA、c.5769del、c.5525_5533del和c.7969A>T。其中观察到一个值得注意的突变,其症状在这些家庭中导致了共济失调。
本研究拓宽了几种遗传性共济失调类型的突变谱,并建议结合临床研究进行下一代测序,以便对巴基斯坦人群中这种疾病的重叠表型进行更准确的诊断。
