Genetics of Ataxias in Indian Population: A Collative Insight from a Common Genetic Screening Tool

Advanced genetics (Hoboken, N.J.) Pub Date : 2022-03-10 DOI:10.1002/ggn2.202100078

Pooja Sharma, Akhilesh Kumar Sonakar, Nishu Tyagi, Varun Suroliya, Manish Kumar, Rintu Kutum, Vivekananda Asokchandran, Sakshi Ambawat, Uzma Shamim, Avni Anand, Ishtaq Ahmad, Sunil Shakya, Bharathram Uppili, Aradhana Mathur, Shaista Parveen, Shweta Jain, Jyotsna Singh, Malika Seth, Sana Zahra, Aditi Joshi, Divya Goel, Shweta Sahni, Asangla Kamai, Saruchi Wadhwa, Aparna Murali, Sheeba Saifi, Debashish Chowdhury, Sanjay Pandey, Kuljeet Singh Anand, Ranganathan Lakshmi Narasimhan, Sanghamitra Laskar, Suman Kushwaha, Mukesh Kumar, Cheruvallill Velayudhan Shaji, Madakasira Vasantha Padma Srivastava, Achal K. Srivastava, Mohammed Faruq, GOMED-Ataxia study group

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引用次数: 4

Abstract

Cerebellar ataxias (CAs) represent a group of autosomal dominant and recessive neurodegenerative disorders affecting cerebellum with or without spinal cord. Overall, CAs have preponderance for tandem nucleotide repeat expansions as an etiological factor (10 TREs explain nearly 30–40% of ataxia cohort globally). The experience of 10 years of common genetic ataxia subtypes for ≈5600 patients’ referrals (Pan-India) received at a single center is shared herein. Frequencies (in %, n) of SCA types and FRDA in the sample cohort are observed as follows: SCA12 (8.6%, 490); SCA2 (8.5%, 482); SCA1 (4.8%, 272); SCA3 (2%, 113); SCA7 (0.5%, 28); SCA6 (0.1%, 05); SCA17 (0.1%, 05), and FRDA (2.2%, 127). A significant amount of variability in TRE lengths at each locus is observed, we noted presence of biallelic expansion, co-occurrence of SCA-subtypes, and the presence of premutable normal alleles. The frequency of mutated GAA-FRDA allele in healthy controls is 1/158 (0.63%), thus an expected FRDA prevalence of 1:100 000 persons. The data of this study are relevant not only for clinical decision making but also for guidance in direction of genetic investigations, transancestral comparison of genotypes, and lastly provide insight for policy decision for the consideration of SCAs under rare disease category.

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印度人群共济失调的遗传学:来自共同遗传筛选工具的合作见解

小脑共济失调(CAs)是一组常染色体显性和隐性影响小脑的神经退行性疾病，伴或不伴脊髓。总的来说，CAs具有串联核苷酸重复扩增的优势，作为一个病因因素(10个TREs解释了全球近30-40%的共济失调队列)。本文分享了在单一中心接收的约5600名转诊患者(泛印度)10年来常见遗传性共济失调亚型的经验。样本队列中SCA类型和FRDA的频率(以%，n为单位)如下:SCA12 (8.6%， 490);Sca2 (8.5%， 482);sc1 (4.8%， 272);Sca3 (2%， 113);Sca7 (0.5%， 28);Sca6 (0.1%， 05);SCA17(0.1%， 05)和FRDA(2.2%， 127)。在每个位点上观察到大量的TRE长度变异性，我们注意到存在双等位基因扩增，sca亚型共发生，以及存在不可变的正常等位基因。健康对照中GAA-FRDA等位基因突变的频率为1/158(0.63%)，因此FRDA的预期患病率为1:10万人。本研究的数据不仅对临床决策有指导意义，而且对遗传调查方向、基因型跨代比较有指导意义，最后为罕见病类别下考虑SCAs的政策决策提供参考。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Advanced genetics (Hoboken, N.J.)

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