Recently, an intronic biallelic (AAGGG)(n) repeat expansion in RFC1 was shown to be a cause of CANVAS and adult-onset ataxia in multiple populations. As the prevalence of the RFC1 repeat expansion in Dutch cases was unknown, we retrospectively tested 9 putative CANVAS cases and two independent cohorts (A and B) of 395 and 222 adult-onset ataxia cases, respectively, using the previously published protocol and, for the first time optical genome mapping to determine the size of the expanded RFC1 repeat. We identified the biallelic (AAGGG)(n) repeat expansion in 5/9 (55%) putative CANVAS patients and in 10/617 (1.6%; cohorts Aâ+âB) adult-onset ataxia patients. In addition to the AAGGG repeat motif, we observed a putative GAAGG repeat motif in the repeat expansion with unknown significance in two adult-onset ataxia patients. All the expanded (AAGGG)(n) repeats identified were in the range of 800-1299 repeat units. The intronic biallelic RFC1 repeat expansion thus explains a number of the Dutch adult-onset ataxia cases that display the main clinical features of CANVAS, and particularly when ataxia is combined with neuropathy. The yield of screening for RFC1 expansions in unselected cohorts is relatively low. To increase the current diagnostic yield in ataxia patients, we suggest adding RFC1 screening to the genetic diagnostic workflow by using advanced techniques that attain long fragments.
Prevalence of intronic repeat expansions in RFC1 in Dutch patients with CANVAS and adult-onset ataxia.
荷兰 CANVAS 和成人发病共济失调患者中 RFC1 内含子重复扩增的患病率
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作者:Ghorbani Fatemeh, de Boer-Bergsma Jelkje, Verschuuren-Bemelmans Corien C, Pennings Maartje, de Boer Eddy N, Kremer Berry, Vanhoutte Els K, de Vries Jeroen J, van de Berg Raymond, Kamsteeg Erik-Jan, van Diemen Cleo C, Westers Helga, van de Warrenburg Bart P, Verbeek Dineke S
| 期刊: | Journal of Neurology | 影响因子: | 4.600 |
| 时间: | 2022 | 起止号: | 2022 Nov;269(11):6086-6093 |
| doi: | 10.1007/s00415-022-11275-9 | 研究方向: | 其它 |
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