Evaluation of pathogenicity of WT1 intron variants by in vitro splicing analysis.

IF 2.2 4区医学 Q2 UROLOGY & NEPHROLOGY

Clinical and Experimental Nephrology Pub Date : 2024-11-01 Epub Date: 2024-06-14 DOI:10.1007/s10157-024-02510-w

Seiya Inoue, Atsushi Kondo, Yuta Inoki, Yuta Ichikawa, Yu Tanaka, Chika Ueda, Hideaki Kitakado, Ryota Suzuki, Eri Okada, Nana Sakakibara, Tomoko Horinouchi, Kandai Nozu

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引用次数: 0

Abstract

Background: Wilms tumor 1 (WT1; NM_024426) causes Denys-Drash syndrome, Frasier syndrome, or isolated focal segmental glomerulosclerosis. Several WT1 intron variants are pathogenic; however, the pathogenicity of some variants remains undefined. Whether a candidate variant detected in a patient is pathogenic is very important for determining the therapeutic options for the patient.

Methods: In this study, we evaluated the pathogenicity of WT1 gene intron variants with undetermined pathogenicity by comparing their splicing patterns with those of the wild-type using an in vitro splicing assay using minigenes. The three variants registered as likely disease-causing genes: Mut1 (c.1017-9 T > C(IVS5)), Mut2 (c.1355-28C > T(IVS8)), Mut3 (c.1447 + 1G > C(IVS9)), were included as subjects along the 34 splicing variants registered in the Human Gene Mutation Database (HGMD)^®.

Results: The results showed no significant differences in splicing patterns between Mut1 or Mut2 and the wild-type; however, significant differences were observed in Mut3.

Conclusion: We concluded that Mut1 and Mut2 do not possess pathogenicity although they were registered as likely pathogenic, whereas Mut3 exhibits pathogenicity. Our results suggest that the pathogenicity of intronic variants detected in patients should be carefully evaluated.

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通过体外剪接分析评估 WT1 内含子变体的致病性。

背景：Wilms tumor 1（WT1；NM_024426）可导致 Denys-Drash 综合征、Frasier 综合征或孤立性局灶节段性肾小球硬化症。有几种 WT1 内含子变异具有致病性，但有些变异的致病性仍未确定。患者体内检测到的候选变体是否致病，对于确定患者的治疗方案非常重要：在这项研究中，我们通过使用迷你基因的体外剪接试验，比较了 WT1 基因内含子变异体与野生型的剪接模式，从而评估了致病性未定的 WT1 基因内含子变异体的致病性。这三个变体可能是致病基因：Mut1（c.1017-9 T > C(IVS5)）、Mut2（c.1355-28C > T(IVS8)）、Mut3（c.1447 + 1G > C(IVS9)）与人类基因突变数据库（HGMD）®中登记的 34 个剪接变体一起被列为研究对象：结果表明，Mut1 或 Mut2 与野生型的剪接模式无明显差异；但在 Mut3 中观察到明显差异：我们得出结论：Mut1 和 Mut2 虽然被登记为可能致病，但不具有致病性，而 Mut3 则具有致病性。我们的结果表明，应仔细评估在患者体内检测到的内含子变异体的致病性。

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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来源期刊

Clinical and Experimental Nephrology UROLOGY & NEPHROLOGY-

CiteScore

4.10

自引率

4.30%

发文量

135

审稿时长

4-8 weeks

期刊介绍： Clinical and Experimental Nephrology is a peer-reviewed monthly journal, officially published by the Japanese Society of Nephrology (JSN) to provide an international forum for the discussion of research and issues relating to the study of nephrology. Out of respect for the founders of the JSN, the title of this journal uses the term “nephrology,” a word created and brought into use with the establishment of the JSN (Japanese Journal of Nephrology, Vol. 2, No. 1, 1960). The journal publishes articles on all aspects of nephrology, including basic, experimental, and clinical research, so as to share the latest research findings and ideas not only with members of the JSN, but with all researchers who wish to contribute to a better understanding of recent advances in nephrology. The journal is unique in that it introduces to an international readership original reports from Japan and also the clinical standards discussed and agreed by JSN.