在孤立性蛋白尿患者中发现 CUBN 的新型致病变体。

IF 1.5 4区医学 Q4 GENETICS & HEREDITY Molecular Genetics & Genomic Medicine Pub Date : 2024-03-01 DOI:10.1002/mgg3.2353

Huihui Yang, Lanfen He, Hongjian Gong, Chunhui Wan, Juanjuan Ding, Panli Liao, Xiaowen Wang

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引用次数: 0

摘要

背景：尽管长期以来，蛋白尿一直被认为是进展性慢性肾脏疾病的独立风险因素，但并非所有形式的蛋白尿都会损害肾功能，其中之一就是由cubilin（CUBN）特异性突变引起的孤立性蛋白尿。CUBN 编码一种内细胞受体，最初被发现是 Imerslund-Gräsbeck 综合征（IGS；OMIM #261100）的病因，其特征是巨幼细胞贫血和蛋白尿的综合表型：在分析了他们的临床和病理特征后，对四名非进行性孤立性蛋白尿患者进行了肾脏疾病基因的新一代测序或全外显子组测序（WES）。通过cDNA-PCR测序、免疫组织化学、迷你基因检测以及包括三维蛋白质建模在内的多种硅学预测工具，鉴定并进一步分析了CUBN双侧致病变体：结果：我们在此报告了四例由 CUBN C 端双倍性致病变体引起的孤立性蛋白尿患者，他们均无典型的 IGS 症状，如贫血和维生素 B12 缺乏。他们的尿蛋白水平在+~++之间波动，估计肾小球滤过率（eGFR）正常或稍高。在三名儿童的肾活检中发现了轻度间质细胞增生。通过 cDNA 测序和免疫组化，证实 CUBN 的一个同源杂合位点变异（c.6821+3 (IVS44) A>G）导致第 44 号外显子跳转和翻译过早终止。在另外三名患儿中发现了复合杂合突变，其中包括另一个新的剪接位点变异（c.10764+1 (IVS66) G>A），该变异导致内含子 66 中前 4 个核苷酸的保留（通过微型基因检测）；两个未报告的错义突变（c.4907G>A (p.R1636Q); c. 9095 A>G (p.Y3032C)），以及在中国报道的两个错义突变（c.8938G>A (p.D2980N); c. 9287T>C (p.L3096P)），位于维生素 B12 结合结构域的后面，分别影响 CUB11、CUB16、CUB22、CUB23 和 CUB27 结构域：这些结果表明，上述 CUBN 突变可导致非进行性和孤立性蛋白尿，从而扩大了 CUBN 的变异谱，有利于我们了解蛋白尿和肾功能。

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Identification of novel pathogenic variants of CUBN in patients with isolated proteinuria.

Background: Although proteinuria is long recognized as an independent risk factor for progressive chronic kidney diseases, not all forms of proteinuria are detrimental to kidney function, one of which is isolated proteinuria caused by cubilin (CUBN)-specific mutations. CUBN encodes an endocytic receptor, initially found to be responsible for the Imerslund-Gräsbeck syndrome (IGS; OMIM #261100) characterized by a combined phenotype of megaloblastic anemia and proteinuria.

Methods: After analyzing their clinical and pathological characterizations, next-generation sequencing for renal disease genes or whole-exome sequencing (WES) was performed on four patients with non-progressive isolated proteinuria. CUBN biallelic pathogenic variants were identified and further analyzed by cDNA-PCR sequencing, immunohistochemistry, minigene assay, and multiple in silico prediction tools, including 3D protein modeling.

Results: Here, we present four patients with isolated proteinuria caused by CUBN C-terminal biallelic pathogenic variants, all of which showed no typical IGS symptoms, such as anemia and vitamin B12 deficiency. Their urine protein levels fluctuated between +~++ and estimated glomerular filtration rate (eGFR) were normal or slightly higher. Mild mesangial hypercellularity was found in three children's renal biopsies. A homozygous splice-site variant of CUBN (c.6821+3 (IVS44) A>G) was proven to result in the exon 44 skipping and premature translation termination by cDNA sequencing and immunohistochemistry. Compound heterozygous mutations were identified among the other three children, including another novel splice-site variant (c.10764+1 (IVS66) G>A) causing the retention of first 4 nucleotides in intron 66 by minigene assay, two unreported missense mutations (c.4907G>A (p.R1636Q); c. 9095 A>G (p.Y3032C)), and two reported missense mutations in China (c.8938G>A (p.D2980N); c. 9287T>C (p.L3096P)), locating behind the vitamin B12-binding domain, affecting CUB11, CUB16, CUB22, CUB23, and CUB27 domains, respectively.

Conclusion: These results demonstrate that above CUBN mutations may cause non-progressive and isolated proteinuria, expanding the variant spectrum of CUBN and benefiting our understanding of proteinuria and renal function.

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来源期刊

Molecular Genetics & Genomic Medicine Biochemistry, Genetics and Molecular Biology-Genetics

CiteScore

4.20

自引率

0.00%

发文量

241

审稿时长

14 weeks

期刊介绍： Molecular Genetics & Genomic Medicine is a peer-reviewed journal for rapid dissemination of quality research related to the dynamically developing areas of human, molecular and medical genetics. The journal publishes original research articles covering findings in phenotypic, molecular, biological, and genomic aspects of genomic variation, inherited disorders and birth defects. The broad publishing spectrum of Molecular Genetics & Genomic Medicine includes rare and common disorders from diagnosis to treatment. Examples of appropriate articles include reports of novel disease genes, functional studies of genetic variants, in-depth genotype-phenotype studies, genomic analysis of inherited disorders, molecular diagnostic methods, medical bioinformatics, ethical, legal, and social implications (ELSI), and approaches to clinical diagnosis. Molecular Genetics & Genomic Medicine provides a scientific home for next generation sequencing studies of rare and common disorders, which will make research in this fascinating area easily and rapidly accessible to the scientific community. This will serve as the basis for translating next generation sequencing studies into individualized diagnostics and therapeutics, for day-to-day medical care. Molecular Genetics & Genomic Medicine publishes original research articles, reviews, and research methods papers, along with invited editorials and commentaries. Original research papers must report well-conducted research with conclusions supported by the data presented.