The diagnostic accuracy of ultrasound and genomic tests for the diagnosis of autosomal-dominant polycystic kidney disease: a systematic mapping review.

IF 4.6 2区医学 Q1 UROLOGY & NEPHROLOGY

Clinical Kidney Journal Pub Date : 2025-06-13 eCollection Date: 2025-07-01 DOI:10.1093/ckj/sfaf187

Sue Harnan, Matthew Gittus, Louise Falzon, Miranda Durkie, Olena Mandrik, Albert C Ong, James Fotheringham

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Abstract

Background: Genomic and ultrasound tests can provide diagnostic and prognostic information on autosomal-dominant polycystic kidney disease (ADPKD), and can screen first-degree relatives in whom early diagnosis can be advantageous. We conducted a systematic mapping review on test accuracy and characteristics over time.

Methods: Medline, Embase, and Cochrane were searched (August 2023) for studies in first-degree relatives/individuals clinically diagnosed with ADPKD receiving genomic or ultrasound tests. Acceptable reference standards for sensitivity/detection rate and specificity were definitive imaging or genomic confirmation. Genomic studies were categorized by technology and read length. Relationships between sensitivity, specificity, genomic technology, diagnostic criteria/reference standard, and genes tested were compared.

Results: From 1029 non-duplicate titles retrieved, 51 genomic and 7 ultrasound studies were included. There were no genomic studies in first-degree relatives. Among studies in patients with clinical diagnoses, genomic sequencing methodologies were highly heterogeneous [next generation (short read (n = 20), long read (n = 1)), targeted Sanger (n = 19), whole exome (n = 1) with additional multi-ligation probe analysis (n = 13)]. Median sensitivity was 78% (Interquartile range 65% to 88%). Ultrasound sensitivity and specificity generally improved with age and were worse in PKD2 patients compared to PKD1 (lowest reported 31% and 88%, respectively, in polycystic kidney disease (PKD) 2 patients aged 5-14; highest 100% and 100%, respectively, in multiple gene/age categories).

Conclusions: Despite technological advances, sensitivity of genomic tests appeared static between 2000 and 2023. Possible explanations include clinical diagnostic criteria (and hence populations recruited) widening from PKD1 to include PKD2 and atypical phenotypes, and small incremental gains of testing genes other than PKD1 and PKD2. For people at risk of ADPKD in genetically unresolved families, the accuracy of ultrasound is uncertain. Unified genomic test taxonomies would facilitate future reviews. Registration: PROSPERO CRD42023456727.

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超声和基因组检测诊断常染色体显性多囊肾病的准确性：一项系统的制图回顾。

背景：基因组和超声检查可以提供常染色体显性多囊肾病（ADPKD）的诊断和预后信息，并可以筛选一级亲属，早期诊断可能有利。随着时间的推移，我们对测试的准确性和特性进行了系统的映射审查。方法：检索Medline， Embase和Cochrane（2023年8月），查找一级亲属/临床诊断为ADPKD的个体接受基因组或超声检查的研究。灵敏度/检出率和特异性的可接受参考标准是明确的影像学或基因组确认。基因组研究按技术和阅读长度进行分类。比较敏感性、特异性、基因组技术、诊断标准/参考标准、检测基因之间的关系。结果：从检索到的1029篇非重复论文中，包括51篇基因组研究和7篇超声研究。没有一级亲属的基因组研究。在临床诊断患者的研究中，基因组测序方法具有高度异质性[下一代（短读（n = 20），长读（n = 1）），靶向Sanger (n = 19)，全外显子组（n = 1），外加多连接探针分析（n = 13）]。中位敏感性为78%（四分位数范围为65%至88%）。超声敏感性和特异性一般随着年龄的增长而提高，PKD2患者比PKD1患者更差(5-14岁多囊肾病（PKD） 2患者报道最低分别为31%和88%；在多个基因/年龄类别中分别最高为100%和100%)。结论：尽管技术进步，但基因组检测的敏感性在2000年至2023年间保持不变。可能的解释包括临床诊断标准（因此招募的人群）从PKD1扩大到包括PKD2和非典型表型，以及检测PKD1和PKD2以外的基因的小增量收益。对于遗传未解决的家族中有ADPKD风险的人，超声波的准确性是不确定的。统一的基因组测试分类将有助于未来的审查。注册：普洛斯彼罗CRD42023456727。

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来源期刊

Clinical Kidney Journal Medicine-Transplantation

CiteScore

6.70

自引率

10.90%

发文量

242

审稿时长

8 weeks

期刊介绍： About the Journal Clinical Kidney Journal: Clinical and Translational Nephrology (ckj), an official journal of the ERA-EDTA (European Renal Association-European Dialysis and Transplant Association), is a fully open access, online only journal publishing bimonthly. The journal is an essential educational and training resource integrating clinical, translational and educational research into clinical practice. ckj aims to contribute to a translational research culture among nephrologists and kidney pathologists that helps close the gap between basic researchers and practicing clinicians and promote sorely needed innovation in the Nephrology field. All research articles in this journal have undergone peer review.