Unusual familial cystic kidney disease: combining fine radiologic and genetic evaluation to solve the case.

IF 2.2 4区 医学 Q2 UROLOGY & NEPHROLOGY BMC Nephrology Pub Date : 2024-09-30 DOI:10.1186/s12882-024-03747-z
Auteurs Sylvain Bodard, Rim Nabbout, Olivier Hélénon, Bertrand Knebelmann
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Abstract

Background: Autosomal dominant polycystic kidney disease (ADPKD) is the most prevalent hereditary kidney disease, characterized by enlarged kidneys with numerous cysts, high blood pressure, and a variety of extrarenal complications. This disease is a significant cause of renal failure and requires accurate differentiation from other cystic kidney diseases, especially when family history does not clearly indicate ADPKD. This is crucial due to differences in prognosis, treatment, and familial implications. Advanced molecular genetics and imaging techniques are employed to diagnose and assess the prognosis of patients and their families.

Case presentation: The case study revolves around three patients from the same family-two sisters and one daughter-referred to a nephrology department for ADPKD management. The initial proband, a 42-year-old woman, experienced abdominal discomfort leading to an ultrasound that suggested ADPKD. However, MRI findings indicated standard-sized kidneys with bilateral parapelvic cysts, and no genetic markers for ADPKD were found. Her sister, presenting with controlled hypertension and similar ultrasound findings, also had her initial ADPKD diagnosis refuted by MRI and genetic testing, which revealed no significant mutations. The daughter, however, exhibited a different scenario with enlarged kidneys and multiple cysts characteristic of early-stage ADPKD. Genetic testing confirmed a deleterious PKD1 mutation, suggesting a de novo mutation, as her father showed no signs of the disease.

Conclusion: This study highlights the complexity and necessity of thorough diagnostic processes in suspected ADPKD cases to prevent misdiagnosis. The initial symptoms and imaging might misleadingly suggest ADPKD, as seen in the cases of the two older patients. Still, further detailed imaging and genetic analyses revealed no ADPKD, preventing inappropriate treatment and stress. In contrast, the younger patient's distinctive clinical and genetic profile confirmed ADPKD, illustrating the variability within even closely related individuals. Such detailed assessments are crucial in guiding correct treatment decisions and providing accurate familial counseling, emphasizing the importance of considering a broader spectrum of renal cystic disorders before confirming a diagnosis of ADPKD.

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异常家族性囊性肾病:结合精细放射学和遗传学评估解决病例。
背景:常染色体显性多囊肾(ADPKD)是最常见的遗传性肾病,其特点是肾脏增大并伴有大量囊肿、高血压和各种肾外并发症。这种疾病是导致肾功能衰竭的重要原因,需要与其他囊性肾脏疾病进行准确鉴别,尤其是当家族病史不能明确显示 ADPKD 时。由于预后、治疗和家族影响方面的差异,这一点至关重要。我们采用先进的分子遗传学和成像技术来诊断和评估患者及其家属的预后:本病例研究围绕来自同一家庭的三名患者展开--两姐妹和一个女儿,他们被转诊到肾内科接受 ADPKD 治疗。最初的原发性患者是一名 42 岁的女性,因腹部不适而接受超声波检查,结果显示她患有 ADPKD。然而,核磁共振成像结果显示肾脏大小正常,双侧肾盂旁有囊肿,而且没有发现 ADPKD 的遗传标记。她的姐姐患有高血压,超声检查结果与她相似,但核磁共振成像和基因检测也没有发现明显的突变,从而推翻了她最初的 ADPKD 诊断。然而,她的女儿却表现出不同的情况,肾脏增大,并出现早期 ADPKD 特征性的多发性囊肿。基因检测证实了一种有害的 PKD1 基因突变,这表明这是一种新发基因突变,因为她的父亲没有任何患病迹象:本研究强调了对疑似 ADPKD 病例进行彻底诊断以防止误诊的复杂性和必要性。最初的症状和影像学检查可能会误导性地提示 ADPKD,两位年长患者的病例就是如此。不过,进一步的详细影像学和基因分析显示并没有 ADPKD,从而避免了不恰当的治疗和压力。与此相反,年轻患者独特的临床和遗传特征证实了 ADPKD,这说明即使是亲缘关系很近的个体也存在变异。这种详细的评估对于指导正确的治疗决策和提供准确的家族咨询至关重要,强调了在确诊 ADPKD 之前考虑更广泛的肾囊性疾病的重要性。
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来源期刊
BMC Nephrology
BMC Nephrology UROLOGY & NEPHROLOGY-
CiteScore
4.30
自引率
0.00%
发文量
375
审稿时长
3-8 weeks
期刊介绍: BMC Nephrology is an open access journal publishing original peer-reviewed research articles in all aspects of the prevention, diagnosis and management of kidney and associated disorders, as well as related molecular genetics, pathophysiology, and epidemiology.
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