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Practice Guideline
Clinical Practice Guideline: Microhematuria in Children and Young Adults—Evaluation for the Early Detection of Kidney Disease.
- Kay Latta, Jan Boeckhaus, Ina Weinreich, Angela Borisch, Dominik Müller, and Oliver Gross.
- Responsible scientific societies: German Society for Pediatric Nephrology GPN, Berlin, and German Society for Nephrology DGfN, Berlin; Clementine Pediatric Hospital, Frankfurt; Department of Pediatric Gastroenterology, Nephrology and Metabolic Diseases, Charité - Berlin University of Medicine, Berlin; Department of Nephrology and Rheumatology, University Medical Center Göttingen.
- Dtsch Arztebl Int. 2024 Jul 12; 121 (14): 461466461-466.
BackgroundOccult blood in the urine, or microhematuria, is a common finding (about 10%) in children and young adults. It is often of brief duration and therefore harmless. In persistent microhematuria, acanthocytes in the urine are a frequently unrecognized early marker of glomerular kidney disease. The purpose of this guideline is to promote the early detection of kidney disease in children and young adults with practical, evidence-based recommendations.MethodsA systematic search for pertinent publications up to January 2023 was conducted in Pubmed, the Cochrane Database, and Livivo. 474 publications were retrieved, summarized in terms of method and content, and classified by Oxford (2011) evidence level.ResultsApproximately 1% of children and young adults have undiagnosed chronic kidney disease. Microhematuria is an early warning sign. A timely nephrological evaluation is indicated if microhematuria persists for 3 to 6 months, if ≥ 5% acanthocytes are detectable in the urine, and if there is also proteinuria, hypertension, or impaired renal function. Ultrasonography of the kidneys and urinary tract is the imaging method of choice; cystoscopy should be avoided. For patients with glomerular microhematuria, molecular genetic testing is recommended. Renal biopsy is recommended in case of florid glomerular diseases, after the determination of various laboratory param eters and clinical findings, including molecular genet ic testing especially in children.ConclusionIn the absence of a guideline until now, findings have often been incorrectly assessed, leading either to an inadequate work-up or to excessive diagnostics. As a result, in approximately 30% of young patients, valuable opportunities for early treatment to protect the kidneys have been missed.
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