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Composition of kidney stone fragments obtained after extracorporeal shock wave lithotripsy

  • Silvia Fernandes Ribeiro da Silva , Sônia Leite da Silva , Elizabeth De Francesco Daher , Henry de Holanda Campos and Carlos Antônio Bruno da Silva
Published/Copyright: February 1, 2010
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Clinical Chemistry and Laboratory Medicine
From the journal Clinical Chemistry and Laboratory Medicine Volume 48 Issue 3

Abstract

Background: The objective of this study was to determine the composition of kidney stone fragments obtained after extracorporeal shock wave lithotripsy (ESWL).

Methods: Kidney stone fragments from 25 patients with urolithiasis treated with ESWL were submitted for morphological analysis. The composition was determined for all the recovered fragments.

Results: Thirteen patients (52%) had pure stones. The most common type of pure stone was calcium oxalate (61.6%), of which half was the monohydrate type (COM) and half was the dihydrate type (COD). The other pure stones consisted of either uric acid (30.8%) or struvite (7.6%). For mixed stones, the most frequently observed component was COM or COD (50%), followed by a mixture of COD and carbapatite (25.1%).

Conclusions: Our findings indicate that the composition of kidney stone fragments recovered after ESWL can be determined. Knowledge of stone composition is fundamental to understand the etiology of lithogenesis.

Clin Chem Lab Med 2010;48:403–4.

Keywords: calcium oxalate; composition; lithotripsy; stone morphology
Corresponding author: Carlos Antâonio Bruno da Silva, Av. Washington Soares 1321, Edson Queiroz, 60811-905, Fortaleza, Ceara, Brazil Phone: +55 85 32 81 58 10,
Received: 2009-7-14
Accepted: 2009-11-11
Published Online: 2010-02-1
Published in Print: 2010-03-01

©2010 by Walter de Gruyter Berlin New York

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https://doi.org/10.1515/CCLM.2010.079
Keywords for this article
calcium oxalate; composition; lithotripsy; stone morphology

Articles in the same Issue

  1. Editorial
  2. Standardization of assays for clinically important enzymes that have high biologic variation: what is all the fuss about?
  3. Minireview
  4. Standardization in clinical enzymology: a challenge for the theory of metrological traceability
  5. Review
  6. Laboratory reporting of hemostasis assays: the final post-analytical opportunity to reduce errors of clinical diagnosis in hemostasis?
  7. Opinion Paper
  8. The underestimated problem of using serum magnesium measurements to exclude magnesium deficiency in adults; a health warning is needed for “normal” results
  9. Genetics and Molecular Diagnostics
  10. Integrated PCR amplification and detection processes on a Lab-on-Chip platform: a new advanced solution for molecular diagnostics
  11. Matrix metalloproteinase-7 (MMP-7) polymorphism is a risk factor for endometrial cancer susceptibility
  12. Association of the CD28/CTLA4/ICOS polymorphisms with susceptibility to rheumatoid arthritis
  13. Lack of association between DAZ gene methylation patterns and spermatogenic failure
  14. General Clinical Chemistry and Laboratory Medicine
  15. Evaluation of five routine glucose methods on an Olympus AU5400 analyzer using the CDC hexokinase reference method
  16. Multicentre evaluation of the Tosoh HbA1c G8 analyser
  17. Performance of a fully automated quantitative neopterin measurement assay in a routine voluntary blood donation setting
  18. Assay of oxidized fibrinogen reactivity (OFR) as a biomarker of oxidative stress in human plasma: the role of lysine analogs
  19. Decrease in uric acid in acute ischemic stroke correlates with stroke severity, evolution and outcome
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  21. Is heparin plasma suitable for the determination of B-type natriuretic peptide on the Beckman-Coulter Access 2?
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  30. Tissue factor +5466A>G and –1208D>I genetic polymorphisms and severity of rheumatoid arthritis
  31. Ability of deferasirox to bind iron during measurement of iron
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