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Published in: Clinical and Experimental Nephrology 2/2008

01-04-2008 | Original Article

Serum levels of cystatin C in patients with malignancy

Authors: Keiko Nakai, Masayuki Kikuchi, Keiko Fujimoto, Yoshito Kaneko, So Omori, Kenji Nakai, Akira Suwabe

Published in: Clinical and Experimental Nephrology | Issue 2/2008

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Abstract

Background

Serum levels of cystatin C have been proposed to be an ideal marker of the glomerular filtration rate (GFR). However, some reports have shown that serum levels of cystatin C increase independently of GFR. In this study, we evaluated the clinical utility of cystatin C in monitoring GFR, especially in patients with a malignancy.

Method

Study subjects consisted of 82 patients with a malignancy, 39 patients with a non-malignancy, 31 healthy volunteers, and 206 patients with various degrees of renal function. We measured serum cystatin C, β2-microglobulin (β2mG), and creatinine (CRE) levels in all patients. Serum CRP levels were measured in 21 patients with a malignancy and 28 patients with a non-malignancy whose creatinine clearance (Ccr) was ≥70 ml/min. Cystatin C, β2mG, and CRP were measured by immune nephelometry and CRE was measured by an enzyme assay.

Results

In patients with a malignancy, regression analysis yielded the equation: 1/cystatin C = 0.06 × Ccr + 0.710, correlation coefficient, r, of 0.33. The r was significantly lower than in patients with various degrees of renal function. There were no significant differences when the r performed on β2mG and CRE was compared between the same groups of patients. In 74 patients with a malignancy, in whom serum CRE levels were ≤1.1 mg/dl, increased levels of cystatin C were observed in 25 patients and increased levels of β2mG were observed in 39 patients. In comparing patients with a malignancy and a non-malignancy, the number of patients with an increased level of cystatin C, despite a Ccr ≥ 70 ml/min (8/33) or a CRE ≤ 1.1 mg/dl (13/41), was larger in the former group than the latter group, although the result was not statistically significant. Similarly, the number of patients with an increased level of β2mG, despite a Ccr ≥ 70 ml/min or a CRE ≤ 1.1 mg/dl was significantly larger in the former group compared to the latter group. Regression analysis between the serum levels of cystatin C and CRP in patients with a malignancy whose Ccr were ≥70 ml/min had a weak correlation (r = 0.31).

Conclusion

The results of our study suggest that the serum levels of cystatin C are not always a reliable marker of the GFR in patients with a malignancy, probably in relation to its nature as a cysteine protease inhibitor.
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Metadata
Title
Serum levels of cystatin C in patients with malignancy
Authors
Keiko Nakai
Masayuki Kikuchi
Keiko Fujimoto
Yoshito Kaneko
So Omori
Kenji Nakai
Akira Suwabe
Publication date
01-04-2008
Publisher
Springer Japan
Published in
Clinical and Experimental Nephrology / Issue 2/2008
Print ISSN: 1342-1751
Electronic ISSN: 1437-7799
DOI
https://doi.org/10.1007/s10157-008-0043-8

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