Abstract

Tartrate-resistant acid phosphatase, isoform 5b (TRACP-5b) is a bone resorption marker not influenced by renal function or food intake. TRACP-5b can be measured with Nittobo Medical enzymatic-immunoassay and IDS-iSYS automated immunoassay. We evaluated the Nittobo assay and established reference ranges for a Western-European population. We compared Nittobo and IDS results in different well-defined clinical populations. We established the limits of detection and quantification (LOD-LOQ), linearity, imprecision and the reference ranges in 119 males, 50 women (<45 years) and 120 women (>60 years) for TRACP-5b with the Nittobo assay. We compared both assays in 30 hemodialyzed (HD), and 40 stage 3-5 patients suffering from chronic kidney disease (CKD), 40 patients suffering from rheumatoid arthritis andosteoporosis and 80 post-menopausal women. We measured TRACP-5b, β-crosslaps (β-CTX), bone alkaline phosphatase (B-ALP) and PTH in 20 hemodialyzed (HD) and 40 CKD patients. LOD and LOQ were 0.02 and 0.35 U/L. CV ranged from 8.3 to 4.3% (2/5 samples presenting CV>desirable CV). Method was linear up to of 11.3 U/L. Upper and lower limits of normality were 0.8-7.6 U/L in men, 0.9-4.7 U/L in women <45 and 0.9-7.1 U/L in women >60. The regression equation between the 2 methods was Nittobo=1.13 (95% CI: 1.09-1.16)×iSYS-0.4 (95% CI:-0.5;-0.3). TRACP-5b and b-ALP were in their respective reference ranges for most of CKD and HD patients. That was not the case for β-CTX, which increased with decreasing eGFR. Nittobo TRACP-5b presents interesting analytical features and a good concordance with IDS iSYS. These methods could thus potentially be harmonized.

Highlights

  • Tartrate-resistant acid phosphatase (TRACP) is an enzyme produced by the ACP5 gene [1] which possesses a dimetal center comprised of two Fe ions in its active center [2]

  • We established the limits of detection and quantification (LOD-LOQ), linearity, imprecision and the reference ranges in 119 males, 50 women (60 years) for TRACP-5b with the Nittobo assay

  • TRACP-5a concentrations are increased in inflammatory pathologies like rheumatoid arthritis whereas TRACP-5b is secreted by the osteoclasts as an active enzyme and reflects bone resorption and the number of active osteoclasts [5, 6]

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Summary

Introduction

Tartrate-resistant acid phosphatase (TRACP) is an enzyme produced by the ACP5 gene [1] which possesses a dimetal center comprised of two Fe ions in its active center [2]. TRACP is expressed by various cells from monocyte/macrophage lineage like osteoclasts, activated macrophages or dendritic cells [3]. Two isoforms of TRACP, namely 5a and 5b are present in human serum [4]. TRACP-5a concentrations are increased in inflammatory pathologies like rheumatoid arthritis whereas TRACP-5b is secreted by the osteoclasts as an active enzyme and reflects bone resorption and the number of active osteoclasts [5, 6]. After release in the circulation, TRACP-5b becomes inactive by losing its iron content and degraded into fragments that are cleared by the liver [7]. Less than 10% of the circulating TRACP-5b circulates as an intact enzymatically active form [8]

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