A novel point-of-care device accurately measures thyrotropin in whole blood, capillary blood and serum

Author:

Kahaly George J.1,Lotz Johannes2,Walder Sara1,Hammad Cara1,Krämer Rebecca1,Frommer Lara1,König Jochem3,Wolf Jan1,Gottwald-Hostalek Ulrike4,Urgatz Bogumila4,Lackner Karl J.2

Affiliation:

1. Molecular Thyroid Research Laboratory, Department of Medicine I , Johannes Gutenberg University (JGU) Medical Center , Mainz , Germany

2. Institute for Clinical Chemistry and Laboratory Medicine , Johannes Gutenberg University (JGU) Medical Center , Mainz , Germany

3. Institute of Medical Biostatistics, Epidemiology and Informatics , Johannes Gutenberg University (JGU) Medical Center , Mainz , Germany

4. Merck Healthcare KGaA , Darmstadt , Germany

Abstract

Abstract Objectives Point-of-care (POC) measurement of thyrotropin (TSH) may facilitate prompt diagnosis of thyroid dysfunction. We evaluated the analytical performance of a new POC TSH assay (Wondfo). Methods TSH measurements were made from 730 consecutive, unselected subjects in an outpatient setting, using Wondfo in whole blood, capillary blood and serum or automated reference equipment (serum only). Results TSH measurements were user-independent. Total intra-and inter-assay variation (CV%) was 12.1 and 16.2%, respectively. Total CV% was 10.6–22.6% and 14.5–21.6% in serum and whole blood, respectively. Linearity was very good. Recovery rate was 97–127%. Prolongation of incubation time increased TSH results of 12% (13%) and 33% (35%) after 2 and 5 additional minutes in serum (blood), respectively. When measured simultaneously in two Wondfo devices, the slope of the regression line was 1.03 (serum) and 1.02 (blood), with Spearman’s correlation of 0.99 for both. TSH measurements between Wondfo and reference correlated strongly (r=0.93–0.96), though TSH measurements were lower with Wondfo (slopes of plots of measurements made using the two devices were 0.94 [serum vs. serum]; 0.83 [whole blood vs. serum] and 0.64 [capillary blood vs. serum]). Depending on sample material, TSH in capillary blood was lower vs. whole blood (slope: 0.82) and for whole blood vs. serum (Wondfo and reference method; slope: 0.69 and 0.83). Total haemolysis, but not elevated bilirubin or lipemia, disrupted TSH measurement. Conclusions The Wondfo system was straightforward to use without need for specialist technicians and demonstrated analytic performance suitable for clinical use for the diagnosis of thyroid dysfunction.

Publisher

Walter de Gruyter GmbH

Subject

Biochemistry (medical),Clinical Biochemistry,General Medicine

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