Clinical risk assessment of biotin interference with a high-sensitivity cardiac troponin T assay

Bryn Mumma; Deborah Diercks; Raphael Twerenbold; André Valcour; André Ziegler; André Schützenmeister; Dusanka Kasapic; Nam Tran

doi:10.1515/cclm-2019-0962

Clinical risk assessment of biotin interference with a high-sensitivity cardiac troponin T assay

Standard

Clinical risk assessment of biotin interference with a high-sensitivity cardiac troponin T assay. / Mumma, Bryn; Diercks, Deborah; Twerenbold, Raphael; Valcour, André; Ziegler, André; Schützenmeister, André; Kasapic, Dusanka; Tran, Nam.

In: CLIN CHEM LAB MED, Vol. 58, No. 11, 25.10.2020, p. 1931-1940.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Mumma, B, Diercks, D, Twerenbold, R, Valcour, A, Ziegler, A, Schützenmeister, A, Kasapic, D & Tran, N 2020, 'Clinical risk assessment of biotin interference with a high-sensitivity cardiac troponin T assay', CLIN CHEM LAB MED, vol. 58, no. 11, pp. 1931-1940. https://doi.org/10.1515/cclm-2019-0962

APA

Mumma, B., Diercks, D., Twerenbold, R., Valcour, A., Ziegler, A., Schützenmeister, A., Kasapic, D., & Tran, N. (2020). Clinical risk assessment of biotin interference with a high-sensitivity cardiac troponin T assay. CLIN CHEM LAB MED, 58(11), 1931-1940. https://doi.org/10.1515/cclm-2019-0962

Vancouver

Mumma B, Diercks D, Twerenbold R, Valcour A, Ziegler A, Schützenmeister A et al. Clinical risk assessment of biotin interference with a high-sensitivity cardiac troponin T assay. CLIN CHEM LAB MED. 2020 Oct 25;58(11):1931-1940. https://doi.org/10.1515/cclm-2019-0962

Bibtex

@article{848cd801340f414a961cea71b79c5c46,

title = "Clinical risk assessment of biotin interference with a high-sensitivity cardiac troponin T assay",

abstract = "Objectives Biotin >20.0 ng/mL (81.8 nmol/L) can reduce Elecsys{\textregistered} Troponin T Gen 5 (TnT Gen 5; Roche Diagnostics) assay recovery, potentially leading to false-negative results in patients with suspected acute myocardial infarction (AMI). We aimed to determine the prevalence of elevated biotin and AMI misclassification risk from biotin interference with the TnT Gen 5 assay. Methods Biotin was measured using an Elecsys assay in two cohorts: (i) 797 0-h and 646 3-h samples from 850 US emergency department patients with suspected acute coronary syndrome (ACS); (ii) 2023 random samples from a US laboratory network, in which biotin distributions were extrapolated for higher values using pharmacokinetic modeling. Biotin >20.0 ng/mL (81.8 nmol/L) prevalence and biotin 99th percentile values were calculated. AMI misclassification risk due to biotin interference with the TnT Gen 5 assay was modeled using different assay cutoffs and test timepoints. Results ACS cohort: 1/797 (0.13%) 0-h and 1/646 (0.15%) 3-h samples had biotin >20.0 ng/mL (81.8 nmol/L); 99th percentile biotin was 2.62 ng/mL (10.7 nmol/L; 0-h) and 2.38 ng/mL (9.74 nmol/L; 3-h). Using conservative assumptions, the likelihood of false-negative AMI prediction due to biotin interference was 0.026% (0-h result; 19 ng/L TnT Gen 5 assay cutoff). US laboratory cohort: 15/2023 (0.74%) samples had biotin >20.0 ng/mL (81.8 nmol/L); 99th percentile biotin was 16.6 ng/mL (68.0 nmol/L). Misclassification risk due to biotin interference (19 ng/L TnT Gen 5 assay cutoff) was 0.025% (0-h), 0.0064% (1-h), 0.00048% (3-h), and <0.00001% (6-h). Conclusions Biotin interference has minimal impact on the TnT Gen 5 assay's clinical utility, and the likelihood of false-negative AMI prediction is extremely low.",

keywords = "Acute Coronary Syndrome/diagnosis, Biomarkers/blood, Biotin/blood, Cohort Studies, Diagnostic Tests, Routine, False Negative Reactions, Female, Humans, Immunoassay, Immunologic Tests, Male, Middle Aged, Myocardial Infarction/diagnosis, Risk Assessment, Troponin T/blood",

author = "Bryn Mumma and Deborah Diercks and Raphael Twerenbold and Andr{\'e} Valcour and Andr{\'e} Ziegler and Andr{\'e} Sch{\"u}tzenmeister and Dusanka Kasapic and Nam Tran",

year = "2020",

month = oct,

day = "25",

doi = "10.1515/cclm-2019-0962",

language = "English",

volume = "58",

pages = "1931--1940",

journal = "CLIN CHEM LAB MED",

issn = "1434-6621",

publisher = "Walter de Gruyter GmbH & Co. KG",

number = "11",

}

RIS

TY - JOUR

T1 - Clinical risk assessment of biotin interference with a high-sensitivity cardiac troponin T assay

AU - Mumma, Bryn

AU - Diercks, Deborah

AU - Twerenbold, Raphael

AU - Valcour, André

AU - Ziegler, André

AU - Schützenmeister, André

AU - Kasapic, Dusanka

AU - Tran, Nam

PY - 2020/10/25

Y1 - 2020/10/25

N2 - Objectives Biotin >20.0 ng/mL (81.8 nmol/L) can reduce Elecsys® Troponin T Gen 5 (TnT Gen 5; Roche Diagnostics) assay recovery, potentially leading to false-negative results in patients with suspected acute myocardial infarction (AMI). We aimed to determine the prevalence of elevated biotin and AMI misclassification risk from biotin interference with the TnT Gen 5 assay. Methods Biotin was measured using an Elecsys assay in two cohorts: (i) 797 0-h and 646 3-h samples from 850 US emergency department patients with suspected acute coronary syndrome (ACS); (ii) 2023 random samples from a US laboratory network, in which biotin distributions were extrapolated for higher values using pharmacokinetic modeling. Biotin >20.0 ng/mL (81.8 nmol/L) prevalence and biotin 99th percentile values were calculated. AMI misclassification risk due to biotin interference with the TnT Gen 5 assay was modeled using different assay cutoffs and test timepoints. Results ACS cohort: 1/797 (0.13%) 0-h and 1/646 (0.15%) 3-h samples had biotin >20.0 ng/mL (81.8 nmol/L); 99th percentile biotin was 2.62 ng/mL (10.7 nmol/L; 0-h) and 2.38 ng/mL (9.74 nmol/L; 3-h). Using conservative assumptions, the likelihood of false-negative AMI prediction due to biotin interference was 0.026% (0-h result; 19 ng/L TnT Gen 5 assay cutoff). US laboratory cohort: 15/2023 (0.74%) samples had biotin >20.0 ng/mL (81.8 nmol/L); 99th percentile biotin was 16.6 ng/mL (68.0 nmol/L). Misclassification risk due to biotin interference (19 ng/L TnT Gen 5 assay cutoff) was 0.025% (0-h), 0.0064% (1-h), 0.00048% (3-h), and <0.00001% (6-h). Conclusions Biotin interference has minimal impact on the TnT Gen 5 assay's clinical utility, and the likelihood of false-negative AMI prediction is extremely low.

AB - Objectives Biotin >20.0 ng/mL (81.8 nmol/L) can reduce Elecsys® Troponin T Gen 5 (TnT Gen 5; Roche Diagnostics) assay recovery, potentially leading to false-negative results in patients with suspected acute myocardial infarction (AMI). We aimed to determine the prevalence of elevated biotin and AMI misclassification risk from biotin interference with the TnT Gen 5 assay. Methods Biotin was measured using an Elecsys assay in two cohorts: (i) 797 0-h and 646 3-h samples from 850 US emergency department patients with suspected acute coronary syndrome (ACS); (ii) 2023 random samples from a US laboratory network, in which biotin distributions were extrapolated for higher values using pharmacokinetic modeling. Biotin >20.0 ng/mL (81.8 nmol/L) prevalence and biotin 99th percentile values were calculated. AMI misclassification risk due to biotin interference with the TnT Gen 5 assay was modeled using different assay cutoffs and test timepoints. Results ACS cohort: 1/797 (0.13%) 0-h and 1/646 (0.15%) 3-h samples had biotin >20.0 ng/mL (81.8 nmol/L); 99th percentile biotin was 2.62 ng/mL (10.7 nmol/L; 0-h) and 2.38 ng/mL (9.74 nmol/L; 3-h). Using conservative assumptions, the likelihood of false-negative AMI prediction due to biotin interference was 0.026% (0-h result; 19 ng/L TnT Gen 5 assay cutoff). US laboratory cohort: 15/2023 (0.74%) samples had biotin >20.0 ng/mL (81.8 nmol/L); 99th percentile biotin was 16.6 ng/mL (68.0 nmol/L). Misclassification risk due to biotin interference (19 ng/L TnT Gen 5 assay cutoff) was 0.025% (0-h), 0.0064% (1-h), 0.00048% (3-h), and <0.00001% (6-h). Conclusions Biotin interference has minimal impact on the TnT Gen 5 assay's clinical utility, and the likelihood of false-negative AMI prediction is extremely low.

KW - Acute Coronary Syndrome/diagnosis

KW - Biomarkers/blood

KW - Biotin/blood

KW - Cohort Studies

KW - Diagnostic Tests, Routine

KW - False Negative Reactions

KW - Female

KW - Humans

KW - Immunoassay

KW - Immunologic Tests

KW - Male

KW - Middle Aged

KW - Myocardial Infarction/diagnosis

KW - Risk Assessment

KW - Troponin T/blood

U2 - 10.1515/cclm-2019-0962

DO - 10.1515/cclm-2019-0962

M3 - SCORING: Journal article

C2 - 32804676

VL - 58

SP - 1931

EP - 1940

JO - CLIN CHEM LAB MED

JF - CLIN CHEM LAB MED

SN - 1434-6621

IS - 11

ER -