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1. T Cell Responses Correlate with Self-Reported Disease Severity and Neutralizing Antibody Responses Predict Protection against SARS-CoV-2 Breakthrough Infection

Author

Zhao, Zhen, Kumanovics, Attila, Love, Tanzy, Melanson, Stacy EF, Meng, Qing H, Wu, Alan HB, Wiencek, Joesph, Apple, Fred S, Ondracek, Caitlin R, Koch, David D, Christenson, Robert H, and Zhang, Yan Victoria

Subjects
Microbiology, Biological Sciences, Infectious Diseases, Biodefense, Vaccine Related, Prevention, Biotechnology, Immunization, Emerging Infectious Diseases, Clinical Research, Prevention of disease and conditions, and promotion of well-being, 3.4 Vaccines, Infection, Good Health and Well Being, Humans, COVID-19 Vaccines, COVID-19, SARS-CoV-2, Self Report, Breakthrough Infections, Prospective Studies, Patient Acuity, Antibodies, Neutralizing, Vaccination, Antibodies, Viral, vaccine, T cell response, neutralizing antibody, breakthrough infection
Abstract

ObjectivesThe objective of this prospective study was to investigate the role of adaptive immunity in response to SARS-CoV-2 vaccines.Design and methodsA cohort of 677 vaccinated individuals participated in a comprehensive survey of their vaccination status and associated side effects, and donated blood to evaluate their adaptive immune responses by neutralizing antibody (NAb) and T cell responses. The cohort then completed a follow-up survey to investigate the occurrence of breakthrough infections.ResultsNAb levels were the highest in participants vaccinated with Moderna, followed by Pfizer and Johnson & Johnson. NAb levels decreased with time after vaccination with Pfizer and Johnson & Johnson. T cell responses showed no significant difference among the different vaccines and remained stable up to 10 months after the study period for all vaccine types. In multivariate analyses, NAb responses (

Published
2023

2. Diagnostic accuracy of a machine learning algorithm using point-of-care high-sensitivity cardiac troponin I for rapid rule-out of myocardial infarction: a retrospective study

Author

Stephensen, Laura, Brownlee, Emily, McCormick, Ellyse, Fincher, Gavin, Hall, Emma J., Hancock, Rebecca, Gaikwad, Niranjan, Gangathimmaiah, Vinay, Hamilton-Craig, Christian, Hobbins-King, Andrew, Keijzers, Gerben, Bayat, Maryam Khorramshahi, Mahmoodi, Ehsan, Perez, Siegfried, Ranasinghe, Isuru, Staib, Andrew, Zournazi, Anna, Than, Martin, Toprak, Betül, Solleder, Hugo, Di Carluccio, Eleonora, Greenslade, Jaimi H, Parsonage, William A, Schulz, Karen, Cullen, Louise, Apple, Fred S, Ziegler, Andreas, and Blankenberg, Stefan

Published
2024
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3. Personalized diagnosis in suspected myocardial infarction

Author

Neumann, Johannes Tobias, Twerenbold, Raphael, Ojeda, Francisco, Aldous, Sally J., Allen, Brandon R., Apple, Fred S., Babel, Hugo, Christenson, Robert H., Cullen, Louise, Di Carluccio, Eleonora, Doudesis, Dimitrios, Ekelund, Ulf, Giannitsis, Evangelos, Greenslade, Jaimi, Inoue, Kenji, Jernberg, Tomas, Kavsak, Peter, Keller, Till, Lee, Kuan Ken, Lindahl, Bertil, Lorenz, Thiess, Mahler, Simon A., Mills, Nicholas L., Mokhtari, Arash, Parsonage, William, Pickering, John W., Pemberton, Christopher J., Reich, Christoph, Richards, A. Mark, Sandoval, Yader, Than, Martin P., Toprak, Betül, Troughton, Richard W., Worster, Andrew, Zeller, Tanja, Ziegler, Andreas, and Blankenberg, Stefan

Published
2023
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4. Uniform or Sex-Specific Cardiac Troponin Thresholds to Rule Out Myocardial Infarction at Presentation

Author

Mills, Nicholas L., Strachan, Fiona E., Tuck, Christopher, Anand, Atul, Akinlade, Olawale Mathias, Barker, Stephanie, Blades, Jennifer, Boeddinghaus, Jasper, Bularga, Anda, de Bakker, Marie, Chapman, Andrew R., Doudesis, Dimitrios, Ferry, Amy V., Fujisawa, Takeshi, Georgiev, Konstantin, Kimenai, Dorien M., Lee, Kuan Ken, Lyell, Iona, Li, Ziwen, Lowry, Matthew TH., McKinlay, Lynn, McDermott, Michael, McPherson, Jean, Mendusic, Filip, Sorbie, Andrew, Souter, Grace, Schulberg, Stacey D., Taggart, Caelan, Thurston, Alexander JF., Tew, Yong Yong, Perez-Vicencio, Daniel, Wang, Yiqing, Wereski, Ryan, Williams, Kelly, Newby, David E., Fox, Keith AA., Berry, Colin, Walker, Simon, Weir, Christopher J., Ford, Ian, Gray, Alasdair, Collinson, Paul O., Apple, Fred S., Reid, Alan, Cruikshank, Anne, Findlay, Iain, Amoils, Shannon, McAllister, David A., Maguire, Donogh, Stevens, Jennifer, Norrie, John, Shah, Anoop SV., Andrews, Jack PM., Adamson, Philip D., Moss, Alastair, Anwar, Mohamed S., Hung, John, Malo, Jonathan, Fischbacher, Colin M., Croal, Bernard L., Leslie, Stephen J., Keerie, Catriona, Parker, Richard A., Walker, Allan, Harkess, Ronnie, Wackett, Tony, Weir, Christopher, Armstrong, Roma, Stirling, Laura, MacDonald, Claire, Sadat, Imran, Finlay, Frank, Harrison, Kathy, Linksted, Pamela, Lavenberg, Stephen, Lowry, Matthew T.H., Tuck, Chris, and Shah, Anoop S.V.

Published
2024
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5. Machine learning for diagnosis of myocardial infarction using cardiac troponin concentrations

Author

Doudesis, Dimitrios, Lee, Kuan Ken, Boeddinghaus, Jasper, Bularga, Anda, Ferry, Amy V., Tuck, Chris, Lowry, Matthew T. H., Lopez-Ayala, Pedro, Nestelberger, Thomas, Koechlin, Luca, Bernabeu, Miguel O., Neubeck, Lis, Anand, Atul, Schulz, Karen, Apple, Fred S., Parsonage, William, Greenslade, Jaimi H., Cullen, Louise, Pickering, John W., Than, Martin P., Gray, Alasdair, Mueller, Christian, and Mills, Nicholas L.

Published
2023
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8. High-sensitivity cardiac troponin and the diagnosis of myocardial infarction in patients with kidney impairment

Author

Mills, Nicholas L., Strachan, Fiona E., Tuck, Christopher, Shah, Anoop S.V., Anand, Atul, Bularga, Anda, Wereski, Ryan, Lowry, Matthew T.H., Taggart, Caelan, Ferry, Amy V., Lee, Kuan Ken, Chapman, Andrew R., Sandeman, Dennis, Adamson, Philip D., Stables, Catherine L., Vallejos, Catalina A., Tsanas, Athanasios, Marshall, Lucy, Stewart, Stacey D., Fujisawa, Takeshi, McPherson, Jean, McKinlay, Lynn, Newby, David E., Fox, Keith A.A., Berry, Colin, Walker, Simon, Weir, Christopher J., Ford, Ian, Gray, Alasdair, Collinson, Paul O., Apple, Fred S., Reid, Alan, Cruikshank, Anne, Findlay, Iain, Amoils, Shannon, McAllister, David A., Maguire, Donogh, Stevens, Jennifer, Norrie, John, Andrews, Jack P.M., Moss, Alastair, Anwar, Mohamed S., Hung, John, Malo, Jonathan, Fischbacher, Colin M., Croal, Bernard L., Leslie, Stephen J., Keerie, Catriona, Parker, Richard A., Walker, Allan, Harkess, Ronnie, Wackett, Tony, Weir, Christopher, Armstrong, Roma, Stirling, Laura, MacDonald, Claire, Sadat, Imran, Finlay, Frank, Charles, Heather, Linksted, Pamela, Young, Stephen, Alexander, Bill, Duncan, Chris, Gallacher, Peter J., Miller-Hodges, Eve, Farrah, Tariq E., Halbesma, Nynke, Blackmur, James P., Cruickshank, Anne, and Dhaun, Neeraj

Published
2022
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10. Validation of the myocardial-ischaemic-injury-index machine learning algorithm to guide the diagnosis of myocardial infarction in a heterogenous population: a prespecified exploratory analysis

Author

Mills, Nicholas L, Strachan, Fiona E, Tuck, Christopher, Shah, Anoop SV, Anand, Atul, Chapman, Andrew R, Ferry, Amy V, Lee, Kuan Ken, Doudesis, Dimitrios, Bularga, Anda, Wereski, Ryan, Taggart, Caelan, Lowry, Matthew TH, Mendusic, Filip, Kimenai, Dorien M, Sandeman, Dennis, Adamson, Philip D, Stables, Catherine L, Vallejos, Catalina A, Tsanas, Athanasios, Marshall, Lucy, Stewart, Stacey D, Fujisawa, Takeshi, Hautvast, Mischa, McPherson, Jean, McKinlay, Lynn, Ford, Ian, Newby, David E, Fox, Keith AA, Berry, Colin, Walker, Simon, Weir, Christopher J, Gray, Alasdair, Collinson, Paul O, Apple, Fred S, Reid, Alan, Cruikshank, Anne, Findlay, Iain, Amoils, Shannon, McAllister, David A, Maguire, Donogh, Stevens, Jennifer, Norrie, John, Andrews, Jack PM, Moss, Alastair, Anwar, Mohamed S, Hung, John, Malo, Jonathan, Fischbacher, Colin, Croal, Bernard L, Leslie, Stephen J, Keerie, Catriona, Parker, Richard A, Walker, Allan, Harkess, Ronnie, Wackett, Tony, Armstrong, Roma, Stirling, Laura, MacDonald, Claire, Sadat, Imran, Finlay, Frank, Charles, Heather, Linksted, Pamela, Young, Stephen, Alexander, Bill, Duncan, Chris, Yang, Jason, Shah, Anoop S V, Pickering, John W, and Than, Martin P

Published
2022
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11. Analytical validation of the Mindray CL1200i analyzer high sensitivity cardiac troponin I assay: MERITnI study.

Author

Fabre-Estremera, Blanca, Schulz, Karen, Ladd, Alanna, Sexter, Anne, and Apple, Fred S.

Subjects
TROPONIN I, CREATINE kinase, TROPONIN, DETECTION limit, TROPOMYOSINS
Abstract

This study performed an analytical validation study of the Mindray high-sensitivity cardiac troponin I (hs-cTnI) assay addressing limit of blank (LoB), limit of detection (LoD), precision, linearity, analytical specificity and sex-specific 99th percentile upper reference limits. LoB, LoD, precision, linearity and analytical specificity were studied according to Clinical and Laboratory Standards Institute. We used one reagent lot and one CL1200i analyzer. Skeletal troponin I and T, cardiac troponin T, troponin C, actin, tropomyosin, myosin light chain, myoglobin and creatine kinase (CK-MB) were studied for cross-reactivity. Interference with biotin was examined. Lithium heparin samples (one freeze thaw cycle) from healthy males and females were measured to determine the 99th percentiles by using the non-parametric method. Analyses were performed before and after excluding subjects with clinical conditions and/or increased surrogate biomarkers. The Mindray hs-cTnI assay met criteria to be considered as a hs-cTn assay. LoB and LoD was <0.1 ng/L and 0.1 ng/L, respectively. Repeatability had a coefficient of variation 1.2–3.8 %, and within-laboratory imprecision 1.7–5.0 %. The measuring interval ranged from 1.1 to 28,180 ng/L. The analytical specificity was clinically acceptable for the interferents studied. After exclusions, the 99th percentile URLs obtained were 10 ng/L overall, 5 ng/L for females and 12 ng/L for males. Analytical observations of the Mindray hs-cTnI assay demonstrated excellent LoB, LoD, precision, linearity and analytical specificity, that were in alignment with the manufacturer's claims and regulatory guidelines for hs-cTnI. The assay is suitable for clinical investigation for patient-oriented studies. [ABSTRACT FROM AUTHOR]

Published
2024
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12. Multicenter assessment of a hemoglobin A1c point-of-care device for diagnosis of diabetes mellitus

Author

Sobolesky, Philip M, Smith, Breland E, Saenger, Amy K, Schulz, Karen, Apple, Fred S, Scott, Mitchell G, Wu, Alan HB, Little, Randie R, and Fitzgerald, Robert L

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Diabetes, Management of diseases and conditions, 7.1 Individual care needs, Good Health and Well Being, Device Approval, Diabetes Mellitus, Type 1, Diabetes Mellitus, Type 2, Glycated Hemoglobin, Humans, Materials Testing, Point-of-Care Testing, Reproducibility of Results, United States, United States Food and Drug Administration, HbA1c, Point-of-care, NGSP, Medical Biochemistry and Metabolomics, General Clinical Medicine, Clinical sciences, Medical biochemistry and metabolomics
Abstract

ObjectiveA multisite investigation compared the analytical performance of a point-of-care (POC) HbA1c device with multiple commonly used HbA1c laboratory methods and an NGSP (National Glycohemoglobin Standardization Program) reference method.Research design and methodsThe Afinion AS100 POC device analyzed HbA1c using 618 EDTA whole blood excess patient specimens with clinically indicated HbA1c testing. Results were compared to measurements across five clinical laboratories and the NGSP reference method. Precision was evaluated over 8-10 consecutive days for low-, mid-, and high-range HbA1c specimens at all five sites.ResultsOver a wide range of HbA1c values (4.0%-15% HbA1c), 97.1% of the POC results and 94.5% of routine laboratory results fell within the target value of ±6% of the NGSP reference method results. The POC HbA1c results at 6.5% exhibited a total relative bias of -0.6% (-0.04% HbA1c) compared to the reference method while the aggregate of laboratory methods displayed a relative bias of -0.9% (-0.06% HbA1c). The total imprecision of the POC results ranged from 0.74-2.13% CV across the analytic measurement range compared to 0.81-3.23% CV for the routine laboratory methods.ConclusionsThe accuracy and precision of the Afinion POC HbA1c method was comparable to the laboratory HbA1c methods supporting the FDA's recent approval of the Afinion HbA1c Dx device for use in the diagnosis of diabetes.

Published
2018

14. Uniform or Sex-Specific Cardiac Troponin Thresholds to Rule Out Myocardial Infarction at Presentation

Author

Li, Ziwen, primary, Wereski, Ryan, additional, Anand, Atul, additional, Lowry, Matthew T.H., additional, Doudesis, Dimitrios, additional, McDermott, Michael, additional, Ferry, Amy V., additional, Tuck, Chris, additional, Chapman, Andrew R., additional, Lee, Kuan Ken, additional, Shah, Anoop S.V., additional, Mills, Nicholas L., additional, Kimenai, Dorien M., additional, Strachan, Fiona E., additional, Tuck, Christopher, additional, Akinlade, Olawale Mathias, additional, Barker, Stephanie, additional, Blades, Jennifer, additional, Boeddinghaus, Jasper, additional, Bularga, Anda, additional, de Bakker, Marie, additional, Fujisawa, Takeshi, additional, Georgiev, Konstantin, additional, Lyell, Iona, additional, Li, Ziwen, additional, Lowry, Matthew TH., additional, McKinlay, Lynn, additional, McPherson, Jean, additional, Mendusic, Filip, additional, Sorbie, Andrew, additional, Souter, Grace, additional, Schulberg, Stacey D., additional, Taggart, Caelan, additional, Thurston, Alexander JF., additional, Tew, Yong Yong, additional, Perez-Vicencio, Daniel, additional, Wang, Yiqing, additional, Williams, Kelly, additional, Newby, David E., additional, Fox, Keith AA., additional, Berry, Colin, additional, Walker, Simon, additional, Weir, Christopher J., additional, Ford, Ian, additional, Gray, Alasdair, additional, Collinson, Paul O., additional, Apple, Fred S., additional, Reid, Alan, additional, Cruikshank, Anne, additional, Findlay, Iain, additional, Amoils, Shannon, additional, McAllister, David A., additional, Maguire, Donogh, additional, Stevens, Jennifer, additional, Norrie, John, additional, Shah, Anoop SV., additional, Andrews, Jack PM., additional, Adamson, Philip D., additional, Moss, Alastair, additional, Anwar, Mohamed S., additional, Hung, John, additional, Malo, Jonathan, additional, Fischbacher, Colin M., additional, Croal, Bernard L., additional, Leslie, Stephen J., additional, Keerie, Catriona, additional, Parker, Richard A., additional, Walker, Allan, additional, Harkess, Ronnie, additional, Wackett, Tony, additional, Weir, Christopher, additional, Armstrong, Roma, additional, Stirling, Laura, additional, MacDonald, Claire, additional, Sadat, Imran, additional, Finlay, Frank, additional, Harrison, Kathy, additional, Linksted, Pamela, additional, and Lavenberg, Stephen, additional

Published
2024
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17. Diagnostic accuracy of a machine learning algorithm using point-of-care high-sensitivity cardiac troponin I for rapid rule-out of myocardial infarction: a retrospective study

Author

Toprak, Betül, Solleder, Hugo, Di Carluccio, Eleonora, Greenslade, Jaimi H, Parsonage, William A, Schulz, Karen, Cullen, Louise, Apple, Fred S, Ziegler, Andreas, Blankenberg, Stefan, Stephensen, Laura, Brownlee, Emily, McCormick, Ellyse, Fincher, Gavin, Hall, Emma J., Hancock, Rebecca, Gaikwad, Niranjan, Gangathimmaiah, Vinay, Hamilton-Craig, Christian, Hobbins-King, Andrew, Keijzers, Gerben, Bayat, Maryam Khorramshahi, Mahmoodi, Ehsan, Perez, Siegfried, Ranasinghe, Isuru, Staib, Andrew, Zournazi, Anna, and Than, Martin

Abstract

Point-of-care (POC) high-sensitivity cardiac troponin (hs-cTn) assays have been shown to provide similar analytical precision despite substantially shorter turnaround times compared with laboratory-based hs-cTn assays. We applied the previously developed machine learning based personalised Artificial Intelligence in Suspected Myocardial Infarction Study (ARTEMIS) algorithm, which can predict the individual probability of myocardial infarction, with a single POC hs-cTn measurement, and compared its diagnostic performance with standard-of-care pathways for rapid rule-out of myocardial infarction.

Published
2024
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18. Single High-Sensitivity Point-of-Care Whole-Blood Cardiac Troponin I Measurement to Rule Out Acute Myocardial Infarction at Low Risk

Author

Apple, Fred S., Smith, Stephen W., Greenslade, Jaimi H., Sandoval, Yader, Parsonage, William, Ranasinghe, Isuru, Gaikwad, Niranjan, Schulz, Karen, Stephensen, Laura, Schmidt, Christian W., Okeson, Brynn, Cullen, Louise, Brownlee, Emily, Fincher, Gavin, Hall, Emma, Hancock, Rebecca, Gangathimmaiah, Vinay, Hamilton-Craig, Christian, Hobbins-King, Andrew, Keijzers, Gerben, Bayat, Maryam Khorramshahi, McCormick, Ellyse, Mahmoodi, Ehsan, Perez, Siegfried, Staib, Andrew, Zournazi, Anna, and Than, Martin

Published
2022
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21. Point-of-care high-sensitivity cardiac troponin in suspected acute myocardial infarction assessed at baseline and 2 h.

Author

Cullen, Louise, Greenslade, Jaimi, Parsonage, William, Stephensen, Laura, Smith, Stephen W, Sandoval, Yader, Ranasinghe, Isuru, Gaikwad, Niranjan, Bayat, Maryam Khorramshahi, Mahmoodi, Ehsan, Schulz, Karen, Than, Martin, Apple, Fred S, and investigators, SAMIE and SEIGE

Subjects
MYOCARDIAL infarction, TROPONIN, TROPONIN I, POINT-of-care testing
Abstract

Background and Aims Strategies to assess patients with suspected acute myocardial infarction (AMI) using a point-of-care (POC) high-sensitivity cardiac troponin I (hs-cTnI) assay may expedite emergency care. A 2-h POC hs-cTnI strategy for emergency patients with suspected AMI was derived and validated. Methods In two international, multi-centre, prospective, observational studies of adult emergency patients (1486 derivation cohort and 1796 validation cohort) with suspected AMI, hs-cTnI (Siemens Atellica® VTLi) was measured at admission and 2 h later. Adjudicated final diagnoses utilized the hs-cTn assay in clinical use. A risk stratification algorithm was derived and validated. The primary diagnostic outcome was index AMI (Types 1 and 2). The primary safety outcome was 30-day major adverse cardiac events incorporating AMI and cardiac death. Results Overall, 81 (5.5%) and 88 (4.9%) patients in the derivation and validation cohorts, respectively, had AMI. The 2-h algorithm defined 66.1% as low risk with a sensitivity of 98.8% [95% confidence interval (CI) 89.3%–99.9%] and a negative predictive value of 99.9 (95% CI 99.2%–100%) for index AMI in the derivation cohort. In the validation cohort, 53.3% were low risk with a sensitivity of 98.9% (95% CI 92.4%–99.8%) and a negative predictive value of 99.9% (95% CI 99.3%–100%) for index AMI. The high-risk metrics identified 5.4% of patients with a specificity of 98.5% (95% CI 96.6%–99.4%) and a positive predictive value of 74.5% (95% CI 62.7%–83.6%) for index AMI. Conclusions A 2-h algorithm using a POC hs-cTnI concentration enables safe and efficient risk assessment of patients with suspected AMI. The short turnaround time of POC testing may support significant efficiencies in the management of the large proportion of emergency patients with suspected AMI. [ABSTRACT FROM AUTHOR]

Published
2024
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22. Prognosis is worse with elevated cardiac troponin in nonacute coronary syndrome compared with acute coronary syndrome

Author

Horiuchi, Yu, Wettersten, Nicholas, Patel, Mitul P., Mueller, Christian, Neath, Sean-Xavier, Christenson, Robert H., Morgenthaler, Nils G., McCord, James, Nowak, Richard M., Vilke, Gary M., Daniels, Lori B., Hollander, Judd E., Apple, Fred S., Cannon, Chad M., Nagurney, John T., Schreiber, Donald, deFilippi, Christopher, Hogan, Christopher, Diercks, Deborah B., Headden, Gary, Limkakeng, Alexander T., Jr., Anand, Inder, Wu, Alan H.B., Ebmeyer, Stefan, Jaffe, Allan S., Peacock, W. Frank, and Maisel, Alan

Published
2022
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24. Performance of Three Anti-SARS-CoV-2 Anti-S and One Anti-N Immunoassays for the Monitoring of Immune Status and Vaccine Response

Author

Zhang, Y. Victoria, primary, Kumanovics, Attila, additional, Wiencek, Joesph, additional, Melanson, Stacy E. F., additional, Love, Tanzy, additional, Wu, Alan H. B., additional, Zhao, Zhen, additional, Meng, Qing H., additional, Koch, David D., additional, Apple, Fred S., additional, Ondracek, Caitlin R., additional, and Christenson, Robert H., additional

Published
2024
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25. Midregional Proadrenomedullin Predicts Mortality and Major Adverse Cardiac Events in Patients Presenting With Chest Pain: Results From the CHOPIN Trial

Author

Shah, Kevin S, Marston, Nicholas A, Mueller, Christian, Neath, Sean-Xavier, Christenson, Robert H, McCord, James, Nowak, Richard M, Vilke, Gary M, Daniels, Lori B, Hollander, Judd E, Apple, Fred S, Cannon, Chad M, Nagurney, John, Schreiber, Donald, deFilippi, Christopher, Hogan, Christopher J, Diercks, Deborah B, Limkakeng, Alexander, Anand, Inder S, Wu, Alan HB, Clopton, Paul, Jaffe, Allan S, Peacock, W Frank, and Maisel, Alan S

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Atherosclerosis, Patient Safety, Heart Disease - Coronary Heart Disease, Clinical Research, Pain Research, Clinical Trials and Supportive Activities, Cardiovascular, Chronic Pain, Heart Disease, 4.2 Evaluation of markers and technologies, Detection, screening and diagnosis, Good Health and Well Being, Acute Disease, Adrenomedullin, Aged, Biomarkers, Chest Pain, Emergency Service, Hospital, Female, Heart Failure, Humans, Hydroxymethylglutaryl-CoA Reductase Inhibitors, Male, Middle Aged, Pravastatin, Predictive Value of Tests, Prognosis, Prospective Studies, Protein Precursors, Risk Assessment, Risk Factors, Severity of Illness Index, Public Health and Health Services, Emergency & Critical Care Medicine, Clinical sciences
Abstract

ObjectivesChest pain is a common complaint to emergency departments (EDs) and clinical risk factors are used to predict which patients are at risk for worse outcomes and mortality. The goal was to assess the novel biomarker midregional proadrenomedullin (MR-proADM) in prediction of mortality and major adverse cardiac events (MACE).MethodsThis was a subanalysis of the CHOPIN study, a 16-center prospective trial that enrolled 2,071 patients presenting with chest pain within 6 hours of onset. The primary endpoint was 6-month all-cause mortality and the secondary endpoint was 30-day and 6-month MACE: ED visits or hospitalization for acute myocardial infarction, unstable angina, reinfarction, revascularization, and heart failure.ResultsMR-proADM performed similarly to troponin (cTnI; c-statistic = 0.845 and 0.794, respectively) for mortality prediction in all subjects and had similar results in those with noncardiac diagnoses. MR-proADM concentrations were stratified by decile, and the cohort in the top decile had a 9.8% 6-month mortality risk versus 0.9% risk for those in the bottom nine deciles (p

Published
2015

26. Sex-Specific Thresholds of High-Sensitivity Troponin in Patients With Suspected Acute Coronary Syndrome

Author

Mills, Nicholas L., Strachan, Fiona E., Tuck, Christopher, Shah, Anoop S.V., Anand, Atul, Ferry, Amy V., Lee, Kuan Ken, Chapman, Andrew R., Sandeman, Dennis, Adamson, Philip D., Stables, Catherine L., Vallejo, Catalina A., Tsanasis, Athanasios, Marshall, Lucy, Stewart, Stacey D., Fujisawa, Takeshi, Hautvast, Mischa, McPherson, Jean, McKinlay, Lynn, Newby, David E., Fox, Keith A.A., Berry, Colin, Walker, Simon, Weir, Christopher J., Ford, Ian, Gray, Alasdair, Collinson, Paul O., Apple, Fred S., Reid, Alan, Cruikshank, Anne, Findlay, Iain, Amoils, Shannon, McAllister, David A., Maguire, Donogh, Stevens, Jennifer, Norrie, John, Weir, Christopher, Andrews, Jack P.M., Moss, Alastair, Anwar, Mohamed S., Hung, John, Malo, Jonathan, Fischbacher, Colin M., Croal, Bernard L., Leslie, Stephen J., Keerie, Catriona, Parker, Richard A., Walker, Allan, Harkess, Ronnie, Wackett, Tony, Armstrong, Roma, Flood, Marion, Stirling, Laura, MacDonald, Claire, Sadat, Imran, Finlay, Frank, Charles, Heather, Linksted, Pamela, Young, Stephen, Alexander, Bill, Duncan, Chris, Kimenai, Dorien M., Meex, Steven J.R., Cruickshank, Anne, and Tuck, Chris

Published
2019
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31. Derivation and Validation of Thresholds Using Synthetic Data Methods for Single-Test Screening of Emergency Department Patients with Possible Acute Myocardial Infarction Using a Point-of-Care Troponin Assay.

Author

Pickering, John W, Young, Joanna M, George, Peter M, Watson, Antony S, Aldous, Sally J, Verryt, Toby, Troughton, Richard W, Pemberton, Christopher J, Richards, A Mark, Cullen, Louise A, Apple, Fred S, and Than, Martin P

Subjects
MYOCARDIAL infarction, MEDICAL screening, HOSPITAL emergency services, PLASMA products, TROPONIN
Abstract

Background: Single-sample (screening) rule-out of acute myocardial infarction (AMI) with troponin requires derivation of a single-test screening threshold. In data sets with small event numbers, the lowest one or two concentrations of myocardial infarction (MI) patients dictate the threshold. This is not optimal. We aimed to demonstrate a process incorporating both real and synthetic data for deriving such thresholds using a novel pre-production high-precision point-of-care assay. Methods: cTnI concentrations were measured from thawed plasma using the Troponin I Next (TnI-Nx) assay (i-STAT; Abbott) in adults on arrival to the emergency department with symptoms suggestive of AMI. The primary outcome was an AMI or cardiac death within 30 days. We used internal–external validation with synthetic data production based on clinical and demographic data, plus the measured TnI-Nx concentration, to derive and validate decision thresholds for TnI-Nx. The target low-risk threshold was a sensitivity of 99% and a high-risk threshold specificity of >95%. Results: In total, 1356 patients were included, of whom 191 (14.1%) had the primary outcome. A total of 500 synthetic data sets were constructed. The mean low-risk threshold was determined to be 5 ng/L. This categorized 38% (95% CI, 6%–68%) to low-risk with a sensitivity of 99.0% (95% CI, 98.6%–99.5%) and a negative predictive value of 99.4% (95% CI, 97.6%–99.8%). A similarly derived high-risk threshold of 25 ng/L had a specificity of 95.0% (95% CI, 94.8%–95.1%) and a positive predictive value of 74.8% (95% CI, 71.5%–78.0%). Conclusions: With the TnI-Nx assay, we successfully demonstrated an approach using synthetic data generation to derive low-risk thresholds for safe and effective screening. [ABSTRACT FROM AUTHOR]

Published
2024
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32. Large-Scale Scientific Study Led by a Professional Organization during the COVID-19 Pandemic: Operations, Best Practices, and Lessons Learned

Author

Ondracek, Caitlin R, primary, Melanson, Stacy E F, additional, Doan, Loretta, additional, Schulz, Karen M, additional, Kleinman, Stefanie, additional, Zhao, Zhen, additional, Kumanovics, Attila, additional, Wu, Alan H B, additional, Wiencek, Joesph, additional, Meng, Qing H, additional, Apple, Fred S, additional, Koch, David, additional, Vesper, Hubert, additional, Pokuah, Fidelia, additional, Bryksin, Janetta, additional, Myers, Gary L, additional, Christenson, Robert H, additional, and Zhang, Y Victoria, additional

Published
2023
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34. Single Troponin Measurement to Rule Out Myocardial Infarction

Author

Jaffe, Allan S., primary, Body, Richard, additional, Mills, Nicholas L., additional, Aakre, Kristin M., additional, Collinson, Paul O., additional, Saenger, Amy, additional, Hammarsten, Ole, additional, Wereski, Ryan, additional, Omland, Torbjørn, additional, Sandoval, Yader, additional, Ordonez-Llanos, Jordi, additional, and Apple, Fred S., additional

Published
2023
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41. Large-Scale Scientific Study Led by a Professional Organization during the COVID-19 Pandemic: Operations, Best Practices, and Lessons Learned.

Author

Ondracek, Caitlin R, Melanson, Stacy E F, Doan, Loretta, Schulz, Karen M, Kleinman, Stefanie, Zhao, Zhen, Kumanovics, Attila, Wu, Alan H B, Wiencek, Joesph, Meng, Qing H, Apple, Fred S, Koch, David, Vesper, Hubert, Pokuah, Fidelia, Bryksin, Janetta, Myers, Gary L, Christenson, Robert H, and Zhang, Y Victoria

Subjects
COVID-19 pandemic, BEST practices, PROFESSIONAL associations, BLOOD collection, ASSOCIATION (Chemistry)
Abstract

In 2021, the Association for Diagnostics & Laboratory Medicine (ADLM) (formerly the American Association for Clinical Chemistry [AACC]) developed a scientific study that aimed to contribute to the understanding of SARS-CoV-2 immunity during the evolving course of the pandemic. This study was led by a group of expert member volunteers and resulted in survey data from 975 individuals and blood collection from 698 of those participants. This paper describes the formulation and execution of this large-scale scientific study, encompassing best practices and insights gained throughout the endeavor. [ABSTRACT FROM AUTHOR]

Published
2024
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43. Biomarkers Enhance Discrimination and Prognosis of Type 2 Myocardial Infarction

Author

Horiuchi, Yu, Wettersten, Nicholas, Patel, Mitul P., Mueller, Christian, Neath, Sean-Xavier, Christenson, Robert H., Morgenthaler, Nils G., McCord, James, Nowak, Richard M., Vilke, Gary M., Daniels, Lori B., Hollander, Judd E., Apple, Fred S., Cannon, Chad M., Nagurney, John T., Schreiber, Donald, deFilippi, Christopher, Hogan, Christopher, Diercks, Deborah B., Headden, Gary, Limkakeng, Alexander T., Jr, Anand, Inder, Wu, Alan H.B., Ebmeyer, Stefan, Jaffe, Allan S., Peacock, W. Frank, and Maisel, Alan

Published
2020
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46. Defining myocardial infarction in trials of people receiving hemodialysis: consensus report from the SONG-HD MI Expert Working group

Author

O’Lone, Emma, primary, Apple, Fred S., additional, Burton, James O., additional, Caskey, Fergus J., additional, Craig, Jonathan C., additional, deFilippi, Christopher R., additional, Forfang, Derek, additional, Hicks, Karen A., additional, Jha, Vivekanand, additional, Mahaffey, Kenneth W., additional, Mark, Patrick B., additional, Rossignol, Patrick, additional, Scholes-Robertson, Nicole, additional, Jaure, Allison, additional, Viecelli, Andrea K., additional, Wang, Angela Y., additional, Wheeler, David C., additional, White, David, additional, Winkelmayer, Wolfgang C., additional, and Herzog, Charles A., additional

Published
2023
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47. Antibody-mediated interferences affecting cardiac troponin assays : recommendations from the IFCC Committee on Clinical Applications of Cardiac Biomarkers

Author

Hammarsten, Ola, Warner, Janet V., Lam, Leo, Kavsak, Peter, Lindahl, Bertil, Aakre, Kristin M., Collinson, Paul, Jaffe, Allan S., Saenger, Amy K., Body, Richard, Mills, Nicholas L., Omland, Torbjørn, Ordonez-Llanos, Jordi, Apple, Fred S., Hammarsten, Ola, Warner, Janet V., Lam, Leo, Kavsak, Peter, Lindahl, Bertil, Aakre, Kristin M., Collinson, Paul, Jaffe, Allan S., Saenger, Amy K., Body, Richard, Mills, Nicholas L., Omland, Torbjørn, Ordonez-Llanos, Jordi, and Apple, Fred S.

Abstract

The International Federation of Clinical Chemistry Committee on Clinical Applications of Cardiac Biomarkers (IFCC C-CB) provides educational documents to facilitate the interpretation and use of cardiac biomarkers in clinical laboratories and practice. Our aim is to improve the understanding of certain key analytical and clinical aspects of cardiac biomarkers and how these may interplay. Measurements of cardiac troponin (cTn) have a prominent place in the clinical work-up of patients with suspected acute coronary syndrome. It is therefore important that clinical laboratories know how to recognize and assess analytical issues. Two emerging analytical issues resulting in falsely high cTn concentrations, often several fold higher than the upper reference limit (URL), are antibody-mediated assay interference due to long-lived cTn-antibody complexes, called macrotroponin, and crosslinking antibodies that are frequently referred to as heterophilic antibodies. We provide an overview of antibody-mediated cTn assay interference and provide recommendations on how to confirm the interference and interpret the results.

Published
2023
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