Cell-free DNA donor fraction analysis in pediatric and adult heart transplant patients by multiplexed allele-specific quantitative PCR: Validation of a rapid and highly sensitive clinical test for stratification of rejection probability

Lifelong noninvasive rejection monitoring in heart transplant patients is a critical clinical need historically poorly met in adults and unavailable for children and infants. Cell-free DNA (cfDNA) donor-specific fraction (DF), a direct marker of selective donor organ injury, is a promising analytica...

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Autores principales: North, Paula E., Ziegler, Emily, Mahnke, Donna K., Stamm, Karl D., Thomm, Angela, Daft, Paul, Goetsch, Mary, Liang, Huan ling, Baker, Maria Angeles, Vepraskas, Adam, Rosenau, Chris, Dasgupta, Mahua, Simpson, Pippa, Mitchell, Michael E., Tomita-Mitchell, Aoy
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2020
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6957190/
https://www.ncbi.nlm.nih.gov/pubmed/31929557
http://dx.doi.org/10.1371/journal.pone.0227385
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author North, Paula E.
Ziegler, Emily
Mahnke, Donna K.
Stamm, Karl D.
Thomm, Angela
Daft, Paul
Goetsch, Mary
Liang, Huan ling
Baker, Maria Angeles
Vepraskas, Adam
Rosenau, Chris
Dasgupta, Mahua
Simpson, Pippa
Mitchell, Michael E.
Tomita-Mitchell, Aoy
author_facet North, Paula E.
Ziegler, Emily
Mahnke, Donna K.
Stamm, Karl D.
Thomm, Angela
Daft, Paul
Goetsch, Mary
Liang, Huan ling
Baker, Maria Angeles
Vepraskas, Adam
Rosenau, Chris
Dasgupta, Mahua
Simpson, Pippa
Mitchell, Michael E.
Tomita-Mitchell, Aoy
author_sort North, Paula E.
collection PubMed
description Lifelong noninvasive rejection monitoring in heart transplant patients is a critical clinical need historically poorly met in adults and unavailable for children and infants. Cell-free DNA (cfDNA) donor-specific fraction (DF), a direct marker of selective donor organ injury, is a promising analytical target. Methodological differences in sample processing and DF determination profoundly affect quality and sensitivity of cfDNA analyses, requiring specialized optimization for low cfDNA levels typical of transplant patients. Using next-generation sequencing, we previously correlated elevated DF with acute cellular and antibody-mediated rejection (ACR and AMR) in pediatric and adult heart transplant patients. However, next-generation sequencing is limited by cost, TAT, and sensitivity, leading us to clinically validate a rapid, highly sensitive, quantitative genotyping test, myTAI(HEART)(®), addressing these limitations. To assure pre-analytical quality and consider interrelated cfDNA measures, plasma preparation was optimized and total cfDNA (TCF) concentration, DNA fragmentation, and DF quantification were validated in parallel for integration into myTAI(HEART) reporting. Analytical validations employed individual and reconstructed mixtures of human blood-derived genomic DNA (gDNA), cfDNA, and gDNA sheared to apoptotic length. Precision, linearity, and limits of blank/detection/quantification were established for TCF concentration, DNA fragmentation ratio, and DF determinations. For DF, multiplexed high-fidelity amplification followed by quantitative genotyping of 94 SNP targets was applied to 1168 samples to evaluate donor options in staged simulations, demonstrating DF call equivalency with/without donor genotype. Clinical validation studies using 158 matched endomyocardial biopsy-plasma pairs from 76 pediatric and adult heart transplant recipients selected a DF cutoff (0.32%) producing 100% NPV for ≥2R ACR. This supports the assay’s conservative intended use of stratifying low versus increased probability of ≥2R ACR. myTAI(HEART) is clinically validated for heart transplant recipients ≥2 months old and ≥8 days post-transplant, expanding opportunity for noninvasive transplant rejection assessment to infants and children and to all recipients >1 week post-transplant.
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spelling pubmed-69571902020-01-26 Cell-free DNA donor fraction analysis in pediatric and adult heart transplant patients by multiplexed allele-specific quantitative PCR: Validation of a rapid and highly sensitive clinical test for stratification of rejection probability North, Paula E. Ziegler, Emily Mahnke, Donna K. Stamm, Karl D. Thomm, Angela Daft, Paul Goetsch, Mary Liang, Huan ling Baker, Maria Angeles Vepraskas, Adam Rosenau, Chris Dasgupta, Mahua Simpson, Pippa Mitchell, Michael E. Tomita-Mitchell, Aoy PLoS One Research Article Lifelong noninvasive rejection monitoring in heart transplant patients is a critical clinical need historically poorly met in adults and unavailable for children and infants. Cell-free DNA (cfDNA) donor-specific fraction (DF), a direct marker of selective donor organ injury, is a promising analytical target. Methodological differences in sample processing and DF determination profoundly affect quality and sensitivity of cfDNA analyses, requiring specialized optimization for low cfDNA levels typical of transplant patients. Using next-generation sequencing, we previously correlated elevated DF with acute cellular and antibody-mediated rejection (ACR and AMR) in pediatric and adult heart transplant patients. However, next-generation sequencing is limited by cost, TAT, and sensitivity, leading us to clinically validate a rapid, highly sensitive, quantitative genotyping test, myTAI(HEART)(®), addressing these limitations. To assure pre-analytical quality and consider interrelated cfDNA measures, plasma preparation was optimized and total cfDNA (TCF) concentration, DNA fragmentation, and DF quantification were validated in parallel for integration into myTAI(HEART) reporting. Analytical validations employed individual and reconstructed mixtures of human blood-derived genomic DNA (gDNA), cfDNA, and gDNA sheared to apoptotic length. Precision, linearity, and limits of blank/detection/quantification were established for TCF concentration, DNA fragmentation ratio, and DF determinations. For DF, multiplexed high-fidelity amplification followed by quantitative genotyping of 94 SNP targets was applied to 1168 samples to evaluate donor options in staged simulations, demonstrating DF call equivalency with/without donor genotype. Clinical validation studies using 158 matched endomyocardial biopsy-plasma pairs from 76 pediatric and adult heart transplant recipients selected a DF cutoff (0.32%) producing 100% NPV for ≥2R ACR. This supports the assay’s conservative intended use of stratifying low versus increased probability of ≥2R ACR. myTAI(HEART) is clinically validated for heart transplant recipients ≥2 months old and ≥8 days post-transplant, expanding opportunity for noninvasive transplant rejection assessment to infants and children and to all recipients >1 week post-transplant. Public Library of Science 2020-01-13 /pmc/articles/PMC6957190/ /pubmed/31929557 http://dx.doi.org/10.1371/journal.pone.0227385 Text en © 2020 North et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
North, Paula E.
Ziegler, Emily
Mahnke, Donna K.
Stamm, Karl D.
Thomm, Angela
Daft, Paul
Goetsch, Mary
Liang, Huan ling
Baker, Maria Angeles
Vepraskas, Adam
Rosenau, Chris
Dasgupta, Mahua
Simpson, Pippa
Mitchell, Michael E.
Tomita-Mitchell, Aoy
Cell-free DNA donor fraction analysis in pediatric and adult heart transplant patients by multiplexed allele-specific quantitative PCR: Validation of a rapid and highly sensitive clinical test for stratification of rejection probability
title Cell-free DNA donor fraction analysis in pediatric and adult heart transplant patients by multiplexed allele-specific quantitative PCR: Validation of a rapid and highly sensitive clinical test for stratification of rejection probability
title_full Cell-free DNA donor fraction analysis in pediatric and adult heart transplant patients by multiplexed allele-specific quantitative PCR: Validation of a rapid and highly sensitive clinical test for stratification of rejection probability
title_fullStr Cell-free DNA donor fraction analysis in pediatric and adult heart transplant patients by multiplexed allele-specific quantitative PCR: Validation of a rapid and highly sensitive clinical test for stratification of rejection probability
title_full_unstemmed Cell-free DNA donor fraction analysis in pediatric and adult heart transplant patients by multiplexed allele-specific quantitative PCR: Validation of a rapid and highly sensitive clinical test for stratification of rejection probability
title_short Cell-free DNA donor fraction analysis in pediatric and adult heart transplant patients by multiplexed allele-specific quantitative PCR: Validation of a rapid and highly sensitive clinical test for stratification of rejection probability
title_sort cell-free dna donor fraction analysis in pediatric and adult heart transplant patients by multiplexed allele-specific quantitative pcr: validation of a rapid and highly sensitive clinical test for stratification of rejection probability
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6957190/
https://www.ncbi.nlm.nih.gov/pubmed/31929557
http://dx.doi.org/10.1371/journal.pone.0227385
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