Persistent Molecular Disease in Adult Patients With AML Evaluated With Whole-Exome and Targeted Error-Corrected DNA Sequencing

PURPOSE: Persistent molecular disease (PMD) after induction chemotherapy predicts relapse in AML. In this study, we used whole-exome sequencing (WES) and targeted error-corrected sequencing to assess the frequency and mutational patterns of PMD in 30 patients with AML. MATERIALS AND METHODS: The stu...

Descripción completa

Detalles Bibliográficos
Autores principales: Slade, Michael J., Ghasemi, Reza, O'Laughlin, Michelle, Burton, Tasha, Fulton, Robert S., Abel, Haley J., Duncavage, Eric J., Ley, Timothy J., Jacoby, Meagan A., Spencer, David H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Wolters Kluwer Health 2023
Materias:
Original Reports
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10530963/
https://www.ncbi.nlm.nih.gov/pubmed/37079859
http://dx.doi.org/10.1200/PO.22.00559
_version_ 1785111608592171008
author Slade, Michael J.
Ghasemi, Reza
O'Laughlin, Michelle
Burton, Tasha
Fulton, Robert S.
Abel, Haley J.
Duncavage, Eric J.
Ley, Timothy J.
Jacoby, Meagan A.
Spencer, David H.
author_facet Slade, Michael J.
Ghasemi, Reza
O'Laughlin, Michelle
Burton, Tasha
Fulton, Robert S.
Abel, Haley J.
Duncavage, Eric J.
Ley, Timothy J.
Jacoby, Meagan A.
Spencer, David H.
author_sort Slade, Michael J.
collection PubMed
description PURPOSE: Persistent molecular disease (PMD) after induction chemotherapy predicts relapse in AML. In this study, we used whole-exome sequencing (WES) and targeted error-corrected sequencing to assess the frequency and mutational patterns of PMD in 30 patients with AML. MATERIALS AND METHODS: The study cohort included 30 patients with adult AML younger than 65 years who were uniformly treated with standard induction chemotherapy. Tumor/normal WES was performed for all patients at presentation. PMD analysis was evaluated in bone marrow samples obtained during clinicopathologic remission using repeat WES and analysis of patient-specific mutations and error-corrected sequencing of 40 recurrently mutated AML genes (MyeloSeq). RESULTS: WES for patient-specific mutations detected PMD in 63% of patients (19/30) using a minimum variant allele fraction (VAF) of 2.5%. In comparison, MyeloSeq identified persistent mutations above 0.1% VAF in 77% of patients (23/30). PMD was usually present at relatively high levels (>2.5% VAFs), such that WES and MyeloSeq agreed for 73% of patients despite differences in detection limits. Mutations in DNMT3A, ASXL1, and TET2 (ie, DTA mutations) were persistent in 16 of 17 patients, but WES also detected non-DTA mutations in 14 of these patients, which for some patients distinguished residual AML cells from clonal hematopoiesis. Surprisingly, MyeloSeq detected additional variants not identified at presentation in 73% of patients that were consistent with new clonal cell populations after chemotherapy. CONCLUSION: PMD and clonal hematopoiesis are both common in patients with AML in first remission. These findings demonstrate the importance of baseline testing for accurate interpretation of mutation-based tumor monitoring assays for patients with AML and highlight the need for clinical trials to determine whether these complex mutation patterns correlate with clinical outcomes in AML.
format Online
Article
Text
id pubmed-10530963
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Wolters Kluwer Health
record_format MEDLINE/PubMed
spelling pubmed-105309632023-09-28 Persistent Molecular Disease in Adult Patients With AML Evaluated With Whole-Exome and Targeted Error-Corrected DNA Sequencing Slade, Michael J. Ghasemi, Reza O'Laughlin, Michelle Burton, Tasha Fulton, Robert S. Abel, Haley J. Duncavage, Eric J. Ley, Timothy J. Jacoby, Meagan A. Spencer, David H. JCO Precis Oncol Original Reports PURPOSE: Persistent molecular disease (PMD) after induction chemotherapy predicts relapse in AML. In this study, we used whole-exome sequencing (WES) and targeted error-corrected sequencing to assess the frequency and mutational patterns of PMD in 30 patients with AML. MATERIALS AND METHODS: The study cohort included 30 patients with adult AML younger than 65 years who were uniformly treated with standard induction chemotherapy. Tumor/normal WES was performed for all patients at presentation. PMD analysis was evaluated in bone marrow samples obtained during clinicopathologic remission using repeat WES and analysis of patient-specific mutations and error-corrected sequencing of 40 recurrently mutated AML genes (MyeloSeq). RESULTS: WES for patient-specific mutations detected PMD in 63% of patients (19/30) using a minimum variant allele fraction (VAF) of 2.5%. In comparison, MyeloSeq identified persistent mutations above 0.1% VAF in 77% of patients (23/30). PMD was usually present at relatively high levels (>2.5% VAFs), such that WES and MyeloSeq agreed for 73% of patients despite differences in detection limits. Mutations in DNMT3A, ASXL1, and TET2 (ie, DTA mutations) were persistent in 16 of 17 patients, but WES also detected non-DTA mutations in 14 of these patients, which for some patients distinguished residual AML cells from clonal hematopoiesis. Surprisingly, MyeloSeq detected additional variants not identified at presentation in 73% of patients that were consistent with new clonal cell populations after chemotherapy. CONCLUSION: PMD and clonal hematopoiesis are both common in patients with AML in first remission. These findings demonstrate the importance of baseline testing for accurate interpretation of mutation-based tumor monitoring assays for patients with AML and highlight the need for clinical trials to determine whether these complex mutation patterns correlate with clinical outcomes in AML. Wolters Kluwer Health 2023-04-20 /pmc/articles/PMC10530963/ /pubmed/37079859 http://dx.doi.org/10.1200/PO.22.00559 Text en © 2023 by American Society of Clinical Oncology https://creativecommons.org/licenses/by-nc-nd/4.0/Creative Commons Attribution Non-Commercial No Derivatives 4.0 License: http://creativecommons.org/licenses/by-nc-nd/4.0/ (https://creativecommons.org/licenses/by-nc-nd/4.0/)
spellingShingle Original Reports
Slade, Michael J.
Ghasemi, Reza
O'Laughlin, Michelle
Burton, Tasha
Fulton, Robert S.
Abel, Haley J.
Duncavage, Eric J.
Ley, Timothy J.
Jacoby, Meagan A.
Spencer, David H.
Persistent Molecular Disease in Adult Patients With AML Evaluated With Whole-Exome and Targeted Error-Corrected DNA Sequencing
title Persistent Molecular Disease in Adult Patients With AML Evaluated With Whole-Exome and Targeted Error-Corrected DNA Sequencing
title_full Persistent Molecular Disease in Adult Patients With AML Evaluated With Whole-Exome and Targeted Error-Corrected DNA Sequencing
title_fullStr Persistent Molecular Disease in Adult Patients With AML Evaluated With Whole-Exome and Targeted Error-Corrected DNA Sequencing
title_full_unstemmed Persistent Molecular Disease in Adult Patients With AML Evaluated With Whole-Exome and Targeted Error-Corrected DNA Sequencing
title_short Persistent Molecular Disease in Adult Patients With AML Evaluated With Whole-Exome and Targeted Error-Corrected DNA Sequencing
title_sort persistent molecular disease in adult patients with aml evaluated with whole-exome and targeted error-corrected dna sequencing
topic Original Reports
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10530963/
https://www.ncbi.nlm.nih.gov/pubmed/37079859
http://dx.doi.org/10.1200/PO.22.00559
work_keys_str_mv AT slademichaelj persistentmoleculardiseaseinadultpatientswithamlevaluatedwithwholeexomeandtargetederrorcorrecteddnasequencing
AT ghasemireza persistentmoleculardiseaseinadultpatientswithamlevaluatedwithwholeexomeandtargetederrorcorrecteddnasequencing
AT olaughlinmichelle persistentmoleculardiseaseinadultpatientswithamlevaluatedwithwholeexomeandtargetederrorcorrecteddnasequencing
AT burtontasha persistentmoleculardiseaseinadultpatientswithamlevaluatedwithwholeexomeandtargetederrorcorrecteddnasequencing
AT fultonroberts persistentmoleculardiseaseinadultpatientswithamlevaluatedwithwholeexomeandtargetederrorcorrecteddnasequencing
AT abelhaleyj persistentmoleculardiseaseinadultpatientswithamlevaluatedwithwholeexomeandtargetederrorcorrecteddnasequencing
AT duncavageericj persistentmoleculardiseaseinadultpatientswithamlevaluatedwithwholeexomeandtargetederrorcorrecteddnasequencing
AT leytimothyj persistentmoleculardiseaseinadultpatientswithamlevaluatedwithwholeexomeandtargetederrorcorrecteddnasequencing
AT jacobymeagana persistentmoleculardiseaseinadultpatientswithamlevaluatedwithwholeexomeandtargetederrorcorrecteddnasequencing
AT spencerdavidh persistentmoleculardiseaseinadultpatientswithamlevaluatedwithwholeexomeandtargetederrorcorrecteddnasequencing

Ejemplares similares