Rational biomarker development for the early and minimally invasive monitoring of AML

Author:

Abdelhamed Sherif1ORCID,Butler John T.23ORCID,Jung Seul4ORCID,Chen Ding-Wen4ORCID,Jenkins Gaye56,Gao Lina7ORCID,Lim Jeong Y.7,Klco Jeffery M.1,Horton Terzah M.56,Kurre Peter48

Affiliation:

1. Department of Pathology, St. Jude Children’s Research Hospital, Memphis, TN;

2. Department of Pediatrics, Pape Family Pediatric Research Institute, OHSU, Portland, OR;

3. Department of Biomedical Engineering, OHSU, Portland, OR;

4. Children’s Hospital of Philadelphia, Comprehensive Bone Marrow Failure Center, Philadelphia, PA;

5. Baylor College of Medicine/Dan L. Duncan Cancer Center;

6. Texas Children's Cancer Center, Houston, TX;

7. Biostatistics Shared Resource, Knight Cancer Institute, OHSU, Portland, OR; and

8. University of Pennsylvania, Perelman School of Medicine, Philadelphia, PA

Abstract

Abstract Recurrent disease remains the principal cause for treatment failure in acute myeloid leukemia (AML) across age groups. Reliable biomarkers of AML relapse risk and disease burden have been problematic, as symptoms appear late and current monitoring relies on invasive and cost-ineffective serial bone marrow (BM) surveillance. In this report, we discover a set of unique microRNA (miRNA) that circulates in AML-derived vesicles in the peripheral blood ahead of the general dissemination of leukemic blasts and symptomatic BM failure. Next-generation sequencing of extracellular vesicle-contained small RNA in 12 AML patients and 12 controls allowed us to identify a panel of differentially incorporated miRNA. Proof-of-concept studies using a murine model and patient-derived xenografts demonstrate the feasibility of developing miR-1246, as a potential minimally invasive AML biomarker.

Publisher

American Society of Hematology

Subject

Hematology

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