Abstract

Simple SummaryImmunotherapy may be an attractive treatment option to increase survival, and to reduce treatment-related side effects, for children with acute myeloid leukemia (AML). While immunotherapies have shown successes in many cancer types, the development and subsequent clinical implementation have proven difficult in pediatric AML. To expedite the development of immunotherapy, it will be crucial to understand which pediatric AML patients are likely to respond to immunotherapies. Emerging research in solid malignancies has shown that the number and phenotype of immune cells in the tumor microenvironment is predictive of response to several types of immunotherapies. Such a predictive model may also be applicable for AML and, thus, knowledge on the immune cells infiltrating the bone marrow environment is needed. Here, we discuss the current state of knowledge on these infiltrating immune cells in pediatric AML, as well as ongoing immunotherapy trials, and provide suggestions concerning the way forward.Immunotherapeutic agents may be an attractive option to further improve outcomes and to reduce treatment-related toxicity for pediatric AML. While improvements in outcome have been observed with immunotherapy in many cancer types, immunotherapy development and implementation into patient care for both adult and pediatric AML has been hampered by an incomplete understanding of the bone marrow environment and a paucity of tumor-specific antigens. Since only a minority of patients respond in most immunotherapy trials across different cancer types, it will be crucial to understand which children with AML are likely to respond to or may benefit from immunotherapies. Immune cell profiling efforts hold promise to answer this question, as illustrated by the development of predictive scores in solid cancers. Such information on the number and phenotype of immune cells during current treatment regimens will be pivotal to generate hypotheses on how and when to intervene with immunotherapy in pediatric AML. In this review, we discuss the current understanding of the number and phenotype of immune cells in the bone marrow in pediatric AML, ongoing immunotherapy trials and how comprehensive immune profiling efforts may pave the way for successful clinical trials (and, ultimately, implementation into patient care).

Highlights

  • Acute myeloid leukemia (AML) is a heterogeneous blood cancer characterized by both aberrant proliferation and arrested differentiation of immature myeloid cells in the bone marrow [1]

  • We describe the current knowledge on both immune cells and target antigen expression in the tumor microenvironment (TME) in pediatric AML, discuss ongoing immunotherapy trials, and delineate how immune profiling efforts may pave the way for immunotherapy implementation into patient care

  • Since the prognostic and predictive potential of immune cells in the bone marrow of AML is increasingly recognized, we summarized the available information on immune cell abundance and phenotype in the TME for children with AML at diagnosis

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Summary

Introduction

Acute myeloid leukemia (AML) is a heterogeneous blood cancer characterized by both aberrant proliferation and arrested differentiation of immature myeloid cells in the bone marrow [1]. This may be due to differences in underlying leukemia biology, treatment, and potentially in host-factors such as the immune cell composition in the bone marrow [29,38]. We describe the current knowledge on both immune cells and target antigen expression in the TME in pediatric AML, discuss ongoing immunotherapy trials, and delineate how immune profiling efforts may pave the way for immunotherapy implementation into patient care

Immune Cells in the TME
Overview
Immune Cells in the TME of AML at Diagnosis
Immune Cells in the TME in Relapsed and Refractory Disease
Immune Cells in the TME during and after Therapy
Genetic Alterations That Affect the Immune Cell Abundance in the TME
The Relevance of Systemic Immunity for Immunotherapy Responses
Target Antigen Expression in Pediatric AML
Immunotherapy Trials in Pediatric AML
The Way Forward in Pediatric AML
Discussions
Findings
Conclusions
Full Text
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