Clonal hematopoiesis and its impact on the aging osteo-hematopoietic niche

Research output: Contribution to journalReview articleContributedpeer-review

Contributors

Abstract

Clonal hematopoiesis (CH) defines a premalignant state predominantly found in older persons that increases the risk of developing hematologic malignancies and age-related inflammatory diseases. However, the risk for malignant transformation or non-malignant disorders is variable and difficult to predict, and defining the clinical relevance of specific candidate driver mutations in individual carriers has proved to be challenging. In addition to the cell-intrinsic mechanisms, mutant cells rely on and alter cell-extrinsic factors from the bone marrow (BM) niche, which complicates the prediction of a mutant cell's fate in a shifting pre-malignant microenvironment. Therefore, identifying the insidious and potentially broad impact of driver mutations on supportive niches and immune function in CH aims to understand the subtle differences that enable driver mutations to yield different clinical outcomes. Here, we review the changes in the aging BM niche and the emerging evidence supporting the concept that CH can progressively alter components of the local BM microenvironment. These alterations may have profound implications for the functionality of the osteo-hematopoietic niche and overall bone health, consequently fostering a conducive environment for the continued development and progression of CH. We also provide an overview of the latest technology developments to study the spatiotemporal dependencies in the CH BM niche, ideally in the context of longitudinal studies following CH over time. Finally, we discuss aspects of CH carrier management in clinical practice, based on work from our group and others.

Details

Original languageEnglish
Pages (from-to)936-946
Number of pages11
JournalLeukemia
Volume38
Issue number5
Early online date21 Mar 2024
Publication statusPublished - 21 Mar 2024
Peer-reviewedYes

External IDs

Scopus 85188247166
ORCID /0000-0002-8691-8423/work/156336008
ORCID /0000-0002-4228-4537/work/156336759
ORCID /0000-0002-2524-1199/work/156338069

Keywords