Mitochondrial metabolism sustains DNMT3A-R882-mutant clonal haematopoiesis

Malgorzata Gozdecka; Monika Dudek; Sean Wen; Muxin Gu; Richard J Stopforth; Justyna Rak; Aristi Damaskou; Guinevere L Grice; Matthew A McLoughlin; Laura Bond; Rachael Wilson; George Giotopoulos; Vijaya Mahalingam Shanmugiah; Rula Bany Bakar; Eliza Yankova; Jonathan L Cooper; Nisha Narayan; Sarah J Horton; Ryan Asby; Dean C Pask; Annalisa Mupo; Graham Duddy; Ludovica Marando; Theodoros Georgomanolis; Paul Carter; Amirtha Priya Ramesh; William G Dunn; Clea Barcena; Paolo Gallipoli; Kosuke Yusa; Slavé Petrovski; Penny Wright; Pedro M Quiros; Christian Frezza; James A Nathan; Arthur Kaser; Siddhartha Kar; Konstantinos Tzelepis; Jonathan Mitchell; Margarete A Fabre; Brian J P Huntly; George S Vassiliou

doi:10.1038/s41586-025-08980-6

Mitochondrial metabolism sustains DNMT3A-R882-mutant clonal haematopoiesis

Nature. 2025 Jun;642(8067):431-441. doi: 10.1038/s41586-025-08980-6. Epub 2025 Apr 16.

Authors

Malgorzata Gozdecka^{1

2}, Monika Dudek^#^{3

4}, Sean Wen^#^{4

5}, Muxin Gu^{3

4}, Richard J Stopforth⁶, Justyna Rak^{3

4}, Aristi Damaskou^{3

4}, Guinevere L Grice⁶, Matthew A McLoughlin^{3

4}, Laura Bond^{3

4}, Rachael Wilson^{3

4}, George Giotopoulos^{3

4}, Vijaya Mahalingam Shanmugiah^{3

4}, Rula Bany Bakar⁶, Eliza Yankova^{3

4

7}, Jonathan L Cooper^{3

4}, Nisha Narayan^{3

4}, Sarah J Horton^{3

4}, Ryan Asby^{3

4}, Dean C Pask^{3

4}, Annalisa Mupo⁸, Graham Duddy⁹, Ludovica Marando^{3

4}, Theodoros Georgomanolis¹⁰, Paul Carter¹¹, Amirtha Priya Ramesh^{3

4}, William G Dunn^{3

4}, Clea Barcena^{3

4

12}, Paolo Gallipoli¹³, Kosuke Yusa¹⁴, Slavé Petrovski⁵, Penny Wright¹⁵, Pedro M Quiros^{3

4

12}, Christian Frezza^{10

16}, James A Nathan⁶, Arthur Kaser^{6

17}, Siddhartha Kar¹⁸, Konstantinos Tzelepis^{3

4

7}, Jonathan Mitchell⁵, Margarete A Fabre^{4

5

19}, Brian J P Huntly^{20

21

22}, George S Vassiliou^{23

24

25

26}

Affiliations

¹ Cambridge Stem Cell Institute, University of Cambridge, Cambridge, UK. mg717@cam.ac.uk.
² Department of Haematology, University of Cambridge, Cambridge, UK. mg717@cam.ac.uk.
³ Cambridge Stem Cell Institute, University of Cambridge, Cambridge, UK.
⁴ Department of Haematology, University of Cambridge, Cambridge, UK.
⁵ Centre for Genomics Research, Discovery Sciences, BioPharmaceuticals Research and Development, AstraZeneca, Cambridge, UK.
⁶ Cambridge Institute of Therapeutic Immunology and Infectious Disease (CITIID), Jeffrey Cheah Biomedical Centre, University of Cambridge, Cambridge, UK.
⁷ Milner Therapeutics Institute, Jeffrey Cheah Biomedical Centre, University of Cambridge, Cambridge, UK.
⁸ Altos Labs, Granta Park, Cambridge, UK.
⁹ The Francis Crick Institute, London, UK.
¹⁰ Cluster of Excellence Cellular Stress Responses in Aging-associated Diseases (CECAD), University Hospital Cologne, Cologne, Germany.
¹¹ Section of Cardiovascular Medicine, The Victor Phillip Dahdalleh Heart and Lung Research Institute, The University of Cambridge, Papworth Road, Cambridge Biomedical Campus, Cambridge, UK.
¹² Departamento de Bioquímica y Biología Molecular, Instituto Universitario de Oncología (IUOPA), Universidad de Oviedo, Oviedo, Spain.
¹³ Centre for Haemato-Oncology, Barts Cancer Institute, Queen Mary University of London, London, UK.
¹⁴ Stem Cell Genetics, Institute for Life and Medical Sciences, Kyoto University, Kyoto, Japan.
¹⁵ Department of Anatomic Pathology, Canterbury Health Laboratories, Christchurch, New Zealand.
¹⁶ Institute of Genetics, Faculty of Mathematics and Natural Sciences, Faculty of Medicine, University of Cologne, Cologne, Germany.
¹⁷ Division of Gastroenterology and Hepatology, Department of Medicine, University of Cambridge, Addenbrooke's Hospital, Cambridge, UK.
¹⁸ Early Cancer Institute, Department of Oncology, University of Cambridge, Cambridge, UK.
¹⁹ Department of Haematology, Cambridge University Hospitals NHS Foundation Trust, Cambridge, UK.
²⁰ Cambridge Stem Cell Institute, University of Cambridge, Cambridge, UK. bjph2@cam.ac.uk.
²¹ Department of Haematology, University of Cambridge, Cambridge, UK. bjph2@cam.ac.uk.
²² Department of Haematology, Cambridge University Hospitals NHS Foundation Trust, Cambridge, UK. bjph2@cam.ac.uk.
²³ Cambridge Stem Cell Institute, University of Cambridge, Cambridge, UK. gsv20@cam.ac.uk.
²⁴ Department of Haematology, University of Cambridge, Cambridge, UK. gsv20@cam.ac.uk.
²⁵ Department of Haematology, Cambridge University Hospitals NHS Foundation Trust, Cambridge, UK. gsv20@cam.ac.uk.
²⁶ Wellcome Sanger Institute, Wellcome Genome Campus, Hinxton, Cambridge, UK. gsv20@cam.ac.uk.

^# Contributed equally.

Abstract

Somatic DNMT3A-R882 codon mutations drive the most common form of clonal haematopoiesis (CH) and are associated with increased acute myeloid leukaemia (AML) risk^1,2. Preventing expansion of DNMT3A-R882-mutant haematopoietic stem/progenitor cells (HSPCs) may therefore avert progression to AML. To identify DNMT3A-R882-mutant-specific vulnerabilities, we conducted a genome-wide CRISPR screen on primary mouse Dnmt3a^R882H/+ HSPCs. Among the 640 vulnerability genes identified, many were involved in mitochondrial metabolism, and metabolic flux analysis confirmed enhanced oxidative phosphorylation use in Dnmt3a^R882H/+ versus Dnmt3a^+/+ (WT) HSPCs. We selected citrate/malate transporter Slc25a1 and complex I component Ndufb11, for which pharmacological inhibitors are available, for downstream studies. In vivo administration of SLC25A1 inhibitor CTPI2 and complex I inhibitors IACS-010759 and metformin suppressed post-transplantation clonal expansion of Dnmt3a^R882H/+, but not WT, long-term haematopoietic stem cells. The effect of metformin was recapitulated using a primary human DNMT3A-R882 CH sample. Notably, analysis of 412,234 UK Biobank participants showed that individuals taking metformin had a markedly lower prevalence of DNMT3A-R882-mutant CH, after controlling for potential confounders including glycated haemoglobin, diabetes and body mass index. Collectively, our data propose modulation of mitochondrial metabolism as a therapeutic strategy for prevention of DNMT3A-R882-mutant AML.

MeSH terms

Animals
Clonal Hematopoiesis* / drug effects
Clonal Hematopoiesis* / genetics
Clone Cells / cytology
Clone Cells / drug effects
Clone Cells / metabolism
DNA (Cytosine-5-)-Methyltransferases* / genetics
DNA Methyltransferase 3A
Electron Transport Complex I / antagonists & inhibitors
Electron Transport Complex I / metabolism
Female
Hematopoietic Stem Cells / cytology
Hematopoietic Stem Cells / drug effects
Hematopoietic Stem Cells / metabolism
Humans
Leukemia, Myeloid, Acute / drug therapy
Leukemia, Myeloid, Acute / genetics
Leukemia, Myeloid, Acute / metabolism
Leukemia, Myeloid, Acute / pathology
Leukemia, Myeloid, Acute / prevention & control
Male
Metformin / pharmacology
Mice
Mitochondria* / drug effects
Mitochondria* / genetics
Mitochondria* / metabolism
Mutation* / genetics
Oxidative Phosphorylation / drug effects

Substances

DNA (Cytosine-5-)-Methyltransferases
Dnmt3a protein, mouse
DNA Methyltransferase 3A
DNMT3A protein, human
Metformin
Electron Transport Complex I

Grants and funding

WT_/Wellcome Trust/United Kingdom