Abstract

Fanconi anemia (FA) is the most common type of inherited bone marrow failure (BMF) syndromes and poses tremendous challenges in health care. The process of FA disease progression in the context of hematopoiesis is characterized by BMF, clonal proliferation of hematopoietic stem and progenitor cells (HSPCs), and progression to myelodysplastic syndrome (MDS) and acute myeloid leukemia (AML). While many studies have established a correlation between FA deficiency and defects in the HSC compartment, the mechanisms by which the FA proteins function in HSC maintenance remain largely unknown. During this past funding period, we have gathered evidence implicating pathogenic role of HSC-specific metabolic abnormality in FA. More recently, we identified the Fancd2-Atad3-Tufm complex using our newly developed Fancd23XFLAGHA knock- in model, and established a potential linkage of FA HSC failure to dysregulated mitochondrial translation and oxidative phosphorylation (OXPHOS). We hypothesize that the FANCD2/FA pathway restricts mitochondrial activity in HSC maintenance, and that loss of FA function leads to augmented mitochondrial translation and OXPHOS contributing to BMF and leukemic progression. The goals of the project are to investigate (1) the mechanism by which the FANCD2/FA pathway controls mitochondrial activity in HSC maintenance and (2) the link between augmented mitochondrial translation/OXPHOS and FA disease progression. To achieve these goals, we will first assess the functional consequence of the interaction between Fancd2 and the mitochondrial translational machinery by determining the structural elements of the biochemical interaction between Fancd2 and the Atad3-Tufm complex, the requirement for the Fancd2-Atad3-Tufm interaction in the control of mitochondrial translation and OXPHOS, and the functional link between the Fancd2-Atad3-Tufm interaction and HSC maintenance. We will then investigate whether there is a direct link between augmented mitochondrial translation/OXPHOS and FA disease progression in FA patients at three different stages (BMF, MDS, and AML), and the cellular mechanisms responsible for leukemic transformation in FA HSCs. Successful completion of the proposed study will not only improve mechanistic understanding of the interplay between the FA pathway and mitochondrial metabolism in the context of HSC maintenance, but also lead to a new avenue of research designed to target specific dysregulated metabolic checkpoints for developing innovative therapeutic strategies in FA and other BM failure and leukemia diseases.

Public Health Relevance

(Relevance Statement): Mitochondrial dysfunction has been implicated in the pathogenesis of many human diseases including Fanconi anemia (FA), a blood disease associated with bone marrow failure and cancer. The goal of this project is to define the function of FA proteins in the maintenance of blood cell survival through regulation of mitochondrial activity. The proposed study will provide valuable information for therapeutic prevention and treatment of bone marrow failure and cancer progression of not only FA but also other blood diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL076712-13
Application #
9939646
Study Section
Molecular and Cellular Hematology Study Section (MCH)
Program Officer
Qasba, Pankaj
Project Start
2005-09-01
Project End
2021-05-31
Budget Start
2020-06-01
Budget End
2021-05-31
Support Year
13
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Cincinnati Children's Hospital Medical Center
Department
Type
DUNS #
071284913
City
Cincinnati
State
OH
Country
United States
Zip Code
45229

  Publications

Du, Wei; Liu, Wei; Mizukawa, Benjamin et al. (2018) A non-myeloablative conditioning approach for long-term engraftment of human and mouse hematopoietic stem cells. Leukemia 32:2041-2046
Du, Wei; Li, Xiaoli; Wilson, Andrew F et al. (2018) A small molecule p53 activator attenuates Fanconi anemia leukemic stem cell proliferation. Stem Cell Res Ther 9:145
Li, Xiaoli; Wilson, Andrew F; Du, Wei et al. (2018) Cell-Cycle-Specific Function of p53 in Fanconi Anemia Hematopoietic Stem and Progenitor Cell Proliferation. Stem Cell Reports 10:339-346
Du, W; Amarachintha, S; Wilson, A et al. (2017) The immune receptor Trem1 cooperates with diminished DNA damage response to induce preleukemic stem cell expansion. Leukemia 31:423-433
Zhang, Tingting; Du, Wei; Wilson, Andrew F et al. (2017) Fancd2 in vivo interaction network reveals a non-canonical role in mitochondrial function. Sci Rep 7:45626
Sertorio, Mathieu; Du, Wei; Amarachintha, Surya et al. (2017) In Vivo RNAi Screen Unveils PPAR? as a Regulator of Hematopoietic Stem Cell Homeostasis. Stem Cell Reports 8:1242-1255
Du, Wei; Amarachintha, Surya; Erden, Ozlem et al. (2016) The Fanconi anemia pathway controls oncogenic response in hematopoietic stem and progenitor cells by regulating PRMT5-mediated p53 arginine methylation. Oncotarget 7:60005-60020
Du, Wei; Amarachintha, Surya; Wilson, Andrew F et al. (2016) Hyper-active non-homologous end joining selects for synthetic lethality resistant and pathological Fanconi anemia hematopoietic stem and progenitor cells. Sci Rep 6:22167
Sertorio, Mathieu; Amarachintha, Surya; Wilson, Andrew et al. (2016) Loss of Fancc Impairs Antibody-Secreting Cell Differentiation in Mice through Deregulating the Wnt Signaling Pathway. J Immunol 196:2986-94
Du, Wei; Amarachintha, Surya; Wilson, Andrew F et al. (2016) SCO2 Mediates Oxidative Stress-Induced Glycolysis to Oxidative Phosphorylation Switch in Hematopoietic Stem Cells. Stem Cells 34:960-71

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