Tipping the balance between erythroid cell differentiation and induction of anemia in response to the inflammatory pathology associated with chronic trypanosome infections
- Author
- Thi Thu Hang Nguyen, Magdalena Radwanska (UGent) and Stefan Magez (UGent)
- Organization
- Project
- Abstract
- Infection caused by extracellular single-celled trypanosomes triggers a lethal chronic wasting disease in livestock and game animals. Through screening of 10 Trypanosoma evansi field isolates, exhibiting different levels of virulence in mice, the current study identifies an experimental disease model in which infection can last well over 100 days, mimicking the major features of chronic animal trypanosomosis. In this model, despite the well-controlled parasitemia, infection is hallmarked by severe trypanosomosis-associated pathology. An in-depth scRNA-seq analysis of the latter revealed the complexity of the spleen macrophage activation status, highlighting the crucial role of tissue resident macrophages (TRMs) in regulating splenic extramedullary erythropoiesis. These new data show that in the field of experimental trypanosomosis, macrophage activation profiles have so far been oversimplified into a bi-polar paradigm (M1 vs M2). Interestingly, TRMs exert a double-sided effect on erythroid cells. On one hand, these cells express an erythrophagocytosis associated signature. On another hand, TRMs show high levels of Vcam1 expression, known to support their interaction with hematopoietic stem and progenitor cells (HSPCs). During chronic infection, the latter exhibit upregulated expression of Klf1, E2f8, and Gfi1b genes, involved in erythroid differentiation and extramedullary erythropoiesis. This process gives rise to differentiation of stem cells to BFU-e/CFU-e, Pro E, and Baso E subpopulations. However, infection truncates progressing differentiation at the orthochromatic erythrocytes level, as demonstrated by scRNAseq and flow cytometry. As such, these cells are unable to pass to the reticulocyte stage, resulting in reduced number of mature circulating RBCs and the occurrence of chronic anemia. The physiological consequence of these events is the prolonged poor delivery of oxygen to various tissues, triggering lactic acid acidosis and the catabolic breakdown of muscle tissue, reminiscent of the wasting syndrome that is characteristic for the lethal stage of animal trypanosomosis.
- Keywords
- Immunology, Immunology and Allergy, Trypanosomosis, tissue resident macrophages, extramedullary erythropoiesis, immunopathology, lactic acidosis, NITRIC-OXIDE SYNTHASE, HEMATOPOIETIC STEM-CELLS, NECROSIS-FACTOR-ALPHA, EVANSI INFECTION, MACROPHAGE ACTIVATION, AFRICAN TRYPANOSOMES, INTERFERON-GAMMA, L-LACTATE, IN-VITRO, BRUCEI
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Citation
Please use this url to cite or link to this publication: http://hdl.handle.net/1854/LU-01GP5ESGCW056A7MB7W9JD6JK3
- MLA
- Nguyen, Thi Thu Hang, et al. “Tipping the Balance between Erythroid Cell Differentiation and Induction of Anemia in Response to the Inflammatory Pathology Associated with Chronic Trypanosome Infections.” FRONTIERS IN IMMUNOLOGY, vol. 13, 2022, doi:10.3389/fimmu.2022.1051647.
- APA
- Nguyen, T. T. H., Radwanska, M., & Magez, S. (2022). Tipping the balance between erythroid cell differentiation and induction of anemia in response to the inflammatory pathology associated with chronic trypanosome infections. FRONTIERS IN IMMUNOLOGY, 13. https://doi.org/10.3389/fimmu.2022.1051647
- Chicago author-date
- Nguyen, Thi Thu Hang, Magdalena Radwanska, and Stefan Magez. 2022. “Tipping the Balance between Erythroid Cell Differentiation and Induction of Anemia in Response to the Inflammatory Pathology Associated with Chronic Trypanosome Infections.” FRONTIERS IN IMMUNOLOGY 13. https://doi.org/10.3389/fimmu.2022.1051647.
- Chicago author-date (all authors)
- Nguyen, Thi Thu Hang, Magdalena Radwanska, and Stefan Magez. 2022. “Tipping the Balance between Erythroid Cell Differentiation and Induction of Anemia in Response to the Inflammatory Pathology Associated with Chronic Trypanosome Infections.” FRONTIERS IN IMMUNOLOGY 13. doi:10.3389/fimmu.2022.1051647.
- Vancouver
- 1.Nguyen TTH, Radwanska M, Magez S. Tipping the balance between erythroid cell differentiation and induction of anemia in response to the inflammatory pathology associated with chronic trypanosome infections. FRONTIERS IN IMMUNOLOGY. 2022;13.
- IEEE
- [1]T. T. H. Nguyen, M. Radwanska, and S. Magez, “Tipping the balance between erythroid cell differentiation and induction of anemia in response to the inflammatory pathology associated with chronic trypanosome infections,” FRONTIERS IN IMMUNOLOGY, vol. 13, 2022.
@article{01GP5ESGCW056A7MB7W9JD6JK3,
abstract = {{Infection caused by extracellular single-celled trypanosomes triggers a lethal chronic wasting disease in livestock and game animals. Through screening of 10 Trypanosoma evansi field isolates, exhibiting different levels of virulence in mice, the current study identifies an experimental disease model in which infection can last well over 100 days, mimicking the major features of chronic animal trypanosomosis. In this model, despite the well-controlled parasitemia, infection is hallmarked by severe trypanosomosis-associated pathology. An in-depth scRNA-seq analysis of the latter revealed the complexity of the spleen macrophage activation status, highlighting the crucial role of tissue resident macrophages (TRMs) in regulating splenic extramedullary erythropoiesis. These new data show that in the field of experimental trypanosomosis, macrophage activation profiles have so far been oversimplified into a bi-polar paradigm (M1 vs M2). Interestingly, TRMs exert a double-sided effect on erythroid cells. On one hand, these cells express an erythrophagocytosis associated signature. On another hand, TRMs show high levels of Vcam1 expression, known to support their interaction with hematopoietic stem and progenitor cells (HSPCs). During chronic infection, the latter exhibit upregulated expression of Klf1, E2f8, and Gfi1b genes, involved in erythroid differentiation and extramedullary erythropoiesis. This process gives rise to differentiation of stem cells to BFU-e/CFU-e, Pro E, and Baso E subpopulations. However, infection truncates progressing differentiation at the orthochromatic erythrocytes level, as demonstrated by scRNAseq and flow cytometry. As such, these cells are unable to pass to the reticulocyte stage, resulting in reduced number of mature circulating RBCs and the occurrence of chronic anemia. The physiological consequence of these events is the prolonged poor delivery of oxygen to various tissues, triggering lactic acid acidosis and the catabolic breakdown of muscle tissue, reminiscent of the wasting syndrome that is characteristic for the lethal stage of animal trypanosomosis.}},
articleno = {{1051647}},
author = {{Nguyen, Thi Thu Hang and Radwanska, Magdalena and Magez, Stefan}},
issn = {{1664-3224}},
journal = {{FRONTIERS IN IMMUNOLOGY}},
keywords = {{Immunology,Immunology and Allergy,Trypanosomosis,tissue resident macrophages,extramedullary erythropoiesis,immunopathology,lactic acidosis,NITRIC-OXIDE SYNTHASE,HEMATOPOIETIC STEM-CELLS,NECROSIS-FACTOR-ALPHA,EVANSI INFECTION,MACROPHAGE ACTIVATION,AFRICAN TRYPANOSOMES,INTERFERON-GAMMA,L-LACTATE,IN-VITRO,BRUCEI}},
language = {{eng}},
pages = {{19}},
title = {{Tipping the balance between erythroid cell differentiation and induction of anemia in response to the inflammatory pathology associated with chronic trypanosome infections}},
url = {{http://doi.org/10.3389/fimmu.2022.1051647}},
volume = {{13}},
year = {{2022}},
}
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