Enhanced Preprints

Reprogramming of host energy metabolism mediated by the TNF-iNOS-HIF-1α axis plays a key role in host resistance to Plasmodium infection

  1. Kely C Matteucci author has email address
  2. Patricia A Assis
  3. Isabella C Hirako
  4. Nathalia PS Leite
  5. Franciele Pioto
  6. Ogooluwa Ojelabi
  7. Juliana E Toller-Kawahisa
  8. Diego L Costa
  9. João S Da Silva
  10. José C Alves-Filho
  11. Ricardo T Gazzinelli author has email address
  1. Translational Medicine Platform Oswaldo Cruz Foundation / Ribeirão Preto Medical School University of Sao Paulo-Brazil.
  2. Department of Biochemistry and Immunology, Ribeirão Preto Medical School, University of Sao Paulo- Brazil.
  3. Department of Pathology, University of Michigan Medical School, Ann Arbor, USA
  4. Laboratory of Immunopathology, Instituto René Rachou, Fundação Oswaldo Cruz - Minas, Belo Horizonte, Minas Gerais – Brazil
  5. Department of Medicine, Division of Infectious Diseases and Immunology, University of Massachusetts Chan Medical School, Worcester, Massachusetts-USA
  6. Departament of Pharmacology, Ribeirão Preto Medical School University of Sao Paulo-Brazil.
  7. Department of Immunology, Institute of Biomedical Sciences, University of Sao Paulo- Brazil.

Peer review process

Not revised: This Reviewed Preprint includes the authors’ original preprint (without revision), an eLife assessment, and public reviews.

Read more about eLife’s peer review process.

Editors

  • Reviewing Editor
    Bryan Bryson
    Massachusetts Institute of Technology, Cambridge, United States of America
  • Senior Editor
    Tadatsugu Taniguchi
    University of Tokyo, Tokyo, Japan

Reviewer #1 (Public Review):

Summary:

The manuscript by Kely C. Matteucc et al. titled "Reprogramming of host energy metabolism mediated by the TNF-iNOS-HIF-1α axis plays a key role in host resistance to Plasmodium infection" describes that TNF induces HIF-1α stabilization that increases GLUT1 expression as well as glycolytic metabolism in monocytic and splenic CD11b+ cells in P. chabaudi infected mice. Also, TNF signaling plays a crucial role in host energy metabolism, controlling parasitemia, and regulating the clinical symptoms in experimental malaria.

Weaknesses:

Even though iNOS deficiency reduced the expression of the glycolytic enzymes as well as reduced GLUT1 expression and lower ECAR in splenic monocytes, there is no data to support that RNI induces the expression and stabilization of HIF-1α.

This paper involves an incredible amount of work, and the authors have done an exciting study addressing the TNF-iNOS-HIF-1α axis as a critical role in host immune defense during Plasmodium infection.

Reviewer #2 (Public Review):

Summary:

The premise of the manuscript by Matteucci et al. is interesting and elaborates on a mechanism via which TNFa regulates monocyte activation and metabolism to promote murine survival during Plasmodium infection. The authors show that TNF signaling (via an unknown mechanism) induces nitrite synthesis, which (via yet an unknown mechanism), and stabilizes the transcription factor HIF1a. Furthermore, HIF1a (via an unknown mechanism) increases GLUT1 expression and increases glycolysis in monocytes. The authors demonstrate that this metabolic rewiring towards increased glycolysis in a subset of monocytes is necessary for monocyte activation including cytokine secretion, and parasite control.

Strengths:

The authors provide elegant in vivo experiments to characterize metabolic consequences of Plasmodium infection, and isolate cell populations whose metabolic state is regulated downstream of TNFa. Furthermore, the authors tie together several interesting observations to propose an interesting model.

Weaknesses:

The main conclusion of this work - that "Reprogramming of host energy metabolism mediated by the TNF-iNOS-HIF1a axis plays a key role in host resistance to Plasmodium infection" is unsubstantiated. The authors show that TNFa induces GLUT1 in monocytes, but never show a direct role for GLUT1 or glucose uptake in monocytes in host resistance to infection (nor the hypoglycemia phenotype they describe).

  1. Howard Hughes Medical Institute
  2. Wellcome Trust
  3. Max-Planck-Gesellschaft
  4. Knut and Alice Wallenberg Foundation