Publications by authors named "C Chague"

Background: Reinstating inflammation resolution represents an innovative concept to regain inflammation control in diseases marked by chronic inflammation. While most therapeutics target inflammatory molecules and inflammatory effector cells and mediators, targeting macrophages to initiate inflammation resolution to control neuroinflammation has not yet been attempted. Resolution-phase macrophages are critical in the resolution process to regain tissue homeostasis, and are programmed through the presence and elimination of apoptotic leukocytes.

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Cancers are consequences of cellular dysfunction leading to an aberrant cellular multiplication and proliferation, subsequently yielding metastasis formation. Inflammatory reaction, with immune cell recruitment, is the main defense against precancerous lesions. However, an inflammatory environment also favors cancer cell progression, with cancer cell evasion from immune surveillance, leading to cancer development.

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Article Synopsis
  • Acute graft-versus-host disease (aGVHD) poses a significant challenge to allogeneic hematopoietic cell transplantation, often triggered by lipopolysaccharides (LPS) from gut bacteria.
  • Research in mouse models indicated that ineffective clearance of LPS due to low HDL levels led to increased aGVHD severity.
  • Administering HDL from human plasma showed promise in reducing aGVHD mortality and severity by modulating immune responses and lowering inflammation.
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Nonresolving inflammation is a critical driver of several chronic inflammatory diseases, including inflammatory bowel diseases (IBD). This unresolved inflammation may result from the persistence of an initiating stimulus or from the alteration of the resolution phase of inflammation. Elimination of apoptotic cells by macrophages (a process called efferocytosis) is a critical step in the resolution phase of inflammation.

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