Publications by authors named "Justine Deroissart"

Article Synopsis
  • Atherosclerosis is a chronic inflammatory disease linked to lipid accumulation and is influenced by both innate and adaptive immune responses, particularly through changes in antibody levels.
  • Research shows that altering antibodies—whether through genetics or immunization—can either worsen or improve atherosclerosis in preclinical studies.
  • The text highlights the connection between various antibody types and their relationship to atherosclerotic cardiovascular disease, focusing on how specific antigens can trigger these antibody responses and affect disease progression.
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Recent studies have demonstrated a role for Ten-Eleven Translocation-2 (TET2), an epigenetic modulator, in regulating germinal center formation and plasma cell differentiation in B-2 cells, yet the role of TET2 in regulating B-1 cells is largely unknown. Here, B-1 cell subset numbers, IgM production, and gene expression were analyzed in mice with global knockout of TET2 compared to wildtype (WT) controls. Results revealed that TET2-KO mice had elevated numbers of B-1a and B-1b cells in their primary niche, the peritoneal cavity, as well as in the bone marrow (B-1a) and spleen (B-1b).

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Immunoglobulin M (IgM) to oxidation specific epitopes (OSE) are inversely associated with atherosclerosis in mice and humans. The B-1b subtype of B-1 cells secrete IgM to OSE, and unlike B-1a cells, are capable of long-lasting IgM memory. What attributes make B-1b cells different than B-1a cells is unknown.

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Hypercholesterolemia is a major risk factor in atherosclerosis development and lipid-lowering drugs (i.e., statins) remain the treatment of choice.

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