Your search keyword '"Julia Ritter"' showing total 3 results

1. Multinucleated Giant Cells Are Specialized for Complement-Mediated Phagocytosis and Large Target Destruction

Author

Ronny Milde, Julia Ritter, Glenys A. Tennent, Andrzej Loesch, Fernando O. Martinez, Siamon Gordon, Mark B. Pepys, Admar Verschoor, and Laura Helming

Subjects

Biology (General), QH301-705.5

Abstract

Multinucleated giant cells (MGCs) form by fusion of macrophages and are presumed to contribute to the removal of debris from tissues. In a systematic in vitro analysis, we show that IL-4-induced MGCs phagocytosed large and complement-opsonized materials more effectively than their unfused M2 macrophage precursors. MGC expression of complement receptor 4 (CR4) was increased, but it functioned primarily as an adhesion integrin. In contrast, although expression of CR3 was not increased, it became functionally activated during fusion and was located on the extensive membrane ruffles created by excess plasma membrane arising from macrophage fusion. The combination of increased membrane area and activated CR3 specifically equips MGCs to engulf large complement-coated targets. Moreover, we demonstrate these features in vivo in the recently described complement-dependent therapeutic elimination of systemic amyloid deposits by MGCs. MGCs are evidently more than the sum of their macrophage parts.

Published

2015

2. Multinucleated Giant Cells Are Specialized for Complement-Mediated Phagocytosis and Large Target Destruction

Author

Siamon Gordon, Laura Helming, Fernando O. Martinez, Ronny Milde, Admar Verschoor, Mark B. Pepys, Andrzej Loesch, Julia Ritter, and Glenys A. Tennent

Subjects

Macrophage colony-stimulating factor, Amyloid, Phagocytosis, Integrin alphaXbeta2, Bone Marrow Cells, Mice, Transgenic, Complement receptor, Giant Cells, Article, General Biochemistry, Genetics and Molecular Biology, Mice, Cricetinae, Macrophage fusion, Animals, Humans, Macrophage, lcsh:QH301-705.5, Mice, Knockout, Chemistry, Macrophage Colony-Stimulating Factor, Macrophages, Receptors, IgG, Complement C3, M2 Macrophage, ddc, CD11c Antigen, Rats, Up-Regulation, Cell biology, Mice, Inbred C57BL, lcsh:Biology (General), Giant cell, CD18 Antigens, Immunology, Tetradecanoylphorbol Acetate, Interleukin-4

Abstract

Summary Multinucleated giant cells (MGCs) form by fusion of macrophages and are presumed to contribute to the removal of debris from tissues. In a systematic in vitro analysis, we show that IL-4-induced MGCs phagocytosed large and complement-opsonized materials more effectively than their unfused M2 macrophage precursors. MGC expression of complement receptor 4 (CR4) was increased, but it functioned primarily as an adhesion integrin. In contrast, although expression of CR3 was not increased, it became functionally activated during fusion and was located on the extensive membrane ruffles created by excess plasma membrane arising from macrophage fusion. The combination of increased membrane area and activated CR3 specifically equips MGCs to engulf large complement-coated targets. Moreover, we demonstrate these features in vivo in the recently described complement-dependent therapeutic elimination of systemic amyloid deposits by MGCs. MGCs are evidently more than the sum of their macrophage parts., Graphical Abstract, Highlights • MGCs are specialized for phagocytosis of large and complement-opsonized particles • MGCs show extensive membrane ruffles containing pre-activated complement receptor 3 • Membrane ruffles provide excess membrane for ingestion of large materials • MGCs eliminate systemic amyloid deposits after immunotherapeutic targeting, Macrophage-derived multinucleated giant cells (MGCs) form in diverse chronic inflammatory diseases, but their functional role remains unclear. Milde et al. show that MGCs are specialized for complement-mediated phagocytosis and destruction of large targets and demonstrate their key role in the therapeutic elimination of the pathogenic amyloid deposits in systemic amyloidosis.

Published

2015

3. Branched-chain keto acids inhibit mitochondrial pyruvate carrier and suppress gluconeogenesis in hepatocytes

Author

Kiyoto Nishi, Akira Yoshii, Lauren Abell, Bo Zhou, Ricardo Frausto, Julia Ritterhoff, Timothy S. McMillen, Ian Sweet, Yibin Wang, Chen Gao, and Rong Tian

Subjects

CP: Metabolism, Biology (General), QH301-705.5

Abstract

Summary: Branched-chain amino acid (BCAA) metabolism is linked to glucose homeostasis, but the underlying signaling mechanisms are unclear. We find that gluconeogenesis is reduced in mice deficient of Ppm1k, a positive regulator of BCAA catabolism, which protects against obesity-induced glucose intolerance. Accumulation of branched-chain keto acids (BCKAs) inhibits glucose production in hepatocytes. BCKAs suppress liver mitochondrial pyruvate carrier (MPC) activity and pyruvate-supported respiration. Pyruvate-supported gluconeogenesis is selectively suppressed in Ppm1k-deficient mice and can be restored with pharmacological activation of BCKA catabolism by BT2. Finally, hepatocytes lack branched-chain aminotransferase that alleviates BCKA accumulation via reversible conversion between BCAAs and BCKAs. This renders liver MPC most susceptible to circulating BCKA levels hence a sensor of BCAA catabolism.

Published

2023