Mutant RBL Mast Cells Defective in FcεRI Signaling and Lipid Raft Biosynthesis Are Reconstituted by Activated Rho-family GTPases

Author:

Field Kenneth A.1,Apgar John R.2,Hong-Geller Elizabeth3,Siraganian Reuben P.4,Baird Barbara1,Holowka David1

Affiliation:

1. Department of Chemistry and Chemical Biology, Cornell University, Ithaca, New York;

2. Scripps Research Institute, LaJolla, California 92093;

3. Department of Molecular Medicine, Cornell University, Ithaca, New York 14853, and

4. NIDCR, National Institutes of Health, Bethesda, Maryland 21814

Abstract

Characterization of defects in a variant subline of RBL mast cells has revealed a biochemical event proximal to IgE receptor (FcεRI)-stimulated tyrosine phosphorylation that is required for multiple functional responses. This cell line, designated B6A4C1, is deficient in both FcεRI-mediated degranulation and biosynthesis of several lipid raft components. Agents that bypass receptor-mediated Ca2+ influx stimulate strong degranulation responses in these variant cells. Cross-linking of IgE-FcεRI on these cells stimulates robust tyrosine phosphorylation but fails to mobilize a sustained Ca2+ response. FcεRI-mediated inositol phosphate production is not detectable in these cells, and failure of adenosine receptors to mobilize Ca2+ suggests a general deficiency in stimulated phospholipase C activity. Antigen stimulation of phospholipases A2 and D is also defective. Infection of B6A4C1 cells with vaccinia virus constructs expressing constitutively active Rho family members Cdc42 and Rac restores antigen-stimulated degranulation, and active Cdc42 (but not active Rac) restores ganglioside and GPI expression. The results support the hypothesis that activation of Cdc42 and/or Rac is critical for FcεRI-mediated signaling that leads to Ca2+ mobilization and degranulation. Furthermore, they suggest that Cdc42 plays an important role in the biosynthesis and expression of certain components of lipid rafts.

Publisher

American Society for Cell Biology (ASCB)

Subject

Cell Biology,Molecular Biology

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1. RhoGDI in RBL-2H3 cells acts as a negative regulator of Rho GTPase signaling to inhibit granule exocytosis;Journal of Leukocyte Biology;2024-06-29

2. The effect of Rho drugs on mast cell activation and degranulation;Journal of Leukocyte Biology;2017-04-14

3. Rotation of Single Cell Surface Receptors Examined by Quantum Dot Probes;Springer Series in Biophysics;2017

4. Mast cell desensitization inhibits calcium flux and aberrantly remodels actin;Journal of Clinical Investigation;2016-09-26

5. Roles for lipid heterogeneity in immunoreceptor signaling;Biochimica et Biophysica Acta (BBA) - Molecular and Cell Biology of Lipids;2016-08

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