3BP2 Deficiency Impairs the Response of B Cells, but Not T Cells, to Antigen Receptor Ligation

Fuente, Miguel A. de la; Kumar, Lalit; Lu, Bao; Geha, Raif S.

doi:10.1128/mcb.00087-06

Cited by 45 publications

(75 citation statements)

References 64 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Osteoclasts from DAP12 ϫ FcR␥-null mice exhibit defectiveNFATc1expressionasaconsequenceofimpairedPLC␥-dependent calcium signaling (6). Of note, B cells from 3BP2 Ϫ/Ϫ mice show impaired PLC␥ phosphorylation, calcium mobilization, and NFAT activation (24). Our observations that in myeloid cells 3BP2 forms a signaling complex with c-Src, Syk, Vav, and Cbl provide a mechanistic explanation of how 3BP2 might participate in RANK-mediated osteoclast formation.…”

Section: Discussionmentioning

confidence: 68%

“…Consistently, 3BP2 was found to positively regulate the activity of NFAT in T and B cells (21,23). In addition, studies in mouse deficient for 3BP2 expression have shown that 3BP2 regulates B cell development and BCR-mediated B cell activation and calcium mobilization (24,25). Finally, genetic evidence linking 3BP2 to the human genetic bone disease cherubism (31,32) indicates that 3BP2 also plays a crucial role during inflammation and bone remodeling.…”

mentioning

confidence: 87%

“…These scaffolds transduce signals to the cytoplasm, cytoskeleton, and nucleus to activate lipid and calcium signaling, gene expression, and metabolic changes involved in leukocyte proliferation, differentiation, and motility. We and others have identified a regulatory role for 3BP2 (c-Abl SH3 domainbinding protein-2, also known as SH3BP2) in immunoreceptor signaling, including T (21,22), B (23)(24)(25)(26), NK (27), and mast (28) cells. Importantly, 3BP2 associates several signaling proteins such as Src/Syk kinases, Vav proteins, and PLC␥, involved in NFAT activation (reviewed in Refs.…”

mentioning

confidence: 99%

See 2 more Smart Citations

3BP2 Adapter Protein Is Required for Receptor Activator of NFκB Ligand (RANKL)-induced Osteoclast Differentiation of RAW264.7 Cells

Guezguez

Prod’homme

Mouska

et al. 2010

Journal of Biological Chemistry

View full text Add to dashboard Cite

The adapter protein 3BP2 (also known as SH3BP2 and Abl SH3-binding protein 2) has been involved in leukocyte signaling and activation downstream immunoreceptors. Genetic studies have further associated 3BP2 mutations to the human disease cherubism and to inflammation and bone dysfunction in mouse. However, how wild type 3BP2 functions in macrophage differentiation remains poorly understood. In this study, using small interfering RNA-mediated silencing of 3BP2 in the RAW264.7 monocytic cell line, we show that 3BP2 was required for receptor activator of NFB ligand (RANKL)-induced differentiation of RAW264.7 cells into multinucleated mature osteoclasts but not for granulocyte macrophage-colony stimulating factor/interleukin-4-induced differentiation into dendritic cells. 3BP2 silencing was associated with impaired activation of multiple signaling events downstream of RANK, including actin reorganization; Src, ERK, and JNK phosphorylation; and up-regulation of osteoclastogenic factors. In addition, 3BP2 knockdown cells induced to osteoclast by RANKL displayed a reduced increase of Src and nuclear factor of activated T cells (NFATc1) mRNA and protein expression. Importantly, 3BP2 interacted with Src, Syk, Vav, and Cbl in monocytic cells, and the introduction of constitutively active mutants of Src and NFATc1 in 3BP2-deficient cells restored osteoclast differentiation. Finally, the expression of a 3BP2 cherubism mutant was found to promote increased Src activity and NFAT-dependent osteoclast formation. Together, this study demonstrates that wild type 3BP2 is a key regulator of RANK-mediated macrophage differentiation into osteoclast through Src and NFATc1 activation.

show abstract

Section: Discussionmentioning

confidence: 68%

mentioning

confidence: 87%

mentioning

confidence: 99%

See 1 more Smart Citation

3BP2 Adapter Protein Is Required for Receptor Activator of NFκB Ligand (RANKL)-induced Osteoclast Differentiation of RAW264.7 Cells

Guezguez

Prod’homme

Mouska

et al. 2010

Journal of Biological Chemistry

View full text Add to dashboard Cite

show abstract

“…Anti-PLC-␥2, anti-CD19, anti-Vav1, and anti-BLNK antibodies were from Santa Cruz Biotechnology (Santa Cruz, CA). Polyclonal anti-3BP2 antibody raised against an amino acid sequence from Leu 359 to Ser 462 of 3BP2, which is capable for the immunoprecipitation of 3BP2, was a gift from Dr. Raif S. Geha (Harvard Medical School) (32). Anti-glutathione S-transferase (GST) mAb was from Nacalai (Kyoto, Japan).…”

Section: Methodsmentioning

confidence: 99%

“…Suppression of the 3BP2 expression by small interfering RNA results in the inhibition of BCR and T cell receptor (TCR)-mediated activation of NFAT (25,31). Analysis of 3BP2-deficient mice demonstrated that 3BP2 is required for B cell proliferation and cell cycle progression (32,33). Lack of 3BP2 results in the abnormal phenotype in splenic marginal-zone B cells and peritoneal B1 B cells and diminished thymus-independent type 2 antigen response (33).…”

mentioning

confidence: 99%

Tyrosine Phosphorylation of 3BP2 Regulates B Cell Receptor-mediated Activation of NFAT

Shukla

Hatani

Nakashima

et al. 2009

Journal of Biological Chemistry

View full text Add to dashboard Cite

Loss of SH3 Domain–Binding Protein 2 Function Suppresses Bone Destruction in Tumor Necrosis Factor–Driven and Collagen‐Induced Arthritis in Mice

Mukai

Gallant

Ishida

et al. 2015

Arthritis & Rheumatology

View full text Add to dashboard Cite

Objective SH3BP2 is a signaling adapter protein which regulates immune and skeletal systems. The purpose of this study was to investigate the role of SH3BP2 in arthritis in human TNF-α transgenic (hTNFtg) and collagen-induced arthritis (CIA) models. Methods First, SH3BP2-deficient (Sh3bp2–/–) and wild-type (Sh3bp2+/+) mice were crossed with hTNFtg mice. Inflammation and bone loss were examined by clinical inspection and histological and micro-CT analyses. Osteoclastogenesis was evaluated with primary bone marrow-derived M-CSF-dependent macrophages (BMMs). Second, CIA was induced in Sh3bp2–/– and Sh3bp2+/+ mice, and the incidence and severity of arthritis were evaluated. Anti-mouse type II collagen (CII) antibody levels were measured by ELISA. Lymph node cell responses to CII were also determined. Results SH3BP2-deficiency did not alter the severity of joint swelling but suppressed bone erosion in the hTNFtg model. Bone loss of talus and tibia was prevented in Sh3bp2–/–/hTNFtg mice compared to Sh3bp2+/+/hTNFtg mice. RANKL- and TNF-α-induced osteoclastogenesis was suppressed in Sh3bp2–/– BMM cultures. NFATc1 nuclear localization in response to TNF-α was decreased in Sh3bp2–/– BMMs compared to Sh3bp2+/+ BMMs. In the CIA model, SH3BP2-deficiency suppressed the incidence of arthritis, which was associated with decreased anti-CII antibody production, while the antigen-specific T-cell responses in lymph nodes were not significantly different between Sh3bp2+/+ and Sh3bp2–/– mice. Conclusion SH3BP2-deficiency prevents bone loss via impaired osteoclastogenesis in the hTNFtg model and suppresses the induction of arthritis via decreased autoantibody production in the CIA model. Therefore, SH3BP2 could be a therapeutic target for rheumatoid arthritis.

show abstract

3BP2 Deficiency Impairs the Response of B Cells, but Not T Cells, to Antigen Receptor Ligation

Cited by 45 publications

References 64 publications

3BP2 Adapter Protein Is Required for Receptor Activator of NFκB Ligand (RANKL)-induced Osteoclast Differentiation of RAW264.7 Cells

3BP2 Adapter Protein Is Required for Receptor Activator of NFκB Ligand (RANKL)-induced Osteoclast Differentiation of RAW264.7 Cells

Tyrosine Phosphorylation of 3BP2 Regulates B Cell Receptor-mediated Activation of NFAT

Loss of SH3 Domain–Binding Protein 2 Function Suppresses Bone Destruction in Tumor Necrosis Factor–Driven and Collagen‐Induced Arthritis in Mice

Contact Info

Product

Resources

About