Mouse B7-H3 induces antitumor immunity

Sun, Xueying; Vale, Marcos Martinez do; Leung, Euphemia; Kanwar, Jagat R.; Gupta, Rakesh; Krissansen, Geoffrey W.

doi:10.1038/sj.gt.3302070

Cited by 115 publications

(113 citation statements)

References 25 publications

(39 reference statements)

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“…Lastly, while our data demonstrating a positive regulatory pathway for B7-H3 are consistent with other work [9,12,14], they differ from reports showing negative regulatory functions of mB7-H3 [15,16]. The reasons for this are unclear, though certainly different targeting strategies, assays, and models were employed.…”

Section: Discussionsupporting

confidence: 81%

“…mB7-H3.Ig was also found to bind to mitogen-activated but not resting mouse T cells [11], and in line with a proposed stimulatory function of human B7-H3, Sun et al [12] demonstrated that intratumoral injection of an mB7-H3 pcDNA3 expression plasmid led to complete regression of about 50% of the tumors. Subsequent studies of intratumor expression of B7-H3 from the Chen laboratory [14] (where B7-H3 was first described) showed a costimulatory effect of B7-H3 and enhanced tumor immunity in vivo and in vitro in a mouse model.…”

Section: Introductionmentioning

confidence: 80%

“…Studies in humans and mice have focused on B7-H3 expression by APC [9][10][11][12][13][14], such that we first assessed whether allogeneic responses were diminished in B7-H3 -/-mice as a result of diminished DC costimulatory function by co-culturing irradiated stimulator DC with allogeneic responder CD4 T cells. We found that BALB/c CD4 T cells had a 13% proliferation rate after co-culture with control C57BL/6 DC for 24 h, whereas the corresponding proliferation of CD4 T cells co-cultured with B7-H3 -/-DC was halved (Fig.…”

Section: B7-h3 Expression By DC and Alloactivation Of T Cells In Vitromentioning

confidence: 99%

“…The otherwise identical human B7-H3 and B7-H3b isoforms likely arose by gene duplication of two exons encoding the IgV-IgC domains of B7-H3 [11]. Mouse B7-H3 (mB7-H3) was subsequently cloned by two groups [11,12], mapped to chromosome 9 [11], and shown to have 88% amino acid sequence identity with human B7-H3, though the dual IgV-IgC structure was not found in mouse genomic DNA. Indeed, non-human primate B7-H3, like human B7-H3, is present in both single and duplicate IgV-IgC forms, whereas hamsters, like mice, possess only the single IgV-IgC form, consistent with broad evolutionary-based differences between primate and rodent B7-H3 [13].…”

Section: Introductionmentioning

confidence: 99%

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B7‐H3 promotes acute and chronic allograft rejection

et al. 2005

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The B7 homolog B7-H3 is important for the regulation of immune responses though its functions in vivo are controversial. We report the first clinical and experimental data concerning expression and function of B7-H3 in alloresponses. Immunohistological and molecular analyses showed B7-H3 expression by cells mediating rejection of human and mouse allografts. To analyze the significance of B7-H3 in rejecting allografts, we generated B7-H3 -/-mice and showed that targeting of B7-H3 was synergistic with other forms of immune modulation; e.g. a regimen of rapamycin gave 12-14 days of survival in wild-type controls but led to permanent cardiac and islet allograft survival in B7-H3 -/-mice. Cardiac allografts in treated B7-H3 -/-mice showed markedly decreased production of key cytokine, chemokine and chemokine receptor mRNA transcripts as compared to wild-type controls. The incidence of chronic rejection in two different cardiac allograft models was also inhibited in B7-H3 -/-as compared to wild-type recipients. Lastly, in addition to the expected antigen-presenting cell expression of B7-H3, CD4 and CD8 T cells showed B7-H3 induction upon cell activation, and both dendritic cell-and T cell-expressed B7-H3 each enhanced T cell proliferation in vitro and in vivo. We conclude that B7-H3 promotes T cell-mediated immune responses and the development of acute and chronic allograft rejection.

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Section: Discussionsupporting

confidence: 81%

Section: Introductionmentioning

confidence: 80%

Section: B7-h3 Expression By DC and Alloactivation Of T Cells In Vitromentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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B7‐H3 promotes acute and chronic allograft rejection

et al. 2005

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“…B7.1, a member of the B7 family, is located on the surface of antigen-presenting cells and is the natural ligand of CD28 on the T-cell surface (31,32). Through engagement of T-cell receptor with its cognate MHC molecules and B7.1 with CD28, interleukin-2-secreting CD4 + effector cells and CD8 + T cells will be maximally activated (31,32).…”

Section: Introductionmentioning

confidence: 99%

Induction of T-Cell Apoptosis in Rats by Genetically Engineered Glioma Cells Expressing Granulocyte-Macrophage Colony-Stimulating Factor and B7.1

Tseng¹,

Chen

Chang

et al. 2005

Clinical Cancer Research

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Human muscle cells express the costimulatory molecule B7‐H3, which modulates muscle–immune interactions

Waschbisch

Wintterle

Lochmüller

et al. 2008

Arthritis & Rheumatism

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Objective. Interactions between the family of B7 ligands and their receptors are increasingly recognized as crucial for stimulation and/or inhibition of immune responses. The present study was undertaken to examine the expression and functional relevance of B7 homolog 3 (B7-H3), a novel B7 homolog attributed significant immunoregulatory functions, in human muscle cells in vivo and in vitro.Methods. Thirty-five muscle biopsy specimens obtained from patients with polymyositis, dermatomyositis, inclusion body myositis, or noninflammatory myopathies and normal controls were analyzed by immunohistochemistry for B7-H3 expression. The expression of B7-H3 protein on primary human myoblasts and TE671 muscle rhabdomyosarcoma cells was studied by flow cytometry and Western blot analysis. B7-H3 small interfering RNA (siRNA) was used to study the impact of knockdown of B7-H3 on CD8؉ cell-mediated lysis in skeletal muscle cells.Results. B7-H3 was not detectable on normal muscle fibers. In contrast, its expression was markedly increased on muscle fibers from patients with inflammatory myopathies. Cell-surface staining was most prominent in the contact areas between muscle fibers and inflammatory cells. B7-H3 protein was detected on myoblasts cultured from control and myositis patient muscle tissue as well as in TE671 muscle rhabdomyosarcoma cells. Knockdown of B7-H3 by siRNA in TE671 cells enhanced CD8؉ T cell-specific lysis, indicating a functional role of B7-H3 in the protection of skeletal muscle from immune-mediated lysis.Conclusion. Our results demonstrate that human muscle cells express B7-H3, a functional coinhibitory molecule of the B7 family. B7-H3 may play an important role in muscle-immune interactions, providing further evidence of the active role of muscle cells in local immunoregulatory processes.

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Mouse B7-H3 induces antitumor immunity

Cited by 115 publications

References 25 publications

B7‐H3 promotes acute and chronic allograft rejection

B7‐H3 promotes acute and chronic allograft rejection

Induction of T-Cell Apoptosis in Rats by Genetically Engineered Glioma Cells Expressing Granulocyte-Macrophage Colony-Stimulating Factor and B7.1

Human muscle cells express the costimulatory molecule B7‐H3, which modulates muscle–immune interactions

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