Bromohydrin pyrophosphate enhances antibody-dependent cell-mediated cytotoxicity induced by therapeutic antibodies

Gertner-Dardenne, Julie; Bonnafous, Cécile; Bezombes, Christine; Capietto, Aude-Hélène; Scaglione, Virginie; Ingoure, Sophie; Cendron, Delphine; Gross, Emilie; Lepage, Jean‐François; Quillet‐Mary, Anne; Ysebaert, Loïc; Laurent, Guy; Sicard, Hélène; Fournié, Jean‐Jacques

doi:10.1182/blood-2008-08-172296

Cited by 121 publications

(138 citation statements)

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“…In a B-cell depletion assay from cynomolgus monkeys treated with a phosphoantigen plus interleukin-2 (IL-2) and rituximab, endogenous cytotoxic cd T cells were enriched in lymph nodes in which CD20 1 B cells had been depleted. 15 Radiolabeling and imaging experiments (our unpublished results) have confirmed the observed cd cell accumulation at tumor sites, illustrating the capacity of these cells to infiltrate tumor sites in vivo. Additionally, when autologous transplants of In 111 -radiolabeled Vc9Vd2 T cells were tracked in 18 patients with advanced solid tumors, the radiolabeled cells trafficked predominantly to the lungs, liver and spleen, as well as to metastatic tumor sites outside of these organs in some patients.…”

Section: Rationale For Harnessing CD Cells In Cancer Immunotherapysupporting

confidence: 55%

“…Given these findings, the conditions for safe and efficient use of BrHPP/IL-2 in patients have now been determined. Given BrHPP's safety profile, its in vivo bioactivity and its use in a preclinical study with BrHPP/IL-2 and rituximab in NHL patients, 15 a multicentric phase II study using the drug was launched by Innate Pharma in relapsed follicular lymphoma patients. This study involved 45 follicular lymphoma patients who had previously received (up to four) previous lines of therapy using rituximab, at least once.…”

Section: Rationale For Harnessing CD Cells In Cancer Immunotherapymentioning

confidence: 99%

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What lessons can be learned from γδ T cell-based cancer immunotherapy trials?

et al. 2012

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During the last several years, research has produced a significant amount of knowledge concerning the characteristics of human cd T lymphocytes. Findings regarding the immune functions of these cells, particularly their natural killer cell-like lytic activity against tumor cells, have raised expectations for the therapeutic applications of these cells for cancer. Pharmaceutical companies have produced selective agonists for these lymphocytes, and several teams have launched clinical trials of cd T cell-based cancer therapies. The findings from these studies include hematological malignancies (follicular lymphoma, multiple myeloma, acute and chronic myeloid leukemia), as well as solid tumors (renal cell, breast and prostate carcinomas), consisting of samples from more than 250 patients from Europe, Japan and the United States. The results of these pioneering studies are now available, and this short review summarizes the lessons learned and the role of cd T cell-based strategies in the current landscape of cancer immunotherapies.

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Section: Rationale For Harnessing CD Cells In Cancer Immunotherapysupporting

confidence: 55%

Section: Rationale For Harnessing CD Cells In Cancer Immunotherapymentioning

confidence: 99%

What lessons can be learned from γδ T cell-based cancer immunotherapy trials?

et al. 2012

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“…Studies on the mechanism of action of therapeutic mAbs (such as Trastuzumab and Rituximab) used in breast cancer and lymphomas suggest an important role for ADCC mediated by CD16 [38 , 39].NK and  T cells have been shown to actively participate in the ADCC of cancer cells coated with therapeutic mAbs [8][9][10]. Since many cancers over-express COX2 and produce high amounts of PGE 2 [16,17], the ability of PGE 2 to down regulate NK and  T cells cytotoxicity triggered by CD16 might be involved in the numerous cases of tumor resistance to treatment with mAbs depicted until now [39].…”

Section: Resultsmentioning

confidence: 99%

“…Thus, a strong activation of TCR V9V2 did not thwart inhibition of  T cell functions by PGE 2 . Since other activating receptors such as NKG2D and CD16 also participate in the recognition and destruction of target cells by  T cells [5,10], we wanted to determine if PGE 2 …”

Section: Pge 2 Inhibits the Responses Of  T Cells Mediated By Tcr Vmentioning

confidence: 99%

“…NK and  T cells highly express NKG2D (a lectin-like type II transmembrane homodimer), a receptor allowing them to respond to ligands (MICA, MICB and ULBP 1-4) upregulated during oncogenic transformation and stress [5][6][7]. CD16 (a FcRIII receptor) expressed by NK and  T cells plays an important role in Antibody Dependant Cell Cytotoxicity (ADCC) which is of particular clinical interest with the increasing number of anti-cancer therapies using monoclonal antibodies [8][9][10]. Finally, NK cells also express NCR (NKp30, NKp44 and NKp46) that are critically involved in tumor cell recognition [11].…”

Section: Introductionmentioning

confidence: 99%

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PGE2 inhibits natural killer and γδ T cell cytotoxicity triggered by NKR and TCR through a cAMP-mediated PKA type I-dependent signaling

Martinet¹,

Jean²,

Dietrich³

et al. 2010

Biochemical Pharmacology

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inhibits Natural Killer and γδ T cell cytotoxicity triggered by NKR and TCR through a cAMPmediated PKA type I-dependent signaling. Biochemical Pharmacology, Elsevier, 2010, 80 (6) This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of the resulting proof before it is published in its final form. Please note that during the production process errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain.

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Functional and metabolic dichotomy of murine γδ T cell subsets in cancer immunity

Lopes

Silva‐Santos

2020

Eur J Immunol

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γδ T cells can display a plethora of immune functions, but recent studies have highlighted their importance, in multiple disease models, as sources of the pro‐inflammatory cytokines, IL‐17A (IL‐17), and IFN‐γ. These are produced by distinct murine effector γδ T cell subsets that diverge during thymic γδ T cell development. Among the multiple roles these subsets play in peripheral tissues, a striking dichotomy has emerged at tumor sites: whereas IFN‐γ + γδ T cells inhibit tumor cell growth, IL‐17 + γδ T cells promote tumor progression and metastasis formation. In this review, we discuss the main lines of evidence, mostly from preclinical studies in mouse models, for this functional dichotomy in cancer immunity. We further highlight very recent advances in our understanding how metabolic sources and pathways can impact on the balance between IFN‐γ + and IL‐17 + γδ T cells in the tumor microenvironment, which opens a new exciting avenue to explore toward the application of γδ T cells in cancer immunotherapy.

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Bromohydrin pyrophosphate enhances antibody-dependent cell-mediated cytotoxicity induced by therapeutic antibodies

Cited by 121 publications

References 50 publications

What lessons can be learned from γδ T cell-based cancer immunotherapy trials?

What lessons can be learned from γδ T cell-based cancer immunotherapy trials?

PGE2 inhibits natural killer and γδ T cell cytotoxicity triggered by NKR and TCR through a cAMP-mediated PKA type I-dependent signaling

Functional and metabolic dichotomy of murine γδ T cell subsets in cancer immunity

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