Your search keyword '"Feldman, Gerald M."' showing total 15 results

1. The many faces of FcγRI: implications for therapeutic antibody function.

Author

Swisher, Jennifer F. A. and Feldman, Gerald M.

Subjects

*FC receptors, *THERAPEUTIC use of immunoglobulins, *TYROSINE, *PHAGOCYTOSIS, *REACTIVE oxygen species, *ANTI-inflammatory agents, *IMMUNE complexes

Abstract

Fcγ receptor I (Fcγ RI or CD64) is the sole human Fc receptor with high affinity for monovalent IgG. While it contains an immunoreceptor tyrosine-based activation motif in its cytoplasmic domain, binding of Fcγ RI can result in a complex array of activating and inhibitory outcomes. For instance, binding of monomeric IgG provides a low-intensity tonic signal through Fcγ RI that is necessary for full interferon γ receptor signaling in the same cell. Interaction of Fcγ RI with larger high-avidity complexes can result in phagocytosis, the generation of reactive oxygen species, as well as the synthesis and release of inflammatory cytokines. However, numerous reports also document potent anti-inflammatory effects brought about by Fcγ RI engagement with immune complexes such as the inhibition of IFNγ and TLR4 signaling, and secretion of interleukin-10. This has led to conflicting hypotheses regarding the function of Fcγ RI, especially with regard to its role in the efficacy of several therapeutic monoclonal antibodies. While many of these issues are still unclear, continued characterization of the regulation and context dependence of Fcγ RI function, as well as the molecular mechanisms responsible for these various outcomes, will improve our understanding of Fcγ RI biology as well as the therapeutic strategies designed to harness or constrain its actions. [ABSTRACT FROM AUTHOR]

Published

2015

2. Mechanistic Insights into the Successful Development of Combination Therapy of Enfortumab Vedotin and Pembrolizumab for the Treatment of Locally Advanced or Metastatic Urothelial Cancer.

Author

Taylor, Caroline, Patterson, Kamai M., Friedman, Devira, Bacot, Silvia M., Feldman, Gerald M., and Wang, Tao

Subjects

*THERAPEUTIC use of monoclonal antibodies, *COMBINATION drug therapy, *CANCER invasiveness, *TREATMENT effectiveness, *IMMUNE checkpoint inhibitors, *MONOCLONAL antibodies, *METASTASIS, *TRANSITIONAL cell carcinoma, *CANCER chemotherapy, *DRUG resistance, *PHARMACODYNAMICS, BLADDER tumors

Abstract

Simple Summary: Antibody–drug conjugates (ADCs) and immune checkpoint inhibitors (ICIs) are two promising therapeutic modalities against many types of cancers. However, many patients develop resistance. The resistance mechanisms to ADCs and ICIs have been comprehensively illuminated in this review. A combination of ADCs and ICIs has been explored to overcome resistance to ADC or ICI single treatment. Recently, a clinical study demonstrated that a combination of enfortumab vedotin (EV), an ADC against Nectin-4, with the ICI pembrolizumab achieves remarkable clinical efficacy as the first-line therapy for the treatment of locally advanced or metastatic urothelial carcinoma. The underlying mechanism is likely due to the enhancement of pembrolizumab-induced anticancer immunity mediated by EV. With the emerging use of combination therapy strategy, it is critical to understand the mechanism of successful and/or failed clinical studies for the future development of combination therapy of ADCs with ICIs. Antibody–drug conjugates (ADCs) consist of an antibody backbone that recognizes and binds to a target antigen expressed on tumor cells and a small molecule chemotherapy payload that is conjugated to the antibody via a linker. ADCs are one of the most promising therapeutic modalities for the treatment of various cancers. However, many patients have developed resistance to this form of therapy. Extensive efforts have been dedicated to identifying an effective combination of ADCs with other types of anticancer therapies to potentially overcome this resistance. A recent clinical study demonstrated that a combination of the ADC enfortumab vedotin (EV) with the immune checkpoint inhibitor (ICI) pembrolizumab can achieve remarkable clinical efficacy as the first-line therapy for the treatment of locally advanced or metastatic urothelial carcinoma (la/mUC)—leading to the first approval of a combination therapy of an ADC with an ICI for the treatment of cancer patients. In this review, we highlight knowledge and understanding gained from the successful development of EV and the combination therapy of EV with ICI for the treatment of la/mUC. Using urothelial carcinoma as an example, we will focus on dissecting the underlying mechanisms necessary for the development of this type of combination therapy for a variety of cancers. [ABSTRACT FROM AUTHOR]

Published

2024

3. The macrophage: Switches from a passenger to a driver during anticancer therapy.

Author

Wang, Tao, Feldman, Gerald M, Herlyn, Meenhard, and Kaufman, Russel E

Subjects

*BRAF genes, *ANTIBODY-dependent cell cytotoxicity, *MACROPHAGE inflammatory proteins, *ANTINEOPLASTIC agents, *MELANOMA prognosis

Abstract

We have recently discovered that BRAF inhibitors induce potent macrophage responses that confer melanoma resistance to therapy. Our studies lay a foundation for the hypothesis that macrophages switch their role from a passenger to a driver for tumor survival during therapeutic treatment, suggesting that agents that target macrophages can be an important component of “cocktail” anticancer therapy. [ABSTRACT FROM AUTHOR]

Published

2015

4. Hck Is a Key Regulator of Gene Expression in Alternatively Activated Human Monocytes.

Author

Bhattacharjee, Ashish, Pal, Srabani, Feldman, Gerald M., and Cathcart, Martha K.

Subjects

*GENE expression, *GENETIC regulation, *MONOCYTES, *CYTOKINES, *INTERLEUKIN-13, *LIPOXYGENASES, *PHOSPHORYLATION, *PROTEIN-tyrosine kinases

Abstract

IL-13 is a Th2 cytokine that promotes alternative activation (M2 polarization) in primary human monocytes. Our studies have characterized the functional IL-13 receptor complex and the downstream signaling events in response to IL-13 stimulation in alternatively activated monocytes/macrophages. In this report, we present evidence that IL-13 induces the activation of a Src family tyrosine kinase, which is required for IL-13 induction of M2 gene expression, including 15-lipoxygenase (15-LO). Our data show that Src kinase activity regulates IL-13-induced p38 MAPK tyrosine phosphorylation via the upstream kinases MKK3 or MKK6. Our findings also reveal that the IL-13 receptor-associated tyrosine kinase Jak2 is required for the activation of both Src kinase as well as p38 MAPK. Further, we found that Src tyrosine kinase-mediated activation of p38 MAPK is required for Stat1 and Stat3 serine 727 phosphorylation in alternatively activated monocytes/macrophages. Additional studies identify Hck as the specific Src family member, stimulated by IL-13 and involved in regulating both p38 MAPK activation and p38 MAPK-mediated 15-LO expression. Finally we show that the Hck regulates the expression of other alternative state (M2)-specific genes (Mannose receptor, MAO-A, and CD36) and therefore conclude that Hck acts as a key regulator controlling gene expression in alternatively activated monocytes/macrophages. [ABSTRACT FROM AUTHOR]

Published

2011

5. In vivo validation of signaling pathways regulating human monocyte chemotaxis

Author

Bhattacharjee, Ashish, Mishra, Ravi S., Feldman, Gerald M., and Cathcart, Martha K.

Subjects

*MONOCYTES, *CHEMOTAXIS, *IMMUNOLOGY, *DISEASES

Abstract

Abstract: Identification of novel signal transduction pathways regulating monocyte chemotaxis can indicate unique targets for preventive therapies for treatment of chronic inflammatory diseases. To aid in this endeavor we report conditions for optimal transfection of primary human monocytes coupled with a new model system for assessing their chemotactic activity in vivo. This method can be used as a tool to identify the relevant signal transduction pathways regulating human monocyte chemotaxis to MCP-1 in the complex in vivo environment that were previously identified to regulate chemotaxis in vitro. MCP-1-dependent chemotaxis of monocytes is studied in an adoptive transfer model where human monocytes transfected with mutant cDNAs are transferred to mice followed by initiation of peritonitis. Harvesting peritoneal cells at 24 h diminishes the contribution of immunologic responses to the cross-species transfer. Validation of relevant regulatory molecules in vivo is critical for understanding the most relevant therapeutic targets for drug development. [Copyright &y& Elsevier]

Published

2008

6. Immune Complexes Suppress IFN-γ-Induced Responses in Monocytes by Activating Discrete Members of the SRC Kinase Family.

Author

Boekhoudt, Gunther H., McGrath, Anna G., Swisher, Jennifer F. A., and Feldman, Gerald M.

Subjects

*REMOVAL of immune complexes, *MONOCYTES, *SRC gene, *IMMUNOSUPPRESSION, *PHOSPHOTYROSINE

Abstract

The regulation of the innate and the adaptive immune responses are extensively intertwined and tightly regulated. Ag-driven immune responses that are modulated by immune complexes (ICs) are known to inhibit IFN-γ-dependent MHC class II expression. We have previously demonstrated that ICs dramatically inhibit IFN-γ-induced activation of human monocytes through the activation of the FcγRI signaling pathway. In the present study we further explore the mechanisms by which ICs regulate IFN-y activation of human monocytes. We demonstrate that members of the SRC kinase family (SKF) are key mediators of IFN-y pathway suppression: inhibitors of the SKF reverse the ability of ICs to suppress IFN-y signaling. Small interfering RNA was used to target specific members of the SKF. The data indicate that SRC and LYN are both required for ICs to elicit their immunosuppressive activity, whereas FYN does not appear to contribute to this function. Similarly, the kinase SYK, though not a member of the SKF, is also demonstrated to be involved in this IC-mediated immunosuppression. Our data suggest a mechanism whereby ICs directly inhibit inflammatory signals by crosslinking FcγRI, resulting in the activation of the specific phosphotyrosine kinases SRC, LYN, and SYK and the concomitant suppression of the IFN-γ signaling pathway. [ABSTRACT FROM AUTHOR]

Published

2015

7. Role of Protein Kinase C Isoforms in the Regulation of Interleukin-13-induced 15-Lipoxygenase Gene Expression in Human Monocytes.

Author

Bo Xu, Bhattacharjee, Ashish, Roy, Biswajit, Feldman, Gerald M., and Cathcart, Martha K.

Subjects

*PROTEIN kinase C, *INTERLEUKINS, *LIPOXYGENASES, *GENE expression, *MONOCYTES, *PHOSPHORYLATION

Abstract

We reported previously that interleukin-13 (IL-13) induces tyrosine phosphorylation/activation of Jak2 and Tyk2 kinases and Stats 1, 3, 5, and 6 in primary human monocytes. We recently revealed that p38 MAPK-mediated serine phosphorylation of both Stat1 and Stat3 is required for the induction of 15-lipoxygenase (15-LO) expression by IL-13. In this study, we present data indicating that another serine/threonine kinase, PKCδ, is also required for IL-13-induced 15-LO expression. PKCδ, a member of the novel protein kinase C (PKC) subclass, was rapidly phosphorylated and activated upon exposure to IL-13. Treatment of cells with rottlerin, a PKCδ inhibitor, blocked IL-13-induced 15-LO mRNA and protein expression, whereas Go6976, an inhibitor of the conventional PKC subclass, had no inhibitory effects. Down-regulation of cellular PKCδ protein levels by PKCδ-specific antisense oligodeoxyribonucleotides also inhibited 15-LO expression markedly. IL-13-induced 15-LO expression resulted in significant inhibition of synthesis of the potent chemotactic factor leukotriene B4, and that process was reversed by rottlerin, presumably through the blockage of PKCδ-dependent 15-LO expression. Furthermore, our data demonstrate that IL-13-mediated activation of PKCδ and p38 MAPK are independent pathways, because inhibition of one kinase activity had no effect on the other, suggesting that the two pathways act in parallel to regulate the downstream targets necessary for 15-LO expression. Inhibition of PKCδ activation by rottlerin also markedly attenuated IL-13-induced Stat3 DNA binding activity. Our findings indicate that PKCδ plays an important role in regulating IL-13-induced 15-LO expression in human monocytes and subsequently modulates the inflammatory responses mediated by 15-LO products. [ABSTRACT FROM AUTHOR]

Published

2004

8. Interleukin-13 Induction of 15-LIpoxygenase Gene Expression Requires p38 Mitogen-Activated Protein Kinase-Mediated Serine 727 Phosphorylation of Stat1 and Stat3.

Author

Bo Xu, Bhattacharjee, Ashish, Roy, Biswajit, Hong-Min Xu, Anthony, David, Frank, David A., Feldman, Gerald M., and Cathcart, Martha K.

Subjects

*INTERLEUKINS, *GENE expression, *PHOSPHORYLATION, *PROTEIN kinases

Abstract

Interleukin-13 (IL-3) is a cytokine secreted by Th2 lymphocytes that is capable of inducing expression of 15-lipoxygenase (15-LO) in primary human monocytes. We recently demonstrated that induction of 15-LO requires the activation of Jak2 and Tyk2 kinases and Stats 1, 3, 5, and 6. Since IL-13-induced 15-LO expression was inhibited by H7 (a serine-threonine kinase inhibitor), we predicted that Stat serine phosphorylation may also be crucial for 15-LO expression. In this study, we present evidence indicating that IL-13-induced 15-LO mRNA expression was detectable as early as 1 h by real-time reverse transcription-PCR. We found that IL-13 induced a time-dependent serine phosphorylation of both Stat1 and Stat3, detectable at 15 min after IL-13 treatment. In addition, the activation of p38 mitogen-activated protein kinase (MAPK) was detected in a time-dependent fashion, with peak phosphorylation at 15 min after IL-13 treatment. SB202190, a p38 MAPKspecific inhibitor, markedly inhibited IL-13-induced Stat1 and Stat3 serine phosphorylation as well as DNA binding. Furthermore, treatment of cells with Stat1 or Stat3 decoys significantly impaired IL-13-induced 15-LO expression. Taken together, our results provide the first evidence that IL-13 induces p38 MAPK phosphorylation/activation, which regulates Stat1 and Stat3 serine 727 phosphorylation. Both of these events are important steps in IL-13-induced 15-LO expression in human monocytes. [ABSTRACT FROM AUTHOR]

Published

2003

9. Nucleoporation of dendritic cells: efficient gene transfer by electroporation into human monocyte-derived dendritic cells1<FN ID="FN1"><NO>1</NO>Disclaimer: The opinions expressed in this article are those of the author and not necessarily those of the Food and Drug Administration or the U.S. Government. The publication of this article should not be construed as an endorsement or approval of either the product or the company.</FN>

Author

Lenz, Petra, Bacot, Silvia M., Frazier-Jessen, Michelle R., and Feldman, Gerald M.

Subjects

*DENDRITIC cells, *GENE therapy, *MONOCYTES

Abstract

Dendritic cells (DCs) are ideal accessory cells in the developing field of gene therapy. Although viral transfection of DCs has become widespread, non-viral transfection of DCs has shown disappointing results. Recently, a new technique for transfecting primary cells has become available – the Amaxa Nucleofector™. Here, we describe the use of this device in the successful non-viral transfection of human monocyte-derived DCs. Using enhanced green fluorescent protein as a reporter gene DCs were transfectable with efficiencies approaching 60%, remaining responsive to lipopolysaccharide-stimulated cytokine production in short-term experiments (though long-term functional assays were hampered by loss of viability). Although these data demonstrate the ease and efficiency with which human monocyte-derived DCs can now be non-virally transfected, they also suggest the limitations of this technology due to the gradual loss of cell viability. The potential use of this system in the development of DC-based cell and gene therapies will be hampered until cell viability can be maintained. [Copyright &y& Elsevier]

Published

2003

10. STAT4 serine phosphorylation is critical for IL-12-induced IFN-γ production but not for cell proliferation.

Author

Morinobu, Akio, Gadina, Massimo, Strober, Warren, Visconti, Roberta, Fornace, Albert, Montagna, Cristina, Feldman, Gerald M., Nishikomon, Ryuta, and O'Shea, John J.

Subjects

*INTERFERONS, *IMMUNE response, *CELLULAR signal transduction, *PROTEIN kinases

Abstract

Examines the role of T helper differentiation and interferon (IFN) production in cell-mediated immune responses. Phosphorylation of signal transducer and activator of transcription 4 (STAT4) serine; Control of IFN by p38 mitogen-activated protein kinase; Mode of actions of STAT4-dependent transcription.

Published

2002

11. NF-κB elements contribute to junB inducibility by lipopolysaccharide in the murine macrophage cell line RAW264.7

Author

Frazier-Jessen, Michelle R., Thompson, Cynthia D., Brown, Robert, Rawat, Rashmi, Nordan, Richard P., and Feldman, Gerald M.

Subjects

*NF-kappa B, *MACROPHAGES

Abstract

Macrophages respond to bacterial lipopolysaccharide (LPS) by activating latent cis-acting factors that initiate transcription of immediate early genes. One such immediate early gene, junB, is induced by LPS in macrophages within 30 min. To identify elements that mediate the induction of junB by LPS, upstream and downstream sequences flanking the junB gene were examined by transient expression in the RAW264.7 murine macrophage cell line using a luciferase reporter gene vector containing the junB minimal promoter. A >10-fold enhancement was associated with a 222 bp region downstream of the junB promoter in response to LPS. Transient reporter assays demonstrated that multiple nuclear factor (NF) κB sites are required for inducibility of junB by LPS in RAW264.7 cells. Electrophoretic mobility shift assays confirmed binding of LPS-induced nuclear proteins included p50/p65 heterodimers at these NF-κB sites. [Copyright &y& Elsevier]

Published

2002

12. IL-10 Signaling Elicited by Nivolumab-Induced Activation of the MAP Kinase Pathway Does Not Fully Contribute to Nivolumab-Modulated Heterogeneous T Cell Responses.

Author

Harper, Taylor A., Bacot, Silvia M., Fennell, Christie Jane, Matthews, Rebecca L., Zhu, Christina, Yue, Peng, Benton, Alexander, Friedman, Devira, Akue, Adovi, KuKuruga, Mark A., Lee, Shiowjen, Wang, Tao, and Feldman, Gerald M.

Subjects

*T cells, *IMMUNE checkpoint proteins, *INTERLEUKIN-10, *IMMUNE checkpoint inhibitors, *CELL death, *NIVOLUMAB, *MITOGEN-activated protein kinases, *PROGRAMMED cell death 1 receptors

Abstract

Immune checkpoint inhibitor (ICI) therapy has revolutionized anti-cancer treatment for many late-stage cancer patients. However, ICI therapy has thus far demonstrated limited efficacy for most patients, and it remains unclear why this is so. Interleukin 10 (IL-10) is a cytokine that has been recognized as a central player in cancer biology with its ability to inhibit anti-tumor T cell responses. Recent studies suggest that IL-10 might also exert some intrinsic anti-tumor T cell responses, and clinical studies using recombinant IL-10 alone or in combination with ICI are underway. This paradoxical effect of IL-10 and its underlying mechanisms impacting ICI-modulated T cell responses remain poorly understood. In this study, using an in vitro mixed lymphocyte reaction assay, we found that treatment with ICIs such as the anti-programmed cell death receptor-1 (PD-1) mAb nivolumab elicits a strong expression of IL-10. While neutralization of IL-10 signaling with an anti-IL-10 specific mAb significantly decreases the production of IFN-γ by T cells in a cohort of donor cells, the opposite effect was observed in other donor cells. Similarly, neutralization of IL-10 signaling significantly decreases the expression of T cell activation markers Ki67 and CD25, as well as the production of Granzyme B in a cohort of donor cells, whereas the opposite effect was observed in others. Furthermore, we found that nivolumab and IL-10 differentially modulate the signal transducer and activator of transcription 3 (STAT3) and AKT serine–threonine kinase pathways. Finally, we found that nivolumab activates the mitogen-activated protein kinase (MAPK) pathway, which in turn is responsible for the observed induction of IL-10 production by nivolumab. These findings provide new insights into the mechanisms underlying anti-PD-1-modulated T cell responses by IL-10, which could lead to the discovery of novel combination treatments that target IL-10 and immune checkpoint molecules. [ABSTRACT FROM AUTHOR]

Published

2021

13. Exploring the Potential Use of a PBMC-Based Functional Assay to Identify Predictive Biomarkers for Anti-PD-1 Immunotherapy.

Author

Bacot, Silvia M., Harper, Taylor A., Matthews, Rebecca L., Fennell, Christie Jane, Akue, Adovi, KuKuruga, Mark A., Lee, Shiowjen, Wang, Tao, and Feldman, Gerald M.

Subjects

*SUPPRESSOR cells, *CELL physiology, *T cells, *BLOOD cells, *IMMUNOTHERAPY, *INTERLEUKIN-9, *T helper cells

Abstract

The absence of reliable, robust, and non-invasive biomarkers for anti- Programmed cell death protein 1 (PD-1) immunotherapy is an urgent unmet medical need for the treatment of cancer patients. No predictive biomarkers have been established based on the direct assessment of T cell functions, the primary mechanism of action of anti-PD-1 therapy. In this study, we established a model system to test T cell functions modulated by Nivolumab using anti-CD3 monoclonal antibody (mAb)-stimulated peripheral blood mononuclear cells (PBMCs), and characterized T cell functions primarily based on the knowledge gained from retrospective observations of patients treated with anti-PD-1 immunotherapy. During a comprehensive cytokine profile assessment to identify potential biomarkers, we found that Nivolumab increases expression of T helper type 1 (Th1) associated cytokines such as interferon-γ (IFN-γ) and interleukin-2 (IL-2) in a subset of donors. Furthermore, Nivolumab increases production of Th2, Th9, and Th17 associated cytokines, as well as many proinflammatory cytokines such as IL-6 in a subset of donors. Conversely, Nivolumab treatment has no impact on T cell proliferation, expression of CD25, CD69, or Granzyme B, and only modestly increases in the expansion of regulatory T cells. Our results suggest that assessment of cytokine production using a simple PBMC-based T cell functional assay could be used as a potential predictive marker for anti-PD-1 immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2020

14. BRAF and MEK inhibitors differentially affect nivolumab-induced T cell activation by modulating the TCR and AKT signaling pathways.

Author

Yue, Peng, Harper, Taylor, Bacot, Silvia M., Chowdhury, Monica, Lee, Shiowjen, Akue, Adovi, Kukuruga, Mark A., Wang, Tao, and Feldman, Gerald M.

Subjects

*T cells, *IPILIMUMAB, *T cell receptors, *MITOGEN-activated protein kinases, *MELANOMA, *CANCER treatment

Abstract

Immune checkpoint inhibitors (ICIs) such as the anti-PD-1 antibody Nivolumab, achieve remarkable clinical efficacy in patients with late stage cancers. However, only a small subset of patients benefit from this therapy. Numerous clinical trials are underway testing whether combining ICIs with other anti-cancer therapies can increase this response rate. For example, anti-PD-1/PD-L1 therapy combined with MAP kinase inhibition using BRAF inhibitors (BRAFi) and/or MEK inhibitors (MEKi) are in development for treatment of late stage melanomas. However, the benefits and underlying mechanisms of these combinatorial therapies remain unclear. In the current study, we assess the effects of MAPK inhibition on Nivolumab-induced T cell responses. Using an in vitro mixed lymphocyte reaction assay, we demonstrate that Nivolumab-induced T cell activation is highly heterogeneous. While BRAFi inhibits Nivolumab-induced cytokine production, T cell proliferation, activation markers (CD69, CD25), and Granzyme B in a substantial proportion of donor pairs, a small subset of donor pairs shows an additive effect. MEKi alone significantly inhibits Nivolumab-induced T cell activation; the addition of BRAFi significantly enhances this inhibitory effect. Mechanistically, the effects of BRAFi and/or MEKi on Nivolumab-induced T cell activation may be due to alteration of the activation of the AKT and T cell receptor (TCR) signaling pathways. Our results suggest that MAPK inhibition may not provide a clinical benefit for most melanoma patients being treated with anti-PD-1 therapy. [ABSTRACT FROM AUTHOR]

Published

2019

15. PS1-58 The role of STAT1 in regulation of mitochondrial gene expression

Author

Sisler, Jennifer D., Szelag, Magdalena, Potla, Ramesh, Zhang, Qifang, Szczepanek, Karol, Derecka, Marta, Wegrzyn, Joanna, Dulak, Jozef, Wenxin Zou, Hamed, Hossein, Timothy Shutt, Cichy, Joanna, Chen, Xiaomin, Baker, Darren P., Dent, Paul, Feldman, Gerald M., Shadel, Gerald, and Larner, Andrew C.

Published

2010