Your search keyword '"Jessica Dang"' showing total 11 results

1. Pro-phagocytic function and structural basis of GPR84 signaling

Author

Xuan Zhang, Yujing Wang, Shreyas Supekar, Xu Cao, Jingkai Zhou, Jessica Dang, Siqi Chen, Laura Jenkins, Sara Marsango, Xiu Li, Guibing Liu, Graeme Milligan, Mingye Feng, Hao Fan, Weimin Gong, and Cheng Zhang

Subjects

Science

Abstract

Abstract GPR84 is a unique orphan G protein-coupled receptor (GPCR) that can be activated by endogenous medium-chain fatty acids (MCFAs). The signaling of GPR84 is largely pro-inflammatory, which can augment inflammatory response, and GPR84 also functions as a pro-phagocytic receptor to enhance phagocytic activities of macrophages. In this study, we show that the activation of GPR84 by the synthetic agonist 6-OAU can synergize with the blockade of CD47 on cancer cells to induce phagocytosis of cancer cells by macrophages. We also determine a high-resolution structure of the GPR84-Gi signaling complex with 6-OAU. This structure reveals an occluded binding pocket for 6-OAU, the molecular basis of receptor activation involving non-conserved structural motifs of GPR84, and an unusual Gi-coupling interface. Together with computational docking and simulations studies, this structure also suggests a mechanism for the high selectivity of GPR84 for MCFAs and a potential routes of ligand binding and dissociation. These results provide a framework for understanding GPR84 signaling and developing new drugs targeting GPR84.

Published

2023

2. Effect of cabazitaxel on macrophages improves CD47-targeted immunotherapy for triple-negative breast cancer

Author

Jing Chen, Bo Xu, BoLei Li, Xu Cao, Jessica Dang, Siqi Chen, E Gulsen Gunes, Lei Tian, Sabina Muend, Mustafa Raoof, Christiane Querfeld, Jianhua Yu, Steven T. Rosen, Yingyu Wang, and Mingye Feng

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background Limited therapeutic options are available for triple-negative breast cancer (TNBC), emphasizing an urgent need for more effective treatment approaches. The development of strategies by targeting tumor-associated macrophages (TAMs) to stimulate their ability of Programmed Cell Removal (PrCR) provides a promising new immunotherapy for TNBC treatment.Methods CD47 is a critical self-protective “don’t eat me” signal on multiple human cancers against macrophage immunosurveillance. Using human and mouse TNBC preclinical models, we evaluated the efficacy of PrCR-based immunotherapy by blocking CD47. We performed high-throughput screens on FDA-approved anti-cancer small molecule compounds for agents potentiating PrCR and enhancing the efficacy of CD47-targeted therapy for TNBC treatment.Results We showed that CD47 was widely expressed on TNBC cells and TAMs represented the most abundant immune cell population in TNBC tumors. Blockade of CD47 enabled PrCR of TNBC cells, but the efficacy was not satisfactory. Our high-throughput screens identified cabazitaxel in enhancing PrCR-based immunotherapy. A combination of CD47 blockade and cabazitaxel treatment yielded a highly effective treatment strategy, promoting PrCR of TNBC cells and inhibiting tumor development and metastasis in preclinical models. We demonstrated that cabazitaxel potentiated PrCR by activating macrophages, independent of its cytotoxicity toward cancer cells. When treated with cabazitaxel, the molecular and phenotypic signatures of macrophages were polarized toward M1 state, and the NF-kB signaling pathway became activated.Conclusion The combination of CD47 blockade and macrophage activation by cabazitaxel synergizes to vastly enhance the elimination of TNBC cells. Our results show that targeting macrophages is a promising and effective strategy for TNBC treatment.

Published

2021

3. A Novel Approach to Achieve Long-Lasting Antitumor Immunity in Multiple Myeloma

Author

Metin Gunes, Jessica Dang, Yate-Ching Yuan, Idit Shachar, Murali Janakiram, Mingye Feng, Steven T. Rosen, and Emine Gulsen Gunes

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

4. Promoting antibody-dependent cellular phagocytosis for effective macrophage-based cancer immunotherapy

Author

Xu Cao, Jing Chen, Bolei Li, Jessica Dang, Wencan Zhang, Xiancai Zhong, Chongkai Wang, Mustafa Raoof, Zuoming Sun, Jianhua Yu, Marwan G. Fakih, and Mingye Feng

Subjects

Multidisciplinary, Phagocytosis, Cell Line, Tumor, Macrophages, Neoplasms, Antibodies, Monoclonal, Humans, Immunotherapy

Abstract

Macrophages are essential in eliciting antibody-dependent cellular phagocytosis (ADCP) of cancer cells. However, a satisfactory anticancer efficacy of ADCP is contingent on early antibody administration, and resistance develops along with cancer progression. Here, we investigate the mechanisms underlying ADCP and demonstrate an effective combinatorial strategy to potentiate its efficacy. We identified paclitaxel as a universal adjuvant that efficiently potentiated ADCP by a variety of anticancer antibodies in multiple cancers. Rather than eliciting cytotoxicity on cancer cells, paclitaxel polarized macrophages toward a state with enhanced phagocytic ability. Paclitaxel-treated macrophages down-regulated cell surface CSF1R whose expression was negatively correlated with patient survival in multiple malignancies. The suppression of CSF1R in macrophages enhanced ADCP of cancer cells, suggesting a role of CSF1R in regulating macrophage phagocytic ability. Together, these findings define a potent strategy for using conventional anticancer drugs to stimulate macrophage phagocytosis and promote the therapeutic efficacy of clinical anticancer antibodies.

Published

2022

5. Targeting macrophages for enhancing CD47 blockade-elicited lymphoma clearance and overcoming tumor-induced immunosuppression

Author

Xu Cao, Yingyu Wang, Wencan Zhang, Xiancai Zhong, E. Gulsen Gunes, Jessica Dang, Jinhui Wang, Alan L. Epstein, Christiane Querfeld, Zuoming Sun, Steven T. Rosen, and Mingye Feng

Subjects

Immunosuppression Therapy, Lymphoma, Paclitaxel, Immunobiology and Immunotherapy, Macrophages, Immunology, CD47 Antigen, Cell Biology, Hematology, Biochemistry, Phagocytosis, hemic and lymphatic diseases, Neoplasms, Tumor Microenvironment, Humans, Immunotherapy

Abstract

Tumor-associated macrophages (TAMs) are often the most abundant immune cells in the tumor microenvironment (TME). Strategies targeting TAMs to enable tumor cell killing through cellular phagocytosis have emerged as promising cancer immunotherapy. Although several phagocytosis checkpoints have been identified, the desired efficacy has not yet been achieved by blocking such checkpoints in preclinical models or clinical trials. Here, we showed that late-stage non-Hodgkin lymphoma (NHL) was resistant to therapy targeting phagocytosis checkpoint CD47 due to the compromised capacity of TAMs to phagocytose lymphoma cells. Via a high-throughput screening of the US Food and Drug Administration–approved anticancer small molecule compounds, we identified paclitaxel as a potentiator that promoted the clearance of lymphoma by directly evoking phagocytic capability of macrophages, independently of paclitaxel’s chemotherapeutic cytotoxicity toward NHL cells. A combination with paclitaxel dramatically enhanced the anticancer efficacy of CD47-targeted therapy toward late-stage NHL. Analysis of TME by single-cell RNA sequencing identified paclitaxel-induced TAM populations with an upregulation of genes for tyrosine kinase signaling. The activation of Src family tyrosine kinases signaling in macrophages by paclitaxel promoted phagocytosis against NHL cells. In addition, we identified a role of paclitaxel in modifying the TME by preventing the accumulation of a TAM subpopulation that was only present in late-stage lymphoma resistant to CD47-targeted therapy. Our findings identify a novel and effective strategy for NHL treatment by remodeling TME to enable the tumoricidal roles of TAMs. Furthermore, we characterize TAM subgroups that determine the efficiency of lymphoma phagocytosis in the TME and can be potential therapeutic targets to unleash the antitumor activities of macrophages.

Published

2021

6. P-102: Novel anti-CD84 humanized monoclonal antibody enhances anti-tumor immunity in multiple myeloma

Author

Metin Gunes, Hadas Lewinsky, Jessica Dang, Ning Ma, Nagarajan Vaidehi, Murali Janakiram, Mingye Feng, Idit Shachar, Steven Rosen, and E. Gulsen Gunes

Subjects

Cancer Research, Oncology, Hematology

Published

2022

7. Effect of cabazitaxel on macrophages improves CD47-targeted immunotherapy for triple-negative breast cancer

Author

Yingyu Wang, Siqi Chen, Jing Chen, Lei Tian, E Gulsen Gunes, Jianhua Yu, Bolei Li, Christiane Querfeld, Xu Cao, Bo Xu, Mingye Feng, Steven T. Rosen, Sabina A Muend, Mustafa Raoof, and Jessica Dang

Subjects

0301 basic medicine, Cancer Research, medicine.medical_treatment, Triple Negative Breast Neoplasms, Mice, 0302 clinical medicine, Antineoplastic Agents, Immunological, Antineoplastic Combined Chemotherapy Protocols, Databases, Genetic, Tumor-Associated Macrophages, Tumor Microenvironment, Immunology and Allergy, Triple-negative breast cancer, RC254-282, Mice, Knockout, education.field_of_study, Mice, Inbred BALB C, NF-kappa B, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Drug Synergism, macrophages, Immunosurveillance, Phenotype, Oncology, Cabazitaxel, 030220 oncology & carcinogenesis, triple-negative breast cancer, Molecular Medicine, Female, Taxoids, immunotherapy, medicine.drug, Signal Transduction, Immunology, Population, CD47 Antigen, 03 medical and health sciences, Phagocytosis, Cell Line, Tumor, medicine, Animals, Humans, education, Pharmacology, Tumor microenvironment, business.industry, CD47, Basic Tumor Immunology, Immunotherapy, Macrophage Activation, Xenograft Model Antitumor Assays, 030104 developmental biology, RAW 264.7 Cells, Cancer cell, Cancer research, business

Abstract

BackgroundLimited therapeutic options are available for triple-negative breast cancer (TNBC), emphasizing an urgent need for more effective treatment approaches. The development of strategies by targeting tumor-associated macrophages (TAMs) to stimulate their ability of Programmed Cell Removal (PrCR) provides a promising new immunotherapy for TNBC treatment.MethodsCD47 is a critical self-protective “don’t eat me” signal on multiple human cancers against macrophage immunosurveillance. Using human and mouse TNBC preclinical models, we evaluated the efficacy of PrCR-based immunotherapy by blocking CD47. We performed high-throughput screens on FDA-approved anti-cancer small molecule compounds for agents potentiating PrCR and enhancing the efficacy of CD47-targeted therapy for TNBC treatment.ResultsWe showed that CD47 was widely expressed on TNBC cells and TAMs represented the most abundant immune cell population in TNBC tumors. Blockade of CD47 enabled PrCR of TNBC cells, but the efficacy was not satisfactory. Our high-throughput screens identified cabazitaxel in enhancing PrCR-based immunotherapy. A combination of CD47 blockade and cabazitaxel treatment yielded a highly effective treatment strategy, promoting PrCR of TNBC cells and inhibiting tumor development and metastasis in preclinical models. We demonstrated that cabazitaxel potentiated PrCR by activating macrophages, independent of its cytotoxicity toward cancer cells. When treated with cabazitaxel, the molecular and phenotypic signatures of macrophages were polarized toward M1 state, and the NF-kB signaling pathway became activated.ConclusionThe combination of CD47 blockade and macrophage activation by cabazitaxel synergizes to vastly enhance the elimination of TNBC cells. Our results show that targeting macrophages is a promising and effective strategy for TNBC treatment.

Published

2021

8. Recombinant antibodies: a new reagent for biological agent detection

Author

Eric A. E. Garber, Henrieta Kulaga, James J. Valdes, Peter J. Stopa, Peter A. Emanuel, Jessica Dang, Joan S Gebhardt, Amanda Dion-Schultz, and Jennifer Aldrich

Subjects

Botulinum Toxins, Phage display, Antibody Affinity, Biomedical Engineering, Biophysics, Enzyme-Linked Immunosorbent Assay, Biosensing Techniques, medicine.disease_cause, Epitope, law.invention, Immunoglobulin Fab Fragments, Mice, Antigen, Antibody Specificity, law, Electrochemistry, medicine, Animals, Biomanufacturing, Surface plasmon resonance, biology, food and beverages, General Medicine, Molecular biology, Recombinant Proteins, Biochemistry, Recombinant DNA, biology.protein, Clostridium botulinum, Antibody, Biotechnology

Abstract

Antibodies are critical reagents used in several biodetection platforms for the identification of biological agents. Recent advances in phage display technology allow isolation of high affinity recombinant antibody fragments (Fabs) that may bind unique epitopes of biological threat agents. The versatility of the selection process lends itself to efficient screening methodologies and can increase the number of antigen binding clones that can be isolated. Pilot scale biomanufacturing can then be used for the economical production of these immunoglobulin reagents in bacterial fermentation systems, and expression vectors with hexahistidine tags can be used to simplify downstream purification. One such Fab reagent directed against botulinum neurotoxin A/B has been shown to be sensitive in a variety of assay formats including surface plasmon resonance (SPR), flow cytometry, enzyme linked immunosorbent assay (ELISA), and hand-held immunochromatographic assay. Recombinant antibodies can provide another source of high quality detection reagents in our arsenal to identify or detect pathogens in environmental samples.

Published

2000

9. Detection of Francisella tularensis within infected mouse tissues by using a hand-held PCR thermocycler

Author

Peter A. Emanuel, Ryan Bell, John C. David, Joseph Thompson, Lisa Collins, Ted L. Hadfield, Rebecca McClanahan, Robert J. Burgess, and Jessica Dang

Subjects

Microbiology (medical), Quality Control, Spleen, Biology, Polymerase Chain Reaction, law.invention, Tularemia, Mice, law, medicine, TaqMan, Animals, Francisella tularensis, Pathogen, Polymerase chain reaction, Mice, Inbred BALB C, Reproducibility of Results, Bacteriology, medicine.disease, biology.organism_classification, Virology, medicine.anatomical_structure, Francisella, Female, Reagent Kits, Diagnostic, Bacteria

Abstract

The diagnosis of human cases of tularemia often relies upon the demonstration of an antibody response toFrancisella tularensisor the direct culturing of the bacteria from the patient. Antibody response is not detectable until 2 weeks or more after infection, and culturing requires special media and suspicion of tularemia. In addition, handling liveFrancisellaposes a risk to laboratory personnel due to the highly infectious nature of this pathogen. In an effort to develop a rapid diagnostic assay for tularemia, we investigated the use of TaqMan 5′ hydrolysis fluorogenic PCR to detect the organism in tissues of infected mice. Mice were infected to produce respiratory tularemia. ThefopAandtul4genes ofF. tularensiswere amplified from infected spleen, lung, liver, and kidney tissues sampled over a 5-day period. The samples were analyzed using the laboratory-based Applied Biosystems International 7900 and the Smiths Detection-Edgewood BioSeeq, a hand-held portable fluorescence thermocycler designed for use in the field. A comparison of culturing and PCR for detection of bacteria in infected tissues shows that culturing was more sensitive than PCR. However, the results for culture take 72 h, whereas PCR results were available within 4 h. PCR was able to detect infection in all the tissues tested. Lung tissue showed the earliest response at 2 days when tested with the ABI 7900 and in 3 days when tested with the BioSeeq. The results were in agreement between the ABI 7900 and the BioSeeq when presented with the same sample. Template preparation may account for the loss of sensitivity compared to culturing techniques. The hand-held BioSeeq thermocycler shows promise as an expedient means of forward diagnosis of infection in the field.

Published

2003

10. Chromatographic Immunoassays for Environmental Monitoring

Author

James J. Valdes, Jafrul A.K. Hasan, Larry Loomis, Peter A. Emanuel, Ray Yin, and Jessica Dang

Subjects

Bioremediation, business.industry, Microorganism, Environmental monitoring, Environmental science, Agricultural pesticides, Contamination, Growth hormone, business, Biotechnology

Abstract

Monitoring the environment for synthetic and naturally occurring chemical and biological toxicants, pathogenic microorganisms, and soil microflora used in bioremediation are diverse aspects of the general rubric known as environmental monitoring and diagnostics. Food and animal feeds need to be screened for disease vectors, both natural and intentionally produced. Meat and milk are often contaminated with antibiotics and growth hormones. Ground water is often polluted with industrial wastes and agricultural pesticides. The viability of pollutant-degrading microorganisms and the efficacy of bioremediation processes need to be ascertained.

Published

2000

11. Purification and Analysis of a Recombinant Human Anti-Cholera Toxin B Antibody

Author

Jessica Dang, Peter A. Emanuel, Darrel E. Menking, Suzanne K. Kracke, and Michael J. Gostomski

Subjects

medicine.diagnostic_test, biology, Cholera toxin, Clostridium difficile toxin B, medicine.disease_cause, biology.organism_classification, Molecular biology, law.invention, law, Immunoassay, medicine, biology.protein, Recombinant DNA, Antibody, Clone (B-cell biology), Escherichia coli, Bacteria

Abstract

A large semi-synthetic recombinant antibody library was constructed based on a human anti-tetanus library. The library was used to isolate a human anti-cholera toxin B antibody cidne, which is expressed in XL-1 Blue E. Coli bacteria. The clone, B-27 cholera Fab, was expressed in small scale and purified by a two column procedure, which uses the histidine affinity tag, which was engineered into the protein. The purified cholera Fab was tested by ELISA to confirm specificity and by surface plasmon resonance to determine affinity binding constants.

Published

1998