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159 results on '"Navenot, Jean-Marc"'

1. Identifying MAGE-A4-positive tumors for TCR T cell therapies in HLA-A∗02-eligible patients

Author

Wang, Tianjiao, Navenot, Jean-Marc, Rafail, Stavros, Kurtis, Cynthia, Carroll, Mark, Van Kerckhoven, Marian, Van Rossom, Sofie, Schats, Kelly, Avraam, Konstantinos, Broad, Robyn, Howe, Karen, Liddle, Ashley, Clayton, Amber, Wang, Ruoxi, Quinn, Laura, Sanderson, Joseph P., McAlpine, Cheryl, Carozza, Carly, Pimpinella, Eric, Hsu, Susan, Brophy, Francine, Elefant, Erica, Bayer, Paige, Williams, Dennis, Butler, Marcus O., Clarke, Jeffrey M., Gainor, Justin F., Govindan, Ramaswamy, Moreno, Victor, Johnson, Melissa, Tu, Janet, Hong, David S., and Blumenschein, George R., Jr.

Published
2024
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2. Afamitresgene autoleucel for advanced synovial sarcoma and myxoid round cell liposarcoma (SPEARHEAD-1): an international, open-label, phase 2 trial

Author

D'Angelo, Sandra P, Araujo, Dejka M, Abdul Razak, Albiruni R, Agulnik, Mark, Attia, Steven, Blay, Jean-Yves, Carrasco Garcia, Irene, Charlson, John A, Choy, Edwin, Demetri, George D, Druta, Mihaela, Forcade, Edouard, Ganjoo, Kristen N, Glod, John, Keedy, Vicki L, Le Cesne, Axel, Liebner, David A, Moreno, Victor, Pollack, Seth M, Schuetze, Scott M, Schwartz, Gary K, Strauss, Sandra J, Tap, William D, Thistlethwaite, Fiona, Valverde Morales, Claudia Maria, Wagner, Michael J, Wilky, Breelyn A, McAlpine, Cheryl, Hudson, Laura, Navenot, Jean-Marc, Wang, Tianjiao, Bai, Jane, Rafail, Stavros, Wang, Ruoxi, Sun, Amy, Fernandes, Lilliam, Van Winkle, Erin, Elefant, Erica, Lunt, Colin, Norry, Elliot, Williams, Dennis, Biswas, Swethajit, and Van Tine, Brian A

Published
2024
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3. Autologous T cell therapy for MAGE-A4+ solid cancers in HLA-A*02+ patients: a phase 1 trial

Author

Hong, David S., Van Tine, Brian A., Biswas, Swethajit, McAlpine, Cheryl, Johnson, Melissa L., Olszanski, Anthony J., Clarke, Jeffrey M., Araujo, Dejka, Blumenschein, Jr, George R., Kebriaei, Partow, Lin, Quan, Tipping, Alex J., Sanderson, Joseph P., Wang, Ruoxi, Trivedi, Trupti, Annareddy, Thejo, Bai, Jane, Rafail, Stavros, Sun, Amy, Fernandes, Lilliam, Navenot, Jean-Marc, Bushman, Frederic D., Everett, John K., Karadeniz, Derin, Broad, Robyn, Isabelle, Martin, Naidoo, Revashnee, Bath, Natalie, Betts, Gareth, Wolchinsky, Zohar, Batrakou, Dzmitry G., Van Winkle, Erin, Elefant, Erica, Ghobadi, Armin, Cashen, Amanda, Grand’Maison, Anne, McCarthy, Philip, Fracasso, Paula M., Norry, Elliot, Williams, Dennis, Druta, Mihaela, Liebner, David A., Odunsi, Kunle, and Butler, Marcus O.

Published
2023
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4. Systemic and local immunity following adoptive transfer of NY-ESO-1 SPEAR T cells in synovial sarcoma

Author

Ramachandran, Indu, Lowther, Daniel E, Dryer-Minnerly, Rebecca, Wang, Ruoxi, Fayngerts, Svetlana, Nunez, Daniel, Betts, Gareth, Bath, Natalie, Tipping, Alex J, Melchiori, Luca, Navenot, Jean-Marc, Glod, John, Mackall, Crystal L, D’Angelo, Sandra P, Araujo, Dejka M, Chow, Warren A, Demetri, George D, Druta, Mihaela, Van Tine, Brian A, Grupp, Stephan A, Abdul Razak, Albiruni R, Wilky, Breelyn, Iyengar, Malini, Trivedi, Trupti, Winkle, Erin Van, Chagin, Karen, Amado, Rafael, Binder, Gwendolyn K, and Basu, Samik

Subjects
Vaccine Related, Biotechnology, Immunization, Cancer, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Antigens, Neoplasm, Biomarkers, Clinical Trials, Phase I as Topic, Clinical Trials, Phase II as Topic, Cytokines, Cytotoxicity, Immunologic, HLA-A Antigens, Humans, Immunohistochemistry, Immunotherapy, Adoptive, Lymphocytes, Tumor-Infiltrating, Membrane Proteins, Receptors, Antigen, T-Cell, Receptors, Chimeric Antigen, Sarcoma, Synovial, T-Cell Antigen Receptor Specificity, T-Lymphocytes, Treatment Outcome, Tumor Microenvironment, Adoptive immunotherapy, Synovial sarcoma, NY-ESO-1, Fludarabine, Cyclophosphamide, T cell, TCR, IL-15, Cytokine, Antigen loss, Checkpoint therapy, Engineered cell therapy
Abstract

BackgroundGene-modified autologous T cells expressing NY-ESO-1c259, an affinity-enhanced T-cell receptor (TCR) reactive against the NY-ESO-1-specific HLA-A*02-restricted peptide SLLMWITQC (NY-ESO-1 SPEAR T-cells; GSK 794), have demonstrated clinical activity in patients with advanced synovial sarcoma (SS). The factors contributing to gene-modified T-cell expansion and the changes within the tumor microenvironment (TME) following T-cell infusion remain unclear. These studies address the immunological mechanisms of response and resistance in patients with SS treated with NY-ESO-1 SPEAR T-cells.MethodsFour cohorts were included to evaluate antigen expression and preconditioning on efficacy. Clinical responses were assessed by RECIST v1.1. Engineered T-cell persistence was determined by qPCR. Serum cytokines were evaluated by immunoassay. Transcriptomic analyses and immunohistochemistry were performed on tumor biopsies from patients before and after T-cell infusion. Gene-modified T-cells were detected within the TME via an RNAish assay.ResultsResponses across cohorts were affected by preconditioning and intra-tumoral NY-ESO-1 expression. Of the 42 patients reported (data cut-off 4June2018), 1 patient had a complete response, 14 patients had partial responses, 24 patients had stable disease, and 3 patients had progressive disease. The magnitude of gene-modified T-cell expansion shortly after infusion was associated with response in patients with high intra-tumoral NY-ESO-1 expression. Patients receiving a fludarabine-containing conditioning regimen experienced increases in serum IL-7 and IL-15. Prior to infusion, the TME exhibited minimal leukocyte infiltration; CD163+ tumor-associated macrophages (TAMs) were the dominant population. Modest increases in intra-tumoral leukocytes (≤5%) were observed in a subset of subjects at approximately 8 weeks. Beyond 8 weeks post infusion, the TME was minimally infiltrated with a TAM-dominant leukocyte infiltrate. Tumor-associated antigens and antigen presentation did not significantly change within the tumor post-T-cell infusion. Finally, NY-ESO-1 SPEAR T cells trafficked to the TME and maintained cytotoxicity in a subset of patients.ConclusionsOur studies elucidate some factors that underpin response and resistance to NY-ESO-1 SPEAR T-cell therapy. From these data, we conclude that a lymphodepletion regimen containing high doses of fludarabine and cyclophosphamide is necessary for SPEAR T-cell persistence and efficacy. Furthermore, these data demonstrate that non-T-cell inflamed tumors, which are resistant to PD-1/PD-L1 inhibitors, can be treated with adoptive T-cell based immunotherapy.Trial registrationClinicalTrials.gov, NCT01343043 , Registered 27 April 2011.

Published
2019

5. A single dose of peripherally infused EGFRvIII-directed CAR T cells mediates antigen loss and induces adaptive resistance in patients with recurrent glioblastoma

Author

O'Rourke, Donald M, Nasrallah, MacLean P, Desai, Arati, Melenhorst, Jan J, Mansfield, Keith, Morrissette, Jennifer JD, Martinez-Lage, Maria, Brem, Steven, Maloney, Eileen, Shen, Angela, Isaacs, Randi, Mohan, Suyash, Plesa, Gabriela, Lacey, Simon F, Navenot, Jean-Marc, Zheng, Zhaohui, Levine, Bruce L, Okada, Hideho, June, Carl H, Brogdon, Jennifer L, and Maus, Marcela V

Subjects
Neurosciences, Immunization, Cancer, Rare Diseases, Brain Cancer, Biotechnology, Brain Disorders, Stem Cell Research - Nonembryonic - Human, Stem Cell Research, Clinical Research, Vaccine Related, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Aged, Brain Neoplasms, Cell- and Tissue-Based Therapy, ErbB Receptors, Female, Glioblastoma, Humans, Immunohistochemistry, Immunotherapy, Adoptive, Male, Middle Aged, Neoplasm Recurrence, Local, Receptors, Antigen, T-Cell, Biological Sciences, Medical and Health Sciences
Abstract

We conducted a first-in-human study of intravenous delivery of a single dose of autologous T cells redirected to the epidermal growth factor receptor variant III (EGFRvIII) mutation by a chimeric antigen receptor (CAR). We report our findings on the first 10 recurrent glioblastoma (GBM) patients treated. We found that manufacturing and infusion of CAR-modified T cell (CART)-EGFRvIII cells are feasible and safe, without evidence of off-tumor toxicity or cytokine release syndrome. One patient has had residual stable disease for over 18 months of follow-up. All patients demonstrated detectable transient expansion of CART-EGFRvIII cells in peripheral blood. Seven patients had post-CART-EGFRvIII surgical intervention, which allowed for tissue-specific analysis of CART-EGFRvIII trafficking to the tumor, phenotyping of tumor-infiltrating T cells and the tumor microenvironment in situ, and analysis of post-therapy EGFRvIII target antigen expression. Imaging findings after CART immunotherapy were complex to interpret, further reinforcing the need for pathologic sampling in infused patients. We found trafficking of CART-EGFRvIII cells to regions of active GBM, with antigen decrease in five of these seven patients. In situ evaluation of the tumor environment demonstrated increased and robust expression of inhibitory molecules and infiltration by regulatory T cells after CART-EGFRvIII infusion, compared to pre-CART-EGFRvIII infusion tumor specimens. Our initial experience with CAR T cells in recurrent GBM suggests that although intravenous infusion results in on-target activity in the brain, overcoming the adaptive changes in the local tumor microenvironment and addressing the antigen heterogeneity may improve the efficacy of EGFRvIII-directed strategies in GBM.

Published
2017

6. Data from Antitumor Activity Associated with Prolonged Persistence of Adoptively Transferred NY-ESO-1 c259T Cells in Synovial Sarcoma

Author

D'Angelo, Sandra P., primary, Melchiori, Luca, primary, Merchant, Melinda S., primary, Bernstein, Donna, primary, Glod, John, primary, Kaplan, Rosandra, primary, Grupp, Stephan, primary, Tap, William D., primary, Chagin, Karen, primary, Binder, Gwendolyn K., primary, Basu, Samik, primary, Lowther, Daniel E., primary, Wang, Ruoxi, primary, Bath, Natalie, primary, Tipping, Alex, primary, Betts, Gareth, primary, Ramachandran, Indu, primary, Navenot, Jean-Marc, primary, Zhang, Hua, primary, Wells, Daniel K., primary, Van Winkle, Erin, primary, Kari, Gabor, primary, Trivedi, Trupti, primary, Holdich, Tom, primary, Pandite, Lini, primary, Amado, Rafael, primary, and Mackall, Crystal L., primary

Published
2023
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7. Figures S1-S7 from Antitumor Activity Associated with Prolonged Persistence of Adoptively Transferred NY-ESO-1 c259T Cells in Synovial Sarcoma

Author

D'Angelo, Sandra P., primary, Melchiori, Luca, primary, Merchant, Melinda S., primary, Bernstein, Donna, primary, Glod, John, primary, Kaplan, Rosandra, primary, Grupp, Stephan, primary, Tap, William D., primary, Chagin, Karen, primary, Binder, Gwendolyn K., primary, Basu, Samik, primary, Lowther, Daniel E., primary, Wang, Ruoxi, primary, Bath, Natalie, primary, Tipping, Alex, primary, Betts, Gareth, primary, Ramachandran, Indu, primary, Navenot, Jean-Marc, primary, Zhang, Hua, primary, Wells, Daniel K., primary, Van Winkle, Erin, primary, Kari, Gabor, primary, Trivedi, Trupti, primary, Holdich, Tom, primary, Pandite, Lini, primary, Amado, Rafael, primary, and Mackall, Crystal L., primary

Published
2023
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8. Preliminary clinical outcomes of ADP-A2M4CD8, a next-generation autologous T-cell receptor T-cell therapy, in patients with advanced urothelial cancer.

Author

Aggen, David H, primary, Hong, David S., additional, Clarke, Jeffrey Melson, additional, Asch, Adam Steven, additional, Calvo, Emiliano, additional, Zugazagoitia, Jon, additional, Butler, Marcus O., additional, Moreno, Victor, additional, Cervantes, Andres, additional, Van Tine, Brian Andrew, additional, Lawrence, Donald P., additional, Johnson, Melissa Lynne, additional, Brophy, Francine Elizabeth, additional, Broad, Robyn, additional, Isabelle, Martin, additional, Gunn, Alasdair, additional, Navenot, Jean-Marc, additional, Saro, Jose, additional, Norry, Elliot, additional, and Charlson, John A., additional

Published
2023
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9. Safety and efficacy from the phase 1 SURPASS trial of ADP-A2M4CD8, a next-generation T-cell receptor T-cell therapy, in patients with advanced esophageal, esophagogastric junction, or gastric cancer.

Author

Blum Murphy, Mariela A., primary, Ajani, Jaffer A., additional, Van Tine, Brian Andrew, additional, Clarke, Jeffrey Melson, additional, Butler, Marcus O., additional, Lawrence, Donald P., additional, Johnson, Melissa Lynne, additional, Cervantes, Andres, additional, Moreno, Victor, additional, Hong, David S., additional, Brophy, Francine Elizabeth, additional, Navenot, Jean-Marc, additional, Lin, Quan, additional, Saro, Jose, additional, and Norry, Elliot, additional

Published
2023
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10. Abstract LB001: Identifying MAGE-A4-positive tumors for SPEAR T-cell therapies in HLA-A*02-eligible patients

Author

Wang, Tianjiao, primary, Navenot, Jean-Marc, additional, Rafail, Stavros, additional, Carroll, Mark, additional, Wang, Ruoxi, additional, McAlpine, Cheryl, additional, Biswas, Swethajit, additional, Brophy, Francine, additional, Elefant, Erica, additional, Bayer, Paige, additional, McGuigan, Sandra, additional, Williams, Dennis, additional, Blumenschein, George, additional, Butler, Marcus, additional, Clarke, Jeffrey M., additional, Gainor, Justin F., additional, Govindan, Ramaswamy, additional, Moreno, Victor, additional, Tu, Janet, additional, and Hong, David S., additional

Published
2022
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11. Phase 1 Clinical Trial Evaluating the Safety and Anti-Tumor Activity of ADP-A2M10 SPEAR T-Cells in Patients With MAGE-A10+ Head and Neck, Melanoma, or Urothelial Tumors

Author

Hong, David S., primary, Butler, Marcus O., additional, Pachynski, Russell K., additional, Sullivan, Ryan, additional, Kebriaei, Partow, additional, Boross-Harmer, Sarah, additional, Ghobadi, Armin, additional, Frigault, Matthew J., additional, Dumbrava, Ecaterina E., additional, Sauer, Amy, additional, Brophy, Francine, additional, Navenot, Jean-Marc, additional, Fayngerts, Svetlana, additional, Wolchinsky, Zohar, additional, Broad, Robyn, additional, Batrakou, Dzmitry G., additional, Wang, Ruoxi, additional, Solis, Luisa M., additional, Duose, Dzifa Yawa, additional, Sanderson, Joseph P., additional, Gerry, Andrew B., additional, Marks, Diane, additional, Bai, Jane, additional, Norry, Elliot, additional, and Fracasso, Paula M., additional

Published
2022
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12. Phase I clinical trial evaluating the safety and efficacy of ADP-A2M10 SPEAR T cells in patients with MAGE-A10+ advanced non-small cell lung cancer

Author

Blumenschein, George R, primary, Devarakonda, Siddhartha, additional, Johnson, Melissa, additional, Moreno, Victor, additional, Gainor, Justin, additional, Edelman, Martin J, additional, Heymach, John V, additional, Govindan, Ramaswamy, additional, Bachier, Carlos, additional, Doger de Spéville, Bernard, additional, Frigault, Matthew J, additional, Olszanski, Anthony J, additional, Lam, Vincent K, additional, Hyland, Natalie, additional, Navenot, Jean-Marc, additional, Fayngerts, Svetlana, additional, Wolchinsky, Zohar, additional, Broad, Robyn, additional, Batrakou, Dzmitry, additional, Pentony, Melissa M, additional, Sanderson, Joseph P, additional, Gerry, Andrew, additional, Marks, Diane, additional, Bai, Jane, additional, Holdich, Tom, additional, Norry, Elliot, additional, and Fracasso, Paula M, additional

Published
2022
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14. 376 Radiation sub-study to characterize safety and tolerability of low-dose radiation in combination with afami-cel in patients with advanced cancers (NCT03132922)

Author

Welsh, James, primary, Ke, Danxia, additional, Osorio, Nahum Puebla, additional, Barsoumian, Hampartsoum, additional, Jackson, Bryan, additional, Bai, Jane, additional, Rosenberg, Marisa, additional, McAlpine, Cheryl, additional, Broad, Robyn, additional, Liddle, Ashley, additional, Navenot, Jean-Marc, additional, Rafail, Stavros, additional, Wang, Ruoxi, additional, Sauer, Amy, additional, Lin, Quan, additional, Danesi, Hassan, additional, and Hong, David, additional

Published
2021
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15. 373 Enhancement of TCR-engineered T-cells targeting MAGE-A4 antigen by co-expression of CD8α and inhibition of AKT signaling during ex vivo T-cell expansion

Author

Schmidt, Emily, primary, Mardilovich, Katerina, additional, Bath, Natalie, additional, Betts, Gareth, additional, Spinner, William, additional, Sun, Kathryn, additional, Donaldson, Ian, additional, McAlpine, Cheryl, additional, Luke, Raymond, additional, Navenot, Jean-Marc, additional, Sanderson, Joseph, additional, Bassett, Phil, additional, Evans, Chris, additional, Miller, Karen, additional, Lin, Quan, additional, Dudley, Mark, additional, and Tipping, Alex, additional

Published
2021
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16. Autologous T cell therapy for MAGE-A4+solid cancers in HLA-A*02+patients: a phase 1 trial

Author

Hong, David S., Van Tine, Brian A., Biswas, Swethajit, McAlpine, Cheryl, Johnson, Melissa L., Olszanski, Anthony J., Clarke, Jeffrey M., Araujo, Dejka, Blumenschein, George R., Kebriaei, Partow, Lin, Quan, Tipping, Alex J., Sanderson, Joseph P., Wang, Ruoxi, Trivedi, Trupti, Annareddy, Thejo, Bai, Jane, Rafail, Stavros, Sun, Amy, Fernandes, Lilliam, Navenot, Jean-Marc, Bushman, Frederic D., Everett, John K., Karadeniz, Derin, Broad, Robyn, Isabelle, Martin, Naidoo, Revashnee, Bath, Natalie, Betts, Gareth, Wolchinsky, Zohar, Batrakou, Dzmitry G., Van Winkle, Erin, Elefant, Erica, Ghobadi, Armin, Cashen, Amanda, Grand’Maison, Anne, McCarthy, Philip, Fracasso, Paula M., Norry, Elliot, Williams, Dennis, Druta, Mihaela, Liebner, David A., Odunsi, Kunle, and Butler, Marcus O.

Abstract

Affinity-optimized T cell receptors can enhance the potency of adoptive T cell therapy. Afamitresgene autoleucel (afami-cel) is a human leukocyte antigen-restricted autologous T cell therapy targeting melanoma-associated antigen A4 (MAGE-A4), a cancer/testis antigen expressed at varying levels in multiple solid tumors. We conducted a multicenter, dose-escalation, phase 1 trial in patients with relapsed/refractory metastatic solid tumors expressing MAGE-A4, including synovial sarcoma (SS), ovarian cancer and head and neck cancer (NCT03132922). The primary endpoint was safety, and the secondary efficacy endpoints included overall response rate (ORR) and duration of response. All patients (N= 38, nine tumor types) experienced Grade ≥3 hematologic toxicities; 55% of patients (90% Grade ≤2) experienced cytokine release syndrome. ORR (all partial response) was 24% (9/38), 7/16 (44%) for SS and 2/22 (9%) for all other cancers. Median duration of response was 25.6 weeks (95% confidence interval (CI): 12.286, not reached) and 28.1 weeks (95% CI: 12.286, not reached) overall and for SS, respectively. Exploratory analyses showed that afami-cel infiltrates tumors, has an interferon-γ-driven mechanism of action and triggers adaptive immune responses. In addition, afami-cel has an acceptable benefit–risk profile, with early and durable responses, especially in patients with metastatic SS. Although the small trial size limits conclusions that can be drawn, the results warrant further testing in larger studies.

Published
2023
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18. 285 Phase I clinical trial evaluating the safety of ADP-A2M10 in patients with MAGE-A10+ head and neck, melanoma, or urothelial tumors

Author

Hong, David, primary, Butler, Marcus, additional, Pachynski, Russell, additional, Sullivan, Ryan, additional, Kebriaei, Partow, additional, Boross-Harmer, Sarah, additional, Frigault, Matthew, additional, Dumbrava, Ecaterina, additional, Sauer, Amy, additional, Brophy, Francine, additional, Navenot, Jean-Marc, additional, Fayngerts, Svetlana, additional, Bai, Jane, additional, Norry, Elliot, additional, and Fracasso, Paula, additional

Published
2020
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19. 379 Initial safety, efficacy, and product attributes from the SURPASS trial with ADP-A2M4CD8, a SPEAR T-cell therapy incorporating an affinity optimized TCR targeting MAGE-A4 and a CD8α co-receptor

Author

Hong, David, primary, Clarke, Jeffrey, additional, Johanns, Tanner, additional, Kebriaei, Partow, additional, Heymach, John, additional, Galal, Ahmed, additional, Saibil, Samuel, additional, Sacher, Adrian, additional, Brophy, Francine, additional, Betts, Gareth, additional, Bath, Natalie, additional, William, Spinner, additional, Tipping, Alex, additional, Tucci, Jessica, additional, Luke, Raymond, additional, Trivedi, Trupti, additional, Lin, Quan, additional, Navenot, Jean-Marc, additional, Fracasso, Paula, additional, Miller, Karen, additional, Norry, Elliot, additional, Dudley, Mark, additional, and Butler, Marcus, additional

Published
2020
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20. 278 Phase I clinical trial evaluating the safety of ADP-A2M10 SPEAR T-cells in patients with MAGE-A10+advanced non-small cell lung cancer

Author

Blumenschein, George, primary, Devarakonda, Siddhartha, additional, Johnson, Melissa, additional, Moreno, Victor, additional, Gainor, Justin, additional, Edelman, Martin, additional, Heymach, John, additional, Govindan, Ramaswamy, additional, Bachier, Carlos, additional, Spéville, Bernard Doger de, additional, Frigault, Matthew, additional, Olszanski, Anthony, additional, Lam, Vincent, additional, Hyland, Natalie, additional, Navenot, Jean-Marc, additional, Fayngerts, Svetlana, additional, Bai, Jane, additional, Norry, Elliot, additional, and Fracasso, Paula, additional

Published
2020
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21. Phase I dose escalation and expansion trial to assess the safety and efficacy of ADP-A2M4 SPEAR T cells in advanced solid tumors.

Author

Hong, David S., primary, Van Tine, Brian A., additional, Olszanski, Anthony J., additional, Johnson, Melissa Lynne, additional, Liebner, David A., additional, Trivedi, Trupti, additional, Lin, Quan, additional, Elefant, Erica, additional, Dryer-Minnerly, Rebecca, additional, Navenot, Jean-Marc, additional, Williams, Dennis, additional, Ramachandran, Indu R., additional, Fracasso, Paula M., additional, Norry, Elliot, additional, and Butler, Marcus O., additional

Published
2020
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23. Long-term safety and activity of NY-ESO-1 SPEAR T cells after autologous stem cell transplant for myeloma

Author

Stadtmauer, Edward A., primary, Faitg, Thomas H., additional, Lowther, Daniel E., additional, Badros, Ashraf Z., additional, Chagin, Karen, additional, Dengel, Karen, additional, Iyengar, Malini, additional, Melchiori, Luca, additional, Navenot, Jean-Marc, additional, Norry, Elliot, additional, Trivedi, Trupti, additional, Wang, Ruoxi, additional, Binder, Gwendolyn K., additional, Amado, Rafael, additional, and Rapoport, Aaron P., additional

Published
2019
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24. Antitumor Activity Associated with Prolonged Persistence of Adoptively Transferred NY-ESO-1 c259T Cells in Synovial Sarcoma

Author

D'Angelo, Sandra P., primary, Melchiori, Luca, additional, Merchant, Melinda S., additional, Bernstein, Donna, additional, Glod, John, additional, Kaplan, Rosandra, additional, Grupp, Stephan, additional, Tap, William D., additional, Chagin, Karen, additional, Binder, Gwendolyn K., additional, Basu, Samik, additional, Lowther, Daniel E., additional, Wang, Ruoxi, additional, Bath, Natalie, additional, Tipping, Alex, additional, Betts, Gareth, additional, Ramachandran, Indu, additional, Navenot, Jean-Marc, additional, Zhang, Hua, additional, Wells, Daniel K., additional, Van Winkle, Erin, additional, Kari, Gabor, additional, Trivedi, Trupti, additional, Holdich, Tom, additional, Pandite, Lini, additional, Amado, Rafael, additional, and Mackall, Crystal L., additional

Published
2018
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25. A single dose of peripherally infused EGFRvIII-directed CAR T cells mediates antigen loss and induces adaptive resistance in patients with recurrent glioblastoma

Author

O’Rourke, Donald M., primary, Nasrallah, MacLean P., additional, Desai, Arati, additional, Melenhorst, Jan J., additional, Mansfield, Keith, additional, Morrissette, Jennifer J. D., additional, Martinez-Lage, Maria, additional, Brem, Steven, additional, Maloney, Eileen, additional, Shen, Angela, additional, Isaacs, Randi, additional, Mohan, Suyash, additional, Plesa, Gabriela, additional, Lacey, Simon F., additional, Navenot, Jean-Marc, additional, Zheng, Zhaohui, additional, Levine, Bruce L., additional, Okada, Hideho, additional, June, Carl H., additional, Brogdon, Jennifer L., additional, and Maus, Marcela V., additional

Published
2017
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27. Abstract LB-083: Phase I study of T cells redirected to EGFRvIII with a chimeric antigen receptor in patients with EGFRvIII+ glioblastoma

Author

O’Rourke, Donald M., primary, Nasrallah, MacLean P., additional, Morrissette, Jennifer, additional, Melenhorst, Jan J., additional, Lacey, Simon F., additional, Mansfield, Keith, additional, Martinez-Lage, Maria, additional, Desai, Arati, additional, Brem, Steven, additional, Maloney, Eileen, additional, Mohan, Suyash, additional, Wang, Sumei, additional, Verma, Gaurav, additional, Navenot, Jean-Marc, additional, Shen, Angela, additional, Zheng, Zhaohui, additional, Levine, Bruce L., additional, Okada, Hideho, additional, June, Carl H., additional, and Maus, Marcela V., additional

Published
2016
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28. Pilot study of T cells redirected to EGFRvIII with a chimeric antigen receptor in patients with EGFRvIII+ glioblastoma.

Author

O'Rourke, Donald M., primary, Nasrallah, MacLean, additional, Morrissette, Jennifer J., additional, Melenhorst, Jan J., additional, Lacey, Simon F., additional, Mansfield, Keith, additional, Martinez-Lage, Maria, additional, Desai, Arati Suvas, additional, Brem, Steven, additional, Maloney, Eileen, additional, Mohan, Suyash, additional, Wang, Sumei, additional, Verma, Gaurav, additional, Navenot, Jean-Marc, additional, Shen, Angela, additional, Zheng, Zhaohui, additional, Levine, Bruce, additional, Okada, Hideho, additional, June, Carl H., additional, and Maus, Marcela Valderrama, additional

Published
2016
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29. IMCT-15PILOT STUDY OF T CELLS REDIRECTED TO EGFRvIII WITH A CHIMERIC ANTIGEN RECEPTOR IN PATIENTS WITH EGFRvIII+ GLIOBLASTOMA

Author

O'Rourke, Donald, primary, Desai, Arati, additional, Morrissette, Jennifer, additional, Martinez-Lage, Maria, additional, Nasrallah, MacLean, additional, Brem, Steven, additional, Maloney, Eileen, additional, Shen, Angela, additional, Mohan, Suyash, additional, Wang, Sumei, additional, Verma, Gaurav, additional, Lacey, Simon, additional, Melenhorst, Jan, additional, Navenot, Jean-Marc, additional, Zheng, Zhaohui, additional, Levine, Bruce, additional, Okada, Hideho, additional, June, Carl, additional, and Maus, Marcela, additional

Published
2015
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30. Expression and distribution of complement regulatory proteins in Duchenne Muscular Dystrophy, Polymyositis, and X-linked Vacuolated myopathy

Author

Louboutin, Jean-Pierre, Navenot, Jean-Marc, Rouger, Karl, Blanchard, Dominique, Développement et Pathologie du Tissu Musculaire (DPTM), Ecole Nationale Vétérinaire de Nantes-Institut National de la Recherche Agronomique (INRA), Institut National de la Recherche Agronomique (INRA)-Ecole Nationale Vétérinaire de Nantes, and ProdInra, Archive Ouverte

Subjects
[SDV.MHEP] Life Sciences [q-bio]/Human health and pathology, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology
Abstract

absent

Published
2005

33. The metastasis suppressor KISS1 lacks antimetastatic activity in the C8161.9 xenograft model of melanoma.

Author

Navenot, Jean-Marc, Evans, Barry, Oishi, Shinya, Setsuda, Shohei, Fujii, Nobutaka, Peiper, Stephen C, Navenot, Jean-Marc, Evans, Barry, Oishi, Shinya, Setsuda, Shohei, Fujii, Nobutaka, and Peiper, Stephen C

Abstract

The objective of this study was to use the established xenograft model of human melanoma (C8161.9) to test a pharmacological approach to the effect of the metastasis suppressor KISS1. A KISS1 analog was used to inhibit the metastatic development of C8161.9 cells in nude mice. Further experiments were performed to test the validity of the C8161.9 model and test the connection between KISS1 expression and loss of metastatic potential. New clones of C8161.9 cells were obtained, with or without KISS1 expression, and were tested for metastasis formation. The absence of benefit in survival with the KISS1 analog compared with PBS prompted us to revisit the C8161.9 model. We found that the cells expressing KISS1, used in the previous study and obtained by transfection and single-cell cloning, were defective for both formation of orthotopic tumors and metastases. In mixing experiments, these cells could not suppress orthotopic tumor growth of KISS1-negative C8161.9 cells, suggesting that the suppression of metastasis by C8161.9-KISS1 cells may be intrinsic to the selected clone rather than related to KISS1 expression. Isolation of clones from parental C8161.9 cells in soft agar yielded cell populations that phenotypically and genotypically mimicked the KISS1-positive clone. In addition, new clones expressing KISS1 did not show any decrease in metastatic growth. These data demonstrate the heterogeneity of cell types in the C8161.9 cell line and the high risk of artifact linked to single-cell selection. A different xenograft model will be necessary to evaluate the use of KISS1 analogs as antimetastatic therapy.

Published
2012

50. A Point Mutation That Confers Constitutive Activity to CXCR4 Reveals That T140 Is an Inverse Agonist and That AMD3100 and ALX40-4C Are Weak Partial Agonists

Author

Zhang, Wen-bo, primary, Navenot, Jean-Marc, additional, Haribabu, Bodduluri, additional, Tamamura, Hirokazu, additional, Hiramatu, Kenichi, additional, Omagari, Akane, additional, Pei, Gang, additional, Manfredi, John P., additional, Fujii, Nobutaka, additional, Broach, James R., additional, and Peiper, Stephen C., additional

Published
2002
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