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1. KIR/KIR-ligand genotypes and clinical outcomes following chemoimmunotherapy in patients with relapsed or refractory neuroblastoma: a report from the Children’s Oncology Group

Author

Erbe, Amy K, Diccianni, Mitch B, Mody, Rajen, Naranjo, Arlene, Zhang, Fan F, Birstler, Jen, Kim, KyungMann, Feils, Arika S, Hung, Jung-Tung, London, Wendy B, Shulkin, Barry L, Mathew, Varsha, Parisi, Marguerite T, Servaes, Sabah, Asgharzadeh, Shahab, Maris, John M, Park, Julie, Yu, Alice L, Sondel, Paul M, and Bagatell, Rochelle

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Cancer, Neurosciences, Clinical Trials and Supportive Activities, Clinical Research, Pediatric, Vaccine Related, Rare Diseases, Neuroblastoma, Pediatric Cancer, Immunization, Inflammatory and immune system, Humans, Child, Ligands, Granulocyte-Macrophage Colony-Stimulating Factor, Leukocytes, Mononuclear, Genotype, Receptors, KIR, Histocompatibility Antigens, Irinotecan, Immunotherapy, Recurrence, Clinical Trials as Topic, Genetic Markers, Pediatrics, Oncology and carcinogenesis
Abstract

BackgroundIn the Children's Oncology Group ANBL1221 phase 2 trial for patients with first relapse/first declaration of refractory high-risk neuroblastoma, irinotecan and temozolomide (I/T) combined with either temsirolimus (TEMS) or immunotherapy (the anti-GD2 antibody dinutuximab (DIN) and granulocyte macrophage colony stimulating factory (GM-CSF)) was administered. The response rate among patients treated with I/T/DIN/GM-CSF in the initial cohort (n=17) was 53%; additional patients were enrolled to permit further evaluation of this chemoimmunotherapy regimen. Potential associations between immune-related biomarkers and clinical outcomes including response and survival were evaluated.MethodsPatients were evaluated for specific immunogenotypes that influence natural killer (NK) cell activity, including killer immunoglobulin-like receptors (KIRs) and their ligands, Fc gamma receptors, and NCR3. Total white cells and leucocyte subsets were assessed via complete blood counts, and flow cytometry of peripheral blood mononuclear cells was performed to assess the potential association between immune cell subpopulations and surface marker expression and clinical outcomes. Appropriate statistical tests of association were performed. The Bonferroni correction for multiple comparisons was performed where indicated.ResultsOf the immunogenotypes assessed, the presence or absence of certain KIR and their ligands was associated with clinical outcomes in patients treated with chemoimmunotherapy rather than I/T/TEMS. While median values of CD161, CD56, and KIR differed in responders and non-responders, statistical significance was not maintained in logistic regression models. White cell and neutrophil counts were associated with differences in survival outcomes, however, increases in risk of event in patients assigned to chemoimmunotherapy were not clinically significant.ConclusionsThese findings are consistent with those of prior studies showing that KIR/KIR-ligand genotypes are associated with clinical outcomes following anti-GD2 immunotherapy in children with neuroblastoma. The current study confirms the importance of KIR/KIR-ligand genotype in the context of I/T/DIN/GM-CSF chemoimmunotherapy administered to patients with relapsed or refractory disease in a clinical trial. These results are important because this regimen is now widely used for treatment of patients at time of first relapse/first declaration of refractory disease. Efforts to assess the role of NK cells and genes that influence their function in response to immunotherapy are ongoing.Trial registration numberNCT01767194.

Published
2023

4. Improved Outcome in Children With Newly Diagnosed High-Risk Neuroblastoma Treated With Chemoimmunotherapy: Updated Results of a Phase II Study Using hu14.18K322A

Author

Furman, Wayne L, McCarville, Beth, Shulkin, Barry L, Davidoff, Andrew, Krasin, Matthew, Hsu, Chia-Wei, Pan, Haitao, Wu, Jianrong, Brennan, Rachel, Bishop, Michael W, Helmig, Sara, Stewart, Elizabeth, Navid, Fariba, Triplett, Brandon, Santana, Victor, Santiago, Teresa, Hank, Jacquelyn A, Gillies, Stephen D, Yu, Alice, Sondel, Paul M, Leung, Wing H, Pappo, Alberto, and Federico, Sara M

Subjects
Neuroblastoma, Clinical Research, Cancer, Clinical Trials and Supportive Activities, Rare Diseases, Neurosciences, Pediatric, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, 6.2 Cellular and gene therapies, Adolescent, Age Factors, Antibodies, Monoclonal, Humanized, Antineoplastic Agents, Immunological, Antineoplastic Combined Chemotherapy Protocols, Child, Child, Preschool, Female, Granulocyte-Macrophage Colony-Stimulating Factor, Humans, Induction Chemotherapy, Infant, Interleukin-2, Male, Progression-Free Survival, Prospective Studies, Risk Assessment, Risk Factors, Time Factors, Tumor Burden, Clinical Sciences, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

PurposeWe evaluated whether combining a humanized antidisialoganglioside monoclonal antibody (hu14.18K322A) throughout therapy improves early response and outcomes in children with newly diagnosed high-risk neuroblastoma.Patients and methodsWe conducted a prospective, single-arm, three-stage, phase II clinical trial. Six cycles of induction chemotherapy were coadministered with hu14.18K322A, granulocyte-macrophage colony-stimulating factor (GM-CSF), and low-dose interleukin-2 (IL-2). The consolidation regimen included busulfan and melphalan. When available, an additional cycle of parent-derived natural killer cells with hu14.18K322A was administered during consolidation (n = 31). Radiation therapy was administered at the end of consolidation. Postconsolidation treatment included hu14.18K322A, GM-CSF, IL-2, and isotretinoin. Early response was assessed after the first two cycles of induction therapy. End-of-induction response, event-free survival (EFS), and overall survival (OS) were evaluated.ResultsSixty-four patients received hu14.18K322A with induction chemotherapy. This regimen was well tolerated, with continuous infusion narcotics. Partial responses (PRs) or better after the first two chemoimmunotherapy cycles occurred in 42 of 63 evaluable patients (66.7%; 95% CI, 55.0 to 78.3). Primary tumor volume decreased by a median of 75% (range, 100% [complete disappearance]-5% growth). Median peak hu14.18K322A serum levels in cycle one correlated with early response to therapy (P = .0154, one-sided t-test). Sixty of 62 patients (97%) had an end-of-induction partial response or better. No patients experienced progressive disease during induction. The 3-year EFS was 73.7% (95% CI, 60.0 to 83.4), and the OS was 86.0% (95% CI, 73.8 to 92.8), respectively.ConclusionAdding hu14.18K322A to induction chemotherapy improved early objective responses, significantly reduced tumor volumes in most patients, improved end-of-induction response rates, and yielded an encouraging 3-year EFS. These results, if validated in a larger study, may be practice changing.

Published
2022

6. Long-Term Follow-up of a Phase III Study of ch14.18 (Dinutuximab) + Cytokine Immunotherapy in Children with High-Risk Neuroblastoma: COG Study ANBL0032Long-Term Follow-up of Immunotherapy for Neuroblastoma

Author

Yu, Alice L, Gilman, Andrew L, Ozkaynak, M Fevzi, Naranjo, Arlene, Diccianni, Mitchell B, Gan, Jacek, Hank, Jacquelyn A, Batova, Ayse, London, Wendy B, Tenney, Sheena C, Smith, Malcolm, Shulkin, Barry L, Parisi, Marguerite, Matthay, Katherine K, Cohn, Susan L, Maris, John M, Bagatell, Rochelle, Park, Julie R, and Sondel, Paul M

Subjects
Immunization, Rare Diseases, Cancer, Neurosciences, Neuroblastoma, Clinical Trials and Supportive Activities, Pediatric, Vaccine Related, Pediatric Cancer, Prevention, Clinical Research, Adolescent, Antibodies, Monoclonal, Antineoplastic Combined Chemotherapy Protocols, Child, Child, Preschool, Follow-Up Studies, Humans, Infant, Interleukin-2, Isotretinoin, Male, Progression-Free Survival, Recombinant Proteins, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

PurposePreviously our randomized phase III trial demonstrated that immunotherapy including dinutuximab, a chimeric anti-GD2 mAb, GM-CSF, and IL2 improved survival for children with high-risk neuroblastoma that had responded to induction and consolidation therapy. These results served as the basis for FDA approval of dinutuximab. We now present long-term follow-up results and evaluation of predictive biomarkers.Patients and methodsPatients recieved six cycles of isotretinoin with or without five cycles of immunotherapy which consists of dinutuximab with GM-CSF alternating with IL2. Accrual was discontinued early due to meeting the protocol-defined stopping rule for efficacy, as assessed by 2-year event-free survival (EFS). Plasma levels of dinutuximab, soluble IL2 receptor (sIL2R), and human anti-chimeric antibody (HACA) were assessed by ELISA. Fcγ receptor 2A and 3A genotypes were determined by PCR and direct sequencing.ResultsFor 226 eligible randomized patients, 5-year EFS was 56.6 ± 4.7% for patients randomized to immunotherapy (n = 114) versus 46.1 ± 5.1% for those randomized to isotretinoin only (n = 112; P = 0.042). Five-year overall survival (OS) was 73.2 ± 4.2% versus 56.6 ± 5.1% for immunotherapy and isotretinoin only patients, respectively (P = 0.045). Thirteen of 122 patients receiving dinutuximab developed HACA. Plasma levels of dinutuximab, HACA, and sIL2R did not correlate with EFS/OS, or clinically significant toxicity. Fcγ receptor 2A and 3A genotypes did not correlate with EFS/OS.ConclusionsImmunotherapy with dinutuximab improved outcome for patients with high-risk neuroblastoma. Early stoppage for efficacy resulted in a smaller sample size than originally planned, yet clinically significant long-term differences in survival were observed.

Published
2021

7. Irinotecan, Temozolomide, and Dinutuximab With GM-CSF in Children With Refractory or Relapsed Neuroblastoma: A Report From the Children's Oncology Group.

Author

Mody, Rajen, Yu, Alice L, Naranjo, Arlene, Zhang, Fan F, London, Wendy B, Shulkin, Barry L, Parisi, Marguerite T, Servaes, Sabah-E-Noor, Diccianni, Mitchell B, Hank, Jacquelyn A, Felder, Mildred, Birstler, Jennifer, Sondel, Paul M, Asgharzadeh, Shahab, Glade-Bender, Julia, Katzenstein, Howard, Maris, John M, Park, Julie R, and Bagatell, Rochelle

Subjects
Clinical Trials and Supportive Activities, Neurosciences, Cancer, Pediatric, Clinical Research, Rare Diseases, Pediatric Cancer, Neuroblastoma, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Adolescent, Antibodies, Monoclonal, Antineoplastic Combined Chemotherapy Protocols, Child, Child, Preschool, Female, Granulocyte-Macrophage Colony-Stimulating Factor, Humans, Immunotherapy, Infant, Irinotecan, Male, Survival Analysis, Temozolomide, Clinical Sciences, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

PurposeThe combination of irinotecan, temozolomide, dintuximab, and granulocyte-macrophage colony-stimulating factor (I/T/DIN/GM-CSF) demonstrated activity in patients with relapsed/refractory neuroblastoma in the randomized Children's Oncology Group ANBL1221 trial. To more accurately assess response rate and toxicity, an expanded cohort was nonrandomly assigned to I/T/DIN/GM-CSF.Patients and methodsPatients were eligible at first relapse or first designation of refractory disease. Oral T and intravenous (IV) irinotecan were administered on days 1 to 5 of 21-day cycles. DIN was administered IV (days 2-5), and GM-CSF was administered subcutaneously (days 6-12). The primary end point was objective response, analyzed on an intent-to-treat basis per the International Neuroblastoma Response Criteria.ResultsSeventeen eligible patients were randomly assigned to I/T/DIN/GM-CSF (February 2013 to March 2015); 36 additional patients were nonrandomly assigned to I/T/DIN/GM-CSF (August 2016 to May 2017). Objective (complete or partial) responses were observed in nine (52.9%) of 17 randomly assigned patients (95% CI, 29.2% to 76.7%) and 13 (36.1%) of 36 expansion patients (95% CI, 20.4% to 51.8%). Objective responses were seen in 22 (41.5%) of 53 patients overall (95% CI, 28.2% to 54.8%); stable disease was also observed in 22 of 53. One-year progression-free and overall survival for all patients receiving I/T/DIN/GM-CSF were 67.9% ± 6.4% (95% CI, 55.4% to 80.5%) and 84.9% ± 4.9% (95% CI, 75.3% to 94.6%), respectively. Two patients did not receive protocol therapy and were evaluable for response but not toxicity. Common grade ≥ 3 toxicities were fever/infection (18 [35.3%] of 51), neutropenia (17 [33.3%] of 51), pain (15 [29.4%] of 51), and diarrhea (10 [19.6%] of 51). One patient met protocol-defined criteria for unacceptable toxicity (grade 4 hypoxia). Higher DIN trough levels were associated with response.ConclusionI/T/DIN/GM-CSF has significant antitumor activity in patients with relapsed/refractory neuroblastoma. Study of chemoimmunotherapy in the frontline setting is indicated, as is further evaluation of predictive biomarkers.

Published
2020

9. A Phase II Trial of Hu14.18K322A in Combination with Induction Chemotherapy in Children with Newly Diagnosed High-Risk Neuroblastoma

Author

Furman, Wayne L, Federico, Sara M, McCarville, Mary Beth, Shulkin, Barry L, Davidoff, Andrew M, Krasin, Matthew J, Sahr, Natasha, Sykes, April, Wu, Jianrong, Brennan, Rachel C, Bishop, Michael William, Helmig, Sara, Stewart, Elizabeth, Navid, Fariba, Triplett, Brandon, Santana, Victor M, Bahrami, Armita, Anthony, Gwendolyn, Yu, Alice L, Hank, Jacquelyn, Gillies, Stephen D, Sondel, Paul M, Leung, Wing H, and Pappo, Alberto S

Subjects
Clinical Trials and Supportive Activities, Neuroblastoma, Rare Diseases, Cancer, Neurosciences, Pediatric, Pediatric Cancer, Clinical Research, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Adolescent, Adult, Antibodies, Monoclonal, Humanized, Antineoplastic Combined Chemotherapy Protocols, Child, Disease-Free Survival, Female, Gangliosides, Granulocyte-Macrophage Colony-Stimulating Factor, Humans, Induction Chemotherapy, Kaplan-Meier Estimate, Killer Cells, Natural, Male, Progression-Free Survival, Prospective Studies, Young Adult, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

PurposeWe sought to evaluate whether combining a humanized antidisialoganglioside mAb (hu14.18K322A) with induction chemotherapy improves early responses and outcomes in children with newly diagnosed high-risk neuroblastoma.Patients and methodsWe conducted a prospective nonrandomized, single-arm, two-stage, phase II clinical trial. Six courses of induction chemotherapy were coadministered with hu14.18K322A and followed with granulocyte-macrophage colony-stimulating factor (GM-CSF) and low-dose IL2. Consolidation was performed with a busulfan/melphalan preparative regimen. An additional course of hu14.18K322A was administered with parent-derived natural killer cells, when available, during consolidation. Hu14.18K322A, GM-CSF, IL2, and isotretinoin were then administered. Secondary outcomes included reduced tumor volume and semiquantitative 123I-metaiodobenzylguanidine scoring [i.e., Curie scores (CS)] at the end of induction.ResultsForty-two patients received hu14.18K322A and induction chemotherapy. This regimen was well tolerated, with continuous-infusion narcotics adjusted to patient tolerance. Partial responses (PR) or better after the first two chemoimmunotherapy courses occurred in 32 patients [76.2%; 95% confidence interval (CI), 60.6-88.0]. This was accompanied by primary tumor volume reductions (median, -76%; range, -100% to 5%). Of 35 patients with stage IV disease who completed induction, 31 had end-of-induction CSs of 2 or less. No patients experienced progression during induction. Two-year event-free survival (EFS) was 85.7% (95% CI, 70.9-93.3).ConclusionsAdding hu14.18K322A to induction chemotherapy produced early PR or better in most patients, reduced tumor volumes, improved CSs at the end of induction, and yielded an encouraging 2-year EFS. These results, if validated in a larger study, may change the standard of care for children with high-risk neuroblastoma.

Published
2019

10. Multifunctional nanoparticle potentiates the in situ vaccination effect of radiation therapy and enhances response to immune checkpoint blockade

Author

Zhang, Ying, Sriramaneni, Raghava N., Clark, Paul A., Jagodinsky, Justin C., Ye, Mingzhou, Jin, Wonjong, Wang, Yuyuan, Bates, Amber, Kerr, Caroline P., Le, Trang, Allawi, Raad, Wang, Xiuxiu, Xie, Ruosen, Havighurst, Thomas C., Chakravarty, Ishan, Rakhmilevich, Alexander L., O’Leary, Kathleen A., Schuler, Linda A., Sondel, Paul M., Kim, Kyungmann, Gong, Shaoqin, and Morris, Zachary S.

Published
2022
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12. Intratumoral radiation dose heterogeneity augments antitumor immunity in mice and primes responses to checkpoint blockade.

Author

Jagodinsky, Justin C., Vera, Jessica M., Jin, Won Jong, Shea, Amanda G., Clark, Paul A., Sriramaneni, Raghava N., Havighurst, Thomas C., Chakravarthy, Ishan, Allawi, Raad H., Kim, KyungMann, Harari, Paul M., Sondel, Paul M., Newton, Michael A., Crittenden, Marka R., Gough, Michael J., Miller, Jessica R., Ong, Irene M., and Morris, Zachary S.

Subjects
IMMUNE checkpoint inhibitors, TYPE I interferons, ANTIGEN presentation, RADIATION doses, T cells
Abstract

Radiation therapy (RT) activates multiple immunologic effects in the tumor microenvironment (TME), with diverse dose-response relationships observed. We hypothesized that, in contrast with homogeneous RT, a heterogeneous RT dose would simultaneously optimize activation of multiple immunogenic effects in a single TME, resulting in a more effective antitumor immune response. Using high-dose-rate brachytherapy, we treated mice bearing syngeneic tumors with a single fraction of heterogeneous RT at a dose ranging from 2 to 30 gray. When combined with dual immune checkpoint inhibition in murine models, heterogeneous RT generated more potent antitumor responses in distant, nonirradiated tumors compared with any homogeneous dose. The antitumor effect after heterogeneous RT required CD4 and CD8 T cells and low-dose RT to a portion of the tumor. At the 3-day post-RT time point, dose heterogeneity imprinted the targeted TME with spatial differences in immune-related gene expression, antigen presentation, and susceptibility of tumor cells to immune-mediated destruction. At a later 10-day post-RT time point, high-, moderate-, or low-RT-dose regions demonstrated distinct infiltrating immune cell populations. This was associated with an increase in the expression of effector-associated cytokines in circulating CD8 T cells. Consistent with enhanced adaptive immune priming, heterogeneous RT promoted clonal expansion of effector CD8 T cells. These findings illuminate the breadth of dose-dependent effects of RT on the TME and the capacity of heterogeneous RT to promote antitumor immunity when combined with immune checkpoint inhibitors. Editor's summary: Radiation therapy (RT) is usually administered as a single dose across a tumor. However, not all radiation doses are created equal. High radiation doses promote immunogenic cell death, medium radiation doses promote type I interferon responses, and low radiation doses promote inflammatory cytokine production and immune cell trafficking. To reap the benefits of all three doses, Jagodinsky et al. treated murine tumors with heterogeneous RT, where different regions of the tumor were treated with different RT doses. The authors found that this heterogeneous approach outperformed homogeneous dose RT in a T cell–dependent manner and could be combined with immune checkpoint inhibition. These data support further clinical development of heterogeneous RT. —Courtney Malo [ABSTRACT FROM AUTHOR]

Published
2024
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13. Neuroblastoma Patients' KIR and KIR-Ligand Genotypes Influence Clinical Outcome for Dinutuximab-based Immunotherapy: A Report from the Children's Oncology Group

Author

Erbe, Amy K, Wang, Wei, Carmichael, Lakeesha, Kim, KyungMann, Mendonça, Eneida A, Song, Yiqiang, Hess, Dustin, Reville, Patrick K, London, Wendy B, Naranjo, Arlene, Hank, Jacquelyn A, Diccianni, Mitchell B, Reisfeld, Ralph A, Gillies, Stephen D, Matthay, Katherine K, Cohn, Susan L, Hogarty, Michael D, Maris, John M, Park, Julie R, Ozkaynak, M Fevzi, Gilman, Andrew L, Yu, Alice L, and Sondel, Paul M

Subjects
Neurosciences, Immunization, Pediatric, Cancer, Rare Diseases, Pediatric Research Initiative, Clinical Trials and Supportive Activities, Neuroblastoma, Genetics, Clinical Research, Pediatric Cancer, Vaccine Related, Antibodies, Monoclonal, Antineoplastic Agents, Immunological, Cell Line, Tumor, Clinical Trials, Phase III as Topic, Female, Genotype, Humans, Immunotherapy, Ligands, Male, Receptors, KIR, Receptors, KIR2DL1, Receptors, KIR3DL1, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

Purpose: In 2010, a Children's Oncology Group (COG) phase III randomized trial for patients with high-risk neuroblastoma (ANBL0032) demonstrated improved event-free survival (EFS) and overall survival (OS) following treatment with an immunotherapy regimen of dinutuximab, GM-CSF, IL2, and isotretinoin compared with treatment with isotretinoin alone. Dinutuximab, a chimeric anti-GD2 monoclonal antibody, acts in part via natural killer (NK) cells. Killer immunoglobulin-like receptors (KIR) on NK cells and their interactions with KIR-ligands can influence NK cell function. We investigated whether KIR/KIR-ligand genotypes were associated with EFS or OS in this trial.Experimental Design: We genotyped patients from COG study ANBL0032 and evaluated the effect of KIR/KIR-ligand genotypes on clinical outcomes. Cox regression models and log-rank tests were used to evaluate associations of EFS and OS with KIR/KIR-ligand genotypes.Results: In this trial, patients with the "all KIR-ligands present" genotype as well as patients with inhibitory KIR2DL2 with its ligand (HLA-C1) together with inhibitory KIR3DL1 with its ligand (HLA-Bw4) were associated with improved outcome if they received immunotherapy. In contrast, for patients with the complementary KIR/KIR-ligand genotypes, clinical outcome was not significantly different for patients who received immunotherapy versus those receiving isotretinoin alone.Conclusions: These data show that administration of immunotherapy is associated with improved outcome for neuroblastoma patients with certain KIR/KIR-ligand genotypes, although this was not seen for patients with other KIR/KIR-ligand genotypes. Further investigation of KIR/KIR-ligand genotypes may clarify their role in cancer immunotherapy and may enable KIR/KIR-ligand genotyping to be used prospectively for identifying patients likely to benefit from certain cancer immunotherapy regimens. Clin Cancer Res; 24(1); 189-96. ©2017 AACRSee related commentary by Cheung and Hsu, p. 3.

Published
2018

14. Corrigendum: A Comprehensive Safety Trial of Chimeric Antibody 14.18 With GM-CSF, IL-2, and Isotretinoin in High-Risk Neuroblastoma Patients Following Myeloablative Therapy: Children's Oncology Group Study ANBL0931.

Author

Ozkaynak, M Fevzi, Gilman, Andrew L, London, Wendy B, Naranjo, Arlene, Diccianni, Mitchell B, Tenney, Sheena C, Smith, Malcolm, Messer, Karen S, Seeger, Robert, Reynolds, C Patrick, Smith, L Mary, Shulkin, Barry L, Parisi, Marguerite, Maris, John M, Park, Julie R, Sondel, Paul M, and Yu, Alice L

Subjects
anti-GD2 chimeric antibody, cytokine biomarkers, cytokines, immunotherapy, neuroblastoma, safety, Immunology, Medical Microbiology
Abstract

[This corrects the article DOI: 10.3389/fimmu.2018.01355.].

Published
2018

15. A Comprehensive Safety Trial of Chimeric Antibody 14.18 With GM-CSF, IL-2, and Isotretinoin in High-Risk Neuroblastoma Patients Following Myeloablative Therapy: Children's Oncology Group Study ANBL0931.

Author

Ozkaynak, M Fevzi, Gilman, Andrew L, London, Wendy B, Naranjo, Arlene, Diccianni, Mitchell B, Tenney, Sheena C, Smith, Malcolm, Messer, Karen S, Seeger, Robert, Reynolds, C Patrick, Smith, L Mary, Shulkin, Barry L, Parisi, Marguerite, Maris, John M, Park, Julie R, Sondel, Paul M, and Yu, Alice L

Subjects
anti-GD2 chimeric antibody, cytokine biomarkers, cytokines, immunotherapy, neuroblastoma, safety, Neurosciences, Pediatric Research Initiative, Pediatric Cancer, Neuroblastoma, Clinical Trials and Supportive Activities, Clinical Research, Pediatric, Rare Diseases, Orphan Drug, Vaccine Related, Immunization, Cancer, Patient Safety, 6.2 Cellular and gene therapies, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Immunology, Medical Microbiology
Abstract

PurposeA phase 3 randomized study (COG ANBL0032) demonstrated significantly improved outcome by adding immunotherapy with ch14.18 antibody to isotretinoin as post-consolidation therapy for high-risk neuroblastoma (NB). This study, ANBL0931, was designed to collect FDA-required safety/toxicity data to support FDA registration of ch14.18.Experimental designNewly diagnosed high-risk NB patients who achieved at least a partial response to induction therapy and received myeloablative consolidation with stem cell rescue were enrolled to receive six courses of isotretinoin with five concomitant cycles of ch14.18 combined with GM-CSF or IL2. Ch14.18 infusion time was 10-20 h per dose. Blood was collected for cytokine analysis and its association with toxicities and outcome.ResultsOf 105 patients enrolled, five patients developed protocol-defined unacceptable toxicities. The most common grade ≥ 3 non-hematologic toxicities of immunotherapy for cycles 1-5, respectively, were neuropathic pain (41, 28, 22, 31, 24%), hypotension (10, 17, 4, 14, 8%), allergic reactions (ARs) (3, 10, 5, 7, 2%), capillary leak syndrome (1, 4, 0, 2, 0%), and fever (21, 59, 6, 32, 5%). The 3-year event-free survival and overall survival were 67.6 ± 4.8% and 79.1 ± 4.2%, respectively. AR during course 1 was associated with elevated serum levels of IL-1Ra and IFNγ, while severe hypotension during this course was associated with low IL5 and nitrate. Higher pretreatment CXCL9 level was associated with poorer event-free survival (EFS).ConclusionThis study has confirmed the significant, but manageable treatment-related toxicities of this immunotherapy and identified possible cytokine biomarkers associated with select toxicities and outcome. EFS and OS appear similar to that previously reported on ANBL0032.

Published
2018

16. Bispecific GD2 x B7-H3 Antibody Improves Tumor Targeting and Reduces Toxicity while Maintaining Efficacy for Neuroblastoma

Author

Erbe, Amy K, primary, Feils, Arika S, additional, Hampton, Alina, additional, Rosenkrans, Zachary T, additional, Felder, Mildred, additional, Wiwczar, Jessica, additional, Gerhardt, Daniel J., additional, Bercher, Mark, additional, Wenke, Belinda, additional, Haertle, Callie, additional, Heck, Mackenzie, additional, VandenHeuvel, Sabrina N., additional, Frankel, Elizabeth, additional, Nielsen, Megan, additional, Spiegelman, Dan, additional, Tsarovsky, Noah, additional, Zaborek, Jen, additional, Rakhmilevich, Alexander L., additional, Hank, Jacquelyn A., additional, Aluicio-Sarduy, Eduardo, additional, Engle, Jonathan, additional, Davis, Jonathan H., additional, Glaser, Bryan, additional, Subbotin, Vladimir, additional, Green, Roland, additional, Hernandez, Reinier T, additional, Hammer, Bonnie, additional, and Sondel, Paul M., additional

Published
2024
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17. Irinotecan–temozolomide with temsirolimus or dinutuximab in children with refractory or relapsed neuroblastoma (COG ANBL1221): an open-label, randomised, phase 2 trial

Author

Mody, Rajen, Naranjo, Arlene, Van Ryn, Collin, Yu, Alice L, London, Wendy B, Shulkin, Barry L, Parisi, Marguerite T, Servaes, Sabah-E-Noor, Diccianni, Mitchell B, Sondel, Paul M, Bender, Julia G, Maris, John M, Park, Julie R, and Bagatell, Rochelle

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Clinical Trials and Supportive Activities, Neurosciences, Neuroblastoma, Rare Diseases, Patient Safety, Cancer, Pediatric Cancer, Pediatric, Clinical Research, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Adolescent, Alanine Transaminase, Anemia, Antibodies, Monoclonal, Antineoplastic Combined Chemotherapy Protocols, Camptothecin, Child, Child, Preschool, Dacarbazine, Disease-Free Survival, Fever, Ganglioneuroblastoma, Gene Amplification, Granulocyte-Macrophage Colony-Stimulating Factor, Humans, Hypokalemia, Hypoxia, Infant, Infections, Irinotecan, N-Myc Proto-Oncogene Protein, Neoplasm Recurrence, Local, Neutropenia, Pain, Response Evaluation Criteria in Solid Tumors, Retreatment, Sirolimus, Survival Rate, Temozolomide, Thrombocytopenia, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

BackgroundOutcomes for children with relapsed and refractory neuroblastoma are dismal. The combination of irinotecan and temozolomide has activity in these patients, and its acceptable toxicity profile makes it an excellent backbone for study of new agents. We aimed to test the addition of temsirolimus or dinutuximab to irinotecan-temozolomide in patients with relapsed or refractory neuroblastoma.MethodsFor this open-label, randomised, phase 2 selection design trial of the Children's Oncology Group (COG; ANBL1221), patients had to have histological verification of neuroblastoma or ganglioneuroblastoma at diagnosis or have tumour cells in bone marrow with increased urinary catecholamine concentrations at diagnosis. Patients of any age were eligible at first designation of relapse or progression, or first designation of refractory disease, provided organ function requirements were met. Patients previously treated for refractory or relapsed disease were ineligible. Computer-based randomisation with sequence generation defined by permuted block randomisation (block size two) was used to randomly assign patients (1:1) to irinotecan and temozolomide plus either temsirolimus or dinutuximab, stratified by disease category, previous exposure to anti-GD2 antibody therapy, and tumour MYCN amplification status. Patients in both groups received oral temozolomide (100 mg/m2 per dose) and intravenous irinotecan (50 mg/m2 per dose) on days 1-5 of 21-day cycles. Patients in the temsirolimus group also received intravenous temsirolimus (35 mg/m2 per dose) on days 1 and 8, whereas those in the dinutuximab group received intravenous dinutuximab (17·5 mg/m2 per day or 25 mg/m2 per day) on days 2-5 plus granulocyte macrophage colony-stimulating factor (250 μg/m2 per dose) subcutaneously on days 6-12. Patients were given up to a maximum of 17 cycles of treatment. The primary endpoint was the proportion of patients achieving an objective (complete or partial) response by central review after six cycles of treatment, analysed by intention to treat. Patients, families, and those administering treatment were aware of group assignment. This study is registered with ClinicalTrials.gov, number NCT01767194, and follow-up of the initial cohort is ongoing.FindingsBetween Feb 22, 2013, and March 23, 2015, 36 patients from 27 COG member institutions were enrolled on this groupwide study. One patient was ineligible (alanine aminotransferase concentration was above the required range). Of the remaining 35 patients, 18 were randomly assigned to irinotecan-temozolomide-temsirolimus and 17 to irinotecan-temozolomide-dinutuximab. Median follow-up was 1·26 years (IQR 0·68-1·61) among all eligible participants. Of the 18 patients assigned to irinotecan-temozolomide-temsirolimus, one patient (6%; 95% CI 0·0-16·1) achieved a partial response. Of the 17 patients assigned to irinotecan-temozolomide-dinutuximab, nine (53%; 95% CI 29·2-76·7) had objective responses, including four partial responses and five complete responses. The most common grade 3 or worse adverse events in the temsirolimus group were neutropenia (eight [44%] of 18 patients), anaemia (six [33%]), thrombocytopenia (five [28%]), increased alanine aminotransferase (five [28%]), and hypokalaemia (four [22%]). One of the 17 patients assigned to the dinutuximab group refused treatment after randomisation; the most common grade 3 or worse adverse events in the remaining 16 patients evaluable for safety were pain (seven [44%] of 16), hypokalaemia (six [38%]), neutropenia (four [25%]), thrombocytopenia (four [25%]), anaemia (four [25%]), fever and infection (four [25%]), and hypoxia (four [25%]); one patient had grade 4 hypoxia related to therapy that met protocol-defined criteria for unacceptable toxicity. No deaths attributed to protocol therapy occurred.InterpretationIrinotecan-temozolomide-dinutuximab met protocol-defined criteria for selection as the combination meriting further study whereas irinotecan-temozolomide-temsirolimus did not. Irinotecan-temozolomide-dinutuximab shows notable anti-tumour activity in patients with relapsed or refractory neuroblastoma. Further evaluation of biomarkers in a larger cohort of patients might identify those most likely to respond to this chemoimmunotherapeutic regimen.FundingNational Cancer Institute.

Published
2017

18. HLA-Bw4-I-80 Isoform Differentially Influences Clinical Outcome As Compared to HLA-Bw4-T-80 and HLA-A-Bw4 Isoforms in Rituximab or Dinutuximab-Based Cancer Immunotherapy

Author

Erbe, Amy K, Wang, Wei, Reville, Patrick K, Carmichael, Lakeesha, Kim, KyungMann, Mendonca, Eneida A, Song, Yiqiang, Hank, Jacquelyn A, London, Wendy B, Naranjo, Arlene, Hong, Fangxin, Hogarty, Michael D, Maris, John M, Park, Julie R, Ozkaynak, MF, Miller, Jeffrey S, Gilman, Andrew L, Kahl, Brad, Yu, Alice L, and Sondel, Paul M

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Oncology and Carcinogenesis, Immunology, Clinical Trials and Supportive Activities, Immunization, Rare Diseases, Cancer, Hematology, Clinical Research, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, KIR, KIR-ligand, HLA-Bw4, HLA, MHC class I, natural killer cells, cancer immunotherapy, Medical Microbiology, Biochemistry and cell biology, Genetics
Abstract

Killer-cell immunoglobulin-like receptors (KIRs) are a family of glycoproteins expressed primarily on natural killer cells that can regulate their function. Inhibitory KIRs recognize MHC class I molecules (KIR-ligands) as ligands. We have reported associations of KIRs and KIR-ligands for patients in two monoclonal antibody (mAb)-based trials: (1) A Children's Oncology Group (COG) trial for children with high-risk neuroblastoma randomized to immunotherapy treatment with dinutuximab (anti-GD2 mAb) + GM-CSF + IL-2 + isotretinion or to treatment with isotretinoin alone and (2) An Eastern Cooperative Oncology Group (ECOG) trial for adults with low-tumor burden follicular lymphoma responding to an induction course of rituximab (anti-CD20 mAb) and randomized to treatment with maintenance rituximab or no-maintenance rituximab. In each trial, certain KIR/KIR-ligand genotypes were associated with clinical benefit for patients randomized to immunotherapy treatment (immunotherapy in COG; maintenance rituximab in ECOG) as compared to patients that did not receive the immunotherapy [isotretinoin alone (COG); no-maintenance (ECOG)]. Namely, patients with both KIR3DL1 and its HLA-Bw4 ligand (KIR3DL1+/HLA-Bw4+ genotype) had improved clinical outcomes if randomized to immunotherapy regimens, as compared to patients with the KIR3DL1+/HLA-Bw4+ genotype randomized to the non-immunotherapy regimen. Conversely, patients that did not have the KIR3DL1+/HLA-Bw4+ genotype showed no evidence of a difference in outcome if receiving the immunotherapy vs. no-immunotherapy. For each trial, HLA-Bw4 status was determined by assessing the genotypes of three separate isoforms of HLA-Bw4: (1) HLA-B-Bw4 with threonine at amino acid 80 (B-Bw4-T80); (2) HLA-B-Bw4 with isoleucine at amino acid 80 (HLA-B-Bw4-I80); and (3) HLA-A with a Bw4 epitope (HLA-A-Bw4). Here, we report on associations with clinical outcome for patients with KIR3DL1 and these separate isoforms of HLA-Bw4. Patients randomized to immunotherapy with KIR3DL1+/A-Bw4+ or with KIR3DL1+/B-Bw4-T80+ had better outcome vs. those randomized to no-immunotherapy, whereas for those with KIR3DL1+/B-Bw4-I80+ there was no evidence of a difference based on immunotherapy vs. no-immunotherapy. Additionally, we observed differences within treatment types (either within immunotherapy or no-immunotherapy) that were associated with the genotype status for the different KIR3DL1/HLA-Bw4-isoforms. These studies suggest that specific HLA-Bw4 isoforms may differentially influence response to these mAb-based immunotherapy, further confirming the involvement of KIR-bearing cells in tumor-reactive mAb-based cancer immunotherapy.

Published
2017

20. A combined radio-immunotherapy regimen eradicates late-stage tumors in mice.

Author

Rakhmilevich, Alexander L., Tsarovsky, Noah W., Felder, Mildred, Zaborek, Jen, Moram, Sritha, Erbe, Amy K., Pieper, Alexander A., Spiegelman, Dan V., Cheng, Emily M., Witt, Cole M., Overwijk, Willem W., Morris, Zachary S., and Sondel, Paul M.

Subjects
TREATMENT effectiveness, IMMUNOLOGIC memory, T cells, LABORATORY mice, IMMUNOTHERAPY, NEUROBLASTOMA
Abstract

Background: The majority of experimental approaches for cancer immunotherapy are tested against relatively small tumors in tumor-bearing mice, because in most cases advanced cancers are resistant to the treatments. In this study, we asked if even late-stage mouse tumors can be eradicated by a rationally designed combined radio-immunotherapy (CRI) regimen. Methods: CRI consisted of local radiotherapy, intratumoral IL-12, slow-release systemic IL-2 and anti-CTLA-4 antibody. Therapeutic effects of CRI against several weakly immunogenic and immunogenic mouse tumors including B78 melanoma, MC38 and CT26 colon carcinomas and 9464D neuroblastoma were evaluated. Immune cell depletion and flow cytometric analysis were performed to determine the mechanisms of the antitumor effects. Results: Tumors with volumes of 2,000 mm³ or larger were eradicated by CRI. Flow analyses of the tumors revealed reduction of T regulatory (Treg) cells and increase of CD8/Treg ratios following CRI. Rapid shrinkage of the treated tumors did not require T cells, whereas T cells were involved in the systemic effect against the distant tumors. Cured mice developed immunological memory. Conclusions: These findings underscore that rationally designed combination immunotherapy regimens can be effective even against large, late-stage tumors. [ABSTRACT FROM AUTHOR]

Published
2024
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23. Evaluation of a Combinatorial Immunotherapy Regimen That Can Cure Mice Bearing MYCN-Driven High-Risk Neuroblastoma That Resists Current Clinical Therapy.

Author

Zebertavage, Lauren, Schopf, Allison, Nielsen, Megan, Matthews, Joel, Erbe, Amy K., Aiken, Taylor J., Katz, Sydney, Sun, Claire, Witt, Cole M., Rakhmilevich, Alexander L., and Sondel, Paul M.

Subjects
NEUROBLASTOMA, IMMUNOTHERAPY, MICE, IRINOTECAN, TEMOZOLOMIDE, MONOCLONAL antibodies
Abstract

Background: Incorporating GD2-targeting monoclonal antibody into post-consolidation maintenance therapy has improved survival for children with high-risk neuroblastoma. However, ~50% of patients do not respond to, or relapse following, initial treatment. Here, we evaluated additional anti-GD2-based immunotherapy to better treat high-risk neuroblastoma in mice to develop a regimen for patients with therapy-resistant neuroblastoma. Methods: We determined the components of a combined regimen needed to cure mice of established MYCN-amplified, GD2-expressing, murine 9464D-GD2 neuroblastomas. Results: First, we demonstrate that 9464D-GD2 is nonresponsive to a preferred salvage regimen: anti-GD2 with temozolomide and irinotecan. Second, we have previously shown that adding agonist anti-CD40 mAb and CpG to a regimen of radiotherapy, anti-GD2/IL2 immunocytokine and anti-CTLA-4, cured a substantial fraction of mice bearing small 9464D-GD2 tumors; here, we further characterize this regimen by showing that radiotherapy and hu14.18-IL2 are necessary components, while anti-CTLA-4, anti-CD40, or CpG can individually be removed, and CpG and anti-CTLA-4 can be removed together, while maintaining efficacy. Conclusions: We have developed and characterized a regimen that can cure mice of a high-risk neuroblastoma that is refractory to the current clinical regimen for relapsed/refractory disease. Ongoing preclinical work is directed towards ways to potentially translate these findings to a regimen appropriate for clinical testing. [ABSTRACT FROM AUTHOR]

Published
2024
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25. 87 Monitoringin vivoCD8 T and tumor cell metabolic changes in solid tumors during anin situvaccine using autofluorescence imaging

Author

Heaton, Alexa R, primary, Hoefges, Anna, additional, Burkard, Nathaniel J, additional, Feils, Arika S, additional, Tsarovsky, Noah W, additional, Lublin, Garrett M, additional, Hampton, Alina A, additional, Erbe-Gurel, Amy K, additional, Rakhmilevich, Alexander L, additional, Sondel, Paul M, additional, and Skala, Melissa C, additional

Published
2023
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26. 141 C57BL/6 mice cured of B78 melanoma frequently develop antibodies that recognize a 4 amino acid binding motif (SDTG)

Author

Hoefges, Anna, primary, Sondel, Paul M, additional, Mathers, Nicholas, additional, Mcilwain, Sean J, additional, Tetreault, Kaitlin, additional, Hampton, Alina A, additional, Feils, Arika S, additional, Tsarovsky, Noah W, additional, Garcia, Brad H, additional, Patel, Jigar, additional, Morris, Zachary, additional, Erbe-Gurel, Amy K, additional, and Ong, Irene, additional

Published
2023
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29. Phase I trial of fenretinide delivered orally in a novel organized lipid complex in patients with relapsed/refractory neuroblastoma: A report from the new approaches to neuroblastoma therapy (NANT) consortium

Author

Maurer, Barry J, Kang, Min H, Villablanca, Judith G, Janeba, Jitka, Groshen, Susan, Matthay, Katherine K, Sondel, Paul M, Maris, John M, Jackson, Hollie A, Goodarzian, Fariba, Shimada, Hiroyuki, Czarnecki, Scarlett, Hasenauer, Beth, Reynolds, C Patrick, and Marachelian, Araz

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Pediatric, Clinical Trials and Supportive Activities, Cancer, Pediatric Cancer, Neuroblastoma, Rare Diseases, Neurosciences, Clinical Research, Adolescent, Adult, Antineoplastic Agents, Child, Child, Preschool, Female, Fenretinide, Humans, Male, Maximum Tolerated Dose, Neoplasm Recurrence, Local, Young Adult, fenretinide, LYM-X-SORB, neuroblastoma, pediatric, powder, LYM-X-SORB™, Paediatrics and Reproductive Medicine, Oncology & Carcinogenesis, Oncology and carcinogenesis, Paediatrics
Abstract

BackgroundA phase I study was conducted to determine the maximum-tolerated dose, dose-limiting toxicities (DLTs), and pharmacokinetics of fenretinide (4-HPR) delivered in an oral powderized lipid complex (LXS) in patients with relapsed/refractory neuroblastoma.Procedure4-HPR/LXS powder (352-2,210 mg/m(2) /day) was administered on Days 0-6, in 21-day courses, by standard 3 + 3 design.ResultsThirty-two patients (median age = 8 years, range 3-27 years) enrolled with 30 evaluable for dose escalation. Prior therapies included stem cell transplantation/support (n = 26), 13-cis-retinoic acid (n = 22), (125/131) I-MIBG (n = 13), and anti-GD2 antibody (n = 6). 170+ courses were delivered. Course 1 DLTs were a Grade 3 (n = 1) alkaline phosphatase at 352 mg/m(2) /day. Other major toxicities were Grade 4 (n = 1) alkaline phosphatases on Courses 5 and 6 at 774 mg/m(2) /day, and Grade 3 (n = 1) ALT/AST elevation on Course 2 at 1,700 mg/m(2) /day. Of 29 response-evaluable patients, six had stable disease (SD) (4-26 courses); four with marrow- or bone disease-only had complete responses (CR) (10-46 courses). 4-HPR plasma levels were several folds higher (P

Published
2013

30. Combined innate and adaptive immunotherapy overcomes resistance of immunologically cold syngeneic murine neuroblastoma to checkpoint inhibition

Author

Voeller, Julie, Erbe, Amy K., Slowinski, Jacob, Rasmussen, Kayla, Carlson, Peter M., Hoefges, Anna, VandenHeuvel, Sabrina, Stuckwisch, Ashley, Wang, Xing, Gillies, Stephen D., Patel, Ravi B., Farrel, Alvin, Rokita, Jo Lynne, Maris, John, Hank, Jacquelyn A., Morris, Zachary S., Rakhmilevich, Alexander L., and Sondel, Paul M.

Published
2019
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31. Comparative Study of the Effect of Radiation Delivered by Lutetium-177 or Actinium-225 on Anti-GD2 Chimeric Antigen Receptor T Cell Viability and Functions.

Author

Sodji, Quaovi H., Forsberg, Matthew H., Cappabianca, Dan, Kerr, Caroline P., Sarko, Lauren, Shea, Amanda, Adam, David P., Eickhoff, Jens C., Ong, Irene M., Hernandez, Reinier, Weichert, Jamey, Bednarz, Bryan P., Saha, Krishanu, Sondel, Paul M., Capitini, Christian M., and Morris, Zachary S.

Subjects
IN vitro studies, FLOW cytometry, COMBINATION drug therapy, NEUROBLASTOMA, MELANOMA, CELL receptors, RADIOISOTOPES, COMPARATIVE studies, CELL survival, GENE expression, RADIOPHARMACEUTICALS, RESEARCH funding, RADIOTHERAPY, T cells, THERAPEUTICS
Abstract

Simple Summary: Low-dose radiation delivered by radionuclides stimulates an immune response against cancer. We hypothesize that this type of low-dose radiation can potentiate chimeric antigen receptor (CAR) T cell therapy against solid tumors. Before evaluating the combination of these therapies in vivo, we aim to determine the impacts of this type of low-dose radiation on CAR T cell viability and functions to guide the selection of the type of radionuclide (actinium-225 or lutetium-177), the dose of radiation (1, 2 or 6 Gy) and how to best sequence their administration. It follows that increasing the radiation dose results in lower CAR T cell viability while enhancing their killing potential to the same extent. At a similar dose, radiation delivered by actinium-225 is more toxic to CAR T cells than lutetium-177. This suggests that 1 or 2 Gy delivered by lutetium-177 may be optimal for in vivo combination studies with CAR T cells. Background and purpose. Chimeric antigen receptor (CAR) T cells have been relatively ineffective against solid tumors. Low-dose radiation which can be delivered to multiple sites of metastases by targeted radionuclide therapy (TRT) can elicit immunostimulatory effects. However, TRT has never been combined with CAR T cells against solid tumors in a clinical setting. This study investigated the effects of radiation delivered by Lutetium-177 (177Lu) and Actinium-225 (225Ac) on the viability and effector function of CAR T cells in vitro to evaluate the feasibility of such therapeutic combinations. After the irradiation of anti-GD2 CAR T cells with various doses of radiation delivered by 177Lu or 225Ac, their viability and cytotoxic activity against GD2-expressing human CHLA-20 neuroblastoma and melanoma M21 cells were determined by flow cytometry. The expression of the exhaustion marker PD-1, activation marker CD69 and the activating receptor NKG2D was measured on the irradiated anti-GD2 CAR T cells. Both 177Lu and 225Ac displayed a dose-dependent toxicity on anti-GD2 CAR T cells. However, radiation enhanced the cytotoxic activity of these CAR T cells against CHLA-20 and M21 irrespective of the dose tested and the type of radionuclide. No significant changes in the expression of PD-1, CD69 and NKG2D was noted on the CAR T cells following irradiation. Given a lower CAR T cell viability at equal doses and an enhancement of cytotoxic activity irrespective of the radionuclide type, 177Lu-based TRT may be preferred over 225Ac-based TRT when evaluating a potential synergism between these therapies in vivo against solid tumors. [ABSTRACT FROM AUTHOR]

Published
2024
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33. Pilot trial of the hu14.18-IL2 immunocytokine in patients with completely resectable recurrent stage III or stage IV melanoma

Author

Albertini, Mark R., Yang, Richard K., Ranheim, Erik A., Hank, Jacquelyn A., Zuleger, Cindy L., Weber, Sharon, Neuman, Heather, Hartig, Greg, Weigel, Tracey, Mahvi, David, Henry, Mary Beth, Quale, Renae, McFarland, Thomas, Gan, Jacek, Carmichael, Lakeesha, Kim, KyungMann, Loibner, Hans, Gillies, Stephen D., and Sondel, Paul M.

Published
2018
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35. Abstract 2389: In vivo multiphoton autofluorescence imaging is sensitive to CD8 T cell and tumor cell metabolic changes during immunotherapy in a murine melanoma model

Author

Heaton, Alexa R., primary, Hoefges, Anna, additional, Rehani, Peter R., additional, Burkard, Nathaniel J., additional, Feils, Arika S., additional, Spiegelman, Dan V., additional, Tsarovsky, Noah W., additional, Hampton, Alina A., additional, Gurel, Amy K. Erbe, additional, Rakhmilevich, Alexander L., additional, Sondel, Paul M., additional, and Skala, Melissa C., additional

Published
2023
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36. Abstract 4142: CD4 T cell-driven response to immunotherapy against mouse melanoma tumors

Author

Erbe, Amy K., primary, Feils, Arika S., additional, Hampton, Alina, additional, Spiegelman, Dan, additional, Tsarovsky, Noah, additional, Hoefges, Anna, additional, Carlson, Peter M., additional, Pieper, Alex, additional, Haertle, Callie, additional, Heck, Mackenzie, additional, VandenHeuvel, Sabrina, additional, Frankel, Lizzie, additional, Zebertavage, Lauren, additional, Heaton, Alexa, additional, Morris, Zachary S., additional, Patel, Ravi, additional, Rakhmilevich, Alexander, additional, and Sondel, Paul M., additional

Published
2023
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37. Figure S1 from Tumor-Specific Inhibition of In Situ Vaccination by Distant Untreated Tumor Sites

Author

Morris, Zachary S., primary, Guy, Emily I., primary, Werner, Lauryn R., primary, Carlson, Peter M., primary, Heinze, Clinton M., primary, Kler, Jasdeep S., primary, Busche, Sara M., primary, Jaquish, Abigail A., primary, Sriramaneni, Raghava N., primary, Carmichael, Lakeesha L., primary, Loibner, Hans, primary, Gillies, Stephen D., primary, Korman, Alan J., primary, Erbe, Amy K., primary, Hank, Jacquelyn A., primary, Rakhmilevich, Alexander L., primary, Harari, Paul M., primary, and Sondel, Paul M., primary

Published
2023
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38. Data from Tumor-Specific Inhibition of In Situ Vaccination by Distant Untreated Tumor Sites

Author

Morris, Zachary S., primary, Guy, Emily I., primary, Werner, Lauryn R., primary, Carlson, Peter M., primary, Heinze, Clinton M., primary, Kler, Jasdeep S., primary, Busche, Sara M., primary, Jaquish, Abigail A., primary, Sriramaneni, Raghava N., primary, Carmichael, Lakeesha L., primary, Loibner, Hans, primary, Gillies, Stephen D., primary, Korman, Alan J., primary, Erbe, Amy K., primary, Hank, Jacquelyn A., primary, Rakhmilevich, Alexander L., primary, Harari, Paul M., primary, and Sondel, Paul M., primary

Published
2023
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39. Supplemental Figure Legends from Tumor-Specific Inhibition of In Situ Vaccination by Distant Untreated Tumor Sites

Author

Morris, Zachary S., primary, Guy, Emily I., primary, Werner, Lauryn R., primary, Carlson, Peter M., primary, Heinze, Clinton M., primary, Kler, Jasdeep S., primary, Busche, Sara M., primary, Jaquish, Abigail A., primary, Sriramaneni, Raghava N., primary, Carmichael, Lakeesha L., primary, Loibner, Hans, primary, Gillies, Stephen D., primary, Korman, Alan J., primary, Erbe, Amy K., primary, Hank, Jacquelyn A., primary, Rakhmilevich, Alexander L., primary, Harari, Paul M., primary, and Sondel, Paul M., primary

Published
2023
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40. Supplementary Materials from Clinically Relevant Cytotoxic Immune Cell Signatures and Clonal Expansion of T-Cell Receptors in High-Risk MYCN-Not-Amplified Human Neuroblastoma

Author

Wei, Jun S., primary, Kuznetsov, Igor B., primary, Zhang, Shile, primary, Song, Young K., primary, Asgharzadeh, Shahab, primary, Sindiri, Sivasish, primary, Wen, Xinyu, primary, Patidar, Rajesh, primary, Najaraj, Sushma, primary, Walton, Ashley, primary, Auvil, Jaime M. Guidry, primary, Gerhard, Daniela S., primary, Yuksel, Aysen, primary, Catchpoole, Daniel, primary, Hewitt, Stephen M., primary, Sondel, Paul M., primary, Seeger, Robert, primary, Maris, John M., primary, and Khan, Javed, primary

Published
2023
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41. Supplementary Table 1. from A Pilot Trial of Humanized Anti-GD2 Monoclonal Antibody (hu14.18K322A) with Chemotherapy and Natural Killer Cells in Children with Recurrent/Refractory Neuroblastoma

Author

Federico, Sara M., primary, McCarville, M. Beth, primary, Shulkin, Barry L., primary, Sondel, Paul M., primary, Hank, Jacquelyn A., primary, Hutson, Paul, primary, Meagher, Michael, primary, Shafer, Aaron, primary, Ng, Catherine Y., primary, Leung, Wing, primary, Janssen, William E., primary, Wu, Jianrong, primary, Mao, Shenghua, primary, Brennan, Rachel C., primary, Santana, Victor M., primary, Pappo, Alberto S., primary, and Furman, Wayne L., primary

Published
2023
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42. Supplementary Figure from Stress Keratin 17 Expression in Head and Neck Cancer Contributes to Immune Evasion and Resistance to Immune-Checkpoint Blockade

Author

Wang, Wei, primary, Lozar, Taja, primary, Golfinos, Athena E., primary, Lee, Denis, primary, Gronski, Ellery, primary, Ward-Shaw, Ella, primary, Hayes, Mitchell, primary, Bruce, Justine Y., primary, Kimple, Randall J., primary, Hu, Rong, primary, Harari, Paul M., primary, Xu, Jin, primary, Keske, Aysenur, primary, Sondel, Paul M., primary, Fitzpatrick, Megan B., primary, Dinh, Huy Q., primary, and Lambert, Paul F., primary

Published
2023
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43. Supplemental Figure SF-04 from Outcome-Related Signatures Identified by Whole Transcriptome Sequencing of Resectable Stage III/IV Melanoma Evaluated after Starting Hu14.18-IL2

Author

Yang, Richard K., primary, Kuznetsov, Igor B., primary, Ranheim, Erik A., primary, Wei, Jun S., primary, Sindiri, Sivasish, primary, Gryder, Berkley E., primary, Gangalapudi, Vineela, primary, Song, Young K., primary, Patel, Viharkumar, primary, Hank, Jacquelyn A., primary, Zuleger, Cindy, primary, Erbe, Amy K., primary, Morris, Zachary S., primary, Quale, Renae, primary, Kim, KyungMann, primary, Albertini, Mark R., primary, Khan, Javed, primary, and Sondel, Paul M., primary

Published
2023
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44. SUPPLEMENTAL MATERIALS from Neuroblastoma Patients' KIR and KIR-Ligand Genotypes Influence Clinical Outcome for Dinutuximab-based Immunotherapy: A Report from the Children's Oncology Group

Author

Erbe, Amy K., primary, Wang, Wei, primary, Carmichael, Lakeesha, primary, Kim, KyungMann, primary, Mendonça, Eneida A., primary, Song, Yiqiang, primary, Hess, Dustin, primary, Reville, Patrick K., primary, London, Wendy B., primary, Naranjo, Arlene, primary, Hank, Jacquelyn A., primary, Diccianni, Mitchell B., primary, Reisfeld, Ralph A., primary, Gillies, Stephen D., primary, Matthay, Katherine K., primary, Cohn, Susan L., primary, Hogarty, Michael D., primary, Maris, John M., primary, Park, Julie R., primary, Ozkaynak, M. Fevzi, primary, Gilman, Andrew L., primary, Yu, Alice L., primary, and Sondel, Paul M., primary

Published
2023
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45. Supplementary Table S4 from Clinically Relevant Cytotoxic Immune Cell Signatures and Clonal Expansion of T-Cell Receptors in High-Risk MYCN-Not-Amplified Human Neuroblastoma

Author

Wei, Jun S., primary, Kuznetsov, Igor B., primary, Zhang, Shile, primary, Song, Young K., primary, Asgharzadeh, Shahab, primary, Sindiri, Sivasish, primary, Wen, Xinyu, primary, Patidar, Rajesh, primary, Najaraj, Sushma, primary, Walton, Ashley, primary, Auvil, Jaime M. Guidry, primary, Gerhard, Daniela S., primary, Yuksel, Aysen, primary, Catchpoole, Daniel, primary, Hewitt, Stephen M., primary, Sondel, Paul M., primary, Seeger, Robert, primary, Maris, John M., primary, and Khan, Javed, primary

Published
2023
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46. Supplementary Table 2. from A Pilot Trial of Humanized Anti-GD2 Monoclonal Antibody (hu14.18K322A) with Chemotherapy and Natural Killer Cells in Children with Recurrent/Refractory Neuroblastoma

Author

Federico, Sara M., primary, McCarville, M. Beth, primary, Shulkin, Barry L., primary, Sondel, Paul M., primary, Hank, Jacquelyn A., primary, Hutson, Paul, primary, Meagher, Michael, primary, Shafer, Aaron, primary, Ng, Catherine Y., primary, Leung, Wing, primary, Janssen, William E., primary, Wu, Jianrong, primary, Mao, Shenghua, primary, Brennan, Rachel C., primary, Santana, Victor M., primary, Pappo, Alberto S., primary, and Furman, Wayne L., primary

Published
2023
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47. Supplementary Figures from Clinically Relevant Cytotoxic Immune Cell Signatures and Clonal Expansion of T-Cell Receptors in High-Risk MYCN-Not-Amplified Human Neuroblastoma

Author

Wei, Jun S., primary, Kuznetsov, Igor B., primary, Zhang, Shile, primary, Song, Young K., primary, Asgharzadeh, Shahab, primary, Sindiri, Sivasish, primary, Wen, Xinyu, primary, Patidar, Rajesh, primary, Najaraj, Sushma, primary, Walton, Ashley, primary, Auvil, Jaime M. Guidry, primary, Gerhard, Daniela S., primary, Yuksel, Aysen, primary, Catchpoole, Daniel, primary, Hewitt, Stephen M., primary, Sondel, Paul M., primary, Seeger, Robert, primary, Maris, John M., primary, and Khan, Javed, primary

Published
2023
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48. Supplementary Data from Long-Term Follow-up of a Phase III Study of ch14.18 (Dinutuximab) + Cytokine Immunotherapy in Children with High-Risk Neuroblastoma: COG Study ANBL0032

Author

Yu, Alice L., primary, Gilman, Andrew L., primary, Ozkaynak, M. Fevzi, primary, Naranjo, Arlene, primary, Diccianni, Mitchell B., primary, Gan, Jacek, primary, Hank, Jacquelyn A., primary, Batova, Ayse, primary, London, Wendy B., primary, Tenney, Sheena C., primary, Smith, Malcolm, primary, Shulkin, Barry L., primary, Parisi, Marguerite, primary, Matthay, Katherine K., primary, Cohn, Susan L., primary, Maris, John M., primary, Bagatell, Rochelle, primary, Park, Julie R., primary, and Sondel, Paul M., primary

Published
2023
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49. Supplementary Figure 2. from A Pilot Trial of Humanized Anti-GD2 Monoclonal Antibody (hu14.18K322A) with Chemotherapy and Natural Killer Cells in Children with Recurrent/Refractory Neuroblastoma

Author

Federico, Sara M., primary, McCarville, M. Beth, primary, Shulkin, Barry L., primary, Sondel, Paul M., primary, Hank, Jacquelyn A., primary, Hutson, Paul, primary, Meagher, Michael, primary, Shafer, Aaron, primary, Ng, Catherine Y., primary, Leung, Wing, primary, Janssen, William E., primary, Wu, Jianrong, primary, Mao, Shenghua, primary, Brennan, Rachel C., primary, Santana, Victor M., primary, Pappo, Alberto S., primary, and Furman, Wayne L., primary

Published
2023
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50. Table S3 from Neuroblastoma Patients' KIR and KIR-Ligand Genotypes Influence Clinical Outcome for Dinutuximab-based Immunotherapy: A Report from the Children's Oncology Group

Author

Erbe, Amy K., primary, Wang, Wei, primary, Carmichael, Lakeesha, primary, Kim, KyungMann, primary, Mendonça, Eneida A., primary, Song, Yiqiang, primary, Hess, Dustin, primary, Reville, Patrick K., primary, London, Wendy B., primary, Naranjo, Arlene, primary, Hank, Jacquelyn A., primary, Diccianni, Mitchell B., primary, Reisfeld, Ralph A., primary, Gillies, Stephen D., primary, Matthay, Katherine K., primary, Cohn, Susan L., primary, Hogarty, Michael D., primary, Maris, John M., primary, Park, Julie R., primary, Ozkaynak, M. Fevzi, primary, Gilman, Andrew L., primary, Yu, Alice L., primary, and Sondel, Paul M., primary

Published
2023
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