Your search keyword '"Govind Ragupathi"' showing total 79 results

1. Correction: Mitochondrial Ceramide-Rich Macrodomains Functionalize Bax upon Irradiation.

Author

Hyunmi Lee, Jimmy A Rotolo, Judith Mesicek, Tuula Penate-Medina, Andreas Rimner, Wen-Chieh Liao, Xianglei Yin, Govind Ragupathi, Desiree Ehleiter, Erich Gulbins, Dayong Zhai, John C Reed, Adriana Haimovitz-Friedman, Zvi Fuks, and Richard Kolesnick

Subjects

Medicine, Science

Published

2015

2. Mitochondrial ceramide-rich macrodomains functionalize Bax upon irradiation.

Author

Hyunmi Lee, Jimmy A Rotolo, Judith Mesicek, Tuula Penate-Medina, Andreas Rimner, Wen-Chieh Liao, Xianglei Yin, Govind Ragupathi, Desiree Ehleiter, Erich Gulbins, Dayong Zhai, John C Reed, Adriana Haimovitz-Friedman, Zvi Fuks, and Richard Kolesnick

Subjects

Medicine, Science

Abstract

BACKGROUND:Evidence indicates that Bax functions as a "lipidic" pore to regulate mitochondrial outer membrane permeabilization (MOMP), the apoptosis commitment step, through unknown membrane elements. Here we show mitochondrial ceramide elevation facilitates MOMP-mediated cytochrome c release in HeLa cells by generating a previously-unrecognized mitochondrial ceramide-rich macrodomain (MCRM), which we visualize and isolate, into which Bax integrates. METHODOLOGY/PRINCIPAL FINDINGS:MCRMs, virtually non-existent in resting cells, form upon irradiation coupled to ceramide synthase-mediated ceramide elevation, optimizing Bax insertion/oligomerization and MOMP. MCRMs are detected by confocal microscopy in intact HeLa cells and isolated biophysically as a light membrane fraction from HeLa cell lysates. Inhibiting ceramide generation using a well-defined natural ceramide synthase inhibitor, Fumonisin B1, prevented radiation-induced Bax insertion, oligomerization and MOMP. MCRM deconstruction using purified mouse hepatic mitochondria revealed ceramide alone is non-apoptogenic. Rather Bax integrates into MCRMs, oligomerizing therein, conferring 1-2 log enhanced cytochrome c release. Consistent with this mechanism, MCRM Bax isolates as high molecular weight "pore-forming" oligomers, while non-MCRM membrane contains exclusively MOMP-incompatible monomeric Bax. CONCLUSIONS/SIGNIFICANCE:Our recent studies in the C. elegans germline indicate that mitochondrial ceramide generation is obligate for radiation-induced apoptosis, although a mechanism for ceramide action was not delineated. Here we demonstrate that ceramide, generated in the mitochondrial outer membrane of mammalian cells upon irradiation, forms a platform into which Bax inserts, oligomerizes and functionalizes as a pore. We posit conceptualization of ceramide as a membrane-based stress calibrator, driving membrane macrodomain organization, which in mitochondria regulates intensity of Bax-induced MOMP, and is pharmacologically tractable in vitro and in vivo.

Published

2011

3. Data from Human Monoclonal Antibodies to Sialyl-Lewisa (CA19.9) with Potent CDC, ADCC, and Antitumor Activity

Author

Wolfgang W. Scholz, Philip O. Livingston, Govind Ragupathi, Feng Hong, Xiaohong Wu, Shu-Man Sun, and Ritsuko Sawada

Abstract

Purpose: The carbohydrate antigen sialyl-Lewisa (sLea), also known as CA19.9, is widely expressed on epithelial tumors of the gastrointestinal tract and breast and on small-cell lung cancers. Since overexpression of sLea appears to be a key event in invasion and metastasis of many tumors and results in susceptibility to antibody-mediated lysis, sLea is an attractive molecular target for tumor therapy.Experimental Design: We generated and characterized fully human monoclonal antibodies (mAb) from blood lymphocytes from individuals immunized with a sLea–KLH vaccine.Results: Several mAbs were selected based on ELISA and FACS including two mAbs with high affinity for sLea (5B1 and 7E3, binding affinities 0.14 and 0.04 nmol/L, respectively) and further characterized. Both antibodies were specific for Neu5Acα2–3Galβ1–3(Fucα1–4)GlcNAcβ as determined by glycan array analysis. Complement-dependent cytotoxicity against DMS-79 cells was higher (EC50 0.1 μg/mL vs. 1.7 μg/mL) for r7E3 (IgM) than for r5B1 (IgG1). In addition, r5B1 antibodies showed high level of antibody-dependent cell-mediated cytotoxicity activity on DMS-79 cells with human NK cells or peripheral blood mononuclear cells. To evaluate in vivo efficacy, the antibodies were tested in a xenograft model with Colo205 tumor cells engrafted into SCID (severe combined immunodeficient mice) mice. Treatment during the first 21 days with four doses of r5B1 (100 μg per dose) doubled the median survival time to 207 days, and three of five animals survived with six doses.Conclusion: On the basis of the potential of sLea as a target for immune attack and their affinity, specificity, and effector functions, 5B1and 7E3 may have clinical utility. Clin Cancer Res; 17(5); 1024–32. ©2011 AACR.

Published

2023

4. Supplementary Figure Legends from Accelerated Tumor Growth Mediated by Sublytic Levels of Antibody-Induced Complement Activation Is Associated with Activation of the PI3K/AKT Survival Pathway

Author

Philip O. Livingston, Feng Hong, Katherine Panageas, Govind Ragupathi, and Xiaohong Wu

Abstract

Legend for supplementary figures - PDF file 62K, Supplementary Figure Legend

Published

2023

5. Data from Accelerated Tumor Growth Mediated by Sublytic Levels of Antibody-Induced Complement Activation Is Associated with Activation of the PI3K/AKT Survival Pathway

Author

Philip O. Livingston, Feng Hong, Katherine Panageas, Govind Ragupathi, and Xiaohong Wu

Abstract

Purpose: We addressed the possibility that low levels of tumor cell-bound antibodies targeting gangliosides might accelerate tumor growth.Experimental Design: To test this hypothesis, we treated mice with a range of monoclonal antibody (mAb) doses against GM2, GD2, GD3, and CD20 after challenge with tumors expressing these antigens and tested the activity of the same mAbs in vitro. We also explored the mechanisms behind the complement-mediated tumor growth acceleration that we observed and an approach to overcome it.Results: Serologically detectable levels of IgM-mAb against GM2 are able to delay or prevent tumor growth of high GM2 expressing cell lines both in vitro and in a SCID mouse model, whereas very low levels of this mAb resulted in slight but consistent acceleration of tumor growth in both settings. Surprisingly, this is not restricted to IgM mAb targeting GM2 but consistent against an IgG mAb targeting GD3 as well. These findings were mirrored by in vitro studies with antibodies against these antigens as well as GD2 and CD20 (with Rituxan), and shown to be complement-dependent in all cases. Complement-mediated accelerated growth of cultured tumor cell lines initiated by low mAb levels was associated with activation of the phosphoinositide 3-kinase (PI3K)/AKT survival pathway and significantly elevated levels of both p-AKT and p-PRAS40. This complement-mediated PI3K activation and accelerated tumor growth in vitro and in vivo are eliminated by PI3K inhibitors NVP-BEZ235 and Wortmannin. These PI3K inhibitors also significantly increased efficacy of high doses of these four mAbs.Conclusion: Our findings suggest that manipulation of the PI3K/AKT pathway and its signaling network can significantly increase the potency of passively administered mAbs and vaccine-induced antibodies targeting a variety of tumor cell surface antigens. Clin Cancer Res; 19(17); 4728–39. ©2013 AACR.

Published

2023

6. Supplementary Data from Human Monoclonal Antibodies to Sialyl-Lewisa (CA19.9) with Potent CDC, ADCC, and Antitumor Activity

Author

Wolfgang W. Scholz, Philip O. Livingston, Govind Ragupathi, Feng Hong, Xiaohong Wu, Shu-Man Sun, and Ritsuko Sawada

Abstract

Supplementary Figure S1; Supplementary Tables S1-S2.

Published

2023

7. Supplementary Figure A from Accelerated Tumor Growth Mediated by Sublytic Levels of Antibody-Induced Complement Activation Is Associated with Activation of the PI3K/AKT Survival Pathway

Author

Philip O. Livingston, Feng Hong, Katherine Panageas, Govind Ragupathi, and Xiaohong Wu

Abstract

Supplementary Figure B - PDF file 42K, CHLA136Luc or H524 cells treated with Human sera Complement (HuC') or heat inactivated HuC'(De-HuC') with or without the mAbs (3F8, PGNX and R24) for overnight. De- HuC' was achieved by heating the human complement for 30 min at 56{degree sign}C. Plates were read 2-4hrs after WST-1 addition (1:10 ratio) at 415nm. Figures representing the percent change in cell growth calculated according to formula: (OD of mAb+HuC' or de-HuC' - OD of HuC' or de-HuC')/OD of HuC' or de-HuC') X 100

Published

2023

8. Supplementary Results, Figures 1-2, Table 1 from Cancer Biomarkers Defined by Autoantibody Signatures to Aberrant O-Glycopeptide Epitopes

Author

Henrik Clausen, Joy Burchell, Joyce Taylor-Papadimitriou, Michael A. Hollingsworth, Phil O. Livingston, Govind Ragupathi, Ulla Mandel, Eric P. Bennett, Johannes W. Pedersen, Mads A. Tarp, Ola Blixt, and Hans H. Wandall

Abstract

Supplementary Results, Figures 1-2, Table 1 from Cancer Biomarkers Defined by Autoantibody Signatures to Aberrant O-Glycopeptide Epitopes

Published

2023

9. A randomised phase II trial of a trivalent ganglioside vaccine targeting GM2, GD2 and GD3 combined with immunological adjuvant OPT-821 versus OPT-821 alone in metastatic sarcoma patients rendered disease-free by surgery

Author

Evan Rosenbaum, Rashmi Chugh, Christopher W. Ryan, Mark Agulnik, Mohammed M. Milhem, Suzanne George, Robin L. Jones, Bartosz Chmielowski, Brian A. Van Tine, Hussein Tawbi, Anthony D. Elias, William L. Read, G. Thomas Budd, Li-Xuan Qin, Eve T. Rodler, Joe Hirman, Paul Weiden, Cathryn M. Bennett, Philip O. Livingston, Govind Ragupathi, David Hansen, Sandra P. D'Angelo, William D. Tap, Gary K. Schwartz, Robert G. Maki, and Richard D. Carvajal

Subjects

Male, Cancer Research, Vaccines, Oncology, Adjuvants, Immunologic, Humans, Female, G(M2) Ganglioside, Sarcoma, Soft Tissue Neoplasms, Neoplasms, Second Primary, Injection Site Reaction

Abstract

Recurrence after resection of metastatic sarcoma is common. The gangliosides GM2, GD2 and GD3 are strongly expressed across sarcoma subtypes. We hypothesised that generation of anti-ganglioside antibodies would control micrometastases and improve outcomes in sarcoma patients who were disease-free after metastasectomy.We conducted a randomised phase II trial of the immunological adjuvant OPT-821 with a KLH-conjugated ganglioside vaccine targeting GM2, GD2 and GD3, versus OPT-821 alone in patients with metastatic sarcoma following complete metastasectomy. Patients received 10 subcutaneous injections at Weeks 1, 2, 3, 8, 16, 28, 40, 52, 68 and 84 and were followed for evidence of recurrent disease. The primary end-point was relapse-free survival. Secondary end-points included overall survival and serologic response.A total of 136 patients were randomised, 68 to each arm. The mean age was 51.2, 52.2% were male, 90.4% had relapsed disease, 86.8% had high-grade tumours and 14% had ≥4 metastases resected. Histologies included leiomyosarcoma (33%), spindle cell sarcoma (14%), undifferentiated pleomorphic sarcoma (13%), osteosarcoma (10%), synovial sarcoma (9%), liposarcoma (9%) and others (12%). Most adverse events were Grade ≤2 (83.8% and 70.6% in the vaccine and adjuvant arms, respectively). The most common (≥20% of patients) were injection site reaction (89.7%), fatigue (44.1%) and pyrexia (27.9%) on the vaccine arm, and injection site reaction (69.1%) on the adjuvant only arm. The 1-year relapse-free survival rate (34.5% and 34.8% in the vaccine and OPT-821 monotherapy arm, respectively) did not differ between arms (P = 0.725). One-year overall survival rates were 93.1% and 91.5% in the vaccine and OPT-821 monotherapy arm, respectively (P = 0.578). Serologic responses at week 9 were more frequent on the vaccine arm (96.5% of patients) than in the adjuvant arm (32.8%), and the difference between groups was durable.A sustained serologic response to vaccination was induced with the vaccine, but no difference in recurrence-free or overall survival was observed between treatment arms.gov identifier: NCT01141491.

Published

2022

10. Long-term Outcomes of Patients With Recurrent Ovarian Cancer Treated With a Polyvalent Vaccine With Bevacizumab Combination

Author

Ryan M. Kahn, Govind Ragupathi, Qin C. Zhou, Alexia Iasonos, Sara Kravetz, Martee L. Hensley, Jason A. Konner, Vicky Makker, William P. Tew, Carol Aghajanian, Paul J. Sabbatini, and Roisin E. O’Cearbhaill

Subjects

Cancer Research, Oncology, nervous system, genetic structures, Immunology, Immunology and Allergy, behavioral disciplines and activities, psychological phenomena and processes

Abstract

Background: To characterize the safety, immunogenicity, and outcomes of patients with high-grade serous ovarian cancer (HGSOC) in second or greater remission treated with a polyvalent antigen-KLH plus OPT-821 vaccine construct and bevacizumab. Methods: Patients with recurrent HGSOC were treated with the vaccine plus bevacizumab at our institution from 01/05/2011-03/20/2012. Follow-up continued until 03/2021. Blood/urine samples were collected. “Responders” had an immunogenic response to >3 antigens; “non-responders” to <2 antigens. Results: Twenty-one patients were treated on study. One developed a dose limiting-toxicity (grade 4 fever). Two (10%) experienced bevacizumab-related grade 3 hypertension. Thirteen (68%) and 16 (84%) of 19 responded to ≥3 and ≥2 antigens, respectively (Globo-H, GM2, TF cluster Tn, MUC-1). Four of 21 patients were alive >5 years post-treatment. Responders and non-responders had a median PFS of 4.9 months (95% CI: 2.8-8.1) and 5.0 months (95% CI: 0.7-cannot estimate), respectively; median OS was 30.7 months (95% CI: 16.9-52.0) and 34.2 months (95% CI: 12.8-cannot estimate), respectively. On two-time point analysis (baseline, week 17), increased IL-8 exhibited improved PFS (HR as 10-unit increase, 0.43; p=0.04); increased PDGF exhibited worse OS (HR as 10-unit increase, 1.01; p = 0.02). Conclusions: This is the longest follow-up of vaccine administration with bevacizumab among patients with ovarian cancer. The vaccine was well tolerated with bevacizumab. Response was not associated with improved survival. On two-time point analysis, increased IL-8 was associated with significant improvement in PFS; increased PDGF with significantly worse OS. For all time point measurements, cytokine levels were not significantly associated with survival. Trial registration: NCT01223235

Published

2022

11. Long-term outcomes of patients with recurrent ovarian cancer treated with a polyvalent vaccine with bevacizumab combination

Author

Ryan M, Kahn, Govind, Ragupathi, Qin C, Zhou, Alexia, Iasonos, Sara, Kravetz, Martee L, Hensley, Jason A, Konner, Vicky, Makker, William P, Tew, Carol, Aghajanian, Paul J, Sabbatini, and Roisin E, O'Cearbhaill

Abstract

To characterize the safety, immunogenicity, and outcomes of patients with high-grade serous ovarian cancer (HGSOC) in second or greater remission treated with a polyvalent antigen-KLH plus OPT-821 vaccine construct and bevacizumab.Patients with recurrent HGSOC were treated with the vaccine plus bevacizumab at our institution from 01/05/2011 to 03/20/2012. Follow-up continued until 03/2021. Blood/urine samples were collected. "Responders" had an immunogenic response to ≥ 3 antigens; "non-responders" to ≤ 2 antigens.Twenty-one patients were treated on study. One developed a dose-limiting toxicity (grade 4 fever). Two (10%) experienced bevacizumab-related grade 3 hypertension. Thirteen (68%) and 16 (84%) of 19 responded to ≥ 3 and ≥ 2 antigens, respectively (Globo-H, GM2, TF cluster Tn, MUC-1). Four of 21 patients were alive 5 years post-treatment. Responders and non-responders had a median PFS of 4.9 months (95% CI: 2.8-8.1) and 5.0 months (95% CI: 0.7-cannot estimate), respectively; median OS was 30.7 months (95% CI: 16.9-52.0) and 34.2 months (95% CI: 12.8-cannot estimate), respectively. On two-timepoint analysis (baseline, week 17), increased IL-8 exhibited improved PFS (HR as 10-unit increase, 0.43; p = 0.04); increased PDGF exhibited worse OS (HR as 10-unit increase, 1.01; p = 0.02).This is the longest follow-up of vaccine administration with bevacizumab in patients with ovarian cancer. The vaccine was well tolerated with bevacizumab. Response was not associated with improved survival. On two-timepoint analysis, increased IL-8 was associated with significant improvement in PFS; increased PDGF with significantly worse OS. For all timepoint measurements, cytokine levels were not significantly associated with survival.NCT01223235.

Published

2022

12. Phase I Trial of Oral Yeast-Derived β-Glucan to Enhance Anti-GD2 Immunotherapy of Resistant High-Risk Neuroblastoma

Author

Fiorella Iglesias Cardenas, Audrey Mauguen, Irene Y. Cheung, Kim Kramer, Brian H. Kushner, Govind Ragupathi, Nai-Kong V. Cheung, and Shakeel Modak

Subjects

Cancer Research, neuroblastoma, Oncology, β-glucan, anti-GD2 antibody, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Article, RC254-282

Abstract

Simple Summary Beta glucans, complex polysaccharides, can prime leukocyte dectin-1 and CR3-receptors and enhance anti-tumor cytotoxicity of monoclonal antibodies. In a phase I study (clinicaltrials.gov NCT00492167), we treated patients with intravenous 3F8 (fixed dose of 10 mg/m2/day × 10 days) and oral BG (dose-escalated from 10–200 mg/kg/day × 17 days in cohorts of 3–6 patients each). Forty-four patients completed 141 cycles of therapy with 3F8 + BG. One patient developed DLT: transient self-limiting hepatic transaminase elevation at a BG dose of 120 mg/kg/day. Overall, 1, 3, 12 and 24 evaluable patients had complete response, partial response, stable and progressive disease, respectively, at the end of treatment. Positive human anti-mouse antibody response and dectin-1 rs3901533 polymorphism were associated with better overall survival. BG dose level and serum BG levels did not correlate with response. BG lacked major toxicity and, in combination with 3F8, demonstrated anti-neuroblastoma activity against resistant disease. The recommended phase II dose was established at 40 mg/kg/day. Abstract Beta glucans, complex polysaccharides, prime leukocyte dectin-1 and CR3-receptors and enhance anti-tumor cytotoxicity of complement-activating monoclonal antibodies. We conducted a phase I study (clinicaltrials.gov NCT00492167) to determine the safety of the combination of yeast-derived beta glucan (BG) and anti-GD2 murine monoclonal antibody 3F8 in patients with relapsed or refractory high-risk neuroblastoma. Patients received intravenous 3F8 (fixed dose of 10 mg/m2/day × 10 days) and oral BG (dose-escalated from 10–200 mg/kg/day × 17 days in cohorts of 3–6 patients each). Forty-four patients completed 141 cycles. One patient developed DLT: transient self-limiting hepatic transaminase elevation 5 days after starting BG (120 mg/kg/day). Overall, 1, 3, 12 and 24 evaluable patients had complete response, partial response, stable and progressive disease, respectively, at the end of treatment. Positive human anti-mouse antibody response and dectin-1 rs3901533 polymorphism were associated with better overall survival. BG dose level and serum BG levels did not correlate with response. Progression-free and overall survival at 2 years were 28% and 61%, respectively. BG lacked major toxicity. Treatment with 3F8 plus BG was associated with anti-neuroblastoma responses in patients with resistant disease. Although the maximal tolerated dose for yeast BG was not reached, considering the large volume of oral BG, we recommended 40 mg/kg/day as the phase II dose.

Published

2021

13. Imaging Patients with Metastatic Castration-Resistant Prostate Cancer Using89Zr-DFO-MSTP2109A Anti-STEAP1 Antibody

Author

Shutian Ruan, Daniel C. Danila, Mithat Gonen, Stephen E. Fleming, Michael J. Morris, Joseph A. O'Donoghue, Sarah M. Cheal, Josef J. Fox, Steven M. Larson, John L. Humm, Bernard M. Fine, Govind Ragupathi, Howard I. Scher, Serge K. Lyashchenko, Simon Williams, Jorge A. Carrasquillo, and Neeta Pandit-Taskar

Subjects

Male, 0301 basic medicine, Immunoconjugates, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Antigen, Antigens, Neoplasm, Positron Emission Tomography Computed Tomography, Biopsy, medicine, Humans, Tissue Distribution, Radiology, Nuclear Medicine and imaging, Neoplasm Metastasis, Radiometry, Aged, Aged, 80 and over, Radioisotopes, medicine.diagnostic_test, biology, business.industry, Soft tissue, Middle Aged, medicine.disease, Confidence interval, Prostatic Neoplasms, Castration-Resistant, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Toxicity, biology.protein, Immunohistochemistry, Zirconium, Antibody, Oxidoreductases, Nuclear medicine, business

Abstract

Six-transmembrane epithelial antigen of prostate-1 (STEAP1) is a relatively newly identified target in prostate cancer. We evaluated the ability of PET/CT with (89)Zr-DFO-MSTP2109A, an antibody that recognizes STEAP1, to detect lesions in patients with metastatic castration-resistant prostate cancer (mCRPC). Methods: Nineteen mCRPC patients were prospectively imaged using approximately 185 MBq/10 mg of (89)Zr-DFO-MSTP2109A. (89)Zr-DFO-MSTP2109A PET/CT images obtained 4–7 d after injection were compared with bone and CT scans. Uptake in lesions was measured. Fifteen patients were treated with an antibody–drug conjugate (ADC) based on MSTP2109A; ADC treatment–related data were correlated with tumor uptake by PET imaging. Bone or soft-tissue biopsy samples were evaluated. Results: No significant toxicity occurred. Excellent uptake was observed in bone and soft-tissue disease. Median SUV(max) was 20.6 in bone and 16.8 in soft tissue. Sixteen of 17 lesions biopsied were positive on (89)Zr-DFO-MSTP2109A, and all sites were histologically positive (1 on repeat biopsy). Bayesian analysis resulted in a best estimate of 86% of histologically positive lesions being true-positive on imaging (95% confidence interval, 75%–100%). There was no correlation between SUV(max) tumor uptake and STEAP1 immunohistochemistry, survival after ADC treatment, number of ADC treatment cycles, or change in prostate-specific antigen level. Conclusion: (89)Zr-DFO-MSTP2109A is well tolerated and shows localization in mCRPC sites in bone and soft tissue. Given the high SUV in tumor and localization of a large number of lesions, this reagent warrants further exploration as a companion diagnostic in patients undergoing STEAP1-directed therapy.

Published

2019

14. Abstract 5218: Oral beta-glucan enhanced anti-ganglioside antibody titer after vaccination against high-risk neuroblastoma: Results of a randomized trial

Author

Irene Y. Cheung, Audrey Mauguen, Yi Feng, Govind Ragupathi, Ellen Basu, Stephen S. Roberts, Shakeel Modak, Brian H. Kushner, and Nai-Kong V. Cheung

Subjects

Cancer Research, Oncology

Abstract

Background and Aim: Ganglioside GD2/GD3 vaccine stimulated robust antibody response among patients with high-risk metastatic neuroblastoma (HR-NB) who had prior disease progression (J Clin Oncol 39:215-226, 2020). High anti-GD2-IgG1antibody titer was associated with improved progression-free survival and overall survival in multivariable analyses. A gel formulation of yeast beta-glucan was used as an oral vaccine adjuvant, but its importance remained unproven. Patients and Methods: In a follow-up randomized Phase II trial (Clinicaltrials.gov identifier: NCT00911560), seven vaccine injections at 1, 2, 3, 8, 20, 32 and 52 weeks were administered to patients with HR-NB during their first or subsequent remissions. Each subcutaneous vaccine injection consisted of 30 ug each of GD2 and GD3, which was lactonized and conjugated to keyhole limpet hemocyanin and mixed with the subcutaneous saponin OPT-821 adjuvant at 150 µg/m2. No patients in this analysis received prior ganglioside vaccine. They were randomized to Arm 1 (n=54) receiving no glucan, or Arm 2 (n=53) receiving oral beta-glucan regimen (40 mg/kg/day, 14 days on/14 days off) starting at week 1. From week 6 onwards, all 107 patients received oral beta-glucan regimen through year end or up to disease progression. Serum IgG1 against GD2 and GD3, and IgM against GD2 were measured by ELISA at (right before) each vaccine injection. Wilcoxon rank sum test was used to compare antibody titers between the 2 arms. Results: In both arms, patients had comparable disease status at study entry, with 70% each in first remission. The remaining patients were in second remission after one prior disease progression. Consistently higher antibody response was observed among Arm 2 patients. The primary endpoint was met for anti-GD2-IgG1 titer at vaccine injection #6 at 32 weeks (p=0.08). Per protocol design, statistical significance (p Conclusion: Adding oral yeast beta-glucan as vaccine adjuvant during the first 6 weeks of immunization significantly enhanced the anti-GD2-IgG1 antibody response without added toxicities. Its impact on patient survival will require a longer clinical follow-up. Citation Format: Irene Y. Cheung, Audrey Mauguen, Yi Feng, Govind Ragupathi, Ellen Basu, Stephen S. Roberts, Shakeel Modak, Brian H. Kushner, Nai-Kong V. Cheung. Oral beta-glucan enhanced anti-ganglioside antibody titer after vaccination against high-risk neuroblastoma: Results of a randomized trial [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 5218.

Published

2022

15. Survival Impact of Anti-GD2 Antibody Response in a Phase II Ganglioside Vaccine Trial Among Patients With High-Risk Neuroblastoma With Prior Disease Progression

Author

Ellen M. Basu, Audrey Mauguen, Stephen S. Roberts, Irene Y. Cheung, Brian H. Kushner, Yi Feng, Nai-Kong V. Cheung, Govind Ragupathi, and Shakeel Modak

Subjects

Male, Cancer Research, Time Factors, beta-Glucans, medicine.drug_class, Anti-GD2 Antibody, Monoclonal antibody, Cancer Vaccines, Polymorphism, Single Nucleotide, Immunogenicity, Vaccine, Adjuvants, Immunologic, Neuroblastoma, Gangliosides, medicine, Humans, High risk neuroblastoma, Lectins, C-Type, Child, Ganglioside, Errata, business.industry, Brain Neoplasms, Disease progression, Vaccine trial, Infant, ORIGINAL REPORTS, medicine.disease, Progression-Free Survival, Oncology, Child, Preschool, Immunoglobulin G, Cancer research, Disease Progression, Female, business, Glioblastoma, Biomarkers

Abstract

PURPOSE Anti-GD2 monoclonal antibody (mAb) has proven efficacy in high-risk neuroblastoma (HR-NB). A small phase I GD2/GD3 vaccine trial (n = 15) described long-term survival and a favorable safety profile among patients with a history of disease progression (PD). The kinetics of mounting antibody response to vaccine and its prognostic impact on survival are now investigated in a phase II study (ClinicalTrials.gov identifier: NCT00911560 ). PATIENTS AND METHODS One hundred two patients with HR-NB who achieved remission after salvage therapies were enrolled in this trial. They received seven subcutaneous injections of GD2/GD3 vaccine spanning 1 year plus oral β-glucan starting at week 6 after the third dose of vaccine. Serum anti-vaccine antibody titers were quantified by enzyme-linked immunosorbent assay. Single nucleotide polymorphisms (SNPs) were determined by quantitative polymerase chain reaction. Kaplan-Meier and landmark Cox Regression models were used for survival estimates. RESULTS Patients had a history of one (63%), two (21%), or three to six (16%) episodes of PD. 82% of them progressed following anti-GD2 mAb (m3F8/dinutuximab/naxitamab) therapy. Vaccine-related toxicities were self-limited injection–associated local reactions and fever without any > grade 3 toxicities. The progression-free survival (PFS) was 32% ± 6%, and the overall survival (OS) was 71% ± 7% at 5 years. Serum anti-GD2 (immunoglobulin G1 [IgG1] and IgM) and anti-GD3 (IgG1) titers showed notable increases following the initiation of β-glucan at week 6. There was an association between IgG1 titer and SNP rs3901533 of dectin-1, the β-glucan receptor. Multivariable analyses showed that anti-GD2-IgG1 titer ≥ 150 ng/mL by week 8 was associated with favorable PFS and OS, while having prior episodes of PD and the time from last PD to vaccine were associated with PFS. CONCLUSION GD2/GD3 vaccine plus β-glucan elicited robust antibody responses in patients with HR-NB with prior PD. Higher anti-GD2-IgG1 titer was associated with improved survival.

Published

2020

16. Pharmacokinetics and Biodistribution of [(89)Zr]Zr-DFO-MSTP2109A Anti-STEAP1 Antibody in Metastatic Castration-Resistant Prostate Cancer Patients

Author

Stephen E. Fleming, Volkan Beylergil, Steven M. Larson, Sarah M. Cheal, Howard I. Scher, Shutian Ruan, Jorge A. Carrasquillo, Josef J. Fox, Daniel C. Danila, John L. Humm, Joseph A. O'Donoghue, Neeta Pandit-Taskar, Govind Ragupathi, Simon Williams, Michael J. Morris, Serge K. Lyashchenko, Bernard M. Fine, and Pat Zanzonico

Subjects

Male, medicine.medical_specialty, Biodistribution, Urology, Pharmaceutical Science, Bone Neoplasms, Soft Tissue Neoplasms, 02 engineering and technology, Cross Reactions, Antibodies, Monoclonal, Humanized, 030226 pharmacology & pharmacy, Article, Lesion, 03 medical and health sciences, Prostate cancer, Inhibitory Concentration 50, 0302 clinical medicine, Pharmacokinetics, Prostate, Antigens, Neoplasm, Positron Emission Tomography Computed Tomography, Drug Discovery, Biopsy, medicine, Humans, Tissue Distribution, Prospective Studies, Radioisotopes, medicine.diagnostic_test, business.industry, 021001 nanoscience & nanotechnology, medicine.disease, Prostatic Neoplasms, Castration-Resistant, medicine.anatomical_structure, Positron emission tomography, Immunoglobulin G, Injections, Intravenous, Molecular Medicine, Immunohistochemistry, Zirconium, medicine.symptom, Radiopharmaceuticals, 0210 nano-technology, business, Oxidoreductases

Abstract

Six-transmembrane epithelial antigen of prostate-1 (STEAP1) is a newly identified target in prostate cancer. The use of radiolabeled STEAP1-targeting antibodies with positron emission tomography (PET) may allow for detection of sites of metastatic prostate cancer and may refine patient selection for antigen-directed therapies. This was a prospective study in seven patients with metastatic castration-resistant prostate cancer who had at least one archival biopsy that was STEAP1-positive by immunohistochemistry. Patients received intravenous injections of ~185 MBq and 10 mg of [(89)Zr]Zr-DFO-MSTP2109A, a humanized IgG1 monoclonal antibody directed against STEAP1. PET/CT images, blood samples, and whole-body counts were monitored longitudinally in six patients. Here we report on safety, biodistribution, pharmacokinetics, dose estimates to normal tissues, and initial tumor targeting for this group of patients. There was no significant acute or sub-acute toxicity. Favorable biodistribution and enhanced lesion uptake (in both bone and soft tissue) was observed on imaging using a mass of 10 mg of DFO-MSTP2109A. The best lesion discrimination was seen at the latest imaging time, a median of six days post-administration. Pharmacokinetics showed a median serum T (1/2) Beta of 198 h, volume of central compartment of 3.54 L (similar to plasma volume), and clearance of 19.7 mL/h. The median biologic T ½ for whole-body retention was 469 h. The highest mean absorbed doses to normal organs (mGy/MBq) were 1.18, 1.11, 0.78, 0.73, and 0.71 for liver, heart wall, lung, kidney, and spleen, respectively. Excellent targeting of metastatic prostate sites in both bone and soft tissue was observed, with an optimal imaging time of six days post-administration. The liver and heart were the normal organs that experienced the highest absorbed doses. The pharmacokinetics were similar to other antibodies without major cross-reactivity with normal tissues. A more detailed analysis of lesion targeting in a larger patient population with correlation to immunohistology and standard imaging modalities has been reported.

Published

2019

17. 1238. The Novel Semisynthetic Saponin Adjuvant TQL1055 Enhances the Antibody Response to Pertussis Vaccine with an Improved Tolerability Profile over QS-21

Author

Eric Farris, Govind Ragupathi, Sean R Bennett, Chloe Buzz, Phil Livingston, and Tyler Martin

Subjects

biology, business.industry, Immunogenicity, medicine.medical_treatment, Antibody titer, Pharmacology, Immunoglobulin G, Vaccination, Infectious Diseases, AcademicSubjects/MED00290, Oncology, Antigen, Tolerability, Poster Abstracts, medicine, biology.protein, Pertussis vaccine, business, Adjuvant, medicine.drug

Abstract

Background Acellular pertussis vaccines are better tolerated but less immunogenic than older whole cell vaccines. Novel adjuvants may be useful to enhance their immunogenicity. First-generation natural saponins are potent immuno-enhancers but are highly reactogenic. The novel semisynthetic saponin TQL1055 was evaluated for its potential to enhance the immunogenicity of a commercially available acellular pertussis vaccine as part of a National Institute of Allergy and Infectious Disease (NIAID) funded project. Methods Groups of 10 female C57BL/6J mice were immunized subcutaneously (SC) with Adacel® (containing 0.5 mcg pertussis toxin antigen) alone or in combination with QS-21 at 20 mcg/dose or TQL1055 at 50 mcg/dose on Days 0 and 28. Serum antibody titer to pertussis antigen was determined by ELISA (Alpha Diagnostics) at Days 0, 28, and 42 and geometric mean titers (GMT) in IU/mL were determined. Body weights were measured serially for 7 days after dose 1. Results At 28 days following dose 1, mice receiving TQL1055 had an anti-pertussis toxin IgG GMT of 8492, compared with 2263 in mice receiving QS-21 (p = 0.005). At Day 42, 14 days after dose 2, the GMTs increased to 18719 in the TQL1055 group and 10851 in the QS-21 group (p = 0.0653 vs TQL1055 dose 2; p = 0.6038 vs TQL1055 dose 1). Mice in the Adacel and TQL1055 groups gained weight steadily after dose 1, while mice in the QS-21 group had an average weight loss of 10% from baseline at 3 days after dose 1 (p < 0.0001). Figure 1: TQL1055 Enhances the Antibody Response to Adacel® (Commercial Acellular Pertussis Vaccine) in C57BL/6J Female Mice Figure 2: TQL1055 Shows Enhanced Tolerability (measured by decreased weight loss) Compared to QS-21 Following Subcutaneous Injection in C57BL/6J Female Mice Conclusion TQL1055 enhanced the antibody response to a commercial acellular pertussis vaccine to a greater degree than QS-21. Additionally, TQL1055 was better tolerated than QS-21, with no weight loss after vaccination. These findings suggested that TQL1055 may improve the performance of acellular pertussis vaccines without an increase in reactogenicity. Disclosures Chloe Buzz, BS, Adjuvance Technologies (Employee) Sean R. Bennett, MD PhD, Adjuvance Technologies (Employee) Phil Livingston, MD, Adjuvance Technologies (Consultant, Shareholder) Eric Farris, PhD, Adjuvance Technologies (Employee) Tyler Martin, MD, Adjuvance Technologies (Employee, Shareholder)

Published

2020

18. Abstract LB-092: Survival impact of anti-GD2 antibody response - A phase II ganglioside vaccine trial in relapsed neuroblastoma

Author

Govind Ragupathi, Ellen M. Basu, Irene Y. Cheung, Audrey Mauguen, Stephen S. Roberts, Brian H. Kushner, Nai-Kong V. Cheung, and Shakeel Modak

Subjects

Cancer Research, medicine.medical_specialty, Prognostic variable, business.industry, medicine.medical_treatment, Hazard ratio, Vaccine trial, Antibody titer, Dinutuximab, Salvage therapy, Gastroenterology, Oncology, Internal medicine, Medicine, Seroconversion, business, Adjuvant

Abstract

Background and Aim: High-risk neuroblastoma (HR-NB) relapse carries a dismal prognosis. Recent experience, however, suggests that cure is possible when remission is achieved with salvage therapy that includes anti-GD2 monoclonal antibody (mAb). The long-term survival and the favorable safety profile of gangliosides GD2 and GD3 vaccine among these patients in a Phase I trial (n=15, Clinical Cancer Res 2014) need to be confirmed. Moreover, the kinetics of seroconversion (mounting anti-vaccine antibody response) and its prognostic impact on survival need to be explored. Patients and Methods: In this Phase II trial (Clinicaltrials.gov NCT00911560), 102 HR-NB patients who achieved complete remission after salvage therapy were enrolled. They received 7 subcutaneous vaccine injections (week 1-2-3-8-20-32-52) plus oral beta-glucan (starting in week 6 at 40 mg/kg/day, 14 days on/14 days off). Each subcutaneous vaccine injection consisted of 30 µg each of GD2 and GD3, lactonized and conjugated to keyhole limpet hemocyanin and mixed with the saponin OPT-821 adjuvant. Serum anti-vaccine antibody titers were quantified by ELISA. Kaplan-Meier statistics and landmark Cox Regression models were used for survival estimates and prognostic impact analyses. Results: Among 102 patients, 63% had one, 21% had 2, and 16% had 3-6 prior disease progressions. 83/101 patients had failed prior anti-GD2 mAb (m3F8, dinutuximab, or naxitamab) therapy before vaccine: one mAb (n=62), two mAbs (n=15), or all three (n=6). Common toxicities were self-limited injection-related local reactions and fever. No pain, neuropathy, or grade 3/4 toxicities occurred during or post treatment. Progression-free survival (PFS) was 44%±5% and overall survival (OS) was 88%±4% at 2 years, and 36%±7% and 70%±8% at 5 years, respectively. Serum anti-GD2 (IgG1 and IgM) and anti-GD3 (IgG1) titers had marked increases following the initiation of beta-glucan at week 6. In univariate analyses, favorable prognostic factors included: one versus ≥2 prior disease progressions (PFS p=0.005, OS p=0.04), none versus any prior anti-GD2 mAb failures (PFS p=0.004, OS p=0.01); and the induction of ≥150 ng/ml anti-GD2-IgG1 titers by week 8 (PFS p=0.02, OS p=0.06). Factors not prognostic included: time to first NB progression, MYCN amplification status, anti-GD2-IgM, anti-GD3-IgG1 or anti-KLH-IgG1 titers, and treatment with anti-GD2 mAb right before vaccine. In multivariate analyses, week 8 anti-GD2-IgG1 titer ≥150 ng/ml yielded a hazard ratio (HR) of 0.41 [0.20, 0.83], p=0.01 for PFS, and HR=0.15 [0.02, 1.12], p=0.06 for OS. The second independent prognostic variable was the number of prior disease progressions (≥2 vs 1), yielding HR of 2.12 [1.26, 3.58], p=0.005 for PFS, and HR=2.77 (1.03, 7.47), p=0.04 for OS. Conclusions: Even with prior disease progressions, anti-GD2 (though not anti-GD3) seroconversion was associated with notable long-term survival among HR-NB patients previously thought to be unsalvageable. A randomized trial to assess the role of beta-glucan in seroconversion is actively accruing patients. Citation Format: Irene Y. Cheung, Nai-Kong V. Cheung, Shakeel Modak, Audrey Mauguen, Ellen Basu, Stephen S. Roberts, Govind Ragupathi, Brian H. Kushner. Survival impact of anti-GD2 antibody response - A phase II ganglioside vaccine trial in relapsed neuroblastoma [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr LB-092.

Published

2020

19. HLA-DR peptide occupancy can be regulated with a wide variety of small molecules

Author

Govind Ragupathi, Dana Odukoya, Sanjai Kumar, Francesca Blazekovic, Erika Puleo, George Blanck, Shanitra N. Butler, Karoly Szekeres, Dibyendu Dana, James A. Mauro, and Michael Ramsamooj

Subjects

0301 basic medicine, Immunology, Antigen presentation, Peptide, Human leukocyte antigen, 03 medical and health sciences, Immune system, Antigen, HLA-DR, Humans, Immunology and Allergy, Receptor, Pharmacology, chemistry.chemical_classification, Antigen Presentation, B-Lymphocytes, MHC class II, biology, Histocompatibility Antigens Class II, HLA-DR Antigens, Molecular biology, Cell biology, Antigens, Differentiation, B-Lymphocyte, 030104 developmental biology, chemistry, biology.protein, Research Paper

Abstract

HLA-DR is the most commonly expressed and likely the most medically important human MHC class II, antigen presenting protein. In a normal immune response, HLA-DR binds to antigenic peptide and the HLA-DR/peptide complex binds to a T-cell receptor, thus contributing to T-cell activation and stimulation of an immune response against the antigen. When foreign antigen is not present, HLA-DR binds endogenous peptide which, under normal conditions does not stimulate an immune response. In most cases, the human peptide is CLIP, but a certain percentage of HLA-DR molecules will be present at the cell surface with other human peptides. We have recently shown that cell surface, CLIP/HLA-DR ratios are a measure of peptide heterogeneity, and in particular, changes in CLIP/HLA-DR ratios represent changes in the occupancy of HLA-DR by other, endogenous peptides. For example, treatment of cells with the HDAC inhibitor, Entinostat, leads to an upregulation of Cathepsin L1 and replacement of Cathepsin L1 senstitive peptides with HLA-DR binding, Cathepsin L1 resistant peptides, an alteration that can be at least partially assessed via assessment of CLIP/HLA-DR cell surface ratios. Here we assay for CLIP/HLA-DR ratios following treatment of immortalized B-cells with a variety of common drugs, almost all of which indicate significant changes in the CLIP/HLA-DR ratios. Furthermore, the CLIP/HLA-DR ratio changes parallel the impact of the drug panoply on cell viability, suggesting that alterations in the HLA-DR peptidome are governed by a variety of mechanisms, rather than exclusively dependent on a dedicated peptide loading process. These results raise questions about how FDA approved drugs may affect the immune response, and whether any of these drugs could be useful as vaccine adjuvants?

Published

2015

20. Phase I Trial of a Bivalent Gangliosides Vaccine in Combination with β-Glucan for High-Risk Neuroblastoma in Second or Later Remission

Author

Kim Kramer, Shakeel Modak, Irene Y. Cheung, Nai-Kong V. Cheung, Brian H. Kushner, and Govind Ragupathi

Subjects

Male, Cancer Research, medicine.medical_specialty, Neoplasm, Residual, beta-Glucans, Adolescent, medicine.drug_class, medicine.medical_treatment, Cancer Vaccines, Immunostimulant, Gastroenterology, Article, Neuroblastoma, Antigens, Neoplasm, Gangliosides, Internal medicine, medicine, Humans, Outpatient clinic, Dosing, Child, Neoplasm Staging, Radiotherapy, biology, business.industry, Remission Induction, Immunotherapy, Minimal residual disease, Surgery, Treatment Outcome, Oncology, Child, Preschool, Immunologic adjuvant, Toxicity, biology.protein, Female, Neoplasm Recurrence, Local, business, Keyhole limpet hemocyanin

Abstract

Purpose: To report on a phase I trial designed to find the maximally tolerated dose in children of the immunologic adjuvant OPT-821 in a vaccine containing neuroblastoma-associated antigens (GD2 and GD3; Clinicaltrials.gov NCT00911560). Secondary objectives were to obtain preliminary data on immune response and activity against minimal residual disease (MRD). Treatment also included the immunostimulant β-glucan. Experimental Design: Patients with neuroblastoma in ≥2nd complete/very good partial remission received vaccine subcutaneously (weeks 1–2–3–8–20–32–52). Vaccine contained 30 μg each of GD2 and GD3 stabilized as lactones and conjugated to the immunologic carrier protein keyhole limpet hemocyanin; and OPT-821, which was dose escalated as 50, 75, 100, and 150 μg/m2 per injection. Oral β-glucan (40 mg/kg/day, 14 days on/14 days off) started week 6. Results: The study was completed with 15 patients because there was no dose-limiting toxicity at 150 μg/m2 of OPT-821 (the dosing used in adults). Thirteen of fifteen patients received the entire protocol treatment, including 12 who remain relapse-free at 24+ to 39+ (median 32+) months and 1 who relapsed (single node) at 21 months. Relapse-free survival was 80% ± 10% at 24 months. Vaccine and β-glucan were well tolerated. Twelve of fifteen patients had antibody responses against GD2 and/or GD3. Disappearance of MRD was documented in 6 of 10 patients assessable for response. Conclusions: This immunotherapy program lacks major toxicity and is transportable to any outpatient clinic. Patient outcome is encouraging but the efficacy is uncertain because of the complexity and heterogeneity of prior therapies. A larger phase II trial is underway. Clin Cancer Res; 20(5); 1375–82. ©2014 AACR.

Published

2014

21. Applying PET to Broaden the Diagnostic Utility of the Clinically Validated CA19.9 Serum Biomarker for Oncology

Author

Nerissa Viola-Villegas, Marija Drobjnak, Ritsuko Sawada, Govind Ragupathi, Kuntal K. Sevak, Michael J. Evans, Philip O. Livingston, Jason S. Lewis, Samuel L. Rice, Sean Carlin, Xiaohong Wu, and Wolfgang W. Scholz

Subjects

Oncology, PET imaging, Cell Transformation, CA19.9, Mice, Serum biomarkers, Neoplasms, Monoclonal, Cancer, screening and diagnosis, Tumor, medicine.diagnostic_test, biology, Antibodies, Monoclonal, Detection, Nuclear Medicine & Medical Imaging, Cell Transformation, Neoplastic, Positron emission tomography, Biomedical Imaging, Biomarker (medicine), Female, CA19-9, Antibody, Carbohydrate, medicine.medical_specialty, medicine.drug_class, Clinical Sciences, Bioengineering, Monoclonal antibody, Antibodies, Article, Malignant disease, Cell Line, Pancreatic Cancer, Rare Diseases, Clinical Research, Cell Line, Tumor, Internal medicine, pancreatic adenocarcinoma, Biomarkers, Tumor, medicine, Animals, Humans, Antigens, Tumor-Associated, Carbohydrate, Radiology, Nuclear Medicine and imaging, Antigens, Radioisotopes, Neoplastic, business.industry, Tumor-Associated, medicine.disease, 4.1 Discovery and preclinical testing of markers and technologies, Positron-Emission Tomography, biology.protein, Zirconium, Digestive Diseases, business, Biomarkers

Abstract

UnlabelledDespite their considerable advantages, many circulating biomarkers have well-documented limitations. One prominent shortcoming in oncology is a high frequency of false-positive indications for malignant disease in upfront diagnosis. Because one common cause of false positivism is biomarker production from benign disorders in unrelated host tissues, we hypothesized that probing the sites of biomarker secretion with an imaging tool could be a broadly useful strategy to deconvolute the meaning of foreboding but inconclusive circulating biomarker levels.MethodsIn preparation to address this hypothesis clinically, we developed (89)Zr-5B1, a fully human, antibody-based radiotracer targeting tumor-associated CA19.9 in the preclinical setting.Results(89)Zr-5B1 localized to multiple tumor models representing diseases with undetectable and supraphysiologic serum CA19.9 levels. Among these, (89)Zr-5B1 detected orthotopic models of pancreatic ductal adenocarcinoma, an elusive cancer for which the serum assay is measured in humans but with limited specificity in part because of the frequency of CA19.9 secretion from benign hepatic pathologies.ConclusionIn this report, a general strategy to supplement some of the shortcomings of otherwise highly useful circulating biomarkers with immunoPET is described. To expedite the clinical validation of this model, a human monoclonal antibody to CA19.9 (a highly visible but partially flawed serum biomarker for several cancers) was radiolabeled and evaluated, and the compelling preclinical evidence suggests that the radiotracer may enhance the fidelity of diagnosis and staging of pancreatic ductal adenocarcinoma, a notoriously occult cancer.

Published

2013

22. Accelerated Tumor Growth Mediated by Sublytic Levels of Antibody-Induced Complement Activation Is Associated with Activation of the PI3K/AKT Survival Pathway

Author

Katherine S. Panageas, Govind Ragupathi, Xiaohong Wu, Philip O. Livingston, and Feng Hong

Subjects

Cancer Research, medicine.drug_class, Biology, Monoclonal antibody, Article, Wortmannin, Antibodies, Monoclonal, Murine-Derived, Mice, Phosphatidylinositol 3-Kinases, chemistry.chemical_compound, Antigen, Gangliosidoses, GM2, In vivo, Cell Line, Tumor, Gangliosides, medicine, Animals, Humans, Complement Activation, Protein kinase B, PI3K/AKT/mTOR pathway, Adaptor Proteins, Signal Transducing, Antibodies, Monoclonal, Antigens, CD20, Molecular biology, Complement system, Oncology, chemistry, Antigens, Surface, Monoclonal, Rituximab, Proto-Oncogene Proteins c-akt, Signal Transduction

Abstract

Purpose: We addressed the possibility that low levels of tumor cell-bound antibodies targeting gangliosides might accelerate tumor growth. Experimental Design: To test this hypothesis, we treated mice with a range of monoclonal antibody (mAb) doses against GM2, GD2, GD3, and CD20 after challenge with tumors expressing these antigens and tested the activity of the same mAbs in vitro. We also explored the mechanisms behind the complement-mediated tumor growth acceleration that we observed and an approach to overcome it. Results: Serologically detectable levels of IgM-mAb against GM2 are able to delay or prevent tumor growth of high GM2 expressing cell lines both in vitro and in a SCID mouse model, whereas very low levels of this mAb resulted in slight but consistent acceleration of tumor growth in both settings. Surprisingly, this is not restricted to IgM mAb targeting GM2 but consistent against an IgG mAb targeting GD3 as well. These findings were mirrored by in vitro studies with antibodies against these antigens as well as GD2 and CD20 (with Rituxan), and shown to be complement-dependent in all cases. Complement-mediated accelerated growth of cultured tumor cell lines initiated by low mAb levels was associated with activation of the phosphoinositide 3-kinase (PI3K)/AKT survival pathway and significantly elevated levels of both p-AKT and p-PRAS40. This complement-mediated PI3K activation and accelerated tumor growth in vitro and in vivo are eliminated by PI3K inhibitors NVP-BEZ235 and Wortmannin. These PI3K inhibitors also significantly increased efficacy of high doses of these four mAbs. Conclusion: Our findings suggest that manipulation of the PI3K/AKT pathway and its signaling network can significantly increase the potency of passively administered mAbs and vaccine-induced antibodies targeting a variety of tumor cell surface antigens. Clin Cancer Res; 19(17); 4728–39. ©2013 AACR.

Published

2013

23. Gangliosides

Author

Phil Livingston and Govind Ragupathi

Published

2017

24. A Phase I Study of Unimolecular Pentavalent (Globo-H-GM2-sTn-TF-Tn) Immunization of Patients with Epithelial Ovarian, Fallopian Tube, or Peritoneal Cancer in First Remission

Author

Jianglong Zhu, David R. Spriggs, Ouathek Ouerfelli, Maria Spassova, Sara Kravetz, Samuel J. Danishefsky, Svetlana Mironov, Roisin E. O'Cearbhaill, Paul Sabbatini, Alexia Iasonos, Govind Ragupathi, Qian Wan, and Guangbin Yang

Subjects

0301 basic medicine, Cancer Research, medicine.medical_specialty, peptide vaccine, unimolecular vaccine, QS-21, ovarian cancer, remission, immunogenicity, medicine.medical_treatment, lcsh:RC254-282, Gastroenterology, Article, Pentavalent vaccine, 03 medical and health sciences, 0302 clinical medicine, Antigen, Internal medicine, medicine, biology, business.industry, Immunogenicity, Antibody titer, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, 3. Good health, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Immunology, biology.protein, Peptide vaccine, Ovarian cancer, business, Adjuvant, Keyhole limpet hemocyanin

Abstract

We conducted a phase I study in ovarian cancer patients to evaluate the safety and immunogenicity of a synthetic unimolecular pentavalent carbohydrate vaccine (Globo-H, GM2, sTn, TF, and Tn) supported on a peptide backbone, conjugated to keyhole limpet haemocyanin (KLH), and mixed with immunological adjuvant QS-21. Twenty-four advanced-stage, poor-risk, first-remission ovarian cancer patients were enrolled from January 2011–Septermber 2013. Three dose levels were planned (25, 50, 100 mcg) with three cohorts of six patients each, with an additional 6-patient expansion cohort at the MTD. ELISA serologic IgM and IgG responses for each antigen was defined as positive response if antibody titers were ≥1:80 over the respective patient’s pre-vaccination serum. The study would be considered positive if at least four of 12 patients treated at the MTD showed immune responses for at least three of the five antigens. Twenty-four patients (median age, 54 years [range, 36–68]) were included in the safety analysis. Histology was high-grade serous in 22 patients (92%); 18 had stage III and six stage IV disease. The vaccine was well-tolerated at all doses, with no DLTs. At the highest treated dose, IgG and/or IgM responses were recorded against ≥3 antigens in 9/12 patients (75%), ≥4 in 7/12 (58%), and 5 in 3/12 (25%). With a median follow-up of 19 months (range, 2–39), 20 patients (83%) recurred and six (25%) died. The unimolecular pentavalent vaccine construct was shown to be safe and immunogenic. Such a construct greatly simplifies regulatory requirements and manufacturing, facilitates scalability, and provides adaptability.

Published

2016

25. Saponin QS-21 adjuvants in cancer vaccines

Author

David Y. Gin, Jeffrey Gardner, Govind Ragupathi, and Philip O. Livingston

Subjects

chemistry.chemical_classification, chemistry, business.industry, Saponin, Medicine, Cancer, Pharmacology, business, medicine.disease

Published

2011

26. Immunization with N-propionyl polysialic acid–KLH conjugate in patients with small cell lung cancer is safe and induces IgM antibodies reactive with SCLC cells and bactericidal against group B meningococci

Author

Lauren E. Abrey, Lee M. Krug, Govind Ragupathi, Harold J. Jennings, Ronglai Shen, Chandra Hood, Constantine George, Philip O. Livingston, Feng Hong, and Mark G. Kris

Subjects

Male, Blood Bactericidal Activity, Cancer Research, Lung Neoplasms, Immunology, Neisseria meningitidis, Serogroup B, Polysialic acid, Cancer Vaccines, complex mixtures, Article, Animals, Humans, Immunology and Allergy, Aged, Small cell lung cancer, biology, Minimal residual disease, Middle Aged, Small Cell Lung Carcinoma, Survival Analysis, Vaccination, Immunoglobulin M, Oncology, Immunization, Hemocyanins, Disease Progression, Sialic Acids, biology.protein, Female, Neural cell adhesion molecule, Rabbits, Antibody, Keyhole limpet hemocyanin, Conjugate

Abstract

Polysialic acid (polySA) is a polymer side chain bound to the neural cell adhesion molecule that is extensively expressed on the surface of small cell lung cancer (SCLC) cells. In our previous study, a robust antibody response was noted in patients with SCLC after vaccination with 30 μg of keyhole limpet hemocyanin (KLH)-conjugated N-propionylated (NP-) polySA, but peripheral neuropathy and ataxia were detected in several vaccinated patients. The objectives of the current trial were to establish the lowest optimal dose and to confirm the safety of the induction of antibodies against polySA with the NP-polySA vaccine.Patients with SCLC who completed initial treatment and had no evidence of disease progression were injected with either 10 or 3 μg of NP-polySA conjugated to KLH and mixed with 100 μg of immunologic adjuvant (QS-21) at weeks 1, 2, 3, 4, 8, and 16.Nine patients were enrolled at each of the two dose levels. Prior to vaccination, one patient in each group had low-titer antibodies against polysialic acid. All patients at the 10 μg vaccine dose level responded to vaccination with IgM antibody titers against polysialic acid (median titer 1/1,280 by ELISA), and all but one patient made IgM and IgG antibodies against the artificial vaccine immunogen, NP-polysialic acid (median titer 1/10,240). The antibody responses at the 3 μg vaccine dose level were lower; six of nine patients developed antibodies against polysialic acid (median titer 1/160). Post-vaccination sera from 6/9 and 3/9 patients in the 10 and 3 μg groups reacted strongly with human SCLC cells by fluorescent-activated cell sorting (FACS). Sera from all patients in the 10 μg dose group also had bactericidal activity against group B meningococci with rabbit complement. Self-limited grade 3 ataxia of unclear etiology was seen in 1 of 18 patients.Vaccination with NP-polySA-KLH resulted in consistent high-titer antibody responses, with the 10 μg dose significantly more immunogenic than the 3 μg dose. This study establishes the lowest optimally immunogenic dose of NP-polysialic acid in this NP-polysialic acid-KLH conjugate vaccine to be at least 10 μg, and it establishes the vaccine's safety. We plan to incorporate NP-polySA into a polyvalent vaccine against SCLC with four glycolipid antigens also widely expressed in SCLC-GD2, GD3, fucosylated GM1, and globo H.

Published

2011

27. Natural and synthetic saponin adjuvant QS-21 for vaccines against cancer

Author

Philip O. Livingston, Jeffrey Gardner, Govind Ragupathi, and David Y. Gin

Subjects

medicine.medical_treatment, Immunology, Saponin, Pharmacology, Cancer Vaccines, Article, Immune system, Adjuvants, Immunologic, Antigen, Neoplasms, Drug Discovery, medicine, Humans, chemistry.chemical_classification, biology, Quillaja saponaria, Quillaja, Glycoside, Saponins, biology.organism_classification, chemistry, Toxicity, biology.protein, Molecular Medicine, Antibody, Adjuvant

Abstract

One of the most widely used and potent immunological adjuvants is a mixture of soluble triterpene glycosides purified from the soap bark tree (Quillaja saponaria). Despite challenges in production, quality control, stability and toxicity, the QS-21 fraction from this extract has exhibited exceptional adjuvant properties for a range of antigens. It possesses an ability to augment clinically significant antibody and T-cell responses to vaccine antigens against a variety of infectious diseases, degenerative disorders and cancers. The recent synthesis of active molecules of QS-21 has provided a robust method to produce this leading vaccine adjuvant in high purity as well as to produce novel synthetic QS-21 congeners designed to induce increased immune responsiveness and decreased toxicity.

Published

2011

28. The Known Immunologically Active Components ofAstragalusAccount for Only a Small Proportion of the Immunological Adjuvant Activity When Combined with Conjugate Vaccines

Author

Clara Bik-San Lau, Barrie R. Cassileth, Ping-Chung Leung, Govind Ragupathi, K. Simon Yeung, Feng Hong, Constantine George, Wei-Lie Xiao, Edward J. Kennelly, and Philip O. Livingston

Subjects

Antibodies, Neoplasm, medicine.medical_treatment, Saponin, Pharmaceutical Science, Enzyme-Linked Immunosorbent Assay, Cancer Vaccines, Article, Analytical Chemistry, Mice, chemistry.chemical_compound, Astragaloside, Adjuvants, Immunologic, Antigen, Conjugate vaccine, Drug Discovery, medicine, Animals, Flavonoids, Pharmacology, chemistry.chemical_classification, Mice, Inbred BALB C, Vaccines, Conjugate, biology, Plant Extracts, Organic Chemistry, Astragalus propinquus, Saponins, biology.organism_classification, Triterpenes, Mice, Inbred C57BL, Astragalus, Complementary and alternative medicine, chemistry, Antibody Formation, Immunology, Toxicity, Molecular Medicine, Female, Cancer vaccine, Adjuvant

Abstract

The 95 % ethanol extract of Astragalus has been demonstrated to have potent activity as an immunological adjuvant when administered with vaccines of various types. We endeavor here to identify the components of this extract that are responsible for this adjuvant activity. Mice were immunized with KLH conjugated to cancer carbohydrate antigens globo H and GD3 and cancer peptide antigen MUC1 combined with different Astragalus fractions or with commercially available Astragalus saponins and flavonoids. The antibody responses against cancer antigens and KLH were quantitated in ELISA assays, and toxicity was calculated by weight loss. Astragalosides II and IV were the most active components, but the toxicity of these two differed dramatically. Astragaloside II was the most toxic Astragalus component with 5-10 % weight loss at a dose of 500 µg while astragaloside IV showed no weight loss at all at this dose, suggesting that astragaloside IV might be utilized as an immunological adjuvant in future studies. Several flavonoids also had significant adjuvant activity. However, when the activities of these known immunologically active components of Astragalus (and of endotoxin) are calculated based on the extent of their presence in the 95 % ethanol extract, they provide only a small proportion of the immunological activity. This raises the possibility that additional uniquely active components of Astragalus may contribute to adjuvant activity, or that the adjuvant activity of Astragalus is greater than the activity of the sum of its parts.

Published

2010

29. Preclinical evaluation of the synthetic adjuvant SQS-21 and its constituent isomeric saponins

Author

Michelle M. Adams, Jianfeng Hang, Philip O. Livingston, David Y. Gin, Govind Ragupathi, Payal Damani, Kai Deng, and Constantine George

Subjects

medicine.medical_treatment, Drug Evaluation, Preclinical, Saponin, Cancer Vaccines, Article, Mice, chemistry.chemical_compound, Adjuvants, Immunologic, Antigen, In vivo, Gangliosides, medicine, Animals, Apiose, Melanoma, chemistry.chemical_classification, Molecular Structure, General Veterinary, General Immunology and Microbiology, biology, Quillaja saponaria, Public Health, Environmental and Occupational Health, Antibody titer, Saponins, biology.organism_classification, Virology, Mice, Inbred C57BL, Infectious Diseases, chemistry, Biochemistry, Antibody Formation, Hemocyanins, biology.protein, Molecular Medicine, Female, Adjuvant, Keyhole limpet hemocyanin

Abstract

The saponin fraction QS-21 from Quillaja saponaria has been demonstrated to be a potent immunological adjuvant when mixed with keyhole limpet hemocyanin conjugate vaccines, as well as with other classes of subunit antigen vaccines. QS-21 adjuvant is composed of two isomers that include the apiose and xylose forms in a ratio of 65:35, respectively. The chemical syntheses of these two isomers in pure form have recently been disclosed. Herein we describe detailed in vivo immunological evaluations of these synthetic QS-21 isomeric constituents, employing the GD3-KLH melanoma antigen. With this vaccine construct, high antibody titers against GD3 ganglioside and KLH were elicited when GD3-KLH was co-administered with adjuvant, either as the individual separate synthetic QS-21 isomers (SQS-21-Api or SQS-21-Xyl), or as its reconstituted 65:35 isomeric mixture (SQS-21). These antibody titer levels were comparable to that elicited by vaccinations employing naturally derived QS-21 (PQS-21). Moreover, toxicities of the synthetic saponin adjuvants were also found to be comparable to that of naturally derived PQS-21. These findings demonstrate unequivocally that the adjuvant activity of QS-21 resides in these two principal isomeric forms, and not in trace contaminants within the natural extracts. This lays the foundation for future exploration of structure-function correlations to enable the discovery of novel saponins with increased potency, enhanced stability, and attenuated toxicity.

Published

2010

30. Cancer Biomarkers Defined by Autoantibody Signatures to Aberrant O-Glycopeptide Epitopes

Author

Ola Blixt, Hans H. Wandall, Joy Burchell, Michael A. Hollingsworth, Joyce Taylor-Papadimitriou, Johannes W. Pedersen, Phil Livingston, Eric P. Bennett, Mads Agervig Tarp, Ulla Mandel, Henrik Clausen, and Govind Ragupathi

Subjects

0303 health sciences, Cancer Research, biology, Autoantibody, Cancer, medicine.disease, Epitope, 3. Good health, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Oncology, Antigen, 030220 oncology & carcinogenesis, Immunology, medicine, biology.protein, Cancer biomarkers, Antibody, MUC1, 030304 developmental biology

Abstract

Autoantibodies to cancer antigens hold promise as biomarkers for early detection of cancer. Proteins that are aberrantly processed in cancer cells are likely to present autoantibody targets. The extracellular mucin MUC1 is overexpressed and aberrantly glycosylated in many cancers; thus, we evaluated whether autoantibodies generated to aberrant O-glycoforms of MUC1 might serve as sensitive diagnostic biomarkers for cancer. Using an antibody-based glycoprofiling ELISA assay, we documented that aberrant truncated glycoforms were not detected in sera of cancer patients. An O-glycopeptide microarray was developed that detected IgG antibodies to aberrant O-glycopeptide epitopes in patients vaccinated with a keyhole limpet hemocyanin–conjugated truncated MUC1 peptide. We detected cancer-associated IgG autoantibodies in sera from breast, ovarian, and prostate cancer patients against different aberrent O-glycopeptide epitopes derived from MUC1. These autoantibodies represent a previously unaddressed source of sensitive biomarkers for early detection of cancer. The methods we have developed for chemoenzymatic synthesis of O-glycopeptides on microarrays may allow for broader mining of the entire cancer O-glycopeptidome. Cancer Res; 70(4); 1306–13

Published

2010

31. Design and Synthesis of Potent Quillaja Saponin Vaccine Adjuvants

Author

Payal Damani, Philip O. Livingston, Feng Hong, Michelle M. Adams, Annie Won, Nicholas R. Perl, David Y. Gin, and Govind Ragupathi

Subjects

medicine.medical_treatment, Saponin, Immunopotentiator, Pharmacology, Biochemistry, Article, Catalysis, Mice, chemistry.chemical_compound, Colloid and Surface Chemistry, Immune system, Adjuvants, Immunologic, Antigen, Conjugate vaccine, Cell Line, Tumor, medicine, Animals, chemistry.chemical_classification, Vaccines, Natural product, biology, Quillaja, General Chemistry, Saponins, biology.organism_classification, Mice, Inbred C57BL, chemistry, Drug Design, Female, Adjuvant

Abstract

The success of antitumor and antiviral vaccines often requires the use of an adjuvant, a substance that significantly enhances the immune response to a co-administered antigen. Only a handful of adjuvants have both sufficient potency and acceptable toxicity for clinical investigation. One promising adjuvant is QS-21, a saponin natural product that is the immunopotentiator of choice in many cancer and infectious disease vaccine clinical trials. However, the therapeutic promise of QS-21 adjuvant is curtailed by several factors, including its scarcity, difficulty in purification to homogeneity, dose-limiting toxicity, and chemical instability. Here we report the design, synthesis, and evaluation of chemically stable synthetic saponins. These novel, amide-modified, non-natural substances exhibit immunopotentiating effects in vivo that rival or exceed that of QS-21 in evaluations with the GD3-KLH melanoma conjugate vaccine. The highly convergent synthetic preparation of these novel saponins establishes new avenues for discovering improved molecular adjuvants for specifically tailored vaccine therapies.

Published

2010

32. From Synthesis to Biologics: Preclinical Data on a Chemistry Derived Anticancer Vaccine

Author

Samuel J. Danishefsky, Ouathek Ouerfelli, Payal Damani, Jianglong Zhu, Qian Wan, Guangbin Yang, Maria Spassova, Govind Ragupathi, Dongjoo Lee, and Philip O. Livingston

Subjects

Male, Carbohydrate chemistry, medicine.medical_treatment, Breast Neoplasms, Cancer Vaccines, Biochemistry, Article, Catalysis, Epitope, Maleimides, Mice, Colloid and Surface Chemistry, Antigen, Cell Line, Tumor, medicine, Animals, Humans, Antigens, Tumor-Associated, Carbohydrate, Vaccines, Synthetic, biology, Chemistry, Prostatic Neoplasms, General Chemistry, Molecular biology, Glycopeptide, Mice, Inbred C57BL, Cell culture, Antibody Formation, Hemocyanins, Cancer research, biology.protein, Female, Binding Sites, Antibody, Antibody, Adjuvant, Conjugate

Abstract

A fully synthetic anticancer vaccine 2 has been prepared via bio-conjugation of unimolecular pentavalent construct 1 – containing five prostate and breast cancer associated carbohydrate antigens, Globo-H, GM2, STn, TF and Tn – to maleimide-modified carrier protein KLH. An improved conjugation protocol has been developed, which allowed us to obtain a higher epitope ratio of the unimolecular pentavalent glycopeptide antigen to the carrier protein (505/1 versus 228/1 for the previous version). KLH conjugate 2 has been subsequently submitted to preclinical immunogenic evaluation in mice in the presence of QS-21 as an adjuvant. Through standard ELISA assay, this vaccine candidate showed high promise in inducing IgG and IgM antibodies against each of the five individual carbohydrate antigens. In addition, FACS analysis indicated that these antibodies were able to react with MCF-7 breast cancer cell lines expressing these five carbohydrate antigens.

Published

2009

33. Evaluation of widely consumed botanicals as immunological adjuvants

Author

Govind Ragupathi, Andrew J. Vickers, Clara Bik-San Lau, Barrie R. Cassileth, Chandra Hood, Gary Deng, K. Simon Yeung, Ping-Chung Leung, Philip O. Livingston, Mavis Y.H. Lee, and Nai-Kong V. Cheung

Subjects

Immunogen, Antibodies, Neoplasm, Injections, Subcutaneous, medicine.medical_treatment, Immunization, Secondary, Saponin, Enzyme-Linked Immunosorbent Assay, chemical and pharmacologic phenomena, Cancer Vaccines, Article, Microbiology, Mice, Immune system, Adjuvants, Immunologic, Antigen, Gangliosides, medicine, Animals, Potency, chemistry.chemical_classification, Plants, Medicinal, Vaccines, Conjugate, General Veterinary, General Immunology and Microbiology, biology, Traditional medicine, Plant Extracts, Fungi, Public Health, Environmental and Occupational Health, Mice, Inbred C57BL, Infectious Diseases, chemistry, biology.protein, Molecular Medicine, Female, Antibody, Adjuvant, Keyhole limpet hemocyanin

Abstract

Background Many widely used botanical medicines are claimed to be immune enhancers. Clear evidence of augmentation of immune responses in vivo is lacking in most cases. To select botanicals for further study based on immune enhancing activity, we study them here mixed with antigen and injected subcutaneously (s.c.). Globo H and GD3 are cell surface carbohydrates expressed on glycolipids or glycoproteins on the cell surface of many cancers. When conjugated to keyhole limpet hemocyanin (KLH), mixed with an immunological adjuvant and administered s.c. the magnitude of the antibody responses against globo H, GD3 and KLH depend largely on the potency of the adjuvant. We describe here the results obtained using this s.c. immunization model with seven botanicals purported to have immune stimulant effects. Methods Groups of 5–10 mice were immunized with globo H–KLH or GD3–KLH mixed with botanical, saline or positive control immunological adjuvant, s.c. three times at 1 week intervals. Antibody responses were measured 1 and 2 weeks after the 3rd immunization. The following seven botanicals and fractions were tested: (1) H-48 (Honso USA Co.), (2) Coriolus versicolor raw water extract, purified polysaccharide-K (PSK) or purified polysaccharide-peptide (PSP) (Institute of Chinese Medicine (ICM)), (3) Maitake extract (Yukiguni Maitake Co. Ltd. and Tradeworks Group), (4) Echinacea lipophilic, neutral and acidic extracts (Gaia Herbs), (5) Astragalus water, 50% or 95% ethanol extracts (ICM), (6) Turmeric supercritical (SC) or hydro-ethanolic (HE) extracts (New Chapter) or 60% ethanol extract (ICM) and (7) yeast β-glucan (Biotec Pharmacon). Purified saponin extract QS-21 (Antigenics) and semisynthetic saponin GPI-0100 (Advanced BioTherapies) were used as positive control adjuvants. Sera were analyzed by ELISA against synthetic globo H ceramide or GD3 and KLH. Results Consistent significant adjuvant activity was observed after s.c. vaccination with the Coriolus extracts (especially PSK), a 95% ethanol extract of Astragalus and yeast β-glucan, and (to a lesser extent) Maitake. Antibodies against KLH in all cases and against globo H in most cases were induced by these botanicals. Little or no adjuvant activity was demonstrated with H-48 or Echinacea extracts or the Astragalus water extract. Experiments with GD3–KLH as immunogen confirmed the adjuvant activity of the Coriolus, yeast β-glucan and Astragalus extracts. While extraction with ethanol concentrated the active ingredients in Astragalus, it had no impact on Coriolus where the 90% ethanol precipitate and solute were equally active. Conclusions Some, but not all, botanicals purported to be immune stimulants had adjuvant activity in our model. PSK and Astragalus were surprisingly active and are being further fractionated to identify the most active adjuvant components.

Published

2008

34. Inflammation-associated lysophospholipids as ligands for CD1d-restricted T cells in human cancer

Author

Haiteng Deng, Amitabha Mazumder, Radek Spisek, Govind Ragupathi, Sundar Jagannath, Phillip Matthews, David H. Vesole, David H. Chang, Joseph Krasovsky, and Madhav V. Dhodapkar

Subjects

Receptors, Antigen, T-Cell, alpha-beta, T-Lymphocytes, T cell, Immunology, T-Cell Antigen Receptor Specificity, Ligands, Lymphocyte Activation, Biochemistry, Antigens, CD1, Interleukin 21, medicine, Humans, Cytotoxic T cell, IL-2 receptor, Immunobiology, Inflammation, Interleukin-13, CD40, biology, ZAP70, Lysophosphatidylcholines, Cell Biology, Hematology, Natural killer T cell, Killer Cells, Natural, medicine.anatomical_structure, biology.protein, Interleukin 12, lipids (amino acids, peptides, and proteins), Lysophospholipids, Multiple Myeloma

Abstract

CD1d-restricted T cells have been implicated in the pathogenesis of several chronic inflammatory states. However, the nature of the specific ligands recognized by these cells in vivo in patients with inflammatory or malignant diseases remains unknown. We took a biochemical approach to directly isolate and characterize the nature of CD1d-binding ligands from the plasma of myeloma patients. Characterization of these ligands revealed several lysophosphatidylcholine (LPC) species. Human LPC-CD1d dimer binding cells are T-cell receptorαβ+ T cells but predominantly Vα24−Vβ11−. Cytokine secretion by LPC-specific T cells is skewed toward IL-13 secretion, and the frequencies of these cells are increased in myeloma patients relative to healthy donors. These data identify a distinct population of human CD1d-restricted T cells specific for inflammation-associated lysolipids and suggest a novel mechanism for inflammation mediated immune regulation in human cancer.

Published

2008

35. Synthesis of QS-21-Xylose: Establishment of the Immunopotentiating Activity of Synthetic QS-21 Adjuvant with a Melanoma Vaccine

Author

Kai Deng, Michelle M. Adams, Payal Damani, Philip O. Livingston, Govind Ragupathi, and David Y. Gin

Subjects

General Medicine

Published

2008

36. Quillaja saponin variants with central glycosidic linkage modifications exhibit distinct conformations and adjuvant activities

Author

Jesús Jiménez-Barbero, Derek S. Tan, David Y. Gin, Francisco Corzana, William E. Walkowicz, Constantine George, Govind Ragupathi, and Alberto Fernández-Tejada

Subjects

0301 basic medicine, chemistry.chemical_classification, Natural product, Stereochemistry, medicine.medical_treatment, Saponin, Glycosidic bond, General Chemistry, Biology, 010402 general chemistry, biology.organism_classification, 01 natural sciences, Immunoadjuvant, QS21, 0104 chemical sciences, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Biochemistry, chemistry, Quillaja, medicine, Glycosyl, Adjuvant

Abstract

Immunological adjuvants such as the saponin natural product QS-21 help stimulate the immune response to co-administered antigens and have become increasingly important in the development of prophylactic and therapeutic vaccines. However, clinical use of QS-21 is encumbered by chemical instability, dose-limiting toxicity, and low-yielding purification from the natural source. Previous studies of structure-activity relationships in the four structural domains of QS-21 have led to simplified, chemically stable variants that retain potent adjuvant activity and low toxicity in mouse vaccination models. However, modification of the central glycosyl ester linkage has not yet been explored. Herein, we describe the design, synthesis, immunologic evaluation, and molecular dynamics analysis of a series of novel QS-21 variants with different linker lengths, stereochemistry, and flexibility to investigate the role of this linkage in saponin adjuvant activity and conformation. Despite relatively conservative structural modifications, these variants exhibit striking differences in in vivo adjuvant activity that correlate with specific conformational preferences. These results highlight the junction of the triterpene and linear oligosaccharide domains as playing a critical role in the immunoadjuvant activity of the Quillaja saponins and also suggest a mechanism of action involving interaction with a discrete macromolecular target, in contrast to the non-specific mechanisms of emulsion-based adjuvants. © The Royal Society of Chemistry 2016.

Published

2016

37. A polyvalent vaccine for high-risk prostate patients: 'are more antigens better?'

Author

Celina Fernandez, Matthew P. Jefferson, Howard I. Scher, W. Kevin Kelly, David B. Solit, Meghan Diani, Susan F. Slovin, Michael J. Morris, Philip O. Livingston, Andrew Wilton, Henrik Clausen, and Govind Ragupathi

Subjects

Adult, Male, Cancer Research, Time Factors, medicine.medical_treatment, Immunology, Disease-Free Survival, Antigen, Antigens, Neoplasm, medicine, Humans, Immunology and Allergy, Aged, Aged, 80 and over, biology, Polyvalent Vaccine, Immunogenicity, Antibody titer, Prostatic Neoplasms, Middle Aged, Prostate-Specific Antigen, Virology, Vaccination, Immunoglobulin M, Oncology, Immunoglobulin G, Hemocyanins, biology.protein, Immunotherapy, Antibody, Adjuvant, Keyhole limpet hemocyanin

Abstract

We have shown the immunogenicity and safety of synthetic carbohydrate vaccines when conjugated to the carrier keyhole limpet hemocyanin (KLH) and given with the adjuvant, QS-21, in patients with biochemically relapsed prostate cancer. To determine whether immune response could be further enhanced with stimulation by multiple antigens, a hexavalent vaccine was prepared using previously determined doses and administered in a Phase II setting to 30 high-risk patients. The hexavalent vaccine included GM2, Globo H, Lewis(y), glycosylated MUC-1-32mer and Tn and TF in a clustered formation, conjugated to KLH and mixed with QS-21. Eight vaccinations were administered over 13 months. All 30 patients had significant elevations in antibody titers to at least two of the six antigens; 22 patients had increased reactivity with FACS. These serologic responses were lower than that seen previously in patients treated with the respective monovalent vaccines. The reciprocal median combined IgM and IgG antibody titers with ELISA against MUC1, Tn, TF, globo H and GM2 for these 30 patients were 640, 80, 120, 40 and 0, compared to 1280, 640, 1280, 320 and 160 seen in patients receiving individual monovalent vaccines. This hexavalent vaccine of synthetic "self" antigens broke immunologic tolerance against two or more antigens in all 30 vaccinated patients, was safe, but antibody titers against several of the antigens were lower than those seen in individual monovalent trials. No impact on PSA slope was detected. We address the relevance of the multivalent approach for prostate cancer treatment.

Published

2007

38. Immunization of High-Risk Breast Cancer Patients with Clustered sTn-KLH Conjugate plus the Immunologic Adjuvant QS-21

Author

R. Rao Koganty, Teresa Gilewski, Maura N. Dickler, Clifford A. Hudis, Alan N. Houghton, K. Panageas, Sonal Bhuta, Larry Norton, Govind Ragupathi, Philip O. Livingston, Jeannette Chin-Eng, and Shemeeakah Powell

Subjects

Adult, Male, Risk, Cancer Research, medicine.medical_treatment, Breast Neoplasms, Cancer Vaccines, Antibodies, Breast cancer, Adjuvants, Immunologic, Antigen, medicine, Humans, biology, business.industry, Antibody titer, Ovine Submaxillary Mucin, Middle Aged, Saponins, medicine.disease, nervous system diseases, surgical procedures, operative, Immunoglobulin M, nervous system, Oncology, Immunization, Immunologic adjuvant, Immunology, biology.protein, Female, Antibody, business, therapeutics, Adjuvant

Abstract

Purpose: To determine the clinical toxicities and antibody response against sTn and tumor cells expressing sTn following immunization of high-risk breast cancer patients with clustered sTn-KLH [sTn(c)-KLH] conjugate plus QS-21.Experimental Design: Twenty-seven patients with no evidence of disease and with a history of either stage IV no evidence of disease, rising tumor markers, stage II (≥4 positive axillary nodes), or stage III disease received a total of five injections each during weeks 1, 2, 3, 7, and 19. Immunizations consisted of sTn(c)-KLH conjugate containing 30, 10, 3, or 1 μg sTn(c) plus 100 μg QS-21. Induction of IgM and IgG antibodies against synthetic sTn(c) and natural sTn on ovine submaxillary mucin were measured before and after therapy. Fluorescence-activated cell sorting analyses assessed reactivity of antibodies to LSC and MCF-7 tumor cells.Results: The most common toxicities were transient local skin reactions at the injection site and mild flu-like symptoms. All patients developed significant IgM and IgG antibody titers against sTn(c). Antibody titers against ovine submaxillary mucin were usually of lower titers. IgM reactivity with LSC tumor cells was observed in 21 patients and with MCF-7 cells in 13 patients. There was minimal IgG reactivity with LSC cells.Conclusion: Immunization with sTn(c)-KLH conjugate plus QS-21 is well tolerated and immunogenic in high-risk breast cancer patients. Future trials will incorporate sTn(c) as a component of a multiple antigen vaccine.

Published

2007

39. Molecular basis of antibody binding to mucin glycopeptides in lung cancer

Author

Ahmad Trad, Yanyan Lou, Zhi Guo, Fenge Li, Dapeng Zhou, Ting Gong, Jin Qu, Chunlei Zhang, Yunsen Li, Hongtao Yu, Wei Huang, Govind Ragupathi, Patrick Hwu, Bin Zhang, and Cory L. Brooks

Subjects

0301 basic medicine, Cancer Research, Glycosylation, Lung Neoplasms, cancer biomarkers, B-cell receptor, Tn antigen, Complementarity determining region, Biology, Epitope, 03 medical and health sciences, Epitopes, mucin, immunomonitoring, Cell Line, Tumor, immunodiagnosis, Humans, Antigens, Tumor-Associated, Carbohydrate, RNA, Messenger, sialyl-Tn antigen, MUC1, B-Lymphocytes, glycopeptidome, Mucin, Mucin-1, Glycopeptides, Antibodies, Monoclonal, Articles, Molecular biology, Glycopeptide, lung cancer, 030104 developmental biology, Oncology, monoclonal antibody, Immunoglobulin G, biology.protein, glycoproteome, immunotherapy, Antibody, cancer vaccine, Protein Binding

Abstract

Glycopeptides bearing Tn epitopes are emerging targets for cancer diagnosis and immunotherapy. In this study, we analyzed membrane proteins containing O-glycosylated tandem repeat (TR) sequences in lung cancer patients of different types and stages, using gene microarray data in public domain. The expression of Tn and glycopeptide epitopes on the surface of lung cancer cell lines were studied by monoclonal IgG antibodies 14A, 16A, and B72.3. The binding of mAbs to synthetic glycopeptides were studied by surface plasmon resonance. Nine mucin mRNAs were found to be expressed in lung cancer patients but at similar level to healthy individuals. At protein level, a glycopeptide epitope on cancer cell surface is preferably recognized by mAb 16A, as compared to peptide-alone (14A) or sugar-alone epitopes (B72.3). 14A and 16A favor clustered TR containing more than three TR sequences, with 10-fold lower Kd than two consecutive TR. B72.3 preferrably recognized clustered sialyl-Tn displayed on MUC1 but not other O-glycoproteins, with 100-fold stronger binding when MUC1 is transfected as a sugar carrier, while the total sugar epitopes remain unchanged. These findings indicate that clusters of both TR backbones and sugars are essential for mAb binding to mucin glycopeptides. Three rules of antibody binding to mucin glycopeptides at molecular level are presented here: first, the peptide backbone of a glycopeptide is preferentially recognized by B cells through mutations in complementarity determining regions (CDRs) of B cell receptor, and the sugar-binding specificity is acquired through mutations in frame work of heavy chain; secondly, consecutive tandem repeats (TR) of peptides and glycopeptides are preferentially recognized by B cells, which favor clustered TR containing more than three TR sequences; thirdly, certain sugar-specific B cells recognize and accommodate clustered Tn and sialyl-Tn displayed on the surface of a mucin but not other membrane proteins.

Published

2015

40. Cancer Vaccines Targeting Carbohydrate Antigens

Author

Govind Ragupathi and Philip O. Livingston

Subjects

Antibodies, Neoplasm, medicine.medical_treatment, Immunogenicity, Immunology, Antibody titer, Antibodies, Monoclonal, Cancer, Biology, medicine.disease, Cancer Vaccines, Circulating tumor cell, Immune system, Immunoglobulin M, Antigen, Immunoglobulin G, Hemocyanins, medicine, biology.protein, Humans, Antigens, Tumor-Associated, Carbohydrate, General Pharmacology, Toxicology and Pharmaceutics, Antibody, Adjuvant

Abstract

Cancer carbohydrate antigens have been surprisingly potent targets for immune recognition and attack by antibodies, both because of their abundance at the cell surface and their immunogenicity. Antibodies are ideally suited for eradicating pathogens from the bloodstream and from early tissue invasion. Passively administered and vaccine induced antibodies have accomplished this, eliminating circulating tumor cells and systemic or intraperitoneal micrometastases in a variety of preclinical models. A series of carbohydrate cancer cell-surface differentiation antigens have now been identified and synthesized. Antibodies against each can be induced in the majority of vaccinated patients using KLH conjugate vaccines with a potent saponin immunological adjuvant. Polyvalent vaccines will probably be required due to tumor cell heterogeneity, heterogeneity of the human immune response and the correlation between overall antibody titer against tumor cells and antibody effector mechanisms. Trials testing the clinical impact of these polyvalent vaccines in the adjuvant setting are planned for the near future.

Published

2006

41. Preparation and Evaluation of Unimolecular Pentavalent and Hexavalent Antigenic Constructs Targeting Prostate and Breast Cancer: A Synthetic Route to Anticancer Vaccine Candidates

Author

Samuel J. Danishefsky, Atsushi Endo, Maria Spassova, Ouathek Ouerfelli, Qian Wan, Govind Ragupathi, Rebecca M. Wilson, Stacy J. Keding, Philip O. Livingston, Fusataka Koide, Jennifer D. Allen, and Young Shin Cho

Subjects

chemistry.chemical_classification, Chemistry, Immunogenicity, General Chemistry, Oligosaccharide, Biochemistry, Catalysis, Glycopeptide, Sialic acid, chemistry.chemical_compound, Residue (chemistry), Colloid and Surface Chemistry, Aminosugar, Antigen, Peptide synthesis

Abstract

Several novel, fully synthetic, carbohydrate-based antitumor vaccines have been assembled. Each construct consists of multiple cancer-related antigens displayed on a single polypeptide backbone. Recent advances in synthetic methodology have allowed for the incorporation of a complex oligosaccharide terminating in a sialic acid residue (i.e., GM2) as one of the carbohydrate antigens. Details of the vaccine synthesis as well as the results of preliminary immunological investigations are described herein.

Published

2006

42. A bivalent conjugate vaccine in the treatment of biochemically relapsed prostate cancer: a study of glycosylated MUC-2-KLH and Globo H-KLH conjugate vaccines given with the new semi-synthetic saponin immunological adjuvant GPI-0100 OR QS-21

Author

Celso A. Reis, Matthew P. Jefferson, Philip O. Livingston, Andrew Wilton, Govind Ragupathi, Maria Spassova, Susan F. Slovin, Shemeeakah Powell, Samuel J. Danishefsky, Henrick Clausen, Howard I. Scher, Meghan Diani, and Celina Fernandez

Subjects

Male, medicine.medical_treatment, Dose-Response Relationship, Immunologic, Enzyme-Linked Immunosorbent Assay, Cancer Vaccines, Adjuvants, Immunologic, Recurrence, Conjugate vaccine, Humans, Medicine, Immunization Schedule, Aged, Vaccines, Conjugate, General Veterinary, General Immunology and Microbiology, biology, business.industry, Public Health, Environmental and Occupational Health, Antibody titer, Prostatic Neoplasms, Immunotherapy, Middle Aged, Prostate-Specific Antigen, Saponins, Flow Cytometry, QS21, carbohydrates (lipids), Vaccination, Infectious Diseases, Immunology, Toxicity, biology.protein, Molecular Medicine, business, Adjuvant, Keyhole limpet hemocyanin

Abstract

GPI-0100 is a semi-synthetic saponin with modifications designed to augment stability and diminish toxicity. Two batches of GPI-0100 (the second with higher purity) were tested with doses ranging between 100 and 5000 microg in groups of five treated prostate cancer patients who had no evidence of disease except for rising PSA levels. GPI-0100 was mixed with a bivalent vaccine containing the glycolipid Globo H and the glycosylated mucin MUC2 conjugated to keyhole limpet hemocyanin (KLH). All doses were well tolerated and antibody titers against Globo H and MUC-2 escalated with the increasing dose levels. At the 5000 microg dose level in this patient population, toxicity remained minimal with only occasional grade II local toxicity at vaccination sites and occasional sporadic grade I elevations in ALT. Compared with a subsequent trial with the same bivalent vaccine plus QS-21 at the maximal tolerated dose of 100 microg, the 5000 microg dose of GPI-0100 produced comparable antibody titers.

Published

2005

43. Comparison of antigen constructs and carrier molecules for augmenting the immunogenicity of the monosaccharide epithelial cancer antigen Tn

Author

Jeff Gildersleeve, Samuel J. Danishefsky, Govind Ragupathi, Ella Kagan, Daniel Kahne, San San Yi, Celso A. Reis, Philip O. Livingston, and Henrik Clausen

Subjects

Cancer Research, Glycosylation, Antibodies, Neoplasm, medicine.drug_class, Immunology, Tn antigen, Enzyme-Linked Immunosorbent Assay, Monoclonal antibody, Cancer Vaccines, Mice, chemistry.chemical_compound, Antigen, Cell Line, Tumor, medicine, Animals, Humans, Immunology and Allergy, Antigens, Tumor-Associated, Carbohydrate, MUC1, Vaccines, Conjugate, biology, Immunogenicity, Carcinoma, Mucin-1, Flow Cytometry, Microspheres, biological factors, Mice, Inbred C57BL, Oncology, chemistry, Biochemistry, Hemocyanins, biology.protein, Female, Antibody, Keyhole limpet hemocyanin

Abstract

We have demonstrated previously that the optimal method for inducing an antibody response against defined cancer antigens is covalent conjugation of the antigen to keyhole limpet hemocyanin (KLH) and use of the potent saponin adjuvant QS-21. Single molecules of glycolipids (tetrasaccharides, pentasaccharides, or hexasaccharides) and MUC1 peptides (containing between one and five MUC1 tandem repeats) conjugated to KLH have proven sufficient for antibody recognition and vaccine construction. However, cancer specificity of monoclonal antibodies against the monosaccharide Tn and disaccharide sTn comes largely from recognition of clusters (c) of these molecules on the cell surface. Tn consists of a monosaccharide (GalNAc) O-linked to serine or threonine on epithelial cancer mucins which are uniquely rich in serines and threonines. We test here several Tn constructs: Tn monosaccharide, Tn(c) prepared on a triple threonine backbone, and Tn prepared on a partially or fully glycosylated MUC1 backbone. We determine that Tn(c) is more effective than Tn, and conjugation to KLH is more effective than conjugation to BSA or polystyrene beads for inducing ELISA reactivity against Tn, and FACS reactivity against Tn-positive tumor cells. Surprisingly, MUC1 glycosylated with Tn at three or five sites per 20 amino acid MUC1 tandem repeat and conjugated to KLH, induced the strongest antibody response against Tn and tumor cells expressing Tn, and had the additional advantage of inducing antibodies against MUC1.

Published

2004

44. A preclinical study comparing approaches for augmenting the immunogenicity of a heptavalent KLH-conjugate vaccine against epithelial cancers

Author

Govind Ragupathi, Natarajan Sathyan, Fusataka Koide, Maria Spassova, Polly D. Gregor, Celso A. Reis, Philip O. Livingston, Henrik Clausen, Samuel J. Danishefsky, Ella Kagan, and William Bornmann

Subjects

Cancer Research, Antibodies, Neoplasm, medicine.drug_class, T-Lymphocytes, medicine.medical_treatment, Synthetic antigen, Immunology, Drug Evaluation, Preclinical, Biology, Monoclonal antibody, Cancer Vaccines, Mice, Lewis Blood Group Antigens, Antigen, Antigens, Neoplasm, Conjugate vaccine, Gangliosides, medicine, Animals, Immunology and Allergy, Neoplasms, Glandular and Epithelial, Mice, Inbred BALB C, Vaccines, Conjugate, Immunogenicity, Mucin-1, Vaccination, Antibody titer, Saponins, Virology, Peptide Fragments, Mice, Inbred C57BL, Immunoglobulin M, Oncology, Immunoglobulin G, Antibody Formation, Hemocyanins, biology.protein, Female, Immunization, Adjuvant, Keyhole limpet hemocyanin

Abstract

Previously using a series of monovalent vaccines, we demonstrated that the optimal method for inducing an antibody response against cancer cell-surface antigens is covalent conjugation of the antigens to keyhole limpet hemocyanin (KLH) and the use of a saponin adjuvant. We have prepared a heptavalent-KLH conjugate vaccine containing the seven epithelial cancer antigens GM2, Globo H, Lewisy, TF(c), Tn(c), STn(c), and glycosylated MUC1. In preparation for testing this vaccine in the clinic, we tested the impact on antibody induction of administering the individual conjugates plus adjuvant compared with a mixture of the seven conjugates plus adjuvant, and of several variables thought to augment immunogenicity. These include approaches for decreasing suppressor cell activity or increasing helper T-lymphocyte activity (low dose cyclophosphamide or anti-CTLA-4 MAb), different saponin adjuvants at various doses (QS-21 and GPI-0100), and different methods of formulation (lyophilization and use of polysorbate 80). We find that: (1) Immunization with the heptavalent-KLH conjugate plus GPI-0100 vaccine induces antibodies against the seven antigens of comparable titer to those induced by the individual-KLH conjugate vaccines, high titers of antibodies against Tn (median ELISA titer IgM/IgG 320/10,240), STn (640/5,120), TF (320/10,240), MUC1 (80/20,480), and globo H (640/40); while lower titers of antibodies against Lewisy (160/0) and only occasional antibodies against GM2 are induced. (2) These antibodies reacted with the purified synthetic antigens by ELISA, and with naturally expressed antigens on the cancer cell surface by FACS. (3) None of the approaches for further altering the suppressor cell/helper T-cell balance nor changes to the standard formulation by lyophilization or use of polysorbate 80 had any impact on antibody titers. (4) An optimal dose of saponin adjuvant, QS-21 (50 μg) or GPI-0100 (1000 μg), is required for optimal antibody titers. This heptavalent vaccine is sufficiently optimized for testing in the clinic.

Published

2003

45. Correction : Mitochondrial Ceramide-Rich Macrodomains Functionalize Bax upon Irradiation

Author

Richard Kolesnick, John C. Reed, Wen-Chieh Liao, Hyunmi Lee, Andreas Rimner, Erich Gulbins, Govind Ragupathi, Desiree Ehleiter, Tuula Penate-Medina, Jimmy A. Rotolo, Judith Mesicek, Zvi Fuks, Adriana Haimovitz-Friedman, Dayong Zhai, and Xianglei Yin

Subjects

Ceramide, Multidisciplinary, medicine.diagnostic_test, lcsh:R, Medizin, lcsh:Medicine, Biology, Molecular biology, chemistry.chemical_compound, Western blot, chemistry, medicine, lcsh:Q, lcsh:Science

Abstract

The authors would like to correct Fig 5, as errors were introduced in the preparation of this figure for publication. In Fig 5D[b], the image for the Light fraction Bak Western blot and the numbering of the fractions are incorrect. The authors have provided a corrected version of Fig 5 here. Fig 5 Ceramide induces formation of a mitochondrial ceramide-rich macrodomain (MCRM). The authors confirm that these changes do not alter their findings. The authors have provided the original Western blot and additional underlying data as Supporting Information.

Published

2015

46. Design, synthesis, and immunologic evaluation of vaccine adjuvant conjugates based on QS-21 and tucaresol

Author

Jeffrey Gardner, Eric K. Chea, Philip O. Livingston, Alberto Fernández-Tejada, Govind Ragupathi, David Y. Gin, Derek S. Tan, and Constantine George

Subjects

medicine.medical_treatment, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Immunoadjuvant, Benzoates, Immunoglobulin G, Article, Acylation, chemistry.chemical_compound, Mice, Immune system, Antigen, Adjuvants, Immunologic, Drug Discovery, medicine, Animals, Molecular Biology, MUC1, Immunity, Cellular, Natural product, biology, Organic Chemistry, Saponins, Immunity, Humoral, Mice, Inbred C57BL, chemistry, Benzaldehydes, biology.protein, Molecular Medicine, Adjuvant

Abstract

Immunoadjuvants are used to potentiate the activity of modern subunit vaccines that are based on molecular antigens. An emerging approach involves the combination of multiple adjuvants in a single formulation to achieve optimal vaccine efficacy. Herein, to investigate such potential synergies, we synthesized novel adjuvant conjugates based on the saponin natural product QS-21 and the aldehyde tucaresol via chemoselective acylation of an amine at the terminus of the acyl chain domain in QS saponin variants. In a preclinical mouse vaccination model, these QS saponin–tucaresol conjugates induced antibody responses similar to or slightly higher than those generated with related QS saponin variants lacking the tucaresol motif. The conjugates retained potent adjuvant activity, low toxicity, and improved activity–toxicity profiles relative to QS-21 itself and induced IgG subclass profiles similar to those of QS-21, indicative of both Th1 cellular and Th2 humoral immune responses. This study opens the door to installation of other substituents at the terminus of the acyl chain domain to develop additional QS saponin conjugates with desirable immunologic properties.

Published

2014

47. Development of a minimal saponin vaccine adjuvant based on QS-21

Author

Constantine George, Nagavarakishore Pillarsetty, Jason S. Lewis, Eric K. Chea, Philip O. Livingston, Jeffrey Gardner, Alberto Fernández-Tejada, Derek S. Tan, Govind Ragupathi, and David Y. Gin

Subjects

Biodistribution, General Chemical Engineering, medicine.medical_treatment, Saponin, Pharmacology, 010402 general chemistry, 01 natural sciences, Article, 03 medical and health sciences, chemistry.chemical_compound, Antigen, Vaccine adjuvant, Adjuvants, Immunologic, Injection site, medicine, Humans, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Vaccines, Natural product, General Chemistry, Saponins, 3. Good health, 0104 chemical sciences, chemistry, Toxicity, Adjuvant

Abstract

Adjuvants are materials added to vaccines to enhance the immunological response to an antigen. QS-21 is a natural product adjuvant under investigation in numerous vaccine clinical trials, but its use is constrained by scarcity, toxicity, instability and an enigmatic molecular mechanism of action. Herein we describe the development of a minimal QS-21 analogue that decouples adjuvant activity from toxicity and provides a powerful platform for mechanistic investigations. We found that the entire branched trisaccharide domain of QS-21 is dispensable for adjuvant activity and that the C4-aldehyde substituent, previously proposed to bind covalently to an unknown cellular target, is also not required. Biodistribution studies revealed that active adjuvants were retained preferentially at the injection site and the nearest draining lymph nodes compared with the attenuated variants. Overall, these studies have yielded critical insights into saponin structure-function relationships, provided practical synthetic access to non-toxic adjuvants, and established a platform for detailed mechanistic studies.

Published

2013

48. Gangliosides

Author

Phil Livingston and Govind Ragupathi

Subjects

0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis

Published

2013

49. Abstract A73: Antitumor activity of MVT-5873, a monoclonal antibody targeting sialyl Lewisa, alone and in combination with gemcitabine/nab-paclitaxel in a BxPC3 human pancreatic cancer xenograft model

Author

Govind Ragupathi, Christine M. Kearns, Paul W. Maffuid, Wolfgang W. Scholz, Philip O. Livingston, and Xiaohong Wu

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, medicine.drug_class, medicine.medical_treatment, Monoclonal antibody, 03 medical and health sciences, Cmin, chemistry.chemical_compound, Internal medicine, Pancreatic cancer, medicine, Chemotherapy, business.industry, Cancer, Sialyl-Lewis A, medicine.disease, Gemcitabine, 030104 developmental biology, chemistry, Cancer research, Immunohistochemistry, business, medicine.drug

Abstract

Introduction: MVT-5873 (HuMab-5B1) is a fully human monoclonal antibody that specifically targets the sialyl Lewis A (sLea) epitope on CA19-9, a carbohydrate antigen frequently overexpressed in pancreatic and other gastrointestinal malignancies. The antitumor activity of MVT-5873 as a single agent and in combination with gemcitabine (Gem) + nab-paclitaxel (nab-P, Abraxane®), a standard of care combination for pancreatic cancer, was evaluated in SCID mice bearing subcutaneous BxPC3 human pancreatic cancer tumor xenografts, known to express CA19-9. Methods: Treatment was initiated on Day 9 after BxPC3 cell inoculation; mean tumor volume having reached 150 mm3. Groups of mice (n= 5) were given MVT-5873 at dose levels of 5, 15, and 30 mg/kg alone or with Gem 80 mg/kg + nab-P 20 mg/kg intraperitoneally 2x/week for 5 weeks. Control groups received human IgG 30 mg/kg, Gem/nab-P, or saline on the same schedule. Tumor volumes were measured 2x/week through Day 41, trough (Cmin) serum samples for MVT-5873 pharmacokinetic (PK) analysis were obtained Days 13, 16, 23, 30, 37, & 44. Tumor tissue samples for IHC analysis were obtained upon study termination, Day 44. Results: Day 41 tumor volumes were substantially reduced with single-agent MVT-5873 at doses of 5, 15, and 30 mg/kg, with relative mean volumes of 68%, 76%, and 64%, respectively, that of IgG control. Combination of Gem/nab-P with MVT-5873 at 5, 15, or 30 mg/kg further enhanced activity, resulting relative tumor volumes of 39%, 32%, and 31%, respectively, that of IgG control (p Conclusions: MVT-5873 demonstrates antitumor activity as a single agent and enhances the activity of Gem/nab-P chemotherapy in a BxPC3 human pancreatic xenograft model. These findings support the current Phase I clinical investigation of MVT-5873 as a single agent and in combination with Gem/nab-P in patients with advanced pancreatic cancer and other CA19-9 positive malignancies. (NCT02672917) Citation Format: Govind Ragupathi, Xiaohong Wu, Philip Livingston, Wolfgang Scholz, Christine Kearns, Paul Maffuid.{Authors}. Antitumor activity of MVT-5873, a monoclonal antibody targeting sialyl Lewisa, alone and in combination with gemcitabine/nab-paclitaxel in a BxPC3 human pancreatic cancer xenograft model. [abstract]. In: Proceedings of the AACR Special Conference on Pancreatic Cancer: Advances in Science and Clinical Care; 2016 May 12-15; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2016;76(24 Suppl):Abstract nr A73.

Published

2016

50. Abstract 4993: Novel fully human anti-GD2 monoclonal antibodies with potent therapeutic activity against neuroblastoma, sarcoma and melanoma

Author

Ritsuko Sawada, Philip O. Livingston, Govind Ragupathi, Wolfgang W. Scholz, and Xiaohong Wu

Subjects

Antibody-dependent cell-mediated cytotoxicity, Cancer Research, medicine.diagnostic_test, biology, medicine.drug_class, Chemistry, Monoclonal antibody, medicine.disease, Virology, Complement-dependent cytotoxicity, Flow cytometry, Oncology, Antigen, Cell culture, Neuroblastoma, Cancer research, medicine, biology.protein, Antibody

Abstract

Background: Gangliosides such as GD2, GD3 and GM2 are promising targets for antibody-mediated cancer therapy since they are expressed at high levels on the surface of several cancers, including neuroblastomas, sarcomas and melanomas. Anti-GD2 monoclonal antibodies have shown promising clinical outcomes in neuroblastoma and a chimeric anti-GD2 antibody (Unituxin™) was recently approved by FDA. However, murine-derived antibodies discovered so far show adverse effects that limit their clinical utility. Fully human antibodies derived from immunized patients might be able to overcome these limitations, since epitope specificity has evolved in the human tissue environment. Here we describe the characterization and functional evaluation of two potential development candidates. Methods: PBMCs from patients immunized with GD2 lactone-keyhole limpet hemocyanin (GD2L-KLH) conjugate vaccine were utilized to isolate fully human monoclonal antibodies (humAbs). HumAbs were selected for 1) specificity against GD2 initially by ELISA and cell surface binding by flow cytometry 2) by glycan array and affinity assays and 3) by effector functions in complement dependent cytotoxicity (CDC) and antibody dependent cellular cytotoxicity (ADCC) assays. The therapeutic potential of lead antibodies was further evaluated in xenograft models in SCID mice using GD2 positive CHLA255 neuroblastoma as well as with TC71 and SaoS2 sarcoma cell lines. Results: Antibodies that bind specific to purified GD2 by ELISA were expressed as recombinant antibodies in CHO cells. Many recovered antibodies showed cross-reactivity with several gangliosides in ELISA assays. Two antibodies with high specificity for GD2, 1B7 and 31F9 were selected for further studies. Binding to native antigen expressed on the cell surface of different cell lines was confirmed by FACS analysis. 31F9 was monospecific for GD2 (affinity by Surface Plasmon Resonance was ∼4 nM) while 1B7 showed dual specificity for GD2 and GM2 with affinities of ∼1 nM for GD2 and ∼ 370 nM for GM2, respectively. These two antibodies induced CDC ranged between 35% and 80%, and ADCC with human PBMCs between 40% and 65% on CHLA255, TC71 and SaoS2 cell lines. Survival following IV or SC challenge with SaoS2 and TC71 cells (respectively) was at least doubled following six IP treatments with 200 mcg of either 1B7 or 31F9 twice weekly. Inhibition of CHLA255 tumor growth was less dramatic. Conclusions: Vaccinated patients produce antigen-specific IgG antibodies that were further analyzed on the molecular level. Antibodies with single and dual specificity (GD2 and GM2) were recovered and shown to be very active in functional assays. Based on these favorable in vitro and in vivo studies, 1B7 and 31F9 humAbs merit further development efforts to evaluate potential utility for treatment of GD2 positive cancers. Citation Format: Govind Ragupathi, Xiaohong Wu, Ritsuko Sawada, Philip O. Livingston, Wolfgang W. Scholz. Novel fully human anti-GD2 monoclonal antibodies with potent therapeutic activity against neuroblastoma, sarcoma and melanoma. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 4993.

Published

2016