Your search keyword '"Barve, Minal A."' showing total 12 results

1. Pilot Trial of FANG Immunotherapy in Ewing's Sarcoma.

Author

Ghisoli, Maurizio, Barve, Minal, Schneider, Reva, Mennel, Robert, Lenarsky, Carl, Wallraven, Gladice, Pappen, Beena O, LaNoue, John, Kumar, Padmasini, Nemunaitis, Derek, Roth, Alyssa, Nemunaitis, James, Whiting, Sam, Senzer, Neil, Fletcher, Frederick A, and Nemunaitis, John

Subjects

*IMMUNOTHERAPY, *EWING'S sarcoma, *IMMUNOREGULATION, *BONE tumors, *TRANSFORMING growth factors-beta, *THERAPEUTICS, *TUMOR treatment

Abstract

We report on 12 consecutive patients with advanced/metastatic Ewing's sarcoma who were treated as a separate cohort of a phase 1 trial of FANG autologous immunotherapy (1 × 106-2.5 × 107 cells/intradermal injection each month for minimum 4 months). Safety and clinical response were monitored. Patient immune response to unmodified autologous tumor cells was assessed by gamma interferon-enzyme-linked immunospot (γIFN-ELISPOT) assay using peripheral blood mononuclear cells from baseline (pretreatment) and multiple postvaccination time points. None of the 12 patients (47 vaccinations) developed grade 2/3/4 drug-related toxicity. Median product release granulocyte-macrophage colony-stimulating factor expression was 1,941 pg/106 cells, and TGFβ1and TGFβ2 knockdown were 99 and 100%, respectively. Eight patients were assessed for ELISPOT response to autologous tumor cells at baseline and all (100%) were negative. In contrast, follow-up ELISPOT response at month 1 or month 4 (one patient) after FANG was positive in all eight patients. One patient achieved a partial tumor response (38% tumor reduction, RECIST 1.1). The Kaplan-Meier estimated survival of these 12 patients at 1 year was 75%. In this phase 1 study in patients with Ewing's sarcoma, FANG immunotherapy was well tolerated, elicited a tumor-specific systemic immune response in all patients, and was associated with favorable 1-year survival. Further clinical testing is indicated. [ABSTRACT FROM AUTHOR]

Published

2015

2. Phase 1 Trial of Bi-shRNA STMN1 BIV in Refractory Cancer.

Author

Barve, Minal, Wang, Zhaohui, Kumar, Padmasini, Jay, Christopher M, Luo, Xiuquan, Bedell, Cynthia, Mennel, Robert G, Wallraven, Gladice, Brunicardi, Francis Charles, Senzer, Neil, Nemunaitis, John, and Rao, Donald D

Subjects

*STATHMIN, *HAIRPIN (Genetics), *CANCER treatment, *MICROTUBULE-associated proteins, *ANTINEOPLASTIC agents, *CELLULAR signal transduction

Abstract

Stathmin1 (STMN1) is a microtubule modulator that is expressed in multiple cancers and correlates with poor survival. We previously demonstrated in vivo safety of bifunctional (bi) shRNA STMN1 bilamellar invaginated vesicle (BIV) and that systemic delivery correlated with antitumor activity. Patients with superficial advanced refractory cancer with no other standard options were entered into trial. Study design involved dose escalation (four patients/cohort) using a modified Fibonacci schema starting at 0.7 mg DNA administered via single intratumoral injection. Biopsy at baseline, 24/48 hours and resection 8 days after injection provided tissue for determination of cleavage product using next-generation sequencing (NGS) and reverse transcription quantitative polymerase chain reaction (RT-qPCR), 5′ RLM rapid amplification of cDNA ends (RACE) assay. Serum pharmacokinetics of circulating plasmid was done. Twelve patients were entered into three dose levels (0.7, 1.4, 7.0 mg DNA). No ≥ grade 3 toxic effects to drug were observed. Maximum circulating plasmid was detected at 30 seconds with less than 10% detectable in all subjects at 24 hours. No toxic effects were observed. Predicted cleavage product was detected by both NGS (n = 7/7 patients analyzed, cohorts 1, 2) and RLM RACE (n = 1/1 patients analyzed cohort 3). In conclusion, bi-shRNA STMN1 BIV is well tolerated and detection of mRNA target sequence-specific cleavage product confirmed bi-shRNA BIV mechanism of action. [ABSTRACT FROM AUTHOR]

Published

2015

3. ABCL-040: Pirtobrutinib (LOXO-305), a Next-Generation, Highly Selective, Non-Covalent Bruton's Tyrosine Kinase Inhibitor in Previously Treated Mantle Cell Lymphoma and Other Non-Hodgkin Lymphomas: Phase 1/2 BRUIN Study Results.

Author

Cohen, Jonathon B., Shah, Nirav N., Alencar, Alvaro J., Gerson, James N., Patel, Manish R., Fahkri, Bita, Jurczak, Wojciech, Tan, Xuan N., Lewis, Katharine L., Fenske, Timothy S., Coombs, Catherine C., Flinn, Ian, Lewis, David J., Gouill, Stephen Le, Palomba, M Lia, Woyach, Jennifer A., Pagel, John M., Lamanna, Nicole, Barve, Minal A., and Ghia, Paolo

Published

2021

4. CLL-039: Pirtobrutinib (LOXO-305), a Next-Generation, Highly Selective, Non-Covalent BTK Inhibitor in Previously Treated CLL/SLL: Results from the Phase 1/2 BRUIN Study.

Author

Coombs, Catherine C., Pagel, John M., Shah, Nirav N., Lamanna, Nicole, Lech-Maranda, Ewa, Eyre, Toby A., Woyach, Jennifer A., Wierda, William G, Cheah, Chan Y., Roeker, Lindsey, Patel, Manish R., Fakhri, Bita, Barve, Minal A., Tam, Constantine S., Lewis, David J., Gerson, James N., Alencar, Alvaro, Taylor, Justin, Abdel-Wahab, Omar, and Ghia, Paolo

Published

2021

5. Phase I Trial of 'bi-shRNAifurin/GMCSF DNA/Autologous Tumor Cell' Vaccine (FANG) in Advanced Cancer.

Author

Senzer, Neil, Barve, Minal, Kuhn, Joseph, Melnyk, Anton, Beitsch, Peter, Lazar, Martin, Lifshitz, Samuel, Magee, Mitchell, Oh, Jonathan, Mill, Susan W, Bedell, Cynthia, Higgs, Candice, Kumar, Padmasini, Yu, Yang, Norvell, Fabienne, Phalon, Connor, Taquet, Nicolas, Rao, Donald D, Wang, Zhaohui, and Jay, Chris M

Subjects

*GRANULOCYTE-macrophage colony-stimulating factor, *IMMUNOSUPPRESSIVE agents, *ENZYME-linked immunosorbent assay, *ADVERSE health care events, *IMMUNOREGULATION, *IMMUNOSUPPRESSION

Abstract

We performed a phase I trial of FANG vaccine, an autologous tumor-based product incorporating a plasmid encoding granulocyte-macrophage colony-stimulating factor (GMCSF) and a novel bifunctional short hairpin RNAi (bi-shRNAi) targeting furin convertase, thereby downregulating endogenous immunosuppressive transforming growth factors (TGF) β1 and β2. Patients with advanced cancer received up to 12 monthly intradermal injections of FANG vaccine (1 × 107 or 2.5 × 107 cells/ml injection). GMCSF, TGFβ1, TGFβ2, and furin proteins were quantified by enzyme-linked immunosorbent assay (ELISA). Safety and response were monitored. Vaccine manufacturing was successful in 42 of 46 patients of whom 27 received ≥1 vaccine. There were no treatment-related serious adverse events. Most common grade 1, 2 adverse events included local induration (n = 14) and local erythema (n = 11) at injection site. Post-transfection mean product expression GMCSF increased from 7.3 to 1,108 pg/106 cells/ml. Mean TGFβ1 and β2 effective target knockdown was 93.5 and 92.5% from baseline, respectively. Positive enzyme-linked immunospot (ELISPOT) response at month 4 was demonstrated in 9 of 18 patients serially assessed and correlated with survival duration from time of treatment (P = 0.025). Neither dose-adverse event nor dose-response relationship was noted. In conclusion, FANG vaccine was safe and elicited an immune response correlating with prolonged survival. Phase II assessment is justified. [ABSTRACT FROM AUTHOR]

Published

2012

6. Poster: ABCL-040: Pirtobrutinib (LOXO-305), a Next-Generation, Highly Selective, Non-Covalent Bruton's Tyrosine Kinase Inhibitor in Previously Treated Mantle Cell Lymphoma and Other Non-Hodgkin Lymphomas: Phase 1/2 BRUIN Study Results.

Author

Cohen, Jonathon B., Shah, Nirav N., Alencar, Alvaro J., Gerson, James N., Patel, Manish R., Fahkri, Bita, Jurczak, Wojciech, Tan, Xuan N., Lewis, Katharine L., Fenske, Timothy S., Coombs, Catherine C., Flinn, Ian, Lewis, David J., Le Gouill, Stephen, Palomba, M. Lia, Woyach, Jennifer A., Pagel, John M., Lamanna, Nicole, Barve, Minal A., and Ghia, Paolo

Published

2021

7. Poster: CLL-039: Pirtobrutinib (LOXO-305), a Next-Generation, Highly Selective, Non-Covalent BTK Inhibitor in Previously Treated CLL/SLL: Results from the Phase 1/2 BRUIN Study.

Author

Coombs, Catherine C., Pagel, John M., Shah, Nirav N., Lamanna, Nicole, Lech-Maranda, Ewa, Eyre, Toby A., Woyach, Jennifer A., Wierda, William G., Cheah, Chan Y., Roeker, Lindsey, Patel, Manish R., Fakhri, Bita, Barve, Minal A., Tam, Constantine S., Lewis, David J., Gerson, James N., Alencar, Alvaro, Taylor, Justin, Abdel-Wahab, Omar, and Ghia, Paolo

Published

2021

8. Oral Abstract: CLL-039: Pirtobrutinib (LOXO-305), a Next-Generation, Highly Selective, Non-Covalent BTK Inhibitor in Previously Treated CLL/SLL: Results from the Phase 1/2 BRUIN Study.

Author

Coombs, Catherine C., Pagel, John M., Shah, Nirav N., Lamanna, Nicole, Lech-Maranda, Ewa, Eyre, Toby A., Woyach, Jennifer A., Wierda, William G., Cheah, Chan Y., Roeker, Lindsey, Patel, Manish R., Fakhri, Bita, Barve, Minal A., Tam, Constantine S., Lewis, David J., Gerson, James N., Alencar, Alvaro, Taylor, Justin, Abdel-Wahab, Omar, and Ghia, Paolo

Published

2021

9. A Relative Bioavailability, Bioequivalence, and Food Effect Study of Niraparib Tablets in Patients with Advanced Solid Tumors.

Author

Falchook, Gerald, Patnaik, Amita, Richardson, Debra L., Harvey, R. Donald, Sharma, Manish R., Hafez, Navid, Hamilton, Erika, Piha-Paul, Sarina A., Barve, Minal, Wise-Draper, Trisha, Patel, Manish R., Dowlati, Afshin, Pascuzzo, Joseph, Tang, Shou-Ching, Faltermeier, Christina, Malinowska, Izabela A., Shtessel, Luda, Striha, Alina, and Potocka, Elizabeth

Published

2024

10. Gemogenovatucel-T (Vigil) immunotherapy as maintenance in frontline stage III/IV ovarian cancer (VITAL): a randomised, double-blind, placebo-controlled, phase 2b trial.

Author

Rocconi, Rodney P, Grosen, Elizabeth A, Ghamande, Sharad A, Chan, John K, Barve, Minal A, Oh, Jonathan, Tewari, Devansu, Morris, Peter C, Stevens, Erin E, Bottsford-Miller, Justin N, Tang, Min, Aaron, Phylicia, Stanbery, Laura, Horvath, Staci, Wallraven, Gladice, Bognar, Ernest, Manning, Luisa, Nemunaitis, John, Shanahan, David, and Slomovitz, Brian M

Subjects

*RESEARCH, *OVARIAN tumors, *TIME, *RESEARCH methodology, *CANCER relapse, *EVALUATION research, *MEDICAL cooperation, *TREATMENT effectiveness, *TUMOR classification, *COMPARATIVE studies, *RANDOMIZED controlled trials, *ENDOMETRIAL tumors, *BLIND experiment, *CANCER vaccines

Abstract

Background: Gemogenovatucel-T is an autologous tumour cell vaccine manufactured from harvested tumour tissue, which specifically reduces expression of furin and downstream TGF-β1 and TGF-β2. The aim of this study was to determine the safety and efficacy of gemogenovatucel-T in front-line ovarian cancer maintenance.Methods: This randomised, double-blind, placebo-controlled, phase 2b trial involved 25 hospitals in the USA. Women aged 18 years and older with stage III/IV high-grade serous, endometrioid, or clear cell ovarian cancer in clinical complete response after a combination of surgery and five to eight cycles of chemotherapy involving carboplatin and paclitaxel, and an Eastern Cooperative Oncology Group status of 0 or 1 were eligible for inclusion in the study. Patients were randomly assigned (1:1) to gemogenovatucel-T or placebo by an independent third party interactive response system after successful screening using randomly permuted block sizes of two and four and stratified by extent of surgical cytoreduction and neoadjuvant versus adjuvant chemotherapy. Gemogenovatucel-T (1 × 107 cells per injection) or placebo was administered intradermally (one per month) for a minimum of four and up to 12 doses. Patients, investigators, and clinical staff were masked to patient allocation until after statistical analysis. The primary endpoint was recurrence-free survival, analysed in the per-protocol population. All patients who received at least one dose of gemogenovatucel-T were included in the safety analysis. The study is registered with ClinicalTrials.gov, NCT02346747.Findings: Between Feb 11, 2015, and March 2, 2017, 310 patients consented to the study at 22 sites. 217 were excluded. 91 patients received gemogenovatucel-T (n=47) or placebo (n=44) and were analysed for safety and efficacy. The median follow-up from first dose of gemogenovatucel-T was 40·0 months (IQR 35·0-44·8) and from first dose of placebo was 39·8 months (35·5-44·6). Recurrence-free survival was 11·5 months (95% CI 7·5-not reached) for patients assigned to gemogenovatucel-T versus 8·4 months (7·9-15·5) for patients assigned to placebo (HR 0·69, 90% CI 0·44-1·07; one-sided p=0·078). Gemogenovatucel-T resulted in no grade 3 or 4 toxic effects. Two patients in the placebo group had five grade 3 toxic events, including arthralgia, bone pain, generalised muscle weakness, syncope, and dyspnea. Seven patients (four in the placebo group and three in the gemogenovatucel-T group) had 11 serious adverse events. No treatment-related deaths were reported in either of the groups.Interpretation: Front-line use of gemogenovatucel-T immunotherapy as maintenance was well tolerated but the primary endpoint was not met. Further investigation of gemogenovatucel-T in patients stratified by BRCA mutation status is warranted.Funding: Gradalis. [ABSTRACT FROM AUTHOR]

Published

2020

11. Entrectinib in patients with advanced or metastatic NTRK fusion-positive solid tumours: integrated analysis of three phase 1-2 trials.

Author

Doebele, Robert C, Drilon, Alexander, Paz-Ares, Luis, Siena, Salvatore, Shaw, Alice T, Farago, Anna F, Blakely, Collin M, Seto, Takashi, Cho, Byung Chul, Tosi, Diego, Besse, Benjamin, Chawla, Sant P, Bazhenova, Lyudmila, Krauss, John C, Chae, Young Kwang, Barve, Minal, Garrido-Laguna, Ignacio, Liu, Stephen V, Conkling, Paul, and John, Thomas

Subjects

*TUMORS, *PATIENT safety, *GENE fusion, *BLOOD-brain barrier, *GENE rearrangement

Abstract

Background: Entrectinib is a potent inhibitor of tropomyosin receptor kinase (TRK) A, B, and C, which has been shown to have anti-tumour activity against NTRK gene fusion-positive solid tumours, including CNS activity due to its ability to penetrate the blood-brain barrier. We present an integrated efficacy and safety analysis of patients with metastatic or locally advanced solid tumours harbouring oncogenic NTRK1, NTRK2, and NTRK3 gene fusions treated in three ongoing, early-phase trials.Methods: An integrated database comprised the pivotal datasets of three, ongoing phase 1 or 2 clinical trials (ALKA-372-001, STARTRK-1, and STARTRK-2), which enrolled patients aged 18 years or older with metastatic or locally advanced NTRK fusion-positive solid tumours who received entrectinib orally at a dose of at least 600 mg once per day in a capsule. All patients had an Eastern Cooperative Oncology Group performance status of 0-2 and could have received previous anti-cancer therapy (except previous TRK inhibitors). The primary endpoints, the proportion of patients with an objective response and median duration of response, were evaluated by blinded independent central review in the efficacy-evaluable population (ie, patients with NTRK fusion-positive solid tumours who were TRK inhibitor-naive and had received at least one dose of entrectinib). Overall safety evaluable population included patients from STARTRK-1, STARTRK-2, ALKA-372-001, and STARTRK-NG (NCT02650401; treating young adult and paediatric patients [aged ≤21 years]), who received at least one dose of entrectinib, regardless of tumour type or gene rearrangement. NTRK fusion-positive safety evaluable population comprised all patients who have received at least one dose of entrectinib regardless of dose or follow-up. These ongoing studies are registered with ClinicalTrials.gov, NCT02097810 (STARTRK-1) and NCT02568267 (STARTRK-2), and EudraCT, 2012-000148-88 (ALKA-372-001).Findings: Patients were enrolled in ALKA-372-001 from Oct 26, 2012, to March 27, 2018; in STARTRK-1 from Aug 7, 2014, to May 10, 2018; and in STARTRK-2 from Nov 19, 2015 (enrolment is ongoing). At the data cutoff date for this analysis (May 31, 2018) the efficacy-evaluable population comprised 54 adults with advanced or metastatic NTRK fusion-positive solid tumours comprising ten different tumour types and 19 different histologies. Median follow-up was 12.9 months (IQR 8·77-18·76). 31 (57%; 95% CI 43·2-70·8) of 54 patients had an objective response, of which four (7%) were complete responses and 27 (50%) partial reponses. Median duration of response was 10 months (95% CI 7·1 to not estimable). The most common grade 3 or 4 treatment-related adverse events in both safety populations were increased weight (seven [10%] of 68 patients in the NTRK fusion-positive safety population and in 18 [5%] of 355 patients in the overall safety-evaluable population) and anaemia (8 [12%] and 16 [5%]). The most common serious treatment-related adverse events were nervous system disorders (three [4%] of 68 patients and ten [3%] of 355 patients). No treatment-related deaths occurred.Interpretation: Entrectinib induced durable and clinically meaningful responses in patients with NTRK fusion-positive solid tumours, and was well tolerated with a manageable safety profile. These results show that entrectinib is a safe and active treatment option for patients with NTRK fusion-positive solid tumours. These data highlight the need to routinely test for NTRK fusions to broaden the therapeutic options available for patients with NTRK fusion-positive solid tumours.Funding: Ignyta/F Hoffmann-La Roche. [ABSTRACT FROM AUTHOR]

Published

2020

12. Phase I Study of a Systemically Delivered p53 Nanoparticle in Advanced Solid Tumors.

Author

Senzer, Neil, Nemunaitis, John, Nemunaitis, Derek, Bedell, Cynthia, Edelman, Gerald, Barve, Minal, Nunan, Robert, Pirollo, Kathleen F, Rait, Antonina, and Chang, Esther H

Subjects

*P53 antioncogene, *NANOPARTICLES, *METASTASIS, *CANCER treatment, *LIPOSOMES, *TRANSFERRIN receptors

Abstract

Selective delivery of therapeutic molecules to primary and metastatic tumors is optimal for effective cancer therapy. A liposomal nanodelivery complex (scL) for systemic, tumor-targeting delivery of anticancer therapeutics has been developed. scL employs an anti-transferrin receptor (TfR), scFv as the targeting molecule. Loss of p53 suppressor function, through mutations or inactivation of the p53 pathway, is present in most human cancers. Rather than being transiently permissive for tumor initiation, persistence of p53 dysfunction is a continuing requirement for maintaining tumor growth. Herein, we report results of a first-in-man Phase I clinical trial of restoration of the normal human tumor suppressor gene p53 using the scL nanocomplex (SGT-53). Minimal side effects were observed in this trial in patients with advanced solid tumors. Furthermore, the majority of patients demonstrated stable disease. One patient with adenoid cystic carcinoma had his status changed from unresectable to resectable after one treatment cycle. More significantly, we observed an accumulation of the transgene in metastatic tumors, but not in normal skin tissue, in a dose-related manner. These results show not only that systemically delivered SGT-53 is well tolerated and exhibits anticancer activity, but also supply evidence of targeted tumor delivery of SGT-53 to metastatic lesions. [ABSTRACT FROM AUTHOR]

Published

2013