Your search keyword '"Abrouk, Nacer"' showing total 6 results

1. BETA prime: a first-in-man phase 1 study of AdAPT-001, an armed oncolytic adenovirus for solid tumors

Author

Conley, Anthony P., Roland, Christina L., Bessudo, Alberto, Gastman, Brian R., Villaflor, Victoria M., Larson, Christopher, Reid, Tony R., Caroen, Scott, Oronsky, Bryan, Stirn, Meaghan, Williams, Jeannie, Burbano, Erica, Coyle, Angelique, Barve, Minal A., Wagle, Naveed, Abrouk, Nacer, and Kesari, Santosh

Abstract

AdAPT-001 is an oncolytic adenovirus (OAV) with a transforming growth factor beta (TGF-ß) trap, which neutralizes the immunosuppressive and profibrotic cytokine, TGF-ß. The aim or purpose of this phase 1 study was to assess the safety and tolerability and, secondarily, the efficacy of AdAPT-001 after single intratumoral injection (IT) (Part 1) and multidose IT injection (Part 2) in patients with superficially accessible, advanced refractory solid tumors. Part 1 enrolled 9 patients with a 3 + 3 single dose-escalation safety run-in involving 2.5 × 1011, 5.0 × 1011, 1.0 × 1012viral particles (vps). No dose-limiting toxicities or treatment-related serious adverse events (SAEs) were seen. In Part 2, a dose-expansion phase, 19 patients received AdAPT-001 at 1.0 × 1012vps until disease progression according to Response Evaluation Criteria in Solid Tumors or RECIST 1.1. The overall responses to treatment included confirmed partial responses (3), durable stable disease ≥ 6 months (5), and progressive disease (13). AdAPT-001 is well tolerated. Evidence of an anti-tumor effect was seen in both injected and uninjected lesions. The recommended Phase 2 dose was 1.0 × 1012vp administered by intratumoral injection once every 2 weeks. Combination of AdAPT-001 with a checkpoint inhibition is enrolling.

Published

2023

2. Results from a biomarker study to accompany a phase II trial of RRx-001 with reintroduced platinum-based chemotherapy in relapsed small cell carcinoma

Author

Lee, Min-Jung, Tomita, Yusuke, Yuno, Akira, Lee, Sunmin, Abrouk, Nacer E., Oronsky, Bryan, Caroen, Scott, and Trepel, Jane B.

Abstract

ABSTRACTBackground: In a Phase II study RRx-001 was combined with Etoposide platinum (EP) in previously platinum treated SCLC. We correlated expression of the M2 marker, CD206, on HLA-DRlow/-monocytes, a phenotype that correlates with a poor prognosis, with response to RRx-001.Research design and methods: Patients received 4 mg RRx-001 once weekly until progression followed by the start of EP (etoposide 100 mg/m2IV on days 1–3 of a 21-day cycle and either cisplatin 80 mg/m2IV on day 1 or carboplatin AUC 5–6 IV on day 1). Treatment continued until progression or intolerable toxicity. Peripheral blood was collected in Cell Preparation Tubes with sodium citrate from 14 patients for exploratory studies during screening and after therapy on Days 1, 8, and 15. Peripheral blood mononuclear cells (PBMCs) were isolated from blood by centrifugation and multiparameter flow cytometric analysis was performed.Results: CD206 expression on HLA-DRlow/-monocytes was associated with response to chemotherapy and overall survival.Conclusion: During treatment with RRx-001, reduced expression of the protumorigenic M2 marker CD206 on peripheral monocytes positively correlated with increased response and survival.

Published

2021

3. RRx-001: a systemically non-toxic M2-to-M1 macrophage stimulating and prosensitizing agent in Phase II clinical trials

Author

Oronsky, Bryan, Paulmurugan, Ramasamy, Foygel, Kira, Scicinski, Jan, Knox, Susan J., Peehl, Donna, Zhao, Hongjuan, Ning, Shoucheng, Cabrales, Pedro, Summers, Thomas A., Reid, Tony R., Fitch, William L., Kim, Michelle M., Trepel, Jane B., Lee, Min-Jung, Kesari, Santosh, Abrouk, Nacer D., Day, Regina M., Oronsky, Arnold, Ray, Carolyn M., and Carterg, Corey A.

Abstract

ABSTRACTIntroduction: According to Hanahan and Weinberg, cancer manifests as six essential physiologic hallmarks: (1) self-sufficiency in growth signals, (2) insensitivity to growth-inhibitory signals, (3) evasion of programmed cell death, (4) limitless replicative potential, (5) sustained angiogenesis, and (6) invasion and metastasis. As a facilitator of these traits as well as immunosuppression and chemoresistance, the presence of tumor-associated macrophages (TAMs) may serve as the seventh hallmark of cancer. Anticancer agents that successfully reprogram TAMs to target rather than support tumor cells may hold the key to better therapeutic outcomes.Areas covered: This article summarizes the characteristics of the macrophage-stimulating agent RRx-001, a molecular iconoclast, sourced from the aerospace industry, with a particular emphasis on the cell-to-cell transfer mechanism of action (RBCs to TAMs) underlying its antitumor activity as well as its chemo and radioprotective properties, consolidated from various preclinical and clinical studies.Expert opinion: RRx-001 is macrophage-stimulating agent with the potential to synergize with chemotherapy, radiotherapy and immunotherapy while simultaneously protecting normal tissues from their cytotoxic effects. Given the promising indications of activity in multiple tumor types and these normal tissue protective properties, RRx-001 may be used to treat a broad spectrum of malignancies, if it is approved in the future.

Published

2017

4. RRx-001 and the “Right stuff”: Protection and treatment in outer space

Author

Oronsky, Bryan, Caroen, Scott, Abrouk, Nacer, and Reid, Tony R.

Abstract

•RRx-001, a well-tolerated anticancer agent in a Phase 3 clinical trial, has come full circle as a derivative of rocket fuel to potentially mitigate and treat the several prohibitive health hazards that are associated with long duration spaceflight both alone and in combination with other countermeasures.•As an NLRP3 inhibitor, an Nrf2 inducer and hypoxic nitric oxide donor, RRx-001 has anti-inflammatory, antioxidant, antifibrotic, anti-infectious, radioprotective and vasodilatory properties.•RRx-001 will hopefully serve as an “all purpose” therapeutic agent for astronauts to help reduce risks and make exploration-class missions within the solar system a reality.•Further investigation with RRx-001 under conditions that simulate deep spaceflight conditions are underway.

Published

2022

5. Discovery of RRx-001, a Myc and CD47 Downregulating Small Molecule with Tumor Targeted Cytotoxicity and Healthy Tissue Cytoprotective Properties in Clinical Development

Author

Oronsky, Bryan, Guo, XiaoNing, Wang, XiaoHui, Cabrales, Pedro, Sher, David, Cannizzo, Lou, Wardle, Bob, Abrouk, Nacer, Lybeck, Michelle, Caroen, Scott, Oronsky, Arnold, and Reid, Tony R.

Abstract

After extensive screening of aerospace compounds in an effort to source a novel anticancer agent, RRx-001, a first-in-class dinitroazetidine small molecule, was selected for advancement into preclinical and clinical development. RRx-001 is a minimally toxic small molecule with a distinct chemical structure and mechanism of action. The paradox of RRx-001 is that it mediates both antitumor cytotoxicity and normal tissue protection. The question of exactly how RRx-001 does this, and by means of what mechanism(s), depending on the route of delivery, intravenous or intratumoral, are explored. RRx-001 is currently in phase 2 and 3 clinical trials for the treatment of multiple solid tumor malignancies and as a supportive care drug.

Published

2021

6. P2.06-031 QUADRUPLE THREAT: A Pilot Phase 2 Study of RRx-001 in Advanced Lung Cancer Prior to Re-Administration of Platinum Doublets

Author

Brzezniak, Christina, Quinn, Mary, Zeman, Karen, Oronsky, Bryan, Scicinski, Jan, Caroen, Scott, Abrouk, Nacer, Degesys, Aiste, Schmitz, Bruno, Peterson, Paul, Roswarski, Joe, Trepel, Jane, Lee, Min-Jung, Lee, Sunmin, Tomita, Yusuke, Day, Regina, Jha, Saheli, and Carter, Corey

Published

2017