Your search keyword '"Davila, Marco L"' showing total 15 results

1. Adding chimeric antigen receptor-induced killer cells to the medical oncology shelf

Author

Brandjes, Brigett D. and Davila, Marco L.

Subjects

Antigens, Killer cells, Axicabtagene ciloleucel, T cells, Tisagenlecleucel, Automobile industry, Genes, Cancer, Tumors, Health care industry

Abstract

With the approval of CD19-targeted chimeric antigen receptor (CAR) T cells for the treatment of B cell malignancies, clinicians have gained valuable insights into the power and challenges of cellular therapies. In this issue of the JCI, Maluski et al. showed that a CAR containing a CD28 costimulatory domain drives progeny differentiation to resemble that of NK cells, which have the potential for an off-the-shelf cell therapy. These CAR-induced killer (CARiK) cells displayed potent antitumor function and killed across the MHC barrier in vivo. After performing in vitro and in vivo mouse studies, the authors also successfully differentiated human umbilical cord blood-derived progenitor cells into CARiK cells. These unique cells may address some of the current challenges associated with first-generation CARs, such as prolonged production that requires patients to wait weeks for infusion. We believe this innovative progenitor gene-engineered lymphoid system has the potential for clinical translation., Gene-engineered chimeric antigen receptor cell therapies It has been two years since the FDA approved gene-engineered chimeric antigen receptor (CAR) T cell therapy for the treatment of B cell acute [...]

Published

2019

2. CD19-Targeted T Cells for Hematologic Malignancies: Clinical Experience to Date.

Author

Davila, Marco L., Sauter, Craig, and Brentjens, Renier

Subjects

ANTIGENS, IMMUNOTHERAPY, T cells, HEMATOLOGIC malignancies

Abstract

Recently, immunotherapy for cancer has begun to garner traction with encouraging results in a number of malignancies. Included within this arena has been the genetic engineering of autologous T cells with chimeric antigen receptors (CARs) against tumor target. The majority of this experience has included the use of CAR T cells directed against CD19 for B-cell hematologic malignancies. The most striking efficacy to date with CAR T cells directed against CD19 has been in relapsed and refractory B-cell acute lymphoblastic leukemia, with the overwhelming majority of patients experiencing complete remissions. In addition, single-center and largely early-phase studies have demonstrated responses in patients with varying histologic findings of relapsed and refractory B-cell non-Hodgkin lymphoma. The favorable response rates seen with this technology have been tempered by the high risk of toxicity, particularly in the form of cytokine-release syndrome and neurotoxicity. Agents such as tocilizumab and corticosteroids have been used to treat these toxicities. The current state of the science includes strategies to circumvent and treat toxicity, manufacturing, and study of later-generation CAR constructs with the intention of improving efficacy and development of CARs against other tumor targets for both hematologic and solid tumor malignancies. The observation of an early efficacy ensures further integration and development of this modality into future immunotherapeutic strategies for various cancers. [ABSTRACT FROM AUTHOR]

Published

2015

3. CD19 CAR-Targeted T Cells Induce Long-Term Remission and B Cell Aplasia in an Immunocompetent Mouse Model of B Cell Acute Lymphoblastic Leukemia.

Author

Davila, Marco L., Kloss, Christopher C., Gunset, Gertrude, and Sadelain, Michel

Subjects

*CD19 antigen, *T cells, *B cells, *IMMUNOCOMPETENT cells, *LABORATORY mice, *LYMPHOBLASTIC leukemia, *CANCER remission, *IMMUNOTHERAPY

Abstract

Although many adults with B cell acute lymphoblastic leukemia (B-ALL) are induced into remission, most will relapse, underscoring the dire need for novel therapies for this disease. We developed murine CD19-specific chimeric antigen receptors (CARs) and an immunocompetent mouse model of B-ALL that recapitulates the disease at genetic, cellular, and pathologic levels. Mouse T cells transduced with an all-murine CD3ζ/CD28-based CAR that is equivalent to the one being used in our clinical trials, eradicate B-ALL in mice and mediate long-term B cell aplasias. In this model, we find that increasing conditioning chemotherapy increases tumor eradication, B cell aplasia, and CAR-modified T cell persistence. Quantification of recipient B lineage cells allowed us to estimate an in vivo effector to endogenous target ratio for B cell aplasia maintenance. In mice exhibiting a dramatic B cell reduction we identified a small population of progenitor B cells in the bone marrow that may serve as a reservoir for long-term CAR-modified T cell stimulation. Lastly, we determine that infusion of CD8+ CAR-modified T cells alone is sufficient to maintain long-term B cell eradication. The mouse model we report here should prove valuable for investigating CAR-based and other therapies for adult B-ALL. [ABSTRACT FROM AUTHOR]

Published

2013

4. How do CARs work? Early insights from recent clinical studies targeting CD19.

Author

Davila, Marco L., Brentjens, Renier, Xiuyan Wang, Rivière, Isabelle, and Sadelain, Michel

Subjects

*ANTIGEN receptors, *T cells, *HLA histocompatibility antigens, *B cells, *CHIMERIC proteins

Abstract

Second-generation chimeric antigen receptors (CARs) are powerful tools to redirect antigen-specific T cells independently of HLA-restriction. Recent clinical studies evaluating CD19- targeted T cells in patients with B-cell malignancies demonstrate the potency of CAR-engineered T cells. With results from 28 subjects enrolled by five centers conducting studies in patients with chronic lymphocytic leukemia (CLL) or lymphoma, some insights into the parameters that determine T-cell function and clinical outcome of CAR-based approaches are emerging. These parameters involve CAR design, T-cell production methods, conditioning chemotherapy as well as patient selection. Here, we discuss the potential relevance of these findings and in particular the interplay between the adoptive transfer of T cells and pre-transfer patient conditioning. [ABSTRACT FROM AUTHOR]

Published

2012

5. CAR T-Cell Therapy Associated with Unique, Acute Adverse Events Requiring Vigilant Monitoring.

Author

Davila, Marco L.

Subjects

TUMOR treatment, HYPOXEMIA, BIOMARKERS, CANCER patient medical care, CARDIAC output, CELLULAR therapy, CYTOKINES, FERRITIN, FEVER, HYPOTENSION, IMMUNOTHERAPY, INTERLEUKINS, T cells, TACHYCARDIA, UREMIA, TACHYPNEA

Published

2019

6. CAR T cells find strength in polyfunction.

Author

Davila, Marco L.

Subjects

*ANTIGEN receptors, *T cells, *HETEROGENEITY, *REGENERATION (Biology), *AUTOIMMUNITY

Abstract

In this issue of Blood, Rossi et al report that the heterogeneity of personalized chimeric antigen receptor (CAR) T cells has limited the ability to identify product attributes that enhance patient outcomes, but they have showed that by using single-cell analyses, heterogeneity may actually improve clinical outcomes.¹ [ABSTRACT FROM AUTHOR]

Published

2018

7. Insight into next-generation CAR therapeutics: designing CAR T cells to improve clinical outcomes.

Author

Roselli, Emiliano, Faramand, Rawan, and Davila, Marco L.

Subjects

*T cells, *TUMOR lysis syndrome, *CHIMERIC antigen receptors, *THERAPEUTICS, *HEMATOLOGIC malignancies, *CELLULAR therapy

Abstract

Chimeric antigen receptor (CAR) T cell therapy has shown considerable promise for hematologic malignancies, leading to the US Food and Drug Administration approval of two CAR T cell-based therapies for the treatment of B cell acute lymphoblastic leukemia and large B cell lymphoma. Despite success in hematologic malignancies, the treatment landscape of CAR T cell therapy for solid tumors has been limited. There are unique challenges in the development of novel CAR T cell therapies to improve both safety and efficacy. Improved understanding of the immunosuppressive tumor microenvironment and resistance mechanisms has led to encouraging approaches to mitigating these obstacles. This Review will characterize challenges with current CAR T designs for hematologic malignancies and solid tumors and emphasize preclinical and clinical strategies to overcome them with novel CAR T cell therapies. [ABSTRACT FROM AUTHOR]

Published

2021

8. CARs Move To the Fast Lane.

Author

Davila, Marco L and Papapetrou, Eirini P

Subjects

*IMMUNOTHERAPY, *CANCER treatment, *ANTIGEN receptors, *T cells

Abstract

The author reflects on immunotherapy approach to treat cancer which involves genetic retargeting of T cells with chimeric antigen receptors (CARs). The author mentions that CAR technology was started in the late 1980s where scientific organizations including Baylor College of Medicine (BCM), Memorial Sloan-Kettering Cancer Center (MSKCC), and the National Cancer Institute (NCI) have made essential developments. Other topics include antibody, cytokine release syndrome (CRS), and tocilizumab.

Published

2014

9. Human CD83-targeted chimeric antigen receptor T cells prevent and treat graft-versus-host disease.

Author

Shrestha, Bishwas, Walton, Kelly, Reff, Jordan, Sagatys, Elizabeth M., Nhan Tu, Boucher, Justin, Gongbo Li, Ghafoor, Tayyebb, Felices, Martin, Miller, Jeffrey S., Pidala, Joseph, Blazar, Bruce R., Anasetti, Claudio, Betts, Brian C., Davila, Marco L., Tu, Nhan, Boucher, Justin C, Li, Gongbo, Ghafoor, Tayyeb, and Miller, Jeffrey

Subjects

*CHIMERIC antigen receptors, *SUPPRESSOR cells, *GRAFT versus host disease, *T cells, *ACUTE myeloid leukemia, *PRELEUKEMIA, *ACUTE myeloid leukemia treatment, *GRAFT versus host disease prevention, *PROTEINS, *RESEARCH, *IMMUNOGLOBULINS, *IMMUNIZATION, *HOMOGRAFTS, *ANIMAL experimentation, *RESEARCH methodology, *EVALUATION research, *MEDICAL cooperation, *MEMBRANE glycoproteins, *COMPARATIVE studies, *RESEARCH funding, *HEMATOPOIETIC stem cell transplantation, *CELL lines, *ANTIGENS, *MICE

Abstract

Graft-versus-host disease (GVHD) remains an important cause of morbidity and mortality after allogeneic hematopoietic cell transplantation (allo-HCT). For decades, GVHD prophylaxis has included calcineurin inhibitors, despite their incomplete efficacy and impairment of graft-versus-leukemia (GVL). Distinct from pharmacologic immune suppression, we have developed what we believe is a novel, human CD83-targeted chimeric antigen receptor (CAR) T cell for GVHD prevention. CD83 is expressed on allo-activated conventional CD4+ T cells (Tconvs) and proinflammatory dendritic cells (DCs), which are both implicated in GVHD pathogenesis. Human CD83 CAR T cells eradicate pathogenic CD83+ target cells, substantially increase the ratio of regulatory T cells (Tregs) to allo-activated Tconvs, and provide durable prevention of xenogeneic GVHD. CD83 CAR T cells are also capable of treating xenogeneic GVHD. We show that human acute myeloid leukemia (AML) expresses CD83 and that myeloid leukemia cell lines are readily killed by CD83 CAR T cells. Human CD83 CAR T cells are a promising cell-based approach to preventing 2 critical complications of allo-HCT - GVHD and relapse. Thus, the use of human CD83 CAR T cells for GVHD prevention and treatment, as well as for targeting CD83+ AML, warrants clinical investigation. [ABSTRACT FROM AUTHOR]

Published

2020

10. Radiation Therapy as a Bridging Strategy for CAR T Cell Therapy With Axicabtagene Ciloleucel in Diffuse Large B-Cell Lymphoma.

Author

Sim, Austin J., Jain, Michael D., Figura, Nicholas B., Chavez, Julio C., Shah, Bijal D., Khimani, Farhad, Lazaryan, Aleksandr, Krivenko, Gabriel, Davila, Marco L., Liu, Hien D., Falchook, Aaron D., Dahiya, Saurabh, Rapoport, Aaron P., Kim, Sungjune, Locke, Frederick L., and Robinson, Timothy J.

Subjects

*DIFFUSE large B-cell lymphomas, *T cells, *CELLULAR therapy, *RADIOTHERAPY, *CHIMERIC antigen receptors, *LYMPHOCYTE count

Abstract

Purpose: Axicabtagene ciloleucel (axi-cel) is a CD19-directed chimeric antigen receptor (CAR) T-cell therapy for relapsed or refractory diffuse large B-cell lymphoma. Bridging therapy may be required for lymphoma control during the manufacturing interval between collection of autologous T cells and final CAR T product administration. The optimal bridging therapy is not known and patients are often chemorefractory. We present a case series of patients receiving radiation as a bridge to axi-cel.Methods and Materials: Between December 2017 and October 2018, 12 patients were intended to receive bridging radiation before axi-cel. The group was characterized by highly aggressive disease including 6 of 12 with "double hit" lymphoma and 6 of 12 with disease ≥10 cm in diameter. All patients received 2 to 4 Gy/fraction to a median dose of 20 Gy (range, 6-36.5 Gy). Half of patients received either 30 Gy in 10 fractions or 20 Gy in 5 fractions. Seven patients received concurrent chemotherapy. Eleven patients underwent axi-cel infusion and one did not. Median follow-up was 3.3 months (range, 1.1-12.0 months).Results: No significant toxicities were identified during bridging radiation, and no patient experienced in-field progression of disease before axi-cel infusion. One patient experienced abdominal pain, which resolved after dose reduction. Two patients had out-of-field progression of disease during the bridging period. After axi-cel infusion, 3 of 11 patients (27%) experienced severe cytokine release syndrome or neurotoxicity. At 30 days, the objective response rate was 81.8% (11 of 12 evaluable; 1 stable disease, 1 out-of-field progression), with complete response in 27% (3 of 11). At last follow-up, the best objective response rate was 81.8%, with a complete response attained in 45% (5 of 11). Lymphocyte counts decreased slightly in 10 of 12 patients during radiation (median, 0.25 k/uL).Conclusions: Radiation (with or without concurrent chemotherapy) can be safely administered as a bridge to axi-cel in high-risk lymphoma. Caution should be taken if irradiation is started before apheresis, and lymphocyte counts should be monitored closely throughout. Future investigation is warranted to optimize the use of bridging radiation before CAR T therapy. [ABSTRACT FROM AUTHOR]

Published

2019

11. CARDIAC EVENTS AFTER ANTI-BCMA CHIMERIC ANTIGEN RECEPTOR T-CELL (IDECABTAGENE VICLEUCEL) FOR MULTIPLE MYELOMA.

Author

Lee, Dae Hyun, Chandrasekhar, Sanjay Amrith, Jain, Michael, Hansen, Doris, Freeman, Ciara, Alsina, Melissa, Baz, Rachid, Puglianini, Omar Castaneda, Liu, Hien, Blue, Brandon, Davila, Marco L., Faramand, Rawan, Kumar, Abhishek, Shah, Bijal, Lazaryan, Aleksandr, Khimani, Farhad, Nishihori, Taiga, Bachmeier, Christina, Locke, Frederick, and Oliveira, Guilherme Henrique

Subjects

*CHIMERIC antigen receptors, *MULTIPLE myeloma, *T cells

Published

2022

12. Safety and persistence of adoptively transferred autologous CD 19-targeted T cells in patients with relapsed or chemotherapy refractory B-cell leukemias.

Author

Brentjens, Renier J., Rivière, Isabelle, Park, Jae H., Davila, Marco L., Xiuyan Wang, Stefanski, Jolanta, Taylor, Clare, Yeh, Raymond, Bartido, Shirley, Borquez-Ojeda, Oriana, Olszewska, Malgorzata, Bernal, Yvette, Pegram, Hollie, Przybylowski, Mark, Hollyman, Daniel, Usachenko, Yelena, Pirraglia, Domenick, Hosey, James, Santos, Elmer, and Halton, Elizabeth

Subjects

*B cell lymphoma, *T cells, *DRUG therapy, *ANTIGENS, *LYMPHOCYTES

Abstract

We report the findings from the first 10 patients with chemotherapy-refractory chronic lymphocytic leukemia (CLL) or relapsed B-cell acute lymphoblastic leukemia (ALL) we have enrolled for treatment with autologous T cells modified to express 19-28z, a second-generation chimeric antigen (Ag) receptor specific to the B-cell lineage Ag CD19. Eight of the 9 treated patients tolerated 19-28z+ T-cell infusions well. Three of 4 evaluable patients with bulky CLL who received prior conditioning with cyclophosphamide exhibited either a significant reduction or a mixed response in lymphadenopathy without concomitant development of B-cell aplasia. In contrast, one patient with relapsed ALL who was treated in remission with a similar T-cell dose developed a predicted B-cell aplasia. The short-term persistence of infused T cells was enhanced by prior cyclophosphamide administration and inversely proportional to the peripheral blood tumor burden. Further analyses showed rapid trafficking of modified T cells to tumor and retained ex vivo cytotoxic potential of CD19-targeted T cells retrieved 8 days after infusion. We conclude that this adoptive T-cell approach is promising and more likely to show clinical benefit in the setting of prior conditioning chemotherapy and low tumor burden or minimal residual disease. These studies are registered at www.clinicaltrials.org as #NCT00466531 (CLL protocol) and #NCT01044069 (B-ALL protocol). [ABSTRACT FROM AUTHOR]

Published

2011

13. Chimeric Antigen Receptor T Cell Therapy for Acute Myeloid Leukemiachimeric Antigen Receptor T Cell Therapy for Acute Myeloid Leukemia.

Author

Shrestha, Bishwas, Vishwasrao, Paresh, Li, Gongbo, Ghafoor, Tayyebb, and Davila, Marco L.

Subjects

*T cell receptors, *CHIMERIC antigen receptors, *ACUTE myeloid leukemia, *ANTIGEN receptors, *CELL receptors, *CELLULAR therapy, *HEMATOPOIESIS, *T cells

Abstract

Relapse of leukemic cells that do not express the antigen targeted by chimeric antigen receptor (CAR) is still a risk. As is the potential for targeting hematopoietic stem cells (HSCs) that share the same antigen expression, off-tumor on-target toxicity. Further, CAR T cells that bind different epitopes of the same antigen can have different tumor-killing efficacies. Therefore, we screen murine single chain variable fragment (scFv) based for indirect affinity to identify a CAR that targets Acute myeloid leukemia (AML), while minimizing toxicities. Also, recent advances in CAR design have demonstrated that the requirement of two separate tumor antigens to be ligated by CARs can increase the specificity for tumor targets. So designing a CAR that only activates a T cell when it binds two separate AML antigens will allow T cells to enhance safety. Therefore, we set out to develop a affinity based multi-antigen CAR T cell therapy that targets well described antigens for AML, including CD33 and CD123. Mice were immunized with these antigens, spleens collected, and fused with myeloma cell lines. The antibodies of fused hybridomas were screened for binding and activation against antigens by high throughput flow cytometry. After screening, we derived multiple de novo CD33, and CD123 scFvs by sequencing. We incorporated CD33 and CD123 scFvs into standard mono-specific CARs utilizing a 41BB co-stimulatory domain to validate antigen-specificity. Gene transfer assessment of CAR T cells demonstrated about 50-80% transduction efficiency for CD33 and CD123 scFvs. There were no differences in CD4 and CD8 proportions in these CAR T cells. We next examined the CARs for their cytotoxic ability using a Real-Time Cell Analysis (RTCA) system. For the CD33 CARs, 2 (6A11-1 and 27A3-1) out of 5, and for the CD123 CAR, 2 (15A12-11 and 15 A12-12) out of 8, scFv sequences transduced into T cells were highly efficacious at killing target cells and generated significant amounts of cytokines such as IFN-g, TNF- a, and IL-6. CAR T cells with these same scFv sequences were able to proliferate better in response to targeted antigen. To find the best possible combination of CD33 and CD123 scFvs we double transduced T cells with four selected CD33 or CD123 scFvs each with only one co-stimulation domain either CD3z or 4-1BB in "AND" gate fashion. Clear differences in cytotoxic ability and cytokine production were observed. We selected 12 combination of CD33/123 CARs bi-specific CARs to evaluate in vitro efficacy, polyfunctionality, and safety. Finally, to find the best combination of CARs that would be less toxic to HSCs, we performed a Colony Forming Unit (CFU) assay with CD34+ bone marrow stem cells and found 5 bi-specific pairs that were less toxic to HSCs. Based on the CFU assay and PSI index, we were able to select the combination of CD33/123 scFvs that would target AML but minimize the killing of HSCs. [ABSTRACT FROM AUTHOR]

Published

2020

14. 294 - Immunotherapy Target Evaluation for Myeloid Diseases.

Author

Vishwasrao, Paresh, Li, Gongbo, Yu, Bin, and Davila, Marco L.

Subjects

*LEUKEMIA treatment, *IMMUNOTHERAPY, *ANTIGEN receptors, *CELLULAR therapy, *T cells

Published

2017

15. 272 - Optimization of Murine 4-1BB Signaling Results in Enhanced CD19-Targeted CAR T Cell Function in Immune Competent Mice.

Author

Li, Gongbo, Beatty, Nolan, Vishwasrao, Paresh, Yu, Bin, Park, Paul, Zhang, Yongliang, and Davila, Marco L.

Subjects

*T cells, *CANCER chemotherapy, *CD19 antigen, *GENE targeting, *CELLULAR signal transduction, *LABORATORY mice, *MATHEMATICAL optimization, *CLINICAL trials, *THERAPEUTICS

Published

2017