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1. HIV-Specific, Ex Vivo Expanded T Cell Therapy: Feasibility, Safety, and Efficacy in ART-Suppressed HIV-Infected Individuals

Author

Rooney, C.M., Patel, S., Gay, C.L., Eron, J.J., Kuruc, J.D., Sung, J.A., Hanley, P.J., Roesch, L., Margolis, D.M., Tripic, T., Archin, N., Cruz, C.R., Clohosey, M.L., Goonetilleke, N., and Bollard, C.M.

Abstract

Adoptive T cell therapy has had dramatic successes in the treatment of virus-related malignancies and infections following hematopoietic stem cell transplantation. We adapted this method to produce ex vivo expanded HIV-specific T cells (HXTCs), with the long-term goal of using HXTCs as part of strategies to clear persistent HIV infection. In this phase 1 proof-of-concept study (NCT02208167), we administered HXTCs to antiretroviral therapy (ART)-suppressed, HIV-infected participants. Participants received two infusions of 2 × 107 cells/m2 HXTCs at a 2-week interval. Leukapheresis was performed at baseline and 12 weeks post-infusion to measure the frequency of resting cell infection by the quantitative viral outgrowth assay (QVOA). Overall, participants tolerated HXTCs, with only grade 1 adverse events (AEs) related to HXTCs. Two of six participants exhibited a detectable increase in CD8 T cell-mediated antiviral activity following the two infusions in some, but not all, assays. As expected, however, in the absence of a latency reversing agent, no meaningful decline in the frequency of resting CD4 T cell infection was detected. HXTC therapy in ART-suppressed, HIV-infected individuals appears safe and well tolerated, without any clinical signs of immune activation, likely due to the low residual HIV antigen burden present during ART. Sung et al. report the infusion of ex vivo expanded HIV-specific T cells (HXTCs) in antiretroviral-suppressed, HIV-infected individuals was safe and well tolerated. No decrease of the latent HIV reservoir was detected, leaving several challenges ahead, including effective latency reversal and potentially improving in vivo expansion of infused cells.

Published
2018
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2. HIV-Specific T Cells Generated from Naive T Cells Suppress HIV In Vitro and Recognize Wide Epitope Breadths

Author

Hanley, P.J., Archin, N., Eron, J.J., Rooney, C.M., Gay, C.L., Sung, J.A., Patel, S., Roesch, L., Tripic, T., Cruz, C.R., Margolis, D.M., Kuruc, J.D., Bollard, C.M., Goonetilleke, N., and Clohosey, M.L.

Subjects
virus diseases
Abstract

The Berlin Patient represents the first and only functional HIV cure achieved by hematopoietic stem cell transplant (HSCT). In subsequent efforts to replicate this result, HIV rebounded post-HSCT after withdrawal of antiretroviral therapy. Providing HIV-specific immunity through adoptive T cell therapy may prevent HIV rebound post-HSCT by eliminating newly infected cells before they can seed systemic infection. Adoptive T cell therapy has demonstrated success in boosting Epstein-Barr virus and cytomegalovirus-specific immunity post-HSCT, controlling viral reactivation. However, T cell immunotherapies to boost HIV-specific immunity have been limited by single-epitope specificity and minimal persistence or efficacy in vivo. To improve this strategy, we sought to generate allogeneic HIV-specific T cells from human leukocyte antigen (HLA)-A02+ HIV-negative adult or cord blood donors. We focused on HLA-A02+ donors due to well-characterized epitope restrictions observed in HIV+ populations. We show that multi-antigen HIV-specific T cells can be generated from naive T cells of both cord blood and adults using a reproducible good manufacturing practice (GMP)-grade protocol. This product lysed antigen-pulsed targets and suppressed active HIV in vitro. Interestingly, these cells displayed broad epitope recognition despite lacking recognition of the common HLA-A02-restricted HIV epitope Gag SL9. This first demonstration of functional multi-antigen HIV-specific T cells has implications for improving treatment of HIV through allogeneic HSCT. Patel et al. demonstrate the ability to generate HIV-specific T cells from HIV-seronegative adults and cord blood with a good-manufacturing-practice-compliant strategy. These immunotherapies are multi-antigen specific, display cytotoxicity, and suppress HIV in vitro, providing a promising platform for adoptive T cell therapy in a post-transplant setting.

Published
2018
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3. Will Post-Transplantation Cell Therapies for Pediatric Patients Become Standard of Care?

Author

Lankester, A.C., Locatelli, F., Bader, P., Rettinger, E., Egeler, M., Katewa, S., Pulsipher, M.A., Nierkens, S., Schultz, K., Handgretinger, R., Grupp, S.A., Boelens, J.J., Bollard, C.M., and Westhafen Intercontinental Grp

Subjects
Graft Rejection, Male, medicine.medical_treatment, Adoptive cellular therapy, Cell- and Tissue-Based Therapy, Graft vs Host Disease, Hematopoietic stem cell transplantation, Disease, Pediatrics, NATURAL-KILLER-CELLS, 0302 clinical medicine, VERSUS-HOST-DISEASE, Medicine, Child, 0303 health sciences, Hematology, Graft vs Tumor Effect, adoptive cellular therapy, chimeric antigen receptor, pediatrics, stem cell transplantation, Hematopoietic Stem Cell Transplantation, Stem cell transplantation, ALLOGENEIC-DENDRITIC CELLS, Allografts, CHIMERIC ANTIGEN RECEPTOR, 3. Good health, surgical procedures, operative, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, Child, Preschool, Hematologic Neoplasms, Lymphocyte Transfusion, Female, T-REGULATORY CELLS, medicine.medical_specialty, MINOR HISTOCOMPATIBILITY ANTIGENS, Adolescent, chemical and pharmacologic phenomena, MESENCHYMAL STROMAL CELLS, ACUTE MYELOID-LEUKEMIA, Donor lymphocyte infusion, 03 medical and health sciences, Immune system, Internal medicine, Humans, Intensive care medicine, 030304 developmental biology, ACUTE LYMPHOBLASTIC-LEUKEMIA, Transplantation, business.industry, Mesenchymal stem cell, Infant, BONE-MARROW-TRANSPLANTATION, Chimeric antigen receptor, Immunology, business, 030215 immunology
Abstract

Although allogeneic hematopoietic stem cell transplantation (HSCT) is a curative approach for many pediatric patients with hematologic malignancies and some nonmalignant disorders, some critical obstacles remain to be overcome, including relapse, engraftment failure, graft-versus-host disease (GVHD), and infection. Harnessing the immune system to induce a graft-versus-tumor effect or rapidly restore antiviral immunity through the use of donor lymphocyte infusion (DLI) has been remarkably successful in some settings. Unfortunately, however, the responses to DLI can be variable, and GVHD is common. Thus, manipulations to minimize GVHD while restoring antiviral immunity and enhancing the graft-versus-tumor effect are needed to improve outcomes after allogeneic HSCT. Cellular therapies, defined as treatment modalities in which hematopoietic or nonhematopoietic cells are used as therapeutic agents, offer this promise for improving outcomes post-HSCT. This review presents an overview of the field for pediatric cell therapies in the transplant setting and discusses how we can broaden applicability beyond phase I. (C) 2015 American Society for Blood and Marrow Transplantation.

Published
2015

4. Challenges in the harmonization of immune monitoring studies and trial design for cell-based therapies in the context of hematopoietic cell transplantation for pediatric cancer patients

Author

Nierkens, S., Lankester, A.C., Egeler, R.M., Bader, P., Locatelli, F., Pulsipher, M.A., Bollard, C.M., Boelens, J.J., and Westhafen Intercontinental Grp

Subjects
Research design, Cancer Research, medicine.medical_specialty, immune monitoring, Adolescent, Pediatric cancer, medicine.medical_treatment, Immunology, Cell- and Tissue-Based Therapy, Context (language use), Hematopoietic stem cell transplantation, Monitoring, Immunologic, Neoplasms, Humans, Immunology and Allergy, Medicine, Genetics(clinical), Child, Intensive care medicine, Genetics (clinical), Clinical Trials as Topic, Transplantation, Hematopoietic cell transplantation, business.industry, Clinical study design, Hematopoietic Stem Cell Transplantation, Cell Biology, Clinical trial design, Clinical trial, Oncology, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, Research Design, Cell based therapy, business, Adjuvant, Hematopoietic cell transplantation, immune monitoring
Abstract

Clinical trials aimed at improving results of hematopoietic cell transplantation (HCT) by adjuvant cell-based interventions in children have been limited by small numbers and pediatric-specific features. The need for a larger number of pediatric HCT centers to participate in trials has resulted in a demand for harmonization of disease-specific clinical trials and immune-monitoring. Thus far, most phase I/II trials select different end points evaluated at disparate time points, making inter-study comparisons difficult and, sometimes, impossible. In this review, we discuss the various aspects that are important to consider for harmonizing clinical trial design as well as the critical elements for standardized (immune)-monitoring protocols in cell-based intervention trials in the context of HCT. Comparison data from trials applying harmonized trial design will lead to optimized immunotherapeutic treatment protocols to maximize clinical efficacy while minimizing toxicity.

Published
2015

5. Ex vivo fucosylation improves human cord blood engraftment in NOD-SCID IL-2R�� null mice

Author

Bollard, C.M., Brouard, N., Champlin, R.E., Yang, H., Shim, J.-S., Savoldo, B., Miller, L., Carlsbad, Calif, United States, Trilok, S., Thomas, M.W., Simmons, P.J., Xing, D., Zweidler-McKay, P.A., Javni, J.A., Shpall, E.J., Robinson, S.N., Decker, W.K., Shultz, L.D., Dotti, G., and Steiner, D.

Abstract

Delayed engraftment remains a major hurdle after cord blood (CB) transplantation. It may be due, at least in part, to low fucosylation of cell surface molecules important for homing to the bone marrow microenvironment. Because fucosylation of specific cell surface ligands is required before effective interaction with selectins expressed by the bone marrow microvasculature can occur, a simple 30-minute ex vivo incubation of CB hematopoietic progenitor cells with fucosyltransferase-VI and its substrate (GDP-fucose) was performed to increase levels of fucosylation. The physiologic impact of CB hematopoietic progenitor cell hypofucosylation was investigated in vivo in NOD-SCID interleukin (IL)-2R�� null (NSG) mice. By isolating fucosylated and nonfucosylated CD34 + cells from CB, we showed that only fucosylated CD34 + cells are responsible for engraftment in NSG mice. In addition, because the proportion of CD34 + cells that are fucosylated in CB is significantly less than in bone marrow and peripheral blood, we hypothesize that these combined observations might explain, at least in part, the delayed engraftment observed after CB transplantation. Because engraftment appears to be correlated with the fucosylation of CD34 + cells, we hypothesized that increasing the proportion of CD34 + cells that are fucosylated would improve CB engraftment. Ex vivo treatment with fucosyltransferase-VI significantly increases the levels of CD34 + fucosylation and, as hypothesized, this was associated with improved engraftment. Ex vivo fucosylation did not alter the biodistribution of engrafting cells or pattern of long-term, multilineage, multi-tissue engraftment. We propose that ex vivo fucosylation will similarly improve the rate and magnitude of engraftment for CB transplant recipients in a clinical setting.

Published
2012
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6. Adverse events following infusion of T cells for adoptive immunotherapy: A 10-year experience

Author

Torrano, V., Rooney, C.M., Gottschalk, S., Gee, A.P., Bollard, C.M., Heslop, H.E., Louis, C.U., Arce, J.A., Hanley, P.J., Cruz, C.R., Liu, H., Brenner, M.K., Lin, Y.-F., Leen, A.M., Dotti, G., and Savoldo, B.

Abstract

Background aims. The Food and Drug Administration (FDA) currently recommends at least 4 h of recipient monitoring after T cell infusions to detect early infusion reactions. Recent catastrophic reactions to 'first-in-man' biologic agents have emphasized the importance of this rule for initial studies of new products. The value of such monitoring for better established agents is less obvious. Methods. We reviewed infusion-related adverse events (AE) following administration of ex vivo-expanded T cell products (antigen-specific cytotoxic T lymphocytes, allodepleted T cells, and genetically modified T cells) on investigational new drug (IND) studies in our center. Results. From 1998 to 2008, we infused 381 T cell products to 180 recipients, enrolled on 18 studies, receiving T cells targeting malignancies or post-transplant viral infections. There were no grade 34 infusion reactions during initial monitoring or 24-h follow-up. Twenty-four mild (grade 12) AE occurred in 21 infusions either during or immediately following infusion (up to 6 h), most commonly nausea and vomiting (10/24, 41.6%), probably because of the dimethyl sulfoxide cryoprotectant, and hypotension (20.8%), attributable to diphenhydramine pre-medication. Twenty-two additional non-severe events were reported within 24 h of infusion, most commonly culture-negative fever, chills and nausea. An increased risk of adverse events was associated with age [incidence rate ratio (IRR) 0.98; 95% confidence interval (CI) 0.961.00, P 0.05], while an increased risk of immediate infusion-related events was higher in patients reporting allergies (IRR 2.72, 95% CI 1.007.40, P 0.05); sex, disease type and T cell source (allogeneic or autologous) had no effect on frequency of adverse events. Conclusions. Infusion of these T cell products was safe in the outpatient setting and associated with no severe reactions, so monitoring for 1 h after infusion is probably sufficient. As many of the AE were attributable to diphenhydramine premedication, a lower dose (0.25 mg/kg) should be selected.

Published
2010
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7. Repetitive noninvasive monitoring of hsvl-tk-expressing t cells intravenously infused into nonhuman primates using positron emission tomography and computed tomography with 18F-FEAU

Author

Savoldo, B., Dotti, G., Alauddin, M., Kornblau, S., Gelovani, J.G., Borne, A., Gonzalez, C., Paolillo, V., Jackson, J., Shpall, E.J., Decker, W.K., Najjar, A., Steiner, D., Tian, M., Smith, A., Mawlawi, O., Marini, F., Uthamanthil, R., Bollard, C.M., Brammer, D., and Cooper, L.J.N.

Abstract

Adoptive transfer of antigen-specific cytotoxic T lymphocytes (CTLs) has been successfully used to treat patients with different types of cancer. However, the long-term spatial-temporal dynamics of the distribution of systemically infused CTLs rlargely unknown. Noninvasive imaging of adoptively transferred CTLs using molecular-genetic reporter imaging with positron emission tomography and computed tomography (PET-CT) represents an innovative approach to understanding the long-term migratory patterns and therapeutic potential of adoptively transferred T cells. Here we report the application of repetitive PET-CT imaging with [18F]fluoro-5-ethyl-1-beta-D- arabinofuranosyluracil (18F-FEAU) in two nonhuman primates demonstrating that autologous polyclonal macaque T lymphocytes activated and transduced with a retroviral vector encoding for the sr39 mutant herpes simplex virus 1 thymidine kinase (sr39HSV1-tk) reporter gene can be detected after intravenous infusion in discrete lymphoid organs and in sites of inflammation. This study represents a proof of principle and supports the application of 18F-FEAU PET-CT imaging for monitoring the distribution of intravenously administered sr39HSV1-tk gene-transduced CTLs in humans.

Published
2009
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