Your search keyword '"Thomas A. Waldmann"' showing total 590 results

1. Germinal epimutation of Fragile Histidine Triad (FHIT) gene is associated with progression to acute and chronic adult T-cell leukemia diseases

Author

Marcia Bellon, Izabela Bialuk, Veronica Galli, Xue-Tao Bai, Lourdes Farre, Achilea Bittencourt, Ambroise Marçais, Michael N. Petrus, Lee Ratner, Thomas A. Waldmann, Vahid Asnafi, Antoine Gessain, Masao Matsuoka, Genoveffa Franchini, Olivier Hermine, Toshiki Watanabe, and Christophe Nicot

Subjects

HTLV-1, FHIT, ATL, ATLL, TSP, Leukemia, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Human T cell Leukemia virus type 1 (HTLV-I) is etiologically linked to adult T cell leukemia/lymphoma (ATL) and an inflammatory neurodegenerative disease called HTLV-I-associated myelopathy or tropical spastic paraparesis (HAM/TSP). The exact genetic or epigenetic events and/or environmental factors that influence the development of ATL, or HAM/TSP diseases are largely unknown. The tumor suppressor gene, Fragile Histidine Triad Diadenosine Triphosphatase (FHIT), is frequently lost in cancer through epigenetic modifications and/or deletion. FHIT is a tumor suppressor acting as genome caretaker by regulating cellular DNA repair. Indeed, FHIT loss leads to replicative stress and accumulation of double DNA strand breaks. Therefore, loss of FHIT expression plays a key role in cellular transformation. Methods Here, we studied over 400 samples from HTLV-I-infected individuals with ATL, TSP/HAM, or asymptomatic carriers (AC) for FHIT loss and expression. We examined the epigenetic status of FHIT through methylation specific PCR and bisulfite sequencing; and correlated these results to FHIT expression in patient samples. Results We found that epigenetic alteration of FHIT is specifically found in chronic and acute ATL but is absent in asymptomatic HTLV-I carriers and TSP/HAM patients’ samples. Furthermore, the extent of FHIT methylation in ATL patients was quantitatively comparable in virus-infected and virus non-infected cells. We also found that longitudinal HTLV-I carriers that progressed to smoldering ATL and descendants of ATL patients harbor FHIT methylation. Conclusions These results suggest that germinal epigenetic mutation of FHIT represents a preexisting mark predisposing to the development of ATL diseases. These findings have important clinical implications as patients with acute ATL are rarely cured. Our study suggests an alternative strategy to the current “wait and see approach” in that early screening of HTLV-I-infected individuals for germinal epimutation of FHIT and early treatment may offer significant clinical benefits.

Published

2021

2. Clinical trial of a humanized anti‐IL‐2/IL‐15 receptor β chain in HAM/TSP

Author

Yoshimi Enose‐Akahata, Unsong Oh, Joan Ohayon, Bridgette Jeanne Billioux, Raya Massoud, Bonita R. Bryant, Ashley Vellucci, Nyater Ngouth, Irene Cortese, Thomas A. Waldmann, and Steven Jacobson

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Objective Human T cell lymphotropic virus 1 (HTLV‐1)‐associated myelopathy/tropical spastic paraparesis (HAM/TSP) is a chronic, progressive, neurological disease. Chronic activation of CD8+ T cells, as evidenced by increased spontaneous lymphoproliferation and HTLV‐1‐specific cytotoxic T cells, has been demonstrated in HAM/TSP patients. Since IL‐2 and IL‐15 stimulate memory CD8+ T cell activity, these cytokines have been implicated in the immunopathogenesis of HAM/TSP. In this phase I trial, we evaluated the safety, pharmacokinetics, and ability of Hu‐Mikβ1, a humanized monoclonal antibody directed toward the IL‐2/IL‐15 receptor β‐chain (IL‐2/IL‐15Rβ: CD122), to saturate CD122 and regulate abnormal immune responses in patients with HAM/TSP by inhibition of IL‐15 action. Methods Hu‐Mikβ1 was administered intravenously at doses of 0.5 mg/kg, 1.0 mg/kg, or 1.5 mg/kg in a total of nine HAM/TSP patients. Five doses of Hu‐Mikβ1 were administered at 3‐week intervals. The clinical response was evaluated using standardized scales. Viral and immunologic outcome measures were examined including HTLV‐1 proviral load, T cell phenotypic analysis and spontaneous lymphoproliferation in HAM/TSP patients. Results There was no significant toxicity associated with Hu‐Mikβ1 administration in HAM/TSP patients. Saturation of CD122 by Hu‐Mikβ1 was achieved in five out of nine HAM/TSP patients. Administration of Hu‐Mikβ1 was associated with inhibition of aberrant CD8+ T cell function including spontaneous lymphoproliferation and degranulation and IFN‐γ expression, especially in HAM/TSP patients that achieved CD122 saturation. Interpretation The treatment with Hu‐Mikβ1 had a number of immunological effects on HAM/TSP patients although no clinical efficacy was observed. We also did not see any dose‐related toxicity.

Published

2019

3. First-in-human trial of rhIL-15 and haploidentical natural killer cell therapy for advanced acute myeloid leukemia

Author

Sarah Cooley, Fiona He, Veronika Bachanova, Gregory M. Vercellotti, Todd E. DeFor, Julie M. Curtsinger, Paul Robertson, Bartosz Grzywacz, Kevin C. Conlon, Thomas A. Waldmann, David H. McKenna, Bruce R. Blazar, Daniel J. Weisdorf, and Jeffrey S. Miller

Subjects

Specialties of internal medicine, RC581-951

Abstract

Abstract: In vivo expansion of haploidentical natural killer (NK) cell infusions with interleukin-2 (IL-2) can induce remission of refractory acute myeloid leukemia, but efficacy may be hampered by concurrent stimulation of host regulatory T cells. To overcome this limitation, we substituted the NK homeostatic factor IL-15 in 2 phase 1/2 trials. Forty-two patients received either intravenous (IV) (NCT01385423) or subcutaneous (SC) (NCT02395822) recombinant human IL-15 (rhIL-15) after lymphodepleting chemotherapy and haploidentical NK cells. Escalating doses of rhIL-15 (0.3-1.0 μg/kg) were given on 12 consecutive days in a phase 1 trial. Of 26 patients, 36% had robust in vivo NK-cell expansion at day 14, and 32% achieved complete remission. Hypothesizing that SC dosing of rhIL-15 would be safer and better tolerated, 16 patients received 10 once per day doses of SC rhIL-15 at 2.0 μg/kg on a phase 2 trial. NK-cell expansion at day 14 was seen in 27% of the patients, and 40% achieved remission. rhIL-15 induced better rates of in vivo NK-cell expansion and remission compared with previous trials with IL-2, but it was associated with previously unreported cytokine release syndrome (CRS) after SC but not IV dosing. CRS was observed in 56% of patients given SC rhIL-15 (with concurrent neurologic toxicity in 5 of 9 patients) and was responsive to steroids and tocilizumab. SC administration was associated with slower pharmacokinetic clearance and higher levels of IL-6 than IV dosing. These novel trials testing the use of IL-15 to potentiate cell therapy suggest that dosing schedules based on pharmacokinetics and pharmacodynamics will preserve the therapeutic benefits of IL-15 and minimize CRS. These trials were registered at www.clinicaltrials.gov as #NCT01385423 and #NCT02395822.

Published

2019

4. Immunometabolism at the Nexus of Cancer Therapeutic Efficacy and Resistance

Author

Javier Traba, Michael N. Sack, Thomas A. Waldmann, and Olga M. Anton

Subjects

immunometabolism, cancer, immune cells, T cells, NK cells, macrophages, Immunologic diseases. Allergy, RC581-607

Abstract

Constitutive activity of the immune surveillance system detects and kills cancerous cells, although many cancers have developed strategies to avoid detection and to resist their destruction. Cancer immunotherapy entails the manipulation of components of the endogenous immune system as targeted approaches to control and destroy cancer cells. Since one of the major limitations for the antitumor activity of immune cells is the immunosuppressive tumor microenvironment (TME), boosting the immune system to overcome the inhibition provided by the TME is a critical component of oncotherapeutics. In this article, we discuss the main effects of the TME on the metabolism and function of immune cells, and review emerging strategies to potentiate immune cell metabolism to promote antitumor effects either as monotherapeutics or in combination with conventional chemotherapy to optimize cancer management.

Published

2021

5. Enhanced efficacy of JAK1 inhibitor with mTORC1/C2 targeting in smoldering/chronic adult T cell leukemia

Author

Anusara Daenthanasanmak, Yuquan Lin, Meili Zhang, Bonita R. Bryant, Michael N. Petrus, Richard N. Bamford, Craig J. Thomas, Milos D. Miljkovic, Kevin C. Conlon, and Thomas A. Waldmann

Subjects

Adult T cell leukemia, JAK1 inhibitors, mTOR inhibitors, Combination therapy, Smoldering/chronic ATL, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Adult T-cell leukemia (ATL) is an aggressive T-cell lymphoproliferative malignancy of regulatory T lymphocytes (Tregs), caused by human T-cell lymphotropic virus 1 (HTLV-1). Interleukin 2 receptor alpha (IL-2Rα) is expressed in the leukemic cells of smoldering/chronic ATL patients, leading to constitutive activation of the JAK/STAT pathway and spontaneous proliferation. The PI3K/AKT/mTOR pathway also plays a critical role in ATL cell survival and proliferation. We previously performed a high-throughput screen that demonstrated additive/synergistic activity of Ruxolitinib, a JAK1/2 inhibitor, with AZD8055, an mTORC1/C2 inhibitor. However, effects of unintended JAK2 inhibition with Ruxolitinib limits it therapeutic potential for ATL patients, which lead us to evaluate a JAK1-specific inhibitor. Here, we demonstrated that Upadacitinib, a JAK-1 inhibitor, inhibited the proliferation of cytokine-dependent ATL cell lines and the expression of p-STAT5. Combinations of Upadacitinib with either AZD8055 or Sapanisertib, mTORC1/C2 inhibitors, showed anti-proliferative effects against cytokine-dependent ATL cell lines and synergistic effect with reducing tumor growth in NSG mice bearing IL-2 transgenic tumors. Importantly, the combination of these two agents inhibited ex vivo spontaneous proliferation of ATL cells from patients with smoldering/chronic ATL. Combined targeting of JAK/STAT and PI3K/AKT/mTOR pathways represents a promising therapeutic intervention for patients with smoldering/chronic ATL.

Published

2021

6. Interleukin 15 Pharmacokinetics and Consumption by a Dynamic Cytokine Sink

Author

John A. Hangasky, Thomas A. Waldmann, and Daniel V. Santi

Subjects

cytokine, immuno-oncology, NK cells, CD8+ T cells, target-mediated drug disposition, interleukin-15, Immunologic diseases. Allergy, RC581-607

Abstract

Interleukin-15 (IL-15) is crucial for the proliferation and survival of NK and CD8+ T memory cells, and of significant interest in immuno-oncology. Immune cell expansion requires continuous IL-15 exposure above a threshold concentration for an extended period. However, the short t1/2 of IL-15 makes this impossible to achieve after a single injection without a high Cmax and toxicities. The most effective way to deliver IL-15 is continuous intra-venous infusion, but this administration mode is impractical. Efforts have been devoted to developing IL-15 agonists which after a single injection maintain the cytokine in a narrow therapeutic window for a long period. Enigmatically, although the half-life extension technologies used often extend the half-life of a protein to 1 or more weeks, the modified IL-15 agonists studied usually have systemic elimination half-lives of only a few hours and rarely much longer than 1 day. These short half-lives—common to all circulating IL-15 agonists thus far reported—can be explained by a dynamic increase in clearance of the agonists that accompanies target immune cell proliferation. What is needed is an IL-15 agonist that is as effective as continuous intravenous infusion, but with the convenience and acceptance of single injections at 1-week or longer intervals.

Published

2020

7. IL-15 in the Combination Immunotherapy of Cancer

Author

Thomas A. Waldmann, Sigrid Dubois, Milos D. Miljkovic, and Kevin C. Conlon

Subjects

interleukin-15, natural killer cells, CD8 T cells, immunotherapy of cancer, immunological checkpoints, Immunologic diseases. Allergy, RC581-607

Abstract

We completed clinical trials of rhIL-15 by bolus, subcutaneous, and continuous intravenous infusions (CIV). IL-15 administered by CIV at 2 mcg/kg/day yielded a 38-fold increase in 10- day number of circulating NK cells, a 358-fold increase in CD56bright NK cells and a 5.8-fold increase in CD8 T cells. However, IL-15 preparations administered as monotherapy were ineffective, due to actions of immunological checkpoints and due to the lack of tumor specific targeting by NK cells. To circumvent checkpoints, trials of IL-15 in combination with other anticancer agents were initiated. Tumor-bearing mice receiving IL-15 with antibodies to CTLA-4 and PD-L1 manifested marked prolongation of survival compared to mice receiving IL-15 with either agent alone. In translation, a phase I trial was initiated involving IL-15 (rhIL-15), nivolumab and ipilimumab in patients with malignancy (NCT03388632). In rhesus macaques CIV IL-15 at 20 μg/kg/day for 10 days led to an 80-fold increase in number of circulating effector memory CD8 T cells. However, administration of γc cytokines such as IL-15 led to paralysis/depression of CD4 T-cells that was mediated through transient expression of SOCS3 that inhibited the STAT5 signaling pathway. This lost CD4 helper role could be restored alternatively by CD40 agonists. In the TRAMP-C2 prostate tumor model the combination of IL-15 with agonistic anti-CD40 produced additive effects in terms of numbers of TRAMP-C2 tumor specific Spas/SCNC/9H tetramer positive CD8 T cells expressed and tumor responses. A clinical trial is being initiated for patients with cancer using an intralesional anti-CD40 in combination with CIV rhIL-15. To translate IL-15-mediated increases in NK cells, we investigated combination therapy of IL-15 with anticancer monoclonal antibodies including rituximab in mouse models of EL-4 lymphoma transfected with human CD20 and with alemtuzumab (CAMPATH-1H) in a xenograft model of adult T cell leukemia (ATL). IL-15 enhanced the ADCC and therapeutic efficacy of both antibodies. These results provided the scientific basis for trials of IL-15 combined with alemtuzumab (anti-CD52) for patients with ATL (NCT02689453), with obinutuzumab (anti-CD20) for patients with CLL (NCT03759184), and with avelumab (anti-PD-L1) in patients with T-cell lymphoma (NCT03905135) and renal cancer (NCT04150562). In the first trial, there was elimination of circulating ATL and CLL leukemic cells in select patients.

Published

2020

8. Making discoveries in immunology

Author

Thomas A. Waldmann

Subjects

Immunologic diseases. Allergy, RC581-607, Therapeutics. Pharmacology, RM1-950

Published

2019

9. Detection of Lymph Node Involvement in Hematologic Malignancies Using Micromagnetic Resonance Lymphangiography with a Gadolinum-Labeled Dendrimer Nanoparticle

Author

Hisataka Kobayashi, Satomi Kawamoto, Martin W. Brechbiel, Marcelino Bernardo, Noriko Sato, Thomas A. Waldmann, Yutaka Tagaya, and Peter L. Choyke

Subjects

Malignant lymphoma, MRI, lymph node, lymphatic flow, nanoparticle, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Animal models of lymphoma should reflect their counterparts in humans; however, it can be difficult to ascertain whether an induced disease is intralymphatic or extralymphatic based on direct visualization. Current imaging methods are insufficient for identifying lymphatic and intralymphatic involvement. To differentiate intralymphatic from extralymphatic involvement, we have developed a magnetic resonance imaging-based lymphangiography method and tested it on two animal models of lymphoma. A gadolinium (Gd)-labeled dendrimer nanoparticle (generation-6; ~220 kDa/f10 nm) was injected interstitially into mice bearing hematologic malignancies to perform dynamic micromagnetic resonance lymphangiography (micro-MRL). Both a standard T1-weighted 3D fast spoiled gradient echo and a T2/T1-weighted 3D fast imaging employing steady-state acquisition (3D-FIESTA-C) were compared in an imaging study to differentiate intralymphatic from extralymphatic involvement of tumors. The lymphatics and lymph nodes were visualized with both methods in all cases. In addition, 3D-FIESTA-C depicted both the lymphatic system and the extralymphatic tumor. In an animal model, 3D-FIESTA-C demonstrated that the bulk of the tumor thought to be intralymphatic was actually extralymphatic. In conclusion, micro-MRL, using Gd-labeled dendrimer nanoparticles with the combined method, can define both the normal and abnormal lymphatics and can distinguish intralymphatic from extralymphatic diseases in mouse models of malignant lymphoma.

Published

2005

10. Interleukin-15 augments NK cell–mediated ADCC of alemtuzumab in patients with CD52+ T-cell malignancies

Author

Milos D. Miljkovic, Sigrid P. Dubois, Jürgen R. Müller, Bonita Bryant, Elaine Ma, Kevin C. Conlon, and Thomas A. Waldmann

Subjects

Hematology

Abstract

Interleukin-15 (IL-15) monotherapy substantially increases the number and activity of natural killer (NK) cells and CD8+ T cells but has not produced clinical responses. In a xenograft mouse model, IL-15 enhanced the NK cell–mediated antibody-dependent cell cytotoxicity (ADCC) of the anti-CD52 antibody alemtuzumab and led to significantly more durable responses than alemtuzumab alone. To evaluate whether IL-15 potentiates ADCC in humans, we conducted a phase 1 single-center study of recombinant human IL-15 and alemtuzumab in patients with CD52-positive mature T-cell malignances. We gave IL-15 subcutaneously 5 days per week for 2 weeks in a 3 + 3 dose escalation scheme (at 0.5, 1, and 2 μg/kg), followed by standard 3 times weekly alemtuzumab IV for 4 weeks. There were no dose-limiting toxicities or severe adverse events attributable to IL-15 in the 11 patients treated. The most common adverse events were lymphopenia (100%), alemtuzumab-related infusion reactions (90%), anemia (90%), and neutropenia (72%). There were 3 partial and 2 complete responses, with an overall response rate of 45% and median duration of response 6 months. Immediately after 10 days of IL-15, there was a median 7.2-fold increase in NK cells and 2.5-fold increase in circulating CD8+ T cells, whereas the number of circulating leukemic cells decreased by a median 38% across all dose levels. Treatment with IL-15 was associated with increased expression of NKp46 and NKG2D, markers of NK-cell activation, and increased ex vivo ADCC activity of NK cells, whereas inhibitory receptors PD1 and Tim3 were decreased. This trial was registered at www.clinicaltrials.gov as #NCT02689453.

Published

2023

11. Genome-wide CRISPR screens identify CD48 defining susceptibility to NK cytotoxicity in peripheral T-cell lymphomas

Author

Masahiro Chiba, Joji Shimono, Takashi Ishio, Norio Takei, Kohei Kasahara, Reiki Ogasawara, Takahide Ara, Hideki Goto, Koh Izumiyama, Satoko Otsuguro, Liyanage P. Perera, Hiroo Hasegawa, Michiyuki Maeda, Satoshi Hashino, Katsumi Maenaka, Takanori Teshima, Thomas A. Waldmann, Yibin Yang, and Masao Nakagawa

Subjects

Adult, Killer Cells, Natural, Immunology, Humans, Leukemia-Lymphoma, Adult T-Cell, Lymphoma, T-Cell, Peripheral, Clustered Regularly Interspaced Short Palindromic Repeats, Cell Biology, Hematology, CD48 Antigen, Biochemistry

Abstract

Adult T-cell leukemia/lymphoma (ATLL) is one of the aggressive peripheral T-cell neoplasms with a poor prognosis. Accumulating evidence demonstrates that escape from adaptive immunity is a hallmark of ATLL pathogenesis. However, the mechanisms by which ATLL cells evade natural killer (NK)-cell–mediated immunity have been poorly understood. Here we show that CD48 expression in ATLL cells determines the sensitivity for NK-cell–mediated cytotoxicity against ATLL cells. We performed unbiased genome-wide clustered regularly interspaced short palindromic repeat (CRISPR) screening using 2 ATLL-derived cell lines and discovered CD48 as one of the best-enriched genes whose knockout conferred resistance to YT1–NK cell line-mediated cytotoxicity. The ability of CD48-knockout ATLL cells to evade NK-cell effector function was confirmed using human primary NK cells with reduced interferon-γ (IFNγ) induction and degranulation. We found that primary ATLL cells had reduced CD48 expression along with disease progression. Furthermore, other subgroups among aggressive peripheral T-cell lymphomas (PTCLs) also expressed lower concentrations of CD48 than normal T cells, suggesting that CD48 is a key molecule in malignant T-cell evasion of NK-cell surveillance. Thus, this study demonstrates that CD48 expression is likely critical for malignant T-cell lymphoma cell regulation of NK-cell–mediated immunity and provides a rationale for future evaluation of CD48 as a molecular biomarker in NK-cell–associated immunotherapies.

Published

2022

12. Accessory cells precondition naïve T cells and regulatory T cells for cytokine-mediated proliferation

Author

Noriko Sato, Richard N. Bamford, Bonita R. Bryant, Yutaka Tagaya, and Thomas A. Waldmann

Subjects

Multidisciplinary

Abstract

Naïve T cells and regulatory T cells, when purified, do not proliferate to the γ c -cytokines IL-2, IL-7, or IL-15, despite their expression of cognate cytokine receptors. Dendritic cells (DCs) enabled the T cell proliferation to these cytokines, through cell-to-cell contact, but independent of T cell receptor stimulation. This effect lasted after separation of T cells from DCs, enabling enhanced proliferation of the T cells in DC-depleted hosts. We propose calling this a “preconditioning effect”. Interestingly, IL-2 alone was sufficient to induce phosphorylation and nuclear translocation of STAT5 in T cells, but could not activate MAPK and AKT pathways and failed to induce transcription of IL-2 target genes. “Preconditioning” was necessary to activate these two pathways and induced weak Ca 2+ mobilization independent of calcium release-activated channels. When preconditioning was combined with IL-2, full activation of downstream mTOR, 4E-BP1 hyperphosphorylation, and prolonged S6 phosphorylation occurred. Collectively, accessory cells provide T cell preconditioning, a unique activation mechanism, controlling cytokine-mediated proliferation of T cells.

Published

2023

13. Data from IL15 Infusion of Cancer Patients Expands the Subpopulation of Cytotoxic CD56bright NK Cells and Increases NK-Cell Cytokine Release Capabilities

Author

Thomas A. Waldmann, Bonita R. Bryant, Nancy Beltran, Jennifer Hsu-Albert, Jürgen R. Müller, Kevin C. Conlon, and Sigrid Dubois

Abstract

The cytokine IL15 is required for survival and activation of natural killer (NK) cells as well as expansion of NK-cell populations. Here, we compare the effects of continuous IL15 infusions on NK-cell subpopulations in cancer patients. Infusions affected the CD56bright NK-cell subpopulation in that the expansion rates exceeded those of CD56dim NK-cell populations with a 350-fold increase in their total cell numbers compared with 20-fold expansion for the CD56dim subset. CD56bright NK cells responded with increased cytokine release to various stimuli, as expected given their immunoregulatory functions. Moreover, CD56bright NK cells gained the ability to kill various target cells at levels that are typical for CD56dim NK cells. Some increased cytotoxic activities were also observed for CD56dim NK cells. IL15 infusions induced expression changes on the surface of both NK-cell subsets, resulting in a previously undescribed and similar phenotype. These data suggest that IL15 infusions expand and arm CD56bright NK cells that alone or in combination with tumor-targeting antibodies may be useful in the treatment of cancer. Cancer Immunol Res; 5(10); 929–38. ©2017 AACR.

Published

2023

14. Figure S2 from IL15 Infusion of Cancer Patients Expands the Subpopulation of Cytotoxic CD56bright NK Cells and Increases NK-Cell Cytokine Release Capabilities

Author

Thomas A. Waldmann, Bonita R. Bryant, Nancy Beltran, Jennifer Hsu-Albert, Jürgen R. Müller, Kevin C. Conlon, and Sigrid Dubois

Abstract

Representation of surface marker analyses on gated NK cells with constant expressions before and after IL-15 infusions.

Published

2023

15. Data from EGR1 Addiction in Diffuse Large B-cell Lymphoma

Author

Lixin Rui, Christian M. Capitini, Thomas A. Waldmann, Madelyn Chen, Samantha Bebel, Apoorv Kondapelli, Alexander Rosiejka, Yangguang Li, Yunxia Liu, Amanda Kelm, David T. Yang, Shanxiang Zhang, Anusara Daenthanasanmak, Paul D. Bates, Fen Zhu, Nguyet M. Hoang, Li Lu, and Shuichi Kimpara

Abstract

Early growth response gene (EGR1) is a transcription factor known to be a downstream effector of B-cell receptor signaling and Janus kinase 1 (JAK1) signaling in diffuse large B-cell lymphoma (DLBCL). While EGR1 is characterized as a tumor suppressor in leukemia and multiple myeloma, the role of EGR1 in lymphoma is unknown. Here we demonstrate that EGR1 is a potential oncogene that promotes cell proliferation in DLBCL. IHC analysis revealed that EGR1 expression is elevated in DLBCL compared with normal lymphoid tissues and the level of EGR1 expression is higher in activated B cell–like subtype (ABC) than germinal center B cell–like subtype (GCB). EGR1 expression is required for the survival and proliferation of DLBCL cells. Genomic analyses demonstrated that EGR1 upregulates expression of MYC and E2F pathway genes through the CBP/p300/H3K27ac/BRD4 axis while repressing expression of the type I IFN pathway genes by interaction with the corepressor NAB2. Genetic and pharmacologic inhibition of EGR1 synergizes with the BRD4 inhibitor JQ1 or the type I IFN inducer lenalidomide in growth inhibition of ABC DLBCL both in cell cultures and xenograft mouse models. Therefore, targeting oncogenic EGR1 signaling represents a potential new targeted therapeutic strategy in DLBCL, especially for the more aggressive ABC DLBCL.Implications:The study characterizes EGR1 as a potential oncogene that promotes cell proliferation and defines EGR1 as a new molecular target in DLBCL, the most common non-Hodgkin lymphoma.

Published

2023

16. Supplementary Table 1 from EGR1 Addiction in Diffuse Large B-cell Lymphoma

Author

Lixin Rui, Christian M. Capitini, Thomas A. Waldmann, Madelyn Chen, Samantha Bebel, Apoorv Kondapelli, Alexander Rosiejka, Yangguang Li, Yunxia Liu, Amanda Kelm, David T. Yang, Shanxiang Zhang, Anusara Daenthanasanmak, Paul D. Bates, Fen Zhu, Nguyet M. Hoang, Li Lu, and Shuichi Kimpara

Abstract

Supplementary Table S1 including analyzed RNA-seq and ChIP-seq data

Published

2023

17. Table S1 from IL15 Infusion of Cancer Patients Expands the Subpopulation of Cytotoxic CD56bright NK Cells and Increases NK-Cell Cytokine Release Capabilities

Author

Thomas A. Waldmann, Bonita R. Bryant, Nancy Beltran, Jennifer Hsu-Albert, Jürgen R. Müller, Kevin C. Conlon, and Sigrid Dubois

Abstract

antibody table

Published

2023

18. Kaplan-Meier analysis of the survival for patients with ATL who responded to alemtuzumab therapy from Phase II Study of Alemtuzumab (CAMPATH-1) in Patients with HTLV-1–Associated Adult T-cell Leukemia/lymphoma

Author

John C. Morris, Thomas A. Waldmann, Seth M. Steinberg, Cathryn C. Lee, Thomas A. Fleisher, Mark Raffeld, Elaine S. Jaffe, Maryalice Stetler-Stevenson, Stefania Pittaluga, Donn Stewart, Deirdre O'Mahony, John E. Janik, and Kamal Sharma

Abstract

Kaplan-Meier analysis of the survival for patients with ATL who responded to alemtuzumab therapy

Published

2023

19. Translation on this Article from EBV-Related Lymphoproliferative Disease Complicating Therapy with the Anti-CD2 Monoclonal Antibody, Siplizumab, in Patients with T-Cell Malignancies

Author

John E. Janik, Thomas A. Waldmann, Luz Hammershaimb, Karen Kaucic, Dirk Reitsma, Paul S. Albert, Mark Raffeld, Stefania Pittaluga, Thomas Fleisher, Margaret R. Brown, Helen Matthews, Maryalice Stetler-Stevenson, John C. Morris, and Deirdre O'Mahony

Abstract

Translation on this Article from EBV-Related Lymphoproliferative Disease Complicating Therapy with the Anti-CD2 Monoclonal Antibody, Siplizumab, in Patients with T-Cell Malignancies

Published

2023

20. CCR Translation for This Article from Simultaneous Blockade of Multiple Immune System Inhibitory Checkpoints Enhances Antitumor Activity Mediated by Interleukin-15 in a Murine Metastatic Colon Carcinoma Model

Author

Thomas A. Waldmann, John C. Morris, Meili Zhang, Jason C. Steel, and Ping Yu

Abstract

CCR Translation for This Article from Simultaneous Blockade of Multiple Immune System Inhibitory Checkpoints Enhances Antitumor Activity Mediated by Interleukin-15 in a Murine Metastatic Colon Carcinoma Model

Published

2023

21. Data from A20 and RBX1 Regulate Brentuximab Vedotin Sensitivity in Hodgkin Lymphoma Models

Author

Yibin Yang, Thomas A. Waldmann, Michael Petrus, Stefan K. Barta, Yan Zhou, Jiejing Yin, Liqi Chen, Wenming Xiao, Zhihui Song, Yuquan Lin, and Wei Wei

Abstract

Purpose:For patients with refractory/relapsed Hodgkin lymphoma (roughly 20% of total cases), few effective therapeutic options exist. Currently, brentuximab vedotin (BV), a drug-conjugated anti-CD30 antibody, is one of the most effective approved therapy agents for these patients. However, many patients do not achieve complete remission and ultimately develop BV-resistant disease, necessitating a more detailed understanding of the molecular circuitry that drives BV sensitivity and the mechanism of BV resistance.Experimental Design:Here, we established a ubiquitin regulator–focused CRISPR library screening platform in Hodgkin lymphoma and carried out a drug sensitization screen against BV to identify genes regulating BV treatment sensitivity.Results:Our CRISPR library screens revealed the ubiquitin-editing enzymes A20 and RBX1 as key molecule effectors that regulate BV sensitivity in Hodgkin lymphoma line L428. A20 negatively regulates NF-κB activity which is required to prevent BV cytotoxicity. In line with these results, the RNA-seq analysis of the BV-resistant single-cell clones demonstrated a consistent upregulation of NF-κB signature genes, as well as the ABC transporter gene ABCB1. Mechanically, NF-κB regulates BV treatment sensitivity through mediating ABCB1 expression. Targeting NF-κB activity synergized well with BV in killing Hodgkin lymphoma cell lines, augmented BV sensitivity, and overcame BV resistance in vitro and in Hodgkin lymphoma xenograft mouse models.Conclusions:Our identification of this previously unrecognized mechanism provides novel knowledge of possible BV responsiveness and resistance mechanisms in Hodgkin lymphoma, as well as leads to promising hypotheses for the development of therapeutic strategies to overcome BV resistance in this disease.

Published

2023

22. Data from EBV-Related Lymphoproliferative Disease Complicating Therapy with the Anti-CD2 Monoclonal Antibody, Siplizumab, in Patients with T-Cell Malignancies

Author

John E. Janik, Thomas A. Waldmann, Luz Hammershaimb, Karen Kaucic, Dirk Reitsma, Paul S. Albert, Mark Raffeld, Stefania Pittaluga, Thomas Fleisher, Margaret R. Brown, Helen Matthews, Maryalice Stetler-Stevenson, John C. Morris, and Deirdre O'Mahony

Abstract

Purpose: We report an increased incidence of EBV-induced B-cell lymphoproliferative disease (LPD) in patients treated with siplizumab, an anti-CD2 antibody. The development of EBV-LPD has been associated with the use of immunosuppressive agents used in solid organ, bone marrow, and stem cell transplantation and in certain congenital immunodeficiencies.Experimental Design: We conducted a single-institution phase I dose-escalation trial of siplizumab, a humanized monoclonal antibody to CD2, in 29 patients with T-cell malignancies.Results: Although initial responses were encouraging, 4 (13.7%) patients developed EBV-LPD and the trial was stopped. Reductions in CD4+ and CD8+ cell count numbers in response to therapy were seen in all patients, but in those patients developing EBV-LPD a significantly greater reduction in natural killer (NK) cell number and CD2 expression on T cells was seen. These findings highlight the importance of NK-cell depletion and CD2 expression in addition to T-cell depletion in the etiology of EBV-LPD.Conclusions: The emergence of EBV-LPD may be associated with the ability of siplizumab to deplete both T and NK cells without affecting B cells. Agents that deplete T- and NK-cell populations without affecting B cell number should be screened for this potentially serious adverse event.

Published

2023

23. Supplementary Figure from IL15 and Anti–PD-1 Augment the Efficacy of Agonistic Intratumoral Anti-CD40 in a Mouse Model with Multiple TRAMP-C2 Tumors

Author

Thomas A. Waldmann, Elijah F. Edmondson, Richard N. Bamford, and Wei Chen

Abstract

Supplementary Figure from IL15 and Anti–PD-1 Augment the Efficacy of Agonistic Intratumoral Anti-CD40 in a Mouse Model with Multiple TRAMP-C2 Tumors

Published

2023

24. Supplementary Table S3 from IL15 by Continuous Intravenous Infusion to Adult Patients with Solid Tumors in a Phase I Trial Induced Dramatic NK-Cell Subset Expansion

Author

Thomas A. Waldmann, Mario Roederer, Stephen P. Creekmore, Jason L. Yovandich, Joanna H. Shih, Cody J. Peer, William D. Figg, Jennifer Hsu, Liyanage P. Perera, Michael Petrus, Bonita R. Bryant, Sigrid Dubois, Thomas A. Fleisher, Milos D. Miljkovic, Chyi-Chia Richard Lee, Stefania Pittaluga, E. Lake Potter, and Kevin C. Conlon

Abstract

Supplementary Table S3

Published

2023

25. Figure S2 from IL15 by Continuous Intravenous Infusion to Adult Patients with Solid Tumors in a Phase I Trial Induced Dramatic NK-Cell Subset Expansion

Author

Thomas A. Waldmann, Mario Roederer, Stephen P. Creekmore, Jason L. Yovandich, Joanna H. Shih, Cody J. Peer, William D. Figg, Jennifer Hsu, Liyanage P. Perera, Michael Petrus, Bonita R. Bryant, Sigrid Dubois, Thomas A. Fleisher, Milos D. Miljkovic, Chyi-Chia Richard Lee, Stefania Pittaluga, E. Lake Potter, and Kevin C. Conlon

Abstract

Supplementary Figure S2

Published

2023

26. Data from Simultaneous Blockade of Multiple Immune System Inhibitory Checkpoints Enhances Antitumor Activity Mediated by Interleukin-15 in a Murine Metastatic Colon Carcinoma Model

Author

Thomas A. Waldmann, John C. Morris, Meili Zhang, Jason C. Steel, and Ping Yu

Abstract

Purpose: Interleukin 15 (IL-15) is a promising cytokine for immunotherapy of cancer due to its ability to stimulate the immunity of natural killer, B, and T cells. Its effectiveness, however, may be limited by inhibitory checkpoints and pathways that can attenuate immune responses. Finding strategies to abrogate these negative regulators and enhance the efficacy of IL-15 is a critical challenge.Experimental Design: In a preclinical study, we evaluated IL-15 combined with antibodies to block the negative immune regulators cytotoxic T-lymphocyte antigen 4 (CTLA-4) and programmed death ligand 1 (PD-L1) in a metastatic murine CT26 colon carcinoma model.Results: IL-15 treatment resulted in a significant prolongation of survival in mice with metastatic tumor. Administration of IL-15, however, also increased expression of PD-1 on the surface of CD8+ T cells including CD8+CD44high memory phenotype T cells. Moreover, IL-15 also increased the secretion of the immunosuppressive cytokine, IL-10. Combining IL-15 with anti-PD-L1 and anti-CTLA-4 (multiple immune checkpoint blockade) exhibited greater CTL killing and IFNγ secretion. Moreover, this combination resulted in a significant reduction in surface expression of PD-1 on CD8+ T cells, a decrease in IL-10 secretion, and led to significantly longer survival of tumor-bearing animals compared with mice treated with IL-15 alone or combined singularly with anti-PD-L1 or anti-CTLA-4.Conclusions: Combining the immune stimulatory properties of IL-15 with the simultaneous removal of 2 critical immune system inhibitory checkpoints, we showed enhancement of immune responses leading to increased antitumor activity. Clin Cancer Res; 16(24); 6019–28. ©2010 AACR.

Published

2023

27. Supplementary information from A20 and RBX1 Regulate Brentuximab Vedotin Sensitivity in Hodgkin Lymphoma Models

Author

Yibin Yang, Thomas A. Waldmann, Michael Petrus, Stefan K. Barta, Yan Zhou, Jiejing Yin, Liqi Chen, Wenming Xiao, Zhihui Song, Yuquan Lin, and Wei Wei

Abstract

Supplementary Information. Including Supplemental Experimental Procedures, and Supplementary Figure 1-6.

Published

2023

28. Data from IL15 and Anti–PD-1 Augment the Efficacy of Agonistic Intratumoral Anti-CD40 in a Mouse Model with Multiple TRAMP-C2 Tumors

Author

Thomas A. Waldmann, Elijah F. Edmondson, Richard N. Bamford, and Wei Chen

Abstract

Purpose:IL15 promotes activation and maintenance of natural killer (NK) and CD8+ T effector memory cells making it a potential immunotherapeutic agent for the treatment of cancer. However, monotherapy with IL15 was ineffective in patients with cancer, indicating that it would have to be used in combination with other anticancer agents. The administration of high doses of common gamma chain cytokines, such as IL15, is associated with the generation of “helpless” antigen-nonspecific CD8 T cells. The generation of the tumor-specific cytotoxic T cells can be mediated by CD40 signaling via agonistic anti-CD40 antibodies. Nevertheless, parenteral administration of anti-CD40 antibodies is associated with unacceptable side effects, such as thrombocytopenia and hepatic toxicity, which can be avoided by intratumoral administration.Experimental Design:We investigated the combination of IL15 with an intratumoral anti-CD40 monoclonal antibody (mAb) in a dual tumor TRAMP-C2 murine prostate cancer model and expanded the regimen to include an anti–PD-1 mAb.Results:Here we demonstrated that anti-CD40 given intratumorally not only showed significant antitumor activity in treated tumors, but also noninjected contralateral tumors, indicative of abscopal efficacy. The combination of IL15 with intratumoral anti-CD40 showed an additive immune response with an increase in the number of tumor-specific tetramer-positive CD8 T cells. Furthermore, the addition of anti–PD-1 further improved efficacy mediated by the anti-CD40/IL15 combination.Conclusions:These studies support the initiation of a clinical trial in patients with cancer using IL15 in association with the checkpoint inhibitor, anti–PD-1, and intratumoral optimized anti-CD40.

Published

2023

29. Supplementary Tables S1-S3 from EBV-Related Lymphoproliferative Disease Complicating Therapy with the Anti-CD2 Monoclonal Antibody, Siplizumab, in Patients with T-Cell Malignancies

Author

John E. Janik, Thomas A. Waldmann, Luz Hammershaimb, Karen Kaucic, Dirk Reitsma, Paul S. Albert, Mark Raffeld, Stefania Pittaluga, Thomas Fleisher, Margaret R. Brown, Helen Matthews, Maryalice Stetler-Stevenson, John C. Morris, and Deirdre O'Mahony

Abstract

Supplementary Tables S1-S3 from EBV-Related Lymphoproliferative Disease Complicating Therapy with the Anti-CD2 Monoclonal Antibody, Siplizumab, in Patients with T-Cell Malignancies

Published

2023

30. Data from Phase II Study of Alemtuzumab (CAMPATH-1) in Patients with HTLV-1–Associated Adult T-cell Leukemia/lymphoma

Author

John C. Morris, Thomas A. Waldmann, Seth M. Steinberg, Cathryn C. Lee, Thomas A. Fleisher, Mark Raffeld, Elaine S. Jaffe, Maryalice Stetler-Stevenson, Stefania Pittaluga, Donn Stewart, Deirdre O'Mahony, John E. Janik, and Kamal Sharma

Abstract

Purpose: Therapeutic regimens for adult T-cell leukemia/lymphoma (ATL) are limited with unsatisfactory results, thereby warranting development of novel therapies. This study investigated antitumor activity and toxicity of alemtuzumab with regard to response, duration of response, progression-free survival, and overall survival in patients with human T-cell lymphotropic virus-1 (HTLV-1)-associated ATL.Experimental Design: Twenty-nine patients with chronic, acute, and lymphomatous types of ATL were enrolled in a single-institution, nonrandomized, open-label phase II trial wherein patients received intravenous alemtuzumab 30 mg three times weekly for a maximum of 12 weeks.Results: Twenty-nine patients were evaluable for response and toxicity. The overall objective response was 15 of 29 patients [95% confidence interval (CI), 32.5%–70.6%]. The 15 patients who responded manifested a median time to response of 1.1 months. Median response duration was 1.4 months for the whole group and 14.5 months among responders. Median progression-free survival was 2.0 months. Median overall survival was 5.9 months. The most common adverse events were 2 with vasovagal episodes (7%) and 3 with hypotensive episodes (10%), leukopenia (41%) grade 3 and (17%) grade 4, lymphocytopenia (59%) grade 3, neutropenia (31%) grade 3, anemia (24%), and thrombocytopenia (10%). All patients developed cytomegalovirus antigenemia (CMV). Three were symptomatic and all responded to antiviral therapy. Grade 3 or 4 infections were reported in 4 (14%) of patients.Conclusions: Alemtuzumab induced responses in patients with acute HTLV-1–associated ATL with acceptable toxicity, but with short duration of responses. These studies support inclusion of alemtuzumab in novel multidrug therapies for ATL. Clin Cancer Res; 23(1); 35–42. ©2016 AACR.

Published

2023

31. Supplementary Data from IL15 by Continuous Intravenous Infusion to Adult Patients with Solid Tumors in a Phase I Trial Induced Dramatic NK-Cell Subset Expansion

Author

Thomas A. Waldmann, Mario Roederer, Stephen P. Creekmore, Jason L. Yovandich, Joanna H. Shih, Cody J. Peer, William D. Figg, Jennifer Hsu, Liyanage P. Perera, Michael Petrus, Bonita R. Bryant, Sigrid Dubois, Thomas A. Fleisher, Milos D. Miljkovic, Chyi-Chia Richard Lee, Stefania Pittaluga, E. Lake Potter, and Kevin C. Conlon

Abstract

Supplementary Data (Tracking)

Published

2023

32. Kaplan-Meier analysis of progression free survival of all patients with ATL who received alemtuzumab therapy from Phase II Study of Alemtuzumab (CAMPATH-1) in Patients with HTLV-1–Associated Adult T-cell Leukemia/lymphoma

Author

John C. Morris, Thomas A. Waldmann, Seth M. Steinberg, Cathryn C. Lee, Thomas A. Fleisher, Mark Raffeld, Elaine S. Jaffe, Maryalice Stetler-Stevenson, Stefania Pittaluga, Donn Stewart, Deirdre O'Mahony, John E. Janik, and Kamal Sharma

Abstract

Kaplan-Meier analysis of progression free survival of all patients with ATL who received alemtuzumab therapy

Published

2023

33. Data from IL15 by Continuous Intravenous Infusion to Adult Patients with Solid Tumors in a Phase I Trial Induced Dramatic NK-Cell Subset Expansion

Author

Thomas A. Waldmann, Mario Roederer, Stephen P. Creekmore, Jason L. Yovandich, Joanna H. Shih, Cody J. Peer, William D. Figg, Jennifer Hsu, Liyanage P. Perera, Michael Petrus, Bonita R. Bryant, Sigrid Dubois, Thomas A. Fleisher, Milos D. Miljkovic, Chyi-Chia Richard Lee, Stefania Pittaluga, E. Lake Potter, and Kevin C. Conlon

Abstract

Purpose:The first-in-human clinical trial with human bolus intravenous infusion IL15 (rhIL15) was limited by treatment-associated toxicity. Here, we report toxicity, immunomodulation, and clinical activity of rhIL15 administered as a 10-day continuous intravenous infusion (CIV) to patients with cancers in a phase I trial.Patients and Methods:Patients received treatment for 10 days with CIV rhIL15 in doses of 0.125, 0.25, 0.5, 1, 2, or 4 μg/kg/day. Correlative laboratory tests included IL15 pharmacokinetic (PK) analyses, and assessment of changes in lymphocyte subset numbers.Results:Twenty-seven patients were treated with rhIL15; 2 μg/kg/day was identified as the MTD. There were eight serious adverse events including two bleeding events, papilledema, uveitis, pneumonitis, duodenal erosions, and two deaths (one due to likely drug-related gastrointestinal ischemia). Evidence of antitumor effects was observed in several patients, but stable disease was the best response noted. Patients in the 2 μg/kg/day group had a 5.8-fold increase in number of circulating CD8+ T cells, 38-fold increase in total NK cells, and 358-fold increase in CD56bright NK cells. Serum IL15 concentrations were markedly lower during the last 3 days of infusion.Conclusions:This phase I trial identified the MTD for CIV rhIL15 and defined a treatment regimen that produced significant expansions of CD8+ T and NK effector cells in circulation and tumor deposits. This regimen has identified several biological features, including dramatic increases in numbers of NK cells, supporting trials of IL15 with anticancer mAbs to increase antibody-dependent cell-mediated cytotoxicity and anticancer efficacy.

Published

2023

34. Supplementary Table from IL15 and Anti–PD-1 Augment the Efficacy of Agonistic Intratumoral Anti-CD40 in a Mouse Model with Multiple TRAMP-C2 Tumors

Author

Thomas A. Waldmann, Elijah F. Edmondson, Richard N. Bamford, and Wei Chen

Abstract

Supplementary Table from IL15 and Anti–PD-1 Augment the Efficacy of Agonistic Intratumoral Anti-CD40 in a Mouse Model with Multiple TRAMP-C2 Tumors

Published

2023

35. Genome-wide CRISPR screen identifies CDK6 as a therapeutic target in adult T-cell leukemia/lymphoma

Author

Yandan Yang, Sigrid Dubois, Takashi Ishio, Takanori Teshima, Shinya Tanaka, Emmanuel Bachy, Masao Nakagawa, Satoshi Hashino, Yibin Yang, Sarvesh Kumar, Yutaka Hatanaka, Anusara Daenthanasanmak, Joji Shimono, Tomoyuki Endo, Patrick L. Green, Bonita R. Bryant, Yoshihiro Matsuno, Michiyuki Maeda, Hiroo Hasegawa, Da-Wei Huang, Michael N. Petrus, Thomas A. Waldmann, Yuquan Lin, Takashi Yokota, Hideki Goto, Kanako C. Hatanaka, and Louis M. Staudt

Subjects

Adult, Cell cycle checkpoint, Lymphoma, Immunology, Apoptosis, mTORC1, Mechanistic Target of Rapamycin Complex 1, Palbociclib, Malignancy, Biochemistry, Adult T-cell leukemia/lymphoma, immune system diseases, hemic and lymphatic diseases, medicine, Humans, Leukemia-Lymphoma, Adult T-Cell, biology, Cyclin-Dependent Kinase 6, Cell Biology, Hematology, medicine.disease, Leukemia, Cancer research, biology.protein, Cyclin-dependent kinase 6, Signal Transduction

Abstract

Adult T-cell leukemia/lymphoma (ATLL) is an aggressive T-cell malignancy with a poor prognosis with current therapy. Here we report genome-wide CRISPR-Cas9 screening of ATLL models, which identified CDK6, CCND2, BATF3, JUNB, STAT3, and IL10RB as genes that are essential for the proliferation and/or survival of ATLL cells. As a single agent, the CDK6 inhibitor palbociclib induced cell cycle arrest and apoptosis in ATLL models with wild-type TP53. ATLL models that had inactivated TP53 genetically were relatively resistant to palbociclib owing to compensatory CDK2 activity, and this resistance could be reversed by APR-246, a small molecule activator of mutant TP53. The CRISPR-Cas9 screen further highlighted the dependence of ATLL cells on mTORC1 signaling. Treatment of ATLL cells with palbociclib in combination with mTORC1 inhibitors was synergistically toxic irrespective of the TP53 status. This work defines CDK6 as a novel therapeutic target for ATLL and supports the clinical evaluation of palbociclib in combination with mTORC1 inhibitors in this recalcitrant malignancy.

Published

2022

36. IL15 and Anti–PD-1 Augment the Efficacy of Agonistic Intratumoral Anti-CD40 in a Mouse Model with Multiple TRAMP-C2 Tumors

Author

Wei Chen, Richard N. Bamford, Elijah F. Edmondson, and Thomas A. Waldmann

Subjects

Interleukin-15, Male, Cancer Research, Antibodies, Monoclonal, Antineoplastic Agents, CD8-Positive T-Lymphocytes, Mice, Inbred C57BL, Disease Models, Animal, Mice, Oncology, Cell Line, Tumor, Neoplasms, Animals, Humans, CD40 Antigens

Abstract

Purpose: IL15 promotes activation and maintenance of natural killer (NK) and CD8+ T effector memory cells making it a potential immunotherapeutic agent for the treatment of cancer. However, monotherapy with IL15 was ineffective in patients with cancer, indicating that it would have to be used in combination with other anticancer agents. The administration of high doses of common gamma chain cytokines, such as IL15, is associated with the generation of “helpless” antigen-nonspecific CD8 T cells. The generation of the tumor-specific cytotoxic T cells can be mediated by CD40 signaling via agonistic anti-CD40 antibodies. Nevertheless, parenteral administration of anti-CD40 antibodies is associated with unacceptable side effects, such as thrombocytopenia and hepatic toxicity, which can be avoided by intratumoral administration. Experimental Design: We investigated the combination of IL15 with an intratumoral anti-CD40 monoclonal antibody (mAb) in a dual tumor TRAMP-C2 murine prostate cancer model and expanded the regimen to include an anti–PD-1 mAb. Results: Here we demonstrated that anti-CD40 given intratumorally not only showed significant antitumor activity in treated tumors, but also noninjected contralateral tumors, indicative of abscopal efficacy. The combination of IL15 with intratumoral anti-CD40 showed an additive immune response with an increase in the number of tumor-specific tetramer-positive CD8 T cells. Furthermore, the addition of anti–PD-1 further improved efficacy mediated by the anti-CD40/IL15 combination. Conclusions: These studies support the initiation of a clinical trial in patients with cancer using IL15 in association with the checkpoint inhibitor, anti–PD-1, and intratumoral optimized anti-CD40.

Published

2022

37. IL-15 Trans-Presentation Is an Autonomous, Antigen-Independent Process

Author

Katalin Tóth, Ádám Kenesei, Andrea Bodnár, Gábor Mocsár, Julianna Volkó, György Vámosi, Károly Jambrovics, Thomas A. Waldmann, Zoltán Balajthy, and Nikoletta Szalóki

Subjects

MHC class II, biology, Chemistry, CD3, T cell, Immunology, Ligand (biochemistry), Jurkat cells, Immunological synapse, Cell biology, Raji cell, medicine.anatomical_structure, biology.protein, medicine, Immunology and Allergy, Receptor

Abstract

IL-15 plays a pivotal role in the long-term survival of T cells and immunological memory. Its receptor consists of three subunits (IL-15Rα, IL-2/15Rβ, and γc). IL-15 functions mainly via trans-presentation (TP), during which an APC expressing IL-15 bound to IL-15Rα presents the ligand to the βγc receptor-heterodimer on a neighboring T/NK cell. To date, no direct biophysical evidence for the intercellular assembly of the IL-15R heterotrimer exists. Ag presentation (AP), the initial step of T cell activation, is also based on APC–T cell interaction. We were compelled to ask whether AP has any effect on IL-15 TP or whether they are independent processes. In our human Raji B cell–Jurkat T cell model system, we monitored inter-/intracellular protein interactions upon formation of IL-15 TP and AP receptor complexes by Förster resonance energy transfer measurements. We detected enrichment of IL-15Rα and IL-2/15Rβ at the synapse and positive Förster resonance energy transfer efficiency if Raji cells were pretreated with IL-15, giving direct biophysical evidence for IL-15 TP. IL-15Rα and MHC class II interacted and translocated jointly to the immunological synapse when either ligand was present, whereas IL-2/15Rβ and CD3 moved independently of each other. IL-15 TP initiated STAT5 phosphorylation in Jurkat cells, which was not further enhanced by AP. Conversely, IL-15 treatment slightly attenuated Ag-induced phosphorylation of the CD3ζ chain. Our studies prove that in our model system, IL-15 TP and AP can occur independently, and although AP enhances IL-15R assembly, it has no significant effect on IL-15 signaling during TP. Thus, IL-15 TP can be considered an autonomous, Ag-independent process.

Published

2021

38. The implications of IL-15 trans-presentation on the immune response

Author

Thomas A, Waldmann, Robert, Waldmann, Jian-Xin, Lin, and Warren J, Leonard

Subjects

Interleukin-15, Immunity, Humans, Animals, Interleukin Receptor Common gamma Subunit, Protein Binding, Signal Transduction

Abstract

Interleukin-15 is a pleiotropic cytokine type I four alpha-helical bundle cytokine that along with IL-2, IL-4, IL-7, IL-9, and IL-21 shares the common cytokine receptor γ chain, γ

Published

2022

39. Insights Into Thermal Runaway of Li–Ion Cells by Accelerating Rate Calorimetry Coupled with External Sensors and Online Gas Analysis

Author

Michael Kasper, A. A. Abd-El-Latif, Peter Sichler, Margret Wohlfahrt-Mehrens, and Thomas A. Waldmann

Subjects

Overcharge, Materials science, Thermal runaway, Energy Engineering and Power Technology, Thermodynamics, 02 engineering and technology, Calorimetry, 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, 0104 chemical sciences, Ion, Electrochemistry, Gas analysis, Electrical and Electronic Engineering, 0210 nano-technology

Published

2021

40. A novel model of alternative NF-κB pathway activation in anaplastic large cell lymphoma

Author

Marshall E. Kadin, Yangyang Li, Hong-Bo Wang, Yijun Liu, Yibin Yang, Masao Nakagawa, Craig J. Thomas, Mu Sheng Zeng, Michael N. Petrus, Thomas A. Waldmann, Wenming Xiao, Jing Ping Zhang, Zhihui Song, and Wei Wei

Subjects

STAT3 Transcription Factor, 0301 basic medicine, TRAF3, Cancer Research, CD30, Somatic cell, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, hemic and lymphatic diseases, medicine, Humans, T-cell lymphoma, Anaplastic Lymphoma Kinase, Phosphorylation, STAT3, Anaplastic large-cell lymphoma, Janus Kinases, biology, Chemistry, NF-kappa B, NF-κB, Oncogenes, Hematology, medicine.disease, 030104 developmental biology, Oncology, Cell culture, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Lymphoma, Large-Cell, Anaplastic, Signal Transduction

Abstract

Aberrant activation of NF-κB is the most striking oncogenic mechanism in B-cell lymphoma; however, its role in anaplastic large cell lymphomas (ALCL) has not been fully established and its activation mechanism(s) remain unclear. Using ALCL cell line models, we revealed the supporting roles for NFKB2 and the NIK pathway in some ALCL lines. To investigate the detailed activation mechanisms for this oncogenic pathway, we performed specifically designed alternative NF-κB reporter CRISPR screens followed by the RNA-seq analysis, which led us to identify STAT3 as the major mediator for NIK-dependent NF-κB activation in ALCL. Consistently, p-STAT3 level was correlated with NFKB2 nuclear accumulation in primary clinical samples. Mechanistically, we found that in NIK-positive ALK- ALCL cells, common JAK/STAT3 mutations promote transcriptional activity of STAT3 which directly regulates NFKB2 and CD30 expression. Endogenous expression of CD30 induces constitutive NF-κB activation through binding and degrading of TRAF3. In ALK+ ALCL, the CD30 pathway is blocked by the NPM-ALK oncoprotein, but STAT3 activity and resultant NFKB2 expression can still be induced by NPM-ALK, leading to minimal alternative NF-κB activation. Our data suggest combined NIK and JAK inhibitor therapy could benefit patients with NIK-positive ALK- ALCL carrying JAK/STAT3 somatic mutations.

Published

2020

41. Bench-to-bedside translation of interleukin-15 for immunotherapy: principles and challenges

Author

Thomas A. Waldmann and Chalet Tan

Subjects

business.industry, medicine.medical_treatment, Pharmaceutical Science, Translation (biology), Immunotherapy, Bioinformatics, Article, Bench to bedside, On cells, Interleukin 15, medicine, In patient, Effector functions, business, CD8

Abstract

Since its discovery 25 years ago by our group and Grabstein et al. [1–3], interleukin-15 (IL-15) has attracted much attention in terms of its biological activities, mechanism of action and therapeutic modulations under various physiological and pathological conditions. In particular, the stimulatory effects of IL-15 on the proliferation and effector functions of natural killer (NK) cells and CD8+ T cells make it a promising component for immunotherapy in the treatment of malignancies and infectious diseases [4,5]. Here, we present a brief summary on the biological principles of how IL-15 exerts immunostimulatory effects on cells, the clinical investigations on IL-15-based therapeutic agents, and the challenges for safe and efficacious delivery of IL-15 in patients.

Published

2020

42. 90Y-Daclizumab (Anti-CD25), High-Dose Carmustine, Etoposide, Cytarabine, and Melphalan Chemotherapy and Autologous Hematopoietic Stem Cell Transplant Yielded Sustained Complete Remissions in 4 Patients with Recurrent Hodgkin's Lymphoma

Author

Claude Sportes, Martin W. Brechbiel, Millie Whatley, Thomas A. Fleisher, Erin M Corcoran, Jae-Ho Lee, Thomas A. Waldmann, Daniel H. Fowler, Bonita R. Bryant, Kevin C. Conlon, Ronald E. Gress, Jorge A. Carrasquillo, Clara C. Chen, Chang H. Paik, Karen A. Kurdziel, Milos D. Miljkovic, and Stefania Pittaluga

Subjects

0301 basic medicine, Oncology, Melphalan, Cancer Research, medicine.medical_specialty, medicine.medical_treatment, 03 medical and health sciences, 0302 clinical medicine, Daclizumab, immune system diseases, hemic and lymphatic diseases, Internal medicine, medicine, Radiology, Nuclear Medicine and imaging, Pharmacology, Chemotherapy, business.industry, Hematopoietic stem cell, Original Articles, General Medicine, Hodgkin's lymphoma, medicine.disease, Lymphoma, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Radioimmunotherapy, Cytarabine, business, medicine.drug

Abstract

Background: Despite advances in therapy of Hodgkin's lymphoma (HL), a proportion of patients will not respond or relapse. The authors had previously identified CD25, IL-2Rα, as a target for systemic radioimmunotherapy of HL since most normal cells do not express CD25, but it is expressed by a minority of Hodgkin/Reed-Sternberg (HRS) cells and most Tregs rosetting around HRS cells. Study Design and Treatment: This was a single institution, nonrandomized, open-label phase I/II trial of radiolabeled (90)Y-daclizumab, an anti-CD25 monoclonal antibody, BEAM (carmustine, etoposide, cytarabine, and melphalan) conditioning treatment followed by autologous hematopoietic stem cell transplant (ASCT). Four patients with refractory and relapsed HL were treated in this trial with 3 patients receiving a single dose of 564.6–574.6 MBq (90)Y-daclizumab and the fourth patient receiving two doses of 580.9–566.1 MBq (90)Y-daclizumab followed by high-dose chemotherapy and ASCT. Results: All 4 evaluable patients treated with (90)Y-daclizumab obtained complete responses (CRs) that are ongoing 4.5–7 years following their stem cell transplant. The spectrum and severity of adverse events were mild and more importantly none of the patients, including several with multiple therapies before this treatment, developed the myelodysplastic syndrome. Discussion: Targeting by daclizumab was not directed primarily at tumor cells, but rather the nonmalignant CD25-expressing T cells adjacent to the HRS cells and (90)Y-daclizumab provided strong enough β emissions to kill CD25-negative tumor cells at a distance by a crossfire effect. Furthermore, the strong β irradiation killed normal cells in the tumor microenvironment. Conclusions: (90)Y-daclizumab (anti-CD25), high-dose BEAM chemotherapy and ASCT was well tolerated and yielded sustained complete remissions in all 4 patients with recurrent HL patients who completed their treatment. Significance: Despite advances, a proportion of patients with HL will not have a CR to their initial treatment, and some with CRs will relapse. They demonstrated that the addition of (90)Y-daclizumab into the preconditioning regimen for refractory and relapsed HL patients with high-dose BEAM chemotherapy and ASCT provided sustained CRs in the 4 patients studied. Two of these patients were highly refractory to multiple prior treatments with bulky disease at entry into this study, including 1 patient who never entered a remission and had failed 6 different therapeutic regimens. Despite the small number of patients treated in this study, the sustained clinical benefit in these patients indicates a highly effective treatment. The daclizumab was directed primarily not at HRS cells themselves but toward nonmalignant T cells rosetting around malignant cells. (90)Y provided strong β emissions that killed antigen nonexpressing tumor cells at a distance by a crossfire effect. Furthermore, the strong β radiation killed normal cells in the tumor microenvironment that nurtured the malignant cells in the lymphomatous mass. The present study supports expanded analysis of (90)Y-daclizumab as part of the regimen of ASCT in patients with refractory and relapsed HL.

Published

2020

43. A very long-acting IL-15: implications for the immunotherapy of cancer

Author

John A Hangasky, Wei Chen, Sigrid P Dubois, Anusara Daenthanasanmak, Jürgen R Müller, Ralph Reid, Thomas A Waldmann, and Daniel V Santi

Subjects

Male, Cancer Research, Leukemia, T-Cell, Receptors, CCR4, Immunology, Adenocarcinoma, Antineoplastic Agents, Immunological, Drug Delivery Systems, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, Immunology and Allergy, Animals, Humans, Prodrugs, CD40 Antigens, RC254-282, T-lymphocytes, Pharmacology, Clinical/Translational Cancer Immunotherapy, Interleukin-15, natural killer cells, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Prostatic Neoplasms, cytokines, Microspheres, Mice, Inbred C57BL, Disease Models, Animal, Oncology, translational medical research, Molecular Medicine, Immunotherapy, Half-Life

Abstract

BackgroundInterleukin-15 (IL-15) is an important cytokine necessary for proliferation and maintenance of natural killer (NK) and CD8+ T cells, and with great promise as an immuno-oncology therapeutic. However, IL-15 has a very short half-life and a single administration does not provide the sustained exposure required for optimal stimulation of target immune cells. The purpose of this work was to develop a very long-acting prodrug that would maintain IL-15 within a narrow therapeutic window for long periods—similar to a continuous infusion.MethodsWe prepared and characterized hydrogel microspheres (MS) covalently attached to IL-15 (MS~IL-15) by a releasable linker. The pharmacokinetics and pharmacodynamics of MS~IL-15 were determined in C57BL/6J mice. The antitumor activity of MS~IL-15 as a single agent, and in combination with a suitable therapeutic antibody, was tested in a CD8+ T cell-driven bilateral transgenic adenocarcinoma mouse prostate (TRAMP)-C2 model of prostatic cancer and a NK cell-driven mouse xenograft model of human ATL (MET-1) murine model of adult T-cell leukemia.ResultsOn subcutaneous administration to mice, the cytokine released from the depot maintained a long half-life of about 168 hours over the first 5 days, followed by an abrupt decrease to about ~30 hours in accordance with the development of a cytokine sink. A single injection of MS~IL-15 caused remarkably prolonged expansions of NK and ɣδ T cells for 2 weeks, and CD44hiCD8+ T cells for 4 weeks. In the NK cell-driven MET-1 murine model of adult T-cell leukemia, single-agent MS~IL-1550 μg or anti-CCR4 provided modest increases in survival, but a combination—through antibody-depedent cellular cytotoxicity (ADCC)—significantly extended survival. In a CD8+ T cell-driven bilateral TRAMP-C2 model of prostatic cancer, single agent subcutaneous MS~IL-15 or unilateral intratumoral agonistic anti-CD40 showed modest growth inhibition, but the combination exhibited potent, prolonged bilateral antitumor activity.ConclusionsOur results show MS~IL-15 provides a very long-acting IL-15 with low Cmax that elicits prolonged expansion of target immune cells and high anticancer activity, especially when administered in combination with a suitable immuno-oncology agent.

Published

2022

44. The implications of IL-15 trans-presentation on the immune response

Author

Thomas A. Waldmann, Robert Waldmann, Jian-Xin Lin, and Warren J. Leonard

Published

2022

45. Trans -endocytosis of intact IL-15Rα–IL-15 complex from presenting cells into NK cells favors signaling for proliferation

Author

Michael J. Hollander, Eric O. Long, Sumati Rajagopalan, Erik L. Snapp, Olga M. Anton, Thomas A. Waldmann, K. Christopher Garcia, David W. Dorward, Mary E. Peterson, Javier Traba, and Gunjan Arora

Subjects

Multidisciplinary, biology, Chemistry, medicine.medical_treatment, Cell, Biological Sciences, Cell biology, medicine.anatomical_structure, Cytokine, Interleukin 15, Ribosomal protein s6, medicine, biology.protein, Phosphorylation, Gene silencing, Receptor, STAT5

Abstract

Interleukin 15 (IL-15) is an essential cytokine for the survival and proliferation of natural killer (NK) cells. IL-15 activates signaling by the β and common γ (γ(c)) chain heterodimer of the IL-2 receptor through trans-presentation by cells expressing IL-15 bound to the α chain of the IL-15 receptor (IL-15Rα). We show here that membrane-associated IL-15Rα–IL-15 complexes are transferred from presenting cells to NK cells through trans-endocytosis and contribute to the phosphorylation of ribosomal protein S6 and NK cell proliferation. NK cell interaction with soluble or surface-bound IL-15Rα–IL-15 complex resulted in Stat5 phosphorylation and NK cell survival at a concentration or density of the complex much lower than required to stimulate S6 phosphorylation. Despite this efficient response, Stat5 phosphorylation was reduced after inhibition of metalloprotease-induced IL-15Rα–IL-15 shedding from trans-presenting cells, whereas S6 phosphorylation was unaffected. Conversely, inhibition of trans-endocytosis by silencing of the small GTPase TC21 or expression of a dominant-negative TC21 reduced S6 phosphorylation but not Stat5 phosphorylation. Thus, trans-endocytosis of membrane-associated IL-15Rα–IL-15 provides a mode of regulating NK cells that is not afforded to IL-2 and is distinct from activation by soluble IL-15. These results may explain the strict IL-15 dependence of NK cells and illustrate how the cellular compartment in which receptor–ligand interaction occurs can influence functional outcome.

Published

2019

46. Increase of Cycling Stability in Pilot-Scale 21700 Format Li-Ion Cells by Foil Tab Design

Author

Daniel Brändle, Rares-George Scurtu, Margret Wohlfahrt-Mehrens, and Thomas A. Waldmann

Subjects

Materials science, Process Chemistry and Technology, Chemical technology, tab design, Bioengineering, lithium-ion battery, TP1-1185, Lithium-ion battery, Cathode, 21700 format, Anode, law.invention, Chemistry, Electrical resistance and conductance, law, Electrode, Chemical Engineering (miscellaneous), cell production, Graphite, Composite material, cell design, QD1-999, FOIL method, Separator (electricity)

Abstract

Li-ion cells of the industrially-relevant 21700 format were built on pilot-scale with tabs made from (a) the electrodes’ current collecting foils (Al and Cu, “foil tabs”) in comparison with (b) conventional tabs (Al and Ni) welded to the electrodes’ current collecting foils (“welded tabs”). Both cell types use the same anode (graphite), cathode (NMC622), separator, electrolyte, as well as the same tab positions. This allows a direct comparison of welded tabs and foil tabs regarding formation, C-rate capability, cell electrical resistance, and long-term cycling stability tests. Our data reproducibly shows 14.4% longer cycling stability and 11.2% increased total charge throughput in the case of the cells with foil tabs until 80% SOH, which is likely due to less inhomogeneities in the case of the foil tab design.

Published

2021

47. Triple combination of BET plus PI3K and NF-κB inhibitors exhibit synergistic activity in adult T-cell leukemia/lymphoma

Author

Anusara Daenthanasanmak, Richard N. Bamford, Makoto Yoshioka, Shyh-Ming Yang, Philip Homan, Baktiar Karim, Bonita R. Bryant, Michael N. Petrus, Craig J. Thomas, Patrick L. Green, Milos D. Miljkovic, Kevin C. Conlon, and Thomas A. Waldmann

Subjects

Human T-lymphotropic virus 1, Lymphoma, NF-kappa B, Hematology, Mice, Phosphatidylinositol 3-Kinases, Basic-Leucine Zipper Transcription Factors, immune system diseases, hemic and lymphatic diseases, Leukocytes, Mononuclear, Animals, Humans, Leukemia-Lymphoma, Adult T-Cell, Oleanolic Acid

Abstract

Adult T-cell leukemia/lymphoma (ATL) is an aggressive T-cell lymphoproliferative malignancy caused by human T-cell leukemia virus type 1 (HTLV-1). ATL is an orphan disease with no curative drug treatment regimens urgently needing new combination therapy. HTLV-1-infected cells rely on viral proteins, Tax and HBZ (HTLV-1-b-ZIP factor), to activate the transcription of various host genes that are critical for promoting leukemic transformation. Inhibition of bromodomain and extraterminal motif (BET) protein was previously shown to collapse the transcriptional network directed by BATF3 super-enhancer and thereby induced ATL cell apoptosis. In the current work, by using xenograft, ex vivo, and in vitro models, we demonstrated that I-BET762 (BETi) synergized with copanlisib (PI3Ki) and bardoxolone methyl (NF-κBi) to dramatically decrease the growth of ATL cells. Mechanistically, the triple combination exhibited synergistic activity by down-regulating the expression of c-MYC while upregulating the level of the glucocorticoid-induced leucine zipper (GILZ). The triple combination also enhanced apoptosis induction by elevating the expression of active caspase-3 and cleaved PARP. Importantly, the triple combination prolonged the survival of ATL-bearing xenograft mice and inhibited the proliferation of ATL cells from peripheral blood mononuclear cells (PBMCs) of both acute and smoldering/chronic ATL patients. Therefore, our data provide the rationale for a clinical trial exploring the multiagent combination of BET, PI3K/AKT, and NF-κB inhibitors for ATL patients and expands the potential treatments for this recalcitrant malignancy.

Published

2021

48. Identification of Degradation Mechanisms by Post-Mortem Analysis for High Power and High Energy Commercial Li-Ion Cells after Electric Vehicle Aging

Author

A. L. Buzlukov, Karsten Richter, Olivier Raccurt, Pierre Kuntz, Michel Bardet, Margret Wohlfahrt-Mehrens, Thomas A. Waldmann, Philippe Azaïs, and Sylvie Genies

Subjects

Battery (electricity), TK1001-1841, Materials science, business.product_category, Li-ion, 020209 energy, Energy Engineering and Power Technology, degradation mechanisms, 02 engineering and technology, post mortem analysis, Electrochemistry, Production of electric energy or power. Powerplants. Central stations, Electric vehicle, 0202 electrical engineering, electronic engineering, information engineering, Battery electric vehicle, Electrical and Electronic Engineering, battery, aging, 021001 nanoscience & nanotechnology, TP250-261, Chemical engineering, Industrial electrochemistry, Electrode, Degradation (geology), Fade, 0210 nano-technology, business, Cell aging

Abstract

Driven by the rise of the electric automotive industry, the Li-ion battery market is in strong expansion. This technology does not only fulfill the requirements of electric mobility, but is also found in most portable electric devices. Even though Li-ion batteries are known for their numerous advantages, they undergo serious performance degradation during their aging, and more particularly when used in specific conditions such as at low temperature or high charging current rates. Depending on the operational conditions, different aging mechanisms are favored and can induce physical and chemical modifications of the internal components, leading to performance decay. In this article, the identification of the degradation mechanisms was carried out thanks to an in-depth ante- and post mortem study on three high power and high energy commercial 18,650 cells. Li-ion cells were aged using a battery electric vehicle (BEV) aging profile at −20 °C, 0 °C, 25 °C, and 45 °C in accordance with the international standard IEC 62-660, and in calendar aging mode at 45 °C and SOC 100%. Internal components recovered from fresh and aged cells were investigated through different electrochemical (half-coin cell), chemical (EDX, GD-OES, NMR), and topological (SEM) characterization techniques. The influence of power and energy cells’ internal design and Si content in the negative electrode on cell aging has been highlighted vis-à-vis the capacity and power fade.

Published

2021

49. Germinal epimutation of Fragile Histidine Triad (FHIT) gene is associated with progression to acute and chronic adult T-cell leukemia diseases

Author

Olivier Hermine, Vahid Asnafi, Izabela Bialuk, Marcia Bellon, Lee Ratner, Ambroise Marçais, Michael N. Petrus, Thomas A. Waldmann, Genoveffa Franchini, Toshiki Watanabe, Antoine Gessain, Masao Matsuoka, Christophe Nicot, Achiléa L. Bittencourt, Lourdes Farre, Veronica Galli, Xue Tao Bai, University of Kansas Medical Center [Kansas City, KS, USA], National Cancer Institute [Bethesda] (NCI-NIH), National Institutes of Health [Bethesda] (NIH), Ohio State University [Columbus] (OSU), Hospitalet de Llobregat, Universidade Federal da Bahia (UFBA), Institut Necker Enfants-Malades (INEM - UM 111 (UMR 8253 / U1151)), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), Washington University in Saint Louis (WUSTL), Epidémiologie et Physiopathologie des Virus Oncogènes (EPVO (UMR_3569 / U-Pasteur_3)), Institut Pasteur [Paris] (IP)-Université Paris Diderot - Paris 7 (UPD7)-Centre National de la Recherche Scientifique (CNRS), Kyoto University, Kumamoto University, The University of Tokyo (UTokyo), and This work was supported by grant R01CA201309 to Christophe Nicot.

Subjects

0301 basic medicine, MESH: Neoplasm Proteins, Cancer Research, MESH: Paraparesis, Tropical Spastic, Lymphoma, [SDV]Life Sciences [q-bio], viruses, T-cell leukemia, Bisulfite sequencing, Tax, MESH: Acid Anhydride Hydrolases, Epigenesis, Genetic, TSP/HAM, 0302 clinical medicine, MESH: DNA Methylation, FHIT, immune system diseases, hemic and lymphatic diseases, Tropical spastic paraparesis, Leukemia-Lymphoma, Adult T-Cell, MESH: Epigenesis, Genetic, MESH: Leukemia-Lymphoma, Adult T-Cell, Càncer, RC254-282, Cancer, Leukemia, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Epigenetic, virus diseases, Leucèmia, TSP, Paraparesis, Tropical Spastic, Acid Anhydride Hydrolases, Neoplasm Proteins, Oncology, 030220 oncology & carcinogenesis, Disease Progression, Molecular Medicine, MESH: Disease Progression, Epigenetics, Tumor suppressor gene, Biology, ATLL, Methylation, 03 medical and health sciences, MESH: HTLV-I Infections, medicine, Humans, Epimutation, neoplasms, Retrospective Studies, MESH: Humans, Research, MESH: Retrospective Studies, DNA Methylation, medicine.disease, Epigenètica, HTLV-I Infections, HAM, 030104 developmental biology, ATL, HTLV-1, Cancer research

Abstract

Background Human T cell Leukemia virus type 1 (HTLV-I) is etiologically linked to adult T cell leukemia/lymphoma (ATL) and an inflammatory neurodegenerative disease called HTLV-I-associated myelopathy or tropical spastic paraparesis (HAM/TSP). The exact genetic or epigenetic events and/or environmental factors that influence the development of ATL, or HAM/TSP diseases are largely unknown. The tumor suppressor gene, Fragile Histidine Triad Diadenosine Triphosphatase (FHIT), is frequently lost in cancer through epigenetic modifications and/or deletion. FHIT is a tumor suppressor acting as genome caretaker by regulating cellular DNA repair. Indeed, FHIT loss leads to replicative stress and accumulation of double DNA strand breaks. Therefore, loss of FHIT expression plays a key role in cellular transformation. Methods Here, we studied over 400 samples from HTLV-I-infected individuals with ATL, TSP/HAM, or asymptomatic carriers (AC) for FHIT loss and expression. We examined the epigenetic status of FHIT through methylation specific PCR and bisulfite sequencing; and correlated these results to FHIT expression in patient samples. Results We found that epigenetic alteration of FHIT is specifically found in chronic and acute ATL but is absent in asymptomatic HTLV-I carriers and TSP/HAM patients’ samples. Furthermore, the extent of FHIT methylation in ATL patients was quantitatively comparable in virus-infected and virus non-infected cells. We also found that longitudinal HTLV-I carriers that progressed to smoldering ATL and descendants of ATL patients harbor FHIT methylation. Conclusions These results suggest that germinal epigenetic mutation of FHIT represents a preexisting mark predisposing to the development of ATL diseases. These findings have important clinical implications as patients with acute ATL are rarely cured. Our study suggests an alternative strategy to the current “wait and see approach” in that early screening of HTLV-I-infected individuals for germinal epimutation of FHIT and early treatment may offer significant clinical benefits.

Published

2021

50. Rapid progression of adult T-cell leukemia/lymphoma as tumor-infiltrating Tregs after PD-1 blockade

Author

Xingxing Zang, Kevin C. Conlon, Xiaoxin Ren, B. Hilda Ye, Daniel Rauch, Malachi Griffith, Hemalatha Sundaramoorthi, Obi L. Griffith, Zachary L. Skidmore, Thomas A. Waldmann, Murali Janakiram, Lee Ratner, Milos D. Miljkovic, Sydney L. Olson, Jonathan E. Brammer, John C. S. Harding, Xiaogang Cheng, and Ancy Joseph

Subjects

Adult, Immunobiology and Immunotherapy, Lymphoma, Somatic cell, Programmed Cell Death 1 Receptor, Immunology, T-Lymphocytes, Regulatory, Biochemistry, Adult T-cell leukemia/lymphoma, Mice, Antineoplastic Agents, Immunological, immune system diseases, Neoplasms, hemic and lymphatic diseases, Tumor Cells, Cultured, medicine, Animals, Humans, Leukemia-Lymphoma, Adult T-Cell, 610 Medicine & health, Gene Expression Regulation, Leukemic, business.industry, Cancer, Cell Biology, Hematology, medicine.disease, Immune checkpoint, Blockade, Leukemia, Nivolumab, Disease Progression, Cancer research, Immunotherapy, business

Abstract

Immune checkpoint inhibitors are a powerful new tool in the treatment of cancer, with prolonged responses in multiple diseases, including hematologic malignancies, such as Hodgkin lymphoma. However, in a recent report, we demonstrated that the PD-1 inhibitor nivolumab led to rapid progression in patients with adult T-cell leukemia/lymphoma (ATLL) (NCT02631746). We obtained primary cells from these patients to determine the cause of this hyperprogression. Analyses of clonality, somatic mutations, and gene expression in the malignant cells confirmed the report of rapid clonal expansion after PD-1 blockade in these patients, revealed a previously unappreciated origin of these malignant cells, identified a novel connection between ATLL cells and tumor-resident regulatory T cells (Tregs), and exposed a tumor-suppressive role for PD-1 in ATLL. Identifying the mechanisms driving this alarming outcome in nivolumab-treated ATLL may be broadly informative for the growing problem of rapid progression with immune checkpoint therapies.

Published

2019