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155. Frequent expression of the tumor necrosis factor receptor–associated factor 1 in latent membrane protein 1–Positive posttransplant lymphoproliferative disease and HIV-associated lymphomas

Author

Murray, Paul G., primary, Swinnen, Lode J., additional, Flavell, Joanne R., additional, Ragni, Margaret V., additional, Baumforth, Karl R.N., additional, Toomey, Siobhan M., additional, Filipovich, Alexandra H., additional, Lowe, Derek, additional, Schnell, Carrie S., additional, Johl, Jewel, additional, Gulley, Margaret, additional, Young, Lawrence S., additional, and Ambinder, Richard F., additional

Published
2001
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156. Comparative analysis of the expression of the epstein‐barr virus (EBV) anti‐apoptotic gene BHRF1 in nasopharyngeal carcinoma and EBV‐related lymphoid diseases

Author

Nicholls, John, primary, Kremmer, Elisabeth, additional, Meseda, Clement A., additional, Mackett, Mike, additional, Hahn, Peter, additional, Gulley, Margaret L., additional, Brink, Antoinette, additional, Swinnen, Lode J., additional, Greenspan, John, additional, De Souza, Yvonne, additional, Grässer, Friedrich, additional, Sham, Jonathan, additional, Ng, Mun‐Hon, additional, and Arrand, John R., additional

Published
2001
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159. Bevacizumab and cyclosphosphamide, doxorubicin, vincristine and prednisone in combination for patients with peripheral T-cell or natural killer cell neoplasms: an Eastern Cooperative Oncology Group study (E2404).

Author

Ganjoo, Kristen, Hong, Fangxin, Horning, Sandra J., Gascoyne, Randy D., Natkunam, Yasodha, Swinnen, Lode J., Habermann, Thomas M., Kahl, Brad S., and Advani, Ranjana H.

Subjects
HEALTH outcome assessment, PHYSIOLOGICAL effects of chemotherapy, T cells, KILLER cells, VASCULAR endothelial growth factors, LYMPHOMAS, DOXORUBICIN, BEVACIZUMAB, PATIENTS, CANCER
Abstract

Peripheral T-cell lymphoma (PTCL) and natural killer (NK) cell lymphoma have poor survival with conventional cytotoxic chemotherapy. Because angiogenesis plays an important role in the biology of PTCL, a fully humanized anti-vascular endothelial growth factor (VEGF) antibody, bevacizumab (A), was studied in combination with standard cyclosphosphamide, doxorubicin, vincristine and prednisone (CHOP) chemotherapy (ACHOP) to evaluate its potential to improve outcome in these patients. Patients were treated with 6-8 cycles of ACHOP followed by eight doses of maintenance A (15 mg/kg every 21 days). Forty-six patients were enrolled on this phase 2 study from July 2006 through March 2009. Forty-four patients were evaluable for toxicity and 39 were evaluable for response, progression and survival. A total of 324 cycles (range: 2-16, median 7) were administered to 39 evaluable patients and only nine completed all planned treatment. The overall response rate was 90% with 19 (49%) complete response/complete response unconfirmed (CR/CRu) and 16 (41%) a partial response (PR). The 1-year progression-free survival (PFS) rate was 44% at a median follow-up of 3 years. The median PFS and overall survival (OS) rates were 7.7 and 22 months, respectively. Twenty-three patients died (21 from lymphoma, two while in remission). Grade 3 or 4 toxicities included febrile neutropenia ( n = 8), anemia ( n = 3), thrombocytopenia ( n = 5), congestive heart failure ( n = 4), venous thrombosis ( n = 3), gastrointestinal hemorrhage/perforation ( n = 2), infection ( n = 8) and fatigue ( n = 6). Despite a high overall response rate, the ACHOP regimen failed to result in durable remissions and was associated with significant toxicities. Studies of novel therapeutics are needed for this patient population, whose clinical outcome remains poor. [ABSTRACT FROM AUTHOR]

Published
2014
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160. EPSTEIN-BARR VIRUS-INDUCED POSTTRANSPLANT LYMPHOPROLIFERATIVE DISORDERS

Author

Paya, Carlos V., primary, Fung, John J., additional, Nalesnik, Michael A., additional, Kieff, Elliott, additional, Green, Michael, additional, Gores, Gregory, additional, Habermann, Thomas M., additional, Wiesner, Russell H., additional, Swinnen, Lode J., additional, Woodle, E. Steve, additional, and Bromberg, Jonathan S., additional

Published
1999
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169. Brief intensive therapy for older adults with newly diagnosed Burkitt or atypical Burkitt lymphoma/leukemia.

Author

Kasamon, Yvette L., Brodsky, Robert A., Borowitz, Michael J., Ambinder, Richard F., Crilley, Pamela A., Cho, Steve Y., Tsai, Hua-ling, Smith, B. Douglas, Gladstone, Douglas E., Carraway, Hetty E., Huff, Carol Ann, Matsui, William H., Bolaños-Meade, Javier, Jones, Richard J., and Swinnen, Lode J.

Subjects
OLDER patients, BURKITT'S lymphoma, CYCLOPHOSPHAMIDE, ANTHRACYCLINES, VINCRISTINE, RITUXIMAB
Abstract

Older patients with Burkitt lymphoma/leukemia (BL) have inferior outcomes. Because cyclophosphamide is highly active in BL and can be dose-escalated without stem-cell rescue, we designed a short, cyclophosphamide-intensive regimen without anthracyclines for patients aged ≥ 30 with untreated, non-HIV-associated BL/atypical BL. Two cycles involving cyclophosphamide 1500 mg/m2, vincristine, rituximab, prednisone, methotrexate 3 g/m2, and intrathecal cytarabine were delivered 2 weeks apart, followed by intensification with high-dose cyclophosphamide (50 mg/kg/day for 4 days) and rituximab. Of 21 patients, median age 53 (range, 34-75), 71% had stage IV, 95% were high-risk and 29% had performance status 3-4. Response occurred in all evaluable patients post-cycle 2 and in 76% post-intensification. Five non-relapse deaths occurred (four before intensification). The estimated 1-year and 3-year event-free survival was 52%; 1-year and 3-year overall survival was 57%. Seventeen (81%) received intensification (median 30 days to intensification). Brief, anthracycline-sparing, intensive cyclophosphamide (BASIC) therapy yields durable remissions in poorer-risk BL/atypical BL. [ABSTRACT FROM AUTHOR]

Published
2013
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172. Single-agent GVHD prophylaxis with posttransplantation cyclophosphamide after myeloablative, HLA-matched BMT for AML, ALL, and MDS

Author

Kanakry, Christopher G., Tsai, Hua-Ling, Bolaños-Meade, Javier, Smith, B. Douglas, Gojo, Ivana, Kanakry, Jennifer A., Kasamon, Yvette L., Gladstone, Douglas E., Matsui, William, Borrello, Ivan, Huff, Carol Ann, Swinnen, Lode J., Powell, Jonathan D., Pratz, Keith W., DeZern, Amy E., Showel, Margaret M., McDevitt, Michael A., Brodsky, Robert A., Levis, Mark J., Ambinder, Richard F., Fuchs, Ephraim J., Rosner, Gary L., Jones, Richard J., and Luznik, Leo

Abstract

High-dose, posttransplantation cyclophosphamide (PTCy) reduces severe graft-versus-host disease (GVHD) after allogeneic blood or marrow transplantation (alloBMT), but the impact of PTCy on long-term, disease-specific outcomes is unclear. We conducted a retrospective study of 209 consecutive adult patients transplanted for acute myeloid leukemia (AML, n = 138), myelodysplastic syndrome (n = 28), or acute lymphoblastic leukemia (ALL, n = 43) using PTCy as sole GVHD prophylaxis after myeloablative conditioning and HLA-matched–related or –unrelated T-cell–replete allografting. At alloBMT, 30% of patients were not in morphologic complete remission. The cumulative incidences of grades II to IV and III to IV acute GVHD at 100 days and chronic GVHD at 2 years were 45%, 11%, and 13%, respectively. Forty-three percent of patients did not require immunosuppression for any reason beyond PTCy. At 3 years, relapse cumulative incidence was 36%, disease-free survival was 46%, survival free of disease and chronic GVHD was 39%, and overall survival was 58%. Lack of remission at alloBMT, adverse cytogenetics, and low allograft nucleated cell dose were associated with inferior survival for AML patients. Minimal residual disease but not t(9;22) was associated with inferior outcomes for ALL patients. The ability to limit posttransplantation immunosuppression makes PTCy a promising transplantation platform for the integration of postgrafting strategies to prevent relapse.

Published
2014
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174. Ultraviolet irradiation produces cytotoxic synergy and increased DNA interstrand crosslinking with cis- and trans-diamminedichloroplatinum(II).

Author

Swinnen, Lode J., Fisher, Susan G., and Erickson, Leonard C.

Abstract

There is indirect evidence to suggest that the excision-repair mechanism responsible for the removal of UV-induced thymine dimers may also play a role in the repair of -diamminedichloroplatinuin(II) (-DDP)-induced DNA adducts in both bacteria and mammalian cells. It was hypothesized that UV dimers and -DDP adducts, when present simultaneously, might compete for a common repair system. Colony survival assays were performed in HT-29 human colon carcinoma cells exposed either to -DDP alone or to -DDP immediately followed by UV exposure. Progressively greater cytotoxic synergy with both increasing UV dose and -DDP dose was observed, to a point of saturation beyond which further toxicity was purely additive. Alkaline elution analyses for DNA interstrand crosslinking were performed 6 h after exposure. An approximate doubling in crosslink frequency, relative to -DDP alone, was found in cells exposed to -DDP plus UV ( = 0.002). Since -DDP produces both inter- and intrastrand DNA crosslinks similar studies were performed with -DDP, which is incapable of producing intrastrand crosslinks, but does produce interstrand crosslinks. Cytotoxic synergy and increased interstrand crosslinking again resulted from the addition of UV exposure, but not to the same extent as seen with -DDP. These data support the hypothesis that -DDP induced DNA adducts are, at least in part, removed by an excision-repair mechanism. The similar but quantitatively smaller effects with -DDP suggest that intrastrand crosslink removal may also occur by this mechanism. [ABSTRACT FROM PUBLISHER]

Published
1989

175. Allogeneic Transplantation for Philadelphia Chromosome-Positive Acute Lymphoblastic Leukemia with Post-Transplantation Cyclophosphamide: Assessing the Importance of Conditioning Regimen, Donor Choice, and Tyrosine Kinase Inhibitor Use

Author

Webster, Jonathan, Luznik, Leo, Tsai, Hua-Ling, Imus, Philip H., DeZern, Amy E., Pratz, Keith W., Levis, Mark, Gojo, Ivana, Showel, Margaret M., Prince, Gabrielle T., Bolanos-Meade, Javier, Gondek, Lukasz P., Ghiaur, Gabriel, Dalton, William Brian, Jain, Tania, Fuchs, Ephraim J., Gladstone, Douglas E, Gocke, Christian B., Ali, Abbas Abbas, Huff, Carol Ann, Borrello, Ivan M., Swinnen, Lode J., Wagner-Johnston, Nina D., Ambinder, Richard F., Jones, Richard J., and Smith, B. Douglas

Abstract

Webster: Amgen: Consultancy; Pfizer: Consultancy. Luznik:WindMil Therapeutics: Patents & Royalties: Patent holder; Genentech: Research Funding; Merck: Research Funding, Speakers Bureau; AbbVie: Consultancy. DeZern:Abbvie: Consultancy; Astex: Research Funding; MEI: Consultancy; Celgene: Consultancy, Honoraria. Pratz:Jazz Pharmaceutical: Consultancy; Millennium: Research Funding; Daiichi Sankyo: Research Funding; Agios: Other: Scientific Advisory Board, Research Funding; Celgene: Other: Scientific Advisory Board; Boston BioMedical: Consultancy; Astellas: Other: Scientific Advisory Board, Research Funding; AbbVie: Other: Scientific Advisory Board, Research Funding. Levis:Astellas: Honoraria, Research Funding; Menarini: Honoraria; Amgen: Honoraria; FujiFilm: Honoraria, Research Funding; Daiichi-Sankyo: Honoraria. Gojo:Amgen: Research Funding; Merck: Research Funding; Genentech: Research Funding; BMS: Membership on an entity's Board of Directors or advisory committees; Amphivena: Research Funding. Bolanos-Meade:Incyte: Other: DSMB Fees. Dalton:Eli Lilly: Research Funding; AbbVie: Research Funding. Jain:Takeda: Consultancy, Honoraria; Bristol Myer Squibb: Other: for advisory board participation; CareDx: Other: Advisory Board. Ali:Celgene: Membership on an entity's Board of Directors or advisory committees. Borrello:Celgene: Research Funding; Aduro: Patents & Royalties; WindMIL Therapeutics: Other: Founder , Research Funding. Wagner-Johnston:ADC Therapeutics, Regeneron, CALIB-R, Verastem: Membership on an entity's Board of Directors or advisory committees. Smith:Celgene: Consultancy, Membership on an entity's Board of Directors or advisory committees; Agios: Consultancy, Membership on an entity's Board of Directors or advisory committees; Jazz: Consultancy, Membership on an entity's Board of Directors or advisory committees; Novartis: Consultancy, Membership on an entity's Board of Directors or advisory committees; Pfizer: Consultancy, Membership on an entity's Board of Directors or advisory committees.

Published
2020
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176. Epstein–Barr viral load as a marker of lymphoma in AIDS patients

Author

Fan, Hongxin, Kim, Seong Cheol, Chima, Chukwuemeka O., Israel, Bruce F., Lawless, Kathleen M., Eagan, Phyllis A., Elmore, Sandra, Moore, Dominic T., Schichman, Steven A., Swinnen, Lode J., and Gulley, Margaret L.

Abstract

Epstein–Barr virus (EBV) is implicated in the pathogenesis of acquired immunodeficiency syndrome (AIDS) lymphoma, and viral DNA is present within the malignant cells in about half of affected patients. We examined the extent to which EBV viral load is elevated in the plasma of AIDS lymphoma patients compared to AIDS patients with opportunistic infections. Sixty‐one AIDS patients were studied including 35 with lymphoma (24 non‐Hodgkin, six Hodgkin, and five brain lymphoma) and 26 with various opportunistic infections. In situ hybridization revealed EBV encoded RNA (EBER) expression in the malignant cells of 17/28 AIDS lymphomas (61%). In 232 serial plasma samples from 35 lymphoma patients and in 128 samples from AIDS controls, EBV viral load was assayed by quantitative‐polymerase chain reaction (Q‐PCR) using a TaqMan probe targeting the BamH1W sequence. EBV was detected in plasma from all 17 EBER‐positive AIDS lymphoma patients, with viral loads ranging from 34 to 1,500,000 copies per ml (median 3,210). Viral load usually fell rapidly upon initiation of lymphoma therapy and remained undetectable except in two patients with persistent tumor. In 11 AIDS patients, whose lymphoma lacked EBER expression, and in 26 control patients without lymphoma, levels of EBV in plasma were usually low or undetectable (range 0–1,995 and 0–2,409, median 0 and 0, respectively). There was no association between EBV viral load and human immunodeficiency virus (HIV) load or CD4 count. In conclusion, EBV viral load shows promise as a tool to assist in diagnosis and management of EBV‐related lymphoma patients. J. Med. Virol. 75:59–69, 2005. © 2005 Wiley‐Liss, Inc.

Published
2005
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177. An Open Label Trial of Sustained-release Cytarabine (DepoCyt™) for the Intrathecal Treatment of Solid Tumor Neoplastic Meningitis

Author

Jaeckle, Kurt A., Batchelor, Tracy, O'Day, Steven J., Phuphanich, Surasak, New, Pamela, Lesser, Glenn, Cohn, Allen, Gilbert, Mark, Aiken, Robert, Heros, Deborah, Rogers, Lisa, Wong, Eric, Fulton, Dorcas, Gutheil, John C., Baidas, Said, Kennedy, Julia M., Mason, Warren, Moots, Paul, Russell, Christy, and Swinnen, Lode J.

Abstract

Drugs currently available for intrathecal administration are cleared rapidly from the CSF. DepoCyt is a slow-release formulation of cytarabine that maintains cytotoxic concentrations of free cytarabine in the CSF for >14 days following a single injection. DepoCyt was administered to 110 patients with a diagnosis of neoplastic meningitis based on either a positive CSF cytology (76) or neurologic and CT or MRI scan findings sufficient to document neoplastic meningitis (34). Patients were treated with DepoCyt 50 mg every 2 weeks for 1 month of induction therapy by either lumbar puncture (LP) or intraventricular (IVT) injection. Patients without neurologic progression were candidates to receive an additional 3 months of consolidation therapy. All patients received dexamethasone 4 mg BID on days 1–5 of each cycle. Median time to neurologic progression was 55 days; median overall survival was 95 days. Among the 76 patients with a positive CSF cytology at baseline, 70 were evaluable for response, and of this group19 (27%) attained the criteria for response (cytologic response in the absence of neurologic progression). The most important adverse events were headache and arachnoiditis. When drug-related, these were largely low grade, transient, and reversible. Drug-related grade 3 headache occurred on 4% of cycles; grade 3 or 4 arachnoiditis occurred on 6% of cycles. No cumulative toxicity was observed. DepoCyt injected once every 2 weeks produced a response-rate comparable to that previously reported for methotrexate given twice a week. The once in every 2-week-dosing interval offers an advantage over conventional schedules (2–3 doses/week) used for other agents available for intrathecal injection.

Published
2002
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178. Prospective SPECT-CT Organ Dosimetry-Driven Radiation-Absorbed Dose Escalation Using the In-111 (111 In)/Yttrium 90 (90 Y) Ibritumomab Tiuxetan (Zevalin ®) Theranostic Pair in Patients with Lymphoma at Myeloablative Dose Levels.

Author

Wahl, Richard L., Frey, Eric C., Jacene, Heather A., Kahl, Brad S., Piantadosi, Steven, Bianco, Jesus A., Hammes, Richard J., Jung, Miah, Kasecamp, Wayne, He, Bin, Sgouros, George, Flinn, Ian W., and Swinnen, Lode J.

Subjects
LYMPHOMA treatment, THERAPEUTIC use of monoclonal antibodies, RADIOISOTOPE therapy, PILOT projects, CANCER relapse, ANTINEOPLASTIC agents, CANCER patients, TREATMENT effectiveness, SINGLE-photon emission computed tomography, RADIATION doses, DESCRIPTIVE statistics, COMBINED modality therapy, HEMATOPOIETIC stem cell transplantation, DRUG side effects, RADIATION dosimetry, RADIOIMMUNOTHERAPY, LONGITUDINAL method
Abstract

Simple Summary: We prospectively evaluated the feasibility of SPECT-CT/planar organ dosimetry-based radiation dose escalation radioimmunotherapy in patients with recurrent non-Hodgkin's lymphoma using the theranostic pair of 111In and 90Y anti-CD20 ibritumomab tiuxetan (Zevalin®) at myeloablative radiation-absorbed doses with autologous stem cell support. Unlike most routine dose escalation approaches, our approach used patient-individualized measurements of organ radiation absorbed dose from the tracer study, with patient-specific adjustments of the injected therapy dose to deliver a pre-specified radiation absorbed dose to the liver. Our approach was feasible, stem cell engraftment was swift, resulted in an 89% tumor response rate in treated patients, demonstrated over 3 fold variability in liver dosimetry/injected activity among patients, allowed us to exceed the FDA approved administered activity by over 5 fold and demonstrated the normal liver maximum tolerated dose to exceed 28 Gy. Dose escalation was not continued due to lack of drug availability. With modern dosimetry approaches, patient specific dosimetry-driven radiation dose escalation is feasible, allows adjustment of administered activity for heterogeneous pharmacokinetics and allows marked dose escalation vs. non-dosimetry driven approaches. Purpose: We prospectively evaluated the feasibility of SPECT-CT/planar organ dosimetry-based radiation dose escalation radioimmunotherapy in patients with recurrent non-Hodgkin's lymphoma using the theranostic pair of 111In and 90Y anti-CD20 ibritumomab tiuxetan (Zevalin®) at myeloablative radiation-absorbed doses with autologous stem cell support. We also assessed acute non-hematopoietic toxicity and early tumor response in this two-center outpatient study. Methods: 24 patients with CD20-positive relapsed or refractory rituximab-sensitive, low-grade, mantle cell, or diffuse large-cell NHL, with normal organ function, platelet counts > 75,000/mm3, and <35% tumor involvement in the marrow were treated with Rituximab (375 mg/m2) weekly for 4 consecutive weeks, then one dose of cyclophosphamide 2.5 g/m2 with filgrastim 10 mcg/kg/day until stem cell collection. Of these, 18 patients with successful stem cell collection (at least 2 × 106 CD34 cells/kg) proceeded to RIT. A dosimetric administration of 111In ibritumomab tiuxetan (185 MBq) followed by five sequential quantitative planar and one SPECT/CT scan was used to determine predicted organ radiation-absorbed dose. Two weeks later, 90Y ibritumomab tiuxetan was administered in an outpatient setting at a cohort- and patient-specific predicted organ radiation-absorbed dose guided by a Continuous Response Assessment (CRM) methodology with the following cohorts for dose escalation: 14.8 MBq/kg, and targeted 18, 24, 28, and 30.5 Gy to the liver. Autologous stem cell infusion occurred when the estimated marrow radiation-absorbed dose rate was predicted to be <1 cGy/h. Feasibility, short-term toxicities, and tumor response were assessed. Results: Patient-specific hybrid SPECT/CT + planar organ dosimetry was feasible in all 18 cases and used to determine the patient-specific therapeutic dose and guide dose escalation (26.8 ± 7.3 MBq/kg (mean), 26.3 MBq/kg (median) of 90Y (range: 12.1–41.4 MBq/kg)) of ibritumomab tiuxetan that was required to deliver 10 Gy to the liver. Infused stem cells engrafted rapidly. The most common treatment-related toxicities were hematological and were reversible following stem cell infusion. No significant hepatotoxicity was seen. One patient died from probable treatment-related causes—pneumonia at day 27 post-transplant. One patient at dose level 18 Gy developed myelodysplastic syndrome (MDS), 4 patients required admission post-90Y RIT for febrile neutropenia, 16/18 patients receiving 90Y ibritumomab tiuxetan (89%) responded to the therapy, with 13 CR (72%) and 3/18 PR (17%), at 60 days post-treatment. Two patients had progressive disease at sixty days. One patient was lost to follow-up. Median time to progression was estimated to be at least 13 months. MTD to the liver is greater than 28 Gy, but the MTD was not reached as the study was terminated due to unexpected discontinuation of availability of the therapeutic agent. Conclusions: Patient-specific outpatient 90Y ibritumomab tiuxetan RIT with myeloablative doses of RIT up to a targeted 30.5 Gy to the liver is feasible, guided by prospective SPECT/CT + planar imaging with the theranostic pair of 111In and 90Y anti-CD20, with outpatient autologous stem cell transplant support. Administered activity over 5 times the standard FDA-approved activity was well-tolerated. The non-hematopoietic MTD in this study exceeds 28 Gy to the liver. Initial tumor responses were common at all dose levels. This study supports the feasibility of organ dosimetry-driven patient-specific dose escalation in the treatment of NHL with stem cell transplant and provides additional information on the radiation tolerance of the normal liver to radiopharmaceutical therapy. [ABSTRACT FROM AUTHOR]

Published
2021
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179. Long Term Follow up of the Resort Study (E4402): A Randomized Phase III Study Comparing Two Different Rituximab Dosing Strategies for Low Tumor Burden Follicular Lymphoma

Author

Kahl, Brad S., Hong, Fangxin, Peterson, Christopher, Swinnen, Lode J., Habermann, Thomas M., Schuster, Stephen J, Weiss, Matthias, Fishkin, Paul A S, Ehmann, W. Christopher, Fenske, Timothy S., and Williams, Michael E.

Abstract

E4402 was a randomized phase III study comparing two different rituximab dosing strategies for patients with previously untreated, low tumor burden follicular lymphoma (FL). The primary endpoint was time to treatment failure. The initial publication (Kahl, JCO 2014) demonstrated that a retreatment strategy utilized less drug and produced comparable time to treatment failure compared to a maintenance strategy. Here we provide long term follow up results, focusing on response duration, time to first cytotoxic therapy, overall survival, and risk of histologic transformation.

Published
2021
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180. Nonmyeloablative Allogeneic Transplantation in First Remission for Philadelphia Chromosome-Negative B-Cell Acute Lymphoblastic Leukemia with Post-Transplantation Cyclophosphamide: Outcomes By Receipt of Pre-Transplant Blinatumomab

Author

Webster, Jonathan, Smith, B. Douglas, DeZern, Amy E., Ambinder, Alexander J., Levis, Mark, Showel, Margaret M., Prince, Gabrielle T., Gondek, Lukasz P., Ghiaur, Gabriel, Dalton, William Brian, Hourigan, Christopher S., Jain, Tania, Gladstone, Douglas E, Luznik, Leo, Imus, Philip H., Bolanos-Meade, Javier, Fuchs, Ephraim J., Gocke, Christian B., Ali, Abbas Abbas, Huff, Carol Ann, Borrello, Ivan M., Swinnen, Lode J., Wagner-Johnston, Nina D., Ambinder, Richard F., Jones, Richard J., and Gojo, Ivana

Abstract

Background:The benefit of allogeneic blood or marrow transplantation (alloBMT) following myeloablative conditioning (MAC) in first complete remission (CR1) compared to chemotherapy has been demonstrated in a randomized trial for adults with acute lymphoblastic leukemia (ALL). Persistence of measurable residual disease (MRD) prior to alloBMT confers an increased risk of relapse. Blinatumomab eradicates persistent or recurrent MRD at levels ≥10 -3in 78% of B ALL. However, post-hoc analyses of patients who have undergone alloBMT following blinatumomab for MRD demonstrate non-relapse mortality (NRM) of 36.5%. NRM following nonmyeloablative (NMAC) alloBMT with high-dose post-transplantation cyclophosphamide (PTCy) is just 11%. Given broadly similar outcomes between HLA-matched MAC alloBMT and HLA-haploidentical NMAC alloBMT following PTCy, we have shifted to using exclusively NMAC alloBMT with PTCy and sought to explore outcomes depending on receipt of pre-transplant blinatumomab.

Published
2021
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181. Increased risk of lymphoproliferative disorders following the use of OKT3 in cardiac transplantation

Author

Swinnen, Lode J., Costanzo‐Nordin, Maria R., Fisher, Susan G., O'Sullivan, E. Jeanne, Johnson, Maryl R., Heroux, Alain L., Dizikes, George J., Pifarre, Roque, and Fisher, Richard I.

Abstract

A sudden increase in the incidence of post‐transplant lymphoproliferative disorder (PTLD) in our cardiac transplant program prompted a retrospective study of 154 consecutive patients to identify predictive variables. The increase was found to be temporally and statistically related to the introduction of the immunosuppressive antibody OKT3. While effective in the treatment of refractory rejection, the value of OKT3 used prophylactically at the time of transplantation remains to be clearly established. Among 75 patients who had not received the drug, PTLD developed in 1 (1.3%) compared with 9 of 79 patients who had (11.4%), a ninefold higher incidence (p = 0.01). The following factors were assessed in a multivariate model: sex; race; age; weight; reason for transplant; rejection episodes; mean cyclosporine level; use and cumulative dose of OKT3, ATG, and steroids. Only the use of OKT3 was significantly associated with development of PTLD (p = 0.001). Increasing risk with increasing dose was evident, in that 4 of 65 patients (6.2%) who received one course of OKT3 (≤ 75 mg) developed PTLD, while 5 of 14 patients (35.7%) who received more than 1 course did so (p < 0.001). Over the year since the study was completed, two more cases of PTLD have arisen in the group receiving one course of the drug, resulting in an incidence of 9.2% after a single prophylactic course of OKT3 (p=0.03), and an overall incidence of 13.9%. Withholding cyclosporine during the prophylactic course did not reduce the risk of PTLD. Among patients who had received > 75 mg OKT3, all but one presented with widespread, rapidly progressive disease resulting in early organ failure and death. Among the 14 patients who had received > 75 mg, the interval between courses for those who developed PTLD was much shorter (med 13 days, range 0‐33) than for those who did not (med 115 days, range 8‐884, p = 0.02). There was a strong inverse correlation between total OKT3 dose and the time to appearance of PTLD following transplantation; a mean of 11 ± 4.9 mos. for patients who had received one course, compared to a mean of 1.3 ± 0.45 mos. for those who had received two (p < 0.001). It can be concluded that the addition of OKT3 to a triple drug immunosuppressive regimen increases the incidence of PTLD after cardiac transplantation, and that both the risk and clinical pattern of disease are dose related. No conclusions regarding the mechanism for this increase can be drawn from these data. It is suggested that the risks and benefits of prophylactic OKT3 administration be reassessed, that short intervals between courses be avoided, and that patients who have received the drug be monitored closely for indications of PTLD.

Published
1992
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182. Cisplatin preceded by concurrent cytarabine and hydroxyurea: a pilot study based on an in vitro model

Author

Albain, Kathy S., Swinnen, Lode J., Erickson, Leonard C., Stiff, Patrick J., and Fischer, Richard I.

Abstract

As previously reported, cytotoxic synergy is produced when clinically achievable concentrations of cytarabine (Ara-C) and hydroxyurea (HU) are used as potential inhibitors of in vitro DNA repair in cisplatin (cis-Pt)-treated human colon carcinoma cells. This pilot study was subsequently designed to duplicate the in vitro dose and schedule and to determine the toxicity of this three-drug combination in two cohorts of patients. 21 patients had received prior chemotherapy and 19 were not previously treated. All patients had refractory solid tumors. They received monthly cycles of an oral loading dose of 800 mg/m2 HU followed every 2 h by 6 oral doses of 400 mg/m2, a 12-h continuous infusion of 200 or 250 mg/m2/h Ara-C concurrent with the HU, and then 100 mg/m2cis-Pt over 1 h. A total of 95 cycles were given with the expected toxicities of nausea and vomiting and fatigue but no major acute toxicity observed. Thrombocytopenia was significant but transient and was dose-limiting only for patients who had received prior therapy. The median platelet nadir after one cycle was 43,000/µl for all patients and 67,000/µl for those who had not undergone prior treatment. Azotemia was treatment-limiting in responding and stable patients, suggesting the possibility of synergistic nephrotoxicity. Interestingly, there were early transient rises in both uric acid and lactate dehydrogenase (LDH). Partial responses were seen in 9 of 32 patients with measurable disease and there was significant improvement in 5 of 8 patients with only evaluable disease. The responses or improvement occurred in patients with non-small-cell lung cancer, breast carcinoma, glioblastoma, ovarian carcinoma, small-cell lung cancer, and mesothelioma. Of these 14 patients, 9 had failed prior chemotherapy regimens. Significantly, responses were observed in 3 of 8 patients who had previously receivedcis-Pt, suggesting that the HU/Ara-C combination modulatedcis-Pt resistance. Because of these encouraging results, a second pilot study has been initiated with modifications dictated by the toxicity issues raised in this trial.

Published
1990
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183. Diagnosis and treatment of organ transplantrelated lymphoma

Author

Swinnen, Lode J.

Abstract

The incidence and pathogenesis of posttransplant lymphoproliferations are examined in relation to the nature of the transplanted organ and to the use of specific immunosuppressive regimens. Clinical manifestations, pathologic features, and diagnostic considerations are summarized, particularly emphasizing those aspects that differ significantly from classic non-Hodgkin's lymphoma. The relevance of recently developed molecular methods for determining clonal composition to diagnosis and treatment is outlined. A basis for the selection of therapeutic options, including reduction in immunosuppression, surgery, radiation therapy, or chemotherapy, is proposed, and novel approaches to the treatment of organ transplant-related lymphoma are reviewed.

Published
1998

184. Aggressive Treatment for Postcardiac Transplant Lymphoproliferation

Author

Swinnen, Lode J., Mullen, G.Martin, Carr, Thomas J., Costanzo, Maria R., and Fisher, Richard I.

Abstract

Posttransplant lymphoprolKerative disorder (PTLD) is a frequently fatal complication of organ transplantation, occurring in 2% to 6% of cardiac recipients. Treatment remains poorly defined. Reduction in immunosuppression is effective in a proportion of cases, but mortality on the order of 80% is reported for patients requiring chemotherapy. The reason for such poor outcomes is unclear, but may be partly caused by the concomitant use of immunosuppressives. Nineteen consecutive cardiac recipients with PTLD were studied retrospectively in terms of clinical features and outcome. Patients were managed according to a uniform treatment approach. Initial therapy was a trial of reduced immunosuppression with concomitant acyclovir followed, if unsuccessful, by aggressive combination chemotherapy. The regimen used was predominantly ProMACE-CytaBOM. Six patients with phe-notypicalty polyclonal PTLD presented less than 6 months after transplantation (median 6 weeks). Only 1 of 4 (25%) treated patients responded to reduced immunosuppression; the remainder died of multiorgan failure. Thirteen patients presented with phenotypically monoclonal disease ≥6 months after transplantation. In 8 of 12 (75%) treated patients initial therapy was reduction in immunosuppression. None achieved complete remission (CR) and 2 experienced fatal rejection. Two patients achieved durable surgical CR. The remaining 8 patients received chemotherapy; 2 of 8 (25%) died during treatment, 6 of 8 (75%) achieved CR. None have relapsed, at a median duration of follow-up of 38 months. Neutropenic sepsis and subclinical doxorubicin cardiotoxicity at a mean cumulative dose of 63 mg/m2were the principal toxicities. Our data indicate that aggressive chemotherapy is both feasible and effective in phenotypically monoclonal PTLD refractory to reduced immunosuppression. ProMACE-CytaBOM is well suited to cardiac recipients, minimizing doxorubicin exposure and obviating the need for concurrent immunosuppressives.

Published
1995
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185. BCL-2 But Not Its Epstein-Barr Virus-Encoded Homologue, BHRF1, Is Commonly Expressed in Posttransplantation Lymphoproliferative Disorders

Author

Murray, Paul G., Swinnen, Lode J., Constandinou, Christothea M., Pyle, Joseph M., Carr, Thomas J., Hardwick, J.Marie, and Ambinder, Richard F.

Abstract

Posttransplantation lymphoproliferative disease (PTLD) is virtually always associated with Epstein-Barr virus (EBV) infection. BCL-2 and other proteins that confer resistance to apoptosis have been implicated in the pathogenesis of a variety of malignancies including lymphomas. One EBV protein, BHRF1, is a homologue of BCL-2, whereas another, the latency membrane protein 1 (LMP-1), upregulates BCL-2 expression in vitro. In the present study, we used immunohistochemistry to study the expression of these viral and cellular proteins as well as a variety of other EBV-encoded proteins in PTLD. BHRF1 was not detected in any PTLD specimen, whereas BCL-2 was shown in 12 of 17 lesions examined. With one exception, all LMP1-positive cases also expressed BCL-2 and the absence of LMP1 was always associated with a lack of BCL-2 expression. The results do not support a role for the EBV homologue of BCL-2 in PTLD, but they do support a role for viral induction of BCL-2 expression.

Published
1996
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186. “Allogeneic blood or marrow transplant with non-myeloablative conditioning and high dose cyclophosphamide-based graft-versus-host disease prophylaxis for secondary central nervous system lymphoma”

Author

Sterling, Cole H, Tsai, Hua-Ling, Holdhoff, Matthias, Bolaños-Meade, Javier, Luznik, Leo, Fuchs, Ephraim J, Huff, Carol Ann, Gocke, Christian B, Ali, Syed Abbas, Borrello, Ivan M, Varadhan, Ravi, Jones, Richard J, Gladstone, Douglas E, Ambinder, Richard F, Wagner-Johnston, Nina, Swinnen, Lode J, and Imus, Philip H

Abstract

•We reviewed outcomes in 20 patients with secondary CNS lymphoma undergoing alloBMT.•All received non-myeloablative conditioning with post-transplant cyclophosphamide.•Prolonged disease-free survival was achieved in ∼50% of patients.•Myeloablative conditioning and CNS radiotherapy were not required for remission.

Published
2021
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187. Interim positron emission tomography scans in diffuse large B-cell lymphoma: an independent expert nuclear medicine evaluation of the Eastern Cooperative Oncology Group E3404 study

Author

Horning, Sandra J., Juweid, Malik E., Schöder, Heiko, Wiseman, Gregory, McMillan, Alex, Swinnen, Lode J., Advani, Ranjana, Gascoyne, Randy, and Quon, Andrew

Abstract

Positive interim positron emission tomography (PET) scans are thought to be associated with inferior outcomes in diffuse large B-cell lymphoma. In the E3404 diffuse large B-cell lymphoma study, PET scans at baseline and after 3 cycles of rituximab, cyclophosphamide, doxorubicin, vincristine, and prednisone were centrally reviewed by a single reader. To determine the reproducibility of interim PET interpretation, an expert panel of 3 external nuclear medicine physicians visually scored baseline and interim PET scans independently and were blinded to clinical information. The binary Eastern Cooperative Oncology Group (ECOG) study criteria were based on modifications of the Harmonization Criteria; the London criteria were also applied. Of 38 interim scans, agreement was complete in 68% and 71% by ECOG and London criteria, respectively. The range of PET+ interim scans was 16% to 34% (P = not significant) by reviewer. Moderate consistency of reviews was observed: κ statistic = 0.445 using ECOG criteria, and κ statistic = 0.502 using London criteria. These data, showing only moderate reproducibility among nuclear medicine experts, indicate the need to standardize PET interpretation in research and practice. This trial was registered at www.clinicaltrials.gov as #NCT00274924.

Published
2010
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188. Allogenic Stem Cell Transplantation for Secondary CNS Lymphoma: A Retrospective Review of 21 Patients

Author

Sterling, Cole, Wagner-Johnston, Nina D., Gladstone, Douglas E, Ambinder, Richard F., Swinnen, Lode J., and Imus, Philip Hollingsworth

Abstract

Wagner-Johnston: ADC Therapeutics: Membership on an entity's Board of Directors or advisory committees; Jannsen: Membership on an entity's Board of Directors or advisory committees; Gilead: Membership on an entity's Board of Directors or advisory committees; Bayer: Membership on an entity's Board of Directors or advisory committees. Swinnen:Pharmacyclics: Consultancy; AbbVie: Consultancy.

Published
2019
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190. Characteristics and Outcomes of Patients with Double-Protein Expression in Limited Stage Diffuse Large B-Cell Lymphoma (DLBCL): Analysis of SWOG Study S1001 (NCT01359592)

Author

Stephens, Deborah M., Li, Hongli, Persky, Daniel, Park, Steven I., Bartlett, Nancy L., Swinnen, Lode J., Casulo, Carla, Winegarden, Jerome D., Constine, Louis S., Fitzgerald, Thomas J., Leonard, John P., Kahl, Brad S, Leblanc, Michael L., Song, Joo Y., Fisher, Richard I., Rimsza, Lisa M., Smith, Sonali M., and Friedberg, Jonathan W.

Abstract

Introduction

Published
2017
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191. Mismatched donor transplantation with post-transplantation cyclophosphamide for advanced cutaneous T-cell lymphoma: a single-center retrospective study.

Author

Hughes, Michael S., Sterling, Cole H., Varadhan, Ravi, Ambinder, Richard F., Jones, Richard J., Sweren, Ronald J., Rozati, Sima, Bolaños-Meade, Javier, Luznik, Leo, Imus, Philip H., Ali, Syed Abbas, Borrello, Ivan M., Huff, Carol Ann, T., Jain, Ambinder, Alexander, DeZern, Amy E., Gocke, Christian B., Gladstone, Douglas E., Swinnen, Lode J., and Wagner-Johnston, Nina D.

Subjects
*CUTANEOUS T-cell lymphoma, *SEZARY syndrome, *CORD blood transplantation, *HEMATOPOIETIC stem cell transplantation
Abstract

Two individuals (patients 7 and 8) received immune checkpoint inhibition (ICI) prior to BMT; patient 7 received anti-CTLA-4 and anti-PD-1 combination therapy, and patient 8 received anti-PD-L1 and interferon combination therapy. From 2003 to 2020, eight patients received partially mismatched donor BMT for relapsed/refractory MF/SS. Seven patients received grafts from HLA-haploidentical related donors. Primary cutaneous T-cell lymphomas (CTCLs), a heterogeneous group of extranodal non-Hodgkin lymphomas involving the skin, are dominated by two main subtypes: mycosis fungoides (MF) and Sézary syndrome (SS) [[1]]. An eighth patient (patient 5) experienced graft failure after double unrelated donor umbilical cord blood transplantation and within 6 months underwent partially mismatched unrelated donor BMT. [Extracted from the article]

Published
2022
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192. Thrombotic Microangiopathy after Post-Transplantation Cyclophosphamide-Based Graft-versus-Host Disease Prophylaxis.

Author

Imus, Philip H., Tsai, Hua-Ling, DeZern, Amy E., Jerde, Kevin, Swinnen, Lode J., Bolaños-Meade, Javier, Luznik, Leo, Fuchs, Ephraim J., Wagner-Johnston, Nina, Huff, Carol Ann, Gladstone, Douglas E., Ambinder, Richard F., Gocke, Christian B., Ali, Syed Abbas, Borrello, Ivan M., Varadhan, Ravi, Brodsky, Robert, and Jones, Richard J.

Subjects
*THROMBOTIC microangiopathies, *GRAFT versus host disease, *BONE marrow transplantation, *BUSULFAN, *RENAL replacement therapy, *ECULIZUMAB, *LACTATE dehydrogenase, *ALEMTUZUMAB
Abstract

• Transplant-associated thrombotic microangiopathy (taTMA) is a serious complication of allogeneic bone marrow transplantation. • The incidence of taTMA is low at 1.4% using post-transplant cyclophosphamide (PTCy)-based graft-versus-host disease prophylaxis. • Recipient-donor mismatch is unlikely to be a risk factor when PTCy is used. Transplant-associated thrombotic microangiopathy (taTMA) is a systemic vascular illness associated with significant morbidity and mortality, resulting from a convergence of risk factors after allogeneic blood or marrow transplantation (alloBMT). The diagnosis of taTMA has been a challenge, but most criteria include an elevated lactate dehydrogenase (LDH), low haptoglobin, and schistocytes on peripheral blood smear. We performed a retrospective review of the 678 consecutive adults who received high-dose post-transplantation cyclophosphamide (PTCy)-based graft-versus-host disease (GVHD) prophylaxis between January 1, 2015, and August 31, 2018. In April 2016, we initiated a monitoring program of weekly LDH and haptoglobin measurements and blood smears when those 2 parameters were both abnormal on all of our adult patients undergoing alloBMT for hematologic malignancies. During the entire period, the 1-year cumulative incidence of taTMA was 1.4% (95% confidence interval, 0.5% to 2.3%). Eight patients were taking tacrolimus at the time of diagnosis, and 1 was not on any immunosuppression. Eight of 9 patients (89%) were hypertensive. Four patients had invasive infections at the time of diagnosis, 4 patients required renal replacement therapy, and 5 of 9 patients were neurologically impaired. Eculizumab was given to 6 patients (0.9%), of whom 2 died and 4 recovered with resolution of end-organ dysfunction. The paucity of events made the determination of risk factors difficult; however, the low incidence of taTMA in this cohort may be related to the limited use of myeloablative conditioning regimens, low incidence of severe GVHD, and use of PTCy. PTCy-based GVHD prophylaxis appears to be associated with a low incidence of severe taTMA. [ABSTRACT FROM AUTHOR]

Published
2020
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193. Shortened-Duration Immunosuppressive Therapy after Nonmyeloablative, Related HLA-Haploidentical or Unrelated Peripheral Blood Grafts and Post-Transplantation Cyclophosphamide.

Author

DeZern, Amy E., Elmariah, Hany, Zahurak, Marianna, Rosner, Gary L., Gladstone, Douglas E., Ali, Syed Abbas, Huff, Carol Ann, Swinnen, Lode J., Imus, Phil, Borrello, Ivan, Wagner-Johnston, Nina D., Ambinder, Richard F., Brodsky, Robert A., Cooke, Kenneth, Luznik, Leo, Fuchs, Ephraim J., Bolaños-Meade, Javier, and Jones, Richard J.

Subjects
*IMMUNOSUPPRESSIVE agents, *ACUTE myeloid leukemia, *CYCLOPHOSPHAMIDE, *STEM cell transplantation, *CELL transplantation
Abstract

• This safety and feasibility study of haploidentical peripheral blood transplantation and unrelated donors demonstrates that a substantial subset of patients can discontinue immunosuppression as graft-versus-host disease prophylaxis as early as day 60. • Shortened-duration immunosuppression may decrease the risk of relapse and enable earlier and/or more effective post-transplantation therapies to further improve disease-related outcomes. The report includes the proportion of patients who required resumption of immunosuppression. With post-transplantation cyclophosphamide (PTCy) as graft-versus-host disease (GVHD) prophylaxis, nonmyeloablative (NMA) HLA-haploidentical (haplo) and HLA-matched blood or marrow transplantation (BMT) have comparable outcomes. Previous reports have shown that discontinuation of immunosuppression (IS) as early as day 60 after infusion of a bone marrow (BM) haplo allograft with PTCy is feasible. There are certain diseases in which peripheral blood (PB) may be favored over BM, but given the higher rates of GVHD with PB, excessive GVHD is of increased concern. We report a completed, prospective single-center trial of stopping IS at days 90 and 60 after NMA PB stem cell transplantation (PBSCT). Between 12/2015-7/2018, 117 consecutive patients with hematologic malignancies associated with higher rates of graft failure after NMA conditioned BMT and PTCy, received NMA PB allografts on trial. The primary objective of this study was to evaluate the safety and feasibility of reduced‐duration IS (from day 5 through day 90 in the D90 cohort and through day 60 in the D60 cohort). Of the 117 patients (median age, 64 years; range, 22 to 78 years), the most common diagnoses were myelodysplastic syndrome (33%), acute myelogenous leukemia (with minimal residual disease or arising from an antecedent disorder) (32%), myeloproliferative neoplasms (19%), myeloma (9%), and chronic lymphoblastic leukemia (7%). Shortened IS was feasible in 75 patients (64%) overall. Ineligibility for shortened IS resulted most commonly from GVHD (17 patients), followed by early relapse (11 patients), nonrelapse mortality (NRM) (7 patients), patient/ physician preference (4 patients) or graft failure (3 patients). Of the 57 patients in the D90 cohort, 33 (58%) stopped IS early as planned, and among the 60 patients in the D60 cohort, 42 (70%) stopped IS early as planned. The graft failure rate was 2.6%. After IS cessation, the median time to diagnosis of grade II-IV acute GVHD was 21 days in the D90 cohort and 32 days in the D60 cohort, with almost all cases developing within 40 days. Approximately one-third of these patients resumed IS. All outcome measures were similar in the 2 cohorts and our historical outcomes with 180 days of IS. The cumulative incidence of grade III-IV acute GVHD was low, 2% in the D90 cohort and 7% in the D60 cohort. The incidence of severe chronic GVHD at 2 years was 9% in the D90 cohort and 5% in the D60 cohort. The 2-year overall survival was 67% for both the D90 and D60 cohorts. The 2-year progression-free survival was 47% for the D90 cohort and 52% for the D60 cohort, and the GVHD-free, relapse-free survival was <35% for both cohorts. These data suggest that reduced-duration IS in patients undergoing NMA PBSCT with PTCy is feasible and has an acceptable safety profile. © 2020 American Society for Transplantation and Cellular Therapy. Published by Elsevier Inc. [ABSTRACT FROM AUTHOR]

Published
2020
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194. Non-Myeloablative Allogeneic Transplantation with Post-Transplant Cyclophosphamide after Immune Checkpoint Inhibition for Classic Hodgkin Lymphoma: A Retrospective Cohort Study.

Author

Paul, Suman, Zahurak, Marianna, Luznik, Leo, Ambinder, Richard F., Fuchs, Ephraim J., Bolaños-Meade, Javier, Wagner-Johnston, Nina, Swinnen, Lode J., Schoch, Laura, Varadhan, Ravi, Jones, Richard J., and Gladstone, Douglas E.

Subjects
*HODGKIN'S disease, *IMMUNE checkpoint inhibitors, *PROGRAMMED cell death 1 receptors, *BONE marrow transplantation, *PROGNOSIS, *COHORT analysis, *ALEMTUZUMAB
Abstract

• Immune checkpoint inhibition (ICI) before allogeneic bone marrow transplantation (alloBMT) does not increase risk of graft-versus-host disease in patients receiving post-transplantation cyclophosphamide (PTCy). • ICI therapy before alloBMT with PTCy in patients with classic Hodgkin lymphoma may improve disease progression and survival compared with salvage chemotherapy before alloBMT. Immune checkpoint inhibitors (ICIs) are approved in relapsed classic Hodgkin lymphoma (cHL). The safety and effectiveness of allogeneic blood or marrow transplantation (alloBMT) in ICI-pretreated patients with cHL remain unclear. The aim of this study is to assess outcomes of patients with cHL receiving ICIs before alloBMT using post-transplantation cyclophosphamide (PTCy) graft-versus-host-disease (GVHD) prophylaxis. We performed a retrospective study of relapsed/refractory patients with cHL undergoing alloBMT with PTCy at Johns Hopkins between November 2004 and September 2019. Engraftment, GVHD incidence, nonrelapse mortality, progression-free survival (PFS), and overall survival (OS) were compared between patients receiving pre-alloBMT ICI or standard salvage chemotherapy. We identified 105 consecutive relapsed/refractory patients with cHL, of whom 37 (35.2%) received ICIs and 68 (64.7%) received chemotherapy without ICIs (no-ICI) before alloBMT. ICI and no-ICI patients experienced a 3-year estimated OS of 94% versus 78% (hazard ratio [HR], 0.35; 95% confidence interval [CI], 0.08 to 1.56; P =.17) and a 3-year estimated PFS of 90% and 65% (HR, 0.3; 95% CI, 0.09 to 1; P =.05), respectively. We observed no statically significant difference in the 12-month cumulative incidence of acute grade II to IV GVHD or in the 24-month incidence of chronic GVHD. ICIs do not increase acute or chronic GVHD incidence compared with salvage chemotherapy. Patients with cHL receiving ICIs prior to alloBMT experienced outstanding PFS and OS. Thus, ICI therapy is safe in patients with cHL when undergoing alloBMT with PTCy and may improve post-alloBMT disease progression and survival. [ABSTRACT FROM AUTHOR]

Published
2020
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195. Allogeneic Haploidentical Blood or Marrow Transplantation with Post-Transplantation Cyclophosphamide in Chronic Lymphocytic Leukemia.

Author

Paul, Suman, Tsai, Hua-Ling, Lowery, Patrick, Fuchs, Ephraim J., Luznik, Leo, Bolaños-Meade, Javier, Swinnen, Lode J., Shanbhag, Satish, Wagner-Johnston, Nina, Varadhan, Ravi, Ambinder, Richard F., Jones, Richard J., and Gladstone, Douglas E.

Subjects
*CHRONIC lymphocytic leukemia, *BONE marrow transplantation, *BONE marrow, *TRANSPLANTATION of organs, tissues, etc., *BLOOD
Abstract

• Outcomes of haploidentical allogeneic bone marrow transplantation (allo-BMT) may be similar to those reported for matched donor allo-BMT in patients with chronic lymphocytic leukemia (CLL). • Post-transplantation cyclophosphamide prophylaxis is associated with low rates of acute and chronic graft-versus-host disease. • Pre-allo-BMT bone marrow CLL involvement ≥20% hinders engraftment. • Unfavorable risk CLL prognostic features should not preclude the consideration of allo-BMT. Allogeneic blood or marrow transplantation (allo-BMT) remains the only treatment for chronic lymphocytic leukemia (CLL) with curative potential. Although post-transplantation cyclophosphamide (PTCy) reduces allo-BMT toxicity by decreasing the risk of graft-versus-host disease (GVHD), its effect on CLL allo-BMT outcomes is unknown. We studied 64 consecutive patients with CLL who underwent nonmyeloablative (NMA) haploidentical allo-BMT at Johns Hopkins Sidney Kimmel Comprehensive Cancer Center. In this cohort, the 4-year overall survival was 52% (95% confidence interval [CI], 40% to 68%), and progression-free survival was 37% (95% CI, 26% to 54%). Six patients experienced engraftment failure. PTCy prophylaxis was associated with a modest cumulative incidence of 1-year grade II-IV acute GVHD (27%; %95% CI, 15% to 38%) and %%%2-year chronic GVHD (17%; 95% CI, 7% to 26%). We demonstrate that NMA haploidentical allo-BMT with PTCy is a safe and effective treatment option. [ABSTRACT FROM AUTHOR]

Published
2020
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196. Severe Cytokine Release Syndrome after Haploidentical Peripheral Blood Stem Cell Transplantation.

Author

Imus, Philip H., Blackford, Amanda L., Bettinotti, Maria, Luznik, Leo, Fuchs, Ephraim J., Huff, Carol Ann, Gladstone, Douglas E., Ambinder, Richard F., Borrello, Ivan M., Fuchs, Robert J., Swinnen, Lode J., Wagner-Johnston, Nina, Gocke, Christian B., Ali, Syed Abbas, Bolaños-Meade, F. Javier, Jones, Richard J., and Dezern, Amy E

Subjects
*STEM cell transplantation, *BLOOD cells, *CELLULAR therapy, *OLDER patients
Abstract

• Cytokine release syndrome (CRS) occurs at day 0 to day +5 in 90% of haploidentical peripheral blood stem cell transplant recipients. • Overall survival in our cohort was 58% at 2 years, because most CRS was mild. • Older patients and those who received radiation therapy are more prone to severe CRS. • Nonrelapse mortality was 38% at 6 months among patients with severe CRS. Inflammatory cytokines released by activated lymphocytes and innate cells in the context of cellular therapy can cause fever, vasodilatation, and end-organ damage, collectively known as cytokine release syndrome (CRS). CRS can occur after allogeneic blood or marrow transplantation, but is especially prevalent after HLA-haploidentical (haplo) peripheral blood transplantation (PBT). We reviewed charts of all patients who underwent haplo-PBT between October 1, 2013, and September 1, 2017 and graded CRS in these patients. A total of 146 consecutive patients who underwent related haplo-PBT were analyzed. CRS occurred in 130 patients (89%), with most cases of mild severity (grade 0 to 2). Severe CRS (grade 3 to 5) occurred in 25 patients (17%). In this group with severe CRS, 13 patients had encephalopathy, 12 required hemodialysis, and 11 were intubated. Death from the immediate complications of CRS occurred in 6 patients (24% of the severe CRS group and 4% of the entire haplo-PBT cohort). The cumulative probability of nonrelapse mortality (NRM) was 38% at 6 months for the patients with severe CRS and 8% (121 of 146) in patients without severe CRS. In conclusion, CRS occurs in nearly 90% of haplo-PBTs. Older haplo-PBT recipients (odds ratio [OR], 2.4; 95% confidence interval [CI],.83 to 6.75; P =.11) and those with a history of radiation therapy (OR, 3.85; 95% CI, 1.32 to 11.24; P =.01) are at increased risk of developing severe CRS. Although most recipients of haplo-PBT develop CRS, <20% experience severe complications. The development of severe CRS is associated with a significantly increased risk of NRM. [ABSTRACT FROM AUTHOR]

Published
2019
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197. Development of Grade II Acute Graft-versus-Host Disease Is Associated with Improved Survival after Myeloablative HLA-Matched Bone Marrow Transplantation using Single-Agent Post-Transplant Cyclophosphamide.

Author

McCurdy, Shannon R., Kanakry, Christopher G., Tsai, Hua-Ling, Gojo, Ivana, Smith, B. Douglas, Gladstone, Douglas E., Bolaños-Meade, Javier, Borrello, Ivan, Matsui, William H., Swinnen, Lode J., Huff, Carol Ann, Brodsky, Robert A., Ambinder, Richard F., Fuchs, Ephraim J., Rosner, Gary L., Jones, Richard J., and Luznik, Leo

Subjects
*BONE marrow transplantation, *GRAFT versus host disease, *ACUTE diseases, *ORTHOPEDIC braces, *PROGRESSION-free survival, *HEMATOLOGIC malignancies
Abstract

• Grade II acute graft-versus-host disease is associated with improved overall and progression-free survival after HLA-matched BMT with post-transplant cyclophosphamide. • Grade II acute graft-versus-host disease is associated with decreased relapse, but no difference in nonrelapse mortality when using post-transplant cyclophosphamide. Post-transplant cyclophosphamide (PTCy) can be used as the sole immunosuppression after myeloablative conditioning (MAC) for HLA-matched bone marrow transplantation (BMT). However, the effects of graft-versus-host disease (GVHD) with this platform are undefined. We retrospectively analyzed 298 consecutive adult patients with hematologic malignancies who engrafted after MAC HLA-matched sibling donor (MSD; n = 187) or HLA-matched unrelated donor (MUD; n = 111) T-cell–replete BMT with PTCy 50 mg/kg on days +3 and +4. After MSD and MUD BMT, 35% and 57% of patients, respectively, developed grade II acute GVHD (aGVHD) by 100 days, 11% and 14% grade III to IV aGVHD by 100 days, and 9% and 16% chronic GVHD (cGVHD) by 1 year. In landmark analyses at 100 days after HLA-matched BMT, 4-year overall survival (OS) and progression-free survival (PFS) were 57% (95% confidence interval [CI],.49 to.67) and 40% (95% CI,.31 to.51) in patients without grades II to IV aGVHD, and 68% (95% CI,.59 to.78) and 54% (95% CI,.44 to.65) in patients with grade II aGVHD. In adjusted time-dependent multivariable analyses, grade II aGVHD was associated with improved OS (hazard ratio,.58; 95% CI,.37 to.89; P =.01) and PFS (hazard ratio,.50; 95% CI,.34 to.74; P <.001) after HLA-matched BMT with PTCy. The ability of PTCy to limit grades III to IV aGVHD and cGVHD while maintaining grade II aGVHD may contribute to its effectiveness, and further attempts to reduce aGVHD may be detrimental. Landmark Analyses: Effects of Grade II Acute Graft-Versus-Host Disease on Overall and Progression-Free Survival* *curves were truncated at 8-years after bone marrow transplantation OS, overall survival; No aGVHD Gr 2-4, patients without grade 2-4 acute graft-versus-host disease; aGVHD Gr 2, patients with grade II acute graft-versus-host disease; No., number; PSF, progression-free survival; Relp, relapse; NRM, nonrelapse mortality. Graphical Abstract Legend: A) In patients who were alive at day 100 after HLA-matched bone marrow transplantation with post-transplant cyclophosphamide, the probabilities of overall survival (OS) were compared. OS was higher in patients who had developed maximal grade II acute graft-versus-host disease (Grade II Acute GVHD; OS, dark blue line) when compared with patients who had not developed grade II-IV acute graft-versus-host disease (no GVHD; OS, orange line). B) In patients who were alive and who had not relapsed at day 100 after HLA-matched bone marrow transplantation with post-transplant cyclophosphamide, the probabilities of progression-free survival (PFS) were compared. PFS was higher in patients who had developed maximal grade II acute graft-versus-host disease (Grade II Acute GVHD; PFS, dark blue line) when compared with patients who had not developed grade II-IV acute graft-versus-host disease (no GVHD; PFS, orange line). Image, graphical abstract [ABSTRACT FROM AUTHOR]

Published
2019
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198. Early Fever after Haploidentical Bone Marrow Transplantation Correlates with Class II HLA-Mismatching and Myeloablation but Not Outcomes.

Author

McCurdy, Shannon R., Muth, Stephen T., Symons, Heather J., Huff, Carol Ann, Matsui, William H., Borrello, Ivan, Gladstone, Douglas E., Swinnen, Lode J., Cooke, Kenneth R., Brodsky, Robert A., Bolaños-Meade, Javier, Ambinder, Richard F., Luznik, Leo, Jones, Richard J., Fuchs, Ephraim J., Tsai, Hua-Ling, Varadhan, Ravi, and Bettinot, Maria P.

Subjects
*BONE marrow transplantation, *CYCLOPHOSPHAMIDE, *HLA histocompatibility antigens, *IMMUNOTHERAPY, *CHIMERIC antigen receptors, *BUSULFAN
Abstract

Highlights • Early fever after bone marrow transplantation is associated with both HLA haploidentical grafts and myeloablation. • Early fever is associated with Class II mismatching at HLA-DRB1 and HLA-DPB1 and CD3+ graft dose but does not influence survival. Abstract Noninfectious fevers are common early after T cell–replete HLA haploidentical (haplo) peripheral blood transplants and have been associated with cytokine release syndrome and overall mortality. However, less is known regarding the incidence and associations of early fever after bone marrow transplantation (BMT) with post-transplant cyclophosphamide (PTCy). We hypothesized that early fever would be associated with myeloablative conditioning (MAC), because of its relative increase in tissue damage augmenting antigen presentation and class II HLA-mismatching because of recognition of antigen-presenting cells by CD4+ T cells. In 672 recipients of MAC HLA-matched related donor (MRD) (n = 183), MAC HLA-matched unrelated donor (MUD) (n = 115), MAC haplo (n = 79), or nonmyeloablative (NMA) haplo (n = 295) T cell–replete BMT with PTCy, we retrospectively analyzed early noninfectious fever defined as temperature of ≥38.3°C once or ≥38.0°C twice or more on days 1 to 6. Fever occurred in 13% after MAC MRD, 23% after MAC MUD, 44% after NMA haplo, and 84% after MAC haplo BMT (P <.0001). Survival outcomes did not differ between patients with and without early fever. In NMA haplo BMT, mismatch in the graft-versus-host direction at HLA-DRB1 or -DPB1 (but not HLA-A, -B, -Cw, or -DQB1) was associated with early fever compared with no mismatches at these loci (P <.0001 and P =.02, respectively). In multivariable modeling, -DRB1 or -DPB1 mismatch and higher CD3+ graft cell dose were significantly associated with early fever. Early fever is more common after haplo compared with HLA-matched BMT. Fever is associated with myeloablation, -DRB1 or -DPB1 mismatching, and higher CD3+ graft cell dose but not survival. Graphical abstract Image, graphical abstract [ABSTRACT FROM AUTHOR]

Published
2018
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199. Shortened-Duration Tacrolimus after Nonmyeloablative, HLA-Haploidentical Bone Marrow Transplantation.

Author

Kasamon, Yvette L., Fuchs, Ephraim J., Zahurak, Marianna, Rosner, Gary L., Symons, Heather J., Gladstone, Douglas E., Huff, Carol Ann, Swinnen, Lode J., Brodsky, Robert A., Matsui, William H., Borrello, Ivan, Shanbhag, Satish, Cooke, Kenneth R., Ambinder, Richard F., Luznik, Leo, Bolaños-Meade, Javier, and Jones, Richard J.

Subjects
*TACROLIMUS, *MYELOSUPPRESSION, *HLA histocompatibility antigens, *BONE marrow transplantation, *CYCLOPHOSPHAMIDE, *GRAFT versus host disease
Abstract

With post-transplantation cyclophosphamide (PTCy) as graft-versus-host disease (GVHD) prophylaxis, nonmyeloablative HLA-haploidentical (NMA haplo) and HLA-matched blood or marrow transplantation (BMT) have comparable outcomes. Early discontinuation of immunosuppression may reduce the risk of relapse and improve immune reconstitution, but may increase the risk of GVHD. We conducted a prospective trial of NMA haplo BMT for patients with hematologic malignancies (median age, 61 years), evaluating the safety of early discontinuation of tacrolimus. All patients received T cell-replete bone marrow followed by high-dose PTCy, mycophenolate mofetil, and tacrolimus. Tacrolimus was prespecified to stop without taper at day +90, +60, or +120, contingent on having ≥5% donor T cells, no relapse, and no grade II-IV acute or significant chronic GVHD. Safety stopping rules were based on ≥5% graft failure, ≥10% nonrelapse mortality (NRM), or a ≥20% combined incidence of severe acute and chronic GVHD from the tacrolimus stop date through day +180. Of the 47 patients in the day +90 arm, 23 (49%) stopped tacrolimus as planned. Of the 55 patients in the day +60 arm, 38 (69%) stopped as planned. Safety stopping criteria were not met. In both arms, at day +180, the probability of grade II-IV acute GVHD was <40%, that of grade III-IV acute GVHD was <8%, and that of NRM was <5%. The 1-year probabilities of chronic GVHD and NRM were <15% and <10%, respectively, in both arms. The 1-year GVHD-free relapse-free survival was higher in the day 60 arm. Thus, stopping tacrolimus as early as day +60 is feasible and carries acceptable risks after NMA haplo BMT with PTCy. This approach may facilitate post-transplantation strategies for relapse reduction. [ABSTRACT FROM AUTHOR]

Published
2018
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200. Haploidentical Bone Marrow Transplantation with Post-Transplant Cyclophosphamide Using Non–First-Degree Related Donors.

Author

Elmariah, Hany, Kasamon, Yvette L., Zahurak, Marianna, Macfarlane, Karen W., Tucker, Noah, Rosner, Gary L., Bolaños-Meade, Javier, Fuchs, Ephraim J., Wagner-Johnston, Nina, Swinnen, Lode J., Huff, Carol Ann, Matsui, William H., Gladstone, Douglas E., McCurdy, Shannon R., Borrello, Ivan, Gocke, Christian B., Shanbhag, Satish, Cooke, Kenneth R., Ali, Syed Abbas, and Brodsky, Robert A.

Subjects
*BONE marrow transplantation, *CYCLOPHOSPHAMIDE, *BLOOD donors, *HEMATOLOGIC agents, *CHIMERISM
Abstract

Outcomes of nonmyeloablative (NMA) haploidentical (haplo) blood or marrow transplant (BMT) with post-transplantation cyclophosphamide (PTCy) using non–first-degree relatives are unknown. We evaluated 33 consecutive adult patients (median age, 56 years) with hematologic malignancies who underwent NMA haplo T cell–replete BMT with PTCy at Johns Hopkins using second- or third-degree related donors. Donors consisted of 10 nieces (30%), 9 nephews (27%), 7 first cousins (21%), 5 grandchildren (15%), and 2 uncles (6%). Thirty-one patients (94%) reached full donor chimerism by day 60. The estimated cumulative incidence (CuI) of grades II to IV acute graft-versus-host disease (aGVHD) at day 180 was 24% (90% confidence interval [CI], 9% to 38%). Only 1 patient experienced grades III to IV aGVHD. At 1 year the CuI of chronic GVHD was 10% (90% CI, 0% to 21%). The CuI of nonrelapse mortality at 1 year was 5% (90% CI, 0% to 14%). At 1 year the probability of relapse was 31% (90% CI, 12% to 49%), progression-free survival 64% (90% CI, 48% to 86%), and overall survival 95% (90% CI, 87% to 100%). The 1-year probability of GVHD-free, relapse-free survival was 57% (90% CI, 41% to 79%). NMA haplo BMT with PTCy from non–first-degree relatives is an acceptably safe and effective alternative donor platform, with results similar to those seen with first-degree relatives. [ABSTRACT FROM AUTHOR]

Published
2018
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