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Post-Transplant Cyclophosphamide, Abatacept and Short Course of Tacrolimus (CAST) for Graft-Versus-Host Disease Prevention Following Haploidentical Peripheral Blood Stem Cell Transplantation [Meeting Abstract]

Al-Homsi, A. Samer; Cirrone, Frank; Cole, Kelli; Suarez-Londono, Jaime Andres; Gardner, Sharon L.; Hsu, Jingmei; Wo, Stephanie; Stocker, Kelsey; Bruno, Benedetto; Goldberg, Judith; Levinson, Benjamin; Abdul-Hay, Maher
ISI:000893230300285
ISSN: 0006-4971
CID: 5515762

Planned Granulocyte Colony-Stimulating Factor Adversely Impacts Survival after Allogeneic Hematopoietic Cell Transplantation Performed with Thymoglobulin for Myeloid Malignancy

Orfali, Nina; Zhang, Mei-Jie; Allbee-Johnson, Mariam; Boelens, Jaap Jan; Artz, Andrew S; Brunstein, Claudio G; McNiece, Ian K; Milano, Filippo; Abid, Muhammad Bilal; Chee, Lynette; Diaz, Miguel A; Grunwald, Michael R; Hematti, Peiman; Hsu, Jingmei; Lazarus, Hillard M; Munshi, Pashna N; Prestidge, Timothy; Ringden, Olle; Rizzieri, David; Riches, Marcie L; Seo, Sachiko; Solh, Melhem; Solomon, Scott; Szwajcer, David; Yared, Jean; van Besien, Koen; Eapen, Mary
The in vivo depletion of recipient and donor T lymphocytes using antithymocyte globulin (ATG; Thymoglobulin) is widely adopted in allogeneic hematopoietic stem cell transplantation (HCT) to reduce the incidence of both graft failure and graft-versus-host disease (GVHD). However, excess toxicity to donor lymphocytes may hamper immune reconstitution, compromising antitumor effects and increasing infection. Granulocyte-colony stimulating factor (G-CSF) administered early after HCT may increase ATG-mediated lymphotoxicity. This study aimed to investigate the effect of an interaction between ATG and post-transplantation granulocyte colony-stimulating factor (G-CSF) on allogeneic HCT outcomes, using the Center for International Blood and Marrow Transplant Research (CIBMTR) registry. We studied patients age ≥18 years with acute myelogenous leukemia (AML) and myelodysplastic syndrome (MDS) who received Thymoglobulin-containing preparative regimens for HLA-matched sibling/unrelated or mismatched unrelated donor HCT between 2010 and 2018. The effect of planned G-CSF that was started between pretransplantation day 3 and post-transplantation day 12 was studied in comparison with transplantations that did not include G-CSF. Cox regression models were built to identify risk factors associated with outcomes at 1 year after transplantation. A total of 874 patients met the study eligibility criteria, of whom 459 (53%) received planned G-CSF. HCT with planned G-CSF was associated with a significantly increased risk for nonrelapse mortality (NRM) (hazard ratio [HR] 2.03; P <.0001; 21% versus 12%) compared to HCT without G-CSF. The 6-month incidence of viral infection was higher with G-CSF (56% versus 47%; P = .007), with a particular increase in Epstein-Barr virus infections (19% versus 11%; P = .002). The observed higher NRM with planned G-CSF led to lower overall survival (HR, 1.52; P = .0005; 61% versus 72%). There was no difference in GVHD risk between the treatment groups. We performed 2 subgroup analyses showing that our findings held true in patients age ≥50 years and in centers where G-CSF was used in some, but not all, patients. In allogeneic peripheral blood HCT performed with Thymoglobulin for AML and MDS, G-CSF administered early post-transplantation resulted in a 2-fold increase in NRM and a 10% absolute decrement in survival. The use of planned G-CSF in the early post-transplantation period should be carefully considered on an individual patient basis, weighing any perceived benefits against these risks.
PMCID:8671234
PMID: 34507002
ISSN: 2666-6367
CID: 5204002

Long-term clinical outcomes of tisagenlecleucel in patients with relapsed or refractory aggressive B-cell lymphomas (JULIET): a multicentre, open-label, single-arm, phase 2 study

Schuster, Stephen J; Tam, Constantine S; Borchmann, Peter; Worel, Nina; McGuirk, Joseph P; Holte, Harald; Waller, Edmund K; Jaglowski, Samantha; Bishop, Michael R; Damon, Lloyd E; Foley, Stephen Ronan; Westin, Jason R; Fleury, Isabelle; Ho, P Joy; Mielke, Stephan; Teshima, Takanori; Janakiram, Murali; Hsu, Jing-Mei; Izutsu, Koji; Kersten, Marie José; Ghosh, Monalisa; Wagner-Johnston, Nina; Kato, Koji; Corradini, Paolo; Martinez-Prieto, Marcela; Han, Xia; Tiwari, Ranjan; Salles, Gilles; Maziarz, Richard T
BACKGROUND:In the primary analysis of the pivotal JULIET trial of tisagenlecleucel, an autologous anti-CD19 chimeric antigen receptor (CAR) T-cell therapy, the best overall response rate was 52% and the complete response rate was 40% in 93 evaluable adult patients with relapsed or refractory aggressive B-cell lymphomas. We aimed to do a long-term follow-up analysis of the clinical outcomes and correlative analyses of activity and safety in the full adult cohort. METHODS:viable transduced CAR T cells). The primary endpoint was overall response rate (ie, the proportion of patients with a best overall disease response of a complete response or partial response using the Lugano classification, as assessed by an independent review committee) at any time post-infusion and was analysed in all patients who received tisagenlecleucel (the full analysis set). Safety was analysed in all patients who received tisagenlecleucel. JULIET is registered with ClinialTrials.gov, NCT02445248, and is ongoing. FINDINGS:Between July 29, 2015, and Nov 2, 2017, 167 patients were enrolled. As of Feb 20, 2020, 115 patients had received tisagenlecleucel infusion and were included in the full analysis set. At a median follow-up of 40·3 months (IQR 37·8-43·8), the overall response rate was 53·0% (95% CI 43·5-62·4; 61 of 115 patients), with 45 (39%) patients having a complete response as their best overall response. The most common grade 3-4 adverse events were anaemia (45 [39%]), decreased neutrophil count (39 [34%]), decreased white blood cell count (37 [32%]), decreased platelet count (32 [28%]), cytokine release syndrome (26 [23%]), neutropenia (23 [20%]), febrile neutropenia (19 [17%]), hypophosphataemia (15 [13%]), and thrombocytopenia (14 [12%]). The most common treatment-related serious adverse events were cytokine release syndrome (31 [27%]), febrile neutropenia (seven [6%]), pyrexia (six [5%]), pancytopenia (three [3%]), and pneumonia (three [3%]). No treatment-related deaths were reported. INTERPRETATION:Tisagenlecleucel shows durable activity and manageable safety profiles in adult patients with relapsed or refractory aggressive B-cell lymphomas. For patients with large B-cell lymphomas that are refractory to chemoimmunotherapy or relapsing after second-line therapies, tisagenlecleucel compares favourably with respect to risk-benefit relative to conventional therapeutic approaches (eg, salvage chemotherapy). FUNDING:Novartis Pharmaceuticals.
PMID: 34516954
ISSN: 1474-5488
CID: 5204012

Sequential intensive chemotherapy followed by autologous or allogeneic transplantation for refractory lymphoma

Orfali, Nina; Jhanwar, Yuliya; Koo, Calvin; Pasciolla, Michelle; Baldo, Maria; Cuvilly, Edwidge; Furman, Richard; Gergis, Usama; Greenberg, June; Guarneri, Danielle; Hsu, Jing-Mei; Leonard, John P; Mark, Tomer; Mayer, Sebastian; Maignan, Kathleen; Martin, Peter; Opong, Adomah; Pearse, Roger; Phillips, Adrienne; Rossi, Adriana; Ruan, Jia; Rutherford, Sarah C; Ryan, Jessy; Suhu, Grace; Van Besien, Koen; Shore, Tsiporah
We evaluate the safety of bendamustine as a bridge to stem cell transplantation (SCT) in patients with relapsed/refractory lymphoma and residual disease after salvage therapy. Thirty-four subjects without complete responses (CR) received bendamustine 200 mg/m2/day for 2 days followed 14 days later by SCT. Sixteen subjects in partial remission (PR) with maximal FDG-PET SUVs ≤8 prior to bendamustine received autologous SCT, while 13 with suboptimal responses were allografted. Five subjects did not proceed to transplant. No bendamustine toxicities precluded transplantation and no detrimental effect on engraftment or early treatment-related mortality (TRM) was attributable to bendamustine. At 1 year, 75% of auto-recipients and 31% of allo-recipients were alive with CR. Two subjects in the autologous arm developed therapy-related myeloid neoplasia (t-MN). In conclusion, a bendamustine bridge to SCT can be administered without early toxicity to patients with suboptimal responses to salvage chemotherapy. However this approach may increase the risk of t-MN. (NCT02059239).Supplemental data for this article is available online at here.
PMID: 33586581
ISSN: 1029-2403
CID: 5203992

Profiling of immune dysfunction in COVID-19 patients allows early prediction of disease progression

Rendeiro, André F; Casano, Joseph; Vorkas, Charles Kyriakos; Singh, Harjot; Morales, Ayana; DeSimone, Robert A; Ellsworth, Grant B; Soave, Rosemary; Kapadia, Shashi N; Saito, Kohta; Brown, Christopher D; Hsu, JingMei; Kyriakides, Christopher; Chiu, Steven; Cappelli, Luca Vincenzo; Cacciapuoti, Maria Teresa; Tam, Wayne; Galluzzi, Lorenzo; Simonson, Paul D; Elemento, Olivier; Salvatore, Mirella; Inghirami, Giorgio
With a rising incidence of COVID-19-associated morbidity and mortality worldwide, it is critical to elucidate the innate and adaptive immune responses that drive disease severity. We performed longitudinal immune profiling of peripheral blood mononuclear cells from 45 patients and healthy donors. We observed a dynamic immune landscape of innate and adaptive immune cells in disease progression and absolute changes of lymphocyte and myeloid cells in severe versus mild cases or healthy controls. Intubation and death were coupled with selected natural killer cell KIR receptor usage and IgM+ B cells and associated with profound CD4 and CD8 T-cell exhaustion. Pseudo-temporal reconstruction of the hierarchy of disease progression revealed dynamic time changes in the global population recapitulating individual patients and the development of an eight-marker classifier of disease severity. Estimating the effect of clinical progression on the immune response and early assessment of disease progression risks may allow implementation of tailored therapies.
PMCID:7768198
PMID: 33361110
ISSN: 2575-1077
CID: 4770952

Specific Class I HLA Supertypes but Not HLA Zygosity or Expression Are Associated with Outcomes following HLA-Matched Allogeneic Hematopoietic Cell Transplant: HLA Supertypes Impact Allogeneic HCT Outcomes

Camacho-Bydume, Christine; Wang, Tao; Sees, Jennifer A; Fernandez-Viña, Marcelo; Abid, Muhammad Bilal; Askar, Medhat; Beitinjaneh, Amer; Brown, Valerie; Castillo, Paul; Chhabra, Saurabh; Gadalla, Shahinaz M; Hsu, Jing-Mei; Kamoun, Malek; Lazaryan, Aleksandr; Nishihori, Taiga; Page, Kristin; Schetelig, Johannes; Fleischhauer, Katharina; Marsh, Steven G E; Paczesny, Sophie; Spellman, Stephen R; Lee, Stephanie J; Hsu, Katharine C
Maximizing the probability of antigen presentation to T cells through diversity in HLAs can enhance immune responsiveness and translate into improved clinical outcomes, as evidenced by the association of heterozygosity and supertypes at HLA class I loci with improved survival in patients with advanced solid tumors treated with immune checkpoint inhibitors. We investigated the impact of HLA heterozygosity, supertypes, and surface expression on outcomes in adult and pediatric patients with acute myeloid leukemia (AML), myelodysplastic syndrome, acute lymphoblastic leukemia, and non-Hodgkin lymphoma who underwent 8/8 HLA-matched, T cell replete, unrelated, allogeneic hematopoietic cell transplant (HCT) from 2000 to 2015 using patient data reported to the Center for International Blood and Marrow Transplant Research. HLA class I heterozygosity and HLA expression were not associated with overall survival, relapse, transplant-related mortality (TRM), disease-free survival (DFS), and acute graft-versus-host disease following HCT. The HLA-B62 supertype was associated with decreased TRM in the entire patient cohort (hazard ratio [HR], 0.79; 95% CI, 0.69 to 0.90; P = .00053). The HLA-B27 supertype was associated with worse DFS in patients with AML (HR = 1.21; 95% CI, 1.10 to 1.32; P = .00005). These findings suggest that the survival benefit of HLA heterozygosity seen in solid tumor patients receiving immune checkpoint inhibitors does not extend to patients undergoing allogeneic HCT. Certain HLA supertypes, however, are associated with TRM and DFS, suggesting that similarities in peptide presentation between supertype members play a role in these outcomes. Beyond implications for prognosis following HCT, these findings support the further investigation of these HLA supertypes and the specific immune peptides important for transplant outcomes.
PMCID:8015676
PMID: 33053450
ISSN: 2666-6367
CID: 5203972

Cord blood transplants supported by unrelated donor CD34+ progenitor cells

Gomez-Arteaga, Alexandra; Orfali, Nina; Guarneri, Danielle; Cushing, Melissa M; Gergis, Usama; Hsu, Jingmei; Hsu, Yen-Michael S; Mayer, Sebastian A; Phillips, Adrienne A; Chase, Stacy A; Mokhtar, Asmaa E; Shore, Tsiporah B; Van Besien, Koen
Alternative donor transplantation with the haplo-cord platform allows the use of a lower-dose single umbilical cord blood unit (CBU) by co-infusion of third-party CD34+-selected cells from a haploidentical relative, which provides early transient engraftment while awaiting durable CBU engraftment. In our experience, ~15% of patients lack a suitable haploidentical donor. Here we report 26 patients who underwent haplo-cord transplant using CD34+-selected partially matched unrelated donor grafts. Twenty-four were conditioned with fludarabine/melphalan +/- low-dose TBI (n = 16). Twenty-five received ATG and all received posttransplant tacrolimus and mycophenolate mofetil. Median time to neutrophil and platelet recovery was 11 and 18 days. CBU engraftment, with CD33 and CD3 >5% cord chimerism in the myeloid/lymphoid compartment by day +60, occurred in 20 of 24 patients (83%). Incidence of grade 2-4 acute graft-versus-host disease (GVHD) was 27% at day +100, and chronic GVHD was 4% at 1 year. Overall survival at 1 year was 54%. For patients in need of an alternative transplant who lack a haploidentical donor, haplo-cord transplantation using CD34+-selected partially matched unrelated donor grafts results in rapid engraftment with no increased rate of cord graft failure or GVHD.
PMID: 32518291
ISSN: 1476-5365
CID: 5203942

Impact of alemtuzumab dosing and low-dose total body irradiation on cytomegalovirus infection in allogeneic hematopoietic stem cell transplantation [Letter]

Brown, Maxwell; Abasov, Rza; Salerno, David; Shore, Tsiporah B; Gergis, Usama; Mayer, Sebastian; Phillips, Adrienne; Hsu, Jingmei; Kodiyanplakkal, Rosy Priya L; Pasciolla, Michelle; van Besien, Koen
PMID: 32654572
ISSN: 1029-2403
CID: 5203952

Adoptive immunotherapy with CB following chemotherapy for patients with refractory myeloid malignancy: chimerism and response

Chaekal, Ok-Kyong; Scaradavou, Andromachi; Masson Frenet, Emeline; Albano, Maria S; Cushing, Melissa; Desai, Pinkal; Dobrila, Ludy; Gergis, Usama; Guarneri, Danielle; Hsu, Jing-Mei; Lee, Sangmin; Mayer, Sebastian A; Phillips, Adrienne A; Orfali, Nina; Ritchie, Ellen K; Roboz, Gail J; Romeo, Cynthia; Samuel, Michael S; Shore, Tsiporah; van Besien, Koen
We conducted a prospective evaluation of cord blood (CB)-derived adoptive cell therapy, after salvage chemotherapy, for patients with advanced myeloid malignancies and poor prognosis. Previously, we reported safety, feasibility, and preliminary efficacy of this approach. We present updated results in 31 patients who received intensive chemotherapy followed by CB infusion and identify predictors of response. To enhance the antileukemic effect, we selected CB units (CBU) with shared inherited paternal antigens and/or noninherited maternal antigens with the recipients. Twenty-eight patients with acute myeloid leukemia (AML), 2 with myelodysplastic syndrome, and 1 in chronic myeloid leukemia myeloid blast crisis were enrolled; 9 had relapsed after allogeneic transplant. Response was defined as <5% blasts in hypocellular bone marrow at 2 weeks after treatment. Thirteen patients (42%) responded; a rate higher than historical data with chemotherapy only. Twelve had CBU-derived chimerism detected; chimerism was a powerful predictor of response (P < .001). CBU lymphocyte content and a prior transplant were associated with chimerism (P < .01). Safety was acceptable: 3 patients developed mild cytokine release syndrome, 2 had grade 1 and 2 had grade 4 graft-versus-host disease. Seven responders and 6 nonresponders (after additional therapy) received subsequent transplant; 5 are alive (follow-up, 5-47 months). The most common cause of death for nonresponders was disease progression, whereas for responders it was infection. CB-derived adoptive cell therapy is feasible and efficacious for refractory AML. Banked CBU are readily available for treatment. Response depends on chimerism, highlighting the graft-versus-leukemia effect of CB cell therapy. This trial was registered at www.clinicaltrials.gov as #NCT02508324.
PMCID:7594383
PMID: 33091124
ISSN: 2473-9537
CID: 5203982

CHD7 and Runx1 interaction provides a braking mechanism for hematopoietic differentiation

Hsu, Jingmei; Huang, Hsuan-Ting; Lee, Chung-Tsai; Choudhuri, Avik; Wilson, Nicola K; Abraham, Brian J; Moignard, Victoria; Kucinski, Iwo; Yu, Shuqian; Hyde, R Katherine; Tober, Joanna; Cai, Xiongwei; Li, Yan; Guo, Yalin; Yang, Song; Superdock, Michael; Trompouki, Eirini; Calero-Nieto, Fernando J; Ghamari, Alireza; Jiang, Jing; Gao, Peng; Gao, Long; Nguyen, Vy; Robertson, Anne L; Durand, Ellen M; Kathrein, Katie L; Aifantis, Iannis; Gerber, Scott A; Tong, Wei; Tan, Kai; Cantor, Alan B; Zhou, Yi; Liu, P Paul; Young, Richard A; Göttgens, Berthold; Speck, Nancy A; Zon, Leonard I
Hematopoietic stem and progenitor cell (HSPC) formation and lineage differentiation involve gene expression programs orchestrated by transcription factors and epigenetic regulators. Genetic disruption of the chromatin remodeler chromodomain-helicase-DNA-binding protein 7 (CHD7) expanded phenotypic HSPCs, erythroid, and myeloid lineages in zebrafish and mouse embryos. CHD7 acts to suppress hematopoietic differentiation. Binding motifs for RUNX and other hematopoietic transcription factors are enriched at sites occupied by CHD7, and decreased RUNX1 occupancy correlated with loss of CHD7 localization. CHD7 physically interacts with RUNX1 and suppresses RUNX1-induced expansion of HSPCs during development through modulation of RUNX1 activity. Consequently, the RUNX1:CHD7 axis provides proper timing and function of HSPCs as they emerge during hematopoietic development or mature in adults, representing a distinct and evolutionarily conserved control mechanism to ensure accurate hematopoietic lineage differentiation.
PMID: 32883883
ISSN: 1091-6490
CID: 4622752