Your search keyword '"Rybka, W"' showing total 155 results

1. Pembrolizumab plus dinaciclib in patients with hematologic malignancies: the phase 1b KEYNOTE-155 study

Author

Gregory, GP, Kumar, S, Wang, D, Mahadevan, D, Walker, P, Wagner-Johnston, N, Escobar, C, Bannerji, R, Bhutani, D, Chang, J, Hernandez-Ilizaliturri, FJ, Klein, A, Pagel, JM, Rybka, W, Yee, AJ, Mohrbacher, A, Huang, M, Farooqui, M, Marinello, P, Quach, H, Gregory, GP, Kumar, S, Wang, D, Mahadevan, D, Walker, P, Wagner-Johnston, N, Escobar, C, Bannerji, R, Bhutani, D, Chang, J, Hernandez-Ilizaliturri, FJ, Klein, A, Pagel, JM, Rybka, W, Yee, AJ, Mohrbacher, A, Huang, M, Farooqui, M, Marinello, P, and Quach, H

Abstract

Preclinical data demonstrated that combining an anti-programmed cell death 1 (PD-1) inhibitor with a cyclin-dependent kinase 9 (CDK9) inhibitor provided enhanced antitumor activity with no significant toxicities, suggesting this combination may be a potential therapeutic option. The multicohort, phase 1 KEYNOTE-155 study evaluated the safety and antitumor activity of the PD-1 inhibitor pembrolizumab plus the CDK9 inhibitor dinaciclib in patients with relapsed or refractory (rr) chronic lymphocytic leukemia (CLL), diffuse large B-cell lymphoma (DLBCL) and multiple myeloma (MM). Patients enrolled were ≥18 years of age with a confirmed diagnosis of CLL, DLBCL, or MM. The study included 2 phases: a dose-evaluation phase to determine dose-limiting toxicities and a signal-detection phase. Patients received pembrolizumab 200 mg every 3 weeks plus dinaciclib 7 mg/m2 on day 1 and 10 mg/m2 on day 8 of cycle 1 and 14 mg/m2 on days 1 and 8 of cycles 2 and later. Primary endpoint was safety, and a key secondary endpoint was objective response rate (ORR). Seventy-two patients were enrolled and received ≥1 dose of study treatment (CLL, n = 17; DLBCL, n = 38; MM, n = 17). Pembrolizumab plus dinaciclib was generally well tolerated and produced no unexpected toxicities. The ORRs were 29.4% (5/17, rrCLL), 21.1% (8/38, rrDLBCL), and 0% (0/17, rrMM), respectively. At data cutoff, all 72 patients had discontinued treatment, 38 (52.8%) because of progressive disease. These findings demonstrate activity with combination pembrolizumab plus dinaciclib and suggest that a careful and comprehensive approach to explore anti-PD-1 and CDK9 inhibitor combinations is warranted. This trial was registered at www.clinicaltrials.gov as NCT02684617.

Published

2022

2. G-CSF mobilized vs conventional donor lymphocytes for therapy of relapse or incomplete engraftment after allogeneic hematopoietic transplantation

Author

Abbi, K K S, Zhu, J, Ehmann, W C, Epner, E, Carraher, M, Mierski, J, Talamo, G, Lucas, K, Rybka, W, and Claxton, D

Published

2013

3. BU and CY as conditioning regimen for autologous transplant in patients with multiple myeloma

Author

Talamo, G, Claxton, D F, Dougherty, D W, Ehmann, C W, Sivik, J, Drabick, J J, and Rybka, W

Published

2009

4. High-dose chemotherapy and autologous stem cell support followed by post-transplant doxorubicin and taxol as initial therapy for metastatic breast cancer: hematopoietic tolerance and efficacy

Author

deMagalhaes-Silverman, M, Hammert, L, Lembersky, B, Lister, J, Rybka, W, and Ball, E

Published

1998

5. Busulfan and cyclophosphamide (BU/CY2) as preparative regimen for patients with lymphoma

Author

deMagalhaes-Silverman, M, Lister, J, Rybka, W, Wilson, J, and Ball, E

Published

1997

6. Sirolimus in unmanipulated haploidentical cell transplantation

Author

von Reyn Cream, L, Ehmann, W C, Rybka, W B, and Claxton, D F

Published

2008

7. Antitumor activity of pembrolizumab plus dinaciclib in patients with diffuse large B cell lymphoma: the phase 1b KEYNOTE-155 study.

Author

Gwo J., Shortt J., Ma H., Farooqui M., Quach H., Gregory G., Walker P., Mahadevan D., Wang D., Chang J., Hernandez-Ilizaliturri F., Klein A., Rybka W., Wagner-Johnston N., Escobar C., Pagel J.M., Mohrbacher A., Opat S., Gwo J., Shortt J., Ma H., Farooqui M., Quach H., Gregory G., Walker P., Mahadevan D., Wang D., Chang J., Hernandez-Ilizaliturri F., Klein A., Rybka W., Wagner-Johnston N., Escobar C., Pagel J.M., Mohrbacher A., and Opat S.

Abstract

Introduction: KEYNOTE-155 (NCT02684617) evaluated the antitumor activity of pembrolizumab (pembro) plus dinaciclib in patients (pts) with relapsed/refractory (rr) CLL, MM, and DLBCL. Here we present data from an interim analysis of safety and efficacy in pts with rrDLBCL. Method(s): In this phase 1b, two-part, non-randomized, open-label study, pts with rrDLBCL who received >=2 prior therapies were enrolled into a dose-evaluation phase (two 21-day [d] cycles of pembro 200 mg [d1] and dinaciclib 7 mg/m2 [d1], 10 mg/m2 [d8] in cycle 1 and 14 mg/m2 [d1, d8] from cycle 2 onwards). The DLBCL expansion cohort was opened for the signal-detection phase (>=30 patients) if <=4 pts had dose-limiting toxicities (DLTs) during dose-evaluation. Treatment continued up to 35 cycles or until progression (PD) or unacceptable toxicity. Response was assessed every 3 cycles for DLBCL (Revised Response Criteria for Malignant Lymphoma 2007). Pts who discontinued before PD were followed Q12W until PD, new anticancer treatment, or death. The primary endpoint was safety and tolerability. Secondary endpoints included ORR by investigator, DOR, PFS, and OS. Efficacy and safety were assessed in all pts who received >=1 dose of pembrolizumab or dinaciclib. Result(s): As of Apr 25, 2018, 38 pts with rrDLBCL were enrolled and treated. Median age was 64.5 years (range, 39-85), 22 (58%) pts had ECOG PS 1, and 22 (58%) had >=3 prior therapies. After median follow-up of 2.79 mo (range, 1.5-6.8), 36 (95%) pts discontinued treatment: 21 (55%) PD, 12 (32%) by physician decision (10 [26%] clinical progression, 1[3%] logistics, 1 [3%] new therapy), 2 (5%) pt decision, and 1 (3%) AE. Median time on treatment was 51d (range, 1-471). Among 12 pts in all disease cohorts enrolled in the dose-evaluation phase, DLTs occurred in 1 of 6 (17%) evaluable pts (grade 4 thrombocytopenia) with rrDLBCL. Of 38 pts with rrDLBCL, 24 (63%) had a treatment-related AE. Common treatment-related AEs were decreased platelets (21%), l

Published

2019

8. PS1075 ANTITUMOR ACTIVITY OF PEMBROLIZUMAB PLUS DINACICLIB IN PATIENTS WITH DIFFUSE LARGE B CELL LYMPHOMA: THE PHASE 1B KEYNOTE-155 STUDY

Author

Gregory, G., primary, Walker, P., additional, Mahadevan, D., additional, Wang, D., additional, Chang, J., additional, Hernandez-Ilizaliturri, F., additional, Klein, A., additional, Rybka, W., additional, Wagner-Johnston, N., additional, Escobar, C., additional, Pagel, J.M., additional, Mohrbacher, A., additional, Opat, S., additional, Shortt, J., additional, Ma, H., additional, Gwo, J., additional, Farooqui, M., additional, and Quach, H., additional

Published

2019

9. ANTITUMOR ACTIVITY OF PEMBROLIZUMAB PLUS DINACICLIB IN PATIENTS WITH DIFFUSE LARGE B CELL LYMPHOMA: THE PHASE 1B KEYNOTE-155 STUDY

Author

Gregory, G., primary, Walker, P., additional, Mahadevan, D., additional, Wang, D., additional, Chang, J., additional, Hernandez-Ilizaliturri, F., additional, Klein, A., additional, Rybka, W., additional, Wagner-Johnston, N., additional, Escobar, C., additional, Pagel, J.M., additional, Mohrbacher, A., additional, Opat, S., additional, Shortt, J., additional, Ma, H., additional, Gwo, J., additional, Farooqui, M., additional, and Quach, H., additional

Published

2019

10. Inactivated varicella zoster vaccine in autologous haemopoietic stem-cell transplant recipients: an international, multicentre, randomised, double-blind, placebo-controlled trial

Author

Winston, Drew J, primary, Mullane, Kathleen M, additional, Cornely, Oliver A, additional, Boeckh, Michael J, additional, Brown, Janice Wes, additional, Pergam, Steven A, additional, Trociukas, Igoris, additional, Žák, Pavel, additional, Craig, Michael D, additional, Papanicolaou, Genovefa A, additional, Velez, Juan D, additional, Panse, Jens, additional, Hurtado, Kimberly, additional, Fernsler, Doreen A, additional, Stek, Jon E, additional, Pang, Lei, additional, Su, Shu-Chih, additional, Zhao, Yanli, additional, Chan, Ivan S F, additional, Kaplan, Susan S, additional, Parrino, Janie, additional, Lee, Ingi, additional, Popmihajlov, Zoran, additional, Annunziato, Paula W, additional, Arvin, Ann, additional, Basso, AC, additional, Bonvehi, P, additional, Cerana, S, additional, Dictar, MO, additional, Campbell, P, additional, Playford, G, additional, Sasadeusz, J, additional, Maertens, J, additional, Poire, X, additional, Sellesag, D, additional, Schots, R, additional, Theunissen, K, additional, Willems, E, additional, Alves, RS, additional, Camargo, JFC, additional, Castro, NS, additional, Maria Fogliatto, L, additional, Rodrigo, O, additional, Courture, F, additional, McGeer, A, additional, Miller, M, additional, Combariza, JF, additional, Sossa, CL, additional, Velez, JD, additional, Nemet, D, additional, Ostojic Kolonic, S, additional, Jebavy, L, additional, Mayer, J, additional, Novak, J, additional, Pohlreich, D, additional, Maldonado, B, additional, Gastinne, T, additional, Karlin, L, additional, Launay, O, additional, Cornely, OA, additional, Duerk, HA, additional, Haenel, M, additional, Heinz, W, additional, Kaufmann, M, additional, Panse, J, additional, Teschner, D, additional, Verbeek, M, additional, Wulf, G, additional, Aviv, F, additional, Grisariu, S, additional, Nagler, A, additional, Yeshurun, M, additional, Bosi, A, additional, Corradini, P, additional, Martinelli, G, additional, Onida, F, additional, Rambaldi, A, additional, Velardi, A, additional, Trociukas, I, additional, Gomez, AD, additional, Wondergem, MJ, additional, Ypma, PF, additional, Fanilla, E, additional, Moreno Larrea, MDC, additional, Abecasis, MM, additional, Ferreira, RB, additional, Geraldes, C, additional, Castro, J, additional, Afanasyev, BV, additional, Kruchkova, IV, additional, Zaritskiy, AY, additional, Cheong, JW, additional, Kim, SJ, additional, Lee, DG, additional, Yoon, SS, additional, Aguado Bueno, B, additional, Jarque Ramos, I, additional, Solano Vercet, C, additional, Cherif, H, additional, Ljungman, P, additional, Vaht, K, additional, Cook, G, additional, Kanfer, E, additional, Milligan, DW, additional, Parker, A, additional, Akard, L, additional, Bachier, C, additional, Ball, ED, additional, Betts, FR, additional, Braunschweig, I, additional, Brown, JM, additional, Carroll, MP, additional, Chandrasekar, PH, additional, Collins, R, additional, Cooper, B, additional, Craig, M, additional, D'Cunha, N, additional, Donato, ML, additional, Essell, J, additional, Flomenberg, P, additional, Freifeld, A, additional, Freytes, C, additional, Guarino, MJ, additional, Hall, MC, additional, Heimenz, JW, additional, High, KP, additional, Isola, LM, additional, Kaminer, L, additional, Klein, LM, additional, Janakiraman, N, additional, Kane, K, additional, Komanduri, K, additional, Krijanovski, OI, additional, Lawrence, SJ, additional, Leis, JF, additional, Lill, M, additional, Longo, WL, additional, Lynch, JP, additional, Mattar, BI, additional, Mehta, J, additional, Mullane, KM, additional, Nathan, S, additional, Papanicolaou, GA, additional, Pergam, SA, additional, Roy, V, additional, Rybka, W, additional, Safah, H, additional, Saltzman, D, additional, Segal, GM, additional, Selby, GB, additional, Schuster, MW, additional, Shoham, S, additional, Sloan, JM, additional, Strasfeld, LM, additional, Styler, M, additional, Sullivan, K, additional, Tse, W, additional, Vance, EA, additional, Winston, DJ, additional, and Yanovich, S, additional

Published

2018

11. PD-1hiTIM-3+ T cells associate with and predict leukemia relapse in AML patients post allogeneic stem cell transplantation

Author

Kong, Y, primary, Zhang, J, additional, Claxton, D F, additional, Ehmann, W C, additional, Rybka, W B, additional, Zhu, L, additional, Zeng, H, additional, Schell, T D, additional, and Zheng, H, additional

Published

2015

12. Augmentation of Natural Chimerism With Donor Bone Marrow in Orthotopic Liver Recipients

Author

As, Rao, Fontes P, Dodson F, Zeevi A, Mt, Rugeles, Abu-Elmagd K, Aitouche A, Rosner G, Trucco M, Aj, Demetris, Rybka W, Todo S, John Fung, and Te, Starzl

Subjects

Adult, Graft Rejection, Male, Transplantation Chimera, Histocompatibility Testing, Middle Aged, Flow Cytometry, Polymerase Chain Reaction, Article, Monocytes, Tacrolimus, Liver Transplantation, Graft vs Host Reaction, Antigens, CD, Risk Factors, Humans, Prednisone, Female, Lymphocytes, Lymphocyte Culture Test, Mixed, Immunosuppressive Agents, Bone Marrow Transplantation, Retrospective Studies

Published

1996

13. G-CSF mobilized vs conventional donor lymphocytes for therapy of relapse or incomplete engraftment after allogeneic hematopoietic transplantation

Author

Abbi, K K S, primary, Zhu, J, additional, Ehmann, W C, additional, Epner, E, additional, Carraher, M, additional, Mierski, J, additional, Talamo, G, additional, Lucas, K, additional, Rybka, W, additional, and Claxton, D, additional

Published

2012

14. High-dose melphalan on day 2 versus 1 before autologous stem cell transplantation for multiple myeloma.

Author

Rakszawski, K., primary, Drabick, J. J., additional, Dolloff, N. G., additional, Sivik, J. M., additional, Malysz, J., additional, Claxton, D., additional, Ehmann, W. C., additional, Rybka, W. B., additional, and Talamo, G., additional

Published

2011

15. Effect of mobilization chemotherapy with cyclophosphamide and etoposide on stem cell collection by lenalidomide

Author

Talamo, G., primary, Claxton, D. F., additional, Ehmann, W. C., additional, Mierski, J., additional, Rybka, W., additional, and Ibrahin, S., additional

Published

2009

16. Improvement of matched sibling donor engraftment with sirolimus added to a non-myeloablative conditioning regimen

Author

Claxton, D.F., primary, Ehmann, C., additional, Shaffer, M., additional, and Rybka, W., additional

Published

2005

17. Sirolimus and tacrolimus allow engraftment of haploidentical and other alternative donor stem cells after non-myeloablative conditioning

Author

Claxton, D.F., primary, Popescu, D., additional, Carraher, M., additional, Chiafari, F.A., additional, Ehmann, C., additional, and Rybka, W., additional

Published

2004

18. Augmentation of natural chimerism with donor bone marrow in orthotopic liver recipients

Author

Rao, AS, Fontes, P, Dodson, F, Zeevi, A, Rugeles, MT, Abu-Elmagd, K, Aitouche, A, Rosner, G, Trucco, M, Demetris, AJ, Rybka, W, Todo, S, Fung, JJ, Starzl, TE, Rao, AS, Fontes, P, Dodson, F, Zeevi, A, Rugeles, MT, Abu-Elmagd, K, Aitouche, A, Rosner, G, Trucco, M, Demetris, AJ, Rybka, W, Todo, S, Fung, JJ, and Starzl, TE

Published

1996

19. Combined simultaneous kidney/bone marrow transplantation

Author

Shapiro, R, Rao, AS, Fontes, P, Zeevi, A, Jordan, M, Scantlebury, VP, Vivas, C, Gritsch, HA, Corry, RJ, Egidi, F, Rugeles, MT, Rilo, H, Aitouche, A, Demetris, AJ, Rosner, G, Trucco, M, Rybka, W, Irish, W, Fung, JJ, Starzl, TE, Shapiro, R, Rao, AS, Fontes, P, Zeevi, A, Jordan, M, Scantlebury, VP, Vivas, C, Gritsch, HA, Corry, RJ, Egidi, F, Rugeles, MT, Rilo, H, Aitouche, A, Demetris, AJ, Rosner, G, Trucco, M, Rybka, W, Irish, W, Fung, JJ, and Starzl, TE

Abstract

On the basis of observations in patients with longterm (28-30 years) renal allograft survival, all of whom had evidence of systemic microchimerism, we began a program of combined simultaneous kidney/bone marrow transplantation. Between 12/14/92, and 10/31/94,36 kidney transplant recipients received 3-5 x 108 unmodified bone marrow cells/kg; 6 patients also received pancreatic islets, and 7 patients also received a pancreas. The mean recipient age was 39.0 ±10.8 years, and the mean donor age was 31.8 ±16.1 years; the mean cold ischemia time was 23.0±9.1 hr. Twenty control patients received kidneys alone, mainly because of refusal by the donor family to consent to vertebral body recovery; 3 of these patients also received a pancreas. The mean recipient age was 47.9 ±11.7 years, and the mean donor age was 41.5 ±17.9 years; the mean cold ischemia time was 28.6 ±6.2 hr. All patients received tacrolimus-based therapy, without radiation, cytoreduction, or induction antilymphocyte preparations. Blood was drawn prior to and at regular intervals after transplantation for detection of chimerism and for immunologic studies. With a mean follow-up of 11.1 ±5.8 months, all 36 study patients are alive, and 33 (92%) have functioning allografts with a mean serum creatinine of 1.9±1.2 mg/dl and a BUN of 26±9 mg/dl. Graft vs. host disease was not seen in any patient. The incidence of rejection was 72%; 11% of the patients required OKT3 or ATG for steroid-resistant rejection. The incidence of CMV was 14%, and that of delayed graft function was 17%. A total of 18 (90%) control patients are alive, and 17 (85%) have functioning allografts, with a mean serum creatinine of 2.1 ±1.3 mg/ dl, and a BUN of 30±13 mg/dl. The incidence of rejection was 60%, and 10% required OKT3 or ATG. CMV was seen in 15%, and delayed graft function in 20% (P=NS). In the study patients, chimerism was detected in the peripheral blood of 30 of 31 (97%) evaluable patients by either PCR or flow cytometry. In the contr

Published

1995

20. Combined kidney/bone marrow transplantation — Evidence of augmentation of chimerism

Author

Shapiro, R, Rao, AS, Fontes, P, Jordan, M, Scantlebury, VP, Vivas, C, Demetris, AJ, Zeevi, A, Rybka, W, Carroll, P, Trucco, M, Starzl, TE, Shapiro, R, Rao, AS, Fontes, P, Jordan, M, Scantlebury, VP, Vivas, C, Demetris, AJ, Zeevi, A, Rybka, W, Carroll, P, Trucco, M, and Starzl, TE

Published

1995

21. Augmentation with bone marrow of donor leukocyte migration for kidney, liver, heart, and pancreas islet transplantation

Author

Fontes, P, Rao, A, Demetris, AJ, Zeevi, A, Trucco, M, Carroll, P, Rybka, W, Ricordi, C, Dodson, F, Shapiro, R, Tzakis, A, Todo, S, Abu-Elmagd, K, Jordan, M, Fung, JJ, Starzl, TE, Fontes, P, Rao, A, Demetris, AJ, Zeevi, A, Trucco, M, Carroll, P, Rybka, W, Ricordi, C, Dodson, F, Shapiro, R, Tzakis, A, Todo, S, Abu-Elmagd, K, Jordan, M, Fung, JJ, and Starzl, TE

Published

1994

22. Tetraploidy in Acute Myeloid Leukemia Secondary to Large Cell Lymphoma

Author

Kaplan, S. S., primary, Rybka, W. B., additional, Blom, J., additional, and Shekhter-Levin, S., additional

Published

1998

23. POST TRANSPLANT IMMUNOTHERAPY IN METASTATIC BREAST CANCER (MBC)

Author

Magalhaes-Silverman, M, primary, Donnenberg, A, additional, Elder, E, additional, Lembersky, B, additional, Lister, J, additional, Rybka, W, additional, Whiteside, T, additional, and Ball, E D, additional

Published

1996

24. Graft failure after an umbilical cord blood transplant in a patient with severe aplastic anemia [letter] [see comments]

Author

Neudorf, SM, primary, Blatt, J, additional, Corey, S, additional, Koehler, M, additional, Wollman, M, additional, Rosner, G, additional, and Rybka, W, additional

Published

1995

25. Bone marrow augmentation of donor-cell chimerism in kidney, liver, heart, and pancreas islet transplantation

Author

Fontes, P, primary, Rao, A.S, additional, Carroll, P, additional, Dodson, F, additional, Shapiro, R, additional, Tzakis, A, additional, Todo, S, additional, Abu-Elmagd, K, additional, Jordon, M, additional, Fung, J.J, additional, Starzl, T.E, additional, Demetris, A.J, additional, Zeevi, A, additional, Trucco, M, additional, Rudert, W.A, additional, Rybka, W, additional, and Ricordi, C, additional

Published

1994

26. Enumeration of CD34+ hematopoietic stem cells for reconstitution following myeloablative therapy

Author

Roscoe, R. A., primary, Rybka, W. B., additional, Winkelstein, A., additional, Houston, A. M., additional, and Kiss, J. E., additional

Published

1994

27. Pure red cell aplasia following ABO‐incompatible bone marrow transplantation: response to erythropoietin

Author

Paltiel, O., primary, Cournoyer, D., additional, and Rybka, W., additional

Published

1993

28. Relationship of CD34+ cell dose to early and late hematopoiesis following autologous peripheral blood stem cell transplantation.

Author

Kiss, J E, Rybka, W B, Winkelstein, A, deMagalhaes-Silverman, M, Lister, J, D’Andrea, P, and Ball, E D

Subjects

*ANTIGENS, *STEM cells, *HEMATOPOIESIS, *LYMPHOMAS, *BREAST cancer

Abstract

We evaluated early and late hematopoietic reconstitution in 27 patients with advanced lymphoma, Hodgkin’s disease, and breast or ovarian cancer after treatment using high-dose/myeloablative conditioning regimens and autologous peripheral blood stem cell (PBSC) transplantation. Eighteen patients (67%) received G-CSF 5 μ g/kg/day following chemotherapy and nine (33%) were mobilized using G-CSF alone. Each patient had 7 × 108 mononuclear cells (MNC) per kg collected. G-CSF was administered post-PBSC infusion. While all patients showed prompt granulocyte recovery by day 14, platelet recovery failed to occur in four (15%) heavily pretreated patients with non-Hodgkin’s lymphoma. Retrospective analysis in 17 patients revealed that the infused number of CD34 surface antigen-positive cells correlated with time to granulocyte (r = 0.59, P = 0.012) and platelet (r = 0.58, P = 0.021) recovery. Patients receiving the higher numbers of CD34+ cells had consistently better hematologic parameters at all times examined. At 180 days post-transplant, the median Hb level was 124 g/l vs 88 g/l (P = 0.004); platelet count was 202 × 109/l vs 25 × 109/l (P = 0.004); and neutrophil count was 3100 × 106/l vs 1400 × 106/l (P = 0.15). Hemoglobin strongly correlated with the CD34+ cell dose at 360 days (r = 0.90, P = 0.01). We conclude that graft CD34+ cell content appears to be an indicator of the quality of late as well as early hematopoietic function. [ABSTRACT FROM AUTHOR]

Published

1997

29. Busulfan and cyclophosphamide (BU/CY2) as preparative regimen for patients with lymphoma.

Author

deMagalhaes-Silverman, M, Lister, J, Rybka, W, Wilson, J, and Ball, E

Subjects

LYMPHOMAS, DRUG therapy

Abstract

The combination of busulfan and cyclophosphamide has seldom been employed as a conditioning regimen for patients with lymphoma. Twenty patients with relapsed or refractory lymphoma were treated with busulfan (16 mg/kg) and cyclophosphamide (120 mg/kg) (BU/CY) followed by peripheral blood stem cell rescue in 19 patients or autologous bone marrow in one patient. There were 12 females and eight males, with a median age of 48 years (range 30–65). Four patients had Hodgkin’s disease, and 16 patients had non-Hodgkin’s lymphoma. Disease status at the time of BU/CY was: first relapse in 10 patients (four patients with chemosensitive disease and six patients with chemoresistant disease), primary refractory disease in six patients, and more advanced disease in four patients. Excessive treatment-related toxicity was not noted. There were no cases of interstitial pneumonitis, but three cases of veno-occlusive disease occurred. At 2 years, the estimated overall survival and event-free survival are 50% and 33%. We concluded that BU/CY seems to have sufficient anti- lymphoma activity, is devoid of excessive toxicity and warrants further investigation in this patient population. [ABSTRACT FROM AUTHOR]

Published

1997

30. Graft-v-host disease is associated with autoimmune-like thrombocytopenia [see comments]

Author

Anasetti, C, Rybka, W, Sullivan, KM, Banaji, M, and Slichter, SJ

Abstract

Persistent thrombocytopenia after allogeneic marrow transplantation is associated with poor patient survival. To identify the mechanisms of the thrombocytopenia, we studied platelet and fibrinogen kinetics and antiplatelet antibodies in 20 patients between 60 and 649 days (median 90) after transplantation. Seventeen patients had isolated thrombocytopenia (less than 100 X 10(9) platelets/L): the marrow cellularity was normal in five patients and slightly reduced in 12, and there was no discrepancy between thrombopoiesis and myeloerythropoiesis. Three patients had pancytopenia following marrow graft rejection (two) and relapse of leukemia (one). Only three patients had evidence of increased platelet production, indicating that in most cases there is a poor marrow response to thrombocytopenia early after marrow grafting. There was no correlation between platelet count and splenic pooling, suggesting that hypersplenism was an unlikely mechanism of the thrombocytopenia. Although there was a direct relationship between platelet count and platelet survival, the reduction in platelet survival was greater than what could be explained by the fixed platelet removal found in thrombocytopenic patients; this suggests increased platelet destruction. Seven patients had intercurrent infections that reduced both platelet and fibrinogen survivals. In addition, platelet antibodies bound to autologous or marrow donor platelets were present in five of the 12 patients studied. Patients with antiplatelet antibodies had lower platelet counts (30 +/- 10 X 10(9)/L v. 49.1 +/- 28.7 X 10(9)/L, P less than 0.05) and platelet survivals (1.32 +/- 0.92 days v. 3.58 +/- 2.02 days, P less than 0.05) than patients without antiplatelet antibodies. Furthermore, platelet- bound autoantibodies were present in five of six patients with grade II- IV acute or chronic graft-versus-host disease (GVHD), but were not present in six patients free of GVHD (P less than 0.01). We conclude that persistent thrombocytopenia after marrow transplantation is most often secondary to increased platelet destruction mediated by multiple mechanisms and that platelet autoantibodies are found in patients with acute or chronic GVHD.

Published

1989

31. Graft-ν-Host Disease is Associated With Autoimmune-like Thrombocytopenia

Author

Anasetti, C., Rybka, W., Sullivan, K.M., Banaji, M., and Slichter, S.J.

Abstract

Persistent thrombocytopenia after allogeneic marrow transplantation is associated with poor patient survival. To identify the mechanisms of the thrombocytopenia, we studied platelet and fibrinogen kinetics and antiplatelet antibodies in 20 patients between 60 and 649 days (median 90) after transplantation. Seventeen patients had isolated thrombocytopenia (<100 x 109platelets/L): the marrow cellularity was normal in five patients and slightly reduced in 12, and there was no discrepancy between thrombopoiesis and myeloerythropoiesis. Three patients had pancytopenia following marrow graft rejection (two) and relapse of leukemia (one). Only three patients had evidence of increased platelet production, indicating that in most cases there is a poor marrow response to thrombocytopenia early after marrow grafting. There was no correlation between platelet count and splenic pooling, suggesting that hypersplenism was an unlikely mechanism of the thrombocytopenia. Although there was a direct relationship between platelet count and platelet survival, the reduction in platelet survival was greater than what could be explained by the fixed platelet removal found in thrombocytopenic patients; this suggests increased platelet destruction. Seven patients had intercurrent infections that reduced both platelet and fibrinogen survivals. In addition, platelet antibodies bound to autologous or marrow donor platelets were present in five of the 12 patients studied. Patients with antiplatelet antibodies had lower platelet counts (30 ± 10 x 109/L v. 49.1 ± 28.7 x 109/L, P < 0.05) and platelet survivals (1.32 ± 0.92 days v. 3.58 ± 2.02 days, P < 0.05) than patients without antiplatelet antibodies. Furthermore, platelet-bound autoantibodies were present in five of six patients with grade ll-IV acute or chronic graft-versus-host disease (GVHD), but were not present in six patients free of GVHD (P < 0.01). We conclude that persistent thrombocytopenia after marrow transplantation is most often secondary to increased platelet destruction mediated by multiple mechanisms and that platelet autoantibodies are found in patients with acute or chronic GVHD.

Published

1989

32. Intravenous immunoglobulin therapy for refractory chronic idiopathic thrombocytopenic purpura

Author

Leclerc, J R, Sternbach, M, Solymoss, S, Sloan, D, Rybka, W B, and Blake, G

Subjects

Adult, Male, Purpura, Thrombotic Thrombocytopenic, Chronic Disease, Remission Induction, Immunization, Passive, Humans, Research Article

Published

1987

33. Allogeneic peripheral blood stem cell transplant for myelodysplasia after chemotherapy for post-transplant lymphoma in a cardiac transplant recipient at 10 years.

Author

Lister, J, Simpson, J K, deMagalhaes-Silverman, M M, Rybka, W B, Donnenberg, A D, Myers, D J, and Ball, E D

Subjects

STEM cell transplantation, MYELODYSPLASTIC syndromes, LYMPHOMAS, COMPLICATIONS from organ transplantation

Abstract

A 32-year-old male received an allogeneic peripheral blood stem cell transplant (alloPBSCT) for myelodysplasia from his one HLA-A antigen mismatched brother. He is alive with trilineage engraftment and without active GVHD 200 days after transplant. In July 1986 he underwent orthotopic cardiac transplantation for viral cardiomyopathy and has received continuous immunosuppressive therapy. A post-transplant lymphoproliferative disorder with Hodgkin-like histopathology was diagnosed in August 1993 and was successfully treated with four cycles of MOPP chemotherapy. Due to persistent pancytopenia he underwent a bone marrow aspiration and biopsy in May 1996 which revealed monosomy 7 and morphologic changes compatible with myelodysplasia. This is the first report of a cardiac transplant recipient receiving an allogeneic hematopoietic stem cell transplant. [ABSTRACT FROM AUTHOR]

Published

1997

34. Combined bone marrow and whole organ transplantation from the same donor

Author

Rao, A. S., Fontes, P., Zeevi, A., Trucco, M., Shapiro, R., Demetris, A. J., Tzakis, A. G., Carroll, P. B., Rudert, W. A., Dodson, F. S., Rybka, W. B., Pham, S. M., Scantlebury, V., Rohal, S., Camillo Ricordi, Fung, J. J., and Starzl, T. E.

Subjects

Male, Islets of Langerhans Transplantation, DNA, Middle Aged, Kidney Transplantation, Polymerase Chain Reaction, Article, Tissue Donors, Liver Transplantation, Graft vs Host Reaction, Heart Transplantation, Humans, Prednisone, Transplantation, Homologous, Female, Whole-Body Irradiation, Bone Marrow Transplantation, Follow-Up Studies

35. Xenotransplantation of hematopoietic cells resistant to HIV as a potential treatment for patients with AIDS

Author

Camillo Ricordi, Tzakis, A. G., Rybka, W. B., Fontes, P., Ball, E. D., Trucco, M., Kocova, M., Triulzi, D., Mcmichael, J., Doyle, H., Gupta, P., Fung, J. J., and Starzl, T. E.

36. Human-to-baboon bone marrow transplantation after conditioning with nonlethal irradiation

Author

Fontes, P., Rao, A. S., Camillo Ricordi, Zeevi, A., Kocova, M., Rybka, W. B., Ukah, F. O., Mullen, E., Vasko, C., Trucco, M., Demetris, A. J., Fung, J. J., and Starzl, T. E.

37. Human bone marrow obtained from vertebral bodies: Cell isolation, phenotyping, progenitor assay, and transplantation

Author

Fontes, P., Rao, A. S., Ricordi, C., Rybka, W. B., Dodson, F. S., Broznick, B., Lu, L., Zeevi, A., Thomson, A. W., Vasko, C., Seskey, T., Carroll, P. B., John Fung, and Starzl, T. E.

38. Simultaneous solid organ, bone marrow, and islet allotransplantation in type I diabetic patients

Author

Carroll, P. B., Fontes, P., Rao, A. S., Ricordi, C., Rilo, H. L. R., Zeevi, A., Trucco, M., Shapiro, R., Rybka, W. B., Scantlebury, V., Dodson, F. S., Tzakis, A. G., Rudert, W. A., Behboo, R., Karatzas, T., Khan, R., Demetris, A. J., Flohi, J., John Fung, and Starzl, T. E.

39. 127Combination sirolimus and tacrolimus immunoprophylaxis promotes engraftment of haploidentical and alternative donor stem cells with non-myeloablative conditioning in elderly and poor prognosis patients

Author

Claxton, D.F., Popescu, D., Kopp, M., Ehmann, C., and Rybka, W.

Published

2003

40. Leukotrap, a device for white cell poor platelets quality control studies In vitro and In vivo

Author

Sternbach, M., primary, Champagne, J., additional, Rybka, W., additional, and Paquin, M., additional

Published

1989

41. Treatment of relapsed acute lymphoblastic leukemia (ALL) following marrow transplantation by induction of graft-versus-host disease (GVHD) using marrow donor leukocytes

Author

Caplan, S.N., primary, Leclerc, G., additional, Prchal, J.F., additional, Rybka, W., additional, and Srolovitch, H., additional

Published

1986

42. Immunophenotyping suggests that umbilical cord blood (CB) cells contain a high proportion of multipotential CD34+ stem cells

Author

Winkelstein, A., Nimgaonkar, M., Roscoe, R.A., Rybka, W., Hamilton, P., Dracker, R., and Ball, E.D.

Subjects

Fetal blood -- Analysis, Stem cells -- Measurement, Bone marrow -- Transplantation, Business, Health care industry

Abstract

According to an abstract submitted by the authors to the 47th annual meeting of the American Association of Blood Banks, held November 12-17, 1994, in San Diego, California, 'Background: Immunophenotyping [...]

Published

1995

43. Reducing parenteral energy and protein intake improves metabolic homeostasis after bone marrow transplantation

Author

McArdle, A. H., Rybka, W. B., and Taveroff, A.

Subjects

HUMAN beings, NUTRITION

Published

1991

44. Cellular Immunotherapy for Post-transplant Lymphoproliferative Disease (PTLD) Using Recipient's Lymphokine Activated Killer (LAK) Cells Generated Ex-Vivo

Author

Rao, AS, Nalesnik, M, Elders, E, Rowe, D, Rybka, W, Zeevi, A, Whiteside, T, Pham, S, Keenan, R, Griffith, B, Fung, JJ, and Starzl, TE

Published

1996

45. Cellular immunotherapy for post-transplant lympho-proliferative disease (PTLD) using recipeint's lymphokine activated killer (LAK) cells generated Ex-Vivo

Author

Rao, A.S., Nalesnik, M., Elders, E., Rowe, D., Rybka, W., Zeevi, A., Whiteside, T., Pham, S., Keenan, R., Griffith, B., Fung, J.J., and Starzl, T.E.

Published

1996

46. FK 506 interaction with danazol.

Author

Shapiro, R, Venkataramanan, R, Warty, V S, Scantlebury, V P, Rybka, W, McCauley, J, Fung, J J, and Starzl, T E

Subjects

*DANAZOL, *DRUG interactions, *TACROLIMUS

Published

1993

47. Recurrent disease after a matched sibling hematopoietic transplant in an aplastic anemia patient with a disease risk allele, HLA-B*40:02.

Author

Khosla A, Inoue Y, Cioccio J, Rakszawski K, Songdej N, Nickolich M, Zheng H, Naik S, Ehmann C, Claxton D, Rybka W, Sivik J, Mierski J, Silar B, Vajdic C, Hohl R, Shike H, Mineishi S, and Minagawa K

Published

2024

48. Impact of post-transplant cyclophosphamide and splenomegaly on primary graft failure and multi-lineage cytopenia after allogeneic hematopoietic cell transplantation.

Author

Zulch E, Inoue Y, Cioccio J, Rakszawski K, Songdej N, Nickolich M, Zheng H, Naik S, Rybka W, Ehmann C, Sivik J, Mierski J, Silar B, Vajdic C, Greiner R, Brown V, Hohl R, Claxton D, Shike H, Paules CI, Mineishi S, and Minagawa K

Subjects

Humans, Female, Male, Middle Aged, Adult, Adolescent, Young Adult, Aged, Graft Rejection etiology, Transplantation, Homologous adverse effects, Risk Factors, Retrospective Studies, Immunosuppressive Agents adverse effects, Immunosuppressive Agents therapeutic use, Hematologic Neoplasms therapy, Child, Cytopenia, Cyclophosphamide adverse effects, Cyclophosphamide therapeutic use, Hematopoietic Stem Cell Transplantation adverse effects, Splenomegaly etiology, Graft vs Host Disease etiology

Abstract

Primary graft failure (PGF) and multi-lineage cytopenia (MLC) increase the risk of nonrelapse mortality in allogeneic hematopoietic cell transplants (HCT). We evaluated the impact of post-transplant cyclophosphamide (PTCy) and splenomegaly on PGF and MLC for hematological malignancies. This study included patients with PTCy (N=84) and conventional graft-vs.-host disease prophylaxis (N=199). The occurrence of splenomegaly varied widely, ranging from 17.1 % (acute myeloid leukemia) to 66.7 % (myeloproliferative neoplasms). Ten patients (N=8 in the PTCy and N=2 in the non- PTCy) developed PGF, and 44 patients developed MLC (both N=22). PTCy and severe splenomegaly (≥20 cm) were risk factors for PGF (odds ratio (OR): 10.40, p<0.01 and 6.74, p=0.01 respectively). Moreover, severe splenomegaly was a risk factor for PGF in PTCy patients (OR: 10.20, p=0.01). PTCy (hazard ratio (HR) 2.09, p=0.02), moderate (≥15, <20 cm, HR 4.36, p<0.01), and severe splenomegaly (HR 3.04, p=0.01) were independent risk factors for MLC. However, in subgroup analysis in PTCy patients, only mild splenomegaly (≥12, <15 cm, HR 4.62, p=0.01) was a risk factor for MLC. We recommend all patients be screened for splenomegaly before HCT, and PTCy is cautioned in those with splenomegaly., Competing Interests: Declaration of Competing Interest All authors declare no conflicts of interest associated with this manuscript., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

49. The addition of doxycycline to fluoroquinolones for bacterial prophylaxis in autologous stem cell transplantation for multiple myeloma.

Author

Guare EG, Hale CM, Sivik J, Lehman E, Inoue Y, Rakszawski K, Songdej N, Nickolich M, Zheng H, Naik S, Claxton D, Rybka W, Hohl R, Mineishi S, Minagawa K, and Paules CI

Subjects

Humans, Fluoroquinolones pharmacology, Fluoroquinolones therapeutic use, Doxycycline therapeutic use, Anti-Bacterial Agents therapeutic use, Retrospective Studies, Transplantation, Autologous adverse effects, Antibiotic Prophylaxis, Hematopoietic Stem Cell Transplantation adverse effects, Multiple Myeloma therapy, Bacteremia epidemiology, Bacteremia prevention & control, Bacteremia microbiology

Abstract

Background: Bacterial prophylaxis with a fluoroquinolone (FQ) during autologous stem cell transplant (ASCT) is common, although not standardized among transplant centers. The addition of doxycycline (doxy) to FQ prophylaxis was previously linked to reduced neutropenic fever and bacteremia in multiple myeloma (MM) patients undergoing ASCT although several confounders were present. We compared the incidence of neutropenic fever and bacteremia between MM patients variably receiving prophylaxis with FQ alone and FQ-doxy during ASCT., Methods: Systematic retrospective chart review of MM patients who underwent ASCT between January 2016 and December 2021. The primary objective was to determine the effect of bacterial prophylaxis on neutropenic fever and bacteremia within 30 days of ASCT. Multivariable logistic regression for neutropenic fever and univariate logistic regression for bacteremia accounted for differences in subject characteristics between groups., Results: Among 341 subjects, 121 received FQ and 220 received FQ-doxy for prophylaxis. Neutropenic fever developed in 67 (55.4%) and 87 (39.5%) subjects in the FQ and FQ-doxy groups, respectively (p = .005). Bacteremia was infrequent, with 5 (4.1%) and 5 (2.3%) cases developing in the FQ and FQ-doxy groups, respectively (p = .337). Among Gram-negative bacteremia events, 7/7 Escherichia coli strains were FQ-resistant, and 5/7 were ceftriaxone-resistant., Conclusion: The FQ-doxy prophylaxis group had fewer cases of neutropenic fever than the FQ group, however, there was no significant difference in bacteremia. High rates of antibiotic resistance were observed. An updated randomized controlled trial investigating appropriate prophylaxis for ASCT in the context of current oncology standards and changing antimicrobial resistance rates is warranted., (© 2024 The Authors. Transplant Infectious Disease published by Wiley Periodicals LLC.)

Published

2024

50. Donor HLA mismatch promotes full donor T-cell chimerism in the allogeneic stem cell transplant with reduced-intensity conditioning and post-transplant cyclophosphamide GVHD prophylaxis.

Author

Cioccio J, Rakszawski K, Zheng H, Nickolich M, Naik S, Wirk B, Rybka W, Ehmann C, Silar B, Vajdic C, Shah N, Tuanquin L, Greiner R, Brown V, Hohl R, Claxton D, Mineishi S, Minagawa K, and Shike H

Subjects

Humans, Chimerism, T-Lymphocytes, Cyclophosphamide therapeutic use, Stem Cell Transplantation adverse effects, HLA Antigens, Transplantation Conditioning adverse effects, Unrelated Donors, Retrospective Studies, Hematopoietic Stem Cell Transplantation adverse effects, Graft vs Host Disease etiology

Abstract

Full donor T-cell chimerism (FDTCC) after allogeneic stem cell transplant (allo-SCT) has been associated with improved outcomes in hematologic malignancy. We studied if donor human leukocyte antigen (HLA) mismatch improves achievement of FDTCC because mismatched HLA promotes donor T-cell proliferation where recipient T-cells had been impaired by previous treatment. Patients (N = 138) received allo-SCT with reduced-intensity conditioning (RIC) from 39 HLA mismatched donors (16 unrelated; 23 haploidentical) with post-transplant cyclophosphamide (PTCy) or 99 matched donors (21 siblings; 78 unrelated) with PTCy (N = 18) or non-PTCy (N = 81). Achievement of FDTCC by day 100 was higher with HLA mismatched donors than matched donors (82.1% vs. 27.3%, p < 00,001), which was further improved with 200 cGy total body irradiation (87.9%) or lymphoid (versus myeloid) malignancy (93.8%). Since all mismatched transplants used PTCy, FDTCC was higher with PTCy than non-PTCy (68.4% vs. 25.7%, p < 0.00001), but not in the matched transplant with PTCy (38.9%), negating PTCy as the primary driver. Lymphocyte recovery was delayed with PTCy than without (median on day + 30: 100 vs. 630/µL, p < 0.0001). The benefit of FDTCC was not translated into survival outcomes, especially in myeloid malignancies, possibly due to the insufficient graft-versus-tumor effects from the delayed lymphocyte recovery. Further studies are necessary to improve lymphocyte count recovery in PTCy transplants., (© 2022. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published

2023