Trends in utilization and outcomes of autologous transplantation as early therapy for multiple myeloma

Luciano J. Costa; Mei Jie Zhang; Xiaobo Zhong; Angela Dispenzieri; Sagar Lonial; Amrita Krishnan; Cesar Freytes; David Vesole; Robert Peter Gale; Kenneth Anderson; Baldeep Wirk; Bipin N. Savani; Edmund K. Waller; Harry Schouten; Hillard Lazarus; Kenneth Meehan; Manish Sharma; Rammurti Kamble; Ravi Vij; Shaji Kumar; Taiga Nishihori; Tamila Kindwall-Keller; Wael Saber; Parameswaran N. Hari

doi:10.1016/j.bbmt.2013.08.002

Trends in utilization and outcomes of autologous transplantation as early therapy for multiple myeloma

Luciano J. Costa, Mei Jie Zhang, Xiaobo Zhong, Angela Dispenzieri, Sagar Lonial, Amrita Krishnan, Cesar Freytes, David Vesole, Robert Peter Gale, Kenneth Anderson, Baldeep Wirk, Bipin N. Savani, Edmund K. Waller, Harry Schouten, Hillard Lazarus, Kenneth Meehan, Manish Sharma, Rammurti Kamble, Ravi Vij, Shaji KumarTaiga Nishihori, Tamila Kindwall-Keller, Wael Saber, Parameswaran N. Hari

Hematology

Research output: Contribution to journal › Article › peer-review

77 Scopus citations

Abstract

The impact of novel drugs for treating multiple myeloma (MM) on the utilization and outcomes of autologous hematopoietic progenitor cell transplantation (AHPCT) is unknown. We reviewed characteristics and outcomes of 20,278 patients who underwent AHPCT within 12months of diagnosis of MM in the United States and Canada and registered at the Center for International Blood and Marrow Transplant Research (CIBMTR) in 3 time cohorts reflecting the increasing availability of novel drugs: 1995 to 1999 (n=2226), 2000 to 2004 (n=6408), and 2005 to 2010 (n=11,644). In the United States, the number of AHPCTs performed increased at a greater rate than new MM cases. Patients in recent cohorts were older, less likely to have stage 3MM, and more likely to have received previous thalidomide, lenalidomide, or bortezomib. On multivariate analysis, AHPCT in the 2000 to 2004 cohort (HR=0.77) or in the 2005 to 2010 cohort (HR=0.68) were associated with lower risk of death. Survival at 60months post-AHPCT improved from 47% in 1995 to 1999 to 55% in 2000 to 2004 and to 57% in 2005 to 2010, owing less to improvement in progression-free survival (50% versus 55% versus 57% at 24months) than to postrelapse/progression survival (58% versus 65% versus 72% at 24months). AHPCT and new biological agents are complementary, nonredundant therapies and should be combined in the management of MM in suitable patients.

Original language	English (US)
Pages (from-to)	1615-1624
Number of pages	10
Journal	Biology of Blood and Marrow Transplantation
Volume	19
Issue number	11
DOIs	https://doi.org/10.1016/j.bbmt.2013.08.002
State	Published - Nov 2013

Keywords

Autologous stem cell transplantation
Multiple myeloma
Population study
Survival

ASJC Scopus subject areas

Hematology
Transplantation

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10.1016/j.bbmt.2013.08.002

Cite this

Costa, L. J., Zhang, M. J., Zhong, X., Dispenzieri, A., Lonial, S., Krishnan, A., Freytes, C., Vesole, D., Gale, R. P., Anderson, K., Wirk, B., Savani, B. N., Waller, E. K., Schouten, H., Lazarus, H., Meehan, K., Sharma, M., Kamble, R., Vij, R., ... Hari, P. N. (2013). Trends in utilization and outcomes of autologous transplantation as early therapy for multiple myeloma. Biology of Blood and Marrow Transplantation, 19(11), 1615-1624. https://doi.org/10.1016/j.bbmt.2013.08.002

Costa, LJ, Zhang, MJ, Zhong, X, Dispenzieri, A, Lonial, S, Krishnan, A, Freytes, C, Vesole, D, Gale, RP, Anderson, K, Wirk, B, Savani, BN, Waller, EK, Schouten, H, Lazarus, H, Meehan, K, Sharma, M, Kamble, R, Vij, R, Kumar, S, Nishihori, T, Kindwall-Keller, T, Saber, W & Hari, PN 2013, 'Trends in utilization and outcomes of autologous transplantation as early therapy for multiple myeloma', Biology of Blood and Marrow Transplantation, vol. 19, no. 11, pp. 1615-1624. https://doi.org/10.1016/j.bbmt.2013.08.002

@article{dd76efa2cf6349ba9204fba9e8111608,

title = "Trends in utilization and outcomes of autologous transplantation as early therapy for multiple myeloma",

abstract = "The impact of novel drugs for treating multiple myeloma (MM) on the utilization and outcomes of autologous hematopoietic progenitor cell transplantation (AHPCT) is unknown. We reviewed characteristics and outcomes of 20,278 patients who underwent AHPCT within 12months of diagnosis of MM in the United States and Canada and registered at the Center for International Blood and Marrow Transplant Research (CIBMTR) in 3 time cohorts reflecting the increasing availability of novel drugs: 1995 to 1999 (n=2226), 2000 to 2004 (n=6408), and 2005 to 2010 (n=11,644). In the United States, the number of AHPCTs performed increased at a greater rate than new MM cases. Patients in recent cohorts were older, less likely to have stage 3MM, and more likely to have received previous thalidomide, lenalidomide, or bortezomib. On multivariate analysis, AHPCT in the 2000 to 2004 cohort (HR=0.77) or in the 2005 to 2010 cohort (HR=0.68) were associated with lower risk of death. Survival at 60months post-AHPCT improved from 47% in 1995 to 1999 to 55% in 2000 to 2004 and to 57% in 2005 to 2010, owing less to improvement in progression-free survival (50% versus 55% versus 57% at 24months) than to postrelapse/progression survival (58% versus 65% versus 72% at 24months). AHPCT and new biological agents are complementary, nonredundant therapies and should be combined in the management of MM in suitable patients.",

keywords = "Autologous stem cell transplantation, Multiple myeloma, Population study, Survival",

author = "Costa, {Luciano J.} and Zhang, {Mei Jie} and Xiaobo Zhong and Angela Dispenzieri and Sagar Lonial and Amrita Krishnan and Cesar Freytes and David Vesole and Gale, {Robert Peter} and Kenneth Anderson and Baldeep Wirk and Savani, {Bipin N.} and Waller, {Edmund K.} and Harry Schouten and Hillard Lazarus and Kenneth Meehan and Manish Sharma and Rammurti Kamble and Ravi Vij and Shaji Kumar and Taiga Nishihori and Tamila Kindwall-Keller and Wael Saber and Hari, {Parameswaran N.}",

note = "Funding Information: Financial disclosure: The CIBMTR is supported by the Public Health Service (grant/cooperative agreement U24-CA76518) from the National Cancer Institute (NCI) , the National Heart, Lung, and Blood Institute (NHLBI) , and the National Institute of Allergy and Infectious Diseases (NIAID) ; NHLBI and NCI (grant/cooperative agreement 5U01HL069294); Health Resources and Services Administration (HRSA/DHHS; contract HHSH234200637015C); the Office of Naval Research (grants N00014-06-1-0704 and N00014-08-1-0058 ); and by grants from AABB ; Allos Inc ; Amgen Inc ; anonymous donation to the Medical College of Wisconsin; Astellas Pharma US Inc; Be the Match Foundation; Biogen IDEC; BioMarin Pharmaceutical Inc; Biovitrum AB; BloodCenter of Wisconsin; Blue Cross and Blue Shield Association; Bone Marrow Foundation; Buchanan Family Foundation; CaridianBCT; Celgene Corporation; CellGenix GmbH; Children's Leukemia Research Association; ClinImmune Labs; CTI Clinical Trial and Consulting Services; Eisai Inc; Genentech Inc; Genzyme Corporation; Histogenetics Inc; HKS Medical Information Systems; Hospira Inc.; Kirin Brewery Co Ltd; The Leukemia & Lymphoma Society; Merck & Company; The Medical College of Wisconsin; Millennium Pharmaceuticals Inc; Miller Pharmacal Group; Milliman USA Inc; Miltenyi Biotec Inc; National Marrow Donor Program; Nature Publishing Group; Novartis Oncology; Oncology Nursing Society; Osiris Therapeutics Inc; Otsuka America Pharmaceutical Inc; Pall Life Sciences; Pfizer Inc; Schering Corporation; Sigma-Tau Pharmaceuticals; Soligenix Inc; StemCyte Inc; StemSoft Software Inc; Sysmex America Inc; THERAKOS Inc; Vidacare Corporation; ViraCor Laboratories; ViroPharma Inc; and Wellpoint Inc. The views expressed in this article do not reflect the official policy or position of the National Institute of Health, the Department of the Navy, the Department of Defense, or any other agency of the US government. Funding Information: Conflict of interest statement: L.J.C. has been a consultant/advisor for Onyx and Sanofi-Aventis and has received research support from Onyx. A.D. has received research support from Millennium, Pfizer and Celgene. S.L. has been a consultant/advisor for Millennium, Celgene, Novartis, BMS, Onyx, and Sanofi-Aventis. A.K. has been a consultant/advisor for Onyx and Celgene; has received honoraria from Millenium, Onyx, and Celgene; and has stock or an ownership interest in Celgene. C.F. has received research support from Otsuka and has served on the speaker's bureau for Sanofi-Aventis. R.P.G is a part-time employee of Celgene. K.A. has been a consultant/advisor for Onyx, Sanofi-Aventis, Gilead, and Celgene. E.K.W. has received research support from Sanofi-Aventis and Otsuka. H.L. serves on the speaker's bureau for Celgene. R.V. has been a consultant for Cengene and Onyx, has received research support from Celgene and Onyx, and serves on the speaker's bureaus for Celgene, Millennium, and Onyx. S.K. has been a consultant/advisor for Onyx, Celgene, and Millenium. T.K.K. was on the speaker's bureaus for Celgene and Teva. The remaining authors have no relevant conflicts of interest to disclose. ",

year = "2013",

month = nov,

doi = "10.1016/j.bbmt.2013.08.002",

language = "English (US)",

volume = "19",

pages = "1615--1624",

journal = "Biology of Blood and Marrow Transplantation",

issn = "1083-8791",

publisher = "Elsevier Inc.",

number = "11",

}

TY - JOUR

T1 - Trends in utilization and outcomes of autologous transplantation as early therapy for multiple myeloma

AU - Costa, Luciano J.

AU - Zhang, Mei Jie

AU - Zhong, Xiaobo

AU - Dispenzieri, Angela

AU - Lonial, Sagar

AU - Krishnan, Amrita

AU - Freytes, Cesar

AU - Vesole, David

AU - Gale, Robert Peter

AU - Anderson, Kenneth

AU - Wirk, Baldeep

AU - Savani, Bipin N.

AU - Waller, Edmund K.

AU - Schouten, Harry

AU - Lazarus, Hillard

AU - Meehan, Kenneth

AU - Sharma, Manish

AU - Kamble, Rammurti

AU - Vij, Ravi

AU - Kumar, Shaji

AU - Nishihori, Taiga

AU - Kindwall-Keller, Tamila

AU - Saber, Wael

AU - Hari, Parameswaran N.

N1 - Funding Information: Financial disclosure: The CIBMTR is supported by the Public Health Service (grant/cooperative agreement U24-CA76518) from the National Cancer Institute (NCI) , the National Heart, Lung, and Blood Institute (NHLBI) , and the National Institute of Allergy and Infectious Diseases (NIAID) ; NHLBI and NCI (grant/cooperative agreement 5U01HL069294); Health Resources and Services Administration (HRSA/DHHS; contract HHSH234200637015C); the Office of Naval Research (grants N00014-06-1-0704 and N00014-08-1-0058 ); and by grants from AABB ; Allos Inc ; Amgen Inc ; anonymous donation to the Medical College of Wisconsin; Astellas Pharma US Inc; Be the Match Foundation; Biogen IDEC; BioMarin Pharmaceutical Inc; Biovitrum AB; BloodCenter of Wisconsin; Blue Cross and Blue Shield Association; Bone Marrow Foundation; Buchanan Family Foundation; CaridianBCT; Celgene Corporation; CellGenix GmbH; Children's Leukemia Research Association; ClinImmune Labs; CTI Clinical Trial and Consulting Services; Eisai Inc; Genentech Inc; Genzyme Corporation; Histogenetics Inc; HKS Medical Information Systems; Hospira Inc.; Kirin Brewery Co Ltd; The Leukemia & Lymphoma Society; Merck & Company; The Medical College of Wisconsin; Millennium Pharmaceuticals Inc; Miller Pharmacal Group; Milliman USA Inc; Miltenyi Biotec Inc; National Marrow Donor Program; Nature Publishing Group; Novartis Oncology; Oncology Nursing Society; Osiris Therapeutics Inc; Otsuka America Pharmaceutical Inc; Pall Life Sciences; Pfizer Inc; Schering Corporation; Sigma-Tau Pharmaceuticals; Soligenix Inc; StemCyte Inc; StemSoft Software Inc; Sysmex America Inc; THERAKOS Inc; Vidacare Corporation; ViraCor Laboratories; ViroPharma Inc; and Wellpoint Inc. The views expressed in this article do not reflect the official policy or position of the National Institute of Health, the Department of the Navy, the Department of Defense, or any other agency of the US government. Funding Information: Conflict of interest statement: L.J.C. has been a consultant/advisor for Onyx and Sanofi-Aventis and has received research support from Onyx. A.D. has received research support from Millennium, Pfizer and Celgene. S.L. has been a consultant/advisor for Millennium, Celgene, Novartis, BMS, Onyx, and Sanofi-Aventis. A.K. has been a consultant/advisor for Onyx and Celgene; has received honoraria from Millenium, Onyx, and Celgene; and has stock or an ownership interest in Celgene. C.F. has received research support from Otsuka and has served on the speaker's bureau for Sanofi-Aventis. R.P.G is a part-time employee of Celgene. K.A. has been a consultant/advisor for Onyx, Sanofi-Aventis, Gilead, and Celgene. E.K.W. has received research support from Sanofi-Aventis and Otsuka. H.L. serves on the speaker's bureau for Celgene. R.V. has been a consultant for Cengene and Onyx, has received research support from Celgene and Onyx, and serves on the speaker's bureaus for Celgene, Millennium, and Onyx. S.K. has been a consultant/advisor for Onyx, Celgene, and Millenium. T.K.K. was on the speaker's bureaus for Celgene and Teva. The remaining authors have no relevant conflicts of interest to disclose.

PY - 2013/11

Y1 - 2013/11

N2 - The impact of novel drugs for treating multiple myeloma (MM) on the utilization and outcomes of autologous hematopoietic progenitor cell transplantation (AHPCT) is unknown. We reviewed characteristics and outcomes of 20,278 patients who underwent AHPCT within 12months of diagnosis of MM in the United States and Canada and registered at the Center for International Blood and Marrow Transplant Research (CIBMTR) in 3 time cohorts reflecting the increasing availability of novel drugs: 1995 to 1999 (n=2226), 2000 to 2004 (n=6408), and 2005 to 2010 (n=11,644). In the United States, the number of AHPCTs performed increased at a greater rate than new MM cases. Patients in recent cohorts were older, less likely to have stage 3MM, and more likely to have received previous thalidomide, lenalidomide, or bortezomib. On multivariate analysis, AHPCT in the 2000 to 2004 cohort (HR=0.77) or in the 2005 to 2010 cohort (HR=0.68) were associated with lower risk of death. Survival at 60months post-AHPCT improved from 47% in 1995 to 1999 to 55% in 2000 to 2004 and to 57% in 2005 to 2010, owing less to improvement in progression-free survival (50% versus 55% versus 57% at 24months) than to postrelapse/progression survival (58% versus 65% versus 72% at 24months). AHPCT and new biological agents are complementary, nonredundant therapies and should be combined in the management of MM in suitable patients.

AB - The impact of novel drugs for treating multiple myeloma (MM) on the utilization and outcomes of autologous hematopoietic progenitor cell transplantation (AHPCT) is unknown. We reviewed characteristics and outcomes of 20,278 patients who underwent AHPCT within 12months of diagnosis of MM in the United States and Canada and registered at the Center for International Blood and Marrow Transplant Research (CIBMTR) in 3 time cohorts reflecting the increasing availability of novel drugs: 1995 to 1999 (n=2226), 2000 to 2004 (n=6408), and 2005 to 2010 (n=11,644). In the United States, the number of AHPCTs performed increased at a greater rate than new MM cases. Patients in recent cohorts were older, less likely to have stage 3MM, and more likely to have received previous thalidomide, lenalidomide, or bortezomib. On multivariate analysis, AHPCT in the 2000 to 2004 cohort (HR=0.77) or in the 2005 to 2010 cohort (HR=0.68) were associated with lower risk of death. Survival at 60months post-AHPCT improved from 47% in 1995 to 1999 to 55% in 2000 to 2004 and to 57% in 2005 to 2010, owing less to improvement in progression-free survival (50% versus 55% versus 57% at 24months) than to postrelapse/progression survival (58% versus 65% versus 72% at 24months). AHPCT and new biological agents are complementary, nonredundant therapies and should be combined in the management of MM in suitable patients.

KW - Autologous stem cell transplantation

KW - Multiple myeloma

KW - Population study

KW - Survival

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Trends in utilization and outcomes of autologous transplantation as early therapy for multiple myeloma

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