EHA Library - The official digital education library of European Hematology Association (EHA)

AUTOLOGOUS STEM CELL TRANSPLANTATION IS SAFE AND EFFECTIVE FOR OLDER MYELOMA PATIENTS: RESULTS FROM THE MYELOMA XI TRIAL
Author(s): ,
Charlotte Pawlyn
Affiliations:
The Institute of Cancer Research,London,United Kingdom;The Royal Marsden Hospital,London,United Kingdom
,
Faith Davies
Affiliations:
Myeloma Institute,University of Arkansas for Medical Sciences,Little Rock,United States
,
Alina Striha
Affiliations:
Clinical Trials Research Unit,Leeds Institute of Clinical Trials Research,Leeds,United Kingdom
,
David Cairns
Affiliations:
Clinical Trials Research Unit,Leeds Institute of Clinical Trials Research,Leeds,United Kingdom
,
John Jones
Affiliations:
The Institute of Cancer Research,London,United Kingdom
,
Bhuvan Kishore
Affiliations:
Heart of England Foundation Trust,Birmingham,United Kingdom
,
Mamta Garg
Affiliations:
Leicester Royal Infirmary,Leicester,United Kingdom
,
Cathy Williams
Affiliations:
Centre for Clinical Haematology,Nottingham University Hospital,Nottingham,United Kingdom
,
Kamaraj Karunanithi
Affiliations:
University Hospital of North Midlands,Stoke-on-Trent,United Kingdom
,
Jindriska Lindsay
Affiliations:
Kent and Canterbury NHS Trust,Canterbury,United Kingdom
,
Matthew Jenner
Affiliations:
University Hospital Southampton NHS Foundation Trust,Southampton,United Kingdom
,
Gordon Cook
Affiliations:
Leeds Institute of Cancer and Pathology,Leeds,United Kingdom
,
Nigel Russell
Affiliations:
Centre for Clinical Haematology,Nottingham University Hospital,Nottingham,United Kingdom
,
Mark Drayson
Affiliations:
Institute of Immunology and Immunotherapy,Birmingham,United Kingdom
,
Martin Kaiser
Affiliations:
The Institute of Cancer Research,London,United Kingdom;The Royal Marsden Hospital,London,United Kingdom
,
Roger Owen
Affiliations:
St James’s University Hospital,Leeds,United Kingdom
,
Walter Gregory
Affiliations:
Clinical Trials Research Unit,Leeds Institute of Clinical Trials Research,Leeds,United Kingdom
,
Gareth Morgan
Affiliations:
Myeloma Institute,University of Arkansas for Medical Sciences,Little Rock,United States
Graham Jackson
Affiliations:
Department of Haematology,Newcastle University,Newcastle,United Kingdom
(Abstract release date: 05/17/18) EHA Library. Pawlyn C. 06/15/18; 214501; S106
Dr. Charlotte Pawlyn
Dr. Charlotte Pawlyn
Contributions
Abstract

Abstract: S106

Type: Oral Presentation

Presentation during EHA23: On Friday, June 15, 2018 from 11:45 - 12:00

Location: Victoria Hall

Background
The introduction of high-dose therapy with autologous stem cell transplant (ASCT) for myeloma patients in the early 2000s led to a significant improvement in outcomes. Despite the further advances made with the introduction of novel agents, ASCT remains the standard of care for all eligible patients. Initial ASCT studies recruited only patients aged less than 65 years, but registry data suggests a recent increase in transplants for patients aged 65-75.  There are few studies that directly compare ASCT to no ASCT in this age group and the upper age limit for ASCT in routine clinical practice varies around the world. 

Aims

We sought to evaluate the outcomes of older patients receiving ASCT within the UK NCRI Myeloma XI trial.

Methods

The Myeloma XI trial, recruited patients to two pathways; one for younger/fitter patients considered transplant eligible (TE) and one for transplant ineligible patients (TNE).  The choice of pathway was determined on an individual basis, based on performance status, clinician judgment and participant preference. Patients were randomized to receive either thalidomide or lenalidomide combined with cyclophosphamide and dexamethasone (CTD vs CRD, dose attenuated for TNE) for a minimum of 4 (TE) or 6 (TNE) cycles and to maximum response.  Some patients with a suboptimal response received further induction therapy with a proteasome inhibitor based triplet (CVD). TE patients were planned to receive 200mg/m2 melphalan prior to ASCT. There was a maintenance randomization to lenalidomide, lenalidomide/vorinostat or observation. This post-hoc analysis compared outcomes for TE patients of different ages and those of age-matched TNE patients. 

Results

2042 patients were recruited to the TE pathway of the study with median age 61 years(y), range 28-75. 27% (546/2042) of TE patients were aged 65-69y and 5% (101/2042) aged 70-75y. Older patients were less likely to ultimately undergo ASCT than younger patients, despite having entered the TE pathway, (<65y 67%, 65-69y 55%, >=70y 44%).  The reasons given for not undergoing ASCT were more often related to patient fitness in those over 65y. Median CD34+ cell collection also decreased with age from 4.6x106 <65y to 3.8 x106 65-69y to 3.1x106 >=70y.  For those patients who underwent ASCT having entered the TE pathway (<65y n=931, 65-69y n=299 and >=70y n=44) median PFS shortened with increasing age but overall survival was not significantly different (Median PFS: <65y 46.5months, 65-69y 38.7m, >=70y 30.1m and OS: <65y 69m, 65-69y 63.8m, >=70y not reached). There was no difference in 100-day post ASCT mortality between age groups.

1852 patients were concurrently recruited to the TNE pathway with median age 74y, range 54-92. The TE and TNE patients’ ages overlapped as shown in Figure 1.  We defined a group of best-age-matched patients between the TE and TNE pathways that comprised 389 TE patients who received ASCT (TE-ASCT), 310 TE patients who did not (TE-noASCT) and 382 TNE patients. Patients undergoing transplantation had significantly improved outcomes compared to those that did not, irrespective of whether ASCT had been initially planned (Median PFS: TE-ASCT 42.9m, TE-noASCT 15.9m, TNE 17.2m and Median OS: TE-ASCT 63.8m, TE-noASCT 46,1m, TNE 45.8m). These differences were independent of the use of ongoing maintenance therapy.

Conclusion

Our data suggests that ASCT improves outcomes for newly diagnosed myeloma patients and supports its use as standard of care for all considered able to tolerate the procedure, without strict age limits.

Session topic: 14. Myeloma and other monoclonal gammopathies - Clinical

Keyword(s): Autologous bone marrow transplant, Myeloma

Abstract: S106

Type: Oral Presentation

Presentation during EHA23: On Friday, June 15, 2018 from 11:45 - 12:00

Location: Victoria Hall

Background
The introduction of high-dose therapy with autologous stem cell transplant (ASCT) for myeloma patients in the early 2000s led to a significant improvement in outcomes. Despite the further advances made with the introduction of novel agents, ASCT remains the standard of care for all eligible patients. Initial ASCT studies recruited only patients aged less than 65 years, but registry data suggests a recent increase in transplants for patients aged 65-75.  There are few studies that directly compare ASCT to no ASCT in this age group and the upper age limit for ASCT in routine clinical practice varies around the world. 

Aims

We sought to evaluate the outcomes of older patients receiving ASCT within the UK NCRI Myeloma XI trial.

Methods

The Myeloma XI trial, recruited patients to two pathways; one for younger/fitter patients considered transplant eligible (TE) and one for transplant ineligible patients (TNE).  The choice of pathway was determined on an individual basis, based on performance status, clinician judgment and participant preference. Patients were randomized to receive either thalidomide or lenalidomide combined with cyclophosphamide and dexamethasone (CTD vs CRD, dose attenuated for TNE) for a minimum of 4 (TE) or 6 (TNE) cycles and to maximum response.  Some patients with a suboptimal response received further induction therapy with a proteasome inhibitor based triplet (CVD). TE patients were planned to receive 200mg/m2 melphalan prior to ASCT. There was a maintenance randomization to lenalidomide, lenalidomide/vorinostat or observation. This post-hoc analysis compared outcomes for TE patients of different ages and those of age-matched TNE patients. 

Results

2042 patients were recruited to the TE pathway of the study with median age 61 years(y), range 28-75. 27% (546/2042) of TE patients were aged 65-69y and 5% (101/2042) aged 70-75y. Older patients were less likely to ultimately undergo ASCT than younger patients, despite having entered the TE pathway, (<65y 67%, 65-69y 55%, >=70y 44%).  The reasons given for not undergoing ASCT were more often related to patient fitness in those over 65y. Median CD34+ cell collection also decreased with age from 4.6x106 <65y to 3.8 x106 65-69y to 3.1x106 >=70y.  For those patients who underwent ASCT having entered the TE pathway (<65y n=931, 65-69y n=299 and >=70y n=44) median PFS shortened with increasing age but overall survival was not significantly different (Median PFS: <65y 46.5months, 65-69y 38.7m, >=70y 30.1m and OS: <65y 69m, 65-69y 63.8m, >=70y not reached). There was no difference in 100-day post ASCT mortality between age groups.

1852 patients were concurrently recruited to the TNE pathway with median age 74y, range 54-92. The TE and TNE patients’ ages overlapped as shown in Figure 1.  We defined a group of best-age-matched patients between the TE and TNE pathways that comprised 389 TE patients who received ASCT (TE-ASCT), 310 TE patients who did not (TE-noASCT) and 382 TNE patients. Patients undergoing transplantation had significantly improved outcomes compared to those that did not, irrespective of whether ASCT had been initially planned (Median PFS: TE-ASCT 42.9m, TE-noASCT 15.9m, TNE 17.2m and Median OS: TE-ASCT 63.8m, TE-noASCT 46,1m, TNE 45.8m). These differences were independent of the use of ongoing maintenance therapy.

Conclusion

Our data suggests that ASCT improves outcomes for newly diagnosed myeloma patients and supports its use as standard of care for all considered able to tolerate the procedure, without strict age limits.

Session topic: 14. Myeloma and other monoclonal gammopathies - Clinical

Keyword(s): Autologous bone marrow transplant, Myeloma

By clicking “Accept Terms & all Cookies” or by continuing to browse, you agree to the storing of third-party cookies on your device to enhance your user experience and agree to the user terms and conditions of this learning management system (LMS).

Cookie Settings
Accept Terms & all Cookies