Prognostic factors identified three risk groups in the LRF CLL4 trial, independent of treatment allocation
Prognostic factors identified three risk groups in the LRF CLL4 trial, independent of treatment allocation
BACKGROUND: Many prognostic markers have been identified in chronic lymphocytic leukemia, but there have been few opportunities to assess their relative importance in a large randomized trial. The aim of this study was to determine which of the available markers independently predicted outcome in patients requiring treatment and to use these to define new risk groups.
DESIGN AND METHODS: A broad panel of clinical and laboratory markers, measured at randomization in patients entering the LRF CLL4 trial, was assessed with respect to treatment response, progression-free and overall survival, at a median follow-up of 68 months.
RESULTS: Using the factors identified as independent predictors for progression-free survival, patients were subdivided into three risk groups: 6% had poor risk with known TP53 loss of greater than 10%; 72% had an intermediate risk without TP53 loss (? 10%) and with at least one of: unmutated IGHV genes and/or IGHV3-21 usage, 11q deletion, ?-2 microglobulin greater than 4 mg/L; 22% had a good risk (with none of the above and mutated IGHV genes). The 5-year progression-free survival rates for these three groups were 0%, 12% and 34%, respectively, and the corresponding 5-year overall survival rates were 9%, 53% and 79% (both P<0.00005 independent of treatment allocation). In the intermediate risk group 250 patients, with data for all three risk factors, were further subdivided into intermediate-low (one risk factor) or intermediate-high (2 or 3 risk factors). The 5-year progression-free survival rates were 18% and 7% (P=0.0001) and the 5-year overall survival rates were 68% and 40% (P<0.00005), respectively.
CONCLUSIONS: This study demonstrates the role of biomarkers in prognosis and shows that, in patients requiring treatment, disease stage may no longer be an independent predictor of outcome. If validated independently, the risk groups defined here may inform the design of future trials in chronic lymphocytic leukemia.
1705-1712
Oscier, David
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Wade, Rachel
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Davis, Zadie
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Morilla, Alison
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Best, Giles
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Richards, Sue
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Else, Monica
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Matutes, Estella
3da6561d-9c65-48b3-9273-db3c93f77a80
Catovsky, Daniel
0c2a5c78-d841-456e-88c7-581850d4e80a
for the UK National Cancer Research Institute (NCRI) Chronic Lymphocytic Leukaemia Working Group
1 October 2010
Oscier, David
c2620a1d-25bb-48f7-9651-f5d023636381
Wade, Rachel
aa567159-e73a-4f60-a184-e312fc656bfe
Davis, Zadie
ea848a46-b564-448f-b77f-840d86b3cbd9
Morilla, Alison
2bac5d68-04f1-46d1-a34c-445fcae365d8
Best, Giles
fb9587b6-0fc0-4b71-aa13-7ec18fa5f728
Richards, Sue
c6716b3c-db48-40e3-a714-219bb8aa91c5
Else, Monica
3d354259-1969-4d47-9eea-5b95daaf2089
Matutes, Estella
3da6561d-9c65-48b3-9273-db3c93f77a80
Catovsky, Daniel
0c2a5c78-d841-456e-88c7-581850d4e80a
Oscier, David, Wade, Rachel, Davis, Zadie, Morilla, Alison, Best, Giles, Richards, Sue, Else, Monica, Matutes, Estella and Catovsky, Daniel
,
for the UK National Cancer Research Institute (NCRI) Chronic Lymphocytic Leukaemia Working Group
(2010)
Prognostic factors identified three risk groups in the LRF CLL4 trial, independent of treatment allocation.
Haematologica, 95 (10), .
(doi:10.3324/haematol.2010.025338).
(PMID:20511662)
Abstract
BACKGROUND: Many prognostic markers have been identified in chronic lymphocytic leukemia, but there have been few opportunities to assess their relative importance in a large randomized trial. The aim of this study was to determine which of the available markers independently predicted outcome in patients requiring treatment and to use these to define new risk groups.
DESIGN AND METHODS: A broad panel of clinical and laboratory markers, measured at randomization in patients entering the LRF CLL4 trial, was assessed with respect to treatment response, progression-free and overall survival, at a median follow-up of 68 months.
RESULTS: Using the factors identified as independent predictors for progression-free survival, patients were subdivided into three risk groups: 6% had poor risk with known TP53 loss of greater than 10%; 72% had an intermediate risk without TP53 loss (? 10%) and with at least one of: unmutated IGHV genes and/or IGHV3-21 usage, 11q deletion, ?-2 microglobulin greater than 4 mg/L; 22% had a good risk (with none of the above and mutated IGHV genes). The 5-year progression-free survival rates for these three groups were 0%, 12% and 34%, respectively, and the corresponding 5-year overall survival rates were 9%, 53% and 79% (both P<0.00005 independent of treatment allocation). In the intermediate risk group 250 patients, with data for all three risk factors, were further subdivided into intermediate-low (one risk factor) or intermediate-high (2 or 3 risk factors). The 5-year progression-free survival rates were 18% and 7% (P=0.0001) and the 5-year overall survival rates were 68% and 40% (P<0.00005), respectively.
CONCLUSIONS: This study demonstrates the role of biomarkers in prognosis and shows that, in patients requiring treatment, disease stage may no longer be an independent predictor of outcome. If validated independently, the risk groups defined here may inform the design of future trials in chronic lymphocytic leukemia.
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e-pub ahead of print date: 29 May 2010
Published date: 1 October 2010
Organisations:
Cancer Sciences
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Local EPrints ID: 341577
URI: http://eprints.soton.ac.uk/id/eprint/341577
ISSN: 0390-6078
PURE UUID: 3ce2fbcf-6346-4ce2-b74c-656a8d0e50a3
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Date deposited: 30 Jul 2012 09:08
Last modified: 14 Mar 2024 11:42
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Contributors
Author:
David Oscier
Author:
Rachel Wade
Author:
Zadie Davis
Author:
Alison Morilla
Author:
Giles Best
Author:
Sue Richards
Author:
Monica Else
Author:
Estella Matutes
Author:
Daniel Catovsky
Corporate Author: for the UK National Cancer Research Institute (NCRI) Chronic Lymphocytic Leukaemia Working Group
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