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Monitoring CML patients responding to treatment with tyrosine kinase inhibitors: review and recommendations for harmonizing current methodology for detecting BCR-ABL transcripts and kinase domain mutations and for expressing results

Monitoring CML patients responding to treatment with tyrosine kinase inhibitors: review and recommendations for harmonizing current methodology for detecting BCR-ABL transcripts and kinase domain mutations and for expressing results
Monitoring CML patients responding to treatment with tyrosine kinase inhibitors: review and recommendations for harmonizing current methodology for detecting BCR-ABL transcripts and kinase domain mutations and for expressing results
The introduction in 1998 of imatinib mesylate (IM) revolutionized management of patients with chronic myeloid leukemia (CML) and the second generation of tyrosine kinase inhibitors may prove superior to IM. Real-time quantitative polymerase chain reaction (RQ-PCR) provides an accurate measure of the total leukemiacell mass and the degree to which BCR-ABL transcripts are reduced by therapy correlates with progression-free survival. Because a rising level of BCR-ABL is an early indication of loss of response and thus the need to reassess therapeutic strategy, regular molecular monitoring of individual patients is clearly desirable. Here we summarize the results of a consensus meeting that took place at the National Institutes of Health (NIH) in Bethesda in October 2005. We make suggestions for (1) harmonizing the differing methodologies for measuring BCR-ABL transcripts in patients with CML undergoing treatment and using a conversion factor whereby individual laboratories can express BCR-ABL transcript levels on an internationally agreed scale; (2) using serial RQ-PCR results rather than bone marrow cytogenetics or fluorescence in situ hybridization (FISH) for the BCR-ABL gene to monitor individual patients responding to treatment; and (3) detecting and reporting Philadelphia (Ph) chromosome-positive subpopulations bearing BCR-ABL kinase domain mutations. We recognize that our recommendations are provisional and will require revision as new evidence emerges.
methods, research, humans, therapy, patients, tertiary, proteins, chronic, myelogenous, reverse transcriptase polymerase chain reaction, research support, polymerase chain reaction, treatment, protein kinase inhibitors, protein, standards, leukemia, drug monitoring, fluorescence, survival, protein-tyrosine kinases, laboratories, protein structure, bone marrow, diagnosis, protein-tyrosine kinase, australia, in situ hybridization, mutation, drug therapy, bcr-abl, health, review, therapeutic use, fusion proteins, sensitivity and specificity, bcr-abl positive, bone, genetics, antagonists & inhibitors, tyrosine, cytogenetics
0006-4971
28-37
Hughes, T.
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Deininger, M.
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Hochhaus, A.
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Branford, S.
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Radich, J.
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Kaeda, J.
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Baccarani, M.
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Cortes, J.
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Cross, N.C.
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Druker, B.J.
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Gabert, J.
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Grimwade, D.
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Hehlmann, R.
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Kamel-Reid, S.
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Lipton, J.H.
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Longtine, J.
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Martinelli, G.
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Saglio, G.
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Soverini, S.
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Stock, W.
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Goldman, J.M.
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Hughes, T.
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Deininger, M.
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Hochhaus, A.
4c0b9da4-adfa-4253-8af7-78cec9e9a24f
Branford, S.
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Radich, J.
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Kaeda, J.
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Baccarani, M.
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Cortes, J.
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Cross, N.C.
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Druker, B.J.
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Gabert, J.
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Grimwade, D.
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Hehlmann, R.
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Kamel-Reid, S.
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Lipton, J.H.
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Longtine, J.
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Martinelli, G.
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Saglio, G.
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Soverini, S.
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Stock, W.
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Goldman, J.M.
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Hughes, T., Deininger, M., Hochhaus, A., Branford, S., Radich, J., Kaeda, J., Baccarani, M., Cortes, J., Cross, N.C., Druker, B.J., Gabert, J., Grimwade, D., Hehlmann, R., Kamel-Reid, S., Lipton, J.H., Longtine, J., Martinelli, G., Saglio, G., Soverini, S., Stock, W. and Goldman, J.M. (2006) Monitoring CML patients responding to treatment with tyrosine kinase inhibitors: review and recommendations for harmonizing current methodology for detecting BCR-ABL transcripts and kinase domain mutations and for expressing results. Blood, 108 (1), 28-37. (doi:10.1182/blood-2006-01-0092).

Record type: Article

Abstract

The introduction in 1998 of imatinib mesylate (IM) revolutionized management of patients with chronic myeloid leukemia (CML) and the second generation of tyrosine kinase inhibitors may prove superior to IM. Real-time quantitative polymerase chain reaction (RQ-PCR) provides an accurate measure of the total leukemiacell mass and the degree to which BCR-ABL transcripts are reduced by therapy correlates with progression-free survival. Because a rising level of BCR-ABL is an early indication of loss of response and thus the need to reassess therapeutic strategy, regular molecular monitoring of individual patients is clearly desirable. Here we summarize the results of a consensus meeting that took place at the National Institutes of Health (NIH) in Bethesda in October 2005. We make suggestions for (1) harmonizing the differing methodologies for measuring BCR-ABL transcripts in patients with CML undergoing treatment and using a conversion factor whereby individual laboratories can express BCR-ABL transcript levels on an internationally agreed scale; (2) using serial RQ-PCR results rather than bone marrow cytogenetics or fluorescence in situ hybridization (FISH) for the BCR-ABL gene to monitor individual patients responding to treatment; and (3) detecting and reporting Philadelphia (Ph) chromosome-positive subpopulations bearing BCR-ABL kinase domain mutations. We recognize that our recommendations are provisional and will require revision as new evidence emerges.

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More information

Published date: 2006
Keywords: methods, research, humans, therapy, patients, tertiary, proteins, chronic, myelogenous, reverse transcriptase polymerase chain reaction, research support, polymerase chain reaction, treatment, protein kinase inhibitors, protein, standards, leukemia, drug monitoring, fluorescence, survival, protein-tyrosine kinases, laboratories, protein structure, bone marrow, diagnosis, protein-tyrosine kinase, australia, in situ hybridization, mutation, drug therapy, bcr-abl, health, review, therapeutic use, fusion proteins, sensitivity and specificity, bcr-abl positive, bone, genetics, antagonists & inhibitors, tyrosine, cytogenetics
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Identifiers

Local EPrints ID: 59867
URI: http://eprints.soton.ac.uk/id/eprint/59867
DOI: doi:10.1182/blood-2006-01-0092
ISSN: 0006-4971
PURE UUID: 91ce7fe3-f294-41ae-b9b5-fcfe2bf092b4
ORCID for N.C. Cross: ORCID iD orcid.org/0000-0001-5481-2555

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Date deposited: 02 Sep 2008
Last modified: 16 Mar 2024 03:23

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Contributors

Author: T. Hughes
Author: M. Deininger
Author: A. Hochhaus
Author: S. Branford
Author: J. Radich
Author: J. Kaeda
Author: M. Baccarani
Author: J. Cortes
Author: N.C. Cross ORCID iD
Author: B.J. Druker
Author: J. Gabert
Author: D. Grimwade
Author: R. Hehlmann
Author: S. Kamel-Reid
Author: J.H. Lipton
Author: J. Longtine
Author: G. Martinelli
Author: G. Saglio
Author: S. Soverini
Author: W. Stock
Author: J.M. Goldman

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