Phase I Study of Flavopiridol in Combination with Imatinib Mesylate (STI571, Gleevec) in Bcr/Abl+ Hematological Malignancies

Phase I Study of Flavopiridol in Combination with Imatinib Mesylate (STI571, Gleevec) in Bcr/Abl+ Hematological Malignancies

Imatinib (Im), a rationally designed inhibitor of the Bcr/Abl kinase as well as other kinases, represents the standard treatment for Bcr/Abl+ malignancies. Im as a single agent, however, is not curative. Flavopiridol (Fl), an investigational cyclin dependent kinase inhibitor, is broadly active in vi...

Full description

Saved in:
Bibliographic Details
Published in:Blood Vol. 106; no. 11; p. 1102
Main Authors: Grant, Steven, Karp, Judith E., Koc, Omer N., Cooper, Brenda, Luger, Selina, Figg, William D., Egorin, Merrill, Druker, Brian J., Jacobberger, James W., Ramakrishnan, Viswanathan, Perkins, Edward B., Colevas, A. Dimitrios, Roberts, John D.
Format: Journal Article
Language:English
Published: Elsevier Inc 16-11-2005
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Abstract Imatinib (Im), a rationally designed inhibitor of the Bcr/Abl kinase as well as other kinases, represents the standard treatment for Bcr/Abl+ malignancies. Im as a single agent, however, is not curative. Flavopiridol (Fl), an investigational cyclin dependent kinase inhibitor, is broadly active in vitro against human leukemia cells (Blood 91:2482, 1998). Previously we have shown that simultaneous disruption of a survival signaling pathway and a cell cycle regulatory pathway results in a pronounced increase in leukemic cell death (Cancer Res. 61:5106, 2001) and in more recent preclinical studies demonstrated synergistic interactions between Im and Fl in Bcr/Abl+ leukemia cells, including some that were resistant to Im (Clin Cancer Res 8;2976, 2002). Based on these considerations, we have initiated a phase I trial to identify appropriate doses of Im+Fl for further investigation. Eligible patients (pts) have CML with a suboptimal response to prior Im, CML in blast crisis, or Bcr/Abl+ acute lymphocytic leukemia (ALL). CML-BC and ALL patients may be Im-naïve. Pts receive Im by continuous daily oral dosing and Fl by 1 hour intravenous infusion weekly x 3 repeated every 4 weeks. Targeted dose levels are (Fl/Im; mg/m2): 30/400, 30/600, 45/600, 60/600, 60/800, 60/1000. Patients are divided into 2 strata based upon blast percentage in peripheral blood or bone marrow: stratum 1, <15%; and stratum 2, ≥15%. For stratum 1 dose limiting toxicity (DLT) is defined as NCI CTCAE grade 4 ANC/platelet for > 1 week or grade ≥ 3 non-heme toxicity; for stratum 2, DLT is profound marrow hypoplasia in the absence of persistent leukemia. In stratum 1, 16 pts have been treated at 4 dose levels; in stratum 2, 5 pts in the 1st and 3rd dose level. In stratum 1, 1 DLT has occurred at dose level 4 (cholecystitis requiring cholecystectomy); in stratum 2, 1 DLT has occurred at dose level 3 (sepsis/multi-organ failure which was not clearly related to treatment). The only frequent toxicities have been hematological. 4 pts have experienced objective responses including complete hematological remissions in 2 pts in stratum 1 treated with Im/Fl 30/600 who had been previously treated with Im 800 and complete hematological remissions in 2 pts in stratum 2 (who had not received prior Im). Preliminary studies indicate no Fl impact upon Im pharmacokinetics, and variable post-treatment effects on signaling pathways in CML cells. These findings indicate that a regimen consisting of Fl and Im is tolerable and active in at least some patients with Bcr/Abl+ hematologic malignancies, including some with Im-resistant disease. Pending identification of the MTD and the recommended Phase II dose (RPTD), Phase II trials will be necessary to assess the activity of this strategy more definitively.
AbstractList Imatinib (Im), a rationally designed inhibitor of the Bcr/Abl kinase as well as other kinases, represents the standard treatment for Bcr/Abl+ malignancies. Im as a single agent, however, is not curative. Flavopiridol (Fl), an investigational cyclin dependent kinase inhibitor, is broadly active in vitro against human leukemia cells (Blood 91:2482, 1998). Previously we have shown that simultaneous disruption of a survival signaling pathway and a cell cycle regulatory pathway results in a pronounced increase in leukemic cell death (Cancer Res. 61:5106, 2001) and in more recent preclinical studies demonstrated synergistic interactions between Im and Fl in Bcr/Abl+ leukemia cells, including some that were resistant to Im (Clin Cancer Res 8;2976, 2002). Based on these considerations, we have initiated a phase I trial to identify appropriate doses of Im+Fl for further investigation. Eligible patients (pts) have CML with a suboptimal response to prior Im, CML in blast crisis, or Bcr/Abl+ acute lymphocytic leukemia (ALL). CML-BC and ALL patients may be Im-naïve. Pts receive Im by continuous daily oral dosing and Fl by 1 hour intravenous infusion weekly x 3 repeated every 4 weeks. Targeted dose levels are (Fl/Im; mg/m2): 30/400, 30/600, 45/600, 60/600, 60/800, 60/1000. Patients are divided into 2 strata based upon blast percentage in peripheral blood or bone marrow: stratum 1, <15%; and stratum 2, ≥15%. For stratum 1 dose limiting toxicity (DLT) is defined as NCI CTCAE grade 4 ANC/platelet for > 1 week or grade ≥ 3 non-heme toxicity; for stratum 2, DLT is profound marrow hypoplasia in the absence of persistent leukemia. In stratum 1, 16 pts have been treated at 4 dose levels; in stratum 2, 5 pts in the 1st and 3rd dose level. In stratum 1, 1 DLT has occurred at dose level 4 (cholecystitis requiring cholecystectomy); in stratum 2, 1 DLT has occurred at dose level 3 (sepsis/multi-organ failure which was not clearly related to treatment). The only frequent toxicities have been hematological. 4 pts have experienced objective responses including complete hematological remissions in 2 pts in stratum 1 treated with Im/Fl 30/600 who had been previously treated with Im 800 and complete hematological remissions in 2 pts in stratum 2 (who had not received prior Im). Preliminary studies indicate no Fl impact upon Im pharmacokinetics, and variable post-treatment effects on signaling pathways in CML cells. These findings indicate that a regimen consisting of Fl and Im is tolerable and active in at least some patients with Bcr/Abl+ hematologic malignancies, including some with Im-resistant disease. Pending identification of the MTD and the recommended Phase II dose (RPTD), Phase II trials will be necessary to assess the activity of this strategy more definitively.
Imatinib (Im), a rationally designed inhibitor of the Bcr/Abl kinase as well as other kinases, represents the standard treatment for Bcr/Abl+ malignancies. Im as a single agent, however, is not curative. Flavopiridol (Fl), an investigational cyclin dependent kinase inhibitor, is broadly active in vitro against human leukemia cells (Blood91:2482,1998). Previously we have shown that simultaneous disruption of a survival signaling pathway and a cell cycle regulatory pathway results in a pronounced increase in leukemic cell death (Cancer Res.61:5106,2001) and in more recent preclinical studies demonstrated synergistic interactions between Im and Fl in Bcr/Abl+ leukemia cells, including some that were resistant to Im (Clin Cancer Res8;2976,2002). Based on these considerations, we have initiated a phase I trial to identify appropriate doses of Im+Fl for further investigation. Eligible patients (pts) have CML with a suboptimal response to prior Im, CML in blast crisis, or Bcr/Abl+ acute lymphocytic leukemia (ALL). CML-BC and ALL patients may be Im-naïve. Pts receive Im by continuous daily oral dosing and Fl by 1 hour intravenous infusion weekly x 3 repeated every 4 weeks. Targeted dose levels are (Fl/Im; mg/m2): 30/400, 30/600, 45/600, 60/600, 60/800, 60/1000. Patients are divided into 2 strata based upon blast percentage in peripheral blood or bone marrow: stratum 1, <15%; and stratum 2, ≥15%. For stratum 1 dose limiting toxicity (DLT) is defined as NCI CTCAE grade 4 ANC/platelet for > 1 week or grade ≥ 3 non-heme toxicity; for stratum 2, DLT is profound marrow hypoplasia in the absence of persistent leukemia. In stratum 1, 16 pts have been treated at 4 dose levels; in stratum 2, 5 pts in the 1st and 3rd dose level. In stratum 1, 1 DLT has occurred at dose level 4 (cholecystitis requiring cholecystectomy); in stratum 2, 1 DLT has occurred at dose level 3 (sepsis/multi-organ failure which was not clearly related to treatment). The only frequent toxicities have been hematological. 4 pts have experienced objective responses including complete hematological remissions in 2 pts in stratum 1 treated with Im/Fl 30/600 who had been previously treated with Im 800 and complete hematological remissions in 2 pts in stratum 2 (who had not received prior Im). Preliminary studies indicate no Fl impact upon Im pharmacokinetics, and variable post-treatment effects on signaling pathways in CML cells. These findings indicate that a regimen consisting of Fl and Im is tolerable and active in at least some patients with Bcr/Abl+ hematologic malignancies, including some with Im-resistant disease. Pending identification of the MTD and the recommended Phase II dose (RPTD), Phase II trials will be necessary to assess the activity of this strategy more definitively.
Author Jacobberger, James W.
Roberts, John D.
Karp, Judith E.
Perkins, Edward B.
Colevas, A. Dimitrios
Luger, Selina
Figg, William D.
Cooper, Brenda
Grant, Steven
Koc, Omer N.
Egorin, Merrill
Druker, Brian J.
Ramakrishnan, Viswanathan
Author_xml – sequence: 1
  givenname: Steven
  surname: Grant
  fullname: Grant, Steven
  organization: Massey Cancer Center, Virginia Commonwealth University, Richmond, VA
– sequence: 2
  givenname: Judith E.
  surname: Karp
  fullname: Karp, Judith E.
  organization: Sidney Kimmel Cancer Center, Johns Hopkins University, Baltimore, MD
– sequence: 3
  givenname: Omer N.
  surname: Koc
  fullname: Koc, Omer N.
  organization: Ireland Cancer Center, Case Western Reserve University, Cleveland, OH
– sequence: 4
  givenname: Brenda
  surname: Cooper
  fullname: Cooper, Brenda
  organization: Ireland Cancer Center, Case Western Reserve University, Cleveland, OH
– sequence: 5
  givenname: Selina
  surname: Luger
  fullname: Luger, Selina
  organization: University of Pennsylvania Cancer Center, University of Pennsylvania, Philadelphia, PA
– sequence: 6
  givenname: William D.
  surname: Figg
  fullname: Figg, William D.
  organization: Cancer Therapeutics Branch, National Cancer Institute, Bethesda, MD
– sequence: 7
  givenname: Merrill
  surname: Egorin
  fullname: Egorin, Merrill
  organization: University of Pittsburgh Cancer Institute, University of Pittsburgh, Pittsburgh, PA
– sequence: 8
  givenname: Brian J.
  surname: Druker
  fullname: Druker, Brian J.
  organization: Howard Hughes Medical Institute, Oregon Health and Science University, Portland, OR
– sequence: 9
  givenname: James W.
  surname: Jacobberger
  fullname: Jacobberger, James W.
  organization: Ireland Cancer Center, Case Western Reserve University, Cleveland, OH
– sequence: 10
  givenname: Viswanathan
  surname: Ramakrishnan
  fullname: Ramakrishnan, Viswanathan
  organization: Massey Cancer Center, Virginia Commonwealth University, Richmond, VA
– sequence: 11
  givenname: Edward B.
  surname: Perkins
  fullname: Perkins, Edward B.
  organization: Massey Cancer Center, Virginia Commonwealth University, Richmond, VA
– sequence: 12
  givenname: A. Dimitrios
  surname: Colevas
  fullname: Colevas, A. Dimitrios
  organization: Cancer Treatment and Evaluation Program, National Cancer Institute, Behtesda, MD
– sequence: 13
  givenname: John D.
  surname: Roberts
  fullname: Roberts, John D.
  organization: Massey Cancer Center, Virginia Commonwealth University, Richmond, VA
BookMark eNqFkF9LwzAUxYMouE0_g3lUtNtNtqbt4xzuD2wobPpa0vR2i2TJaOpk4Ic323wXLudyLpzL4dcml9ZZJOSOQZexlPcK41zZ_WAggg8D_CQXpMVinkYAHC5JCwBENMgSdk3a3n8CsEGfxy3y87aRHumMLpuv8kBdRcdG7t1O17p0hmpLR25baCsb7Sz91s2GzrbBWF3QBfqDkQ3S--VqFifsiU4M4h7VwzH3rOresDCPdIoh4IxbayUNXUij11ZapdHfkKtKGo-3f7tD3scvq9E0mr9OZqPhPFJMAI9ShUKJKpZJrKDPZFpiJThmXJZVUQ1Snop0IDDOEFAwySDNAJKyCPeiX3Hod0hy_qtq532NVb6r9VbWh5xBfoSYnyDmR4jB50d-JwnJ4TmJod5eY537UNwqLHWNqslLp__98QtSk33e
CitedBy_id crossref_primary_10_1158_0008_5472_CAN_06_1216
crossref_primary_10_1182_asheducation_2008_1_427
crossref_primary_10_1186_1471_2407_13_242
ContentType Journal Article
Copyright 2005 American Society of Hematology
Copyright_xml – notice: 2005 American Society of Hematology
DBID 6I.
AAFTH
AAYXX
CITATION
DOI 10.1182/blood.V106.11.1102.1102
DatabaseName ScienceDirect Open Access Titles
Elsevier:ScienceDirect:Open Access
CrossRef
DatabaseTitle CrossRef
DatabaseTitleList
CrossRef
DeliveryMethod fulltext_linktorsrc
Discipline Medicine
Chemistry
Biology
Anatomy & Physiology
EISSN 1528-0020
EndPage 1102
ExternalDocumentID 10_1182_blood_V106_11_1102_1102
S0006497119759928
GroupedDBID ---
-~X
.55
.GJ
1CY
23N
2WC
34G
39C
4.4
53G
5GY
5RE
5VS
6I.
6J9
9M8
AAEDW
AAFTH
AAXUO
ABOCM
ABVKL
ACGFO
ADBBV
AENEX
AFFNX
AFOSN
AHPSJ
AI.
ALMA_UNASSIGNED_HOLDINGS
BAWUL
BTFSW
C1A
CS3
DIK
DU5
E3Z
EBS
EJD
EX3
F5P
FDB
FRP
GS5
GX1
IH2
J5H
K-O
KQ8
L7B
LSO
MJL
N4W
N9A
OK1
P2P
R.V
RHF
RHI
ROL
SJN
THE
TR2
TWZ
VH1
W2D
W8F
WH7
WOQ
WOW
X7M
YHG
YKV
ZA5
ZGI
0R~
AALRI
AAYXX
ADVLN
AITUG
AKRWK
AMRAJ
CITATION
H13
ID FETCH-LOGICAL-c1602-8ce6c6f5a75c031a8def62e92adfbf48286846e59e0e61a1089007db286b3f203
ISSN 0006-4971
IngestDate Fri Nov 22 00:12:24 EST 2024
Fri Feb 23 02:44:06 EST 2024
IsDoiOpenAccess true
IsOpenAccess true
IsPeerReviewed true
IsScholarly true
Issue 11
Language English
License This article is made available under the Elsevier license.
LinkModel OpenURL
MergedId FETCHMERGED-LOGICAL-c1602-8ce6c6f5a75c031a8def62e92adfbf48286846e59e0e61a1089007db286b3f203
OpenAccessLink https://dx.doi.org/10.1182/blood.V106.11.1102.1102
PageCount 1
ParticipantIDs crossref_primary_10_1182_blood_V106_11_1102_1102
elsevier_sciencedirect_doi_10_1182_blood_V106_11_1102_1102
PublicationCentury 2000
PublicationDate 2005-11-16
PublicationDateYYYYMMDD 2005-11-16
PublicationDate_xml – month: 11
  year: 2005
  text: 2005-11-16
  day: 16
PublicationDecade 2000
PublicationTitle Blood
PublicationYear 2005
Publisher Elsevier Inc
Publisher_xml – name: Elsevier Inc
SSID ssj0014325
Score 1.8345437
Snippet Imatinib (Im), a rationally designed inhibitor of the Bcr/Abl kinase as well as other kinases, represents the standard treatment for Bcr/Abl+ malignancies. Im...
SourceID crossref
elsevier
SourceType Aggregation Database
Publisher
StartPage 1102
Title Phase I Study of Flavopiridol in Combination with Imatinib Mesylate (STI571, Gleevec) in Bcr/Abl+ Hematological Malignancies
URI https://dx.doi.org/10.1182/blood.V106.11.1102.1102
Volume 106
hasFullText 1
inHoldings 1
isFullTextHit
isPrint
link http://sdu.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwtV3db9MwELe6IWAvCDomNj7kB0Cgki5xvnlrS6cVqQOpBfEW2YkNldKmatmkSfzx3NlJmggQIMSLlVxlJ-39evfzx90R8lRwpThnmeVwmJt4Hk8tDkTDsoX0hMtdlek8Beez8OJT9GbsjTudqjLjTvZfNQ0y0DVGzv6FtutBQQDXoHNoQevQ_pHe338Bv9Sb6AOCevf8LOdXxXqxWWRFbmL8ljAbNnrXq7ATJK2rhehN5fY6B-6JrHM2n_iho1fNcymvZIrLB9B7mGK-kYHIn7Eh-CzoWlvPKVD6z6ba77a1V5yXBenLyGyT6cCUU6vtPd-sd0EivXG__qDQJdjfLTE4uZaOimJtsDbEM728tXbhYxCfCa00C2pVUE3rzCd6UCx8ZyAnS7uMibRtZrcMtx00Eeo07DCQGtbw6dXtj_4iwvyzOkag_xHGAwkGRrD-boBWMu6Z5nDwbk4c-nHMoj1yg4GJQws7e3tR7195LjO1M8qvUp4shMed_uJhP-dFDa4zv0vulJMUOjDoukc6ctUlhwMATbG8ps-pPjas92O65Oawuro9qooHdsmtaXlm45B804ikE6oRSQtFm4ikixVtIJIiImmFSFohkr4weHxFSzS-xH6AxVNAYo-2cEibOLxPPpyN56Nzq6z5YaVOgM45lUEaKJ-Hfgr-hkeZVAGTMeOZEsrDpAfAmKUfS1sGDnfsKAaWmwmQC1cx2z0i-6tiJR8QajtZ5Aee8IJUeDwUkbKRrmaprzLXVekxsatfPFmb1C6JnhJHLNFKSlBJcJ-gfnRzTF5XmklKhmqYZwKA-l3nk3_p_JAc7P5Aj8j-182lfEz2ttnlE428743rrjI
link.rule.ids 315,782,786,27933,27934
linkProvider Multiple Vendors
openUrl ctx_ver=Z39.88-2004&ctx_enc=info%3Aofi%2Fenc%3AUTF-8&rfr_id=info%3Asid%2Fsummon.serialssolutions.com&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Ajournal&rft.genre=article&rft.atitle=Phase+I+Study+of+Flavopiridol+in+Combination+with+Imatinib+Mesylate+%28STI571%2C+Gleevec%29+in+Bcr%2FAbl%2B+Hematological+Malignancies&rft.jtitle=Blood&rft.au=Grant%2C+Steven&rft.au=Karp%2C+Judith+E.&rft.au=Koc%2C+Omer+N.&rft.au=Cooper%2C+Brenda&rft.date=2005-11-16&rft.pub=Elsevier+Inc&rft.issn=0006-4971&rft.eissn=1528-0020&rft.volume=106&rft.issue=11&rft.spage=1102&rft.epage=1102&rft_id=info:doi/10.1182%2Fblood.V106.11.1102.1102&rft.externalDocID=S0006497119759928
thumbnail_l http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/lc.gif&issn=0006-4971&client=summon
thumbnail_m http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/mc.gif&issn=0006-4971&client=summon
thumbnail_s http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/sc.gif&issn=0006-4971&client=summon