ABT-199, a potent and selective BCL-2 inhibitor, achieves antitumor activity while sparing platelets

被引:3
|
作者
Andrew J Souers
Joel D Leverson
Erwin R Boghaert
Scott L Ackler
Nathaniel D Catron
Jun Chen
Brian D Dayton
Hong Ding
Sari H Enschede
Wayne J Fairbrother
David C S Huang
Sarah G Hymowitz
Sha Jin
Seong Lin Khaw
Peter J Kovar
Lloyd T Lam
Jackie Lee
Heather L Maecker
Kennan C Marsh
Kylie D Mason
Michael J Mitten
Paul M Nimmer
Anatol Oleksijew
Chang H Park
Cheol-Min Park
Darren C Phillips
Andrew W Roberts
Deepak Sampath
John F Seymour
Morey L Smith
Gerard M Sullivan
Stephen K Tahir
Chris Tse
Michael D Wendt
Yu Xiao
John C Xue
Haichao Zhang
Rod A Humerickhouse
Saul H Rosenberg
Steven W Elmore
机构
[1] AbbVie Inc.,Department of Clinical Hematology and Bone Marrow Transplantation
[2] Genentech,Department of Hematology
[3] Inc.,undefined
[4] The Walter and Eliza Hall Institute of Medical Research,undefined
[5] Faculty of Medicine,undefined
[6] Dentistry and Health Sciences,undefined
[7] University of Melbourne,undefined
[8] Melbourne,undefined
[9] Victoria,undefined
[10] Australia.,undefined
[11] Royal Melbourne Hospital,undefined
[12] Peter MacCallum Cancer Centre,undefined
[13] Present address: Division of Chemistry and Biological Chemistry,undefined
[14] School of Physical and Mathematical Sciences,undefined
[15] Nanyang Technological University,undefined
[16] Singapore.,undefined
来源
Nature Medicine | 2013年 / 19卷
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摘要
Inhibition of prosurvival proteins of the BCL family is a promising anticancer strategy; however, the similarities between the family members make the development of specific agents difficult. Current compounds have been designed to target BCL-2, which is frequently elevated in tumors and is an important prosurvival factor, but also inhibit BCL-XL, which is required for the survival of platelets; thus, thrombocytopenia is a limiting toxic effect in patients. The authors have engineered anti-BCL drugs to generate a more BCL-2–specific compound that has less affinity for BCL-XL and, therefore, reduced platelet toxicity. The compound is effective in several tumor models in vivo and had reduced toxicity in three patients with refractory leukemia, showing a promising activity and safety profile to refine and improve proapoptotic therapy in cancer.
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页码:202 / 208
页数:6
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