| Literature DB >> 27465916 |
Jia-Nan Gong1,2, Tiffany Khong3, David Segal1,2, Yuan Yao1,2,4, Chris D Riffkin1, Jean-Marc Garnier1,2, Seong Lin Khaw1,2,5, Guillaume Lessene1,2,6, Andrew Spencer3, Marco J Herold1,2, Andrew W Roberts1,2,7,8, David C S Huang1,2.
Abstract
New therapeutic targets are needed to address the poor prognosis of patients with high-risk multiple myeloma. Myeloma cells usually express a range of the prosurvival BCL2 proteins. To define the hierarchy of their relative importance for maintaining the survival of myeloma cells, we targeted each of them in a large panel of cell lines, using pharmacological inhibitors or gene editing or by peptide-based approaches, alone or in combination. The majority of well-established immortalized cell lines (17/25) or low-passage myeloma cell lines (5/7) are readily killed when MCL1 is targeted, even including those cell lines sensitive to BCL2 inhibition. Targeting MCL1 also constrained the growth of myeloma in vivo. We also identified a previously unrecognized subset of myeloma that is highly BCLXL-dependent, and has the potential for cotargeting MCL1 and BCLXL. As MCL1 is pivotal for maintaining survival of most myelomas, it should be prioritized for targeting in the clinic once high-quality, validated inhibitors become available.Entities:
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Year: 2016 PMID: 27465916 DOI: 10.1182/blood-2016-03-704908
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113