Histone deacetylase inhibitors restore toxic BH3 domain protein expression in anoikis-resistant mammary and brain cancer stem cells,thereby enhancing the response to anti-ERBB1/ERBB2 therapy |
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| Authors: | Nichola Cruickshanks Hossein A Hamed Laurence Booth Seyedmehrad Tavallai Jahangir Syed Gangadharan B Sajithlal Steven Grant Andrew Poklepovic Paul Dent |
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| Institution: | 1.Department of Neurosurgery; Virginia Commonwealth University; Richmond, VA USA;2.Department of Medicine; Virginia Commonwealth University; Richmond, VA USA |
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| Abstract: | The present studies focused on defining the mechanisms by which anoikis-resistant (AR) mammary carcinoma cells can be reverted to a therapy-sensitive phenotype. AR mammary carcinoma cells had reduced expression of the toxic BH3 domain proteins BAX, BAK, NOXA, and PUMA. In AR cells expression of the protective BCL-2 family proteins BCL-XL and MCL-1 was increased. AR cells were resistant to cell killing by multiple anti-tumor cell therapies, including ERBB1/2 inhibitor + MCL-1 inhibitor treatment, and had a reduced autophagic flux response to these therapies, despite similarly exhibiting increased levels of LC3II processing. Knockdown of MCL-1 and BCL-XL caused necro-apoptosis in AR cells to a greater extent than in parental cells. Pre-treatment of anoikis-resistant cells with histone deacetylase inhibitors (HDACIs) for 24 h increased the levels of toxic BH3 domain proteins, reduced MCL-1 levels, and restored/re-sensitized the cell death response of AR tumor cells to multiple toxic therapies. In vivo, pre-treatment of AR breast tumors in the brain with valproate restored the chemo-sensitivity of the tumors and prolonged animal survival. These data argue that one mechanism to enhance the anti-tumor effect of chemotherapy could be HDACI pre-treatment. |
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| Keywords: | autophagy anoikis BH3 domain MCL-1 ERBB1 tumor signaling necrosis BAK NOXA |
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