Inhibition of <i>NANOG/NANOGP8</i> Downregulates MCL-1 in Colorectal Cancer Cells and Enhances the Therapeutic Efficacy of BH3 Mimetics

Mattoo, Abid R.; Zhang, Jingyu; Espinoza, Luis; Jessup, J. Milburn

doi:10.1158/1078-0432.ccr-14-1134

Cited by 30 publications

(29 citation statements)

References 39 publications

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“…Inhibition of MCL-1 sensitizes cancer cells to chemotherapeutic drugs and IR (12,(14)(15)(16). Consistent with the current literature, we found that MCL-1 depletion ( Fig.…”

Section: Resultssupporting

confidence: 92%

MCL-1 Depletion Impairs DNA Double-Strand Break Repair and Reinitiation of Stalled DNA Replication Forks

Mattoo

Pandita

Chakraborty

et al. 2017

Molecular and Cellular Biology

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Myeloid cell leukemia 1 (MCL-1) is a prosurvival BCL-2 protein family member highly expressed in hematopoietic stem cells (HSCs) and regulated by growth factor signals that manifest antiapoptotic activity. Here we report that depletion of MCL-1 but not its isoform MCL-1S increases genomic instability and cell sensitivity to ionizing radiation (IR)-induced death. MCL-1 association with genomic DNA increased postirradiation, and the protein colocalized with 53BP1 foci. Postirradiation, MCL-1-depleted cells exhibited decreased ␥-H2AX foci, decreased phosphorylation of ATR, and higher levels of residual 53BP1 and RIF1 foci, suggesting that DNA double-strand break (DSB) repair by homologous recombination (HR) was compromised. Consistent with this model, MCL-1-depleted cells had a reduced frequency of IRinduced BRCA1, RPA, and Rad51 focus formation, decreased DNA end resection, and decreased HR repair in the DR-GFP DSB repair model. Similarly, after HU induction of stalled replication forks in MCL-1-depleted cells, there was a decreased ability to subsequently restart DNA synthesis, which is normally dependent upon HRmediated resolution of collapsed forks. Therefore, the present data support a model whereby MCL-1 depletion increases 53BP1 and RIF1 colocalization at DSBs, which inhibits BRCA1 recruitment, and sensitizes cells to DSBs from IR or stalled replication forks that require HR for repair.KEYWORDS MCL-1, BCL-2, HR, ICL, apoptosis, 53BP1, DSB repair M CL-1 is a member of the prosurvival BCL-2 family and plays an important role in the regulation of the intrinsic or mitochondrial apoptotic pathway by inhibiting both BH3-only proteins and the proapoptotic proteins (1-3). MCL-1 is mainly located at the outer mitochondrial membrane and inhibits the progression of apoptosis by sequestering executioner proapoptotic proteins BAK and BAX, which are capable of inducing pore formation in the mitochondrial membrane. The subsequent release of cytochrome c into the cytoplasm activates caspases which are responsible for the majority of the macromolecular degradation observed during apoptosis (3). Suppression of BAK and BAX polymerization by MCL-1 is prevented either by MCL-1 degradation or by saturating and inhibiting the MCL-1 binding sites on BAK/BAX with BH3 proteins or mimetics.Under normal growth conditions, MCL-1 is important for mouse embryonic survival (4) and critical for the survival of neutrophils, lymphocytes, hematopoietic stem cells, and neurons (5). MCL-1 overexpression is the hallmark of several cancers, including hematological malignancies as well as solid tumors. Elevated cellular MCL-1 expression correlates with resistance to drug toxicity and ionizing radiation (IR), whereas its inhibition sensitizes cells to both. The BCL-2 family of proteins is characterized by the presence of BCL-2 homology (BH) domains (1, 2). The MCL-1 protein itself is unique among BCL-2 members in also containing multiple N-terminal PEST motifs in addition to BH1, BH2, BH3, and C-terminal transmembrane (TM) domains. PEST is ...

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“…Inhibition of MCL-1 sensitizes cancer cells to chemotherapeutic drugs and IR (12,(14)(15)(16). Consistent with the current literature, we found that MCL-1 depletion ( Fig.…”

Section: Resultssupporting

confidence: 92%

MCL-1 Depletion Impairs DNA Double-Strand Break Repair and Reinitiation of Stalled DNA Replication Forks

Mattoo

Pandita

Chakraborty

et al. 2017

Molecular and Cellular Biology

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“…High level of c-FLIP may protect cancer cells from the apoptotic signaling exists in circumstance. Therefore, reducing the expression of c-FLIP in tumor cells is able to improve the sensitivity of them to drugs [29,30]. In this study, we demonstrated that overexpression of c-FLIP in HCC can be abolished by miR-382 introduction.…”

Section: Mir-382-overexpressed Hcc Model Is Sensitive To γδ T Cells Tmentioning

confidence: 57%

WITHDRAWN: Overexpression of miR-382 sensitizes hepatocellular carcinoma cells to γδ T cells through inhibiting the expression of c-FLIP

Hou¹,

Chen²,

Zheng³

et al. 2018

Oncotarget

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“…Interestingly, although Mcl-1 had previously been shown to confer resistance to ABT-737 and ABT-199 in other hematological malignancies and solid tumors, 10,[18][19][20]43,44 its role in mediating resistance in CLL had remained somewhat controversial. For example, in the study of Vogler et al, 15 induction of Mcl-1 expression by stimulation with interleukin-4 or interferon-g was associated with only marginal protection, prompting the authors to conclude that resistance to ABT-737 in CLL is largely Mcl-1 independent.…”

Section: Discussionmentioning

confidence: 99%

“…17 Previous studies by our group have shown that sustained engagement of the BCR induces Mcl-1, 6 and high levels of Mcl-1 were shown to inversely correlate with treatment response in the phase 1 study of ABT-263 in CLL. 12 In addition, high levels of Mcl-1 have been shown to protect other hematological malignancies and certain solid tumors from ABT-199, [18][19][20] suggesting that Mcl-1 could also confer ABT-199 resistance to CLL cells. To further explore this possibility, we evaluated whether BCR-induced Mcl-1 overexpression can protect CLL cells from ABT-199 and whether this protection can be overcome by available BCR signaling inhibitors.…”

mentioning

confidence: 99%

BCR signaling inhibitors differ in their ability to overcome Mcl-1–mediated resistance of CLL B cells to ABT-199

Bojarczuk

Sasi

Gobessi

et al. 2016

Blood

102

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Key Points• BCR signals induce resistance in CLL cells by upregulating Mcl-1.• SYK inhibitors prevent BCRmediated Mcl-1 induction more effectively than BTK or PI3Kd inhibitors.The Bcl-2 antagonist has demonstrated promising clinical activity in patients with chronic lymphocytic leukemia (CLL). ABT-199 is strongly cytotoxic against unstimulated peripheral blood CLL cells in vitro but is much less effective against CLL cells that have received survival signals from the microenvironment. In particular, stimulation of CLL cells with CD40L results in substantial resistance mediated by induction of the antiapoptotic Bcl-2 family proteins Bcl-xL and Bfl-1. In this study, we investigated whether resistance to ABT-199 can be conferred by B-cell receptor (BCR) stimulation, which is another important survival signal from the leukemic microenvironment. We show that sustained BCR stimulation results in significant ABT-199 resistance, which correlates with induction of the antiapoptotic protein Mcl-1 and less consistently with downregulation of proapoptotic Bmf, Hrk, and Bim EL . A major role for Mcl-1 in conferring ABT-199 resistance is additionally supported by knockdown and enforced expression experiments with primary CLL cells. We further show that SYK, BTK, and phosphatidylinositol 3-kinase d (PI3Kd) inhibitors significantly downregulate Mcl-1, but with different efficacy. Complete Mcl-1 downregulation was consistently achieved only with SYK inhibitors R406 and GS-9973 (entospletinib), whereas the BTK inhibitor ibrutinib and the PI3Kd inhibitor idelalisib in more than half of the cases had only a partial effect. The greater ability of SYK inhibitors to downregulate Mcl-1 correlated with their greater capacity to block BCR-mediated inactivation of GSK-3, a major negative regulator of Mcl-1. The finding that BCR signaling inhibitors differ in their ability to target Mcl-1 is relevant for the design of clinical trials combining these agents with ABT-199. (Blood. 2016;127(25):3192-3201)

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Inhibition of NANOG/NANOGP8 Downregulates MCL-1 in Colorectal Cancer Cells and Enhances the Therapeutic Efficacy of BH3 Mimetics

Cited by 30 publications

References 39 publications

MCL-1 Depletion Impairs DNA Double-Strand Break Repair and Reinitiation of Stalled DNA Replication Forks

MCL-1 Depletion Impairs DNA Double-Strand Break Repair and Reinitiation of Stalled DNA Replication Forks

WITHDRAWN: Overexpression of miR-382 sensitizes hepatocellular carcinoma cells to γδ T cells through inhibiting the expression of c-FLIP

BCR signaling inhibitors differ in their ability to overcome Mcl-1–mediated resistance of CLL B cells to ABT-199

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