The BCL-2 protein family, BH3-mimetics and cancer therapy

Delbridge, Alex R. D.; Strasser, Andreas

doi:10.1038/cdd.2015.50

Cited by 413 publications

(331 citation statements)

References 167 publications

(188 reference statements)

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“…The latter, is an interesting observation that can be explained as an unsuccessful attempt of cells after the removal of carboranes form the culture to overcome the agent-triggered cell-cycle arrest mediated by p53/p21. Importantly enough, through these opposing molecular pathways impinging on to either proliferation and survival, or growth arrest and apoptosis [45][46][47], the treatment of glioblastoma U87 MG cultures with carboranes leads to a such functional balance in gene expression that permanently leads them to inability for cell cycling and division. Overall, these bifunctional acting Upper panels: The EGFR neg primary GBM CSCs, which grow in culture as monolayers, were treated at specified concentrations of BOR2, BOR3 and BOR4 for 48 h. Cell proliferation was assessed by the MTT assay, as described under A significance level of p < 0.05 denoted significance.…”

Section: Discussionmentioning

confidence: 99%

Pharmacological Development of Target-Specific Delocalized Lipophilic Cation-Functionalized Carboranes for Cancer Therapy

et al. 2016

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PURPOSE: Tumor cell heterogeneity and microenvironment represent major hindering factors in the clinical setting toward achieving the desired selectivity and specificity to malignant tissues for molecularly targeted cancer therapeutics. In this study, the cellular and molecular evaluation of several delocalized lipophilic cation (DLC)-functionalized carborane compounds as innovative anticancer agents is presented. METHODS:The anticancer potential assessment of the DLC-carboranes was performed in established normal (MRC-5, Vero), cancer (U-87 MG, HSC-3) and primary glioblastoma cancer stem (EGFR pos , EGFR neg ) cultures. Moreover, the molecular mechanism of action underlying their pharmacological response is also analyzed. RESULTS:The pharmacological anticancer profile of DLC-functionalized carboranes is characterized by: a) a marked in vitro selectivity, due to lower concentration range needed (ca. 10 fold) to exert their cell growth-arrest effect on U-87 MG and HSC-3, as compared with that on MRC-5, Vero; b) a similar selective growth inhibition behavior towards EGFR pos and EGFR neg cultures (>10 fold difference in potency) without, however, the activation of apoptosis in cultures; c) notably, in marked contrast to cancer cells, normal cells are capable of recapitulating their full proliferation potential following exposure to DLC-carboranes; and, d) such pharmacological effects of DLC-carboranes has been unveiled to be elicited at the molecular level through activation of the p53/p21 axis. CONCLUSIONS:Overall, the data presented in this work indicates the potential of the DLC-functionalized carboranes to act as new selective anticancer therapeutics that 3 may be used autonomously or in therapies involving radiation with thermal neutrons.Importantly, such bifunctional capacity may be beneficial in cancer therapy.

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Section: Discussionmentioning

confidence: 99%

Pharmacological Development of Target-Specific Delocalized Lipophilic Cation-Functionalized Carboranes for Cancer Therapy

et al. 2016

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“…Notable in this regard is the Bcl-2 protein family. Proapoptotic Bcl-2-related proteins Bax and Bak initiate cytochrome C release from mitochondria in response to diverse apoptotic stimuli, whereas antiapoptotic Bcl-2-related proteins, including Bcl-2 and Bcl-x L , antagonize Bax/Bak by forming heterodimers that prevent their oligomerization and apoptosis initiation (22,23). Heterodimerization is mediated by interactions of proapoptotic Bcl-2 homology 3 (BH3) domains with a hydrophobic groove on the surface of antiapoptotic Bcl-2 proteins (23) that is a therapeutic target in diseases, including cancer (22).…”

mentioning

confidence: 99%

“…Proapoptotic Bcl-2-related proteins Bax and Bak initiate cytochrome C release from mitochondria in response to diverse apoptotic stimuli, whereas antiapoptotic Bcl-2-related proteins, including Bcl-2 and Bcl-x L , antagonize Bax/Bak by forming heterodimers that prevent their oligomerization and apoptosis initiation (22,23). Heterodimerization is mediated by interactions of proapoptotic Bcl-2 homology 3 (BH3) domains with a hydrophobic groove on the surface of antiapoptotic Bcl-2 proteins (23) that is a therapeutic target in diseases, including cancer (22). Whereas a central feature of molecular models of apoptosis is the control of outer mitochondrial membrane permeability by Bcl-2-related proteins, a substantial body of evidence has demonstrated that these proteins localize to the ER (24,25), bind to InsP 3 Rs (26)(27)(28)(29)(30)(31)(32) and, by modulating InsP 3 R-mediated Ca 2+ release, regulate ERmediated cell death and survival (15,27,(32)(33)(34).…”

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confidence: 99%

Biphasic regulation of InsP ₃ receptor gating by dual Ca ²⁺ release channel BH3-like domains mediates Bcl-x _L control of cell viability

Yang

Vais

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Antiapoptotic Bcl-2 family members interact with inositol trisphosphate receptor (InsP 3 R) Ca 2+ release channels in the endoplasmic reticulum to modulate Ca 2+ signals that affect cell viability. However, the molecular details and consequences of their interactions are unclear. Here, we found that Bcl-x L activates single InsP 3 R channels with a biphasic concentration dependence. The Bcl-x L Bcl-2 homology 3 (BH3) domain-binding pocket mediates both high-affinity channel activation and low-affinity inhibition. Bcl-x L activates channel gating by binding to two BH3 domain-like helices in the channel carboxyl terminus, whereas inhibition requires binding to one of them and to a previously identified Bcl-2 interaction site in the channelcoupling domain. Disruption of these interactions diminishes cell viability and sensitizes cells to apoptotic stimuli. Our results identify BH3-like domains in an ion channel and they provide a unifying model of the effects of antiapoptotic Bcl-2 proteins on the InsP 3 R that play critical roles in Ca 2+ signaling and cell viability.T he inositol trisphosphate receptors (InsP 3 R) are a family of intracellular cation channels that release Ca 2+ from the endoplasmic reticulum (ER) in response to a variety of extracellular stimuli (1). Three InsP 3 R isoforms are ubiquitously expressed and regulate diverse cell processes, including cell viability (1). Activation of the channels by InsP 3 elicits changes in cytoplasmic Ca 2+ concentration ([Ca 2+ ] i ) that provide versatile signals to regulate molecular processes with high spatial and temporal fidelity (1). Regions of close proximity to mitochondria enable localized Ca 2+ release events to be transduced to mitochondria (2, 3). Ca 2+ released from the ER during cell stimulation modulates activities of effector molecules and is taken up by mitochondria to stimulate oxidative phosphorylation and enhance ATP production (4-6) to match energetic supply with enhanced demand. In addition, cells in vivo are constantly exposed to low levels of circulating hormones, transmitters, and growth factors that bind to plasma membrane receptors to provide a background level of cytoplasmic InsP 3 (7) that generates low-level stochastic InsP 3 R-mediated localized or propagating [Ca 2+ ] i signals (8-10). Such signals also play an important role in maintenance of cellular bioenergetics (8). Nevertheless, under conditions of cell stress the close proximity of mitochondria to Ca 2+ release sites may result in mitochondrial Ca 2+ overload and initiate Ca 2+ -dependent forms of cell death, including necrosis and apoptosis (11-13). It has been suggested that high levels of ER Ca 2+ (14-16) and enhanced activity of the InsP 3 R (17-19) promote cell death by providing a higher quantity of released Ca 2+ to mitochondria (3,20,21).Protein interactions modulate the magnitude and quality of InsP 3 R-mediated [Ca 2+ ] i signals that regulate apoptosis and cell viability. Notable in this regard is the Bcl-2 protein family. Proapoptotic Bcl-2-related proteins Bax ...

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“…The use of chemotherapy for the clinical management of lung cancer causes notable side effects (18,19); therefore, new effective drugs to treat lung cancer are required. Previous studies have shown that polyoxometalates exert their antitumor properties by regulating cell invasion, proliferation and migration in a variety of malignancies such as breast, kidney, lung, ovary, pancreas and prostate cancer (17).…”

Section: Discussionmentioning

confidence: 99%

K9(C4H4FN2O2)2Nd(PW11O39)2·25H2O induces apoptosis in human lung cancer A549 cells

et al. 2016

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Abstract. Lung cancer is the leading cause of cancer-associated mortality worldwide. The present study investigated the effects of K 9 (C 4 H 4 FN 2 O 2 ) 2 Nd(PW 11 O 39 ) 2 ·25H 2 O (FNdPW), a chemically synthesized polyoxometalate that contains rare earth elements, on lung cancer growth, and explored the mechanism underlying its actions. The effects of FNdPW on the cell viability and apoptosis of human lung cancer A549 cells were measured using MTT assay, acridine orange/ethidium bromide staining and electron microscopy. The expression of apoptosis-related proteins, including B-cell lymphoma (Bcl)-2-associated death promoter (Bad), phosphorylated (p)-Bad, X-linked inhibitor of apoptosis (XIAP), apoptosis-inducing factor (AIF), Bcl-2-associated X protein (Bax) and Bcl-2, was determined by western blotting. Caspase-3 activity was measured using a caspase-3 activity kit. After 72 h of incubation, FNdPW reduced cell viability and induced apoptosis in A549 cells in a concentration-and time-dependent manner. FNdPW upregulated the pro-apoptotic Bad and Bax proteins, and downregulated the anti-apoptotic p-Bad, Bcl-2 and XIAP proteins. Furthermore, FNdPW also enhanced caspase-3 activity and increased the protein level of AIF in A549 cells, which was independent of the caspase-3 pathway. These events were associated with the regulation exerted by FNdPW on multiple targets involved in A549 cell proliferation. Therefore, FNdPW may be a novel drug for the treatment of lung cancer.

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The BCL-2 protein family, BH3-mimetics and cancer therapy

Cited by 413 publications

References 167 publications

Pharmacological Development of Target-Specific Delocalized Lipophilic Cation-Functionalized Carboranes for Cancer Therapy

Pharmacological Development of Target-Specific Delocalized Lipophilic Cation-Functionalized Carboranes for Cancer Therapy

Biphasic regulation of InsP ₃ receptor gating by dual Ca ²⁺ release channel BH3-like domains mediates Bcl-x _L control of cell viability

K9(C4H4FN2O2)2Nd(PW11O39)2·25H2O induces apoptosis in human lung cancer A549 cells

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The BCL-2 protein family, BH3-mimetics and cancer therapy

Cited by 413 publications

References 167 publications

Pharmacological Development of Target-Specific Delocalized Lipophilic Cation-Functionalized Carboranes for Cancer Therapy

Pharmacological Development of Target-Specific Delocalized Lipophilic Cation-Functionalized Carboranes for Cancer Therapy

Biphasic regulation of InsP 3 receptor gating by dual Ca 2+ release channel BH3-like domains mediates Bcl-x L control of cell viability

K9(C4H4FN2O2)2Nd(PW11O39)2·25H2O induces apoptosis in human lung cancer A549 cells

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Biphasic regulation of InsP ₃ receptor gating by dual Ca ²⁺ release channel BH3-like domains mediates Bcl-x _L control of cell viability