A Small Molecule that Induces Intrinsic Pathway Apoptosis with Unparalleled Speed

Palchaudhuri, Rahul; Lambrecht, Michael J.; Botham, Rachel C.; Partlow, Kathryn C.; Ham, Tjakko J. van; Putt, Karson S.; Nguyen, Laurie T.; Kim, Seok Ho; Peterson, Randall T.; Fan, Timothy M.; Hergenrother, Paul J.

doi:10.1016/j.celrep.2015.10.042

Cited by 78 publications

(75 citation statements)

References 45 publications

(58 reference statements)

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“…Cells were treated with 1 µM of staurosporine for 24 h or with 13 µM of raptinal(37) for 3 h as positive control, DMSO as negative control and indicated concentrations of PAC-1 and vemurafenib for 0, 2, 4, 7, 10, 12, 16, 20 or 24 h. Plates were then assessed for caspase-3/7 activity via addition of bifunctional lysis and activity buffer (200 mM HEPES, 400 mM NaCl, 40 mM DTT, 0.4 mM EDTA, 1% Triton-X, pH 7.4) with 20 µM of Ac-DEVD-AFC (Cayman Chemicals) as the fluorogenic substrate (λ ex =400 nm, λ em =505 nm). Plates were pre-incubated at 37 °C at 30 min in the Synergy multi-mode reader (BioTek) then read for 30 min at 3 min intervals.…”

Section: Methodsmentioning

confidence: 99%

The Combination of Vemurafenib and Procaspase-3 Activation Is Synergistic in Mutant BRAF Melanomas

Peh

Fan

Wycislo

et al. 2016

Molecular Cancer Therapeutics

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The development of vemurafenib resistance limits the long-term efficacy of this drug for treatment of metastatic melanomas with the V600EBRAF mutation. Inhibition of downstream MAPK signaling with vemurafenib induces apoptotic cell death mediated by caspase-3, suggesting that addition of a procaspase-3 activator could enhance anticancer effects. Here we show that the combination of PAC-1, a procaspase-activating compound, and vemurafenib is highly synergistic in enhancing caspase-3 activity and apoptotic cell death in melanoma cell lines harboring the V600EBRAF mutation. In vivo, the combination displays a favorable safety profile in mice, and exerts significant antitumor effects. We further demonstrate that addition of PAC-1 to the clinically useful combination of vemurafenib and a MEK inhibitor, trametinib, starkly enhances the caspase-3 activity and proapoptotic effect of the combination. Moreover, addition of low concentration PAC-1 also delays the regrowth of cells following treatment with vemurafenib. Finally, PAC-1 remains potent against vemurafenib-resistant A375VR cells in cell culture and synergizes with vemurafenib to exert antitumor effects on A375VR cell growth in vivo. Collectively, our data suggest that inhibition of MAPK signaling combined with concurrent procaspase-3 activation is an effective strategy to enhance the antitumor activity of vemurafenib and mitigate the development of resistance.

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Section: Methodsmentioning

confidence: 99%

The Combination of Vemurafenib and Procaspase-3 Activation Is Synergistic in Mutant BRAF Melanomas

Peh

Fan

Wycislo

et al. 2016

Molecular Cancer Therapeutics

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“…For reasons that remain poorly understood, cell death kinetics vary considerably between lethal stimuli, cell lines and cell death pathways, as well as between individual cells within the same population (Bernheim et al, 1977; Biton and Ashkenazi, 2011; Dixon et al, 2012; Lu et al, 2014; Shimizu et al, 2004; Spencer et al, 2009; Vanden Berghe et al, 2010). A major goal of the present work was to develop means to quantify this variability in cell death kinetics at the population level, as this knowledge may enhance our understanding of different lethal pathways, improve the classification of lethal perturbations and help identify new drugs that act through unique mechanisms (Grootjans et al, 2016; Hafner et al, 2016; Harris et al, 2016; Palchaudhuri et al, 2015; Tyson et al, 2012). …”

Section: Introductionmentioning

confidence: 99%

Systematic Quantification of Population Cell Death Kinetics in Mammalian Cells

et al. 2017

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Summary Cytotoxic compounds are important drugs and research tools. Here, we introduce a method, Scalable Time-lapse Analysis of Cell death Kinetics (STACK), to quantify the kinetics of compound-induced cell death in mammalian cells at the population level. STACK uses live and dead cell markers, high-throughput time-lapse imaging, and mathematical modeling to determine the kinetics of population cell death over time. We used STACK to profile the effects of 1,819 bioactive compounds on cell death in two human cancer cell lines, resulting in a large and freely dataset [doi:10.17632/3pnv5wh5jm.2]. 79 potent lethal compounds common to both cell lines caused cell death with widely divergent kinetics. Thirteen compounds triggered cell death within hours, including the metallophore zinc pyrithione (ZP). Mechanistic studies demonstrated that this rapid onset lethal phenotype was caused in human cancer cells by metabolic disruption and ATP depletion. These results provide the first comprehensive survey of cell death kinetics and analysis of rapid onset lethal compounds.

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“…A landmark research by Paul Hergenrother and his team (Nature Clinical Biology) nearly found a way around this natural biological process that kick starts apoptosis [7]. They found a synthetic molecule that directly activates procaspase-3 to caspase-3 thus initiating apoptosis in the tumour.…”

Section: Can a Cancer Cell Be Tricked Into Dying By Using The Mechnismentioning

confidence: 99%

“…So it was postulated that therapy could be tailored to the cancer, the organ and patient's condition by measuring the levels of pro-caspase-3. This selective treatment was expected to minimize collateral damage and toxic effects of chemotherapy [5][6][7].…”

Section: Can a Cancer Cell Be Tricked Into Dying By Using The Mechnismentioning

confidence: 99%

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Tricking a Cancer Cell into Committing Suicide or Apoptosis

Chintamani

2017

Indian J Surg

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A Small Molecule that Induces Intrinsic Pathway Apoptosis with Unparalleled Speed

Cited by 78 publications

References 45 publications

The Combination of Vemurafenib and Procaspase-3 Activation Is Synergistic in Mutant BRAF Melanomas

The Combination of Vemurafenib and Procaspase-3 Activation Is Synergistic in Mutant BRAF Melanomas

Systematic Quantification of Population Cell Death Kinetics in Mammalian Cells

Tricking a Cancer Cell into Committing Suicide or Apoptosis

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