Pretreatment Mitochondrial Priming Correlates with Clinical Response to Cytotoxic Chemotherapy

Chonghaile, Tríona Ní; Sarosiek, Kristopher A.; Vo, Thanh Trang T.; Ryan, Jeremy; Tammareddi, Anupama; Moore, Victoria Del Gaizo; Deng, Jing; Anderson, Kenneth C.; Richardson, Paul G.; Tai, Yu Tzu; Mitsiades, Constantine S.; Matulonis, Ursula A.; Drapkin, Ronny; Stone, Richard; DeAngelo, Daniel J.; McConkey, David J.; Sallan, Stephen E.; Silverman, Lewis B.; Hirsch, Michelle S.; Carrasco, Daniel R.; Letaï, Anthony

doi:10.1126/science.1206727

Cited by 499 publications

(554 citation statements)

References 35 publications

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“…[39][40][41][42] In particular, the present study utilizes full-length BH3-only proteins, which differ in the strengths of their protein-protein interactions compared with isolated BH3 peptides, 49 and places those BH3-only proteins in the context of cellular signaling networks 2,45 rather than isolated mitochondria. Thus, although BH3 profiling is being explored as a strategy to predict sensitivity or resistance of particular cell lines or cancers to specific treatments, 50 measurement of BH3-only tolerance has the potential to provide insight into endogenous signaling networks within intact cells that include BCL2 family members bound to surfaces other than the MOM.…”

Section: Discussionmentioning

confidence: 99%

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Measurement of BH3-only protein tolerance

et al. 2017

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The BCL2 family of proteins regulates cellular life and death decisions. Among BCL2 family members, BH3-only proteins have critical roles by neutralizing antiapoptotic family members, as well as directly activating BAX and BAK. Despite widespread occurrence of BH3-only protein upregulation in response to various stresses, this process is rarely quantified. Moreover, it is unclear whether all BH3-only proteins are equipotent at inducing cell death. Here we show that BH3-only proteins increase as much as 15-to 20-fold after various treatments and define a parameter, termed BH3-only tolerance, which measures how many copies of a particular BH3-only protein can be expressed before the majority of cells in a population undergo apoptosis. We not only assess the relative contributions of anti-and proapoptotic BCL2 family members to BH3-only tolerance, but also illustrate how the study of this parameter can be used to understand cellular sensitivity to anticancer drugs and new combinations. These observations provide a new quantitative framework for assessing apoptotic susceptibility under various conditions.

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Section: Discussionmentioning

confidence: 99%

“…41,42 This assay involves treating mitochondria or permeabilized cells with isolated BH3 peptides and measuring cytochrome c release or mitochondrial depolarization. In a recent modification termed 'dynamic BH3 profiling,' cells are exposed to potential anticancer drugs versus diluent and assayed for BIM BH3 peptideinduced mitochondrial depolarization.…”

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confidence: 99%

Measurement of BH3-only protein tolerance

et al. 2017

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“…Due to the above motivated similarity in apoptosis pathways between cancer cells and cardiomyocytes, any strategy that aims to protect cardiomyocytes while killing cancer cells would aim to exploit differences in apoptosis likelihood rather than invoking distinct apoptosis pathways [43][44][45]. To this end, the Deshmukh lab has shown that differentiated rat cardiomyocytes, similar to primary neurons, have down-regulated levels of the pro-apoptotic APAF-1 and increased expression of the anti-apoptotic XIAP compared to less differentiated cells.…”

Section: Are Differentiated Cardiomyocytes Less Likely To Succumb Tomentioning

confidence: 99%

“…In the context of cancer cells this mechanism was coined as apoptosis priming, aiming to explain why cancer cells are more susceptible to chemotherapy than normal cells. Specifically, proponents of the priming hypothesis such as the Letai group suggest that cancer cells increase their apoptosis likelihood in response to continuous somatic attack by the immune system [45,54], making them more likely than somatic cells to respond to cytotoxic chemotherapy. Indeed, we observe some parallelism between cancer cells primed by somatic apoptosis [45,55] and cardiomyocyte being exposed to (sub-lethal) DOX with respect to metabolic programming and apoptosis sensitization ( Figure 2).…”

Section: Does Dox Exposure Change Apoptosis Likelihood To Later Somatmentioning

confidence: 99%

“…In addition, as cancer cells are continuously attacked by the immune system, the constant somatic stress makes them more sensitized to undergo chemotherapy-induced apoptosis. This sensitization was coined as apoptosis priming [45,55] and was recently explained by us through systematic change in balance in favor of pro-apoptotic proteins using a systems analysis [54]. MOMP apoptosis, APOPTO-CELL.…”

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Doxorubicin-induced chronic dilated cardiomyopathy—the apoptosis hypothesis revisited

Kankeu

Clarke²,

Passante

et al. 2016

J Mol Med

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The chemotherapeutic Doxorubicin (DOX) has significantly increased survival rates of pediatric and adult cancer patients. However, 10 % of pediatric cancer survivors will 10-20 years later develop severe Dilated Cardiomyopathy (DCM) and the exact molecular mechanisms of disease progression after this long latency time remain puzzling. We here revisit the hypothesis that elevated apoptosis signaling or its increased likelihood after DOX exposure can lead to an impairment of cardiac function and cause a cardiac dilation. Based on recent literature evidences, we first argue why even little detectable apoptosis may be sufficient to cause a dilated phenotype. We then review findings suggesting that mature cardiomyocytes are protected against DOX-induced apoptosis downstream, but not upstream to Mitochondrial Outer Membrane Permeabilisation (MOMP). This lack of prevention of MOMP-induction then is proposed to alter the metabolic phenotype, induce hypertrophic remodeling and lead to functional cardiac impairment even in absence of cardiomyocyte apoptosis. We further discuss findings that DOX exposure can lead to increased sensitivity to further cardiomyocyte apoptosis, which may cause a gradual loss in cardiomyocytes over time and a compensatory hypertrophic remodeling after treatment, potentially explaining the long lag time in disease onset. We finally note similarities between DOX-exposed cardiomyocytes and apoptosisprimed cancer cells and propose computational systems biology as tool to predict patient individual DOX doses. In conclusion, combining recent findings in rodent hearts and cardiomyocytes exposed to DOX with insights from apoptosis signal transduction allowed us to obtain a molecularly deeper insight in this delayed and still enigmatic pathology of DCM. Key messages1. Differentiated cardiomyocyte are protected to post but not pre-MOMP apoptosis 2. MOMP-induction can lead to cardiac hypertrophy and metabolic remodeling after DOX 3. DOX-exposed cardiomyocytes may be more sensitive to apoptosis over life time 4. DOX-exposed cardiomyocytes show similarities to apoptosis-primed cancer cells

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Heat-shock protein 27 (HSP27, HSPB1) is synthetic lethal to cells with oncogenic activation of MET, EGFR and BRAF

et al. 2017

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The small heat‐shock protein of 27 kDa (HSP27) is highly expressed in many cancers and is associated with aggressive tumour behaviour, metastasis, poor prognosis and resistance to chemotherapy. We aimed at assessing the role of HSP27 in modulating responses to target therapies. We selected several oncogene‐addicted cancer cell lines, which undergo either cell cycle blockade or cell death in response to agents that target the specific oncogene. Surprisingly, HSP27 suppression alone resulted in the apoptotic death of MET‐addicted EBC‐1 lung cancer cells, epidermal growth factor receptor (EGFR)‐addicted colorectal carcinoma (CRC) DiFi cells and BRAF‐addicted CRC COLO205 and OXCO‐1 and melanoma COLO741 cells, all of which also undergo death when treated with the specific targeted agent. In other cell lines, such as MET‐addicted gastric carcinoma MKN45 and EGFR‐addicted CRC SW48 lines, where oncogene inhibition only blocked proliferation, HSP27 knockdown made targeted agents switch from cytostatic to cytotoxic activity. Mechanistically, the more the cells were susceptible to HSP27 suppression, the more they were primed for death, as demonstrated by increased levels of mitochondrial outer membrane permeabilization. Priming for death was accompanied by the increase in pro‐apoptotic proteins of the BCL2 family and of active caspase‐3 and lamin B. Together, these data suggest that oncogene‐addicted cells require HSP27 for survival and that HSP27 might interfere with the effectiveness of targeted agents.

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Pretreatment Mitochondrial Priming Correlates with Clinical Response to Cytotoxic Chemotherapy

Cited by 499 publications

References 35 publications

Measurement of BH3-only protein tolerance

Measurement of BH3-only protein tolerance

Doxorubicin-induced chronic dilated cardiomyopathy—the apoptosis hypothesis revisited

Heat-shock protein 27 (HSP27, HSPB1) is synthetic lethal to cells with oncogenic activation of MET, EGFR and BRAF

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