Autophagy Inhibition for Chemosensitization and Radiosensitization in Cancer: Do the Preclinical Data Support This Therapeutic Strategy?

Bristol, Molly L.; Emery, Sean M.; Maycotte, Paola; Thorburn, Andrew; Chakradeo, Shweta; Gewirtz, David A.

doi:10.1124/jpet.112.199802

Cited by 88 publications

(73 citation statements)

References 48 publications

(118 reference statements)

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“…Because autophagy inhibition results in the up-regulation of p62 proteins that are normally degraded by autophagy (41), our data provide a mechanism by which autophagy inhibitors, including chloroquine (11,16,(42)(43)(44) or bortezomib, can sensitize cancer cells to chemotherapy-induced apoptosis. In addition to chloroquine, recent data indicate that bortezomib can also inhibit autophagy via a cathepsin-dependent mechanism that results in p62 up-regulation (12).…”

Section: Discussionmentioning

confidence: 85%

p62/Sequestosome-1 Up-regulation Promotes ABT-263-induced Caspase-8 Aggregation/Activation on the Autophagosome

Huang

Okamoto

et al. 2013

Journal of Biological Chemistry

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Background: Autophagy inhibition up-regulates p62/sequestosome-1, an ubiquitin-binding and multifunctional protein.Results: Up-regulation of p62 promotes caspase-8 self-aggregation and activation by ABT-263, resulting in apoptosis that can be disrupted by p62 mutations at its functional domains. Caspase-8 aggregates co-localize with p62 and the autophagosome marker, LC3. Conclusion: p62 up-regulation can mediate ABT-263-induced apoptosis via caspase-8 activation. Significance: p62 can mediate apoptosis in the setting of autophagy inhibition.

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Section: Discussionmentioning

confidence: 85%

p62/Sequestosome-1 Up-regulation Promotes ABT-263-induced Caspase-8 Aggregation/Activation on the Autophagosome

Huang

Okamoto

et al. 2013

Journal of Biological Chemistry

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“…43 However, a controversy exists in terms of chloroquine efficacy. 44 One explanation is that normal cells also use autophagy to maintain homeostasis, and inhibition of autophagy by chloroquine would also sensitize healthy organs such as kidneys to chemotherapy resulting in severe side effects. 45 Given that basal levels of EGR1 and MIR152 are relatively high in normal cells, activation of the EGR1-MIR152 pathway may not affect signaling of normal cells, but will greatly increase the therapeutic response in cancer cells.…”

Section: Discussionmentioning

confidence: 99%

Downregulation of ATG14 by EGR1-MIR152 sensitizes ovarian cancer cells to cisplatin-induced apoptosis by inhibiting cyto-protective autophagy

et al. 2015

Autophagy

143

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Cisplatin is commonly used in ovarian cancer treatment by inducing apoptosis in cancer cells as a result of lethal DNA damage. However, the intrinsic and acquired resistance to cisplatin in cancer cells remains a big challenge for improving overall survival. The cyto-protective functions of autophagy in cancer cells have been suggested as a potential mechanism for chemoresistance. Here, we reported MIR152 as a new autophagy-regulating miRNA that plays a role in cisplatin-resistance. We showed that MIR152 expression was dramatically downregulated in the cisplatinresistant cell lines A2780/CP70, SKOV3/DDP compared with their respective parental cells, and in ovarian cancer tissues associated with cisplatin-resistance. Overexpression of MIR152 sensitized cisplatin-resistant ovarian cancer cells by reducing cisplatin-induced autophagy, enhancing cisplatin-induced apoptosis and inhibition of cell proliferation. A mouse subcutaneous xenograft tumor model using A2780/CP70 cells with overexpressing MIR152 was established and displayed decreased tumor growth in response to cisplatin. We also identified that ATG14 is a functional target of MIR152 in regulating autophagy inhibition. Furthermore, we found that EGR1 (early growth response 1) regulated the MIR152 gene at the transcriptional level. Ectopic expression of EGR1 enhanced efficacy of chemotherapy in A2780/CP70 cells. More importantly, these findings were relevant to clinical cases. Both EGR1 and MIR152 expression levels were significantly lower in ovarian cancer tissues with high levels of ERCC1 (excision repair cross-complementation group 1), a marker for cisplatin-resistance. Collectively, these data provide insights into novel mechanisms for acquired cisplatinresistance. Activation of EGR1 and MIR152 may be a useful therapeutic strategy to overcome cisplatin-resistance by preventing cyto-protective autophagy in ovarian cancer.

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“…In a recent publication, 7 Dr. Andrew Thorburn and I have postulated the existence of another form of autophagy that will be termed "nonprotective." More specifically, we have observed induction by radiation of a form of autophagy whose inhibition neither sensitizes nor protects the tumor cell from radiation.…”

mentioning

confidence: 99%

“…Leaving aside the vexing question of what would be the most appropriate animal models (xenografts vs. syngeneic vs. transgenic vs. carcinogen-induced, among others), the data in tumor-bearing animals treated with chemotherapy and the autophagy inhibitor chloroquine, is at best equivocal, as described in some detail in our recent paper. 7 That is, in approximately half the studies in the literature, the inclusion of chloroquine produces a modest or minimal increase in tumor growth delay over and above that of the therapeutic modality alone. In our own work, chloroquine fails to improve the response to radiation in a syngeneic model (4T1 cells) of breast cancer.…”

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confidence: 99%

Cytoprotective and nonprotective autophagy in cancer therapy

Gewirtz

2013

Autophagy

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Autophagy Inhibition for Chemosensitization and Radiosensitization in Cancer: Do the Preclinical Data Support This Therapeutic Strategy?

Cited by 88 publications

References 48 publications

p62/Sequestosome-1 Up-regulation Promotes ABT-263-induced Caspase-8 Aggregation/Activation on the Autophagosome

p62/Sequestosome-1 Up-regulation Promotes ABT-263-induced Caspase-8 Aggregation/Activation on the Autophagosome

Downregulation of ATG14 by EGR1-MIR152 sensitizes ovarian cancer cells to cisplatin-induced apoptosis by inhibiting cyto-protective autophagy

Cytoprotective and nonprotective autophagy in cancer therapy

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