Plumbagin sensitizes breast cancer cells to tamoxifen-induced cell death through GRP78 inhibition and Bik upregulation

Kawiak, Anna; Domachowska, Anna; Jaworska, Anna; Łojkowska, Ewa

doi:10.1038/srep43781

Cited by 30 publications

(24 citation statements)

References 45 publications

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“…Our data seems to be consistent with research conducted in breast cancer. The researchers proposed that plumbagin (anticancer drug) induces apoptosis in estrogenpositive breast cancer cells through HSPA5 (GRP78) inhibition (18). Nevertheless, in accordance to our studies afatinib by itself induces apoptosis and mRNA level of HSPA5 decreases.…”

Section: Discussionsupporting

confidence: 88%

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The Effect of Afatinib Treatment in Non-small Cell Lung Cancer Cells

Pancewicz-Wojtkiewicz

Bernatowicz

2017

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Section: Discussionsupporting

confidence: 88%

“…In our results, it seems that apoptosis is caused by afatinib treatment and HSPA5 mRNA level reduction depends on morphological changes. However, our interpretations require further experiments, although it appears there is some connection between anticancer drugs apoptotic effect and HSPA5 in cancer cells (18).…”

Section: Discussionmentioning

confidence: 77%

The Effect of Afatinib Treatment in Non-small Cell Lung Cancer Cells

Pancewicz-Wojtkiewicz

Bernatowicz

2017

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“…For this reason, the development of specific BiP inhibitors represents an important goal. In fact, a natural product of the naphthoquinone family, plumbagin, was identified that initiates cell death in ER-positive breast cancer cells by upregulating BIK levels [ 219 , 220 ]. Plumbagin-mediated BiP inhibition also sensitized breast cancer cells to tamoxifen-mediated cell death.…”

Section: Bip Upregulation Is a Marker For Drug Resistance In Breast Cmentioning

confidence: 99%

“…Plumbagin-mediated BiP inhibition also sensitized breast cancer cells to tamoxifen-mediated cell death. In addition, BiP knock down impaired the plumbagin-mediated increase in Bik, suggesting an inhibitory role of this compound on BiP-mediated downregulation of BIK in breast cancers [ 220 ]. Overall, BiP is emerging as a novel target to predict cancer outcomes and therapeutic options [ 209 , 221 – 223 ].…”

Section: Bip Upregulation Is a Marker For Drug Resistance In Breast Cmentioning

confidence: 99%

Targeting protein quality control pathways in breast cancer

Sannino¹,

Brodsky²

2017

BMC Biol

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The efficient production, folding, and secretion of proteins is critical for cancer cell survival. However, cancer cells thrive under stress conditions that damage proteins, so many cancer cells overexpress molecular chaperones that facilitate protein folding and target misfolded proteins for degradation via the ubiquitin-proteasome or autophagy pathway. Stress response pathway induction is also important for cancer cell survival. Indeed, validated targets for anti-cancer treatments include molecular chaperones, components of the unfolded protein response, the ubiquitin-proteasome system, and autophagy. We will focus on links between breast cancer and these processes, as well as the development of drug resistance, relapse, and treatment.

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“…Another emerging target is the cytosolic Hsp70 molecular chaperone, which is upregulated in many cancers and inhibits multiple steps in the apoptotic pathway (Garrido et al, 2006;Santarosa et al, 1997;Uozaki et al, 2000). Inhibition of Hsp70 or the ER luminal homolog, BiP (also known as GRP78 and HSPA5), kills colorectal carcinomas, breast cancers, leukemia cells, glioblastomas and ovarian cancer cells (Cerezo et al, 2016;Guo et al, 2005;Kawiak et al, 2017;Lee, 2001Lee, , 2007Ni et al, 2009;Powers et al, 2008Powers et al, , 2009Sabnis et al, 2016). Furthermore, Hsp70 promotes chemotherapeutic resistance, and Hsp70 induction predicts metastasis in several cancers (Brodsky and Chiosis, 2006;Calderwood and Gong, 2016;Nanbu et al, 1998;Patury et al, 2009;Powers et al, 2009).…”

Section: Introductionmentioning

confidence: 99%

Compensatory increases of select proteostasis networks after Hsp70 inhibition in cancer cells

Sannino

Guerriero

Sabnis

et al. 2018

Journal of Cell Science

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Cancer cells thrive when challenged with proteotoxic stress by inducing components of the protein folding, proteasome, autophagy and unfolded protein response (UPR) pathways. Consequently, specific molecular chaperones have been validated as targets for anti-cancer therapies. For example, inhibition of Hsp70 family proteins (hereafter Hsp70) in rhabdomyosarcoma triggers UPR induction and apoptosis. To define how these cancer cells respond to compromised proteostasis, we compared rhabdomyosarcoma cells that were sensitive (RMS13) or resistant (RMS13-R) to the Hsp70 inhibitor MAL3-101. We discovered that endoplasmic reticulum-associated degradation (ERAD) and autophagy were activated in RMS13-R cells, suggesting that resistant cells overcome Hsp70 ablation by increasing misfolded protein degradation. Indeed, RMS13-R cells degraded ERAD substrates more rapidly than RMS cells and induced the autophagy pathway. Surprisingly, inhibition of the proteasome or ERAD had no effect on RMS13-R cell survival, but silencing of select autophagy components or treatment with autophagy inhibitors restored MAL3-101 sensitivity and led to apoptosis. These data indicate a route through which cancer cells overcome a chaperone-based therapy, define how cells can adapt to Hsp70 inhibition, and demonstrate the value of combined chaperone and autophagy-based therapies.This article has an associated First Person interview with the first author of the paper.

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Plumbagin sensitizes breast cancer cells to tamoxifen-induced cell death through GRP78 inhibition and Bik upregulation

Cited by 30 publications

References 45 publications

The Effect of Afatinib Treatment in Non-small Cell Lung Cancer Cells

The Effect of Afatinib Treatment in Non-small Cell Lung Cancer Cells

Targeting protein quality control pathways in breast cancer

Compensatory increases of select proteostasis networks after Hsp70 inhibition in cancer cells

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