Small Molecule Antagonists of the σ-1 Receptor Cause Selective Release of the Death Program in Tumor and Self-Reliant Cells and Inhibit Tumor Growth 
 in Vitro
 and 
 in Vivo

Spruce, Barbara A.; Campbell, Louise; McTavish, Niall; Cooper, Michelle A.; Appleyard, M Virginia L; O’Neill, Mary; Howie, J. W.; Samson, Jayne; Watt, Stephen A.; Murray, Kermit K.; McLean, Doris; Leslie, Nicholas R.; Safrany, Stephen T.; Ferguson, Michelle; Peters, John A.; Prescott, Alan R.; Box, Gary; Hayes, Angela; Nutley, Bernard; Raynaud, Florence I.; Downes, C P; Lambert, Jeremy J.; Thompson, Alastair; Eccles, Suzanne A.

doi:10.1158/0008-5472.can-03-3180

Cited by 157 publications

(216 citation statements)

References 45 publications

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“…Also other σ-2 ligands, haloperidol and rimcazole, induced a rapid rise in the lysosomal pH in MCF-7 cells when added at concentrations with anti-proliferative effects comparable to 8 μM siramesine, i.e., 50 μM and 20 μM, respectively. 10,15 Contrary to the siramesine-induced rise in the lysosomal pH that persisted for up to 16 h (data not shown), the lysosomal pH gradient was re-established in haloperidol-and rimcazole-treated cells already 4 h after the addition of the drug (Fig. 1A).…”

Section: Resultsmentioning

confidence: 80%

“…13 σ-2 selective ligands (e.g., siramesine, CB-184, CB-64D, ibogaine and PB28) as well as non-selective ligands that bind both σ-1 and σ-2 receptors (haloperidol, rimcazole and SR31474A) display anti-tumor activity in many tumor cell lines in vitro as well as in tumor xenografts in vivo. [14][15][16][17] Siramesine is the most potent anti-cancer agent among the known σ-ligands. It kills tumor cell lines originating from breast, cervix, lung, prostate and connective tissue at low micromolar concentrations in vitro and its per oral administration shows potent anti-tumor activity against fibrosarcoma and breast carcinoma grafts in mice.…”

Section: Research Papermentioning

confidence: 99%

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Anti-cancer agent siramesine is a lysosomotropic detergent that induces cytoprotective autophagosome accumulation

Ostenfeld¹,

Høyer-Hansen²,

Bastholm³

et al. 2008

Autophagy

138

120

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A σ-2 receptor ligand siramesine induces lysosomal leakage and cathepsin-dependent death of cancer cells in vitro and displays potent anti-cancer activity in vivo. The mechanism by which siramesine destabilizes lysosomes is, however, unknown. Here, we show that siramesine induces a rapid rise in the lysosomal pH that is followed by lysosomal leakage and dysfunction. The rapid accumulation of siramesine into cancer cell lysosomes, its ability to destabilize isolated lysosomes, and its chemical structure as an amphiphilic amine indicate that it is a lysosomotropic detergent. Notably, siramesine triggers also a substantial Atg6-and Atg7-dependent accumulation of autophagosomes that is associated with a rapid and sustained inhibition of mammalian target of rapamycin complex 1 (mTORC1; an inhibitor of autophagy). Siramesine fails, however, to increase the degradation rate of long-lived proteins. Thus, the massive accumulation of autophagosomes is likely to be due to a combined effect of activation of autophagy signaling and decreased autophagosome turnover. Importantly, pharmacological and RNA interference-based inhibition of autophagosome formation further sensitizes cancer cells to siramesine-induced cytotoxicity. These data identify siramesine as a lysosomotropic detergent that triggers cell death via a direct destabilization of lysosomes and cytoprotection by inducing the accumulation of autophagosomes. Threrefore, the combination of siramesine with inhibitors of autophagosome formation appears as a promising approach for future cancer therapy.

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Section: Resultsmentioning

confidence: 80%

Section: Research Papermentioning

confidence: 99%

Anti-cancer agent siramesine is a lysosomotropic detergent that induces cytoprotective autophagosome accumulation

Ostenfeld¹,

Høyer-Hansen²,

Bastholm³

et al. 2008

Autophagy

138

120

View full text Add to dashboard Cite

show abstract

“…In addition to the calcium regulation, antagonists of Sig-1R inhibit the activity of PKB/Akt in an apparently calcium-independent manner. Thus, PLC activation and PKB/Akt inhibition in response to Sig-1R antagonists appear to constitute biochemically separable signal transduction responses, which are to restrain the proapoptotic signaling pathway and to stimulate a prosurvival signaling cascade (Spruce et al, 2004). Based on these results that Sig-1R regulates apoptosis and survival signaling pathways for the cell survival, cellular protective ability of meGAL against oxidative stress may be linked to the induction of Sig-1R gene by meGAL.…”

Section: Discussionmentioning

confidence: 88%

“…RCC1 is known to be involved in cell cycle, cell proliferation, nuclear transport and the inhibition of the Ran-GEF activity of RCC1 was reported to cause cell death through premature chromatin condensation (Nishijima et al, 2003;Zheng, 2004). Sig-1R also has the variety of functions such as a novel opioid receptor, cellular proliferation and modulations of ion channel, ankyrin, Ca 2+ and sphingolipid levels (Hayashi and Su, 2001;Aydar et al, 2004;Spruce et al, 2004). Similar to RCC1, small molecule antagonists of Sig-1R inhibit tumor cell survival by activating programmed cell death (Zheng, 2004).…”

Section: Discussionmentioning

confidence: 99%

Methyl gallate and chemicals structurally related to methyl gallate protect human umbilical vein endothelial cells from oxidative stress

Whang

Park²,

Ham³

et al. 2005

Exp Mol Med

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“…This synergistic effect could be related to the fact that BD1047 also presented an affinity for the σ 2 receptor (K i = 47 nM). Because σ 1 receptors appear to be antiapoptotic and σ 2 receptors are proapoptotic [17,18], the activation of σ 1 receptors by an agonist and the inhibition of σ 2 receptors by an antagonist should lead to a synergistic effect in terms of cells protection. Indeed, cell protection does not occur when the σ 1 receptors are already blocked by an antagonist, as in the case of the pretreatment with BD1047.…”

Section: Discussionmentioning

confidence: 99%

Neuroactive steroids protect retinal pigment epithelium against oxidative stress

Bucolo

Drago²,

Lin³

et al. 2005

NeuroReport

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This study was undertaken to assess whether neuroactive steroids, 17β-estradiol and dehydroepiandrosterone-sulfate, enhance survival and protect DNA of human retinal pigment epithelial cells challenged by oxidative stress, and to investigate the role of σ 1 receptors in the effects of neuroactive steroids. Retinal pigment epithelial cells were treated with various concentrations of neuroactive steroids and then exposed to hydrogen peroxide. Pretreatment with steroids resulted in significant increased viability in a dose-related manner. DNA damage induced by oxidative insult was significantly lower with steroid pretreatment. The effects of 17β-estradiol and dehydroepiandrosterone-sulfate were antagonized by pretreatment with a σ 1 receptor antagonist. The results suggest that neuroactive steroids protect retinal cells from oxidative stress, and that this effect is mediated by σ 1 receptors.

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Small Molecule Antagonists of the σ-1 Receptor Cause Selective Release of the Death Program in Tumor and Self-Reliant Cells and Inhibit Tumor Growth in Vitro and in Vivo

Cited by 157 publications

References 45 publications

Anti-cancer agent siramesine is a lysosomotropic detergent that induces cytoprotective autophagosome accumulation

Anti-cancer agent siramesine is a lysosomotropic detergent that induces cytoprotective autophagosome accumulation

Methyl gallate and chemicals structurally related to methyl gallate protect human umbilical vein endothelial cells from oxidative stress

Neuroactive steroids protect retinal pigment epithelium against oxidative stress

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