Functional Evaluation of a Fluorescent Schweinfurthin: Mechanism of Cytotoxicity and Intracellular Quantification

Kuder, Craig H.; Sheehy, Ryan; Neighbors, Jeffrey D.; Wiemer, David F.; Hohl, Raymond J.

doi:10.1124/mol.111.077107

Cited by 13 publications

(30 citation statements)

References 38 publications

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“…In the A549 cells, 3dSB incubation leads to APO-A1 specific cholesterol efflux further emphasizing the differences between sensitive and insensitive cell lines. We have previously noted that 3-dSB induces ERstress in the SF-295 cell line, as demonstrated by increasing GRP78 expression [39]. Increased ER-stress has been shown to reduce the cellular level of ABCA1 in hepatocellular carcinoma HepG2 cells, and to cause a reduction in cholesterol efflux [38,40].…”

Section: Discussionmentioning

confidence: 92%

“…After indicated incubation conditions, cells were collected and lysed in buffer containing (0.15 M NaCl, 0.05 M Tris HCl, 1 % w/v sodium deoxycholate, 1 % w/v SDS, 1 % w/v TX-100, and 1 mM EDTA, and protease inhibitor cocktail, Sigma-Aldrich). Lysate was incubated on ice for 30 min prior to passage through a 27-G needle [27]. Lysate was centrifuged at 14,000×g for 15 min.…”

Section: Western Blot Analysismentioning

confidence: 99%

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3‐Deoxyschweinfurthin B Lowers Cholesterol Levels by Decreasing Synthesis and Increasing Export in Cultured Cancer Cell Lines

Kuder

Weivoda

Zhang

et al. 2015

Lipids

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The schweinfurthins have potent antiproliferative activity in multiple glioblastoma multiforme (GBM) cell lines; however, the mechanism by which growth is impeded is not fully understood. Previously, we demonstrated that the schweinfurthins reduce the level of key isoprenoid intermediates in the cholesterol biosynthetic pathway. Here in, we describe the effects of the schweinfurthins on cholesterol homeostasis. Intracellular cholesterol levels are greatly reduced in cells incubated with 3-deoxyschweinfurthin B (3dSB), an analog of the natural product schweinfurthin B. Decreased cholesterol levels are due to decreased cholesterol synthesis and increased cholesterol efflux, both of these cellular actions can be influenced by liver X-receptor (LXR) activation. The effects of 3dSB on ATP-binding cassette transporter 1 (ABCA1) levels and other LXR targets are similar to that of 25-hydroxycholesterol, an LXR agonist. Unlike 25-hydroxycholesterol, 3dSB does not act as a direct agonist for LXR α or β. These data suggest that cholesterol homeostasis plays a significant role in the growth inhibitory activity of the schweinfurthins and may elucidate a mechanism that can be targeted in human cancers such as GBM.

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Section: Discussionmentioning

confidence: 92%

Section: Western Blot Analysismentioning

confidence: 99%

3‐Deoxyschweinfurthin B Lowers Cholesterol Levels by Decreasing Synthesis and Increasing Export in Cultured Cancer Cell Lines

Kuder

Weivoda

Zhang

et al. 2015

Lipids

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“…Synthesis of the natural products and development of synthetic analogs opened the door for explorations into the mechanism of schweinfurthin action and initial studies delved into the nature of schweinfurthin cytotoxicity. For sensitive cell lines, schweinfurthin treatment results in a cytotoxic cellular response that is both dose and time dependent (Kuder et al, ). In the sensitive SF‐295 cells, caspase‐9 and PARP cleavage are observed 24 and 36 h, respectively, after treatment with 1 μM of the schweinfurthin analog 3dSB.…”

Section: Mechanismmentioning

confidence: 99%

Schweinfurthins: Lipid Modulators with Promising Anticancer Activity

Koubek

Weissenrieder

Neighbors

et al. 2018

Lipids

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The schweinfurthin family of compounds displays exciting potent and differential cytotoxicity against human cancer cell lines. Currently, the effect of schweinfurthins on tumor development and progression is being explored in animal models of cancer with promising results. The first schweinfurthin family member, vedelianin, was isolated in 1992, followed by other schweinfurthins in 1998. This opened up the door for the synthesis of additional analogs. At present, the focus of research lies on delineating the mechanism of schweinfurthin action and identifying the nature of sensitivity. It appears that many of the intracellular effects of schweinfurthins are due to, or impacted by, the effect of schweinfurthins on lipid metabolism, synthesis, and homeostasis. These effects include impaired trafficking from the trans-golgi network, disruption of lipid rafts, changes in oxysterol-binding protein activity, and interference with the isoprenoid biosynthesis pathway (IBP). Cancer cells are known to rely heavily on fatty acid, lipid, and sterol synthesis for growth and proliferation. Therefore, compounds that target these needs, such as schweinfurthins, display promise as novel therapeutics. This timely review will take an in-depth look at the history of schweinfurthins, their synthesis, where the research presently stands, and the questions that remain.

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“…4G), confirming an ER stress induction effect by SB after a 9 h treatment in cells. 7 Notably, a higher drug concentration was required to induce significant p-EIF2a up-regulation than to inhibit AKT phosphorylation in the same WSU-DLCL2 cells (Figs. 1F, 4G), suggesting that induction of ER stress contributed to inhibition of AKT activation by schweinfurthins.…”

Section: Tgn Trafficking Arrest By Schweinfurthins Leads To Lipid Rafmentioning

confidence: 99%

“…[4][5][6] However, this effort has been hampered by a lack of understanding of mechanism. Recently, schweinfurthin A (SA) was shown to interfere with phosphorylation of Rho in glioma cells 5 and to induce expression of glucose-related protein 78 and phosphorylation of eukaryotic initiation factor 2a, 7 suggesting regulatory roles in signaling and endoplasmic reticulum (ER) induction by schweinfurthins. Interestingly, OSBP and ORP4L, 2 members of the oxysterol-binding protein related family proteins (ORPs) were reported as potential targets for SA and for a few other natural compounds that showed a similar anti-proliferative pattern in the NCI-60 cancer cell panel.…”

Section: Introductionmentioning

confidence: 99%

Small molecule schweinfurthins selectively inhibit cancer cell proliferation and mTOR/AKT signaling by interfering with trans-Golgi-network trafficking

Bao

Zheng

Sugi

et al. 2015

Cancer Biology & Therapy

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Abbreviations: SA-J schweinfurthin A-J; TGN trans-Golgi-network; PTEN phosphatase and tensin homolog; DLBCL diffuse large B cell lymphoma; mTOR mammalian target of rapamycin; PDK1 phosphoinositide-dependent kinase 1; PIP3 phosphatidylinositol (3,4,5)-triphosphate; WGA wheat germ agglutinin; ConA concanavalin; MAA Maackia amurensis agglutinin; PNA peanut agglutinin; ORPs oxysterol-binding protein related family proteins Natural compound schweinfurthins are of considerable interest for novel therapy development because of their selective anti-proliferative activity against human cancer cells. We previously reported the isolation of highly active schweinfurthins E-H, and in the present study, mechanisms of the potent and selective anti-proliferation were investigated. We found that schweinfurthins preferentially inhibited the proliferation of PTEN deficient cancer cells by indirect inhibition of AKT phosphorylation. Mechanistically, schweinfurthins and their analogs arrested trans-Golginetwork trafficking, an intracellular vesicular trafficking system, resulting in the induction of endoplasmic reticulum stress and the suppression of both lipid raft-mediated PI3K activation and mTOR/RheB complex formation, which collectively led to an effective inhibition of mTOR/AKT signaling. The trans-Golgi-network traffic arresting effect of schweinfurthins was associated with their in vitro binding activity to oxysterol-binding proteins that are known to regulate intracellular vesicular trafficking. Moreover, schweinfurthins were found to be highly toxic toward PTENdeficient B cell lymphoma cells, and displayed 2 orders of magnitude lower activity toward normal human peripheral blood mononuclear cells and primary fibroblasts in vitro. These results revealed a previously unrecognized role of schweinfurthins in regulating trans-Golgi-network trafficking, and linked mechanistically this cellular effect with mTOR/ AKT signaling and with cancer cell survival and growth. Our findings suggest the schweinfurthin class of compounds as a novel approach to modulate oncogenic mTOR/AKT signaling for cancer treatment.

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Functional Evaluation of a Fluorescent Schweinfurthin: Mechanism of Cytotoxicity and Intracellular Quantification

Cited by 13 publications

References 38 publications

3‐Deoxyschweinfurthin B Lowers Cholesterol Levels by Decreasing Synthesis and Increasing Export in Cultured Cancer Cell Lines

3‐Deoxyschweinfurthin B Lowers Cholesterol Levels by Decreasing Synthesis and Increasing Export in Cultured Cancer Cell Lines

Schweinfurthins: Lipid Modulators with Promising Anticancer Activity

Small molecule schweinfurthins selectively inhibit cancer cell proliferation and mTOR/AKT signaling by interfering with trans-Golgi-network trafficking

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