Novel sesquiterpene lactone analogues as potent anti‐breast cancer agents

Nakagawa‐Goto, Kyoko; Chen, Jo-Yu; Cheng, Yu; Lee, Wai Leng; Takeya, Munehisa; Saito, Yohei; Lee, Kuo Hsiung̀; Shyur, Lie‐Fen

doi:10.1016/j.molonc.2016.03.002

Cited by 30 publications

(31 citation statements)

References 25 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The synthesis of DETD-35 followed the method described by Nakagawa-Goto et al (2016). The chemical purity of DET and DETD-35 were >99% as judged by NMR spectrometry.…”

Section: Methodsmentioning

confidence: 99%

Phytoagent Deoxyelephantopin and Its Derivative Inhibit Triple Negative Breast Cancer Cell Activity through ROS-Mediated Exosomal Activity and Protein Functions

et al. 2017

Self Cite

View full text Add to dashboard Cite

A novel plant sesquiterpene lactone derivative, DET derivative (DETD)-35, originating from parental deoxyelephantopin (DET) was previously observed to effectively suppress human triple negative breast cancer (TNBC) MDA-MB-231 cell activity and tumor growth in mice. In this study, the mechanisms underlying the activity of DETD-35 were elucidated. DET and DETD-35 induced reactive oxygen species (ROS) which caused structural damage and dysfunction of mitochondria and increased cytosolic calcium level, subsequently evoking exosome release from the cancer cells. Intriguingly, exosomes induced by both compounds had an atypical function. Cancer cell-derived exosomes commonly show metastatic potential, but upon DET/DETD-35 treatment exosomes showed anti-proliferative activity against MDA-MB-231 cells. Quantitative proteome analysis of TNBC cell-secreted exosomes showed that DET and DETD-35 attenuated the expression of proteins related to cell migration, cell adhesion, and angiogenesis. Furthermore, several exosomal proteins participating in biological mechanisms such as oxidative stress and decrease of transmembrane potential of mitochondria were found deregulated by treatment with either compound. Pretreatment with ROS scavenger, N-acetylcysteine, blockaded DET- or DETD-35-induced oxidative stress and calcium dependent exosome release mechanisms, and also reverted DET- or DETD-35-induced reprogramming exosomal protein expression profiles resulting in attenuation of exosomal toxicity against TNBC cell proliferation. In summary, this study shows that a plant-derived sesquiterpene lactone DET and its analog DETD-35 inhibitory TNBC cell activities through oxidative stress-induced cancer cell releasing exosomes in tandem with alteration of exosomal protein composition and functions. The findings of this study suggest that DETD-35 may be suitable for further development into an anti-TNBC drug.

show abstract

“…The synthesis of DETD-35 followed the method described by Nakagawa-Goto et al (2016). The chemical purity of DET and DETD-35 were >99% as judged by NMR spectrometry.…”

Section: Methodsmentioning

confidence: 99%

Phytoagent Deoxyelephantopin and Its Derivative Inhibit Triple Negative Breast Cancer Cell Activity through ROS-Mediated Exosomal Activity and Protein Functions

et al. 2017

Self Cite

View full text Add to dashboard Cite

show abstract

“…DETD-3 was derived from DET by translactonization via the hydrolysis of DET followed by acidic treatment. DETD-5, −6, −13, −17, −19, −24, −31, −33, −35, −39, and −43 were further synthesized from DETD-3 (26). …”

Section: Methodsmentioning

confidence: 99%

A Novel Plant Sesquiterpene Lactone Derivative, DETD-35, Suppresses BRAFV600E Mutant Melanoma Growth and Overcomes Acquired Vemurafenib Resistance in Mice

Feng

Nakagawa‐Goto

Lee

et al. 2016

Molecular Cancer Therapeutics

Self Cite

View full text Add to dashboard Cite

Acquired resistance to vemurafenib develops through reactivation of RAF/MEK/ERK signaling or bypass mechanisms. Recent combination therapies such as a MEK inhibitor combined with vemurafenib show improvement in major clinical end points but the percentage of patients with adverse toxic events is higher than with vemurafenib monotherapy and most patients ultimately relapse. Therefore, there is an urgent need to develop new anti-melanoma drugs and/or adjuvant agents for vemurafenib therapy. In this study, we created a novel semi-organically modified derivative, DETD-35, from deoxyelephantopin (DET), a plant sesquiterpene lactone demonstrated as an anti-inflammatory and anti-mammary tumor agent. Our results show that DETD-35 inhibited proliferation of a panel of melanoma cell lines, including acquired vemurafenib resistance A375 cells (A375-R) established in this study, with superior activities to DET and no cytotoxicity to normal melanocytes. DETD-35 suppressed tumor growth and reduced tumor mass as effectively as vemurafenib in A375 xenograft study. Furthermore, DETD-35 also reduced tumor growth in both acquired (A375-R) and intrinsic (A2058) vemurafenib resistance xenograft models, where vemurafenib showed no anti-tumor activity. Notably, the combination of DETD-35 and vemurafenib exhibited the most significant effects in both in vitro and in vivo xenograft studies due to synergism of the compound and the drug. Mechanistic studies suggested that DETD-35 overcame acquired vemurafenib resistance at least in part through deregulating MEK-ERK, Akt, and STAT3 signaling pathways and promoting apoptosis of cancer cells. Overall, our results suggest that DETD-35 may be useful as a therapeutic or adjuvant agent against BRAFV600E mutant and acquired vemurafenib resistance melanoma.

show abstract

“…which can be classified as electrophilic sesquiterpenes (ESs). Application of ES compounds to TNBC treatment shows promising prospects . These ESs may exercise their biological activities by reacting with an appropriately positioned nucleophilic residue available on targeted proteins or enzymes (usually, but not always, a cysteine thiol amino acid group) .…”

Section: Introductionmentioning

confidence: 99%

“…Moreover, thiol/disulphide homeostasis was reported to play a critical role in antioxidant defence and detoxification in the body . Thus, through Michel's reaction, ESs with specific electrophilic groups alkylate the enzymes or transcription factors, regulate key cellular signal pathways, and then produce anti‐TNBC activity . Targeted covalent modification has emerged as a validated approach to drug discovery with the recent US Food and Drug Administration (FDA) approvals of afatanib (2013), ibrutinib (2013), and osimertinib (2015) drugs that were designed to undergo an irreversible hetero‐Michael addition reaction with a unique cysteine residue of a specific protein …”

Section: Introductionmentioning

confidence: 99%

“…Application of ES compounds to TNBC treatment shows promising prospects. [7][8][9] These ESs may exercise their biological activities by reacting with an appropriately positioned nucleophilic residue available on targeted proteins or enzymes (usually, but not always, a cysteine thiol amino acid group). 6,7,[10][11][12] Thiol groups plays an important role in TNBC-related pathways and physiology.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Targeting pharmacophore with probe‐reactivity‐guided fractionation to precisely identify electrophilic sesquiterpenes and its activity of anti‐TNBC

Jiang

Zhu

Shou

et al. 2019

Phytochemical Analysis

View full text Add to dashboard Cite

Introduction Innovative strategy is urgently needed to precisely discover novel natural products as lead compounds for development of new drugs against orphan diseases such as triple‐negative breast cancer (TNBC). Herein, we describe a targeting pharmacophore with probe‐reactivity‐guided strategy for the discovery of electrophilic sesquiterpene (ES), a class of bioactive natural product. Objective This study aimed to identify pharmacophore, based on pharmacophore with probe‐reactivity‐guided strategy for precisely discovering ESs from ethyl acetate extract of Eupatorium chinense L. (EEEChL) Methodology MTT assay combined with ultra‐performance liquid chromatography (UPLC) analysis was used to identify pharmacophore. UPLC‐mass spectrometry (MS) was applied to carefully compare the intrinsic reactivity characteristics of two chemoselective nucleophilic probes: glutathione (GSH) and 4‐bromothiophenol (BTP) reaction with ESs. ESs was isolated and identified from EEEChL by phytochemical methods. Furthermore, stoichiometric ratio and binding site of one typical ES 8β‐[4′‐hydroxytigloyloxy]‐5‐desoxy‐8‐desacyleuparotin (HDDE) reaction with BTP were studied by UPLC‐quadrupole time‐of‐flight (Q‐TOF)‐MS and two‐dimensional nuclear magnetic resonance (NMR). Results Eleven ESs were identified from EEEChL, MTT assay illustrated that all of the 11 ESs possess fairly good anti‐TNBC activity Conclusions Electrophilic groups were confirmed as pharmacophore of bioactive compounds contained in EEEChL. An optimised halogenated aromatic probe BTP furnishes ES‐BTP conjugates that are highly conspicuous via MS by virtue of a unique isotopic bromine signature, conjugates also have a considerable separation on C18 column. The new probe‐reactivity‐guided strategy can effectively improve the traditional bioassay‐guided approaches, and significantly increase the probability of obtaining designated bioactive compounds.

show abstract

Novel sesquiterpene lactone analogues as potent anti‐breast cancer agents

Cited by 30 publications

References 25 publications

Phytoagent Deoxyelephantopin and Its Derivative Inhibit Triple Negative Breast Cancer Cell Activity through ROS-Mediated Exosomal Activity and Protein Functions

Phytoagent Deoxyelephantopin and Its Derivative Inhibit Triple Negative Breast Cancer Cell Activity through ROS-Mediated Exosomal Activity and Protein Functions

A Novel Plant Sesquiterpene Lactone Derivative, DETD-35, Suppresses BRAFV600E Mutant Melanoma Growth and Overcomes Acquired Vemurafenib Resistance in Mice

Targeting pharmacophore with probe‐reactivity‐guided fractionation to precisely identify electrophilic sesquiterpenes and its activity of anti‐TNBC

Contact Info

Product

Resources

About