10&lt;em&gt;H&lt;/em&gt;-3,6-Diazaphenothiazine  induces G&lt;sub&gt;2&lt;/sub&gt;/M phase cell cycle arrest and caspase-dependent apoptosis and inhibits cell invasion of A2780 ovarian carcinoma cells through the regulation of NF-&amp;kappa;B and (BIRC6-XIAP) complexes

Zhang, Jianxin; Chen, Ming; Zhang, Wenzhi; Okechukwu, Patrick Nwabueze; Morak‐Młodawska, Beata; Pluta, Krystian; Jeleń, Małgorzata; Akim, Abdah Md; Ang, Kok Pian; Ooi, Kah Kooi

doi:10.2147/dddt.s144415

Cited by 22 publications

(32 citation statements)

References 71 publications

(98 reference statements)

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“…X-chromosome-linked IAP (XIAP), one of the eight human IAP proteins, has been found to exert the most pronounced antiapoptotic function, which is associated with its ability to block caspase−3, −7, and −9 (61). Moreover, some studies have demonstrated that XIAP has also been implicated in the regulation of NF-κB (62). In a previous study, it was found that -Ru1 induces apoptosis through the mitochondrial-mediated pathway, and regulates the expression of proapoptotic proteins, including the downregulation of Bcl-2/Bcl-xl, and the up-regulation of cytochrome c (Cyt C), caspase 9 and caspase 3 (32).…”

Section: Discussionmentioning

confidence: 99%

Combination of Ruthenium Complex and Doxorubicin Synergistically Inhibits Cancer Cell Growth by Down-Regulating PI3K/AKT Signaling Pathway

et al. 2020

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Combinational use of drugs has been a common strategy in cancer treatment because of synergistic advantages in reducing dose and toxicity, minimizing or delaying drug resistance. To improve the efficacy of chemotherapy, various potential combinations have been investigated. Ruthenium complex is considered a potential alternative of the platinum-based drugs due to its significant efficacy and safety. Previously, we reported that ruthenium(II) complex ( -Ru1) has great anticancer potential and minor toxicity toward normal tissues. However, the therapeutic efficacy and mechanism of action of ruthenium(II) complex combined with other anticancer drugs is still unknown. Here, we investigated the combinational effect of -Ru1 and doxorubicin in different cancer cells. The data assessed by Chou-Talalay method showed significant synergism in MCF-7 cells. Furthermore, the results in antiproliferation efficacy indicated that the combination showed strong cytotoxicity and increasing apoptosis of MCF-7 cells in 2D and 3D multicellular tumor spheroids (MCTSs). Significant inhibition of MCF-7 cells accompanied with increased ROS generation was observed. Furthermore, the expression of PI3K/AKT was significantly down-regulated, while the expression of PTEN was strongly up-regulated in cells treated with combination of -Ru1 and doxorubicin. The expression of NF-κB and XIAP decreased while the expression of P53 increased and associated with apoptosis. These findings suggest that the combination of ruthenium complex and doxorubicin has a significant synergistic effect by down-regulating the PI3K/AKT signaling pathway in MCF-7 cells. This study may trigger more research in ruthenium complex and combination therapy that will be able to provide opportunities for developing better therapeutics for cancer treatment.

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Section: Discussionmentioning

confidence: 99%

Combination of Ruthenium Complex and Doxorubicin Synergistically Inhibits Cancer Cell Growth by Down-Regulating PI3K/AKT Signaling Pathway

et al. 2020

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“…The tested compound for present study, namely PTZ was the tested compound preceded from previous studies. [19] Phenothiazine derivative was synthesized by professional medicinal chemistry research group from Medical University of Silesia, Sosnowiec, Republic of Poland; and this compound was synthesized according to the information obtained from respective publications. The detailed characteristic of this compound was explained in respective reports.…”

Section: Tested Compoundmentioning

confidence: 99%

“…[15][16][17] Beyond the routine metabolic functions of estrogen hormone, binding of the estrogen to its membrane-bound receptors (ESR1 and ESR2) tends to produce several downstream targeted genes, which are generally involved in regulation of cell division and proliferation, inhibit cell death mechanism, and promote secondary metastasis of cancer cells. [18][19][20] It is commonly known that dietary factors such as high glucose diet intake would increase the risk to have breast cancer. [21] In cellular biology, the AKT1 gene detected presence of high glucose molecules and send the signals to pancreas for secretion of insulin hormone for glycolysis process; despite high amount of insulin eventually promoting cells to synthesize more insulin-like growth factor-1 receptor (IGF-1R) on surface of plasma membrane for cellular intake of glucose and subsequent glycolysis process.…”

Section: Introductionmentioning

confidence: 99%

“…Unfortunately, estrogen hormone binds nonselectively toward IGF-1R instead of its own estrogen receptor-1 (ESR1) or -2 (ESR2) and results in activation of cell proliferation signalling cascade and promoting cell survival via inhibition of programmed cell death mechanism. [19] In contrast, high mitochondrial thioredoxin reductase (TrxR) enzymatic activity boosts the mitochondrial activities of cancer cells and contributes to reduction in efficacy of chemotherapeutic compounds, thus yielding to resistance features of breast cancer. [20] Excessive electron sources surrounding the cancer cells eventually provided enough electron supplies for cancer cells' mitochondria to carry out routine tasks: (a) reduction of thioredoxin, the substrate of TrxR enzyme; (b) electron transport chain reaction for ATP production, which encouraged proliferation of cancer cells.…”

Section: Introductionmentioning

confidence: 99%

“…[24] Previous studies on anticancer activities of phenothiazine derivative compound, namely 10H-3,6-diazaphenothiazine (named as PTZ, for this report) on A2780 ovarian cancer cells exhibited inhibition on proliferation of cancer cells by induction of G 2 /M-phase cell cycle checkpoint and induced apoptosis via inhibitory regulation on NF-κB gene and BIRC6-XIAP complexes. [19] For instance, ovarian and breast cancers were both cancers related estrogen hormone and the interaction of estrogen hormone with several pro-proliferation membrane-bound receptor; this steroid-derived hormone enhances conjugation of NF-κB gene with BIRC gene family, for example, NF-κB-XIAP-BIRC6 complex. Thus leading to the inhibition of caspase activation, negative regulation of apoptosis pathways and contribute to the death signals resistance.…”

Section: Introductionmentioning

confidence: 99%

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10H‐3,6‐Diazaphenothiazines triggered the mitochondrial‐dependent and cell death receptor‐dependent apoptosis pathways and further increased the chemosensitivity of MCF‐7 breast cancer cells via inhibition of AKT1 pathways

Ren

Hao

Yang

et al. 2020

J Biochem & Molecular Tox

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Breast cancer is one of the leading causes of death in cancer categories, followed by lung, colorectal, and ovarian among the female gender across the world. 10H‐3,6‐diazaphenothiazine (PTZ) is a thiazine derivative compound that exhibits many pharmacological activities. Herein, we proceed to investigate the pharmacological activities of PTZ toward breast cancer MCF‐7 cells as a representative in vitro breast cancer cell model. The PTZ exhibited a proliferation inhibition (IC50 = 0.895 µM) toward MCF‐7 cells. Further, cell cycle analysis illustrated that the S‐phase checkpoint was activated to achieve proliferation inhibition. In vitro cytotoxicity test on three normal cell lines (HEK293 normal kidney cells, MCF‐10A normal breast cells, and H9C2 normal heart cells) demonstrated that PTZ was more potent toward cancer cells. Increase in the levels of reactive oxygen species results in polarization of mitochondrial membrane potential (ΔΨm), together with suppression of mitochondrial thioredoxin reductase enzymatic activity suggested that PTZ induced oxidative damages toward mitochondria and contributed to improved drug efficacy toward treatment. The RT2 PCR Profiler Array (human apoptosis pathways) proved that PTZ induced cell death via mitochondria‐dependent and cell death receptor‐dependent pathways, through a series of modulation of caspases, and the respective morphology of apoptosis was observed. Mechanistic studies of apoptosis suggested that PTZ inhibited AKT1 pathways resulting in enhanced drug efficacy despite it preventing invasion of cancer cells. These results showed the effectiveness of PTZ in initiation of apoptosis, programmed cell death, toward highly chemoresistant MCF‐7 cells, thus suggesting its potential as a chemotherapeutic drug.

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Expedition of sulfur‐containing heterocyclic derivatives as cytotoxic agents in medicinal chemistry: A decade update

Laxmikeshav

Kumari

Shankaraiah

2021

Medicinal Research Reviews

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This review article proposes a comprehensive report of the design strategies engaged in the development of various sulfur-bearing cytotoxic agents. The outcomes of various studies depict that the sulfur heterocyclic framework is a fundamental structure in diverse synthetic analogs representing a myriad scope of therapeutic activities. A number of five-, six-and seven-membered sulfur-containing heterocyclic scaffolds, such as thiazoles, thiadiazoles, thiazolidinediones, thiophenes, thiopyrans, benzothiazoles, benzothiophenes, thienopyrimidines, simple and modified phenothiazines, and thiazepines have been discussed. The subsequent studies of the derivatives unveiled their cytotoxic effects through multiple mechanisms (viz. inhibition of tyrosine kinases, topoisomerase I and II, tubulin, COX, DNA synthesis, and PI3K/Akt and Raf/MEK/ERK signaling pathways), and several others. Thus, our concise illustration explains the design strategy and anticancer potential of these five-and six-membered sulfur-containing heterocyclic molecules along with a brief outline on seven-membered sulfur heterocycles. The thorough assessment of antiproliferative activities with the reference drug allows a proficient assessment of the structure-activity relationships (SARs) of the diversely synthesized molecules of the series.

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10<em>H</em>-3,6-Diazaphenothiazine induces G<sub>2</sub>/M phase cell cycle arrest and caspase-dependent apoptosis and inhibits cell invasion of A2780 ovarian carcinoma cells through the regulation of NF-κB and (BIRC6-XIAP) complexes

Cited by 22 publications

References 71 publications

Combination of Ruthenium Complex and Doxorubicin Synergistically Inhibits Cancer Cell Growth by Down-Regulating PI3K/AKT Signaling Pathway

Combination of Ruthenium Complex and Doxorubicin Synergistically Inhibits Cancer Cell Growth by Down-Regulating PI3K/AKT Signaling Pathway

10H‐3,6‐Diazaphenothiazines triggered the mitochondrial‐dependent and cell death receptor‐dependent apoptosis pathways and further increased the chemosensitivity of MCF‐7 breast cancer cells via inhibition of AKT1 pathways

Expedition of sulfur‐containing heterocyclic derivatives as cytotoxic agents in medicinal chemistry: A decade update

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