Your search keyword '"Dokudovskaya, Svetlana"' showing total 8 results

1. Laherradurin Inhibits Colorectal Cancer Cell Growth by Induction of Mitochondrial Dysfunction and Autophagy Induction.

Author

Delgado-Waldo, Izamary, Dokudovskaya, Svetlana, Loissell-Baltazar, Yahir A., Pérez-Arteaga, Eduardo, Coronel-Hernández, Jossimar, Martínez-Vázquez, Mariano, Pérez-Yépez, Eloy Andrés, Lopez-Saavedra, Alejandro, Jacobo-Herrera, Nadia, and Pérez Plasencia, Carlos

Subjects

*MITOCHONDRIAL dynamics, *CANCER cell growth, *CELL survival, *APOPTOSIS, *WESTERN immunoblotting

Abstract

LAH, an acetogenin from the Annonaceae family, has demonstrated antitumor activity in several cancer cell lines and in vivo models, where it reduced the tumor size and induced programmed cell death. We focused on the effects of LAH on mitochondrial dynamics, mTOR signaling, autophagy, and apoptosis in colorectal cancer (CRC) cells to explore its anticancer potential. Methods: CRC cells were treated with LAH, and its effects on mitochondrial respiration and glycolysis were measured using Seahorse XF technology. The changes in mitochondrial dynamics were observed through fluorescent imaging, while Western blot analysis was used to examine key autophagy and apoptosis markers. Results: LAH significantly inhibited mitochondrial complex I activity, inducing ATP depletion and a compensatory increase in glycolysis. This disruption caused mitochondrial fragmentation, a trigger for autophagy, as shown by increased LC3-II expression and mTOR suppression. Apoptosis was also confirmed through the cleavage of caspase-3, contributing to reduced cancer cell viability. Conclusions: LAH's anticancer effects in CRC cells are driven by its disruption of mitochondrial function, triggering both autophagy and apoptosis. These findings highlight its potential as a therapeutic compound for further exploration in cancer treatment. [ABSTRACT FROM AUTHOR]

Published

2024

2. The Role of mTORC1 Pathway and Autophagy in Resistance to Platinum-Based Chemotherapeutics.

Author

Pan, Zhenrui, Zhang, Hanxiao, and Dokudovskaya, Svetlana

Subjects

PLATINUM, AUTOPHAGY, CISPLATIN, ANTINEOPLASTIC agents

Abstract

Cisplatin (cis-diamminedichloroplatinum I) is a platinum-based drug, the mainstay of anticancer treatment for numerous solid tumors. Since its approval by the FDA in 1978, the drug has continued to be used for the treatment of half of epithelial cancers. However, resistance to cisplatin represents a major obstacle during anticancer therapy. Here, we review recent findings on how the mTORC1 pathway and autophagy can influence cisplatin sensitivity and resistance and how these data can be applicable for the development of new therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2023

3. Keeping Cell Death Alive: An Introduction into the French Cell Death Research Network.

Author

Ichim, Gabriel, Gibert, Benjamin, Adriouch, Sahil, Brenner, Catherine, Davoust, Nathalie, Desagher, Solange, Devos, David, Dokudovskaya, Svetlana, Dubrez, Laurence, Estaquier, Jérôme, Gillet, Germain, Guénal, Isabelle, Juin, Philippe P., Kroemer, Guido, Legembre, Patrick, Levayer, Romain, Manon, Stéphen, Mehlen, Patrick, Meurette, Olivier, and Micheau, Olivier

Subjects

THANATOLOGY, CELL death, CANCER cells, CAENORHABDITIS elegans, NOBEL Prizes, APOPTOSIS

Abstract

Since the Nobel Prize award more than twenty years ago for discovering the core apoptotic pathway in C. elegans, apoptosis and various other forms of regulated cell death have been thoroughly characterized by researchers around the world. Although many aspects of regulated cell death still remain to be elucidated in specific cell subtypes and disease conditions, many predicted that research into cell death was inexorably reaching a plateau. However, this was not the case since the last decade saw a multitude of cell death modalities being described, while harnessing their therapeutic potential reached clinical use in certain cases. In line with keeping research into cell death alive, francophone researchers from several institutions in France and Belgium established the French Cell Death Research Network (FCDRN). The research conducted by FCDRN is at the leading edge of emerging topics such as non-apoptotic functions of apoptotic effectors, paracrine effects of cell death, novel canonical and non-canonical mechanisms to induce apoptosis in cell death-resistant cancer cells or regulated forms of necrosis and the associated immunogenic response. Collectively, these various lines of research all emerged from the study of apoptosis and in the next few years will increase the mechanistic knowledge into regulated cell death and how to harness it for therapy. [ABSTRACT FROM AUTHOR]

Published

2022

4. Identification of Small Molecules Inhibiting Cardiomyocyte Necrosis and Apoptosis by Autophagy Induction and Metabolism Reprogramming.

Author

Liu, Dawei, Peyre, Félix, Loissell-Baltazar, Yahir Alberto, Courilleau, Delphine, Lacas-Gervais, Sandra, Nicolas, Valérie, Jacquet, Eric, Dokudovskaya, Svetlana, Taran, Frédéric, Cintrat, Jean-Christophe, and Brenner, Catherine

Subjects

SMALL molecules, CELL death, AUTOPHAGY, HEART cells, APOPTOSIS, NECROSIS

Abstract

Improvement of anticancer treatments is associated with increased survival of cancer patients at risk of cardiac disease. Therefore, there is an urgent need for new therapeutic molecules capable of preventing acute and long-term cardiotoxicity. Here, using commercial and home-made chemolibraries, we performed a robust phenotypic high-throughput screening in rat cardiomyoblast cell line H9c2, searching for small molecules capable of inhibiting cell death. A screen of 1600 compounds identified six molecules effective in preventing necrosis and apoptosis induced by H2O2 and camptothecin in H9c2 cells and in rat neonatal ventricular myocytes. In cells treated with these molecules, we systematically evaluated the expression of BCL-2 family members, autophagy progression, mitochondrial network structure, regulation of mitochondrial fusion/fission, reactive oxygen species, and ATP production. We found that these compounds affect autophagy induction to prevent cardiac cell death and can be promising cardioprotective drugs during chemotherapy. [ABSTRACT FROM AUTHOR]

Published

2022

5. SEA and GATOR 10 Years Later.

Author

Loissell-Baltazar, Yahir A. and Dokudovskaya, Svetlana

Subjects

*SACCHAROMYCES cerevisiae, *NEURODEGENERATION, *BIOLOGY, *YEAST, *NEUROLOGICAL disorders

Abstract

The SEA complex was described for the first time in yeast Saccharomyces cerevisiae ten years ago, and its human homologue GATOR complex two years later. During the past decade, many advances on the SEA/GATOR biology in different organisms have been made that allowed its role as an essential upstream regulator of the mTORC1 pathway to be defined. In this review, we describe these advances in relation to the identification of multiple functions of the SEA/GATOR complex in nutrient response and beyond and highlight the consequence of GATOR mutations in cancer and neurodegenerative diseases. [ABSTRACT FROM AUTHOR]

Published

2021

6. HIV-1 Tat Activates Akt/mTORC1 Pathway and AICDA Expression by Downregulating Its Transcriptional Inhibitors in B Cells.

Author

Akbay, Burkitkan, Germini, Diego, Bissenbaev, Amangeldy K., Musinova, Yana R., Sheval, Evgeny V., Vassetzky, Yegor, Dokudovskaya, Svetlana, and Goncharova, Elena A.

Subjects

HIV, TAT protein, CYTIDINE deaminase, T cells, CELL transformation, B cells

Abstract

HIV-1 infects T cells, but the most frequent AIDS-related lymphomas are of B-cell origin. Molecular mechanisms of HIV-1-induced oncogenic transformation of B cells remain largely unknown. HIV-1 Tat protein may participate in this process by penetrating and regulating gene expression in B cells. Both immune and cancer cells can reprogram communications between extracellular signals and intracellular signaling pathways via the Akt/mTORC1 pathway, which plays a key role in the cellular response to various stimuli including viral infection. Here, we investigated the role of HIV-1 Tat on the modulation of the Akt/mTORC1 pathway in B cells. We found that HIV-1 Tat activated the Akt/mTORC1 signaling pathway; this leads to aberrant activation of activation-induced cytidine deaminase (AICDA) due to inhibition of the AICDA transcriptional repressors c-Myb and E2F8. These perturbations may ultimately lead to an increased genomic instability and proliferation that might cause B cell malignancies. [ABSTRACT FROM AUTHOR]

Published

2021

7. Oncogenic Properties of the EBV ZEBRA Protein.

Author

Germini, Diego, Sall, Fatimata Bintou, Shmakova, Anna, Wiels, Joëlle, Dokudovskaya, Svetlana, Drouet, Emmanuel, and Vassetzky, Yegor

Subjects

CARCINOGENESIS, EPSTEIN-Barr virus, GENE expression, GRAFT versus host disease, ONCOGENES, PROTEINS, TRANSCRIPTION factors, TUMOR markers, DISEASE progression, IMMUNOCOMPROMISED patients

Abstract

Epstein Barr Virus (EBV) is one of the most common human herpesviruses. After primary infection, it can persist in the host throughout their lifetime in a latent form, from which it can reactivate following specific stimuli. EBV reactivation is triggered by transcriptional transactivator proteins ZEBRA (also known as Z, EB-1, Zta or BZLF1) and RTA (also known as BRLF1). Here we discuss the structural and functional features of ZEBRA, its role in oncogenesis and its possible implication as a prognostic or diagnostic marker. Modulation of host gene expression by ZEBRA can deregulate the immune surveillance, allow the immune escape, and favor tumor progression. It also interacts with host proteins, thereby modifying their functions. ZEBRA is released into the bloodstream by infected cells and can potentially penetrate any cell through its cell-penetrating domain; therefore, it can also change the fate of non-infected cells. The features of ZEBRA described in this review outline its importance in EBV-related malignancies. [ABSTRACT FROM AUTHOR]

Published

2020

8. Modulation of mTORC1 Signaling Pathway by HIV-1.

Author

Akbay, Burkitkan, Shmakova, Anna, Vassetzky, Yegor, and Dokudovskaya, Svetlana

Subjects

CELL proliferation, VIRAL replication, VIRUS diseases, LIFE cycles (Biology)

Abstract

Mammalian target of rapamycin complex 1 (mTORC1) is a master regulator of cellular proliferation and survival which controls cellular response to different stresses, including viral infection. HIV-1 interferes with the mTORC1 pathway at every stage of infection. At the same time, the host cells rely on the mTORC1 pathway and autophagy to fight against virus replication and transmission. In this review, we will provide the most up-to-date picture of the role of the mTORC1 pathway in the HIV-1 life cycle, latency and HIV-related diseases. We will also provide an overview of recent trends in the targeting of the mTORC1 pathway as a promising strategy for HIV-1 eradication. [ABSTRACT FROM AUTHOR]

Published

2020