Каспаза-2 - новый молекулярно-генетический прогностический фактор контроля эффективности хирургического лечения карциномы яичника
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1.Caspase-2 as a master regulator of genomic stability
- 关键词:
- APOPTOSIS INHIBITOR 5; DNA-DAMAGE RESPONSE; CELL-DEATH; PIDDOSOME; ACTIVATION; COMPLEX; CLEAVAGE; PIDD; MDM2; P53
- Kopeina, Gelina S.;Zhivotovsky, Boris
- 《TRENDS IN CELL BIOLOGY》
- 2021年
- 31卷
- 9期
- 期刊
Genomic instability underlies genesis and the development of various types of cancer. During tumorigenesis, cancer initiating cells assume a set of features, which allow them to survive and proliferate. Different mutations and chromosomal alterations promote a selection of the most aggressive cancer clones that worsen the prognosis of the disease. Despite that caspase-2 was described as a protease fulfilling an initiator and an effector function in apoptosis, it has recently been discovered to play an important role in the maintenance of genomic integrity and normal chromosome configuration. This protein is able to stabilize p53 and affect the level of transcription factors, which activates cell response to oxidative stress. Here we focus on the discussion on the mechanism(s) of how caspase-2 regulates genomic stability and decreases tumorigenesis.
...2.Long non-coding RNAs: A view to kill ovarian cancer
- 关键词:
- EPITHELIAL-MESENCHYMAL TRANSITION; PROMOTES CELL-PROLIFERATION; PREDICTS POOR-PROGNOSIS; WNT/BETA-CATENIN PATHWAY; CISPLATIN RESISTANCE; TARGETING MIR-330-5P; LNCRNA HOTAIR; INVASION; METASTASIS; PROGRESSION
- Zamaraev, Alexey, V;Volik, Pavel, I;Sukhikh, Gennady T.;Kopeina, Gelina S.;Zhivotovsky, Boris
- 《BIOCHIMICA ET BIOPHYSICA ACTA-REVIEWS ON CANCER》
- 2021年
- 1876卷
- 1期
- 期刊
An emerging role of long non-coding RNAs (lncRNAs) in tumor progression has been revealed in the last decade. Through interactions with nucleic acids and proteins, lncRNAs could act as enhancers, scaffolds or decoys for a number of oncoproteins and tumor suppressors. The aberrant lncRNA expression or mutations are often associated with changes in a variety of cellular processes, including proliferation, stress response and cell death. Here, we will focus on the tumor-associated lncRNAs in ovarian cancer according to their contribution to cancer hallmarks, such as intense proliferation, cell death resistance, altered energy metabolism, invasion and metastasis, and immune evasion. Moreover, the potential clinical implications of lncRNAs and their significance for the diagnosis, prognosis and therapy of ovarian cancer will be discussed.
...3.Simple and Efficient Protocol for Subcellular Fractionation of Normal and Apoptotic Cells
- 关键词:
- apoptosis; cytosol; nuclei; fractionation; translocation
- Senichkin, Viacheslav V.;Prokhorova, Evgeniia A.;Zhivotovsky, Boris;Kopeina, Gelina S.
- 《CELLS》
- 2021年
- 10卷
- 4期
- 期刊
Subcellular fractionation approaches remain an indispensable tool among a large number of biochemical methods to facilitate the study of specific intracellular events and characterization of protein functions. During apoptosis, the best-known form of programmed cell death, numerous proteins are translocated into and from the nucleus. Therefore, suitable biochemical techniques for the subcellular fractionation of apoptotic cells are required. However, apoptotic bodies and cell fragments might contaminate the fractions upon using the standard protocols. Here, we compared different nucleus/cytoplasm fractionation methods and selected the best-suited approach for the separation of nuclear and cytoplasmic contents. The described methodology is based on stepwise lysis of cells and washing of the resulting nuclei using non-ionic detergents, such as NP-40. Next, we validated this approach for fractionation of cells treated with various apoptotic stimuli. Finally, we demonstrated that nuclear fraction could be further subdivided into nucleosolic and insoluble subfractions, which is crucial for the isolation and functional studies of various proteins. Altogether, we developed a method for simple and efficient nucleus/cytoplasm fractionation of both normal and apoptotic cells.
...4.Bak and Bcl-xL Participate in Regulating Sensitivity of Solid Tumor Derived Cell Lines to Mcl-1 Inhibitors.
- 关键词:
- BH3-mimetics; Bcl-2 family proteins; Mcl-1; cancer therapy; sensitivity
- Senichkin, Viacheslav V;Pervushin, Nikolay V;Zamaraev, Alexey V;Sazonova, Elena V;Zuev, Anton P;Streletskaia, Alena Y;Prikazchikova, Tatiana A;Zatsepin, Timofei S;Kovaleva, Olga V;Tchevkina, Elena M;Zhivotovsky, Boris;Kopeina, Gelina S
- 《Cancers》
- 2021年
- 14卷
- 1期
- 期刊
BH3 mimetics represent a promising tool in cancer treatment. Recently, the drugs targeting the Mcl-1 protein progressed into clinical trials, and numerous studies are focused on the investigation of their activity in various preclinical models. We investigated two BH3 mimetics to Mcl-1, A1210477 and S63845, and found their different efficacies in on-target doses, despite the fact that both agents interacted with the target. Thus, S63845 induced apoptosis more effectively through a Bak-dependent mechanism. There was an increase in the level of Bcl-xL protein in cells with acquired resistance to Mcl-1 inhibition. Cell lines sensitive to S63845 demonstrated low expression of Bcl-xL. Tumor tissues from patients with lung adenocarcinoma were characterized by decreased Bcl-xL and increased Bak levels of both mRNA and proteins. Concomitant inhibition of Bcl-xL and Mcl-1 demonstrated dramatic cytotoxicity in six of seven studied cell lines. We proposed that co-targeting Bcl-xL and Mcl-1 might lead to a release of Bak, which cannot be neutralized by other anti-apoptotic proteins. Surprisingly, in Bak-knockout cells, inhibition of Mcl-1 and Bcl-xL still resulted in pronounced cell death, arguing against a sole role of Bak in the studied phenomenon. We demonstrate that Bak and Bcl-xL are co-factors for, respectively, sensitivity and resistance to Mcl-1 inhibition.
...5.Anastasis: Return Journey from Cell Death.
- 关键词:
- anastasis; apoptosis; mitochondria; stress; survival
- Zaitceva, Victoria;Kopeina, Gelina S;Zhivotovsky, Boris
- 《Cancers》
- 2021年
- 13卷
- 15期
- 期刊
For over 20 years, it has been a dogma that once the integrity of mitochondria is disrupted and proapoptotic proteins that are normally located in the intermembrane space of mitochondria appeared in the cytoplasm, the process of cell death becomes inevitable. However, it has been recently shown that upon removal of the death signal, even at the stage of disturbance in the mitochondria, cells can recover and continue to grow. This phenomenon was named anastasis. Here, we will critically discuss the present knowledge concerning the mechanisms of cell death reversal, or development of anastasis, methods for its detection, and what role signaling from different intracellular compartments plays in anastasis stimulation.
...6.Requirement for Serine-384 in Caspase-2 processing and activity
- 关键词:
- CELL-DEATH; APOPTOSIS; PHOSPHORYLATION; SPECIFICITY; ACTIVATION; SIDE
- Zamaraev, Alexey V.;Volik, Pavel I.;Nilov, Dmitry K.;Turkina, Maria V.;Egorshina, Aleksandra Yu.;Gorbunova, Anna S.;Iarovenko, Svetlana Iu.;Zhivotovsky, Boris;Kopeina, Gelina S.
- 《CELL DEATH & DISEASE》
- 2020年
- 11卷
- 10期
- 期刊
Caspase-2 is a unique and conservative cysteine protease which plays an important role in several cellular processes including apoptotic cell death. Although the molecular mechanisms of its activation remain largely unclear, a major role belongs to the architecture of the caspase-2 active center. We demonstrate that the substitution of the putative phosphorylation site of caspase-2, Serine-384 to Alanine, blocks caspase-2 processing and decreases its enzymatic activity. Strikingly, in silico analysis using molecular dynamics simulations has shown that Serine-384 is crucially involved in interactions within the caspase-2 active center. It stabilizes Arginine-378, which forms a crucial hydrogen bond with the aspartate residue of a substrate. Hence, Serine-384 is essential for supporting a proper architecture of the active center of caspase-2. Moreover, molecular modeling strongly proved steric inaccessibility of Ser-384 to be phosphorylated. Importantly, a multiple alignment has demonstrated that both Serine-384 and Arg-378 residues are highly conservative across all members of caspase family, which allows us to suggest that this diade is indispensable for caspase processing and activity. Spontaneous mutations in this diade might influence oncosuppressive function of caspases, in particular of caspase-2. Likewise, the mutation of Ser-384 is associated with the development of lung squamous cell carcinoma and adenocarcinoma. Taken together, we have uncovered a central feature of the caspase-2 activation mechanism which is crucial for the regulation of its signaling network.
...7.Programmed Cell Death: Historical Notes from Russia
- 关键词:
- CYTOCHROME-C; POLY(ADP-RIBOSE) POLYMERASE; MITOCHONDRIAL-MEMBRANE; DNA FRAGMENTATION; RADIATION; APOPTOSIS; ACTIVATION; INHIBITOR; RELEASE; PROTEIN
- Zhivotovsky, B.
- 《BIOCHEMISTRY-MOSCOW》
- 2020年
- 85卷
- 10期
- 期刊
The investigation of cell death mechanisms is one of the fastest growing areas of modern biomedicine. A particular interest in this research topic arose in 1972 after publication of an article by Kerr, Wyllie, and Currie, in which apoptosis, one of the types of cell death, was first considered as a basic biological phenomenon regulating tissue homeostasis. Several Russian groups involved in the investigation of the mechanisms of radiation-induced cell death have drawn attention to the similarity between these two mechanisms. Unfortunately, these studies have been for a long time inaccessible to the international scientific community. These introductory remarks attempt to restore the chain of events that have taken place during the past 50 years.
...8.Nutrient Deprivation Promotes MCL-1 Degradation in an Autophagy-Independent Manner
- 关键词:
- apoptosis; autophagy; Mcl-1; nutrient deprivation; adenocarcinoma;CALORIC RESTRICTION; PROTEINS; CLEAVAGE; CANCER; CELLS; APOPTOSIS; LC3
- Pervushin, N. V.;Senichkin, V. V.;Kapusta, A. A.;Gorbunova, A. S.;Kaminskyy, V. O.;Zhivotovsky, B.;Kopeina, G. S.
- 《BIOCHEMISTRY-MOSCOW》
- 2020年
- 85卷
- 10期
- 期刊
The antiapoptotic protein Mcl-1, which is an attractive target for cancer treatment, is degraded under nutrient deprivation conditions in different types of cancer. This process sensitizes cancer cells to chemotherapy. It has been found that nutrient deprivation leads to suppression of Mcl-1 synthesis; however, the mechanisms of Mcl-1 degradation under such conditions remain to be elucidated. In this study, we have investigated the contribution of autophagy and proteasomal degradation to the regulation of the level of Mcl-1 protein under nutrient deprivation conditions. We found that these circumstances cause a decrease in the level of Mcl-1 in cancer cells in a macroautophagy-independent manner via proteasomal degradation.
...9.Viral Infections:Negative Regulators of Apoptosis and Oncogenic Factors
- 关键词:
- EPSTEIN-BARR-VIRUS; NF-KAPPA-B; SARCOMA-ASSOCIATED HERPESVIRUS; HUMAN-PAPILLOMAVIRUS TYPE-16; CELL-DEATH; MEDIATED APOPTOSIS; TUMOR-SUPPRESSOR; LARGE-T; PROTEIN; P53
- Zamaraev, A. V.;Zhivotovsky, B.;Kopeina, G. S.
- 《BIOCHEMISTRY-MOSCOW》
- 2020年
- 85卷
- 10期
- 期刊
The disruption of apoptotic cell death process is closely associated with the etiology of various diseases, including cancer. Permanent viral infections can cause different types of cancers. Oncogenic viruses manipulate both external and internal apoptosis pathways, and inhibit the activity of proapoptotic proteins and signaling pathways, which facilitates carcinogenesis. Ineffective immune surveillance or immune response suppression can induce uncontrolled virus propagation and host cell proliferation. In this review, we discuss current data that provide insights into mechanisms of apoptotic death suppression by viruses and their role in oncogenesis.
...10.Isolation of High-Molecular-Weight Activation Complexes of Initiator Caspases in DNA Damage
- 关键词:
- apoptosis; initiator caspase; DNA damage; cisplatin;APOPTOSIS; REGULATOR; PIDDOSOME; CLEAVAGE
- Zamaraev, A., V;Egorshina, A. Yu;Lavrik, I. N.;Zhivotovsky, B. D.;Kopeina, G. S.
- 《BULLETIN OF EXPERIMENTAL BIOLOGY AND MEDICINE》
- 2019年
- 168卷
- 1期
- 期刊
Initiation of apoptosis by chemotherapeutic drugs is one of the most effective approaches to the treatment of cancers. Caspases, the main enzymes of apoptosis, undergo activation to initiate cell death. Activation of initiator caspases requires their binding to special protein complexes. For elucidation of the mechanisms of apoptosis, these complexes should be isolated. However, their purification is challenging because they are formed in the cell in negligible amounts and rapidly degrade. We have developed an effective way to isolate caspase activation complexes formed in tumor cells in response to DNA damage. The method is based on combination of gel filtration with immunoprecipitation. The first stage is aimed at the separation of the high-molecular-weight caspase activation complexes and their monomeric forms, which allows increasing the efficiency of isolation of complexes at the second stage.
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