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1. Heat stress stimulates colon cancer cells to secret specific population of extracellular nanovesicles enriched by HSP70 and microRNAs

Author

I. V. Nazarova, L. M. Zabegina, N. S. Nikiforova, M. A. Slusarenko, E. I. Sidina, A. V. Zhakhov, A. M. Ishchenko, B. A. Margulis, I. V. Guzhova, and A. V. Malek

Subjects
extracellular nanovesicles, colorectal cancer, heat stress, microrna, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Background. Heat stress (HS) induces the cellular secretion of heat shock proteins (HSP ) and extracellular nanovesicles (ENVs). The biological link between these phenomena is poorly understood. In the case of colorectal cancer (CRC) cells, the secretion of HSP s and ENV may be involved in the clinical response to intraperitoneal therapy of peritoneal carcinomatosis.Material and Methods. Established colon cancer cell lines COLO 320, HCT 116, HT29 and DLD 1 were used. ENVs were isolated from culture media by differential ultra-centrifugation and analyzed by dynamic light scattering, nanoparticle tracking analysis, atomic force microscopy and flow cytometry. Super-paramagnetic particles (SPMP ) covered by antibodies to the membrane form of Hsp70 were used for isolation and quantification of Hsp70(+) ENVs. Vesicular microRNA was assayed by RT-qPC R.Results. HS induces the secretion of ENVs by CRC cells, the resistance to HS correlates with the activity of HS-induced ENVs secretion. HS induces the secretion of a specific population of ENVs enriched by membrane form Hsp70 (mHsp70). The microRNA content of mHsp70(+) ENVs has qualitative and quantitative features. The concentration of miR-126-3p, -181-5p, -155-5p, -223 is increased in mHSP 70(+) ENVs secreted by three CRC cell lines.Conclusion. HS induces the secretion of mHSP 70(+) ENVs by CRC cells. This phenomenon may be involved in a clinical response to intraperitoneal chemo-hyperthermic perfusion therapy of peritoneal carcinomatosis.

Published
2022
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4. Динамика функциональной активности и экспрессии субъединиц протеасом в условиях адаптации клетки к тепловому шоку

Author

A. V. Morozov, Vadim L. Karpov, A. V. Burov, B A Margulis, Daria S. Spasskaya, and T. M. Astakhova

Subjects
Messenger RNA, U937 cell, Cellular adaptation, medicine.diagnostic_test, Chemistry, Proteolysis, Cell, General Medicine, Cell biology, medicine.anatomical_structure, Proteasome, medicine, Gene, Homeostasis
Abstract

The ubiquitin-proteasome system (UPS) performs proteolysis of most intracellular proteins. The key components of the UPS are the proteasomes, multi-subunit protein complexes, playing an important role in cellular adaptation to various types of stress. We analyzed the dynamics of the proteasome activity, the content of proteasome subunits, and the expression levels of genes encoding catalytic subunits of proteasomes in the human histiocytic lymphoma U937 cell line immediately, 2, 4, 6, 9, 24, and 48 h after a heat shock (HS). The initial decrease (up to 62%) in the proteasome activity in cellular lysates was revealed, then 10 h after HS the activity began to recover. The amount of proteasomal α-subunits in the cells decreased 2 h after HS, and was restored to 24-48 h after HS. Fluctuations in the levels of mRNAs encoding proteasome catalytic subunits with the maximum expression 2 h after HS and a gradual decrease to 48 h after HS were observed. The average estimated number of mRNA copies per cell ranged from 10 for weakly to 150 for highly expressed proteasome genes. Thus, the recovery efficiency of UPS functionality after HS, which reflects the important role of proteasomes in maintaining cell homeostasis, was evaluated.

Published
2019
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5. [Dynamics of the Functional Activity and Expression of Proteasome Subunits during Cellular Adaptation to Heat Shock]

Author

A V, Morozov, A V, Burov, T M, Astakhova, D S, Spasskaya, B A, Margulis, and V L, Karpov

Subjects
Proteasome Endopeptidase Complex, Protein Subunits, Ubiquitin, Proteolysis, Humans, U937 Cells, Heat-Shock Response
Abstract

The ubiquitin-proteasome system (UPS) performs proteolysis of most intracellular proteins. The key components of the UPS are the proteasomes, multi-subunit protein complexes, playing an important role in cellular adaptation to various types of stress. We analyzed the dynamics of the proteasome activity, the content of proteasome subunits, and the expression levels of genes encoding catalytic subunits of proteasomes in the human histiocytic lymphoma U937 cell line immediately, 2, 4, 6, 9, 24, and 48 h after a heat shock (HS). The initial decrease (up to 62%) in the proteasome activity in cellular lysates was revealed, then 10 h after HS the activity began to recover. The amount of proteasomal α-subunits in the cells decreased 2 h after HS, and was restored to 24-48 h after HS. Fluctuations in the levels of mRNAs encoding proteasome catalytic subunits with the maximum expression 2 h after HS and a gradual decrease to 48 h after HS were observed. The average estimated number of mRNA copies per cell ranged from 10 for weakly to 150 for highly expressed proteasome genes. Thus, the recovery efficiency of UPS functionality after HS, which reflects the important role of proteasomes in maintaining cell homeostasis, was evaluated.

Published
2018

6. CLIN-IMMUNOTHERAPY/BIOLOGIC THERAPIES

Author

I. F. Pollack, R. I. Jakacki, L. Butterfield, H. Okada, Y. Chiba, N. Hashimoto, N. Kagawa, M. Kinoshita, N. Kijima, R. Hirayama, Y. Oji, A. Tsuboi, Y. Oka, H. Sugiyama, T. Yoshimine, R. D. Valle, S. Tejada, S. Inoges, M. A. Idoate, A. L. D. de Cerio, J. Espinos, J. Aristu, J. Gallego, J. P. Calvo, M. Bendandi, J. Zhu, C. Chen, A. Ravelo, E. Yu, R. Dhanda, I. D. Schnadig, L. Zhang, H. Fan, I. Zhang, X. Chen, H. Wang, A. Da Fonseca, B. Badie, L. H. Butterfield, R. L. Hamilton, A. H. Mintz, J. A. Engh, J. Drappatz, M. O. Lively, M. D. Chan, A. M. Salazar, D. M. Potter, E. G. Shaw, F. S. Lieberman, J. Wei, L.-Y. Kong, F. Wang, S. Xu, T. A. Doucette, S. D. Ferguson, Y. Yang, K. McEnery, K. Jethwa, O. Gjyshi, W. Qiao, F. F. Lang, G. Rao, G. N. Fuller, G. A. Calin, A. B. Heimberger, S. Yang, G. E. Archer, H. Miao, X. Cui, W. Xie, D. Snyder, A. J. Pretorian, A. Dechkovskaia, E. Reap, L. A. S. Perez, P. Norberg, R. Schmittling, D. A. Mitchell, J. H. Sampson, F. Lang, G. Calin, D. G. Walker, T. Crough, L. Beagley, C. Smith, L. Jones, R. Khanna, Y. Kanemura, M. Sumida, E. Yoshioka, A. Yamamoto, D. Kanematsu, Y. Matsumoto, H. Fukusumi, A. Takada, M. Nonaka, S. Nakajima, K. Mori, S. Goto, T. Kamigaki, R. Maekawa, T. Shofuda, S. Moriuchi, M. Yamasaki, J. T. Yeung, R. Hamilton, R. Jakacki, I. Pollack, S. Pellegatta, M. Eoli, C. Antozzi, S. Frigerio, M. G. Bruzzone, L. Cuppini, S. Nava, E. Anghileri, G. Cantini, E. Prodi, E. Ciusani, P. Ferroli, M. Saini, G. Broggi, R. Mantegazza, E. A. Parati, G. Finocchiaro, M. Hegde, A. Corder, K. K. Chow, M. Mukherjee, V. S. Brawley, H. E. Heslop, S. Gottschalk, E. Yvon, N. Ahmed, D. M. Gibo, W. Debinski, J. Bonomo, J. Rossmeisl, J. Robertson, P. Dickinson, M. E. Salacz, P. J. Camarata, M. Ots, J. McIntire, D. Lovick, G. Archer, D. Bigner, H. Friedman, D. Lally-Goss, B. Perry, J. Herndon, S. McGehee, R. McLendon, R. E. Coleman, J. Sampson, Z. Grada, T. Byrd, D. R. Shaffer, A. Ghazi, K. Schonfeld, G. Dotti, H. Heslop, W. Wels, M. L. Baker, J. M. Robbins, P. J. Dickinson, D. York, B. K. Sturges, B. Martin, R. J. Higgins, J. Bringas, K. Bankiewicz, H. E. Gruber, D. J. Jolly, A. Narayana, M. Mathew, R. Kannan, K. Madden, J. Golfinos, E. Parker, P. Ott, A. Pavlick, D. A. Bota, C. Pretto, P. Hantos, F. M. Hofman, T. C. Chen, J. A. Carrillo, V. E. Schijns, A. A. Stathopoulos, R. M. Prins, R. Everson, H. Soto, D. N. Lisiero, E. Young, L. M. Liau, A. Friedman, D. D. Bigner, D. Boczkowski, S. G. Gururangan, G. Grant, T. Driscoll, J. King, S. Nair, H. Fuchs, J. Kurtzberg, M. A. Shevtsov, A. V. Pozdnyakov, A. V. Kim, K. A. Samochernych, I. V. Guzhova, I. V. Romanova, B. A. Margulis, and W. A. Khachatryan

Subjects
Abstracts, Cancer Research, Oncology, business.industry, medicine.medical_treatment, Biologic therapies, Medicine, Neurology (clinical), Immunotherapy, Bioinformatics, business
Published
2012
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8. Heat-Shock Protein (Hsp70) Protects Glutamatergic Synaptic Transmission in Cells of the Rat Olfactory Cortex against Acute Anoxia in Vitro

Author

A. A. Mokrushin, B. A. Margulis, L. I. Pavlinova, and Irina V. Guzhova

Subjects
Male, Olfactory system, General Immunology and Microbiology, Chemistry, Glutamic Acid, Olfactory Pathways, General Medicine, Neurotransmission, Synaptic Transmission, Cell Hypoxia, General Biochemistry, Genetics and Molecular Biology, In vitro, Rats, Hsp70, Glutamatergic, Synaptic fatigue, Biochemistry, Heat shock protein, Synaptic augmentation, Animals, Cattle, HSP70 Heat-Shock Proteins, Rats, Wistar, General Agricultural and Biological Sciences, Neuroscience
Published
2004
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9. Accumulation of major stress protein 70kDa protects myeloid and lymphoid cells from death by apoptosis

Author

E. B. Lasunskaia, I. I. Fridlianskaia, I. V. Guzhova, V. M. Bozhkov, and B. A. Margulis

Subjects
Pharmacology, Cancer Research, Myeloid, Biochemistry (medical), Clinical Biochemistry, Cell, Pharmaceutical Science, Cell Biology, Biology, Jurkat cells, Hsp70, Cell biology, medicine.anatomical_structure, Cell culture, Apoptosis, Heat shock protein, medicine, Cancer research, Cytotoxic T cell
Abstract

The major heat shock protein, hsp70, is known to contribute to the mechanisms of cell protection against a variety of stress and cytotoxic factors, providing an increase of cell survival. Whether hsp70 could be implicated in the rescue of cells from stress-induced death proceeding on apoptotic pathway is not well established. Here we report that susceptibility of myeloid and lymphoid cell lines to apoptosis induced by heat shock or ethanol coincides with hsp70 content and can be modulated by changes in expression of this protein. Cells of lymphoid and myeloid lines differing in basal and inducible level of the protein were tested. The cells containing higher amounts of hsp70 (U937, Jurkat, Molt4) were more resistant to the apoptosis-inducing stimuli then cells which accumu-late lower amounts of the protein (HL60) and especially those lacking the protein (NSO). Inhibition of hsp70 accumulation by quercetin made cells more susceptible to the same apoptotic inducer. Enhancement of hsp70 expression by previous heating or by liposomal delivery of the exogenic protein to the cells lacking hsp70 made them more resistant to apoptosis. The possible mechanisms of the hsp70 protective effect in apoptosis are discussed.

Published
1997
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10. [Biodistribution of the recombinant heat shock protein rhHsp70 in intracranial C6 glioma models in Wistar rats and subcutaneos B16/F10 melanoma in C57BL/6 mice]

Author

M A, Shevtsov, S V, Shatik, Tokarev, M I, Mostova, L A, Tiutin, N V, Bychkova, A L, Mikhrina, K V, Onokhin, D A, Meshalkina, I V, Romanova, O N, Savchenko, A A, Ivanova, S V, Abkin, V A, Kharatian, I V, Guzhova, and B A, Margulis

Subjects
Male, Tomography, Emission-Computed, Single-Photon, Skin Neoplasms, Time Factors, Brain Neoplasms, Melanoma, Experimental, Glioma, Neoplasms, Experimental, Injections, Intralesional, Rats, Iodine Radioisotopes, Mice, Inbred C57BL, Mice, Liver, Injections, Intravenous, Animals, HSP70 Heat-Shock Proteins, Tissue Distribution, Rats, Wistar, Fluorescent Dyes
Abstract

For the first time, the biodistribution of recombinant heat shock protein in rhHsp70 rats with grafted intracranial C6 glioma was evaluated. It was assessed using the fluorescent antibody accumulation chaperone rhHsp70 conjugated with fluorochrome Alexa Fluor 555 in tumor cells by intratumoral or intravenous administration. Assessment of the distribution and accumulation of labeled protein was carried out on the model of subcutaneous B16/F10 melanoma in C57BL/6 mice with the use of single-photon emission computer tomography. After 60 minutes after intravenous administration rhHsp70-I123 (20 MBq, 5 mg chaperone) accumulation of the drug mainly in the liver and tumor tissue was showed. The coefficient of the differential accumulation of the labeled protein KDN(tumor/background) was 3.14. It was turned out that comparing the level of fixation of rhHsp70-I123 in the liver and the tumor KDN(tumor/ liver) = 0.76. After 24 hours from the time of injection of rhHsp70-I123 it was observed increase the level of fixation of the labeled protein in the liver and melanoma: KDN(tumor/background) = 3.43; KDN(tumor/liver = 0.78.

Published
2013

11. [Chaperone therapy in the rat model of intracranial glioblastoma]

Author

M A, Shevtsov, V A, Kharatrian, A V, Pozdniakov, I V, Romanova, I V, Guzhova, and B A, Margulis

Subjects
Infusions, Intralesional, Brain Neoplasms, T-Lymphocytes, Antineoplastic Agents, Adaptive Immunity, Survival Analysis, Immunity, Innate, Recombinant Proteins, Rats, Killer Cells, Natural, Disease Models, Animal, Interferon-gamma, Adjuvants, Immunologic, Tumor Cells, Cultured, Animals, HSP70 Heat-Shock Proteins, Rats, Wistar, Glioblastoma
Abstract

Molecular chaperons can effectively activate innate and adaptive anti-tumor immune response. In the model of intracranial glioma C6 in Wistar rats we assessed immunomodulatory activity of recombinant protein Hsp70 in case of local, intratumoral injection. Single intratumoral infusion of chaperone had led to dramatic delay in tumor volume growth (on MRI of rat brain), which was accompanied by increase in survival rates. Incubation of rat spleenocytes with C6 cells elevated the levels of INF-gamma, that shows an immunologically specific T-cell response. With immunohistochemical assay we observed a marked infiltration of the tumor by T-lymphocytes and NK-cells. Thus, purified Hsp70 can efficiently induce innate and adaptive anti-tumor response and could be used as adjuvant in treatment of malignant brain tumors of central nervous system.

Published
2013

12. [Untitled]

Author

I. A. Gerasimova, A. V. V’yushina, S. G. Pivina, B. A. Margulis, I. V. Guzhova, Natalia Ordyan, and M. A. Flerov

Subjects
Adaptive behavior, business.industry, Immunology, food and beverages, Physiology, Medicine, General Medicine, business, General Biochemistry, Genetics and Molecular Biology, Hsp70
Abstract

We studied whether intranasal treatment with HSP70 can be used for the correction of maladaptive behavior in rats after unavoidable stress. After 3 intranasal injection of HSP70 in a dose of 3.25 μg we observed normalization of adaptive behavior after unavoidable stress and improvement of physiological reserves of the organism.

Published
2003
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13. [Novel compounds increasing chaperone Hsp70 expression and their biological activity]

Author

E M, Eremenko, O I, Antimonova, O G, Shekalova, S G, Polonik, B A, Margulis, and I V, Guzhova

Subjects
Dose-Response Relationship, Drug, Lithospermum, Protein Biosynthesis, Sea Urchins, Drug Evaluation, Preclinical, Animals, Humans, HSP70 Heat-Shock Proteins, K562 Cells, Drugs, Chinese Herbal, Naphthoquinones
Abstract

Hsp70 possesses chaperonic activity, the property associated with the protective function that was demonstrated in experiments on a great number of cell and animal models. Therefore, it seems important to search for the substances able to innocuously elevate the chaperone concentration in an organism cells and tissues. In our work, we screened of more that 60 compounds and found two chemicals, derivatives of shikonin and echinochrome that able to increase the chaperone level in a variety of human cells. It was shown that in human erythroleukemia K562 cells treated with the both substances concomitantly with elevation of Hsp70 level the absolute chaperonic activity was also increased; this can indicate mobilization of the whole cellular chaperonic machinery by above mentioned compounds. Estimating biological activity of the two substances, we demonstrated that treatments of cells by them prior to hard heat stress, hydrogen peroxide or staurosporine reduced cell mortality by 20-50 % depending on a cytotoxic factor. The results show that after simple chemical modifications these compounds might be taken as a basis of pharmaceuticals for therapy of wide range of disorders.

Published
2010

15. [The role of extracellular chaperone Hsp70 in creating antitumor immunity in rat rhabdomyosarcoma RA-2 model]

Author

I V, Guzhova, E Iu, Komarova, A A, Pimenova, Iu B, Bakhtin, E V, Kaminskaia, and B A, Margulis

Subjects
Male, Disease Models, Animal, Rhabdomyosarcoma, Animals, Female, HSP70 Heat-Shock Proteins, Cancer Vaccines, Rats
Abstract

Immunization of experimental animals with extract or membranes of rat rhabdomyosarcoma RA-2 in combination with pure Hsp70 did not offer any significant effect of protection from subsequent RA-2 cells-stimulated tumor growth. By contrast, immunization with preparations of pure Hsp70 led to a significant decrease in number and size of tumors as well as elevation of concentrations of antibodies against RA-2 cells. Also, enhanced blood levels of Hsp70 involved delayed tumor growth. In vitro tests Hsp70 incubation with RA-2 cells was followed by a 30-35% rise in cytotoxic lymphocytes levels. An ability of pure Hsp70 preparations to stimulate humoral and antitumor response was demonstrated. Hence, they may be used in developing vaccine formulas.

Published
2008

16. [Molecular chaperone Hsp70 protects neuroblastoma SK-N-SH cells from hypoxic stress]

Author

N S, Tikhonova, O S, Moskaleva, B A, Margulis, and I V, Guzhova

Subjects
Cell Line, Tumor, Humans, HSP70 Heat-Shock Proteins, Cobalt, Hypoxia, Hypoxia-Inducible Factor 1, alpha Subunit, Recombinant Proteins, Signal Transduction
Abstract

HIF-1alpha is synthesized constutively, however under normoxia it is specifically degraded. Hypoxia blocks the factor degradation, and it activates the transcription of genes whose products control multiple cellular processes. Hsp70 molecular chaperone is known to protect neural cells from the deleterious effects of hypoxic stress, though the mechanism of this action remains elusive. To understand how Hsp70 protects cells affected by hard hypoxia the model cell line was constructed based on human neuroblastoma SK-N-SH cells and over-expressing the chaperone when treated by zinc salt. The cells were shown to be resistant to the treatment by CoCl2 imitating in the experiments the reaction to hypoxia. Life span of HIF-1alpha was elevated in these cells as compared with parental line due to the fact that Hsp70 formed long-time complex with HIF-1alpha. The data show that Hsp70 interferes with signaling pathways of cellular response to hypoxic stress at the level of regulation of HIF-1alpha stability.

Published
2008

17. [HSC70 protein of human blood mononuclears as a sign of adaptation under normobaric hypoxia training]

Author

A A, Boĭkova, L I, Andreeva, and B A, Margulis

Subjects
Adult, Male, HSC70 Heat-Shock Proteins, Leukocytes, Mononuclear, Humans, Protein Isoforms, Female, Anaerobiosis, Adaptation, Physiological, Exercise, Biomarkers
Abstract

We investigated two isoforms of heat shock protein 70 kDa: HSP70 and HSC70, in the human blood mononuclears under normobaric hypoxia training. It was shown that hypoxia regimen does not lead to manifestation of stress but exerts activation of the organism. The obtained organism adaptation is achieved with a little cost that is confirmed by absence of HSP70 content increase. HSC70 content in the blood mononuclears was increased in most case up to 1.5-2.0 fold. HSC70 displays itself as a sign of adaptation. We connect the increase of HSC70 with mitochondria biogenesis which is given a leading importance under adaptation of aerobic organism cells to hypoxia.

Published
2007

18. [The balance between Hsp70 and its cochaperones Hdj1 and Bag1 determines its substrate-binding activity]

Author

S S, Novoselov, T V, Novoselova, M V, Verbova, B A, Margulis, and I V, Guzhova

Subjects
Hot Temperature, Time Factors, Blotting, Western, Enzyme-Linked Immunosorbent Assay, HSP40 Heat-Shock Proteins, Culture Media, DNA-Binding Proteins, Adenosine Triphosphate, Humans, HSP70 Heat-Shock Proteins, K562 Cells, Cells, Cultured, Protein Binding, Transcription Factors
Abstract

Heat shock protein Hsp70 presents one of the most effective cell protective systems. Its protective activity is mostly due to the fact that Hsp70 is able to restore native conformation of newly synthesized or damaged proteins. Two other proteins. Hdj and Bag 1, are involved in the process, allowing Hsp70 to perform binding-release cyclec of target proteins. The aim of this study was to investigate interactions between cochaperones Hdj 1 and Bag 1, and the major cell chaperone Hsp in vitro. The accumulation of Hsp70 and Hdj 1 in human erythroleukemia K562 cells was stimulated by heat stress (43 degrees C, 60 min). Cells were collected at certain time periods after heat stress, and amounts of cell chaperones were measured using Western blotting and ELISA assay. The level of Hsp70 chaperone activity in cell extracts was estimated using original technique. The effects of exogenous cochaperones and of their parts on this activity were also investigated. The results of the study indicate that Hsp70 chaperone activity is regulated by the level of its cochaperones, especially Hdj 1. At the same time the amount of ATP appears to be critical for functional activity of Hsp70. Hdj 1 and Bag 1 peptides, which bind to Hsp70 with high affinity, are able to significally reduce its chaperone activity. This finding confirms the possibility of using peptide approach for regulation of Hsp70 function at the cellular and organismal levels.

Published
2006

19. [Hsp70 chaperone and the prospects of its application in anticancer therapy]

Author

I V, Guzhova, S S, Novoselov, and B A, Margulis

Subjects
Models, Molecular, Immunity, Cellular, T-Lymphocytes, Apoptosis, HSP40 Heat-Shock Proteins, Cancer Vaccines, Protein Structure, Tertiary, DNA-Binding Proteins, Killer Cells, Natural, Eukaryotic Cells, Antigens, Neoplasm, Neoplasms, Animals, Humans, Immunologic Factors, HSP70 Heat-Shock Proteins, Signal Transduction, Transcription Factors
Abstract

Major stress protein Hsp70 is known to possess two important properties: ATP-dependent activity and protective activity; these two are thought to play a significant role in anticancer therapy. Many malignant tumors contain high amounts of intracellular Hsp70. Moreover, many anticancer drugs themselves are able to elevate Hsp70 expression in tumor cells. Since Hsp70 was found to disturb many signal pathways of apoptosis in many points, the high chaperone expression may lead to an increased resistance of tumor cells to anticancer drugs. On the other hand, when overexpressed by a certain mechanism, Hsp70 is able to emerge at the cell surface by itself or together with tumor antigens and present these to immune cells T-lymphocytes and natural killers, in such a manner that makes cancer cell recognized and abolished. These properties make Hsp70 very promising instrument in designing some novel anticancer vaccines.

Published
2006

20. [Dynamics of chaperone complex Hdj1-Hsp70-Bag1 as a response of erythroleukemia K562 cells to heat stress]

Author

S S, Novoselov, T V, Novoselova, O S, Moskaleva, B A, Margulis, and I V, Guzhova

Subjects
DNA-Binding Proteins, Hot Temperature, Time Factors, Chaperonins, Humans, Membrane Proteins, HSP70 Heat-Shock Proteins, HSP40 Heat-Shock Proteins, K562 Cells, Heat-Shock Proteins, Protein Binding, Transcription Factors
Abstract

Heat shock protein Hsp70 is known to play an important role in cell protection against a variety of harmful factors. This property, at least in part, is due to Hsp70 ability to restore the native conformation of newly synthetized or damaged proteins. In this activity Hsp70 is accompanied by two proteins, Hdj1 and Bag1, that enable Hsp70 to peform cycles of binding-release of target proteins. The aim of this study was to investigate interactions of Hdj1 and Bag1 co-chaperones with Hsp70 in vivo. The accumulation of Hsp70 was stimulated by heat stress, and later, at certain periods following the stress, cell probes were collected for biochemical and microscopic analysis. The data of Western blotting showed that within 24 h after heat shock amounts of Hsp70 and Hdj1 raised to remain at the elevated level for nearly 48 h. Several time points within this period were chosen for analysis of the complexes between Hsp70 and co-chaperones. The data of reciprocal immunoprecipitation/immunoblotting and confocal microscopy showed that Hsp70-Hdj1 complexes were detected primarily at early stage after heat shock, then Hsp70 was preferably bound to Bag1. The dynamics of chaperone complex formation and changes in their intracellular localization are discussed in terms of cell reaction to stress.

Published
2004

21. [The role of Hsp70 chaperone in the reaction of human leukemic cells to anticancer drugs]

Author

E Iu, Komarova, B A, Margulis, and I V, Guzhova

Subjects
Caspase 7, Antibiotics, Antineoplastic, Hot Temperature, Caspase 3, Doxorubicin, Cell Line, Tumor, Humans, Apoptosis, HSP70 Heat-Shock Proteins, Transfection, Antineoplastic Agents, Phytogenic, Caspase Inhibitors, Etoposide
Abstract

Most of anti-tumor factors are designed to kill selectively cancer cells; in most cases this action is related to the ability of the above substances to induce apoptosis. One of potent anti-apoptotic mechanisms is based on Hsp70 protein. Since the level of this protein is often higher in malignant tumors than in normal tissues, the aim of this study was to establish whether the elevated Hsp70 content may influence the process of apoptosis induced by anti-tumor drugs in cancer cells population. The increase of intracellular content of Hsp70 in human leukemia U-937 cells was attained by a mild heat stress or by transfection of cells with the human hsp70 gene. The elevation of Hsp70 quantity, irrespective of the way it was performed, leads to the inhibition of apoptosis in cells treated with two substances, etoposide or adriamycin. The inhibition of apoptosis was accompanied with the reducing of the share of cells with fragmented nuclei and with the delay in caspase activation. It is suggested that in addition to the previously discovered targets, whose activity is suppressed by the Hsp70 chaperone, this protein can inhibit the activity of caspase-3 and -7; this delays the onset of apoptosis in part of a cancer cell population.

Published
2004

22. Effects of exogenous heat shock protein (Hsp70) on glutaminergic synaptic transmission in rat olfactory cortex in vitro

Author

A. A. Mokrushin, Irina V. Guzhova, L. I. Pavlinova, and B. A. Margulis

Subjects
Olfactory system, Male, N-Methylaspartate, Presynaptic Terminals, Neurotransmission, Biology, Synaptic Transmission, General Biochemistry, Genetics and Molecular Biology, Heat shock protein, Excitatory Amino Acid Agonists, Animals, HSP70 Heat-Shock Proteins, Rats, Wistar, alpha-Amino-3-hydroxy-5-methyl-4-isoxazolepropionic Acid, Neurons, General Immunology and Microbiology, Dose-Response Relationship, Drug, Excitatory Postsynaptic Potentials, General Medicine, Olfactory Pathways, In vitro, Cell biology, Hsp70, Rats, Biochemistry, Receptors, Glutamate, Cattle, General Agricultural and Biological Sciences
Published
2004

23. [Accumulation of heat-shock proteins 70 in insect fat bodies as evidence of stress in Microsporidia-infected insects]

Author

K V, Seleznev, A V, Kinev, and B A, Margulis

Subjects
Gryllidae, Juvenile Hormones, Corpora Allata, Hemolymph, Fat Body, Microsporidia, Animals, HSP70 Heat-Shock Proteins, Chromatography, Affinity, Host-Parasite Interactions
Abstract

At present a concept prevails that pathological alterations in insect hosts infected with microsporidia, and those associated with hormone imbalance may be explained by the production of juvenile hormone-like (JH) substances by microsporidia. According to another view point, this pathology is a consequence of the host response. We suggested that the microsporidian infection can provoke a stress reaction in insects, which may cause JH secretion by these insects. To confirm this hypothesis, we have analysed major stress protein Hsp70 levels in the infected insects. Using affinity chromatography on ATP-agarose and immunoblotting, we have shown that Hsp70 was accumulated in infected crickets, and that it was the host protein. The consequence of events accompanying the infection in the insects is discussed in relation to the response of hormonal system of the host organism.

Published
2004

24. [Effect of EGF on the intracellular distribution of heat-shock proteins in A431 cells]

Author

A L, Evdonin, N V, Tsupkina, B A, Margulis, and N D, Medvedeva

Subjects
Cell Nucleus, Cytoplasm, Hot Temperature, Time Factors, Epidermal Growth Factor, Antibodies, Monoclonal, Fluorescent Antibody Technique, HSP40 Heat-Shock Proteins, Protein-Tyrosine Kinases, Tyrphostins, Pyrrolidinones, ErbB Receptors, Cell Line, Tumor, Type C Phospholipases, Carcinoma, Squamous Cell, Quinazolines, Humans, HSP70 Heat-Shock Proteins, Enzyme Inhibitors, Estrenes, Phosphorylation, Vanadates, Heat-Shock Proteins
Abstract

The intracellular distribution of hsp70 and hdj1 was studied using immunofluorescent method. In nonstimulated cells hsp70 and hdj1 were observed in the cytoplasm of A431 cells. When 100 ng/ml EGF was added for 15 min, both hsp70 and hdj1 were accumulated in the nuclei. Later on (up to 1 h) hsp70 was exported from the nuclei to be observed mainly in the cytoplasm, whereas hdj1 remained in the nuclei. In cells exposed to tyrphostin AG1478, this inhibitor of tyrosine kinase activity of EGF receptor prevented EGF-dependent accumulation of hsp70 and hdj1 in the nuclei. U73122, an inhibitor of phospholipase C activity, induced tyrosine phosphorylation of EGF receptor without EGF stimulation. In cells treated with U73122, both hsp70 and hdj1 were detected in the nuclei of non-stimulated cells. It is concluded that the intracellular distribution of heat shock proteins in A431 cells depends on tyrosine kinase activity of EGF receptor. Here we report for the first time the influence of EGF on the intracellular redistribution of heat shock proteins.

Published
2004

25. [Expression of Hsp70 and Hdj1 chaperone proteins in human tumor cells]

Author

S S, Novoselov, M V, Verbova, E V, Vasil'eva, N K, Vorob'ëva, B A, Margulis, and I V, Guzhova

Subjects
Ovarian Neoplasms, Breast Neoplasms, HSP40 Heat-Shock Proteins, Prognosis, Endometrial Neoplasms, Gene Expression Regulation, Neoplastic, Immunoenzyme Techniques, Predictive Value of Tests, Biomarkers, Tumor, Humans, Female, HSP70 Heat-Shock Proteins, Heat-Shock Proteins, Molecular Chaperones
Abstract

Heat shock proteins (Hsp), or "stress proteins", play an important role in maintenance of cellular homeostasis both under normal conditions and during cellular stress. We tested malignant female urogenital and breast tumors for Hsp70 and Hdj1 (Hsp40) chaperones. Immunoenzyme procedure (based on Hsp70 and ATP interaction) was used to assay Hsp70 levels. Hsp70 and Hdj1 expression was higher in malignant cells than in benign ones. We were the first to demonstrate the feasibility of using Hdj1 expression as a novel prognostic factor for neoplastic disease.

Published
2004

26. Exogenous heat shock protein with a molecular weight of 70 kDa changes behavior in white rats

Author

L. I. Andreeva, B. A. Margulis, and P. D. Shabanov

Subjects
Male, General Immunology and Microbiology, Behavior, Animal, General Medicine, Biology, Grooming, General Biochemistry, Genetics and Molecular Biology, Cell biology, Rats, White (mutation), Heat shock protein, Animals, HSP70 Heat-Shock Proteins, Rats, Wistar, General Agricultural and Biological Sciences, Administration, Intranasal
Published
2004

27. The use of HSP70 for prevention of consequences of unavoidable stress in rats

Author

M A, Flerov, N E, Ordyan, B A, Margulis, I V, Guzhova, A V, V'yushina, S G, Pivina, and I A, Gerasimova

Subjects
Male, Behavior, Animal, Helplessness, Learned, Animals, HSP70 Heat-Shock Proteins, Rats, Wistar, Administration, Intranasal, Electric Stimulation, Stress, Psychological, Rats
Abstract

We studied whether intranasal treatment with HSP70 can be used for the correction of maladaptive behavior in rats after unavoidable stress. After 3 intranasal injection of HSP70 in a dose of 3.25 microg we observed normalization of adaptive behavior after unavoidable stress and improvement of physiological reserves of the organism.

Published
2002

28. [Adaptation to hyperthermia and changes in peripheral blood leukocytes in humans]

Author

L I, Andreeva, V V, Goranchuk, E B, Shustov, A A, Boĭkova, V S, Petrova, M K, Rzhepetskaia, V N, Kuznetsov, I A, Men'shakov, B A, Margulis, and P D, Shabanov

Subjects
Adult, Male, Hot Temperature, Blood Pressure, Nitric Oxide, Adaptation, Physiological, Respiratory Function Tests, Immunoenzyme Techniques, Heart Rate, Leukocytes, Mononuclear, Humans, Interleukin-2, Protein Isoforms, HSP70 Heat-Shock Proteins, Body Temperature Regulation
Abstract

Heating humans up to rectal temperature 39.0-39.5 degrees C induces a heat stress and a physiological adaptation. Blood cells were found to produce nitric oxide under these conditions, neutrophiles playing a major role in the process. In our opinion, the HSC 70 takes part in the process of the long cell adaptation augmenting the cells' functional activity. Hyperthermia leads to a massive temporal HSP 72 expression in the blood mononuclears. This expression seems to be due to alterations in the cellular proteins and to oxidative stress.

Published
2002

29. Hsp70 and ceramide release by diode laser-treated mouse skin cells in vivo

Author

B A Margulis, I. S. Tarasov, K K Soboleva, N A Pikhtin, I V Guzova, G S Sokolovskii, S B Onikienko, and A V Zemlyanoi

Subjects
History, Ceramide, Materials science, Abiotic stress, Laser, Computer Science Applications, Education, Hsp70, law.invention, chemistry.chemical_compound, Biochemistry, chemistry, In vivo, law, Heat shock protein, Extracellular, Biophysics, Irradiation
Abstract

We report experimental study of generation of extracellular heat shock proteins (Hsp70) and ceramides under pulsed irradiation by quantum-well laser diodes. Our results are of great promise for applications in practical medicine such as protection against biopathogenes and abiotic stress factor challenges.

Published
2014
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30. [Induction of apoptosis in murine myeloma cells NS0/1, transfected with the gene for the basic heat shock protein HSP70i]

Author

I I, Fridlianskaia, O N, Demideov, M M, Bulatova, E V, Ignat'eva, A N, Semkina, I V, Guzhova, and B A, Margulis

Subjects
Mice, Tumor Cells, Cultured, Animals, Apoptosis, HSP70 Heat-Shock Proteins, Hydrogen Peroxide, Multiple Myeloma, Transfection, Culture Media, Serum-Free
Abstract

Murine myelomas are rare cell variants deficient in inducible isoform of Hsp70 that protects cells from injury. In these cells Hsp70 is absent and is not induced under stress conditions. In this study myeloma cells NS0/1 were transfected with hsp70, and their susceptibility to apoptosis was challenged by serum deprivation or hydrogen peroxide. Expression of Hsp70 in NS0/1 cells made them more resistant to apoptosis in serum-free medium but did not affect their response to hydrogen peroxide. Hsp70 involvement in the protection of myeloma cells from apoptosis caused by different agents is discussed.

Published
2001

31. [Induction and accumulation of HSP70 leads to formation of its complexes with other cell proteins]

Author

I V, Guzhova and B A, Margulis

Subjects
Hot Temperature, Tumor Necrosis Factor-alpha, Immunoblotting, Humans, Tetradecanoylphorbol Acetate, HSP70 Heat-Shock Proteins, U937 Cells, Chromatography, Affinity
Abstract

The expression of a major stress protein Hsp70 may be induced by a great number of cytotoxic agents and also by factors known to cause process of cell proliferation or apoptosis. After induction the synthesis of Hsp70 is reduced to its basic level within first 2-6 hours after inducer application, while the high content of the protein may persist up to several days. The aim of this study was to understand the reason of such a long storage of Hsp70 in U-937 cells induced with three distinct factors. The data of immunoblotting showed that the mild heat shock at 43 degrees C for 60 min, phorbol ester and tumor necrosis factor (the two latter known to induce differentiation and apoptosis, respectively) caused Hsp70 accumulation, the protein level being high within 48 hours and then slowly declined to the basal level. According to the results of chromatography on anti-Hsp70 antibody-Sepharose gel, approximately 50% of the protein was retarded by the gel, while the other part was not recognized by immunoglobulins. Among proteins bound to the Hsp70, three polypeptides were identified as actin, p65 and c-Rel, two latter being constituents of NF-kappa B regulatory complex. The data demonstrate that besides its traditional target, i.e. newly synthesized or abnormal polypeptides, Hsp70 is able to bind mature, active proteins.

Published
2000

32. [Stress proteins in eukaryotic cells]

Author

B A, Margulis and I V, Guzhova

Subjects
Eukaryotic Cells, Bacteria, Gene Expression Regulation, Humans, Heat-Shock Proteins
Abstract

The review concerns properties and function of heat shock proteins (hsp) in the eukaryotic cell. The factors inducing Hsps' expression are considered with the emphasis on the fact that most of these agents are able to affect the function of peptide-synthesizing and protein-modifying machineries. The common outcome of this effect is accumulation of wrongly assembled protein structures which results in activation of heat shock transcription factors. The major property of proteins belonging to Hsp70 and Hsp90 is their chaperonic activity or the ability to bind newly synthesized or damaged polypeptides followed by restoration of the native structure of the latter. In this activity Hsp70 and Hsp90 are assisted by other proteins, and the work of such chaperonic systems is described. The function of the major stress protein Hsp70 in the eukaryotic cell was analysed, and on the base of a huge amount of data in has been resumed that proteins of this family constitute one of the most abundant systems of cell protection against cytotoxic factors. In the concluding part of the review we present some ways of application of our knowledge of Hsp in ecology, for analysing biological pollution, and in medicine, for increasing tissue or organismal resistance to injuring factors.

Published
2000

33. Effects of exogenous stress protein 70 on the functional properties of human promonocytes through binding to cell surface and internalization

Author

I V, Guzhova, A C, Arnholdt, Z A, Darieva, A V, Kinev, E B, Lasunskaia, K, Nilsson, V M, Bozhkov, A P, Voronin, and B A, Margulis

Subjects
Tumor Necrosis Factor-alpha, HSC70 Heat-Shock Proteins, Genes, fos, Apoptosis, Cell Differentiation, DNA, Original Articles, Flow Cytometry, Endocytosis, Monocytes, Cell Line, Antigens, CD, Animals, Humans, Tetradecanoylphorbol Acetate, Cattle, HSP70 Heat-Shock Proteins, Carrier Proteins, Muscle, Skeletal, Promoter Regions, Genetic, Cell Division, Transcription Factors
Abstract

The presence of antibodies against the major stress protein, Hsp70, in patients with autoimmune diseases led us to hypothesize that Hsp70 may occur extracellularly, and could exert chaperoning and regulatory effects on various cells. We examined the action of pure Hsp/Hsc70 on the main physiological functions of human promonocytic U-937 cells. The protein was isolated from calf muscle and was shown to be a mixture of inducible Hsp70 (60%) and constitutive Hsc70 (40%) isoforms. It was observed that the addition of the protein up-regulated two major monocyte/macrophage differentiation markers, CD11c and CD23, by 20–35%, while it had no effect on CD14. The experiments performed to investigate the influence of Hsp/Hsc70 on the reaction of U-937 cells to differentiation stimuli demonstrated that the addition of the protein prior to PWlA was able to inhibit binding of proper transcription factors to double-symmetry and cAMP-response elements of the c-fos early response gene promoter. Administration of exogenous Hsp/Hsc70 prior to treatment with the tumor necrosis factor-alpha significantly lowered the number of apoptotic and necrotic cells. In no case did the control protein, ovalbumin, taken in the same concentration give a comparable effect on U-937 cells. Since the Hsp/Hsc70 effects occurred within the first hour of co-incubation, and therefore they might be explained by its interaction with the cell surface, we assayed binding of the biotinylated protein to U-937 cells by immunoenzyme assay, flow cytometry and indirect immunofluorescence. Using these three techniques we were able to detect Hsp/Hsc70 bound to cells after a 20 min incubation. According to flow cytometry data, at this time 32% of cells were positively stained with streptavidin-FITC. lmmunofluorescence studies demonstrated Hsp/Hsc70 bound to the cell surface after a 20 min incubation followed by induction of patch and cap-like structures. One hour later, the majority of the protein had been internalized by U-937 cells.

Published
1998

34. Major stress protein Hsp70 interacts with NF-kB regulatory complex in human T-lymphoma cells

Author

I V, Guzhova, Z A, Darieva, A R, Melo, and B A, Margulis

Subjects
Cell Nucleus, Inflammation, Lipopolysaccharides, Hot Temperature, Blotting, Western, NF-kappa B, Fluorescent Antibody Technique, Original Articles, Lymphoma, T-Cell, Proto-Oncogene Proteins c-rel, Kinetics, Stress, Physiological, Proto-Oncogene Proteins, Phorbol Esters, Tumor Cells, Cultured, Humans, HSP70 Heat-Shock Proteins, Transcription Factors
Abstract

Polypeptides belonging to the Hsp70 major stress protein family and to the NF-kB/Rel multi-functional regulatory complex are known to be involved in cellular defense mechanisms. It was suggested that both systems may interact in cells that respond to injuring stimuli. To check this, Molt4 human lymphoma cells were heated at 43 degrees C for 15 min and, after a 6 h post-shock recovery period, the cells were activated with phorbol ester or bacterial lipopolysaccharide. It was found that mild heat shock caused a substantial increase of the intracellular Hsp70 content with the concomitant suppression of NF-kB complexes, though the latter was properly activated in non-stressed cells. After a 24 h period of being inactive the complex fully recovered its activity and p65 and c-Rel subunits migrated to the nucleus. This new active period lasted even longer than that in non-heated control cells. As this suggested the existence of a Hsp70-related mechanism of NF-kB/Rel complex retention in cytoplasm, we carried out immunoprecipitation with the use of anti-Hsp70 and anti-Rel antibodies. All three Rel family members p65, c-Rel, p50, but not their precursors and IkB alpha inhibitory protein were shown to co-precipitate with the stress protein and anti-Hsp70 antibodies from both heated and non-heated cells. We conclude that the Hsp70 stress protein may confer a new mechanism of NF-kB regulation in cells affected by elevated temperature or other factors related to the cellular response to stress.

Published
1997

35. [Amyloidosis and antibodies to heat-shock proteins]

Author

N A, Mukhin, V N, Liashko, B A, Margulis, Kh A, Ul'masov, and B Ch, Karryeva

Subjects
Adult, Male, Nephrotic Syndrome, Amyloidosis, Middle Aged, Antibodies, Dermatomyositis, Immunoenzyme Techniques, Glomerulonephritis, Humans, Lupus Erythematosus, Systemic, Female, Renal Insufficiency, Heat-Shock Proteins
Published
1992

36. P.5.025 On the action of HSP70 preparation onthe central nervous system

Author

I. V. Guzhova, B. A. Margulis, P.D. Shabanov, and L.I. Andreyeva

Subjects
Pharmacology, Psychiatry and Mental health, medicine.anatomical_structure, Neurology, Action (philosophy), business.industry, Central nervous system, Medicine, Pharmacology (medical), Neurology (clinical), business, Neuroscience, Biological Psychiatry
Published
2005
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38. The Use of HSP70 for Prevention of Consequences of Unavoidable Stress in Rats.

Author

M. A. Flerov, N. E. Ordyan, B. A. Margulis, I. V. Guzhova, A. V. V'yushina, and S. G. Pivina

Abstract

We studied whether intranasal treatment with HSP70 can be used for the correction of maladaptive behavior in rats after unavoidable stress. After 3 intranasal injection of HSP70 in a dose of 3.25 μg we observed normalization of adaptive behavior after unavoidable stress and improvement of physiological reserves of the organism. [ABSTRACT FROM AUTHOR]

Published
2003

40. [Effect of hyperthermia on protein synthesis in monolayer and suspension cultures of mouse L cells]

Author

B A, Margulis, V V, Barlovskaia, and E G, Semenova

Subjects
Mice, Hot Temperature, L Cells, Cell Survival, Temperature, Animals, Electrophoresis, Polyacrylamide Gel, Heat-Shock Proteins
Abstract

Changes in protein synthesis that occurred under the influence of heat shock (HS) in monolayer (L929) and suspension (LS) mouse cell cultures were studied. The rates of protein synthesis determined as 35S-methionine incorporations were seen reduced from the initial level up to 40-60 and 6-13% after HS at 42 and 44 degrees C, respectively. Simultaneously the rate of actin and tubulin syntheses decreased, the decrease being more pronounced in LS cells. According to electrophoresis and autoradiography data, after hyperthermia both the cell cultures were able to synthesize heat shock proteins (HSP), primarily HSP70. After a 40 min HS towards L929 and LS cells at 43 degrees C, the shares of their HSP70 bands in the total label loaded on the gel constituted, resp., 8.8 and 5.4%. The data suggest that L929 cells, with their synthetic activity lower than in LS cells, appear more resistant to HS and are able eventually to synthesize larger amounts of HSP70, compared to the latter.

Published
1987

44. [Protein synthesis and antibody production in hybridoma cells under hyperthermia]

Author

L V, Smagina and B A, Margulis

Subjects
Hot Temperature, Hybridomas, Time Factors, Radioimmunoassay, Temperature, Antibodies, Monoclonal, Proteins, Electrophoresis, Disc, Mice, Protein Biosynthesis, Interferon Type I, Animals, Humans, Heat-Shock Proteins
Abstract

The relation between rates of protein synthesis and antibody production was studied for hybridoma cells treated at 42 degrees and 44 degrees C. Both the biosynthetic parameters were shown to recover after a mild heat shock at 42 degrees C with approximately the same kinetics. The treatment at 44 degrees C led to a full inhibition of Ig production, and the protein electrophoretic pattern was not recovered to normal state within 4-6 hours. The synthesis of heat shock proteins (HSP) was found only after the treatment at 42 degrees C. It is suggested that the expression of HSP is necessary for the recovery of hybridoma cell activities.

Published
1988

45. [Expression of heat-shock proteins in neuroblastoma cells differing genetically in thermal sensitivity]

Author

B Kh, Nisman, B A, Margulis, and V V, Barlovskaia

Subjects
Molecular Weight, Mice, Neuroblastoma, Hot Temperature, Temperature, Animals, Electrophoresis, Polyacrylamide Gel, Cells, Cultured, Heat-Shock Proteins, Cell Line, Neoplasm Proteins
Abstract

Electrophoretic analysis of cell proteins of 3 mouse neuroblastoma strains differing in thermostability has shown that a distinctive feature of one of the strains (stable to the action of temperature at 44 degrees C) is the accumulation under normal conditions (37 degrees C) of heat shock protein with the molecular mass of 70 kD. Such accumulation of the specific protein does not take place in cells of the thermosensitive strain, stable to temperature of 40 degrees C.

Published
1987

46. [Actin and tubulin synthesis in monolayer and suspension cultures of murine L cells]

Author

B A, Margulis, V V, Barlovskaia, and E G, Semenova

Subjects
Mice, L Cells, Methionine, Tubulin, Animals, Phosphoric Acids, Phosphorylation, Sulfur Radioisotopes, Phosphorus Radioisotopes, Actins
Abstract

The rates of total protein, actin and tubulin synthesis were studied for monolayer (L-929) and suspension (LS) cultures of mouse L cell. Data on pulse 34S-label incorporation into the cellular protein pool show that LS characterized by a short cell cycle have, comparatively to L-929, higher rates of protein synthesis and phosphorylation. According to PAGE data, the level of actin and tubulin synthesis in suspension line exceeds that in monolayer one. The correlation between growth conditions, biosynthetic parameters and dynamics of cytoskeleton is discussed.

Published
1987

47. [Chromosome fractionation. II. Features of the composition and behavior of biphasic polymer systems of metaphase chromosomes obtained from HeLa cells at acidic and neutral pH values]

Author

O K, Glebov, O I, Podgornaia, B A, Margulis, and G P, Pinaev

Subjects
Histones, Chromosomal Proteins, Non-Histone, Chromosomes, Human, Humans, RNA, DNA, Hydrogen-Ion Concentration, Cell Fractionation, Metaphase, HeLa Cells, Polyethylene Glycols
Abstract

Metaphase chromosomes (MCh) isolated at pH 2.1 and 6.5 slightly differ in their composition and contain in average: 17% of DNA, 9% of RNA and 74% of protein. The three-fold increase of protein content in MCh was not accompanied by the change in nonhistone protein composition. The behaviour of chromosomes isolated at pH 2.1 (acid) and 6.5 (neutral) in two-phase polymer system is shown to be very similar. The function of certain chromosome components in the determination of MCh behaviour in two-phase systems and possible usefulness of acid and neutral MCh for fractionation of total MCh are discussed.

Published
1981

48. [Removal of surface antigens and changes in metastatic potential of transplantable rat rhabdomyosarcoma RA-2 cells]

Author

I V, Guzhova and B A, Margulis

Subjects
Molecular Weight, Antigens, Neoplasm, Antigens, Surface, Rhabdomyosarcoma, Animals, Electrophoresis, Polyacrylamide Gel, Female, Neoplasm Metastasis, Rats
Abstract

Cells of rat rhabdomyosarcoma RA-2 selected for high metastatic potential and affinity to lung tissue were (125I)-labelled in the presence of iodogene. The spectrum of 125I-labelled cell surface antigens was investigated by SDS-PAGE. Radionuclide was incorporated by proteins (or glycoproteins) with molecular weight of 30, 36, 47, 57, 78, 90, 102, 124, 180 and 250 kDa. After incubation of cells with 0.05-0.2% triton X-100 solution all the proteins except for those with molecular weight of 47 and 57 kDa were washed off the cellular surface; metastatic potential (MP) of triton-100 treated cells was 10 times as low as that of intact cells.

Published
1988

49. [Sarcoplasmic actin in muscle cells of ambulacral tubes of the sea star]

Author

O I, Podgornaia, A L, Drozdov, B A, Margulis, and G P, Pinaev

Subjects
Sarcoplasmic Reticulum, Starfish, Muscles, Animals, Actins, Cytoskeleton
Abstract

Protein solubilized in large quantities in solutions of low ionic strength, when myofibril-like preparations were isolated from ambulacral tube, was shown to be actin. When gelation of sarcoplasmic proteins occurs a gel consisting of actin microfilaments bundles is formed. The factor which inhibits actin polymerization is liberated during gel formation. The aggregate substance of sarcoplasmic actin under cell ionic conditions may be determined by binding with this factor.

Published
1982

50. [Effect of mitogenic stimulation and heat shock on protein syntheses in human T cells]

Author

B A, Margulis, O Iu, Antropova, I Ia, Kazhdan, and A S, Tsveĭbakh

Subjects
Hot Temperature, Time Factors, T-Lymphocytes, Temperature, Humans, Mitogens, Phytohemagglutinins, Cell Division, Cells, Cultured, Heat-Shock Proteins, Stimulation, Chemical
Abstract

Effects of moderate (42 degrees C, 1 hour) and strong (44 degrees C, 1 hour) heat shocks on resting (TR) and phytohemagglutinin stimulated human T-cells (TP) were studied. Both treatments were shown to cause in the latter considerable fall of the level of protein synthesis, as compared to resting cells. Mitogen-stimulated cells stopped their proliferation irreversibly and part of them (approx: 40%) died after even mild shock (at 42 degrees C). Following heat treatment in both the cell types the synthesis of heat shock 70 and 90 kDa proteins was induced which was much more pronounced in TR. These and earlier results of the authors allow a conclusion that involvement of cells in active proliferation may decrease their resistance to stress, and that this phenomenon coincides with the diminishing in synthesis and accumulation of stress proteins.

Published
1989

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