Your search keyword '"Matrosova, Vera Y."' showing total 5 results

1. Expression of Birt-Hogg-Dubé gene mRNA in normal and neoplastic human tissues.

Author

Warren MB, Torres-Cabala CA, Turner ML, Merino MJ, Matrosova VY, Nickerson ML, Ma W, Linehan WM, Zbar B, and Schmidt LS

Subjects

Brain metabolism, Exocrine Glands metabolism, Fibroma genetics, Fibroma pathology, Gene Expression, Humans, In Situ Hybridization, Fluorescence methods, Kidney metabolism, Kidney Neoplasms genetics, Kidney Neoplasms pathology, Lung metabolism, Neoplasms genetics, Palatine Tonsil metabolism, Pancreas metabolism, Parotid Gland metabolism, Proto-Oncogene Proteins, RNA, Messenger genetics, Skin metabolism, Spleen metabolism, Tissue Array Analysis methods, Tumor Suppressor Proteins, Neoplasms pathology, Proteins genetics, RNA, Messenger metabolism

Abstract

Birt-Hogg-Dubé (BHD) syndrome is an inherited autosomal genodermatosis characterized by hamartomas of the hair follicle called fibrofolliculomas and an increased risk for developing spontaneous pneumothorax, lung cysts and renal neoplasia. BHD was localized to chromosome 17p11.2 by linkage analysis in BHD families, and germline insertion/deletion and nonsense mutations in a novel gene were identified which were predicted to prematurely truncate the BHD protein, folliculin. No homology to other human proteins was found although folliculin was conserved across species. As a first step toward understanding the function of BHD in the cell and how BHD mutations can lead to the BHD phenotype, we measured the expression of BHD mRNA in normal and neoplastic human tissues by fluorescent in situ hybridization. BHD mRNA was expressed in a variety of tissues, including the skin and its appendages, the distal nephron of the kidney, stromal cells and type 1 pneumocytes of the lung, acinar cells of the pancreas and parotid gland, and epithelial ducts of the breast and prostate. In the brain, BHD mRNA was expressed in neurons of the cerebrum, and Purkinje cells in the cerebellum. BHD mRNA was also expressed in macrophage and lymphocytes in the tonsils and spleen. Tissues with reduced expression of BHD mRNA included heart, muscle and liver. BHD mRNA was expressed strongly in the proliferating epithelial strands of fibrofolliculomas, the cutaneous lesions characteristic of BHD, but not in renal tumors from BHD patients. These results indicate a wide expression pattern for BHD mRNA in many tissues, including skin, lung and kidney, which are involved in the BHD phenotype, and support a tumor suppressor role for BHD in renal cancer.

Published

2004

2. Microbial cells can cooperate to resist high-level chronic ionizing radiation.

Author

Shuryak, Igor, Matrosova, Vera Y., Gaidamakova, Elena K., Tkavc, Rok, Grichenko, Olga, Klimenkova, Polina, Volpe, Robert P., and Daly, Michael J.

Subjects

*PHYSIOLOGICAL effects of ionizing radiation, *MICROBIAL cells, *MICROBIAL growth, *RADIOACTIVE waste sites, *MICROBIAL remediation, *QUANTITATIVE research

Abstract

Understanding chronic ionizing radiation (CIR) effects is of utmost importance to protecting human health and the environment. Diverse bacteria and fungi inhabiting extremely radioactive waste and disaster sites (e.g. Hanford, Chernobyl, Fukushima) represent new targets of CIR research. We show that many microorganisms can grow under intense gamma-CIR dose rates of 13–126 Gy/h, with fungi identified as a particularly CIR-resistant group of eukaryotes: among 145 phylogenetically diverse strains tested, 78 grew under 36 Gy/h. Importantly, we demonstrate that CIR resistance can depend on cell concentration and that certain resistant microbial cells protect their neighbors (not only conspecifics, but even radiosensitive species from a different phylum), from high-level CIR. We apply a mechanistically-motivated mathematical model of CIR effects, based on accumulation/removal kinetics of reactive oxygen species (ROS) and antioxidants, in bacteria (3 Escherichia coli strains and Deinococcus radiodurans) and in fungi (Candida parapsilosis, Kazachstania exigua, Pichia kudriavzevii, Rhodotorula lysinophila, Saccharomyces cerevisiae, and Trichosporon mucoides). We also show that correlations between responses to CIR and acute ionizing radiation (AIR) among studied microorganisms are weak. For example, in D. radiodurans, the best molecular correlate for CIR resistance is the antioxidant enzyme catalase, which is dispensable for AIR resistance; and numerous CIR-resistant fungi are not AIR-resistant. Our experimental findings and quantitative modeling thus demonstrate the importance of investigating CIR responses directly, rather than extrapolating from AIR. Protection of radiosensitive cell-types by radioresistant ones under high-level CIR is a potentially important new tool for bioremediation of radioactive sites and development of CIR-resistant microbiota as radioprotectors. [ABSTRACT FROM AUTHOR]

Published

2017

3. MDP: A Deinococcus Mn2+-Decapeptide Complex Protects Mice from Ionizing Radiation.

Author

Gupta, Paridhi, Gayen, Manoshi, Smith, Joan T., Gaidamakova, Elena K., Matrosova, Vera Y., Grichenko, Olga, Knollmann-Ritschel, Barbara, Daly, Michael J., Kiang, Juliann G., and Maheshwari, Radha K.

Subjects

DEINOCOCCUS, RADIATION damage, RADIATION-protective agents, VACCINES, LABORATORY mice

Abstract

The radioprotective capacity of a rationally-designed Mn2+-decapeptide complex (MDP), based on Mn antioxidants in the bacterium Deinococcus radiodurans, was investigated in a mouse model of radiation injury. MDP was previously reported to be extraordinarily radioprotective of proteins in the setting of vaccine development. The peptide-component (DEHGTAVMLK) of MDP applied here was selected from a group of synthetic peptides screened in vitro for their ability to protect cultured human cells and purified enzymes from extreme damage caused by ionizing radiation (IR). We show that the peptides accumulated in Jurkat T-cells and protected them from 100 Gy. MDP preserved the activity of T4 DNA ligase exposed to 60,000 Gy. In vivo, MDP was nontoxic and protected B6D2F1/J (female) mice from acute radiation syndrome. All irradiated mice treated with MDP survived exposure to 9.5 Gy (LD70/30) in comparison to the untreated mice, which displayed 63% lethality after 30 days. Our results show that MDP provides early protection of white blood cells, and attenuates IR-induced damage to bone marrow and hematopoietic stem cells via G-CSF and GM-CSF modulation. Moreover, MDP mediated the immunomodulation of several cytokine concentrations in serum including G-CSF, GM-CSF, IL-3 and IL-10 during early recovery. Our results present the necessary prelude for future efforts towards clinical application of MDP as a promising IR countermeasure. Further investigation of MDP as a pre-exposure prophylactic and post-exposure therapeutic in radiotherapy and radiation emergencies is warranted. [ABSTRACT FROM AUTHOR]

Published

2016

4. Protein oxidation: key to bacterial desiccation resistance?

Author

Fredrickson, James K., Li, Shu-mei W., Gaidamakova, Elena K., Matrosova, Vera Y., Min Zhai, Sulloway, Heather M., Scholten, Johannes C., Brown, Mindy G., Balkwill, David L., and Daly, Michael J.

Subjects

IONIZATION (Atomic physics), BACTERIA, PROTEINS, IRRADIATION, PHYLOGENY, OXIDATION

Abstract

For extremely ionizing radiation-resistant bacteria, survival has been attributed to protection of proteins from oxidative damage during irradiation, with the result that repair systems survive and function with far greater efficiency during recovery than in sensitive bacteria. Here we examined the relationship between survival of dry-climate soil bacteria and the level of cellular protein oxidation induced by desiccation. Bacteria were isolated from surface soils of the shrub-steppe of the US Department of Energy's Hanford Site in Washington State. A total of 63 isolates were used for phylogenetic analysis. The majority of isolates were closely related to members of the genus Deinococcus, with Chelatococcus, Methylobacterium and Bosea also among the genera identified. Desiccation-resistant isolates accumulated high intracellular manganese and low iron concentrations compared to sensitive bacteria. In vivo, proteins of desiccation-resistant bacteria were protected from oxidative modifications that introduce carbonyl groups in sensitive bacteria during drying. We present the case that survival of bacteria that inhabit dry-climate soils are highly dependent on mechanisms, which limit protein oxidation during dehydration.The ISME Journal (2008) 2, 393–403; doi:10.1038/ismej.2007.116; published online 14 February 2008 [ABSTRACT FROM AUTHOR]

Published

2008

5. Protein Oxidation Implicated as the Primary Determinant of Bacterial Radioresistance.

Author

Daly, Michael J., Gaidamakova, Elena K., Matrosova, Vera Y., Vasilenko, Alexander, Min Zhai, Leapman, Richard D., Lai, Barry, Ravel, Bruce, Li, Shu-Mei W., Kemner, Kenneth M., and Fredrickson, James K.

Subjects

IONIZING radiation, DNA, PROKARYOTES, DEINOCOCCUS radiodurans, BACTERIA, PROTEINS

Abstract

In the hierarchy of cellular targets damaged by ionizing radiation (IR), classical models of radiation toxicity place DNA at the top. Yet, many prokaryotes are killed by doses of IR that cause little DNA damage. Here we have probed the nature of Mn-facilitated IR resistance in Deinococcus radiodurans, which together with other extremely IR-resistant bacteria have high intracellular Mn/Fe concentration ratios compared to IR-sensitive bacteria. For in vitro and in vivo irradiation, we demonstrate a mechanistic link between Mn(II) ions and protection of proteins from oxidative modifications that introduce carbonyl groups. Conditions that inhibited Mn accumulation or Mn redox cycling rendered D. radiodurans radiation sensitive and highly susceptible to protein oxidation. X-ray fluorescence microprobe analysis showed that Mn is globally distributed in D. radiodurans, but Fe is sequestered in a region between dividing cells. For a group of phylogenetically diverse IR-resistant and IR-sensitive wild-type bacteria, our findings support the idea that the degree of resistance is determined by the level of oxidative protein damage caused during irradiation. We present the case that protein, rather than DNA, is the principal target of the biological action of IR in sensitive bacteria, and extreme resistance in Mn-accumulating bacteria is based on protein protection. [ABSTRACT FROM AUTHOR]

Published

2007