Your search keyword '"O. Somova"' showing total 3 results

1. A comparative study of sphingolipids in transplanted melanomas with high and low metastatic activity.

Author

A. Kandyba, A. Kozlov, O. Somova, and E. Dyatlovitskaya

Subjects

SPHINGOLIPIDS, MELANOMA, CERAMIDES, SIALIC acids

Abstract

Abstract  The content of sphingolipids in M3 and B16/F10 melanomas with a high metastatic potential and in Claudmanís and B16/F1 melanomas with a low metastatic potential was studied. It was shown that the content of total lipid-bound sialic acids and ganglioside GM3 in melanomas with a high metastatic potential is considerably higher than that in melanomas with a low metastatic potential. On the other hand, the ceramide to glucosylceramide molar ratio is higher in melanomas with a low metastatic potential. [ABSTRACT FROM AUTHOR]

Published

2008

2. Biologically active sphingolipids in transplantable tumors of different histogenesis.

Author

A. Kandyba, A. Kozlov, O. Somova, and E. Dyatlovitskaya

Abstract

The composition of biologically active sphingolipids in hepatoma 22, breast adenocarcinoma, Lewis lung carcinoma, large intestine adenocarcinoma, cervical carcinoma, and melanomas M3 and B16 was compared to elucidate the similarity and differences in sphingolipids of subcutaneously transplantable murine tumors. The sphingolipid composition of the tumors was found to widely vary. The sphingomyelin, ceramide, glucosyl-and lactosylceramide, and ganglioside GD3 contents in hepatoma 22 are higher than those in normal tissue. No common regularities for tumors of different origin were observed in the ratios of bioeffectors inhibiting proliferation and stimulating apoptosis and bioeffectors stimulating cell growth and survival. However, the Cer/(GlcCer + LacCer) ratios were very low and practically equal in two melanoma strains, which probably indicates the degree of tumor malignancy. The results suggest that the content and composition of sphingolipids in tumors depend on their histogenesis. [ABSTRACT FROM AUTHOR]

Published

2006

3. Electrokinetic injection of DNA from gel micropads: basis for coupling polony technology with CE separation.

Author

Kosobokova O, Gavrilov DN, Khozikov V, Stepukhovich A, Tsupryk A, Pan'kov S, Somova O, Abanshin N, Gudkov G, Tcherevishnik M, and Gorfinkel V

Subjects

Base Sequence, Electrophoresis, Microchip instrumentation, Equipment Design, Gels chemistry, Indicators and Reagents, Polymerase Chain Reaction instrumentation, Reproducibility of Results, Sensitivity and Specificity, Sequence Analysis, DNA instrumentation, Spectrophotometry, Ultraviolet, DNA isolation & purification, Electrophoresis, Microchip methods, Models, Chemical, Nanotechnology methods, Polymerase Chain Reaction methods, Sequence Analysis, DNA methods

Abstract

We propose a novel method for electrokinetic injection of DNA samples into capillaries from nanoliter gel micropads, deposited on glass slides, which are coated with electroconducting film. Theoretical and experimental proof is presented for the proposed method. The method allows efficient and highly precise injection without physical contact between the gel pad and the capillary. Read length of more than 700 bp at Q20 has been reproducibly demonstrated in fused-silica capillaries using the proposed injection technique. Based on the obtained results we discuss a novel DNA sequencing system which combines DNA amplification and cycle sequencing in arrays of subnanoliter gel micropads and high-throughput electrophoretic separation in monolith multicapillary arrays.

Published

2007