Vlasta Sovová
Czechoslovak Academy of Sciences
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Featured researches published by Vlasta Sovová.
International Journal of Cancer | 1999
Zdena Tuháčková; Vlasta Sovová; Eva Šloncová; Christopher G. Proud
Increased phosphorylation of the translational repressor protein 4E‐BP1 was found in the cell line derived from the tumor induced in Syrian hamster by Rous sarcoma virus (RSV). This was accompanied by its dissociation from the complex with initiation factor eIF4E. The ribosomal S6 protein kinase p70S6k is supposed to be regulated by the same or a closely related rapamycin‐sensitive signalling pathway to that which modulates 4E‐BP1. Phosphorylation and activity of p70S6k were found to be also increased in RSV‐transformed H19 cells that express significantly higher amounts of the Src protein (p60src) relative to the non‐transformed hamster fibroblasts NIL‐2. The increased activity and phosphorylation of p70S6k were blocked by rapamycin, indicating that the rapamycin‐sensitive pathway is involved in its regulation in v‐src‐transformed hamster fibroblasts. In agreement with this, rapamycin reduced the expression of elongation factor eEF1α (whose translation is regulated by a rapamycin‐sensitive mechanism thought to involve p70S6k) and did not affect the production of a housekeeping protein, α‐tubulin, in these cells. Synthesis of Src protein was also inhibited in cells treated with rapamycin. However, treatment of cells with a concentration of rapamycin sufficient to completely inhibit the activity and phosphorylation of p70S6k resulted in only partial de‐phosphorylation of 4E‐BP1 and its re‐association with eIF4E in the transformed cells, indicating that additional rapamycin‐insensitive mechanisms/pathways are implicated in the control of 4E‐BP1 phosphorylation in RSV‐transformed hamster fibroblasts. Over‐expression of eIF4E favours cell proliferation and can lead to a transformed phenotype, while over‐expression of 4E‐BP1 has the opposite effect. The altered signalling to the phosphorylation of 4E‐BP1 in RSV‐transformed cells, which leads to its dissociation from eIF4E and thus relief of inhibition of eIF4E function, may therefore represent an important regulatory mechanism in malignant cell growth. Int. J. Cancer 81:963–969, 1999.
Avian Pathology | 1981
Vlasta Sovová; I. Hlozanek; H. Cerna; V. Dostalova; H. Sainerova
A cell line derived from a transplantable chicken hepatoma induced by virus MC29 was established. This cell line grew permanently over 2 years and could be easily recovered from frozen state. Morphology of cells did not change during the period of cultivation. Karyological analysis revealed the hypodiploid stemline with reduced numbers of microchromosomes. The cell line was not transplantable in 1-day-old chicks, but induced multiple tumour nodules in the mesenterium and liver about 8 weeks postinoculation. The cell line is virus productive. The analysis of viral proteins with the gag specific determinants showed the presence of pr76 and p110.
International Journal of Cancer | 1971
J. Svoboda; O. Machala; L. Donner; Vlasta Sovová
International Journal of Cancer | 2009
Vlasta Sovová; Helena Fidlerová; I. Hlozánek; R. Friis
International Journal of Molecular Medicine | 2002
Dana Kučerová; Jitka Štokrová; Jan Korb; Eva Šloncová; Zdena Tuháčková; Vlasta Sovová
Hereditas | 2008
Helena Fidlerová; Vlasta Sovová; Ivan Krekule; Göran Levan
International Journal of Oncology | 2006
Jitka Štokrová; Eva Šloncová; Vlasta Sovová; Dana Kučerová; Vojtech Zíla; Jolana Turecková; Martina Vojtechova; Jan Korb; Zdena Tuháčková
International Journal of Molecular Medicine | 2004
Zdena Tuháčková; Eva Šloncová; Martina Vojtechova; Vlasta Sovová
International Journal of Molecular Medicine | 2001
Dana Kučerová; Eva Šloncová; Zdena Tuháčková; Martina Vojtechova; Vlasta Sovová
International Journal of Oncology | 2005
Jitka Štokrová; Vlasta Sovová; Eva Šloncová; Dana Kučerová; Zdena Tuháčková; Jan Korb