Nelly Sh. Padyukova
Engelhardt Institute of Molecular Biology
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Breast Cancer Research and Treatment | 2002
Gregory G. Reinholz; Barbara Getz; Emily S. Sanders; Marat Ya. Karpeisky; Nelly Sh. Padyukova; Sergey N. Mikhailov; James N. Ingle; Thomas C. Spelsberg
While the effects of bisphosphonates on bone-resorbing osteoclasts have been well documented, the effects of bisphosphonates on other cell types are not as well studied. Recently, we reported that bisphosphonates have direct effects on bone-forming human fetal osteoblast cells (hFOB) [1]. In this report, the role of the mevalonate pathway in the actions of bisphosphonates on hFOB, and MDA-MB-231 human breast cancer cells was examined. These studies included a novel bisphosphonate analog, the anhydride formed between arabinocytidine 5′ phosphate and etidronate (Ara-CBP). Ara-CBP was the most potent inhibitor of hFOB and MDA-MB-231 cell proliferation, and stimulator of hFOB cell mineralization compared to etidronate, the anhydride formed between AMP and etidronate (ABP), pamidronate, and zoledronate. Inhibition of hFOB cell proliferation by Ara-CBP and zoledronate was partially reversed by mevalonate pathway intermediates, and stimulation of hFOB cell mineralization was completely reversed by mevalonate pathway intermediates. These results suggest that zoledronate and Ara-CBP act, at least in part, via inhibition of the mevalonate pathway in hFOB cells. In contrast, none of the mevalonate pathway intermediates reversed the inhibition of MDA-MB-231 cell proliferation by the bisphosphonates, or the effects of pamidronate on hFOB cells. As a positive control, the effects of mevastatin on hFOB and MDA-MB-231 cells were completely reversed by mevalonate. In summary, these data suggest that zoledronate and Ara-CBP induce human osteoblast differentiation via inhibition of the mevalonate pathway. In contrast, the inhibition of MDA-MB-231 cell proliferation by the bisphosphonates appears to be through mechanisms other than inhibition of the mevalonate pathway.
Carbohydrate Research | 1983
Sergey N. Mikhailov; Leon N. Beigelman; Galyna V. Gurskaya; Nelly Sh. Padyukova; Gennady I. Yakovlev; Marat Ya. Karpeisky
Abstract 3′- C -Methyluridine and 3′- C -methylcytidine were synthesized in 11 steps starting from d -glucose. The conformation of 3′- C -methylnucleosides was studied in solution and in the crystal by using the techniques of c.d., 1 H-n.m.r. spectroscopy, and X-ray diffraction analysis. 3′- C -Methyluridine 2′,3′-cyclophosphate was prepared, and its hydrolysis with nucleases was studied. 3′- C -Methyluridine 5′- mono- and 5′-tri-phosphate were also synthesized.
Collection of Czechoslovak Chemical Communications | 1982
Marat Yu. Karpeisky; Leon N. Beigelman; Sergey N. Mikhailov; Nelly Sh. Padyukova; Jiří Smrt
Collection of Czechoslovak Chemical Communications | 1989
S. N. Mikhailov; Nelly Sh. Padyukova; Marat Ya. Karpeiskii; L. I. Kolobushkina; Leon N. Beigelman
Tetrahedron Letters | 1987
Nelly Sh. Padyukova; Marat Ya. Karpeisky; L. I. Kolobushkina; Sergey N. Mikhailov
European Journal of Organic Chemistry | 1998
Sergey N. Mikhailov; Andrei A. Rodionov; Ekaterina V. Efimtseva; Boris S. Ermolinsky; Marina V. Fomitcheva; Nelly Sh. Padyukova; Klaus Rothenbacher; Eveline Lescrinier; Piet Herdewijn
Journal of Organic Chemistry | 1993
Mikko Oivanen; Sergey N. Mikhailov; Nelly Sh. Padyukova; Harri Lönnberg
Collection of Czechoslovak Chemical Communications | 1996
Ekaterina V. Efimtseva; Boris S. Ermolinsky; Marina V. Fomitcheva; Sergey V. Meshkov; Nelly Sh. Padyukova; Sergey N. Mikhailov; Arthur Van Aerschot; Jef Rozenski; Piet Herdewijn
Nucleosides, Nucleotides & Nucleic Acids | 1999
Sergey N. Mikhailov; Andrei A. Rodionov; Ekaterina V. Efimtseva; Boris S. Ermolinsky; Marina V. Fomitcheva; Nelly Sh. Padyukova; Klaus Rothenbacher; Eveline Lescrinier; Piet Herdewijn
Acta Chemica Scandinavica | 1995
Mikko Oivanen; Nelly Sh. Padyukova; Satu Kuusela; Sergey N. Mikhailov; Harri Lönnberg; Jan Arnarp; Lars Björk; Ryszard Gawinecki