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volume 19 issue 6 pages 73-81

INHIBITION OF REDD1 EXPRESSION FOR THE REDUCTION OF GLUCOCORTICOID-INDUCED SIDE EFFECTS

E S Lylova 1
Ekaterina M. Zhidkova 3
I Budunova 5
Publication typeJournal Article
Publication date2020-12-31
scimago Q4
SJR0.134
CiteScore0.6
Impact factor
ISSN18144861, 23123168
Cancer Research
Oncology
Abstract

Glucocorticoids (GC ) have been an integral component of the treatment of leukemias and lymphomas for several decades. Specific cytotoxic effect of GC on transformed lymphoblasts mediates their use at the stage of the remission induction as well as consolidation of treatment. However, the main problem of the long-term GC use is the development of atrophic and metabolic side effects as well as GC resistance. The biological effects of GC are realized via activation of the glucocorticoid receptor (GR) by two mechanisms: transrepression (TR) associated with the therapeutic effects of GC , and transactivation (TA ), which mediates the development of metabolic and atrophic complications. It was demonstrated that an increase in the expression of the GC - dependent gene REDD1 associated with GC -induced skin, muscle and bone atrophy of the skin, muscle and bone tissue was realized via the induction of transactivation. Therefore, identification of potential inhibitors of REDD1 expression and study of their biological effects in combination with GC in models of leukemia and lymphoma is of particular interest. In our recent study we have selected a number of drugs from the class of PI 3K/Akt/mTO R modulators using bioinformatic screening. These drugs effectively inhibited REDD1 expression, modulated GR activity and shifted it towards transrepression, and prevented the development of GC -induced side effects in mice. Here we aimed to study the effects of potential inhibitors of REDD1 expression from different pharmacological groups, the compounds Emetine and CGP -60474, on leukemia and lymphoma cells in combination with GC . We demonstrated antitumor effect of the compounds in vitro, a decrease in the expression of TA -associated genes and an increase in TR induction. Further studies of the antitumor effects of REDD1 expression inhibitors (Emetine and CGP -60474 is a promising area of research.

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Siberian Journal of Oncology
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Lylova E. S. et al. INHIBITION OF REDD1 EXPRESSION FOR THE REDUCTION OF GLUCOCORTICOID-INDUCED SIDE EFFECTS // Siberian Journal of Oncology. 2020. Vol. 19. No. 6. pp. 73-81.
GOST all authors (up to 50) Copy
Lylova E. S., Savinkova A. V., Zhidkova E. M., Kirsanov K. I., Yakubovskaya M. G., Budunova I., Lesovaya E. A. INHIBITION OF REDD1 EXPRESSION FOR THE REDUCTION OF GLUCOCORTICOID-INDUCED SIDE EFFECTS // Siberian Journal of Oncology. 2020. Vol. 19. No. 6. pp. 73-81.
RIS |
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RIS Copy
TY - JOUR
DO - 10.21294/1814-4861-2020-19-6-73-81
UR - https://doi.org/10.21294/1814-4861-2020-19-6-73-81
TI - INHIBITION OF REDD1 EXPRESSION FOR THE REDUCTION OF GLUCOCORTICOID-INDUCED SIDE EFFECTS
T2 - Siberian Journal of Oncology
AU - Lylova, E S
AU - Savinkova, A V
AU - Zhidkova, Ekaterina M.
AU - Kirsanov, Kirill I.
AU - Yakubovskaya, Marianna G.
AU - Budunova, I
AU - Lesovaya, Ekaterina A.
PY - 2020
DA - 2020/12/31
PB - Tomsk Cancer Research Institute
SP - 73-81
IS - 6
VL - 19
SN - 1814-4861
SN - 2312-3168
ER -
BibTex |
Cite this
BibTex (up to 50 authors) Copy
@article{2020_Lylova,
author = {E S Lylova and A V Savinkova and Ekaterina M. Zhidkova and Kirill I. Kirsanov and Marianna G. Yakubovskaya and I Budunova and Ekaterina A. Lesovaya},
title = {INHIBITION OF REDD1 EXPRESSION FOR THE REDUCTION OF GLUCOCORTICOID-INDUCED SIDE EFFECTS},
journal = {Siberian Journal of Oncology},
year = {2020},
volume = {19},
publisher = {Tomsk Cancer Research Institute},
month = {dec},
url = {https://doi.org/10.21294/1814-4861-2020-19-6-73-81},
number = {6},
pages = {73--81},
doi = {10.21294/1814-4861-2020-19-6-73-81}
}
MLA
Cite this
MLA Copy
Lylova, E. S., et al. “INHIBITION OF REDD1 EXPRESSION FOR THE REDUCTION OF GLUCOCORTICOID-INDUCED SIDE EFFECTS.” Siberian Journal of Oncology, vol. 19, no. 6, Dec. 2020, pp. 73-81. https://doi.org/10.21294/1814-4861-2020-19-6-73-81.