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@article{616405, author = {Bryja, V. and Pacherník, J. and Souček, K. and Horvath, V. and Dvořák, P. and Hampl, Aleš}, article_number = {11}, keywords = {stem cells}, language = {eng}, issn = {1420-682X}, journal = {Cellular and molecular life sciences}, title = {Increased apoptosis in differentiating p27-deficient mouse embryonic stem cells}, volume = {61}, year = {2004} }
TY - JOUR ID - 616405 AU - Bryja, V. - Pacherník, J. - Souček, K. - Horvath, V. - Dvořák, P. - Hampl, Aleš PY - 2004 TI - Increased apoptosis in differentiating p27-deficient mouse embryonic stem cells JF - Cellular and molecular life sciences VL - 61 IS - 11 SP - 1384-1400 EP - 1384-1400 SN - 1420682X KW - stem cells N2 - In mouse embryonic stem (mES) cells, the expression of p27 is elevated when differentiation is induced. Using mES cells lacking p27 we tested the importance of p27 for the regulation of three critical cellular processes: proliferation, differentiation, and apoptosis. Although cell cycle distribution, DNA synthesis, and the activity of key G1/S-regulating cyclin-dependent kinases remained unaltered in p27-deficient ES cells during retinoic acid-induced differentiation, the amounts of cyclin D2 and D3 in such cells were much lower compared with normal mES cells. The onset of differentiation induces apoptosis in p27-deficient cells, the extent of which can be reduced by artificially increasing the level of cyclin D3. We suggest that the role of p27 in at least some differentiation pathways of mES cells is to prevent apoptosis, and that it is not involved in slowing cell cycle progression. We also propose that the pro-survival function of p27 is realized via regulation of metabolism of D-type cyclin(s). ER -
BRYJA, V., J. PACHERNÍK, K. SOUČEK, V. HORVATH, P. DVOŘÁK a Aleš HAMPL. Increased apoptosis in differentiating p27-deficient mouse embryonic stem cells. \textit{Cellular and molecular life sciences}. 2004, roč.~61, č.~11, s.~1384-1400. ISSN~1420-682X.
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