SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W55958259> ?p ?o ?g. }

Showing items 1 to 100 of ±135 with 100 items per page.

W55958259 endingPage "1939" @default.
W55958259 startingPage "1933" @default.
W55958259 abstract "Abstract Chronic myeloid leukemia (CML) is a malignant stem cell disease characterized by an expansion of myeloid progenitor cells expressing the constitutively activated Bcr-Abl kinase. This oncogenic event causes a deregulation of apoptosis and cell cycle progression. Although the molecular mechanisms protecting from apoptosis in CML cells are well characterized, the cell cycle regulatory event is poorly understood. An inhibitor of the cyclin-dependent kinases, p27, plays a central role in the regulation of growth factor dependent proliferation of hematopoietic cells. Therefore, we have analyzed the influence of Bcr-Abl in the regulation of p27 expression in various hematopoietic cell systems. An active Bcr-Abl kinase causes down-regulation of p27 expression in murine Ba/F3 cells and human M07 cells. Bcr-Abl blocks up-regulation of p27 after growth factor withdrawal and serum reduction. In addition, p27 induction by transforming growth factor-beta (TGF-β) is completely blocked in Bcr-Abl positive M07/p210 cells. This deregulation is directly mediated by the activity of the Bcr-Abl kinase. A Bcr-Abl kinase inhibitor completely abolishes p27 down-regulation by Bcr-Abl in both Ba/F3 cells transfected either with a constitutively active Bcr-Abl or with a temperature sensitive mutant. The down-regulation of p27 by Bcr-Abl depends on proteasomal degradation and can be blocked by lactacystin. Overexpression of wild-type p27 partially antagonizes Bcr-Abl–induced proliferation in Ba/F3 cells. We conclude that Bcr-Abl promotes cell cycle progression and activation of cyclin-dependent kinases by interfering with the regulation of the cell cycle inhibitory protein p27." @default.
W55958259 created "2016-06-24" @default.
W55958259 creator A5040777952 @default.
W55958259 creator A5047674033 @default.
W55958259 creator A5076077834 @default.
W55958259 creator A5081028472 @default.
W55958259 creator A5083668977 @default.
W55958259 creator A5084729483 @default.
W55958259 creator A5088789978 @default.
W55958259 date "2000-09-01" @default.
W55958259 modified "2023-10-09" @default.
W55958259 title "Bcr-Abl kinase down-regulates cyclin-dependent kinase inhibitor p27 in human and murine cell lines" @default.
W55958259 cites W1501358984 @default.
W55958259 cites W1805917608 @default.
W55958259 cites W1971245466 @default.
W55958259 cites W1975324295 @default.
W55958259 cites W1982768428 @default.
W55958259 cites W1986464453 @default.
W55958259 cites W1988935612 @default.
W55958259 cites W1994572080 @default.
W55958259 cites W1996413533 @default.
W55958259 cites W1999294280 @default.
W55958259 cites W2003907692 @default.
W55958259 cites W2007255413 @default.
W55958259 cites W2015066175 @default.
W55958259 cites W2015519364 @default.
W55958259 cites W2016086822 @default.
W55958259 cites W2018574431 @default.
W55958259 cites W2019692551 @default.
W55958259 cites W2027612041 @default.
W55958259 cites W2031514188 @default.
W55958259 cites W2033156691 @default.
W55958259 cites W2038588592 @default.
W55958259 cites W2041440798 @default.
W55958259 cites W2048721919 @default.
W55958259 cites W2055085859 @default.
W55958259 cites W2060892787 @default.
W55958259 cites W2066848701 @default.
W55958259 cites W2069023125 @default.
W55958259 cites W2080639515 @default.
W55958259 cites W2081638226 @default.
W55958259 cites W2085307511 @default.
W55958259 cites W2088966640 @default.
W55958259 cites W2089218510 @default.
W55958259 cites W2091403769 @default.
W55958259 cites W2092104789 @default.
W55958259 cites W2096657295 @default.
W55958259 cites W2100790734 @default.
W55958259 cites W2100837269 @default.
W55958259 cites W2116711648 @default.
W55958259 cites W2122883220 @default.
W55958259 cites W2128792199 @default.
W55958259 cites W2133124453 @default.
W55958259 cites W2139548754 @default.
W55958259 cites W2140661114 @default.
W55958259 cites W2156185468 @default.
W55958259 cites W2170331239 @default.
W55958259 cites W2328477578 @default.
W55958259 cites W2329193471 @default.
W55958259 cites W2331701350 @default.
W55958259 cites W2403235282 @default.
W55958259 cites W2419636384 @default.
W55958259 cites W24291559 @default.
W55958259 cites W4248137658 @default.
W55958259 cites W4293247451 @default.
W55958259 cites W85529956 @default.
W55958259 doi "https://doi.org/10.1182/blood.v96.5.1933" @default.
W55958259 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/10961897" @default.
W55958259 hasPublicationYear "2000" @default.
W55958259 type Work @default.
W55958259 sameAs 55958259 @default.
W55958259 citedByCount "89" @default.
W55958259 countsByYear W559582592012 @default.
W55958259 countsByYear W559582592013 @default.
W55958259 countsByYear W559582592014 @default.
W55958259 countsByYear W559582592015 @default.
W55958259 countsByYear W559582592016 @default.
W55958259 countsByYear W559582592019 @default.
W55958259 crossrefType "journal-article" @default.
W55958259 hasAuthorship W55958259A5040777952 @default.
W55958259 hasAuthorship W55958259A5047674033 @default.
W55958259 hasAuthorship W55958259A5076077834 @default.
W55958259 hasAuthorship W55958259A5081028472 @default.
W55958259 hasAuthorship W55958259A5083668977 @default.
W55958259 hasAuthorship W55958259A5084729483 @default.
W55958259 hasAuthorship W55958259A5088789978 @default.
W55958259 hasConcept C125418893 @default.
W55958259 hasConcept C170493617 @default.
W55958259 hasConcept C184235292 @default.
W55958259 hasConcept C190283241 @default.
W55958259 hasConcept C2778729363 @default.
W55958259 hasConcept C29537977 @default.
W55958259 hasConcept C42362537 @default.
W55958259 hasConcept C43907098 @default.
W55958259 hasConcept C502942594 @default.
W55958259 hasConcept C55493867 @default.
W55958259 hasConcept C62112901 @default.
W55958259 hasConcept C62478195 @default.