Effects of deregulated Raf activation on integrin, cytokine-receptor expression and the induction of apoptosis in hematopoietic cells

Abstract: The effects of deregulated Raf activation on the growth and differentiation of hematopoietic cells were investigated. The cytokine-dependent murine myeloid FDC-P1 and human erythroleukemic TF-1 cell lines were transformed to grow in response to deregulated Raf expression in the absence of exogenous cytokines. The conditionally active Raf proteins were regulated by ␤-estradiol as cDNAs containing the Raf catalytic, but lacking negative-regulatory domains, were ligated to the hormone binding domain of the estrog… Show more

“…P-selectin, CINC-2β, and MCP-1 stayed lowered in the estrogen treated rats 24 hours after injury. The decrease in adhesion molecules and chemokines is modulated by estrogen and could be a result of a reduction of cell-surface integrin expression [57], or reductions of oxidative stress [58][59][60].…”

Sex differences and estrogen modulation of the cellular immune response after injury

“…P-selectin, CINC-2β, and MCP-1 stayed lowered in the estrogen treated rats 24 hours after injury. The decrease in adhesion molecules and chemokines is modulated by estrogen and could be a result of a reduction of cell-surface integrin expression [57], or reductions of oxidative stress [58][59][60].…”

Sex differences and estrogen modulation of the cellular immune response after injury

“…[259][260][261] However, when TF-1 cells are stimulated with PMA they are induced to differentiate. [262][263][264] Growth inhibition mediated by PMA may be mediated in part by p21 WAF1 induction 265 and this occurs in the absence of apoptosis. Thus the direct effects of PMA on apoptosis are hard to interpret.…”

Kinases: positive and negative regulators of apoptosis

“…18 Spontaneous factorindependent cells are rarely recovered from this cell line, which makes it an attractive model system to analyze the effects that various oncogenes have on signal transduction and the transition to cytokine independence and leukemogenesis. 7,18,[19][20][21][22][23][24][25][26][27][28][29][30][31][32][33][34] Oncogene-transformed cytokine-independent cells have been obtained after infection/transfection of this cell line. 7 These cytokine-dependent and oncogene-transformed derivative cells represent appropriate tools to screen for novel therapeutic compounds as well as to evaluate their effectiveness in suppressing the growth and differentiation capacity of certain types of leukemias containing various oncogene mutations and chromosomal translocations.…”

“…7,8 N-terminal deleted forms of Raf and MEK1 proteins, which remove the Ras binding domain and the negative regulatory sites in CR1 and CR2 in Raf and the negative regulatory domain of MEK1, result in activated oncoproteins due to the aberrant stimulation of downstream kinases, transcription factors and molecules involved in the prevention of apoptosis. [23][24][25][26][27][28][29][30][31][40][41][42] Conditional Raf and MEK oncogenes were developed by ligation of the 5 0 deleted Raf and MEK cDNAs to the cDNA encoding the hormone binding domain of the estrogen receptor (ER). The activity of the kinases encoded by these cDNAs are dependent upon estrogen (b-estradiol).…”

“…The activity of the kinases encoded by these cDNAs are dependent upon estrogen (b-estradiol). [23][24][25][26][27][28][29][30][31][40][41][42] The ER antagonist, 4-hydroxytamoxifen (4HT) also activates the ER-coupled oncoprotein and does not have the estrogenic effects of b-estradiol that can both promote as well as inhibit growth. Conditional oncoproteins are in some cases better tools to understand the effects of oncogenes on proliferation and apoptosis because once the regulator is taken away, the cells revert to the 'cytokine-dependent' state.…”

Differential effects of kinase cascade inhibitors on neoplastic and cytokine-mediated cell proliferation