We have found that GM-CSF and DMSO have antagonistic effects on the proliferation but not maturation of asynchronously growing HL-60 cells such that growth in the presence of both more closely resembles normal hematopoiesis (Brennan et al., J. Cell Physiol. 132:246, 1987). Studies were undertaken to
Interactions of dimethyl sulfoxide and granulocyte-macrophage colony-stimulating factors on the growth and maturation of HL-60 cells
โ Scribed by J. K. Brennan; K. S. Lee; C. N. Abboud; C. L. Erickson-Miller; P. C. Keng
- Publisher
- John Wiley and Sons
- Year
- 1987
- Tongue
- English
- Weight
- 972 KB
- Volume
- 132
- Category
- Article
- ISSN
- 0021-9541
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โฆ Synopsis
We have studied the interactions of dimethyl sulfoxide (DMSO), Giant Cell Tumor (GCT) cell-conditioned medium (GCT CM), and highly purified granulocyte-macrophage colony-stimulating factors (GM-CSF) on t h e growth and maturation of a highly passaged population of HL-60 cells. DMSO produced dose-dependent inhibition of HL-60 growth in liquid and semisolid media. Growth was partially to completely restored by the addition of GCT CM to cultures. Experiments in which cell volume, cell cycle kinetics, tritiated thymidine (3HTdr) incorporation, cell number, and nitroblue tetrazolium (NBT) reduction were compared during culture indicated that DMSO inhibited t h e spontaneous increase in cell volume and flow of cells through t h e cell cycle which occurred in the first day of culture, the increase in 3HTdr incorporation which was detectable by day 2; and the increment in cell counts which occurred by day 3. These effects were opposed by GCT CM. In contrast, t h e DMSO-induced increase in NBT reduction which occurred by day 6 was not influenced by GCT CM. The major principle opposing DMSO was GM-CSF, since (I) highly purified GM-CSF from GCT cells and recombinant GM-CSF from COS cells transfected with the Mo cell GM-CSF gene overcame greater than 50% of DMSO inhibition; and (2) conditioned media from cells not producing CSF, G-CSF from GCT cells, and recombinant G-CSF from Escherichia coli transfected with the G-CSF gene from 5,637 cells were inactive. DMSO had little or no effect on the elaboration of autostimulatory activity by HL-60 cells. DMSO is a useful agent for inhibiting t h e spontaneous growth of HL-60 cells and restoring their deDendence on GM-CSF. a mooertv which mav be mediated through ;he effec'ts of maturation.
I ,
I
DMSO on cell cycle kinetics andlor (DMSO), a potent promoter of granulocytic maturation in lower-passage cells and studied the effects of conditioned media and CSF subsets on their growth and maturation. We have found that DMSO inhibits autonomous HL-60 growth and permits clear delineation of a continuing responsiveness to exogenous GM-CSF which partially to completely restores growth in DMSO-inhibited cultures.
MATERIALS AND METHODS
Culture of HL-60 cells
The HL-60 population, originally obtained from Dr. Robert Gallo's laboratory at the National Cancer Institute in 1979 has been continuously maintained (over 500 passages) in McCoy's 5A medium supplemented with 10% fetal bovine serum, 2 mM HEPES buffer, 100
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