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1 aIota, remained stable in subjects receiving sargramostim.
2 mumab, 10 mg/kg, intravenously on day 1 plus sargramostim, 250 mug subcutaneously, on days 1 to 14 of
3 load excluded any 0.5 log10 increase due to sargramostim (95% confidence interval, -0.68 to 0.44).
4 sargramostim and filgrastim were superior to sargramostim alone for the mobilization of CD34(+) cells
5 s of filgrastim, sargramostim, or sequential sargramostim and filgrastim on CD34(+) cell yields and m
6 oncluded that filgrastim alone or sequential sargramostim and filgrastim were superior to sargramosti
7 ints in the CDAI score on day 57 between the sargramostim and placebo groups (54 percent vs. 44 perce
9 lgrastim (n = 51), sargramostim (n = 52), or sargramostim for 5 days followed by filgrastim (n = 53)
10 acrophage colony-stimulating factor (GM-CSF; sargramostim) for malignant liver tumors, predominantly
13 f remission were significantly higher in the sargramostim group than in the placebo group on day 29 o
14 However, significantly more patients in the sargramostim group than in the placebo group reached the
15 8%-54.4%) of patients in the ipilimumab plus sargramostim group vs 58.3% (95% CI, 49.0%-67.2%) of pat
16 ctions and bone pain were more common in the sargramostim group, and three patients in this group had
21 e randomized to receive filgrastim (n = 51), sargramostim (n = 52), or sargramostim for 5 days follow
23 dy was to compare the effects of filgrastim, sargramostim, or sequential sargramostim and filgrastim
25 e active Crohn's disease to receive 6 mug of sargramostim per kilogram per day or placebo subcutaneou
26 gs for the secondary end points suggest that sargramostim therapy decreased disease severity and impr
29 IV melanoma, treatment with ipilimumab plus sargramostim vs ipilimumab alone resulted in longer OS a
30 n OS as of December 2012 for ipilimumab plus sargramostim was 17.5 months (95% CI, 14.9-not reached)
32 The 1-year survival rate for ipilimumab plus sargramostim was 68.9% (95% CI, 60.6%-85.5%) compared to
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