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2 sponse rates in breast cancer with high-dose megestrol acetate (MA) 800 mg/d, this phase II trial ass
4 utethimide (AG) and hydrocortisone (HC) plus megestrol acetate (MA) improved response rates, response
6 to receive either dexamethasone 0.75 mg qid, megestrol acetate 800 mg orally every day, or fluoxymest
7 cancer patients were randomized to (1) oral megestrol acetate 800 mg/d liquid suspension plus placeb
10 ], 0.75 to 1.24) for anastrozole 1 mg versus megestrol acetate and 0.92 (97.5% CI, 0.71 to 1.19) for
12 hoice for treating cancer anorexia/cachexia, megestrol acetate and dexamethasone have similar appetit
13 owth hormone, testosterone, oxandrolone, and megestrol acetate and emerging data on the orexigenic pe
14 ential of combining natural supplements with megestrol acetate and found that the addition of the nat
15 relevant benefit, letrozole is equivalent to megestrol acetate and should be considered for use as an
17 eneration aromatase inhibitors have replaced megestrol acetate as second-line hormonal therapy in rec
18 e first time that the anti-tumor activity of megestrol acetate can be enhanced by combining with pter
20 e potential application of pterostilbene and megestrol acetate combination for the treatment of endom
24 nastrozole 10-mg group, and 20 (7.9%) in the megestrol acetate group had a complete or partial respon
26 patients in the anastrozole groups than the megestrol acetate group; the difference between the anas
27 difference between the anastrozole 10 mg and megestrol acetate groups was significant (P = .005).
33 daily, is well tolerated and as effective as megestrol acetate in the treatment of postmenopausal wom
35 ial was formulated to evaluate the impact of megestrol acetate on quality of life, toxicity, response
36 eive second-line hormone therapy with either megestrol acetate or an aromatase inhibitor (fadrozole o
38 natural phenolic compound, pterostilbene, to megestrol acetate resulted in a synergistic inhibition o
40 occurred more often in patients who received megestrol acetate versus placebo (9% v 2%, P = .01).
43 h-dose progestin treatment of breast cancer (megestrol acetate) also increase VEGF in the media of cu
44 steroids (eg, growth hormone, testosterone, megestrol acetate) in malnutrition and other catabolic s
45 (progesterone, medroxyprogesterone acetate, megestrol acetate, mifepristone, pregnanediol, 17alpha-h
46 double-blind for anastrozole, open-label for megestrol acetate, parallel-group, multicenter trials we
47 rel, cyproterone acetate, norethindrone, and megestrol acetate, were found to be only weak stimulator
48 n improvement in quality of life (QOL) among megestrol acetate-treated and combination-treated patien
56 sease with botulinum toxin; weight loss with megestrol acetate; and sialorrhea with glycopyrollate.
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