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1                                              2ME induced apoptosis in these cells in a dose-dependent
2                                              2ME(2) also suppresses osteoclast differentiation and in
3                                              2ME(2) inhibited tumor growth in soft tissue, metastasis
4 PbI(3) exhibits 10x higher solubility in 30% 2ME in GBL than in 2ME alone and 40% higher solubility t
5                    Equivalent binding of [3H]2ME occurred when the drug was added to preformed polyme
6 ded to preformed polymer, but binding of [3H]2ME to polymer was not readily inhibited by colchicine s
7                   Significant amounts of [3H]2ME were also incorporated into microtubule polymer form
8 el protofilaments, increasing amounts of [3H]2ME were incorporated into polymer, reaching near-stoich
9                                      The [3H]2ME binds avidly to tubulin even on ice, and it is readi
10  We have now examined interactions of [4-3H]-2ME with unpolymerized tubulin and polymer.
11                                     Although 2ME(2) significantly reduced tumor growth at late stages
12                            However, although 2ME(2) reduced the number of MIN lesions in the preventi
13 gic or genetic (e.g. siRNA) means attenuated 2ME-induced mitochondrial injury, XIAP and Mcl-1 downreg
14 action rate is observed for the bifunctional 2ME (4 abstraction positions) over n-butanol (5 abstract
15  the response to oxidative stress induced by 2ME.
16 t Id-1 expression is negatively regulated by 2ME(2), which may be an additional mechanism for the ant
17                                  Conversely, 2ME lethality was potentiated by the phosphatidylinosito
18 o these differences in apparent affinity for 2ME are unknown, but presumably interaction of the estro
19                                 However, for 2ME the energy barriers increase in the order alpha < be
20 gen receptors (ERs) as molecular targets for 2ME(2).
21 gy and accelerated tumor growth may occur if 2ME(2) is administered in a prevention setting for prolo
22  higher solubility in 30% 2ME in GBL than in 2ME alone and 40% higher solubility than in GBL alone at
23 ecyl sulfate (SDS) and beta-mercaptoethanol (2ME), suggesting the recognition of nonlinear or conform
24                          2-Methoxyestradiol (2ME(2)) is an endogenous metabolite of 17beta-estradiol
25                          2-Methoxyestradiol (2ME(2)), a metabolite of 17-beta-estradiol, inhibits ang
26                          2-Methoxyestradiol (2ME(2)), a physiologic metabolite of 17beta-estradiol (e
27                          2-Methoxyestradiol (2ME) is an endogenous mammalian catabolite of estradiol
28           The effects of 2-Methoxyestradiol (2ME)-induced apoptosis was examined in human leukemia ce
29  oxidation of bifunctional 2-Methoxyethanol (2ME) biofuel using methyl radical was introduced.
30 ma-butyrolactone (GBL) and 2-methoxyethanol (2ME), a phenomenon where FAPbI(3) shows higher solubilit
31 ear-stoichiometry with tubulin at 100 microM 2ME.
32 ot inhibit the antiproliferative activity of 2ME(2).
33 sts, and we demonstrate that the affinity of 2ME(2) for ERbeta is even lower.
34 l mechanism for the antiangiogenic effect of 2ME(2).
35 analyzed the tumor stage-specific effects of 2ME(2) in the C3(1)/Tag transgenic mouse model for breas
36 ese findings suggest a hierarchical model of 2ME-related apoptosis induction in human leukemia cells
37 iferative activity of ICI 182,780 but not of 2ME(2).
38 ce for various channels for the oxidation of 2ME was studied at density function theory (M06-2X) and
39 f organic compounds, from different sites of 2ME were examined.
40  active myristolated Akt construct prevented 2ME-mediated mitochondrial injury, XIAP and Mcl-1 downre
41  was significantly reduced in mice receiving 2ME(2).
42                         In the latter study, 2ME(2) (10, 25, and 50 mg/kg/d) treatment began on the s
43         Our data support the conclusion that 2ME(2) could be an important new therapy in the arsenal
44                              We confirm that 2ME(2) has a lower binding affinity for ERalpha as compa
45     Collectively, these results suggest that 2ME(2) is distinct among estradiol metabolites because o
46                                     In vitro 2ME(2) inhibits a large variety of tumor and nontumor ce
47                                    In vitro, 2ME(2) repressed osteoclast number by inducing apoptosis
48 these observations, we have examined whether 2ME(2) could effectively target metastasis to bone, oste
49 ose of this study was to investigate whether 2ME(2) is able to engage ERs as an agonist and whether i
50 enzyme inhibitor, at concentrations at which 2ME(2) interacts with ERalpha in an in vitro binding ass
51 s induction in human leukemia cells in which 2ME-induced oxidative injury represents a primary event
52  cystic tumor formation in mice treated with 2ME(2) at early ages are consistent with an impaired ang
53 ption of the hydrogen bonding network within 2ME, allowing its hydroxyl and ether groups to interact