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1 n 185 is surrounded by other residues and is volume sensitive.
2 Taken together, these findings indicate that volume-sensitive activation of PI 3-kinase and the gener
3             We conclude that bestrophins are volume sensitive and that they could play a novel role i
4  is concluded that activity of the beta-cell volume-sensitive anion channel can be modulated by chang
5 lular adenine nucleotides on activity of the volume-sensitive anion channel in single, isolated rat p
6 s were used to investigate the expression of volume-sensitive anion channels in acinar cells isolated
7  an absolute requirement for the activity of volume-sensitive anion channels in rat lacrimal gland ac
8 ments in DCFS precluded glutamate release by volume-sensitive anion channels, P2X7 purinergic recepto
9                                            A volume-sensitive anion conductance was observed when cel
10 ory activity and may involve activation of a volume-sensitive anion conductance.
11                                              Volume-sensitive anion conductances were observed in bot
12 dynamic changes in cell volume, resulting in volume-sensitive channel activation, and efflux of cytos
13               Our observations indicate that volume-sensitive channel may constitute a previously unc
14 t p38 negatively modulates the set point for volume-sensitive channel opening.
15           The effect of noradrenaline on the volume-sensitive chloride current (I(Cl(swell))) was stu
16 been implicated in several tissues as a cell-volume-sensitive Cl(-) channel.
17                     It is concluded that the volume-sensitive Cl- conductance in ROS 17/2.8 cells is
18     The effects of arachidonic acid upon the volume-sensitive Cl- current present in cultured osteobl
19                                          The volume-sensitive conductance was permeable to Na(+) appr
20                                 Of these two volume-sensitive conductances, L-alanine elicited a spec
21 ibited by wortmannin or LY294002 and because volume-sensitive current activation was inhibited by int
22 ermine possible molecular candidates for the volume-sensitive current.
23 ivator, MEK-6, which substantially inhibited volume-sensitive currents.
24 e that H2O2 strongly up-regulates astrocytic volume-sensitive EAA release via a CaMKII-dependent mech
25                                          The volume-sensitive glutamine transport process features ch
26                 These findings indicate that volume-sensitive increases in p60(c-src) and/or related
27 ast five distinct Cl- channels; a ClCO-like, volume-sensitive, inward rectifying, Ca2+-activated and
28 of hepatocytes and other epithelia activates volume-sensitive ion channels that facilitate fluid and
29 motic gradients and cellular volume requires volume-sensitive ion channels.
30 eads to fluid and electrolyte efflux through volume-sensitive K(+) and Cl(-) channels.
31                                              Volume-sensitive K+ influxes in high potassium-containin
32 n a volume-dependent manner and so regulates volume-sensitive K+ transport.
33                                      A Cl(-)/volume-sensitive kinase has been proposed to coordinatel
34 integral component of the long-sought "Cl(-)/volume-sensitive kinase" of the cation-Cl(-) cotransport
35 plicating it as (one of) the long-sought Cl-/volume-sensitive kinase(s).
36  represent an important target for modifying volume-sensitive liver functions.
37           To determine whether IK1 underwent volume-sensitive localization, we expressed a green fluo
38 er (VSOR) anion channel, also referred to as volume-sensitive organic osmolyte-anion channel (VSOAC),
39 sed as a molecular candidate responsible for volume-sensitive osmolyte and anion channels (VSOACs) in
40    Short ClC3 isoform (sClC3) functions as a volume-sensitive outwardly rectifying anion channel (VSO
41 tween endogenous ClC-3 expression and native volume-sensitive outwardly rectifying anion channels (VS
42 is increase does not stem from activation of volume-sensitive P2 receptors.
43 ose of these studies was to evaluate whether volume-sensitive tyrosine kinases mediate cell volume in

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