ライフサイエンスコーパス: ligand stimulation

1 e promote their rapid interactions only upon ligand stimulation.

2 recruited independently to IL-1R1 following ligand stimulation.

3 to induce Erk phosphorylation in response to ligand stimulation.

4 ted in dissociated sympathetic neurons after ligand stimulation.

5 lated on tyrosine residues in the absence of ligand stimulation.

6 tle colocalization was observed after 4 h of ligand stimulation.

7 NF receptor-associated factor 2 (TRAF2) upon ligand stimulation.

8 h components of the ERK1/2 cascade following ligand stimulation.

9 cAMP response and Erk phosphorylation after ligand stimulation.

10 enhanced activation of EGFR signalling upon ligand stimulation.

11 stitutive complexes that are not affected by ligand stimulation.

12 ty to produce IL-12p70 after subsequent CD40 ligand stimulation.

13 recruited to TLR2 signalling complexes after ligand stimulation.

14 a (TGF-beta) receptors are internalized upon ligand stimulation.

15 m endogenous arachidonic acid in response to ligand stimulation.

16 ore than doubled the sensitivity of cells to ligand stimulation.

17 ne proteins translocate to the nucleus after ligand stimulation.

18 ptors and translocated into the nucleus upon ligand stimulation.

19 blot analysis and immunoprecipitation after ligand stimulation.

20 and recruited to the CD40 receptor upon CD40 ligand stimulation.

21 pathways can be conditionally activated upon ligand stimulation.

22 d degradation of the receptor in response to ligand stimulation.

23 th the C-terminal Src kinase (CSK) following ligand stimulation.

24 ated with Stat1 but not Stat2 or Stat3 after ligand stimulation.

25 ors of transcription 5 (STAT5) activation on ligand stimulation.

26 localization, and reduced responsiveness to ligand stimulation.

27 e activated in normal neurons in response to ligand stimulation.

28 tional mode of signal transduction following ligand stimulation.

29 n and are differentially regulated by ephrin ligand stimulation.

30 eceptor Smoothened in the primary cilia upon ligand stimulation.

31 activities, particularly in the presence of ligand stimulation.

32 GF-B signaling that is rapidly degraded upon ligand stimulation.

33 otch1 in presence of myocardin or by Jagged1 ligand stimulation.

34 gulate their signaling output in response to ligand stimulation.

35 ce of ephrin-A ligands and is disrupted upon ligand stimulation.

36 that initiate signal cascades in response to ligand stimulation.

37 as variable responsiveness to exogenous Wnt ligand stimulation.

38 amily receptor signaling in conjunction with ligand stimulation.

39 ion of type I IFNs and IL12p40 following TLR ligand stimulation.

40 and independent of adaptation to persistent ligand stimulation.

41 ownstream cytokine expression in response to ligand stimulation.

42 re defective in cytokine production upon RLR ligand stimulation.

43 phorylated, ubiquitinated, and degraded upon ligand stimulation.

44 somes and lysosome-mediated degradation upon ligand stimulation.

45 elective and undergoes dynamic regulation by ligand stimulation.

46 the activation of T cells via specific notch ligand stimulation.

47 and degraded in the lysosome upon long-term ligand stimulation.

48 erleukin-8 and MCP-1 in response to specific ligand stimulation.

49 d intranuclear mobility especially following ligand stimulation.

50 ivation events in response to membrane-bound ligand stimulation.

51 th an activated TGFbeta receptor and TGFbeta ligand stimulation.

52 ignal-regulated kinase ERK1 and -2 following ligand stimulation.

53 esses and inhibits the activity of MAPK upon ligand stimulation.

54 nuclear Smad3 was a more precise outcome of ligand stimulation.

55 ed protein kinase activation is sustained on ligand stimulation.

56 lation in response to constant extracellular ligand stimulation.

57 epidermal growth factor or heregulin (a HER3 ligand) stimulation.

58 mplexes of Lyn-Cbl and Cbl-p85 exist without ligand stimulation, (2) upon ligand binding, Lyn becomes

59 R) can lead to cell transformation, and with ligand stimulation, a broader spectrum of phosphorylated

60 Upon ligand stimulation, a fragment of Notch is released prot

61 pathway activity specifically in response to ligand stimulation--a process that involves endocytic tr

62 re transcription sites, indicating that upon ligand stimulation, AhR is recruited to active transcrip

63 accumulate at or are depleted from points of ligand stimulation along the axons.

64 ion by desensitizing Met signaling following ligand stimulation and by eliminating potentially oncoge

65 ithin an embryonic epithelial sheet by local ligand stimulation and coordinates a long-range contract

66 l maturation of LSECs can be achieved by TLR ligand stimulation and elucidated the mechanisms involve

67 sought to characterize pathway targets using ligand stimulation and genetic models of activation.

68 Also, severe oxidative stress (unlike ligand stimulation and moderate oxidative stress, both o

69 orms, with PKCtheta being more responsive to ligand stimulation and PKCalpha/beta to growth-factor av

70 maturation exclusively in response to TLR1/2 ligand stimulation and that the immunological status of

71 lice variant of NRP2 becomes sumoylated upon ligand stimulation and translocates to the inner nuclear

72 ncreasing ESR1 protein cellular content upon ligand stimulation and upregulated the expression of est

73 -derived growth factor (PDGF) receptor after ligand stimulation, and binding of SHPTP2 to this recept

74 ate microtiter plates, one for cell culture, ligand stimulation, and cell lysis/receptor solubilizati

75 and dephosphorylated receptor in response to ligand stimulation, and that this may be a general mecha

76 gammaR each form discrete nanoclusters after ligand stimulation, and their synergistic co-activation

77 In response to membrane-bound ligand stimulation, antigen aggregation occurs in B cell

78 After ligand stimulation, approximately 60-70% of transfected

79 e plasma membrane and is overactivated after ligand stimulation because of destabilization and degrad

80 ion and release in response to TLR4 and TLR2 ligand stimulation but not for TLR-independent stimuli.

81 growth, and slow their cell cycle following ligand stimulation but show increased cellular migration

82 creases in effector activity after 15 min of ligand stimulation, but only the serine phosphorylation

83 is not phosphorylated by MET in response to ligand stimulation, but rather to increasing levels of M

84 diated innate immunity due to inadequate Wnt ligand stimulation by monocytes provides an additional m

85 ution of the AhR/ARNT complex in response to ligand stimulation, by using live-cell confocal and high

86 which rapidly attenuate signals elicited by ligand stimulation, causing desensitization.

87 At low levels of receptor and UCP2, ligand stimulation creates a distinct temporal response

88 Upon ligand stimulation, epidermal growth factor receptor (EG

89 to MyD88 in mouse macrophages following TLR7 ligand stimulation, highlighting species-specific differ

90 After PPARgamma ligand stimulation, HMGA1 and PPARgamma were recruited t

91 ative stability of IGF-IR in the presence of ligand stimulation, IGF-IR ubiquitination sites have yet

92 This mutant receptor fails to respond to ligand stimulation, implicating the GREAT gene in the et

93 f the HERP family, HERP1, was not induced by ligand stimulation in any cells tested, leading to the s

94 rmal growth factor receptor (EGFR) following ligand stimulation in breast and lung cancer cells.

95 dings indicate that EGFR does not respond to ligand stimulation in M phase and suggest that a negativ

96 g, conditional deletion, mosaic analysis and ligand stimulation in mice to determine that both villou

97 e studies suggest a role for continuous self-ligand stimulation in the periphery for the maintenance

98 eraction partners of endogenous NOTCH2 after ligand stimulation in the presence of a gamma-secretase

99 s were hyper-responsive to anti-IgM and TLR7 ligand stimulation in vitro and produced high concentrat

100 he ALK1 pathway and respond robustly to ALK1 ligand stimulation in vitro.

101 be up-regulated by chemokine CXCL13 and CD40 ligand stimulation in wild-type B cells, elevation of ly

102 ulations of receptors as soon as 1 min after ligand stimulation, indicating early diversification of

103 Rgamma, increased activation was observed by ligand stimulation, indicating that both PPARgamma-depen

104 Ligand stimulation induced phosphorylation of cortactin

105 oughout receptor internalization, direct EGF ligand stimulation initiates the internalization of EGFR

106 - and hetero-oligomers both before and after ligand stimulation is controversial.

107 oop may contribute to the mechanism by which ligand stimulation is coupled to discrete biological res

108 way by which arachidonate released following ligand stimulation is made available only to prostagland

109 at tonic T cell receptor signaling from self-ligand stimulation is required to maintain a basal state

110 let-derived growth factor receptor ECD, upon ligand stimulation, is coupled to its intracellular doma

111 with lipid rafts in the apparent absence of ligand stimulation, it has been proposed that raft-assoc

112 Our results provide evidence that ligand stimulation leads to internalization of the insul

113 After ligand stimulation, many G protein-coupled receptors (GP

114 induced by both mechanical LIS and chemical ligand stimulation may determine downstream signaling ch

115 In agreement with this, ligand stimulation of ALK7 suppressed POX and KLF15 expr

116 t was less responsive to H3 relaxin based on ligand stimulation of cAMP production.

117 Data herein show that ligand stimulation of cells that express both the EGFR a

118 In contrast, CD95 ligand stimulation of cells unable to internalize CD95 r

119 ponses to provocative stimulation, including ligand stimulation of cultured cardiomyocytes, pressure

120 1R) inhibitors had a synergistic effect, and ligand stimulation of EGFR and MET rescued DDR2-mutant l

121 Herein, we demonstrate that ligand stimulation of EphA2 promotes the nucleus translo

122 The results show that ligand stimulation of Flt3 can induce association of SOC

123 Ligand stimulation of fTie1 resulted in Tie1 autophospho

124 f Cl- flux reflected selective disruption of ligand stimulation of GCC rather than the chloride chann

125 Ligand stimulation of IGF1R promotes its clathrin-depend

126 taurosporine treatment of HeLa cells and Fas ligand stimulation of Jurkat cells.

127 ucts is not reduced by DEP or PAHs following ligand stimulation of macrophages or fibroblasts.

128 It is also well established that ligand stimulation of many plasma membrane receptors lea

129 Instead, ligand stimulation of mGluR5 caused a dynamic transactiv

130 By contrast, ligand stimulation of non-overexpressed ERBB2 transientl

131 e mechanism of signal transmission following ligand stimulation of receptor tyrosine kinases in livin

132 o differed between AngII and beta-arr-biased ligand stimulation of receptors and between azF-labeled

133 s EGFR-dependent phosphorylation of RON, but ligand stimulation of RON does not trigger EGFR phosphor

134 These observations indicate that ligand stimulation of RTKs is not generic, and point to

135 xpressing RAGEv1 in tumor cells altered RAGE ligand stimulation of several novel classes of genes tha

136 in 293T and NIH 3T3 cells demonstrated that ligand stimulation of several RPTKs (epidermal growth fa

137 tic cell, G proteins in the Gq family couple ligand stimulation of the m1 muscarinic receptor to acti

138 timulates a similar Ca2+ transient as native ligand stimulation of the naive precursors, consistent w

139 Upon ligand stimulation of the receptors, Jaks are activated

140 Moreover, altered peptide ligand stimulation of the Th1 line stimulates a similar

141 In particular, ephrin-A ligand stimulation of tumor cells induces EphA2 receptor

142 ivation of signaling pathways in response to ligand stimulation of upstream cell surface receptors.

143 stimulation of Eph-B4 signaling, either via ligand stimulation or expression of a constitutively act

144 ibited genotype selection under RTK-targeted ligand stimulation or pharmacologic inhibition in vitro.

145 or ATPgammaS effectively sensitized GC-A to ligand stimulation over prolonged periods of time in eit

146 On EGFR ligand stimulation, phosphorylation of PLCgamma-1 increa

147 Following ligand stimulation, phosphorylation of specific tyrosyl

148 Ligand stimulation promoted recruitment of PELP1 to 17be

149 Furthermore, the mutated receptor was, upon ligand-stimulation, quickly internalized and degraded.

150 d cytokine responses to TLR4 ligand and TLR5 ligand stimulation relative to PB DCs, yet similarly pro

151 MP2A induces a heightened sensitivity to TLR ligand stimulation, resulting in increased proliferation

152 Receptor activator for NF-kappaB (RANK) ligand stimulation results in IFN-beta upregulation, whi

153 A proteolytic cascade induced by ligand stimulation results in release of the intracellul

154 Activation of FGFR3, through mutation or ligand stimulation, results in autophosphorylation of mu

155 After Fas ligand stimulation, SB-HCV-infected Molt-4 cells had inc

156 Upon ER Ca(2+) depletion or via ligand stimulation, Sig-1Rs dissociate from BiP, leading

157 to produce large amounts of IL-12 after CD40 ligand stimulation, similar to IL-4 priming of DCs.

158 (InsP3R) channels responding to incremental ligand stimulation, single-channel patch-clamp electroph

159 t down-regulation efficiently in response to ligand stimulation, suggesting that activation of classi

160 ntly delays dephosphorylation of CXCR2 after ligand stimulation, suggesting that clathrin-mediated en

161 and exhibited increased MED1 occupancy upon ligand stimulation, suggesting their involvement in gene

162 Upon ligand stimulation, TGFbeta receptors phosphorylate Smad

163 with the IGF-I receptor (IGF-IR), and after ligand stimulation the association of IGF-IR with Galpha

164 Upon ligand stimulation, the endoplasmic reticulum (ER) prote

165 After ligand stimulation, the internalized CXCR2 colocalized w

166 In this report, we demonstrate that, after ligand stimulation, the PDGF beta receptor (PDGFRbeta) b

167 BR2 and TGFBR1 form a signaling complex upon ligand stimulation, they are expected to be equally impo

168 In contrast, with TLR2 ligand stimulation, TNF-alpha production was reduced, wh

169 addition to receptor activator of NF-kappaB ligand stimulation to initiate greater bone remodeling.

170 phosphorylation in response to non-androgen ligand stimulation using phospho-specific antibodies.

171 ar cytokine production in the absence of TLR ligand stimulation was elevated in cells from older comp

172 The initial response to ligand stimulation was increased and sensitization to re

173 okine production in mast cells following TLR ligand stimulation was markedly reduced by HIF-1alpha kn

174 R signals influence responses to agonist TCR ligand stimulation, we analyzed naive CD4(+) cells expre

175 e the cell populations able to respond to Hh ligand stimulation, we expressed an oncogenic allele of

176 ocyte cytokine production in response to TLR ligand stimulation were associated with PTD but not SGA

177 tor (IR)/IGF-1R is augmented upon respective ligand stimulation, whereas association with STAT3 is co

178 pithelial alphaTN4-1 cells in the absence of ligand stimulation, whereas the mutants exhibited signif

179 nderwent rapid cellular internalization upon ligand stimulation, whereas the TRAIL/DR4 complex was no

180 Thus, LLPS of NLRP6 is a common response to ligand stimulation, which serves to direct NLRP6 to dist

181 The effects can be reversed by ligand stimulation, which triggers the intrinsic tumor s

182 On ligand stimulation with CB agonists, CB receptors induce

183 Ligand stimulation with Sema6A does not change the degre