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1 e biological responses via G protein-coupled serpentine receptors.
2 ost chemokine receptors and is rare in other serpentine receptors.
3 , and srd families of seven-transmembrane or serpentine receptors.
4 pression under free-running conditions; (iv) Serpentine receptor 10 (SR10) has a 24 h transcriptional
5 (ER) to prevent maturation of Frizzled (Fz) serpentine receptors and fibroblast growth factor recept
6 nary conservation of the switch mechanism of serpentine receptors and help to constrain models of how
7 rtussis toxin (PTX) is a potent inhibitor of serpentine receptor-associated inhibitory trimeric guani
10 but distinct from, the previously described serpentine receptor class a (sra) family and shows a dif
11 have identified a chemosensory gene family, serpentine receptor class ab (srab), which exists in bot
13 ent chemoattractant for cells expressing the serpentine receptor CMKLR1 (chemokine-like receptor 1),
15 ommunication that is mediated by a family of serpentine receptors containing seven transmembrane doma
16 riety of other chemoattractants that bind to serpentine receptors coupled to heterotrimeric G protein
18 rity in all three systems is mediated by the serpentine receptor Frizzled and a number of additional
21 lassic components of this system include the serpentine receptors, heterotrimeric G-proteins, adenyly
23 rimeric GTP-binding proteins (G-proteins) to serpentine receptors involves several independent contac
24 gnaling through the Frizzled (FZD) family of serpentine receptors is essential for embryogenesis and
25 We show that the mast cell-expressed orphan serpentine receptor mCCRL2 is not required for expressio
27 interaction with receptors, and, in several serpentine receptors, regions similar to those in rhodop
28 ing seven-transmembrane G-protein-coupled or serpentine receptors related to the ODR-10 diacetyl chem
29 that inhibits Hh signaling by targeting the serpentine receptor Smoothened (SMO), has produced promi
32 pressin, angiotensin II, and endothelin bind serpentine receptors that interact with G(q) and activat
34 asmic ends of these two helices in two other serpentine receptors, the beta2-adrenoreceptor and the p
35 nding pockets within the seven-helix core of serpentine receptors, the topography of these binding po
36 eceptor that acts together with the Frizzled serpentine receptor to initiate Wnt signal transduction.
39 e findings show that acquired mutations in a serpentine receptor with features of a G protein-coupled