2012
DOI: 10.1016/j.celrep.2012.09.012
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The GPS Motif Is a Molecular Switch for Bimodal Activities of Adhesion Class G Protein-Coupled Receptors

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Cited by 23 publications
(64 citation statements)
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References 28 publications
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“…It is required for cleavage of aGPCR pro-receptor molecules and mediates noncovalent reassociation of the cleaved fragments (Arac et al, 2012). However, GPS cleavage is dispensable for aGPCR function and the consensus GPS sequence is frequently lost in individual aGPCR homologs (Pr€ omel et al, 2012). Thus, the physiological relevance of GPS cleavage and the functional difference between cleavable versus noncleavable aGPCR have remained controversial to date.…”
Section: Gpr111 and Gpr115 Are Not Autoproteolyzed At The Gps Motifmentioning
confidence: 99%
See 1 more Smart Citation
“…It is required for cleavage of aGPCR pro-receptor molecules and mediates noncovalent reassociation of the cleaved fragments (Arac et al, 2012). However, GPS cleavage is dispensable for aGPCR function and the consensus GPS sequence is frequently lost in individual aGPCR homologs (Pr€ omel et al, 2012). Thus, the physiological relevance of GPS cleavage and the functional difference between cleavable versus noncleavable aGPCR have remained controversial to date.…”
Section: Gpr111 and Gpr115 Are Not Autoproteolyzed At The Gps Motifmentioning
confidence: 99%
“…We have used this strategy to systematically uncover the requirement of conserved protein domains in the N terminus of the latrophilin-type aGPCR LAT-1 (Vakonakis et al, 2008;Langenhan et al, 2009). Using this approach, we have recently shown that cleavage at the GPS motif is not necessary for activity of LAT-1 in development and fertility, that the ''splitpersonality'' hypothesis, the ambiguous pairing of cleaved N-and C-terminal subunits of different aGPCR (Silva et al, 2009), is not required for LAT-1 function in the worm, and that two different signal activities are relayed through the LAT-1 receptor (Pr€ omel et al, 2012). In addition to dissecting molecular dependencies of aGPCR signals, the worm also permits analysis of genetic interactions for the two invertebrate aGPCR groups, latrophilins and Flamingo/CELSR, under physiological conditions.…”
Section: Introductionmentioning
confidence: 99%
“…We demonstrated that the receptor is activated by a 13 amino acid short intrinsic sequence located in the extracellular N terminus. Based on several lines of experimental evidence 14 we speculate that this intrinsic activation occurs by structural changes within the receptor upon binding to a yet unknown extracellular agonist and interaction of this sequence with the 7 transmembrane region (Fig. 2).…”
Section: Lat-1 Mediates a G S Protein/adenylyl Cyclase/ Camp Signal Umentioning
confidence: 99%
“…18 Our previous analyses revealed that the receptor mediates its function in spindle orientation via a signaling mode depending on its 7 transmembrane domain suggesting a classical GPCR signal involving heterotrimeric G proteins. 6,14 To address this question we employed an in vitro assay system based on heterologous expression of lat-1 and observed functional G-protein coupling of the receptor to the 3 major G proteins G s , G q and G i by measuring second messengers. Due to the high conservation of these G proteins among metazoan species 19 heterologous coupling of these to the nematode receptor is possible.…”
Section: Lat-1 Mediates a G S Protein/adenylyl Cyclase/ Camp Signal Umentioning
confidence: 99%
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