The adhesion GPCR latrophilin – a novel signaling cascade in oriented cell division and anterior-posterior polarity

Winkler, Jana Barbro; Prömel, Simone

doi:10.1080/21624054.2016.1170274

Cited by 6 publications

(3 citation statements)

References 32 publications

(36 reference statements)

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“…Although TENs and LPHNs are co-expressed and have key roles during embryogenesis, the role of the TEN/LPHN interaction in embryonic development has not been studied. LPHNs were reported to mediate embryogenesis in C. elegans by modulating intracellular cAMP levels (Winkler and Promel, 2016), prompting us to test whether human TEN binding to LPHN also induces trans-cellular cAMP signaling. We established a cAMP-based signaling assay for LPHN1 or LPHN-3 in mammalian cells (Figure 4D–E and Figure S7A–F), and used it as a readout to monitor receptor activity.…”

Section: Resultsmentioning

confidence: 99%

“…Similar to TENs, LPHNs are also conserved between vertebrates and invertebrates, have broad expression patterns, and are involved in embryogenesis (Langenhan et al, 2009; Muller et al, 2015; Scholz et al, 2015). In both C. elegans and Drosophila , LPHN was suggested to act in development by modulating cAMP levels (Scholz et al, 2017; Winkler and Promel, 2016). Considering that cAMP regulates diverse cellular functions including migration, adhesion and differentiation, our results suggest a role for the TEN-LPHN interaction and the subsequent modulation of cAMP levels in various contexts, including development.…”

Section: Discussionmentioning

confidence: 99%

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Structural Basis for Teneurin Function in Circuit-Wiring: A Toxin Motif at the Synapse

Shalev-Benami

Sando

et al. 2018

Cell

113

248

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Teneurins (TENs) are cell-surface adhesion proteins with critical roles in tissue development and axon guidance. Here, we report the 3.1-Å cryoelectron microscopy structure of the human TEN2 extracellular region (ECR), revealing a striking similarity to bacterial Tc-toxins. The ECR includes a large β barrel that partially encapsulates a C-terminal domain, which emerges to the solvent through an opening in the mid-barrel region. An immunoglobulin (Ig)-like domain seals the bottom of the barrel while a β propeller is attached in a perpendicular orientation. We further show that an alternatively spliced region within the β propeller acts as a switch to regulate trans-cellular adhesion of TEN2 to latrophilin (LPHN), a transmembrane receptor known to mediate critical functions in the central nervous system. One splice variant activates trans-cellular signaling in a LPHN-dependent manner, whereas the other induces inhibitory postsynaptic differentiation. These results highlight the unusual structural organization of TENs giving rise to their multifarious functions.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Structural Basis for Teneurin Function in Circuit-Wiring: A Toxin Motif at the Synapse

Shalev-Benami

Sando

et al. 2018

Cell

113

248

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“…Thus, exogenous Stachel peptide caused a pertussis toxin-sensitive decrease in cAMP levels (Nazarko et al, 2018). By contrast, NTF ligands usually increase cAMP levels (Figure 1C, left) [e.g., after activation of LAT-1 by its endogenous ligand in Caenorhabditis elegans (Winkler and Prömel, 2016) or activation of rat LPHN1 expressed in COS7 cells by LTX (Lelianova et al, 1997)]. Also, the NTF-CTF complex did not bind Gαi in pull-down experiments (while Gαs was not tested) (Rahman et al, 1999).…”

Section: Signalingmentioning

confidence: 99%

Catching Latrophilin With Lasso: A Universal Mechanism for Axonal Attraction and Synapse Formation

Ushkaryov

Lelianova

Vysokov³

2019

Front. Neurosci.

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Latrophilin-1 (LPHN1) was isolated as the main high-affinity receptor for α-latrotoxin from black widow spider venom, a powerful presynaptic secretagogue. As an adhesion G-protein-coupled receptor, LPHN1 is cleaved into two fragments, which can behave independently on the cell surface, but re-associate upon binding the toxin. This triggers intracellular signaling that involves the Gαq/phospholipase C/inositol 1,4,5-trisphosphate cascade and an increase in cytosolic Ca 2+ , leading to vesicular exocytosis. Using affinity chromatography on LPHN1, we isolated its endogenous ligand, teneurin-2/Lasso. Both LPHN1 and Ten2/Lasso are expressed early in development and are enriched in neurons. LPHN1 primarily resides in axons, growth cones and presynaptic terminals, while Lasso largely localizes on dendrites. LPHN1 and Ten2/Lasso form a trans-synaptic receptor pair that has both structural and signaling functions. However, Lasso is proteolytically cleaved at multiple sites and its extracellular domain is partially released into the intercellular space, especially during neuronal development, suggesting that soluble Lasso has additional functions. We discovered that the soluble fragment of Lasso can diffuse away and bind to LPHN1 on axonal growth cones, triggering its redistribution on the cell surface and intracellular signaling which leads to local exocytosis. This causes axons to turn in the direction of spatio-temporal Lasso gradients, while LPHN1 knockout blocks this effect. These results suggest that the LPHN1-Ten2/Lasso pair can participate in long- and short-distance axonal guidance and synapse formation.

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Identification of two novel chicken GPR133 variants and their expression in different tissues

Tian

Xiao

Zhang

et al. 2017

Funct Integr Genomics

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GPR133 (G protein-coupled receptor 133) plays significant roles in various physiological processes. Alternatively splicing (AS) variants of GPR133 in many species have been predicted in multiple databases, but there is no available information about the AS events of chicken GPR133 (cGPR133). In the present study, two chicken GPR133 variants, cGPR133-va and cGPR133-vb, were identified by a combination of reverse transcription PCR (RT-PCR) and rapid amplification of cDNA 5'-ends (5' RACE). Sequence analysis shows that cGPR133-va and cGPR133-vb are resulting from different AS modules and their sequences are predicted to encode two distinct putative proteins, respectively. Quantitative real-time PCR (qRT-PCR) analysis revealed that cGPR133-va and cGPR133-vb are widely expressed in different tissues, while exhibiting specific expression profile. Altogether, our results first demonstrate the existence of novel cGPR133 variants and illustrate its transcriptional diversity and their widespread distribution, which provides a foundation for the further research of GPR133.

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The adhesion GPCR latrophilin – a novel signaling cascade in oriented cell division and anterior-posterior polarity

Cited by 6 publications

References 32 publications

Structural Basis for Teneurin Function in Circuit-Wiring: A Toxin Motif at the Synapse

Structural Basis for Teneurin Function in Circuit-Wiring: A Toxin Motif at the Synapse

Catching Latrophilin With Lasso: A Universal Mechanism for Axonal Attraction and Synapse Formation

Identification of two novel chicken GPR133 variants and their expression in different tissues

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