洞見 - Pharmacology - # β-arrestin Inhibition

A Novel Lipopeptide, ARIP, Derived from the Vasopressin 2 Receptor, Shows Promise as a β-arrestin Inhibitor

核心概念

ARIP, a novel lipidated peptide derived from the C-terminal tail of the vasopressin 2 receptor (V2R), effectively inhibits β-arrestin recruitment to various 7TMRs, showing promise as a new pharmacological tool for studying β-arrestin function.

摘要

Bibliographic Information: Brouillette, R. L., Monac, C. E., Desgagné, M., Hassanzedeh, M., Breault, É., Lussier, F., ... & Sarret, P. (Year). A lipidated peptide derived from the C-terminal tail of the vasopressin 2 receptor shows promise as a new β-arrestin inhibitor. [Journal Name].
Research Objective: This study aimed to develop and characterize a novel β-arrestin inhibitor, ARIP, based on the C-terminal tail of the vasopressin 2 receptor (V2R), and to evaluate its efficacy in inhibiting β-arrestin recruitment to various 7TMRs in vitro and in vivo.
Methodology: The researchers designed and synthesized ARIP, a lipidated phosphomimetic peptide, using standard Fmoc-based solid-phase peptide synthesis. They employed BRET2-based assays in HEK293 cells to assess ARIP's ability to inhibit agonist-induced β-arrestin 1 and 2 recruitment to a panel of five 7TMRs: V2R, CXCR4, APJ, MOPR, and GLP1R. Additionally, they investigated ARIP's potential to recruit β-arrestins directly and its impact on G protein signaling. Molecular modeling studies were conducted to analyze the binding mode of ARIP to β-arrestin 1. Finally, the researchers evaluated ARIP's analgesic effects in vivo using a rat tail-flick test.
Key Findings: ARIP effectively inhibited agonist-induced β-arrestin 1 and 2 recruitment to the selected 7TMRs, albeit with varying efficacies depending on the receptor and β-arrestin subtype. Notably, ARIP did not directly recruit β-arrestins to the cell membrane and did not interfere with G protein signaling. Molecular modeling studies revealed that ARIP binds to β-arrestin 1 similarly to V2Rpp, the phosphorylated peptide derived from V2R. Importantly, intrathecal administration of ARIP potentiated the analgesic effect of morphine in the rat tail-flick test, consistent with β-arrestin inhibition.
Main Conclusions: ARIP represents a promising new pharmacological tool for investigating the roles of β-arrestins in 7TMR signaling and trafficking. Its ability to selectively inhibit β-arrestin recruitment without affecting G protein signaling makes it a valuable tool for dissecting the complex interplay between these signaling pathways.
Significance: The development of ARIP as a selective β-arrestin inhibitor provides a valuable tool for studying the physiological and pathophysiological roles of β-arrestins in 7TMR signaling. This could lead to a better understanding of diseases involving 7TMR dysfunction and potentially facilitate the development of novel therapeutics targeting these receptors.
Limitations and Future Research: Further research is needed to optimize ARIP's potency and selectivity, as well as to explore its therapeutic potential in various disease models. Investigating the molecular mechanisms underlying ARIP's differential efficacy against different 7TMRs and β-arrestin subtypes would provide valuable insights into the complexities of β-arrestin-mediated signaling.

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統計資料

ARIP inhibited b-arrestin 2 recruitment to CXCR4 by 82 ± 5.0% at 25 µM.
ARIP increased the EC50 of Apelin-13 for b-arrestin 1 recruitment to APJ by 13 ± 6.1-fold.
ARIP increased the EC50 of DAMGO for b-arrestin 1 recruitment to MOPR by 5 ± 1.6-fold.
ARIP inhibited b-arrestin 2 recruitment to APJ following Apelin-13 stimulation by 79 ± 2.2% (comparing area under the curve (AUC) values).

引述

從以下內容提煉的關鍵洞見

A lipidated peptide derived from the C-terminal tail of the vasopressin 2 receptor shows promise as a new \b{eta}-arrestin inhibitor

by Rebe... 於 arxiv.org 11-13-2024

https://arxiv.org/pdf/2411.07258.pdf

$A lipidated peptide derived from the C-terminal tail of the vasopressin 2 receptor shows promise as a new \b{eta}-arrestin inhibitor$

深入探究

How might the development of ARIP as a selective β-arrestin inhibitor impact the development of future therapeutics targeting 7TMRs, particularly in the context of personalized medicine?

The development of ARIP as a selective β-arrestin inhibitor holds significant potential to revolutionize the development of future therapeutics targeting 7TMRs, particularly in the realm of personalized medicine. Here's how:

Deciphering β-arrestin's Role: ARIP can be a powerful tool to dissect the intricate roles of β-arrestins in 7TMR signaling. By selectively inhibiting β-arrestin recruitment to specific receptors, researchers can gain a clearer understanding of the distinct contributions of G protein-dependent and β-arrestin-dependent signaling pathways. This knowledge is crucial for developing more targeted and effective therapies.
Tailoring Treatment Strategies:  The varying efficacy of ARIP against different 7TMRs, as observed in the study, hints at the possibility of developing  personalized medicine approaches. By understanding how ARIP interacts with specific receptor subtypes and their associated phosphorylation patterns, clinicians could potentially tailor treatments based on a patient's genetic profile and the specific 7TMR involved in their condition.
Targeting Specific Signaling Pathways:  The ability to selectively target either G protein or β-arrestin pathways opens doors for developing biased agonists or antagonists. These are drugs that preferentially activate or inhibit a specific signaling pathway downstream of a receptor, leading to a more desirable therapeutic outcome with potentially fewer side effects.
Addressing Complex Diseases: Many complex diseases, such as cancer and heart failure, involve dysregulation of multiple 7TMR signaling pathways. ARIP and similar β-arrestin inhibitors could pave the way for developing combination therapies that target both G protein and β-arrestin signaling in a personalized manner, offering more effective treatment options for these challenging conditions.
In essence, ARIP's emergence as a selective β-arrestin inhibitor provides a valuable tool for dissecting the complexities of 7TMR signaling. This deeper understanding has the potential to transform drug discovery by enabling the development of more precise and personalized therapies for a wide range of diseases.

Could ARIP's varying efficacy against different 7TMRs be attributed to differences in the receptors' phosphorylation patterns or other structural features beyond the C-terminal tail?

Yes, ARIP's varying efficacy against different 7TMRs could be attributed to several factors beyond just the C-terminal tail, with differences in receptor phosphorylation patterns being a primary candidate:

Phosphorylation Barcode: The "barcode" hypothesis posits that the specific pattern and extent of 7TMR phosphorylation act as a signaling code, dictating the affinity and selectivity of β-arrestin binding. ARIP, being a phosphomimetic peptide, likely interacts with β-arrestins based on this phosphorylation code. Variations in the number, location, and specific amino acid residues that are phosphorylated on different 7TMRs could explain why ARIP exhibits varying efficacies.
Structural Divergence Beyond the C-Terminal Tail: While ARIP is derived from the V2R C-terminal tail, it's crucial to remember that β-arrestin binding can involve interactions with other intracellular domains of the receptor, such as intracellular loops (ICLs).  Structural differences in these regions, even among receptors with similar C-terminal tails, could influence ARIP's ability to effectively compete for binding.
Receptor Conformation and Accessibility: The activation state and conformation of a 7TMR can influence the accessibility of its intracellular domains, including phosphorylation sites, to both kinases and β-arrestins.  It's plausible that certain receptors, upon agonist binding, adopt conformations that either favor or hinder ARIP's access to the β-arrestin binding site.
Cellular Context and β-arrestin Isoforms: The cellular environment, including the expression levels of different GRKs and β-arrestin isoforms (β-arrestin 1 and 2), can also influence ARIP's efficacy. Different cell types might exhibit variations in their phosphorylation machinery and β-arrestin expression profiles, leading to differences in ARIP's inhibitory effects.
Further investigations are needed to fully elucidate the precise molecular determinants governing ARIP's selectivity. Understanding these factors will be crucial for optimizing ARIP's design and developing next-generation β-arrestin inhibitors with enhanced selectivity and potency against specific 7TMR subtypes.

Considering the complex interplay between G protein and β-arrestin signaling pathways, how might the discovery of ARIP contribute to a paradigm shift in our understanding of 7TMR signaling and its implications for drug discovery?

The discovery of ARIP has the potential to trigger a paradigm shift in our understanding of 7TMR signaling by challenging the traditional linear view of these pathways and highlighting the intricate interplay between G protein and β-arrestin signaling. This shift in understanding has profound implications for drug discovery:

From Linear to Networked Signaling:  Traditionally, 7TMR signaling was viewed as a linear cascade: agonist binding, G protein activation, second messenger production, and downstream effects. ARIP's ability to selectively inhibit β-arrestin recruitment while leaving G protein signaling intact underscores the fact that these pathways are not isolated but rather part of a complex and interconnected network.
Unveiling Hidden Complexity and Crosstalk:  ARIP can help unravel the intricate crosstalk between G protein and β-arrestin pathways. By selectively blocking one arm of the signaling network, researchers can observe compensatory mechanisms, feedback loops, and previously unknown interactions between these pathways.
Redefining "On" and "Off" States:  The classic view of β-arrestins as simply "turning off" G protein signaling is being challenged. ARIP can help elucidate the context-dependent roles of β-arrestins, which can act as both signal terminators and transducers, depending on the receptor and cellular context.
Expanding the Drug Target Landscape:  ARIP's discovery expands the drug target landscape beyond the traditional focus on orthosteric ligands that bind the agonist binding site. By targeting β-arrestins directly, ARIP opens avenues for developing allosteric modulators that fine-tune 7TMR signaling with greater precision.
Enabling Pathway-Selective Therapies:  The ability to selectively target either G protein or β-arrestin pathways using tools like ARIP paves the way for developing pathway-selective therapies. This approach holds promise for achieving a more desirable therapeutic outcome with potentially fewer side effects, as it allows for fine-tuning of receptor signaling rather than complete activation or blockade.
In conclusion, ARIP's emergence as a selective β-arrestin inhibitor challenges the traditional linear view of 7TMR signaling and highlights the importance of understanding the complex interplay between G protein and β-arrestin pathways. This paradigm shift has significant implications for drug discovery, opening doors for developing more precise and effective therapies that target specific signaling pathways and address the complexities of human diseases.