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About the Authors:

Chen Zheng

Roles Investigation, Visualization, Writing – original draft, Writing – review & editing

Affiliation: Department of Pharmacology, Vanderbilt University, Nashville, United States of America

ORCID logo http://orcid.org/0000-0002-3610-5715

Jonas Tholen

Roles Investigation

Affiliation: University of Applied Sciences Emden/Leer, Emden, Germany

Vsevolod V. Gurevich

Roles Conceptualization, Funding acquisition, Methodology, Project administration, Resources, Supervision, Visualization, Writing – original draft, Writing – review & editing

* E-mail: [email protected]

Affiliation: Department of Pharmacology, Vanderbilt University, Nashville, United States of America

ORCID logo http://orcid.org/0000-0002-3950-5351

Introduction

G-protein coupled receptors (GPCRs) are the largest family of signaling proteins in mammals, with ~500 different subtypes in dolphins, ~800 in primates, and more than 3,400 in elephants (sevens.cbrc.jp). GPCRs are involved in almost every aspect of life activity by mediating most cellular responses to hormones, neurotransmitters, odorants, light, etc. [1].

All GPCRs share a common seven transmembrane (7TM) α-helical segments linked by extracellular loops (ECLs) and intracellular loops (ICLs). ECLs, ICLs, as well as the extracellular N-termini and intracellular C-termini are diverse in sequence and length [2,3]. The activation of GPCRs induced by external stimuli leads to the activation of many molecules of heterotrimeric G-proteins to amplify signal. Ultimately GPCR signaling via G proteins is terminated by receptor phosphorylation by specific GPCR kinases (GRKs; of which most mammals only have seven, with some nocturnal rodents having only six [4]), and specific binding of arrestins to active phosphorylated receptors [5,6]. Mammals express even fewer arrestin subtypes than GRKs, the total of four, two out of which are specialized visual that are expressed in retinal photoreceptors and quench photopigment signaling [7,8]. In contrast, non-visual subtypes arrestin-2 and -3 (also known as β-arrestin1 and 2; note that we use systematic names of arrestin proteins, where the number after the dash indicates the order of cloning: arrestin-1 (historic names S-antigen, 48 kDa protein, visual or rod arrestin), arrestin-2 (β-arrestin or β-arrestin1), arrestin-3 (β-arrestin2 or hTHY-ARRX), and arrestin-4 (cone or X-arrestin)), are ubiquitously expressed and bind hundreds of non-visual GPCRs.

Identified >800 GPCRs in humans account for ~ 3% of coding genes [9]. Abnormal GPCR functions due to mutations are associated with a wide variety of congenital disorders [10–12]. Currently, about 30% of clinically used drugs target various GPCRs [2]. For gain-of-function GPCR mutations, engineered enhanced arrestins with higher ability to bind phosphorylated and unphosphorylated receptors may have therapeutic potential, as these proteins can reduce the excessive signaling of overactive GPCRs [12,13].

Considering that visual and non-visual arrestins are highly conserved with only a few residues different [8], the high specificity of visual arrestin for rhodopsin might be tuned by those key residues. Previous study suggests that receptor preference of visual arrestin-1 and non-visual arrestin-2 can be switched by the exchange of ten residues on the receptor-binding interface [14]. A double mutation in arrestin-3 yielded up to 50-fold preference for particular receptors over others [15], indicating the possibility of narrowing arrestin-3 receptor preference and constructing receptor-specific variants. Recent structural studies of the arrestin-1 complex with rhodopsin revealed that several arrestin elements directly participate in receptor binding [16,17]. Here we test how mutations in these regions of arrestin-3 affect its binding to the four model GPCRs: β2-adrenergic, M2 muscarinic, and D1 and D2 dopamine receptors.

Materials and methods

Materials

Restriction endonucleases and other DNA modifying enzymes were from New England Biolabs (Ipswich, MA). Cell culture reagents and media were from GIBCO (Gaithersburg, MD). Transfection reagent TransHi was from FormuMax (Sunnyvale, CA). Coelenterazine h was from NanoLight (Pinetop, AZ). All plasmid DNAs were prepared by Qiagen (Germantown, MD) Plasmid Maxi kit. All other reagents and chemicals were purchased from Amresco (Solon, OH) or Sigma-Aldrich (St Louis, MO).

Plasmid constructs

All arrestin mutants were N-terminally tagged with Venus, whereas the receptors were C-terminally tagged with Renilla luciferase variant 8 (RLuc8), as described [14,15].

Bioluminescence resonance energy transfer (BRET) assay

BRET-based assays [18–21] with Venus as the acceptor and RLuc8 as the donor were used to measure the binding of Venus-tagged arrestins to the M2 muscarinic acetylcholine receptor (M2R-RLuc8), β2-adrenergic receptor (β2AR-RLuc8), dopamine D1 (D1R-RLuc8) and D2 (D2R-RLuc8) receptors. The long isoform of D2R was used in this study, as in previous ones [15,22]. HEK293 arrestin-2/3 KO cells [23,24] (a kind gift of Dr. A. Inoue, Tohoku University, Japan) were transfected using TransHi according to the manufacturer’s instructions (3 μl of TransHi /1 μg of DNA) in 6-well plates.

We have previously determined the amounts of plasmid DNA that produce sufficient excess of arrestin-3 over receptor that saturates the BRET signal [15,25,26]. 48 h post-transfection, cells expressing similar levels of receptor and arrestins (S1 Fig) were transferred into 96-well plate, then appropriate agonists (10 μM) were added: carbachol (carbamoylcholine) for M2R, isoproterenol for β2AR, dopamine for D1R, and quinpirole for D2R. Coelenterazine h was added immediately after agonist as luciferase substrate at 5 μM. The net BRET (the difference in BRET in the presence and absence of an agonist) was measured as previously described [15,26,27].

Co-immunoprecipitation

HEK293 arrestin 2/3 KO cells were seeded into 6-well plate 24 h prior to transfection. Cells were transfected with indicated Ve-Arr3 mutants and HA-D2R using TransHi. The cells were serum-starved overnight one day prior to test. At 48 h post-transfection, cells were washed with PBS and treated with 10 μM quinpirole for 10 min. Then cells were immediately lysed on ice in 400 μL of lysis buffer containing 50 mM Tris pH 7.5, 150 mM NaCl, 1% NP-40, 1 mM Benzamidine, 1 mM PMSF. The lysates were centrifugated for 10 min at 11, 000xg to pellet cell debris, and the supernatants were used for immunoprecipitation. A total of 400 μg protein from each transfection were pre-cleared with 25 μL protein G agarose (Millipore, MO) in binding buffer (25 mM HEPES, pH 7.3, 150 mM NaCl, 1 mM TCEP), followed by incubation for 2 h with 2 μg Anti-HA antibody (Roche, NJ). The immunoprecipitates were incubated with 25 μL of protein G agarose beads overnight at 4°C. The next day the beads were sedimented by centrifugation for min at 4°C at 5, 000 xg and washed three times with 500 μL binding buffer. Bound proteins were eluted with 50 μL of SDS sample buffer. Cell lysates and immunoprecipitated proteins were subjected to Western blot using anti-HA and anti-GFP antibodies, peroxidase-coupled secondary antibodies (Jackson Immuno, PA), and SuperSignal WestPico reagent (ThermoFisher, IL). Developed blots were visualized by LI-COR C-DiGit Blot Scanner (LI-COR, NE). Bands were quantified using QuantityOne software (Bio-Rad, CA). Non-specific binding to beads (in the absence of HA-D2R bait) was subtracted.

Data analysis and statistics

BRET data were analyzed, as described [15,22]. Statistical significance (p < 0.05) was determined using one-way analysis of variance (ANOVA) with Dunnett's multiple comparison test using GraphPad Prism software. P values<0.05 were considered statistically significant and indicated, as follows: *p<0.05; ***p<0.001; ****p<0.0001.

Results

Selection of receptor-specific mutants

Crystal structures indicate high similarity of the basal state of all vertebrate arrestins [28–33]. Receptor-binding surface of all arrestins was localized to the concave sides of the two domains and the central crest on the receptor-binding side of the molecule by different labs using a variety of methods [34–40]. The crystal structure of the arrestin-1 complex with activated phosphorylated rhodopsin (P-Rh*) has identified two interaction interfaces in arrestins largely responsible for the binding of non-phosphorylated parts of the receptor [16,17]. The first interface consists of the finger loop (residues G65-S75 in arrestin-3, corresponding to G68-S78 in arrestin-1), which was shown to be the key region for receptor binding of arrestin-3 [41]. Second interface consists of the middle loop (Q131-A140 in arrestin-3; Q133-S142 in arrestin-1), C-loop (residues C243-Q247 in arrestin-3; V247-Y254 in arrestin-1, residue Y251 region at the central loop in the arrestin C-domain) and back loop (K313 loop, K310 in arrestin-1, R319/R322 in mouse/human arrestin-1). The P-Rh*-arrestin-1 complex structure shows that the middle and C-loop are close in the basal state but move away from each other upon activation, opening a cleft in the central crest. The shift of the back loop apparently twists the arrestin C-domain, which allows back loop (K319 and T320) interact with TM5/6 of rhodopsin through hydrogen bonds, and allows the 157-loop (residue D162 in arrestin-1, E157 in arrestin-3) move closer to the finger loop [16,36,42].

Sequence comparison identifies a few residue differences in those loops at the interfaces. Most of these residues are exposed in the basal state, so that they might be directly engaged by the receptor (Fig 1A). Based on these data, we substituted several residues in arrestin-3 targeting those loops that were expected to be flexible. For example, G65 (in bovine arrestin-3) is the first residue of the finger loop and it is conserved in all arrestin subtypes (Fig 1B). As finger loop is highly flexible, the small size of glycine might allow finger loop movement during activation process [43]. We made the G65P mutant because proline provides more rigidity than glycine, while also breaking any secondary structure. We also tested the G65 deletion (ΔG65) because of high conservation of this residue in arrestin evolution (Fig 1B) [7,8].

[Figure omitted. See PDF.]

Fig 1. Arrestin residues mutated in this study.

A. Crystal structure of arrestin-3 (Protein Data Bank entry 3P2D [33]) with selected mutations indicated. Arrestin elements are colored, as follows: (Red: finger loop; Green: 157-loop; Yellow: C-loop; Blue: back-loop). B. Sequence alignment of elements containing selected mutations in arrestin-3 and other subtypes from different species. Shaded residues in each loop are the mutations selected in this study.

https://doi.org/10.1371/journal.pone.0213792.g001

E157, located on the flexible 157-loop, is conserved in non-visual arrestins, but replaced with Asn in the corresponding position of arrestin-1 where it interacts with the TM6 of the rhodopsin via a hydrogen bond (Fig 1B) [44]. We chose to introduce E157A mutation to break the potential hydrogen bond formation by this side chain.

In arrestin-1 both Y251 (F245 in arestin-3) in the C-loop and K319 (K313 in arrestin-3) in the back loop participate in rhodopsin binding via interaction with ICL2 and TM5, respectively, suggesting their importance in stabilizing the arrestin-receptor complex. Phe is conserved in non-visual arrestins at the position. However, the substitution of Phe with Tyr at this site in arrestin-2 does not change its receptor preference [14]. So, we chose the F245A mutation to eliminate this aromatic side chain. K313A mutation was chosen to eliminate positively charged side chain.

Highly conserved G65 in the finger loop is essential for receptor binding

To measure arrestin-3 interaction with GPCRs, we used bioluminescence resonance energy transfer (BRET) in HEK293 arrestin2/3 KO cells [22] co-transfected with Venus-tagged arrestin-3 (Ve-Arr3) and Renilla luciferase-tagged (RLuc) receptors M2R, β2AR, D1R and D2R. In all tests, we used arrestin-3 KNC mutant as negative control. The KNC mutant does not bind GPCRs because 12 key receptor-binding residues in it were replaced with Ala [25,26]. All mutations were introduced on arrestin-3 A87V background. The A87V mutation makes arrestin-3 N-domain more rigid [15]. This substitution likely enhances receptor specificity of arrestins [30] without significantly affecting the binding to any GPCR used in this study [15].

Base mutant A87V showed a robust binding upon agonist stimulation, while KNC mutant consistently showed extremely low binding, as expected (Fig 2). Four mutations did not significantly affect arrestin-3 binding to any of the four GPCRs tested: G65P, E157A, F245A and K313A (Fig 2). However, ΔG65 dramatically reduced the binding to all four receptors (Fig 2). The magnitude of the reduction varied from ~30% to ~80%. In particular, ΔG65 dramatically reduced arrestin-3 binding to D2R, almost to the level observed with the KNC mutant. Considering that receptor specificity of arrestins appears to be determined by several residues [15,27], it is surprising that a single mutation can make such a dramatic difference. More importantly, although ΔG65 reduced binding to all of four GPCRs, this mutation affected D2R binding to a much greater extent than others, suggesting that stability of D2R-arrestin complex is more dependent on the receptor interaction with the finger loop of arrestin.

[Figure omitted. See PDF.]

Fig 2. Substitution of selected residues in arrestin-3 loops differentially affects agonist-induced binding to individual GPCRs.

BRET between Venus-tagged arrestin-3 and luciferase-tagged human M2R (A), β2AR(B), D1R(C), D2R(D) in HEK293 arrestin 2/3 KO cells. Net BRET was calculated by subtracting basal BRET (no agonist) from agonist-induced BRET. Average BRET at 10 and 15 min (means ± S.E.M.) from at least three independent experiments is shown for each arrestin-receptor pair. Each experiment was performed in quadruplicate. Statistical significance was determined using one-way ANOVA, followed by Dunnett's post-hoc test with correction for multiple comparisons. *, p< 0.05; ***, p< 0.001; ****, p<0.0001, as compared to A87V base mutant.

https://doi.org/10.1371/journal.pone.0213792.g002

Receptor binding might be sterically hindered by the deletion of G65

To elucidate the mechanism of action of ΔG65 mutation, we tested the time dependence of net BRET, comparing ΔG65 to non-binding KNC and robustly binding A87V base mutant. For all four receptors, A87V showed increased net BRET in the first 10–15 min after the addition of the agonist, which subsequently decreased at 25–30 min. In contrast, KNC mutant consistently showed low binding at all time points (Fig 3A–3D). The time course of the binding of mutant with the deletion of G65 was similar to that of A87V, while being consistently lower than the binding of A87V at all time points. Since ΔG65 mutant never reaches the BRET value demonstrated by A87V, this mutation likely affects receptor binding by reducing the stability of the arrestin-receptor complex, i.e., by increasing the rate of arrestin dissociation, so that there is less arrestin bound at any given moment, without significant changes in the kinetics of the initial arrestin-3 recruitment to receptors (Fig 3).

[Figure omitted. See PDF.]

Fig 3. Time course of the interaction of selected arrestins with indicated receptors.

Net BRET of selected Venus-tagged arrestin-3 mutants measured at indicated time points with luciferase-tagged M2R (A), β2AR(B), D1R(C), D2R(D) is shown (means ± S.E.M.). Note similar time dependence of A87V and ΔG65 mutant binding to the receptors, even though ΔG65 consistently demonstrates much lower binding.

https://doi.org/10.1371/journal.pone.0213792.g003

Independent assessment of arrestin-receptor interaction by co-immunoprecipitation

As our in-cell BRET studies of the interaction of arrestin-3 mutants with GPCRs yielded surprising results, we sought to test these interactions by an independent method. We used co-immunoprecipitation (co-IP) of receptors with various forms of arrestin-3. HEK293 arrestin 2/3 KO cells transfected with Venus-tagged arrestin-3 mutants without HA-tagged D2R served as control for non-specific arrestin binding to the beads. Cells were co-transfected with indicated forms of Ve-Arr3 and HA-D2R. Following stimulation with the agonist, cell lysates were immunoprecipitated with anti-HA antibody and immunoblotted with anti-GFP and anti-HA antibodies (Fig 4). As shown in Fig 3A, upon stimulation KNC has almost no ability to bind the receptor, as compared to fully functional A87V base mutant. The deletion of G65 dramatically reduced arrestin-3 binding to D2R (Fig 3B). The same changes were observed by co-IP (Fig 4), confirming BRET results.

[Figure omitted. See PDF.]

Fig 4. Deletion of G65 impedes arrestin-3 binding to D2R in vitro.

(A). Serum-starved HEK293 arrestin 2/3 KO cells were co-transfected with indicated Ve-Arr3 mutants with or without (no bait control) HA- D2R. Cells were stimulated with 10 μM quinpirole. Cleared cell lysates were immunprecipitated with HA antibody, and immunoblotted with anti-HA and anti-GFP antibodies. (B) Quantification of the specific receptor binding of different arrestin-3 mutants in three independent experiments. Non-specific binding observed in cells that do not express HA -D2R was subtracted in all cases.

https://doi.org/10.1371/journal.pone.0213792.g004

Discussion

Mutations in numerous proteins underlie a variety of human disorders. Mutations in GPCRs fall into two categories: loss- and gain-of-function [11,12]. Despite the initial enthusiasm about editing errors out of the genome, careful studies show that CRISPR/Cas-9 gene editing often generates off-target changes, some of which could be expected, whereas others could not [45]. In more traditional gene therapy approach, the strategy in case of loss-of-function mutations is clear: the delivery of the coding sequence for the normal receptor should solve the problem. Loss-of-function mutations are usually recessive, as one normal allele is in most cases sufficient, so that only compound heterozygotes are affected. In contrast, gain-of-function mutations are dominant: normal product of the second allele cannot dampen the signaling by an overactive mutant receptor. One strategy was proposed to fight gain-of-function GPCR mutations: dampening their excessive signaling with enhanced arrestins that have higher propensity to bind these receptors. So far this compensational approach had shown promise in the visual system, where the only important receptor is rhodopsin, which is shut off by arrestin-1 [13,46]. While due to highly conserved activation mechanisms non-visual arresins can be enhanced by the same mutations as visual arrestin-1 [47–49], non-visual arrestins have broad receptor specificity [15,50,51]. Most cells express multiple GPCR subtypes. While the expression of enhanced non-visual arrestin would likely dampen excessive signaling by the mutant, at the same time it would reduce the signaling of perfectly normal other GPCRs in the same cell. Thus, the use of the same compensational approach requires non-visual arrestin variants with narrow receptor specificity, that would target only the “offending” receptor mutant, but not the other GPCRs.

Arrestins in mammals are represented by only four subtypes [7,8], so that the two non-visual arrestins control hundreds of different GPCRs [12]. However, arrestin-1 shows high specificity toward one receptor (rhodopsin), suggesting that narrow receptor specificity is possible [14,51]. Structural analysis of arrestins suggests similarity of the mechanism of receptor binding [29–31,33,52]. Arrestin-3 has been reported to bind virtually every GPCR tested [33,50], often demonstrating higher affinity for the receptors that both non-visual subtypes bind [50,53]. Thus, arrestin-3 appears to be a more promising starting point for the design of receptor-specific mutants than highly homologous arrestin-2 [54,55]. Previously, we have successfully changed the arrestin-3 specificity for particular GPCRs through manipulating relatively few residues on the receptor-binding surface [14,15,22,35]. Here we tested several mutations in the loops of arrestin-3 that are expected to engage the receptors using in-cell BRET assay.

The results clearly show that G65 in the finger loop is required for arrestin-3 binding to all tested receptors: M2R, D1R, D2R, β2AR. The deletion of G65 had the greatest effect on D2R binding (Fig 2). D2R, in contrast to D1R and β2AR, has a long third ICL [56,57]. However, it shares this structural feature with M2R [58], where the reduction of binding was similar to that of D1R and β2AR, so that the size of the third ICL per se (and likely consequent different “pose” of bound arrestin), does not explain greater suppression of the D2R binding. Other mutations (G65P, E157A, F245A and K313A) do not significantly change arrestin-3 binding to these GPCRs. Available crystal structures show that the finger loop of arrestin can be presented to the receptor in distinct conformations and at different angles (relative to the rest of the molecule) [41,43], suggesting that the flexibility of finger loop is important to allow the recognition of different receptors by non-visual arrestins. The mutations that perturb the flexibility of the finger loop were shown to interfere with receptor binding [41]. In particular, substitution of several residues with a rigid proline (D68P, D70P) has been shown to greatly decrease arrestin-3 binding to M2R and D2R [41]. Substitution of many residues by alanines generally decreases the binding of arrestin-1 to rhodopsin [21,59]. Unlike these mutations, ΔG65 and G65P differentially affect arrestin-3 binding without altering the charges in the finger loop. Glycine is the most sterically flexible residue among all amino acids due to its smallest side chain. The absence of this glycine apparently “tightens” the finger loop and/or allows an extension of the β-strand V, as Gly is known to break the secondary structure. Both mechanisms would explain uniformly negative effect of its deletion on GPCR binding (Fig 2).

The replacement of glycine with proline not only eliminates the flexibility of finger loop, but also bends the loop to a fixed angle due to the cyclic structure of the Pro residue. Our data show that G65P does not significantly affect the binding to the four receptors tested, suggesting that the interruption of the strand even by a sharp turn allows finger loop to accommodate these receptors. Considering that a glycine in position equivalent to G65 in arrestin-3 is conserved in virtually all arrestins [7,8], both high flexibility and proper length of the finger loop seem to be very important for arrestin function. Consequently, it is possible that G65P may impair arrestin-3 binding to other GPCRs, narrowing the broad receptor specificity of arrestin-3. This needs to be tested experimentally.

Arrestins appear to independently recognize two features in a GPCR: its active conformation and the presence of receptor-attached phosphates [60] (this mechanism was reviewed and illustrated in [5]). Recent findings suggest that, at least in case of GPCRs where all phosphorylation sites are localized on the receptor C-terminus, arrestin binds to just the phosphorylated elements tightly enough to yield stable receptor complexes with the “partially engaged” arrestins [61–63]. Our data indicate that the deletion of G65 in the finger loop, which engages non-phosphorylated parts of the receptor, the inter-helical cavity that opens upon GPCR activation [16,17,64], has a very strong negative effect on the arrestin-receptor interaction. As ΔG65 mutation is unlikely to directly affect arrestin-3 interactions with the receptor-attached phosphates directly, it appears that mutant finger loop weakens arrestin-3 binding even to the phosphorylated receptor elements indirectly, via an allosteric mechanism. Interestingly, D2 receptor, where the effect is the strongest, is a special case: in it GRK phosphorylation sites are localized exclusively on the ICL3, and phosphorylation does not seem to be required for the arrestin-3 binding [19]. Although GRK phosphorylation sites are also localized on the ICL3 in the M2 muscarinic receptor [58], in this case phosphorylation is necessary for the arrestin binding [58,65]. Thus, the magnitude of the effect of ΔG65 mutation on arrestin-3 interaction with tested GPCRs might reflect relative contribution of the arrestin binding to the receptor-attached phosphates: the greater the role of phosphate binding (which is very different in GPCR subtypes used here [20,26]), the smaller the effects of the mutation that does not affect phosphate-binding arrestin elements identified in several studies [41,66,67].

E157 and K313 are charged residues. In fact, K313 is the only positively charged amino acid in the back loop. The common strategy of substitution is to change to oppositely charged amino acid to check the role of this residue. We constructed E157K and K313E mutants with charge reversals and found that both showed very low expression level in cells, suggesting that these mutants have folding problems. In contrast, charge elimination mutations E157A and K313A appear to be well tolerated (Fig 1).

To summarize, our data indicate that the absence of a highly flexible glycine and/or the length of the finger loop, which likely affects its ability to “mold” itself to fit the receptor in the complex, plays a more important role in receptor binding than the actual sequence in other elements. This is consistent with the interaction of the finger loop with the inter-helical cavity in the core of active GPCRs, revealed by the structure of the arrestin-1 complex with rhodopsin [16,17], supporting the idea that this element plays the same critical role in the binding of non-visual arrestins to other GPCRs.

Supporting information

[Figure omitted. See PDF.]

S1 Fig. Expression of Venus-arrestin and receptor-Rluc8.

The expression of Venus-arrestin and receptor-RLuc8 were evaluated by the fluorescence and the basal luminescence density, respectively. The expression level was normalized to the A87V base mutant, as follows: M2R (A), β2AR(B), D1R(C), D2R(D).

https://doi.org/10.1371/journal.pone.0213792.s001

(PDF)

Citation: Zheng C, Tholen J, Gurevich VV (2019) Critical role of the finger loop in arrestin binding to the receptors. PLoS ONE 14(3): e0213792. https://doi.org/10.1371/journal.pone.0213792

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© 2019 Zheng et al. This is an open access article distributed under the terms of the Creative Commons Attribution License: http://creativecommons.org/licenses/by/4.0/ (the “License”), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.

Abstract

We tested the interactions with four different G protein-coupled receptors (GPCRs) of arrestin-3 mutants with substitutions in the four loops, three of which contact the receptor in the structure of the arrestin-1-rhodopsin complex. Point mutations in the loop at the distal tip of the N-domain (Glu157Ala), in the C-loop (Phe255Ala), back loop (Lys313Ala), and one of the mutations in the finger loop (Gly65Pro) had mild variable effects on receptor binding. In contrast, the deletion of Gly65 at the beginning of the finger loop reduced the binding to all GPCRs tested, with the binding to dopamine D2 receptor being affected most dramatically. Thus, the presence of a glycine at the beginning of the finger loop appears to be critical for the arrestin-receptor interaction.

Details

Title
Critical role of the finger loop in arrestin binding to the receptors
Author
Chen, Zheng; ⨯ Jonas Tholen; Vsevolod V Gurevich ⨯
First page
e0213792
Section
Research Article
Publication year
2019
Publication date
Mar 2019
Publisher
Public Library of Science
e-ISSN
19326203
Source type
Scholarly Journal
Language of publication
English
DOI
https://doi.org/10.1371/journal.pone.0213792
ProQuest document ID
2193112381
Copyright
© 2019 Zheng et al. This is an open access article distributed under the terms of the Creative Commons Attribution License: http://creativecommons.org/licenses/by/4.0/ (the “License”), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.