Coggins2014 - CXCL12 dependent recruitment of beta arrestin

Model Identifier

BIOMD0000000599

Short description

Nathaniel L. Coggins, Danielle Trakimas, S. Laura Chang, Anna Ehrlich, Paramita Ray, Kathryn E. Luker, Jennifer J. Linderman & Gary D. Luker. CXCR7 controls competition for recruitment of β-arrestin 2 in cells expressing both CXCR4 and CXCR7. PLoS ONE 9, 6 (2014).

Chemokine CXCL12 promotes growth and metastasis of more than 20 different human cancers, as well as pathogenesis of other common diseases. CXCL12 binds two different receptors, CXCR4 and CXCR7, both of which recruit and signal through the cytosolic adapter protein β-arrestin 2. Differences in CXCL12-dependent recruitment of β-arrestin 2 in cells expressing one or both receptors remain poorly defined. To quantitatively investigate parameters controlling association of β-arrestin 2 with CXCR4 or CXCR7 in cells co-expressing both receptors, we used a systems biology approach combining real-time, multi-spectral luciferase complementation imaging with computational modeling. Cells expressing only CXCR4 maintain low basal association with β-arrestin 2, and CXCL12 induces a rapid, transient increase in this interaction. In contrast, cells expressing only CXCR7 have higher basal association with β-arrestin 2 and exhibit more gradual, prolonged recruitment of β-arrestin 2 in response to CXCL12. We developed and fit a data-driven computational model for association of either CXCR4 or CXCR7 with β-arrestin 2 in cells expressing only one type of receptor. We then experimentally validated model predictions that co-expression of CXCR4 and CXCR7 on the same cell substantially decreases both the magnitude and duration of CXCL12-regulated recruitment of β-arrestin 2 to CXCR4. Co-expression of both receptors on the same cell only minimally alters recruitment of β-arrestin 2 to CXCR7. In silico experiments also identified β-arrestin 2 as a limiting factor in cells expressing both receptors, establishing that CXCR7 wins the "competition" with CXCR4 for CXCL12 and recruitment of β-arrestin 2. These results reveal how competition for β-arrestin 2 controls integrated responses to CXCL12 in cells expressing both CXCR4 and CXCR7. These results advance understanding of normal and pathologic functions of CXCL12, which is critical for developing effective strategies to target these pathways therapeutically.

Format

SBML (L2V4)

Related Publication

CXCR7 controls competition for recruitment of β-arrestin 2 in cells expressing both CXCR4 and CXCR7.
Nathaniel L Coggins, Danielle Trakimas, S Laura Chang, Anna Ehrlich, Paramita Ray, Kathryn E Luker, Jennifer J Linderman, Gary D Luker
PloS one , 0/ 2014 , Volume 9 , Issue 6 , pages: e98328 , PubMed ID: 24896823

Affiliation: Center for Molecular Imaging, Department of Radiology, Department of Microbiology and Immunology, University of Michigan, Ann Arbor, Michigan, United States of America.

Abstract: Chemokine CXCL12 promotes growth and metastasis of more than 20 different human cancers, as well as pathogenesis of other common diseases. CXCL12 binds two different receptors, CXCR4 and CXCR7, both of which recruit and signal through the cytosolic adapter protein β-arrestin 2. Differences in CXCL12-dependent recruitment of β-arrestin 2 in cells expressing one or both receptors remain poorly defined. To quantitatively investigate parameters controlling association of β-arrestin 2 with CXCR4 or CXCR7 in cells co-expressing both receptors, we used a systems biology approach combining real-time, multi-spectral luciferase complementation imaging with computational modeling. Cells expressing only CXCR4 maintain low basal association with β-arrestin 2, and CXCL12 induces a rapid, transient increase in this interaction. In contrast, cells expressing only CXCR7 have higher basal association with β-arrestin 2 and exhibit more gradual, prolonged recruitment of β-arrestin 2 in response to CXCL12. We developed and fit a data-driven computational model for association of either CXCR4 or CXCR7 with β-arrestin 2 in cells expressing only one type of receptor. We then experimentally validated model predictions that co-expression of CXCR4 and CXCR7 on the same cell substantially decreases both the magnitude and duration of CXCL12-regulated recruitment of β-arrestin 2 to CXCR4. Co-expression of both receptors on the same cell only minimally alters recruitment of β-arrestin 2 to CXCR7. In silico experiments also identified β-arrestin 2 as a limiting factor in cells expressing both receptors, establishing that CXCR7 wins the "competition" with CXCR4 for CXCL12 and recruitment of β-arrestin 2. These results reveal how competition for β-arrestin 2 controls integrated responses to CXCL12 in cells expressing both CXCR4 and CXCR7. These results advance understanding of normal and pathologic functions of CXCL12, which is critical for developing effective strategies to target these pathways therapeutically.

Contributors

Submitter of the first revision: Jennifer Linderman
Submitter of this revision: Lucian Smith
Curator: Lucian Smith
Modellers: administrator, Jennifer Linderman

Metadata information

is (2 statements)

BioModels Database BIOMD0000000599
BioModels Database MODEL1408060000

isDescribedBy (1 statement)

PubMed 24896823

hasTaxon (1 statement)

Taxonomy Homo sapiens

isVersionOf (2 statements)

Gene Ontology chemokine (C-X-C motif) ligand 12 signaling pathway
Gene Ontology CXCL12-activated CXCR4 signaling pathway

hasProperty (1 statement)

Mathematical Modelling Ontology Ordinary differential equation model

Curation status

Curated

Modelling approach(es)

ordinary differential equation model

Connected external resources

SBGN view in Newt Editor

Name	Description	Size	Actions
Model files (1)
BIOMD0000000599_url.xml	SBML L2V4 representation of Coggins2014 - CXCL12 dependent recruitment of beta arrestin	203.96 KB	Preview \| Download
Additional files (15)
BIOMD0000000599-biopax2.owl	Auto-generated BioPAX (Level 2)	69.20 KB	Preview \| Download
BIOMD0000000599-biopax3.owl	Auto-generated BioPAX (Level 3)	112.89 KB	Preview \| Download
BIOMD0000000599-matlab.m	Auto-generated Matlab file.	22.25 KB	Preview \| Download
BIOMD0000000599-octave.m	Auto-generated Octave file.	22.25 KB	Preview \| Download
BIOMD0000000599.m	Auto-generated Octave file	22.25 KB	Preview \| Download
BIOMD0000000599.ode	Auto-generated ODE file for XPP.	19.19 KB	Preview \| Download
BIOMD0000000599.pdf	Auto-generated PDF file	398.35 KB	Preview \| Download
BIOMD0000000599.png	Auto-generated Reaction graph (PNG)	759.95 KB	Preview \| Download
BIOMD0000000599.svg	Auto-generated Reaction graph (SVG)	124.50 KB	Preview \| Download
MODEL1408060000.cps	The COPASI file reproduces all plots described in the curation tab.	248.46 KB	Preview \| Download
MODEL1408060000.sedml	CRBM-processed SED-ML file, based on original COPASI save file export.	61.94 KB	Preview \| Download
curation_image.png	Reproduced figure(s) from original curation.	123.61 KB	Preview \| Download
curation_notes.txt	Notes from original curation (describes curation_image).	387.00 Bytes	Preview \| Download
manifest.xml	Auto-generated manifest file for OMEX archives.	1.86 KB	Preview \| Download
metadata.rdf	Auto-generated annotation metadata file.	1.70 KB	Preview \| Download

Model originally submitted by : Jennifer Linderman
Submitted: Aug 6, 2014 2:11:40 PM
Last Modified: Aug 21, 2024 11:31:24 PM

Revisions

Version: 4
- Submitted on: Aug 21, 2024 11:31:24 PM
- Submitted by: Lucian Smith
- With comment: CRBM-sponsored manual and automated updates.
Version: 3
- Submitted on: Dec 21, 2018 6:16:01 PM
- Submitted by: administrator
- With comment: Include the additional files provided by the submitter in the original submission: MODEL1408060000.cps
Version: 2
- Submitted on: Apr 18, 2016 3:58:25 PM
- Submitted by: Jennifer Linderman
- With comment: Current version of Coggins2014 - CXCL12 dependent recruitment of beta arrestin
Version: 1
- Submitted on: Aug 6, 2014 2:11:40 PM
- Submitted by: Jennifer Linderman
- With comment: Original import of New Model

(*) You might be seeing discontinuous revisions as only public revisions are displayed here. Any private revisions of this model will only be shown to the submitter and their collaborators.

Legends
: Variable used inside SBML models

Species	Initial Concentration/Amount
species 5 Luciferase ; Stromal cell-derived factor 1 ; Beta-arrestin-2 ; C-X-C chemokine receptor type 4	0.0 item
species 9 Atypical chemokine receptor 3 ; Stromal cell-derived factor 1 ; Luciferase	0.0 item
species 15 C-X-C chemokine receptor type 4 ; Luciferase	133539.963932179 item
species 24 Beta-arrestin-2 ; Luciferase ; C-X-C chemokine receptor type 4	8151.72873852455 item
species 8 C-X-C chemokine receptor type 4 ; Luciferase ; Beta-arrestin-2 ; Stromal cell-derived factor 1	0.0 item
species 30 Luciferase ; Atypical chemokine receptor 3 ; Beta-arrestin-2	151851.62433362 item
species 4 Stromal cell-derived factor 1 ; C-X-C chemokine receptor type 4 ; Luciferase	0.0 item
species 12 Beta-arrestin-2 ; Stromal cell-derived factor 1 ; Luciferase ; Atypical chemokine receptor 3	0.0 item
species 19 Beta-arrestin-2 ; Atypical chemokine receptor 3 ; Luciferase	97340.7848290227 item

Reactions	Rate	Parameters
species_1 + species_16 => species_5; species_1, species_16, species_5	compartment_2parameter_1parameter_7/(parameter_28parameter_30)(species_1species_16-parameter_5parameter_9parameter_28parameter_30/parameter_7/parameter_21*species_5)	parameter_30 = 8.4E-12; parameter_5 = 40.0; parameter_9 = 5100000.0; parameter_28 = 6.02E23; parameter_7 = 1.0E9; parameter_21 = 7800000.0; parameter_1 = 0.0021
species_1 + species_20 => species_9; species_1, species_20, species_9	compartment_2parameter_2parameter_7/(parameter_28parameter_30)(species_20species_1-parameter_6parameter_28parameter_30/parameter_7species_9)	parameter_30 = 8.4E-12; parameter_28 = 6.02E23; parameter_7 = 1.0E9; parameter_2 = 0.0014; parameter_6 = 0.84
species_2 + species_15 => species_16; species_15, species_16, species_2	compartment_2parameter_3(species_2species_15-parameter_21species_16)	parameter_21 = 7800000.0; parameter_3 = 8.5E-9
species_23 => species_15; species_23	compartment_2parameter_16species_23	parameter_16 = 6.9E-5
species_24 => species_23 + species_3; species_24	compartment_2parameter_11species_24	parameter_11 = 0.0023
species_7 => species_8 + species_14; species_7	compartment_2parameter_23species_7	parameter_23 = 0.0047
species_30 => species_18 + species_3; species_30	compartment_2parameter_15species_30	parameter_15 = 0.0025
species_1 + species_15 => species_4; species_1, species_15, species_4	compartment_2parameter_1parameter_7/(parameter_28parameter_30)(species_15species_1-parameter_5parameter_28parameter_30/parameter_7species_4)	parameter_30 = 8.4E-12; parameter_5 = 40.0; parameter_28 = 6.02E23; parameter_7 = 1.0E9; parameter_1 = 0.0021
species_1 + species_19 => species_12; species_1, species_12, species_19	compartment_2parameter_2parameter_7/(parameter_28parameter_30)(species_1species_19-parameter_6parameter_10parameter_28parameter_30/parameter_7/parameter_22*species_12)	parameter_30 = 8.4E-12; parameter_28 = 6.02E23; parameter_10 = 650000.0; parameter_7 = 1.0E9; parameter_22 = 2300000.0; parameter_2 = 0.0014; parameter_6 = 0.84
species_3 + species_20 => species_19; species_19, species_20, species_3	compartment_2parameter_4(species_3species_20-parameter_22species_19)	parameter_4 = 1.4E-8; parameter_22 = 2300000.0

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Curator's comment:
(added: 18 Apr 2016, 12:44:35, updated: 18 Apr 2016, 12:44:35)

The results from Figure 4 for CXCR4+-CXCR7+ cells were reproduced, as were panels C and D of Supplementary Figure B. Note that FigSB panel C is reproduced qualitatively, but there are some slight quantitative differences from the reference figure. The curation simulations were performed in Copasi, with figures combined in OmniGraffle. The reference publication simulations used Matlab.