# Biasing CXCR3 Signaling to Modulate the Inflammatory Response

> **NIH NIH R01** · DUKE UNIVERSITY · 2024 · $76,475

## Abstract

CXCR3 is a chemokine receptor (CKR) that plays a central role in inflammation through its regulation of T cell
migration and function. Despite the established clinical relevance of CKRs in disease, there are only three FDA
approved drugs that target the entire chemokine system, which consists of approximately twenty receptors and
fifty ligands that regulate nearly every aspect of inflammation. Reasons for this difficulty in CKR drug develop-
ment include the potential redundancy between multiple chemokine ligands for a given CKR and a lack of
knowledge of how the signaling pathways activated by CKRs regulate immune cell function and inflammation.
Thus, there is a critical unmet need for drugs targeting the chemokine system. This puts into context work from
my group on the chemokine receptor CXCR3. We have shown that the chemokine ligands of CXCR3, CXCL9,
10 and 11, act as biased agonists, generating quantitatively and qualitatively distinct signals from one another
through their interactions with heterotrimeric G proteins and β-arrestin adapter proteins. In the previous project
period, we have identified small-molecule G protein- and β-arrestin-biased CXCR3 agonists that (1) differentially
activate signaling pathways downstream of CXCR3, and (2) have distinct effects in a mouse model of T-cell-
mediated inflammatory skin disease. These findings suggest distinct roles for G proteins and β-arrestin in pro-
moting the CXCR3-mediated inflammatory response. The long-term goal of our research is to determine the
mechanisms underlying biased agonism to develop novel therapies targeting CKRs in inflammation. The overall
objective of this proposal is to determine how CXCR3 biased agonists promote different effector conformations
that lead to distinct patterns of signaling resulting in changes in T cell function and inflammation. Our central
hypothesis is that β-arrestin-biased agonists promote unique receptor and β-arrestin conformations that favor
“location-biased” endosomal signaling that promotes a unique transcriptional response in T cells and inflamma-
tion. To address our objective, first, we will determine how the receptor:ligand complex promotes biased re-
sponses through allosteric regulation of effectors. We have found that CXCR3 biased agonists promote different
β-arrestin-mediated effects, which we will explore further by using receptor mutants. Then, we will determine
how endosomal signaling and location bias contribute to CXCR3 biased signaling. We have found that some
CXCR3 biased agonists promote transcription that can be prevented by inhibiting receptor endocytosis. Lastly,
we will determine how CXCR3 G protein- and β-arrestin-mediated signaling pathways contribute to T cell function
and the inflammatory response. We will use CXCR3 mutants to test the contributions of specific signaling path-
ways to T cell chemotaxis in vitro and inflammation in vivo. This project explores an innovative approach to study
CXCR3 signaling that will provide...

## Key facts

- **NIH application ID:** 11097498
- **Project number:** 3R01GM122798-08S1
- **Recipient organization:** DUKE UNIVERSITY
- **Principal Investigator:** Sudarshan K Rajagopal
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2024
- **Award amount:** $76,475
- **Award type:** 3
- **Project period:** 2017-09-20 → 2026-06-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/11097498

## Citation

> US National Institutes of Health, RePORTER application 11097498, Biasing CXCR3 Signaling to Modulate the Inflammatory Response (3R01GM122798-08S1). Retrieved via AI Analytics 2026-05-23 from https://api.ai-analytics.org/grant/nih/11097498. Licensed CC0.

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