# Structural Basis for Chemokine Function

> **NIH NIH R37** · MEDICAL COLLEGE OF WISCONSIN · 2020 · $385,000

## Abstract

PROJECT SUMMARY
The long-term goal of this research is to understand how chemokines recognize their binding partners in order
to develop new molecules that alter chemokine signaling for therapeutic benefit. Chemokines and their cell-
surface receptors form a network of signaling proteins that orchestrate the development and function of the
cellular immune system by guiding the migration of white blood cells and homing of stem cells. Many of these
proteins have been validated as drug targets for inflammatory and autoimmune diseases, HIV-AIDS,
cardiovascular disease and cancer. Our previous work revealed the structural basis and functional importance
of self-association, glycosaminoglycan binding, and receptor sulfotyrosine recognition for the chemokine
CXCL12 and its receptor CXCR4, and demonstrated that engineered CXCL12 variants can be used to block
cancer progression in animal models of metastatic disease. Atomic resolution details of other chemokine-
receptor complexes are needed to guide the development of new small molecule and biologic drugs. With 46
chemokine ligands and 23 receptors, the human chemokine network represents the largest GPCR family with
respect to the number of endogenous ligands and receptors. Across the chemokine family, ligand-receptor
specificity varies from strictly monogamous to highly promiscuous, but the molecular determinants of selectivity
are unknown. Until recently, details of the full chemokine-receptor interface were lacking due to the extreme
challenges presented by crystallization of active GPCR complexes. However, the availability of a rich
sequence database and multiple structures of chemokine-receptor complexes reported since the last renewal
of this R01 now enable us to address the most pressing question in the chemokine field: how is selective
promiscuity embedded in a collection of highly conserved chemokine and receptor structures? In the first
specific aim of this competing renewal application we propose a comprehensive analysis of this complex
signaling network, in order to decipher the ‘chemokine code’ governing receptor-ligand selectivity and
promiscuity. The second aim will test the hypothesis that selective chemokine promiscuity is encoded across a
broad protein-protein interface using the chemokines CXCL11 and CXCL12 and their receptors ACKR3,
CXCR3 and CXCR4 as a model system to test the validity of the hierarchical model developed in aim 1. Aim 3
tackles the puzzle of extreme promiscuity in the chemokine family with the atypical receptor ACKR1 as an
experimental testbed. ACKR1/DARC is a scavenger receptor on red blood cells that binds many different
chemokines but also plays an essential role in hematopoiesis in the bone marrow. We hypothesize that
ACKR1 uses an elongated disordered N-terminal domain to bind many protein ligands with distinct but
overlapping binding sites. Completion of the work proposed here will provide a new foundation upon which the
molecular determinants of chemokine-rece...

## Key facts

- **NIH application ID:** 10049899
- **Project number:** 2R37AI058072-15A1
- **Recipient organization:** MEDICAL COLLEGE OF WISCONSIN
- **Principal Investigator:** Brian F Volkman
- **Activity code:** R37 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $385,000
- **Award type:** 2
- **Project period:** 2004-06-11 → 2025-05-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10049899

## Citation

> US National Institutes of Health, RePORTER application 10049899, Structural Basis for Chemokine Function (2R37AI058072-15A1). Retrieved via AI Analytics 2026-05-24 from https://api.ai-analytics.org/grant/nih/10049899. Licensed CC0.

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