# Targeting leukocyte traffic in intestinal inflammation

> **NIH NIH R21** · UNIVERSITY OF ILLINOIS AT CHICAGO · 2020 · $239,850

## Abstract

Abstract
The disorders collectively known as inflammatory bowel disease (IBD) including Crohn's disease and
ulcerative colitis affect over 4 million people worldwide. Inappropriate accumulation of effector T cells in the
intestinal mucosa plays a pivotal role in maintaining disease pathology. As such, blocking pathogenic T cell
trafficking to the inflamed intestine is an area of intense investigation in IBD therapy. Recent studies have
established that GPR15, a G protein coupled receptor that had been known as an HIV co-receptor, serves as a
novel homing receptor that mediates T cell recruitment to colon. In the IBD mouse model where effector T cells
migrate to colon and induce inflammation, genetic disruption of GPR15 in T cells was shown to prevent
occurrence of colitis. In addition, most recent studies identified C10orf99, a novel chemokine that is
predominantly expressed in colon, as a natural ligand that binds to and activates GPR15. These findings
together highlight an emerging role of GPR15 as a critical chemokine receptor that mediates recruitment of
pathogenic T cells to colon in response to C10orf99. Hence, the GPR15 is a promising new target for immune
therapy of IBD. However, no reagents that can specifically modulate GPR15 activity are currently available. We
propose to develop a novel peptide-based nanoparticle that inhibit ligand-induced activation of GPR15. This
approach is based on a recent development of a nanoparticle forming peptide X4-2-6, a transmembrane helical
peptide analog which specifically targets CXCR4 receptor for inhibition of breast cancer metastasis. The same
strategy has been also applied to another chemokine receptor to develop an inhibitor peptide R321, which
blocks CCR3 signaling and prevents the eosinophil recruitment to lung and airways in the mouse asthma
model. Based on the well-conserved structure of chemokine receptors and the knowledge we have gained
from these transmembrane peptides, we have now embarked on developing the nanoparticle inhibitor peptides
containing transmembrane and extracellular loop portions of GPR15. We hypothesize that these GPR15
peptide analogs will display properties similar to X4-2-6 and R321, namely, they will form nanoparticles and
inhibit the ligand-induced activation of GPR15 that is involved in pathogenic T cell recruitment to the tissues
including colon. By specifically targeting GPR15 activity that plays a critical role in mediating colon homing of
inflammatory cells, our study is likely to significantly impact the general approach to the development of IBD
therapeutics. In Aim 1, we will use biochemical, biophysical, and molecular biology approaches to characterize
the inhibitory effects of GPR15 peptides on the ligand-induced signaling in vitro, their potential for nanoparticle
formation, and their mechanism of action. The peptides selected from these studies will be tested in Aim 2 for
their in vivo efficacy in suppressing the colon inflammation in the clinically relev...

## Key facts

- **NIH application ID:** 9820716
- **Project number:** 5R21AI142060-02
- **Recipient organization:** UNIVERSITY OF ILLINOIS AT CHICAGO
- **Principal Investigator:** SOJIN SHIKANO
- **Activity code:** R21 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $239,850
- **Award type:** 5
- **Project period:** 2018-11-08 → 2021-10-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9820716

## Citation

> US National Institutes of Health, RePORTER application 9820716, Targeting leukocyte traffic in intestinal inflammation (5R21AI142060-02). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/9820716. Licensed CC0.

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