# Research Project  Cervical Cancer

> **NIH NIH U54** · WASHINGTON UNIVERSITY · 2024 · $247,065

## Abstract

PROJECT 1 SUMMARY (CERVIX)
The standard of care (SOC) for locally advanced cervical cancer, pelvic radiation (RT) with concurrent cisplatin,
is associated with a 30-50% failure rate, and there is no cure for recurrent disease. Most cervical cancers are
caused by infection with Human Papilloma Virus (HPV), and persistent expression of HPV oncogenes supports
a state of chronic stromal inflammation mediated by macrophages. Preclinical studies suggest that tumor
associated macrophages (TAMs) are the most abundant cell type in the tumor microenvironment (TME) after RT
and exhibit “M2-like” phenotypes that suppress the development of anti-tumor immunity. In our previous work,
we demonstrated that cervical tumor 18F-Fluoro-deoxy-glucose (FDG) uptake on pretreatment positron emission
tomography (PET) is associated with increased TAMs with “M2-like” phenotypes in the cervix TME, and that co-
culture of cervix tumor cells with TAMs increases tumor cell glucose uptake. We propose that TAMs and tumor
cells in the TME co-evolve and mutually adapt their glucose and ROS metabolism to optimize tumor growth. In
this proposal, we will test the hypothesis that SOC CRT induces ROS-mediated “metabolic switches” that alter
gene transcription and metabolism in each cell type, providing a therapeutic opportunity to limit this metabolic
co-dependency and improve outcomes after SOC CRT by promoting RT induced anti-tumor immunity. Here we
will use a combination of state of the art single cell and spatially resolved profiling of human tumors together with
state of the are imaging to determine the impact of SOC CRT induced changes in metabolism in tumor cells and
TAMs on CRT sensitivity, and perform mechanistic preclinical studies to determine how this impacts the
development of anti-tumor immunity. In Aim 1 we will determine the longitudinal impact of SOC CRT on
metabolism and inflammatory signaling in cervix tumor cells. Our preliminary data supports targeting CRT
induced upregulation of SOD2 and NRF2 in tumor cells. We will study CRT associated changes in ROS and
mitochondrial metabolism using tumor organoids and novel mouse models. In Aim 2 we will determine the impact
of SOC CRT on TAM and T cell phenotype and function in the cervix TME. We will study the effect of TAM
targeting using novel imaging approaches, antibody depletion and CCR2 inhibitors in mouse models. In Aim 3
we will integrate longitudinal changes in PET imaging features with CRT associated changes in gene expression
to improve patient classifiers and response prediction. In these studies, we will use FDG in addition to 64Cu-
DOTA-ECLi, a novel PET tracer for CCR2+ TAMs. Finally, we will work with a trainee from our Training Core,
METEORITE, to prioritize new leads from our human data. This trainee will explore the contribution of immune
checkpoint blockade (ICB) when added to SOC CRT. ICB is well known to alter metabolism in immune cells,
and we will synthesize our data and approaches to achieve our ulti...

## Key facts

- **NIH application ID:** 10912702
- **Project number:** 5U54CA274318-02
- **Recipient organization:** WASHINGTON UNIVERSITY
- **Principal Investigator:** Julie Kristina Schwarz
- **Activity code:** U54 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2024
- **Award amount:** $247,065
- **Award type:** 5
- **Project period:** 2023-09-01 → 2028-08-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10912702

## Citation

> US National Institutes of Health, RePORTER application 10912702, Research Project  Cervical Cancer (5U54CA274318-02). Retrieved via AI Analytics 2026-05-25 from https://api.ai-analytics.org/grant/nih/10912702. Licensed CC0.

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