# Identifying the Cellular and Molecular Targets of JAK/STAT-Driven Adipose Wasting to Reverse Cancer Cachexia

> **NIH NIH R01** · UT SOUTHWESTERN MEDICAL CENTER · 2024 · $198,888

## Abstract

Research, Mentoring, and Career Development Plan
I. Research Plan
Parent Grant Title: JAK/STAT dependent Tumor-Cytokine-Adipose Axis Regulating Cachexia
Parent Grant Abstract:
Cancer cachexia (CCX), wasting of muscle and/or adipose, is associated with 20-30% of all cancer related
deaths. Our clinical studies have shown that the presence of CCX is associated with a 50% decrease in median
survival (14 months vs 28 months, p<0.001) independent of tumor-directed therapies. There are no FDAapproved
CCX regimens, with a majority of trials focused on limiting sarcopenia. Using multiple established
murine CCX mouse models, we consistently observed significant adipose tissue loss compared to muscle
atrophy. Furthermore, blocking adipocyte lipolysis using global lipase null mice limited both adipose wasting and
sarcopenia in murine models of CCX. Understanding upstream mechanisms cancers use to provoke adipose
lipolysis and wasting could offer novel therapeutic targets to reverse CCX syndrome.
The complex intracellular (stromal, vascular, immune, and adipocyte) interactions within adipose tissue
ultimately regulate CCX wasting by altering the relative signals of adipocyte triglyceride lipolysis and synthesis.
To understand the convergence of these interactions, we developed an in vitro CCX adipocyte assay to screen
secreted factors from CCX lines that increase adipose inflammation and wasting by inducing adipocyte lipolysis
and identified the cytokine leukemia inhibitory factor (LIF). Through the JAK-dependent inflammatory
reprogramming of adipose tissue in mice, recombinant LIF caused a decrease in adipose mass by >50%, lean
mass, and body weight by >10%, recapitulating CCX. LIF also altered the adipose expression and systemic
levels of other cyto/adipokines to amplify this inflammation. Use of JAK inhibitors in murine CCX models led to
decreased adipose inflammation (decreased STAT3 phosphorylation), adipocyte lipolysis, and adipose/muscle
wasting, all increasing survival. To understand the contributions of adipose intracellular signaling in the regulation
of CCX adipose inflammation, we selectively silenced LIFR-a or STAT3 in adipocytes. Both mouse models
doubled their adipose mass compared to littermate controls during development highlighting an inverse CCX
phenotype. When allotransplanted with CCX tumors, both models still demonstrated adipose inflammation with
persistent STAT3 phosphorylation, resulting in a partial suppression of CCX and defining the non-adipocyte
cellular contributions of adipose to CCX wasting. FACS analysis verified longitudinal enrichment of immune cells
during CCX progression, offering additional tumor/cytokine targets supporting CCX adipose inflammation and
wasting. We hypothesize that CCX adipose inflammation occurs via a JAK-dependent Tumor-CytokineAdipose
Axis that reprograms adipose through JAK/STAT signaling of multiple cellular subtypes to increase
adipocyte lipolysis and alter secretion of cyto/adipokines, resulting in...

## Key facts

- **NIH application ID:** 11063032
- **Project number:** 3R01CA266900-03S1
- **Recipient organization:** UT SOUTHWESTERN MEDICAL CENTER
- **Principal Investigator:** Rodney E Infante
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2024
- **Award amount:** $198,888
- **Award type:** 3
- **Project period:** 2022-09-22 → 2025-08-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/11063032

## Citation

> US National Institutes of Health, RePORTER application 11063032, Identifying the Cellular and Molecular Targets of JAK/STAT-Driven Adipose Wasting to Reverse Cancer Cachexia (3R01CA266900-03S1). Retrieved via AI Analytics 2026-05-23 from https://api.ai-analytics.org/grant/nih/11063032. Licensed CC0.

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