# An organotypic model recapitulating colon cancer microenvironment and metastasis

> **NIH NIH U01** · UT SOUTHWESTERN MEDICAL CENTER · 2021 · $521,870

## Abstract

PROJECT SUMMARY
 This U01 is in response to FOA PAR-16-105 Cancer Tissue Engineering Collaborative: Enabling
Biomimetic Tissue-Engineered Technologies for Cancer Research. In it we will address the substantial gap in
our knowledge of the initiation and progression of metastatic colorectal cancer (CRC). This gap is due, in large
part, to the fact that current in vitro, ex vivo, and even in vivo research models are hard to establish or have
limited applicability. Accordingly, our objectives are to show the utility of three innovative models of metastasis
(a long-term organotypic model and a model that uses multi-organ microfluidic devices) and a new in vivo model
(immunocompetent blastocyst model). Using these models, we will investigate the interactive cellular secretome,
differentiation, migration and invasion of the primary and metastatic fibroblast tumor microenvironment in order
to identify critical contributions to CRC metastasis. Our hypothesis is: inflammation-associated fibroblasts and
altered metabolic conditions promote epithelial metastasis via transcriptional regulation. Based on our recent
successful engineering of novel models, we propose 3 Aims. Aim 1. To integrate cytokine-secreting stroma into
our organotypic model in order to study the influence of inflammation on cancer stem cells (SCs) and on
invasion/migration cell phenotypes. Aim 2. To engineer a liver metastasis model using a microfluidic body-on-a-
chip platform to study transcriptome and epigenetic reprogramming of metastatic cells. Aim 3. To validate our in
vitro models using in vivo immunoproficient murine metastatic models. In Aim 1, decellularized human colons
will be repopulated with normal or cancerous fibroblasts from the stroma, and cancer epithelial cells in the form
of cancer SCs and organoids to ask how these manipulations influence invasion and differentiation in this model.
To complement the cellular findings, we will identify alterations in the transcriptome using RNA-seq and ATAC-
seq. Aim 2 uses the innovative body-on-a chip microfluidic device to test autocrine and paracrine proliferative
and secretory responses under conditions that favor oncogenic progression, including hypoxia and low glucose.
As in Aim 1, epithelia and fibroblasts in the different milieus will be transcriptionally profiled. Aim 3 uses a new
immunocompetent blastocyst model and will undergo the same transcriptional profiling. All 3 models will be
linked using comparative, informatics approaches. The approach is innovative as it uses human colon tissues in
all Aims and asks about the transcriptional contribution and landscape of accessible chromatin in each model.
Our multidisciplinary team includes a colorectal surgeon-scientist and biomedical engineers with expertise in
cancer SCs, signaling, metastases, and organotypic and organ-on-a-chip platforms. The findings will be
significant, as they will establish improved approaches for studying the pathogenesis of advanced CRC, and for
devel...

## Key facts

- **NIH application ID:** 10246419
- **Project number:** 5U01CA214300-06
- **Recipient organization:** UT SOUTHWESTERN MEDICAL CENTER
- **Principal Investigator:** Emina Hui-Na Huang
- **Activity code:** U01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2021
- **Award amount:** $521,870
- **Award type:** 5
- **Project period:** 2017-09-25 → 2024-08-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10246419

## Citation

> US National Institutes of Health, RePORTER application 10246419, An organotypic model recapitulating colon cancer microenvironment and metastasis (5U01CA214300-06). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/10246419. Licensed CC0.

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