# Determine the mechanisms of acquired brain-tropism

> **NIH NIH U54** · STANFORD UNIVERSITY · 2021 · $345,831

## Abstract

ABSTRACT – PROJECT 1
For patients with advanced cancer, 30% will be afflicted with brain metastases, the cause of devastating
neurologic morbidity and mortality. As a result, the incidence of brain metastasis is 170,000 new cases per a
year. For screening, MRI is the preferred imaging modality for brain metastasis, but is prohibitively expensive
and lacks relevant molecular information. We lack predictive models to identify patients at high risk for brain
metastases for screening, as treatment efficacy and morbidity are linked to early detection. Treatment involves
surgery and radiotherapy but with a noticeable lack of prognostic or predictive biomarkers for disease
progression or treatment. Our central hypothesis is that there are common intrinsic features to the tumor and
extrinsic features to the brain microenvironment relevant for cancer brain tropism and response to therapies.
We will determine these features’ association to microglia (Project 2) and peripheral immune surveillance
(Project 3), leveraging biological models to test these discoveries. We will identify intrinsic cellular genomic
features relevant for brain metastasis that can be generalized across many primary tumor types. Likewise, we
hypothesize there are extrinsic features of the tumor cellular milieu in the brain that facilitate the seeding and
maintenance of these metastases. (1) For determining extrinsic cellular tropism, we will characterize the immune
cell types’ states and function in the brain metastasis tumor microenvironment. Using single cell genomics, we
will determine the distribution and functional status of the TME microglia and macrophages across different tumor
types that have CNS metastasis. In parallel, using three dimensional organoids, we will determine the TME-
based macrophage response to anti-CD47, a potent modulator of macrophage function. Our results will
determine the cellular genomic characteristics and functional status of TME macrophages/microglial cells and
their regulatory states. (2) For intrinsic tropism factors, we will analyze genomic features of the primary tumor
and extrinsic features of the brain that indicate increased propensity for brain metastasis. We will conduct
genomic sequencing analysis on matched primary and metachronous brain metastasis, with complete treatment
exposure patient history. With this data, we will determine critical cancer genome features such as the extent of
genomic instability, intratumoral clonal diversity, treatment selection pressure, and TME immune cell composition
that are associated with brain metastatic risk. Our results will identify genomic biomarkers indicative of increased
risk of brain metastasis across different tumor types. (3) Finally, we will use the overlapping data set for intrinsic
genomic factors to determine if there are predictive genomic signatures of radioresistant brain metastases. We
hypothesize there are specific genomic features of primary tumors that are radiotherapy predictors. Thes...

## Key facts

- **NIH application ID:** 10272359
- **Project number:** 1U54CA261717-01
- **Recipient organization:** STANFORD UNIVERSITY
- **Principal Investigator:** Hanlee P Ji
- **Activity code:** U54 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2021
- **Award amount:** $345,831
- **Award type:** 1
- **Project period:** 2021-09-21 → 2026-08-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10272359

## Citation

> US National Institutes of Health, RePORTER application 10272359, Determine the mechanisms of acquired brain-tropism (1U54CA261717-01). Retrieved via AI Analytics 2026-05-24 from https://api.ai-analytics.org/grant/nih/10272359. Licensed CC0.

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