# Immunomodulatory effects of bortezomib on antitumor CD8 T-NK cell crosstalk

> **NIH NIH SC1** · MEHARRY MEDICAL COLLEGE · 2020 · $327,375

## Abstract

Adoptive cell immunotherapy with immune checkpoint inhibitors has shown clinical promise. Unfortunately,
despite optimizations of treatments, relapse-free survival rates still range between 17-21% in most metastatic
solid tumors. This occurs via various tumor-induced abnormalities including immunosuppression and
emergence of immune escape tumor variants. Tumor growth can induce immunosuppression by multiple
mechanisms. We identified a novel mechanism of immunosuppression wherein tumor interferes with the host
hematopoietic Notch system that is critical for lymphocyte differentiation and function. Our studies in solid
tumor models demonstrate that lymphocyte teamwork, specifically between CD8+T cell and NK cell effectors, is
essential to eradicate tumor cells. However, immunosuppressive chronic inflammation in the tumor
microenvironment hinders this phenomenon. Thus, strategies that can reverse Notch dysfunction in
lymphocytes and restore the CD8+T–NK crosstalk are critical for effective tumor eradication and durable
remission. Facilitated by SCORE funding support, we found that proteasome inhibitor bortezomib modulates
Notch signaling in lymphocytes and enhances their antitumor activity. Additionally, our data also indicate that
bortezomib may augment CD8+T and NK cell crosstalk. Based on these data, we hypothesize that bortezomib
overcomes tumor-induced immunosuppression by enhancing the antitumor adaptive and innate immune
effector crosstalk via modulation of the hematopoietic Notch system. In this competing renewal application, we
propose to extend our studies to the next level whereby we can advance our basic insights into CD8+T–NK
crosstalk and Notch-mediated lymphocyte mechanisms into a preclinical therapeutic setting. We will test our
hypothesis by addressing how bortezomib can facilitate the CD8+T–NK crosstalk (Aim 1), and Notch-
dependent mechanisms affecting antitumor lymphocyte cross-talk (Aim 2). Investigations will include genetic
approaches based on the use of unique cell type-specific Notch ligand conditional knockout mice that we have
generated to clearly define the roles of dendritic cell-bound ligands in antitumor CD8+T–NK functional
crosstalk. In Aim 3, we propose to evaluate the therapeutic impact of bortezomib-mediated enhancement of
Notch signaling and CD8+T–NK crosstalk on tumor rejection and relapse-free survival. We will use an inducible
lung cancer model carrying EGFR mutations. We will integrate bortezomib and adoptive CD8+T and NK cell
transfers along with EGFR-targeted therapy and evaluate the impact of this combinatorial regimen on tumor
remission and relapse-free survival. Altogether, the studies proposed in this SC1 renewal application will
unravel novel mechanisms underlying lymphocyte antitumor crosstalk, and will provide innovative insight into
modulation of Notch regulatory lymphocyte mechanisms using bortezomib for translation into clinically relevant
therapeutics in advanced-stage, mutant, or resistant lung c...

## Key facts

- **NIH application ID:** 9999944
- **Project number:** 5SC1CA182843-08
- **Recipient organization:** MEHARRY MEDICAL COLLEGE
- **Principal Investigator:** Anil Shanker
- **Activity code:** SC1 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $327,375
- **Award type:** 5
- **Project period:** 2013-07-12 → 2023-08-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9999944

## Citation

> US National Institutes of Health, RePORTER application 9999944, Immunomodulatory effects of bortezomib on antitumor CD8 T-NK cell crosstalk (5SC1CA182843-08). Retrieved via AI Analytics 2026-05-26 from https://api.ai-analytics.org/grant/nih/9999944. Licensed CC0.

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