Combined Immune Checkpoint Blockade Increases CD8+CD28+PD-1+ Effector T Cells and Provides a Therapeutic Strategy for Patients with Neuroblastoma

Overview

Journal Oncoimmunology

Specialty Allergy & Immunology

Date 2021 Jan 25

PMID 33489468

Citations 21

Authors

Soheila Shirinbak

Randall Y Chan

Shilpa Shahani

Sakunthala Muthugounder

Rebekah Kennedy

Long T Hung

G Esteban Fernandez

Michael D Hadjidaniel

Babak Moghimi

Michael A Sheard

Alan L Epstein

Muller Fabbri

Hiroyuki Shimada

Shahab Asgharzadeh

Affiliations

Soon will be listed here.

Abstract

Immune checkpoint therapy has resulted in minimal clinical response in many pediatric cancers. We sought to understand the influence of immune checkpoint inhibition using anti-PD-1 and anti-CTLA-4 antibodies individually, in combination, and after chemotherapy on immune responses in minimal and established murine neuroblastoma models. We also sought to understand the role of the tumor microenvironment (TME) and PD-L1 expression and their alteration post-chemotherapy in our models and human tissues. PD-L1 expression was enriched in human tumor-associated macrophages and up-regulated after chemotherapy. In a murine minimal disease model, single and dual immune checkpoint blockade promoted tumor rejection, improved survival, and established immune memory with long-term anti-tumor immunity against re-challenge. In an established tumor model, only dual immune checkpoint blockade showed efficacy. Interestingly, dual immune checkpoint therapy distinctly influenced adaptive and innate immune responses, with significant increase in CD8CD28PD-1 T cells and inflammatory macrophages (CD11bCD11cF4/80Ly6C) in tumor-draining lymph nodes. Adding chemotherapy before immunotherapy provided significant survival benefit for mice with established tumors receiving anti-PD-1 or dual immune checkpoint blockade. Our findings demonstrate anti-PD-1 and anti-CTLA-4 therapy induces a novel subset of effector T cells, and support administration of induction chemotherapy immediately prior to immune checkpoint blockade in children with high-risk neuroblastoma.

Citing Articles

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