Immune landscape of neoadjuvant chemoradiotherapy: involvement of MAL, a T-cell differentiation protein
KOSEI NAKAJIMA, YOSHINORI INO

TL;DR
This study shows that neoadjuvant therapy boosts anti-tumor immunity by increasing CD8+ T-cells and activating immune pathways like DC-SIGN and MAL in pancreatic cancer patients.
Contribution
The first report of increased MAL+ lymphocytes following neoadjuvant therapy in solid tumors.
Findings
NAT upregulated 212 immune-related genes, including DC-SIGN and MAL.
NAT activated 13 immune pathways, such as T-cell receptor signaling.
NAT increased CD8+ T-cells and accumulation of DC-SIGN+ dendritic cells and MAL+ lymphocytes.
Abstract
Neoadjuvant/preoperative therapy (NAT) involves the administration of chemotherapy, with or without radiation, prior to surgical resection. This approach is commonly used for locally advanced tumors to reduce tumor volume, improve resectability, and minimize the need for extensive surgical procedures. While NAT has been shown to be effective in inducing local anti-tumor immunity in potentially resectable solid tumors, the underlying molecular mechanisms remain poorly understood. Cohort samples from pancreatic cancer patients who underwent NAT (n = 26) and those who did not (n = 20) were analyzed. Changes in the immune microenvironment induced by NAT were assessed using stratified bioinformatic approaches, including heatmap analysis of immune-related genes selected via Gene Ontology, Gene Set Enrichment Analysis (GSEA) with the immunologic signature database, and Ingenuity Pathway…
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Taxonomy
TopicsCancer Immunotherapy and Biomarkers · Colorectal and Anal Carcinomas · Mycobacterium research and diagnosis
