Reprogramming Antitumor Immune Responses with microRNAs

Abstract

During the previous funding cycle we demonstrated that miR-181a is up-regulated in tumor-reactive T cells as they survive in the ovarian cancer microenvironment, and that miR-181a overexpressing anti-tumor T cells exert defective protection against malignant progression, compared to control anti-tumor lymphocytes. These effects are not the result of impaired memory differentiation, but are most likely caused by a functional defect in their effector activity, probably due to impaired Tryptophan (and, subsequently, glucose) metabolism. Correspondingly, downregulating, rather than augmenting, the expression of miR-181a in anti-tumor T cells, becomes a desirable goal for lymphocyte adoptive transfer protocols. Furthermore, we have demonstrated for the first time the feasibility of re-programming immune responses against established ovarian orthotropic tumors through intraperitoneal delivery of nanocomplexes carrying synthetic miRNAs. Our results provide a rationale for the modulation of miRNA activity in tumor leukocytes as a novel cancer intervention.

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Document Details

Document Type
Technical Report
Publication Date
Oct 01, 2012
Accession Number
ADA585107

Entities

People

  • Jose R Conejo-Garcia

Organizations

  • University of Pennsylvania

Tags

DTIC Thesaurus Topics

  • Adaptive Immunity
  • Biological Factors
  • Blood
  • Cancer
  • Cell Physiological Processes
  • Cells
  • Epithelial Cells
  • Health Services
  • Lymphatic System
  • Lymphocytes
  • Neoplasms
  • Ovarian Cancer
  • Peptides
  • Proteins

Fields of Study

  • Biology

Readers

  • Molecular and Cellular Biology
  • Oncology (Cancer Research).