Adoptive Cell Therapy for Patients with Melanoma, Using Tumor-infiltrating Lymphocytes Genetically Engineered to Secrete Interleukin-2

Overview

Journal Hum Gene Ther

Specialties Genetics
Pharmacology

Date 2008 May 1

PMID 18444786

Citations 68

Authors

Bianca Heemskerk

Ke Liu

Mark E Dudley

Laura A Johnson

Andrew Kaiser

Stephanie Downey

Zhili Zheng

Thomas E Shelton

Kant Matsuda

Paul F Robbins

Richard A Morgan

Steven A Rosenberg

Affiliations

Soon will be listed here.

Abstract

Adoptive cell transfer of tumor-infiltrating lymphocytes (TILs) after lymphodepletion mediates regression in 50% of patients with metastatic melanoma. In vivo persistence and telomere length of the transferred cells correlate with antitumor response. In an attempt to prolong the in vivo survival of the transferred cells, TILs were genetically engineered to produce interleukin (IL)-2. In vitro, these transduced TILs secreted IL-2 while retaining tumor specificity and exhibited prolonged survival after IL-2 withdrawal. In a phase I/II clinical trial, seven evaluable patients received transduced TILs and one patient experienced a partial response associated with in vivo persistence of IL-2-transduced TILs in circulating lymphocytes. An additional five patients received transduced TILs in conjunction with IL-2 administration. Persistence of IL-2-transduced TILs was observed in three patients, including one partial responder. The transgene DNA as well as vector-derived IL2 mRNA could be detected for 4 months in responding patients. The low response rate in this trial was possibly due to a reduction in telomere length in cells as a result of prolonged in vitro culture. In this study, insertion of the IL-2 gene into antitumor TILs increased their ability to survive after IL-2 withdrawal in vitro but did not increase their in vivo persistence or clinical effectiveness.

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