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New checkpoint gene demonstrates ability to supercharge immune cells against cancer

Date:
September 13, 2022
Source:
University of Minnesota Medical School
Summary:
Researchers have investigated the role of a new intracellular checkpoint gene in regulating T-cell function against solid tumors. Results show that the checkpoint gene plays a key role in suppressing the ability of human T-cells to recognize and attack cancer cells.
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University of Minnesota researchers and their collaborators at the National Cancer Institute (NCI) investigated the role of a new intracellular checkpoint gene in regulating T-cell function against solid tumors. Known as CISH, the team published results in Med, a Cell Press journal, that show the checkpoint gene plays a key role in suppressing the ability of human T-cells to recognize and attack cancer cells.

When CISH is disabled, T-cells more effectively recognize mutated proteins produced by tumors. CISH inhibition also preserved T-cell fitness and made T-cells more responsive to existing checkpoint therapies, suggesting a new avenue to make breakthroughs in cancer immunotherapy.

"It is a true bench-to-bedside story that is currently being deployed in patients with metastatic gastrointestinal cancer who have exhausted virtually all other treatment options," said Beau Webber, PhD, an assistant professor at the University of Minnesota Medical School and member of the Masonic Cancer Center. "We are applying what we found in the lab to patients seeking care for gastrointestinal cancer."

As CISH resides within the cell, it cannot be inhibited using antibody blockades in the same way that other checkpoint molecules have been targeted. To overcome this challenge, the research team led by University faculty Branden Moriarity, PhD, and Dr. Webber utilized CRISPR gene editing -- a process of cutting a DNA sequence to delete and insert other sequences -- to safely and effectively knockout the CISH gene in human T-cells. This process robustly enhanced T-cells' ability to recognize and kill tumor cells, and served as the preclinical basis for the first-in-human clinical trial using CRISPR engineered T cells at the University of Minnesota -- only the second CRISPR clinical trial authorized by the Food and Drug Administration at the time.

"This work is the culmination of a tremendous, multidisciplinary effort encompassing basic mechanistic immune biology, cutting-edge techniques in genome editing, and the latest advancements in adoptive cellular immunotherapy," said Dr. Webber.

Gene editing offers a powerful new tool that allows researchers to hard-wire checkpoint inhibition into the specific immune cells that are fighting the tumor, thereby accelerating clinical translation of new approaches. Intracellular checkpoint genes, like CISH, are of particular interest because they offer a new avenue to enhance immune cell function against cancer.

The research team continues its ongoing clinical trial and is conducting correlative studies to evaluate the efficacy and safety of CISH edited tumor infiltrating lymphocytes. They are also investigating additional strategies to further improve the function of engineered immune cells against solid cancers.

Funding was provided by Intima Bioscience and the Intramural program CCR at NCI..


Story Source:

Materials provided by University of Minnesota Medical School. Original written by Alex Smith. Note: Content may be edited for style and length.


Journal Reference:

  1. Douglas C. Palmer, Beau R. Webber, Yogin Patel, Matthew J. Johnson, Christine M. Kariya, Walker S. Lahr, Maria R. Parkhurst, Jared J. Gartner, Todd D. Prickett, Frank J. Lowery, Rigel J. Kishton, Devikala Gurusamy, Zulmarie Franco, Suman K. Vodnala, Miechaleen D. Diers, Natalie K. Wolf, Nicholas J. Slipek, David H. McKenna, Darin Sumstad, Lydia Viney, Tom Henley, Tilmann Bürckstümmer, Oliver Baker, Ying Hu, Chunhua Yan, Daoud Meerzaman, Kartik Padhan, Winnie Lo, Parisa Malekzadeh, Li Jia, Drew C. Deniger, Shashank J. Patel, Paul F. Robbins, R. Scott McIvor, Modassir Choudhry, Steven A. Rosenberg, Branden S. Moriarity, Nicholas P. Restifo. Internal checkpoint regulates T cell neoantigen reactivity and susceptibility to PD1 blockade. Med, 2022; DOI: 10.1016/j.medj.2022.07.008

Cite This Page:

University of Minnesota Medical School. "New checkpoint gene demonstrates ability to supercharge immune cells against cancer." ScienceDaily. ScienceDaily, 13 September 2022. <www.sciencedaily.com/releases/2022/09/220913140901.htm>.
University of Minnesota Medical School. (2022, September 13). New checkpoint gene demonstrates ability to supercharge immune cells against cancer. ScienceDaily. Retrieved December 21, 2024 from www.sciencedaily.com/releases/2022/09/220913140901.htm
University of Minnesota Medical School. "New checkpoint gene demonstrates ability to supercharge immune cells against cancer." ScienceDaily. www.sciencedaily.com/releases/2022/09/220913140901.htm (accessed December 21, 2024).

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