The Dynamic Entropy of Tumor Immune Infiltrates: The Impact of Recirculation, Antigen-Specific Interactions, and Retention on T Cells in Tumors

Tiffany C Blair; Alejandro F Alice; Lauren Zebertavage; Marka R Crittenden; Michael J Gough

doi:10.3389/fonc.2021.653625

The Dynamic Entropy of Tumor Immune Infiltrates: The Impact of Recirculation, Antigen-Specific Interactions, and Retention on T Cells in Tumors

Front Oncol. 2021 Apr 22:11:653625. doi: 10.3389/fonc.2021.653625. eCollection 2021.

Authors

Tiffany C Blair^{1

2}, Alejandro F Alice², Lauren Zebertavage^{1

2}, Marka R Crittenden^{2

3}, Michael J Gough²

Affiliations

¹ Molecular Microbiology and Immunology, Oregon Health and Sciences University (OHSU), Portland, OR, United States.
² Earle A. Chiles Research Institute, Providence Cancer Institute, Providence Portland Medical Center, Portland, OR, United States.
³ The Oregon Clinic, Portland, OR, United States.

Abstract

Analysis of tumor infiltration using conventional methods reveals a snapshot view of lymphocyte interactions with the tumor environment. However, lymphocytes have the unique capacity for continued recirculation, exploring varied tissues for the presence of cognate antigens according to inflammatory triggers and chemokine gradients. We discuss the role of the inflammatory and cellular makeup of the tumor environment, as well as antigen expressed by cancer cells or cross-presented by stromal antigen presenting cells, on recirculation kinetics of T cells. We aim to discuss how current cancer therapies may manipulate lymphocyte recirculation versus retention to impact lymphocyte exclusion in the tumor.

Keywords: T cell; clonality analysis; recirculation; recruitment; retention; tumor.

Publication types

Review

Abstract

Publication types

Grants and funding