In Situ T Cell Responses Against Melanoma Comprise High Numbers of Locally Expanded T Cell Clonotypes

Author:

thor Straten Per1,Guldberg Per1,Grønbæk Kirsten12,Hansen Mia Riise1,Kirkin Alexei F.1,Seremet Tina1,Zeuthen Jesper1,Becker Jürgen C.3

Affiliation:

1. *Department of Tumor Cell Biology, Institute of Cancer Biology, Danish Cancer Society, Copenhagen, Denmark;

2. †Department of Pathology, Herlev Hospital, Copenhagen, Denmark; and

3. ‡Department of Dermatology, School of Medicine, Würzburg, Germany

Abstract

Abstract It is well established that melanoma cells express Ags that are recognized by autologous T cells in vitro. Tumor-infiltrating lymphocytes in situ comprise clonotypic T cells, suggesting that their expansion is driven by Ag stimulation. Still, little is known about the detailed characteristics of the in situ T cell response. In the present study, we scrutinized this response by analyzing multiple metastatic lesions for the presence of clonotypic T cells. This approach was chosen to distinguish whether the clonal T cell expansion occurs as a systemic or localized phenomenon. TCR clonotype mapping of six s.c. metastases from two patients revealed the presence of multiple (from 40 to >60) clonotypic T cells in all lesions. Clonotypic T cells were present in TCR β-variable regions expressed both at high and low levels. Comparison of the T cell clonotypes present in different lesions from individual patients demonstrated that, in general, clonotypes were exclusively detected in a single lesion. Hence, anti-melanoma T cell responses are much more heterogeneous than previously anticipated and accommodate a predominance of strictly localized T cell clonotypes.

Publisher

The American Association of Immunologists

Subject

Immunology,Immunology and Allergy

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