An Expanded Peripheral T Cell Population to a Cytotoxic T Lymphocyte (Ctl)-Defined, Melanocyte-Specific Antigen in Metastatic Melanoma Patients Impacts on Generation of Peptide-Specific Ctls but Does Not Overcome Tumor Escape from Immune Surveillance in Metastatic Lesions

It is not known if immune response to T cell–defined human histocompatibility leukocyte antigen (HLA) class I–restricted melanoma antigens leads to an expanded peripheral pool of T cells in all patients, affects cytotoxic T lymphocyte (CTL) generation, and correlates with anti-tumor response in meta...

Descripción completa

Detalles Bibliográficos
Autores principales: Anichini, Andrea, Molla, Alessandra, Mortarini, Roberta, Tragni, Gabrina, Bersani, Ilaria, Di Nicola, Massimo, Gianni, Alessandro M., Pilotti, Silvana, Dunbar, Rod, Cerundolo, Vincenzo, Parmiani, Giorgio
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1999
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2195616/
https://www.ncbi.nlm.nih.gov/pubmed/10477550
_version_ 1782147886908178432
author Anichini, Andrea
Molla, Alessandra
Mortarini, Roberta
Tragni, Gabrina
Bersani, Ilaria
Di Nicola, Massimo
Gianni, Alessandro M.
Pilotti, Silvana
Dunbar, Rod
Cerundolo, Vincenzo
Parmiani, Giorgio
author_facet Anichini, Andrea
Molla, Alessandra
Mortarini, Roberta
Tragni, Gabrina
Bersani, Ilaria
Di Nicola, Massimo
Gianni, Alessandro M.
Pilotti, Silvana
Dunbar, Rod
Cerundolo, Vincenzo
Parmiani, Giorgio
author_sort Anichini, Andrea
collection PubMed
description It is not known if immune response to T cell–defined human histocompatibility leukocyte antigen (HLA) class I–restricted melanoma antigens leads to an expanded peripheral pool of T cells in all patients, affects cytotoxic T lymphocyte (CTL) generation, and correlates with anti-tumor response in metastatic lesions. To this end, a limiting dilution analysis technique was developed that allowed us to evaluate the same frequency of peptide-specific T cells as by staining T cells with HLA–peptide tetrameric complexes. In four out of nine patients, Melan-A/Mart-1(27–35)–specific CTL precursors (CTLp) were ≥1/2,000 peripheral blood lymphocytes and found mostly or only in the CD45RO(+) memory T cell subset. In the remaining five patients, a low (<1/40,000) peptide-specific CTLp frequency was measured, and the precursors were only in the CD45RA(+) naive T cell subset. Evaluation of CTL effector frequency after bulk culture indicated that peptide-specific CTLs could be activated in all patients by using professional antigen-presenting cells as dendritic cells, but CTLp frequency determined the kinetics of generation of specificity and the final number of effectors as evaluated by both limiting dilution analysis and staining with HLA-A*0201–Melan-A/Mart-1 tetrameric complexes. Immunohistochemical analysis of 26 neoplastic lesions from the nine patients indicated absence of tumor regression in most instances, even in patients with an expanded peripheral T cell pool to Melan-A/Mart-1 and whose neoplastic lesions contained a high frequency of tetramer-positive Melan-A/Mart-1–specific T cells. Furthermore, frequent lack of a “brisk” or “nonbrisk” CD3(+)CD8(+) T cell infiltrate or reduced/absent Melan-A/Mart-1 expression in several lesions and lack of HLA class I antigens were found in some instances. Thus, expansion of peripheral immune repertoire to Melan-A/Mart-1 takes place in some metastatic patients and leads to enhanced CTL induction after antigen-presenting cell–mediated selection, but, in most metastatic lesions, it does not overcome tumor escape from immune surveillance.
format Text
id pubmed-2195616
institution National Center for Biotechnology Information
language English
publishDate 1999
publisher The Rockefeller University Press
record_format MEDLINE/PubMed
spelling pubmed-21956162008-04-16 An Expanded Peripheral T Cell Population to a Cytotoxic T Lymphocyte (Ctl)-Defined, Melanocyte-Specific Antigen in Metastatic Melanoma Patients Impacts on Generation of Peptide-Specific Ctls but Does Not Overcome Tumor Escape from Immune Surveillance in Metastatic Lesions Anichini, Andrea Molla, Alessandra Mortarini, Roberta Tragni, Gabrina Bersani, Ilaria Di Nicola, Massimo Gianni, Alessandro M. Pilotti, Silvana Dunbar, Rod Cerundolo, Vincenzo Parmiani, Giorgio J Exp Med Original Article It is not known if immune response to T cell–defined human histocompatibility leukocyte antigen (HLA) class I–restricted melanoma antigens leads to an expanded peripheral pool of T cells in all patients, affects cytotoxic T lymphocyte (CTL) generation, and correlates with anti-tumor response in metastatic lesions. To this end, a limiting dilution analysis technique was developed that allowed us to evaluate the same frequency of peptide-specific T cells as by staining T cells with HLA–peptide tetrameric complexes. In four out of nine patients, Melan-A/Mart-1(27–35)–specific CTL precursors (CTLp) were ≥1/2,000 peripheral blood lymphocytes and found mostly or only in the CD45RO(+) memory T cell subset. In the remaining five patients, a low (<1/40,000) peptide-specific CTLp frequency was measured, and the precursors were only in the CD45RA(+) naive T cell subset. Evaluation of CTL effector frequency after bulk culture indicated that peptide-specific CTLs could be activated in all patients by using professional antigen-presenting cells as dendritic cells, but CTLp frequency determined the kinetics of generation of specificity and the final number of effectors as evaluated by both limiting dilution analysis and staining with HLA-A*0201–Melan-A/Mart-1 tetrameric complexes. Immunohistochemical analysis of 26 neoplastic lesions from the nine patients indicated absence of tumor regression in most instances, even in patients with an expanded peripheral T cell pool to Melan-A/Mart-1 and whose neoplastic lesions contained a high frequency of tetramer-positive Melan-A/Mart-1–specific T cells. Furthermore, frequent lack of a “brisk” or “nonbrisk” CD3(+)CD8(+) T cell infiltrate or reduced/absent Melan-A/Mart-1 expression in several lesions and lack of HLA class I antigens were found in some instances. Thus, expansion of peripheral immune repertoire to Melan-A/Mart-1 takes place in some metastatic patients and leads to enhanced CTL induction after antigen-presenting cell–mediated selection, but, in most metastatic lesions, it does not overcome tumor escape from immune surveillance. The Rockefeller University Press 1999-09-06 /pmc/articles/PMC2195616/ /pubmed/10477550 Text en © 1999 The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Original Article
Anichini, Andrea
Molla, Alessandra
Mortarini, Roberta
Tragni, Gabrina
Bersani, Ilaria
Di Nicola, Massimo
Gianni, Alessandro M.
Pilotti, Silvana
Dunbar, Rod
Cerundolo, Vincenzo
Parmiani, Giorgio
An Expanded Peripheral T Cell Population to a Cytotoxic T Lymphocyte (Ctl)-Defined, Melanocyte-Specific Antigen in Metastatic Melanoma Patients Impacts on Generation of Peptide-Specific Ctls but Does Not Overcome Tumor Escape from Immune Surveillance in Metastatic Lesions
title An Expanded Peripheral T Cell Population to a Cytotoxic T Lymphocyte (Ctl)-Defined, Melanocyte-Specific Antigen in Metastatic Melanoma Patients Impacts on Generation of Peptide-Specific Ctls but Does Not Overcome Tumor Escape from Immune Surveillance in Metastatic Lesions
title_full An Expanded Peripheral T Cell Population to a Cytotoxic T Lymphocyte (Ctl)-Defined, Melanocyte-Specific Antigen in Metastatic Melanoma Patients Impacts on Generation of Peptide-Specific Ctls but Does Not Overcome Tumor Escape from Immune Surveillance in Metastatic Lesions
title_fullStr An Expanded Peripheral T Cell Population to a Cytotoxic T Lymphocyte (Ctl)-Defined, Melanocyte-Specific Antigen in Metastatic Melanoma Patients Impacts on Generation of Peptide-Specific Ctls but Does Not Overcome Tumor Escape from Immune Surveillance in Metastatic Lesions
title_full_unstemmed An Expanded Peripheral T Cell Population to a Cytotoxic T Lymphocyte (Ctl)-Defined, Melanocyte-Specific Antigen in Metastatic Melanoma Patients Impacts on Generation of Peptide-Specific Ctls but Does Not Overcome Tumor Escape from Immune Surveillance in Metastatic Lesions
title_short An Expanded Peripheral T Cell Population to a Cytotoxic T Lymphocyte (Ctl)-Defined, Melanocyte-Specific Antigen in Metastatic Melanoma Patients Impacts on Generation of Peptide-Specific Ctls but Does Not Overcome Tumor Escape from Immune Surveillance in Metastatic Lesions
title_sort expanded peripheral t cell population to a cytotoxic t lymphocyte (ctl)-defined, melanocyte-specific antigen in metastatic melanoma patients impacts on generation of peptide-specific ctls but does not overcome tumor escape from immune surveillance in metastatic lesions
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2195616/
https://www.ncbi.nlm.nih.gov/pubmed/10477550
work_keys_str_mv AT anichiniandrea anexpandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT mollaalessandra anexpandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT mortariniroberta anexpandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT tragnigabrina anexpandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT bersaniilaria anexpandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT dinicolamassimo anexpandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT giannialessandrom anexpandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT pilottisilvana anexpandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT dunbarrod anexpandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT cerundolovincenzo anexpandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT parmianigiorgio anexpandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT anichiniandrea expandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT mollaalessandra expandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT mortariniroberta expandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT tragnigabrina expandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT bersaniilaria expandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT dinicolamassimo expandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT giannialessandrom expandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT pilottisilvana expandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT dunbarrod expandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT cerundolovincenzo expandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions
AT parmianigiorgio expandedperipheraltcellpopulationtoacytotoxictlymphocytectldefinedmelanocytespecificantigeninmetastaticmelanomapatientsimpactsongenerationofpeptidespecificctlsbutdoesnotovercometumorescapefromimmunesurveillanceinmetastaticlesions

Ejemplares similares