recast-jats-build

ec6cccc6e1

jitc

J Immunother Cancer

40425

Journal for ImmunoTherapy of Cancer

J Immunother Cancer

2051-1426

BMJ Publishing Group Ltd

BMC2051-1426-2-S3-P243

694

10.1186/2051-1426-2-S3-P243

/jitc/2/Suppl_3/P243.atom

Poster Presentation

Predictive immune biomarker signatures in the tumor microenvironment of melanoma metastases associated with tumor-infiltrating lymphocyte (TIL) therapy

Chen

Jieqing

12Creasy

Caitlin

1Torres-Cabala

Carlos Antonio

1Ekmekcioglu

Suhendan

1Maiti

Sourindra N

1Kale

Charuta

1Haymaker

Cara

1Roszik

Jason

1Bassett

Roland L

Jr1Hu

Jianhua

1Wang

Zhiqiang

1Ma

Wencai

1Davis

R Eric

1Bernatchez

Chantale

1Hwu

Patrick

1Radvanyi

Laszlo

23 Aff1

grid.267308.8

0000000092062401

M.D. Anderson Cancer Centre (MDACC)University of Texas

Houston

USA Aff2

Lion Biotechnologies

Woodland Hills

USA Aff3

grid.170693.a

000000012353285X

Moffitt Cancer Center

Tampa

USA

122014

6112014

8112019

6112014

2Suppl 3

Abstracts of the 29th Annual Scientific Meeting of the Society for Immunotherapy of Cancer (SITC)

P243

Â© The Author(s). 2014

2014

This article is published under license to BioMed Central Ltd. This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.

MelanomaOverall SurvivalAdoptive Cell TherapyArchive Tumor SampleRegulate NFkB Signaling

6-9 November 2014

Society for Immunotherapy of Cancer 29th Annual Meeting

National Harbor, MD, USA

publisher-imprint-name

BioMed Central

volume-issue-count

issue-article-count

290

issue-toc-levels

issue-copyright-holder

The Author(s)

issue-copyright-year

2014

article-contains-esm

article-numbering-style

Unnumbered

article-registration-date-year

2014

article-registration-date-month

article-registration-date-day

article-toc-levels

toc-levels

volume-type

Regular

journal-product

ArchiveJournal

numbering-style

Unnumbered

article-grants-type

OpenChoice

metadata-grant

OpenAccess

abstract-grant

OpenAccess

bodypdf-grant

OpenAccess

bodyhtml-grant

OpenAccess

bibliography-grant

OpenAccess

esm-grant

OpenAccess

online-first

false

pdf-file-reference

BodyRef/PDF/40425_2014_Article_694.pdf

target-type

OnlinePDF

issue-type

Supplement

article-type

Abstract

journal-subject-primary

Medicine & Public Health

journal-subject-secondary

Oncology

conf-event-url-1

http://www.eventscribe.com/2014/sitc/

Meeting abstracts

Adoptive cell therapy using autologous TIL is a promising immunotherapy for metastatic melanoma. This study was aimed at finding predictive biomarkers in TIL patients, using IHC and gene expression analysis on original tumors used to expand TIL. The purpose was to find factors associated with optimal TIL outgrowth from melanoma tumors and ultimately clinical response to therapy. We found a significant differences in CD8, CD4 and CD3 staining in the tumors between good TIL growers and poor growers by IHC (p < 0.0001, respectively). Interestingly, the CD8 expression in the original tumors also correlated with the percentage of CD8+ T cells in the final TIL product after expansion. Using a new droplet digital PCR assay using TCR Vβ-specific primers called QuanTILfy™, we also found that good TIL growers had a higher TCR Vβ gene signal than samples from poor growers (p = 0.008 Mann-Whitney test) suggesting that this genetic test may be useful in selecting patients for TIL therapy. Gene expression profiling of 595 immunologically-relevant genes found differences in a number of genes in tumors of patients having good TIL growth versus poor TIL growth, such as CD8β and CD3δ, CD45RA, ICOS, PD-1, STAT4. Interestingly, CD8 gene expression was significantly correlated with immunosuppression pathway genes, such as PD-L1, PD-1, FoxP3, and IDO that was confirmed by IHC analysis. Strikingly, IHC analysis of these markers in original tumors, together with CD8, were also found to be predictive of overall survival (OS) after TIL infusion. There were also differences in key genes in tumors of clinical responders and non-responders to TIL treatment. One gene, IRAK1, was particularly interesting as it regulates NFkB signaling and pro-inflammatory cytokine production associated with decreased anti-tumor adaptive immunity. Both gene expression and IHC analysis found an association between higher IRAK1 and decreased OS and relapse-free survival after TIL infusion. In conclusion, our IHC and gene profiling assays on archived tumor samples have uncovered predictive biomarker signatures identifying patients eligible for TIL therapy and who will most likely benefit from TIL therapy, as well as possible new tumor resistance pathways to immunotherapy for melanoma that can be targets of novel combination therapies to enhance TIL therapy.