Expression of the Apoptosis Inhibitor Protease Inhibitor 9 Predicts Clinical Outcome in Vaccinated Patients with Stage III and IV Melanoma

Overview

Journal Clin Cancer Res

Specialty Oncology

Date 2005 Sep 8

PMID 16144945

Citations 36

Authors

Inge S van Houdt

Joost J Oudejans

Alfonsus J M van den Eertwegh

Arnold Baars

Wim Vos

Bellinda A Bladergroen

Donata Rimoldi

Jettie J F Muris

Erik Hooijberg

Chad M Gundy

Chris J L M Meijer

Jean A Kummer

Affiliations

Soon will be listed here.

Abstract

Purpose: There have been reports of successful treatment of metastatic melanoma patients with active specific immunotherapy (ASI) using irradiated autologous tumor cell vaccination. It is still unknown why some patients respond and others do not. Tumor cells can evade the immune system, for example through interference with antigen presentation by down-regulation of MHC molecules or expressing proteins interfering with cytotoxic lymphocyte-induced apoptosis like the granzyme B antagonist protease inhibitor 9 (PI-9).

Experimental Design: PI-9 expression was detected in melanoma cell lines. To investigated if PI-9 is important in the response to ASI, paraffin-embedded tissues from stage III or IV melanoma patients were stained.

Results: PI-9 is expressed in melanoma cells and expression in metastasized melanoma cells is, in this group of patients, an adverse prognostic marker with regard to overall and disease-free survival. Moreover, loss of MHC-1 expression frequently occurs during tumor progression but is not associated with poor clinical outcome. Interestingly, melanoma patients with a favorable clinical outcome after ASI therapy usually have high percentages of activated (granzyme B-positive) tumor-infiltrating lymphocytes at time of first diagnosis and low percentages of activated lymphocytes at time of recurrent tumor.

Conclusions: Expression of PI-9 in metastatic melanoma cells is associated with unfavorable clinical outcome whereas MHC-1 down-regulation is not. Although it cannot be proven that PI-9 expression is directly responsible for failure of immunotherapy, these data suggest that expression of PI-9 could be an important immune escape mechanism and that modulation of this inhibitor may enhance the efficacy of immunotherapy.

Citing Articles

Optimizing CAR-T cell therapy for solid tumors: current challenges and potential strategies.

Ai K, Liu B, Chen X, Huang C, Yang L, Zhang W J Hematol Oncol. 2024; 17(1):105.

PMID: 39501358 PMC: 11539560. DOI: 10.1186/s13045-024-01625-7.

Crystallization and crystallographic studies of human serine protease inhibitor (serpin) B9.

Yan T, Zhou A Acta Crystallogr F Struct Biol Commun. 2024; 80(Pt 11):286-293.

PMID: 39382088 PMC: 11533364. DOI: 10.1107/S2053230X24009439.

The biological function of Serpinb9 and Serpinb9-based therapy.

Huang H, Mu Y, Li S Front Immunol. 2024; 15:1422113.

PMID: 38966643 PMC: 11222584. DOI: 10.3389/fimmu.2024.1422113.

Harada M, Kotani H, Iida Y, Tanino R, Minami T, Komohara Y Cancer Sci. 2024; 115(5):1405-1416.

PMID: 38413363 PMC: 11093193. DOI: 10.1111/cas.16133.

Decoding the mechanisms of chimeric antigen receptor (CAR) T cell-mediated killing of tumors: insights from granzyme and Fas inhibition.

Montalvo M, Bandey I, Rezvan A, Wu K, Saeedi A, Kulkarni R Cell Death Dis. 2024; 15(2):109.

PMID: 38307835 PMC: 10837176. DOI: 10.1038/s41419-024-06461-8.