Genetic evolution of uveal melanoma guides the development of an inflammatory microenvironment

被引:0
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作者
Gülçin Gezgin
Mehmet Dogrusöz
T. Huibertus van Essen
Wilhelmina G. M. Kroes
Gregorius P. M. Luyten
Pieter A. van der Velden
Vonn Walter
Robert M. Verdijk
Thorbald van Hall
Sjoerd H. van der Burg
Martine J. Jager
机构
[1] Leiden University Medical Center,Department of Ophthalmology
[2] Leiden University Medical Center,Department of Clinical Genetics
[3] Penn State Milton S. Hershey Medical Center,Department of Biochemistry
[4] Erasmus MC University Medical Center,Department of Pathology, Section Ophthalmic Pathology
[5] Leiden University Medical Center,Department of Clinical Oncology
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关键词
BAP1; Infiltration; Macrophages; T cells; Lymphocytes; Chromosome;
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摘要
Uveal melanoma (UM) is characterized by a number of genetic aberrations that follow a certain chronology and are tightly linked to tumor recurrence and survival. Loss of chromosome 3, bi-allelic loss of BAP1 expression, and gain in chromosome 8q have been associated with metastasis formation and death, while loss of chromosome 3 has been associated with the influx of macrophages and T cells. We used a set of genetically-classified UM to study immune infiltration in the context of their genetic evolution. We show in two independent cohorts that lack of BAP1 expression is associated with an increased density of CD3+ T cells and CD8+ T cells. The presence of extra copies of chromosome 8q in disomy 3 tumors with a normal BAP1 expression is associated with an increased influx of macrophages (but not T cells). Therefore, we propose that the genetic evolution of UM is associated with changes in the inflammatory phenotype. Early changes resulting in gain of chromosome 8q may activate macrophage infiltration, while sequential loss of BAP1 expression seems to drive T cell infiltration in UM.
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页码:903 / 912
页数:9
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