We use cookies to understand how you use our site and to improve your experience. This includes personalizing content and advertising. To learn more, click here. By continuing to use our site, you accept our use of cookies. Cookie Policy.

LabMedica

Download Mobile App
Recent News Expo Medica 2024 Clinical Chem. Molecular Diagnostics Hematology Immunology Microbiology Pathology Technology Industry Focus

Biomarker Identifies Uveal Melanoma Patients at Risk for Metastasis

By LabMedica International staff writers
Posted on 15 Mar 2016
Uveal melanoma is a cancer (melanoma) of the eye involving the iris, ciliary body, or choroid, collectively referred to as the uvea. Tumors arise from the pigment cells (melanocytes) that reside within the uvea giving color to the eye.

Uveal melanoma (UM) can be classified by gene expression profiling (GEP) into Class 1 (low metastatic risk) and Class 2 (high metastatic risk), the latter being strongly associated with mutational inactivation of the tumor suppressor gene BRCA1 Associated Protein-1 (Ubiquitin Carboxy-Terminal Hydrolase (BAP1).

Image: A cancer of the iris known as uveal melanoma (Photo courtesy of Dr. Jonathan Trobe, MD).
Image: A cancer of the iris known as uveal melanoma (Photo courtesy of Dr. Jonathan Trobe, MD).

Scientists at the University of Miami Miller School of Medicine (Miami, FL, USA) performed genome-wide analysis of messenger ribonucleic acid (mRNA) isolated from five class 1 uveal melanomas that metastasized and eight class 1 tumors that did not metastasize. A total of 389 consecutive patients with UM were assigned to Class 1 or Class 2 using a prospectively validated 12-gene prognostic classifier. Selected tumors were further analyzed using global GEP and single nucleotide polymorphism microarrays. PRAME (preferentially expressed antigen in melanoma) mRNA expression was analyzed in 64 Class 1 tumors by quantitative polymerase chain reaction (PCR).

Among 64 class 1 uveal melanoma samples analyzed by quantitative PCR, 39 (61%) had low levels of PRAME mRNA (PRAME negative) and 25 (39%) had high levels of PRAME mRNA (PRAME positive). None of the patients with PRAME-negative tumors developed metastasis while seven of the patients with PRAME-positive tumors did. The 5-year actuarial rate of metastasis was 0% for Class1PRAME−, 38% for Class1PRAME+, and 71% for Class 2 tumors. Median metastasis-free survival for Class1PRAME+ patients was 88 months, compared to 32 months for Class 2 patients.

J. William Harbour, MD, the senior author of the study said, “We were surprised to find that one biomarker alone PRAME was sufficient to identify the subgroup of class 1 tumors with increased metastatic risk. These findings could have immediate clinical impact. The data imply that patients with class 1 uveal melanomas with increased PRAME expression should be managed differently than patients with class 1 uveal melanomas without PRAME expression. They should be monitored more closely for metastatic disease and they should be considered for clinical trials of adjuvant therapy.” The study was published on March 1, 2016 in the journal Clinical Cancer Research.

Related Links:

University of Miami Miller School of Medicine



New
Gold Member
Pneumocystis Jirovecii Detection Kit
Pneumocystis Jirovecii Real Time RT-PCR Kit
Antipsychotic TDM AssaysSaladax Antipsychotic Assays
New
Chemistry Analyzer
MS100
New
Urine Strips
11 Parameter Urine Strips

Latest Pathology News

New Microscopy Method Enables Detailed Whole Brain 3D RNA Analysis

AI Model Identifies Signs of Disease Faster and More Accurately Than Humans

New Barcode Technology to Help Diagnose Cancer More Precisely