CXCR4 Pathway Associated with Family History of Melanoma

Overview

Journal Cancer Causes Control

Specialties Oncology
Public Health

Date 2013 Oct 26

PMID 24158781

Citations 3

Authors

Wen-Qing Li

Jiali Han

Hans R Widlund

Mick Correll

Yaoyu E Wang

John Quackenbush

Martin C Mihm

Alvaro Laga Canales

Shaowei Wu

Todd Golub

Yujin Hoshida

David J Hunter

George Murphy

Thomas S Kupper

Abrar A Qureshi

Affiliations

Soon will be listed here.

Abstract

Purpose: Genetic predisposition plays a major role in the etiology of melanoma, but known genetic markers only account for a limited fraction of family-history-associated melanoma cases. Expression microarrays have offered the opportunity to identify further genomic profiles correlated with family history of melanoma. We aimed to distinguish mRNA expression signatures between melanoma cases with and without a family history of melanoma.

Methods: Based on the Nurses' Health Study, family history was defined as having one or more first-degree family members diagnosed with melanoma. Melanoma diagnosis was confirmed by reviewing pathology reports, and tumor blocks were collected by mail from across the USA. Genomic interrogation was accomplished through evaluating expression profiling of formalin-fixed paraffin-embedded tissues from 78 primary cutaneous invasive melanoma cases, on either a 6K or whole-genome (24K) Illumina gene chip. Gene set enrichment analysis was performed for each batch to determine the differentially enriched pathways and key contributing genes.

Results: The CXC chemokine receptor 4 (CXCR4) pathway was consistently up-regulated within cases of familial melanoma in both platforms. Leading edge analysis showed four genes from the CXCR4 pathway, including MAPK1, PLCG1, CRK, and PTK2, were among the core members that contributed to the enrichment of this pathway. There was no association between the enrichment of CXCR4 pathway and NRAS, BRAF mutation, or Breslow thickness of the primary melanoma cases.

Conclusions: We found that the CXCR4 pathway might constitute a novel susceptibility pathway associated with family history of melanoma in first-degree relatives.

Citing Articles

Silencing of the chemokine CXC receptor 4 (CXCR4) hampers cancer progression and increases cisplatin (DDP)-sensitivity in clear cell renal cell carcinoma (ccRCC).

Wang W, Gan Z, Liu Q, Yan S, Mulati R, Wang Y Bioengineered. 2021; 12(1):2957-2969.

PMID: 34180759 PMC: 8806489. DOI: 10.1080/21655979.2021.1943112.

Host Characteristics and Risk of Incident Melanoma by Breslow Thickness.

Li W, Cho E, Wu S, Li S, Matthews N, Qureshi A Cancer Epidemiol Biomarkers Prev. 2018; 28(1):217-224.

PMID: 30341099 PMC: 6324995. DOI: 10.1158/1055-9965.EPI-18-0607.

Epidemiological Assessments of Skin Outcomes in the Nurses' Health Studies.

Li W, Cho E, Weinstock M, Mashfiq H, Qureshi A Am J Public Health. 2016; 106(9):1677-83.

PMID: 27459457 PMC: 4981523. DOI: 10.2105/AJPH.2016.303315.

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