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Data from Genetic Variation and Recurrent Haplotypes on Chromosome 6q23-25 Risk Locus in Familial Lung Cancer

Posted on 2023-03-31 - 04:28
Abstract

Although lung cancer is known to be caused by environmental factors, it has also been shown to have genetic components, and the genetic etiology of lung cancer remains understudied. We previously identified a lung cancer risk locus on 6q23-25 using microsatellite data in families with a history of lung cancer. To further elucidate that signal, we performed targeted sequencing on nine of our most strongly linked families. Two-point linkage analysis of the sequencing data revealed that the signal was heterogeneous and that different families likely had different risk variants. Three specific haplotypes were shared by some of the families: 6q25.3-26 in families 42 and 44, 6q25.2-25.3 in families 47 and 59, and 6q24.2-25.1 in families 30, 33, and 35. Region-based logarithm of the odds scores and expression data identified the likely candidate genes for each haplotype overlap: ARID1B at 6q25.3, MAP3K4 at 6q26, and UTRN (6q24.1) and PHACTR2 (6q24.2). Further annotation was used to zero in on potential risk variants in those genes. All four genes are good candidate genes for lung cancer risk, having been linked to either lung cancer specifically or other cancers. However, this is the first time any of these genes has been implicated in germline risk. Functional analysis of these four genes is planned for future work.

Significance:

This study identifies four genes associated with lung cancer risk, which could help guide future lung cancer prevention and treatment approaches.

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NIH

NCI

National Institutes of Health

National Institute of Environmental Health Sciences

Department of Health and Human Services

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Cancer Research

AUTHORS (18)

  • Anthony M. Musolf
    Claire L. Simpson
    Bilal A. Moiz
    Claudio W. Pikielny
    Candace D. Middlebrooks
    Diptasri Mandal
    Mariza de Andrade
    Michael D. Cole
    Colette Gaba
    Ping Yang
    Ming You
    Yafang Li
    Elena Y. Kupert
    Marshall W. Anderson
    Ann G. Schwartz
    Susan M. Pinney
    Christopher I. Amos
    Joan E. Bailey-Wilson
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