A major lung cancer susceptibility locus maps to chromosome 6q23-25.

Abstract

Lung cancer is a major cause of death in the United States and other countries. The risk of lung cancer is greatly increased by cigarette smoking and by certain occupational exposures, but familial factors also clearly play a major role. To identify susceptibility genes for familial lung cancer, we conducted a genomewide linkage analysis of 52 extended pedigrees ascertained through probands with lung cancer who had several first-degree relatives with the same disease. Multipoint linkage analysis, under a simple autosomal dominant model, of all 52 families with three or more individuals affected by lung, throat, or laryngeal cancer, yielded a maximum heterogeneity LOD score (HLOD) of 2.79 at 155 cM on chromosome 6q (marker D6S2436). A subset of 38 pedigrees with four or more affected individuals yielded a multipoint HLOD of 3.47 at 155 cM. Analysis of a further subset of 23 multigenerational pedigrees with five or more affected individuals yielded a multipoint HLOD score of 4.26 at the same position. The 14 families with only three affected relatives yielded negative LOD scores in this region. A predivided samples test for heterogeneity comparing the LOD scores from the 23 multigenerational families with those from the remaining families was significant (P=.007). The 1-HLOD multipoint support interval from the multigenerational families extends from C6S1848 at 146 cM to 164 cM near D6S1035, overlapping a genomic region that is deleted in sporadic lung cancers as well as numerous other cancer types. Parametric linkage and variance-components analysis that incorporated effects of age and personal smoking also supported linkage in this region, but with somewhat diminished support. These results localize a major susceptibility locus influencing lung cancer risk to 6q23-25.

EDRN PI Authors
Medline Author List
  • Amos CI
  • Anderson MW
  • Bailey-Wilson JE
  • Coons T
  • Fain P
  • Franklin W
  • Gaba C
  • Gazdar A
  • Klein C
  • Kupert E
  • Lee J
  • Liu Q
  • Mandal D
  • Minna J
  • Perez A
  • Petersen GM
  • Pinney SM
  • Rothschild H
  • Schwartz AG
  • Seminara D
  • Slusser J
  • Wiest JS
  • You M
  • Zeng D
  • Zhang Q
  • Zhou X
  • de Andrade M
PubMed ID
Appears In
Am J Hum Genet, 2004 Sep, volume 75 (issue 3)