Interacting genetic loci on chromosomes 20 and 10 influence extreme human obesity

Chuanhui Dong¹, Shuang Wang, Wei-Dong Li, Ding Li, Hongyu Zhao, R Arlen Price

Affiliations

PMID: 12478478
PMCID: PMC378615
DOI: 10.1086/345648

Interacting genetic loci on chromosomes 20 and 10 influence extreme human obesity

Chuanhui Dong et al. Am J Hum Genet. 2003 Jan.

. 2003 Jan;72(1):115-24.

doi: 10.1086/345648. Epub 2002 Dec 11.

Authors

Chuanhui Dong¹, Shuang Wang, Wei-Dong Li, Ding Li, Hongyu Zhao, R Arlen Price

Affiliation

¹ Center for Neurobiology and Behavior, University of Pennsylvania, Philadelphia, PA 19104-6140, USA.

PMID: 12478478
PMCID: PMC378615
DOI: 10.1086/345648

Abstract

Obesity is a multigenic trait that has a substantial genetic component. Animal models confirm a role for gene-gene interactions, and human studies suggest that as much as one-third of the heritable variance may be due to nonadditive gene effects. To evaluate potential epistatic interactions among five regions, on chromosomes 7, 10, and 20, that have previously been linked to obesity phenotypes, we conducted pairwise correlation analyses based on alleles shared identical by descent (IBD) for independent obese affected sibling pairs (ASPs), and we determined family-specific nonparametric linkage (NPL) scores in 244 families. The correlation analyses were also conducted separately, by race, through use of race-specific allele frequencies. Conditional analyses for a qualitative trait (body mass index [BMI] >/=27) and hierarchical models for quantitative traits were used to further refine evidence of gene interaction. Both the ASP-specific IBD-sharing probability and the family-specific NPL score revealed that there were strong positive correlations between 10q (88-97 cM) and 20q (65-83 cM), through single-point and multipoint analyses with three obesity thresholds (BMI >/=27, >/=30, and >/=35) across African American and European American samples. Conditional analyses for BMI >/=27 found that the LOD score at 20q rises from 1.53 in the baseline analysis to 2.80 (empirical P=.012) when families were weighted by evidence for linkage at 10q (D10S1646) through use of zero-one weights (weight(0-1)) and to 3.32 (empirical P<.001) when proportional weights (weight(prop)) were used. For percentage fat mass, variance-component analysis based on a two-locus epistatic model yielded significant evidence for interaction between 20q (75 cM) and the chromosome 10 centromere (LOD = 1.74; P=.024), compared with a two-locus additive model (LOD = 0.90). The results from multiple methods and correlated phenotypes are consistent in suggesting that epistatic interactions between loci in these regions play a role in extreme human obesity.

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Figures

**Figure 1**
Multipoint analyses of chromosome 20 for BMI ⩾27 in the combined sample. Conditional allele-sharing multipoint analyses were performed by weighting the families on the basis of the evidence for linkage at D10S1646.

**Figure 2**
Multipoint analyses of chromosome 20 for BMI ⩾27 in the combined sample. Conditional allele-sharing multipoint analyses were performed by weighting the families on the basis of the evidence for linkage at D10S537.

**Figure 3**
Epistatic-interaction analyses for percentage fat mass by variance-component approach in the combined sample. Oligogenic analyses were performed using both additive and epistatic two-locus models to look for evidence of joint effects.

See this image and copyright information in PMC

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References

Electronic-Database Information

1. Genetic Location Database, The, http://cedar.genetics.soton.ac.uk/public_html/ldb.html (for map location)
1. Genome Database, The, http://gdbwww.gdb.org/ (for map location)
1. Online Mendelian Inheritance in Man (OMIM), http://www.ncbi.nlm.nih.gov/Omim/ (for obesity [MIM 601665])
1. Whitehead Institute/MIT Center for Genome Research, http://www-genome.wi.mit.edu/ (for map location)

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