| Literature DB >> 21311593 |
Kyung-Tai Lee1, Mi-Jeong Byun, Kyung-Soo Kang, Eung-Woo Park, Seung-Hwan Lee, Seoae Cho, Hyoyoung Kim, Kyu-Won Kim, Taeheon Lee, Jong-Eun Park, Woncheoul Park, Donghyun Shin, Hong-Seog Park, Jin-Tae Jeon, Bong-Hwan Choi, Gul-Won Jang, Sang-Haeng Choi, Dae-Won Kim, Dajeong Lim, Hae-Suk Park, Mi-Rim Park, Jurg Ott, Lawrence B Schook, Tae-Hun Kim, Heebal Kim.
Abstract
Obesity represents a major global public health problem that increases the risk for cardiovascular or metabolic disease. The pigs represent an exceptional biomedical model related to energy metabolism and obesity in humans. To pinpoint causal genetic factors for a common form of obesity, we conducted local genomic de novo sequencing, 18.2 Mb, of a porcine QTL region affecting fatness traits, and carried out SNP association studies for backfat thickness and intramuscular fat content in pigs. In order to relate the association studies in pigs to human obesity, we performed a targeted genome wide association study for subcutaneous fat thickness in a cohort population of 8,842 Korean individuals. These combined association studies in human and pig revealed a significant SNP located in a gene family with sequence similarity 73, member A (FAM73A) associated with subscapular skin-fold thickness in humans (rs4121165, GC-corrected p-value = 0.0000175) and with backfat thickness in pigs (ASGA0029495, p-value = 0.000031). Our combined association studies also suggest that eight neuronal genes are responsible for subcutaneous fat thickness: NEGR1, SLC44A5, PDE4B, LPHN2, ELTD1, ST6GALNAC3, ST6GALNAC5, and TTLL7. These results provide strong support for a major involvement of the CNS in the genetic predisposition to a common form of obesity.Entities:
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Year: 2011 PMID: 21311593 PMCID: PMC3032728 DOI: 10.1371/journal.pone.0016356
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Figure 1A Pig QTL 18 Mb region affecting fatness and meat quality on SSC6.
The information was compiled from PigQTLdb (http://www.genome.iastate.edu/cgi-bin/QTLdb/SS/index). The QTL region and confidence interval of the 18 Mb region is displayed. Reference(s) of each QTL indexed by number in parenthesis are in .
Figure 2Comparative genomic analysis of pig QTL region affecting fatness and meat quality on SSC6.
Similar genomic structure and contents was revealed by comparative analysis between the human syntenic region and the pig QTL region (A) and visualization of syntenic blocks along the region between pig (Ss) and the four other species: human(Hs), mouse(Mm), dog(Cf) and cow(Bt) (B). In the dot-plot analysis (A), protein coding genes are shown as forward (upper) and reverse (lower) in brown color according to x- and y-axis for pigs and human, respectively. The conserved segments from 70-100% are plotted. The genomic feature of pig appear in order from top to bottom under dot-plot: CpG islands, Tandem repeats, G+C content, SINE (blue) and LINE (red) repeat densities using a sliding window of 100 kbp, Interspersed repeat elements (SINEs, LINEs, LTR elements, Simple repeats and Low complextiy). In the synteny maps (B), the rings depict from outside to inside: synteny regions of each chromosome, SINE (blue) and LINE (red) repeat density using a sliding window of 100 kb and protein-coding genes (purple). Genomic coordinates are shown in 100 kb intervals. Synteny blocks larger than 5 kb are displayed by connecting lines.
Figure 3–log10(p-value) of SNPs in the 18.2 Mb pig genomic region.
52 SNPs were identified to be associated with backfat thickness trait (A), and none of the SNPs were found to be significantly associated with intramuscular fat content (B). Gene locations are shown by bars and gene symbols beneath the figure. Genes on the same side indicate same transcriptional direction of the genes.
Figure 4–log10(Genomic control-corrected p-value) of 2,143 SNPs associated with SUB (A) and SUP (B) in the human syntenic region.
Using a false discovery rate (FDR) q value <0.05 [41], a SNP located in FAM73A gene is significantly associated with SUB indicated in red. The genomic control parameter λ value in SUB-SNP association study was 1.037 and the λ value in SUP-SNP association study was 1.187 indicated by the QQ-plots. Genomic control-corrected p-value threshold of 0.01 is indicated by the dotted line.
Figure 5Summary of genes identified in our combined association studies in humans and pigs in the predefined fatness related pig QTL region.
Intersection of the three association studies show three most likely genes, FAM73A, NEGR1 and TTLL7, as being responsible for genetic predisposition to common forms of obesity, especially subcutaneous fat thickness. Eight neuronal genes identified in the pig SNP-BFT association study are indicated in pink.