The functional interaction on in vitro gene expression of APOA5 SNPs, defining haplotype APOA52, and their paradoxical association with plasma triglyceride but not plasma apoAV levels
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- 作者:Jutta Palmen ; Andrew J.P. Smith ; Birgit Dorfmeister ; Wendy Putt ; Steve E. Humphries ; Philippa J. Talmud
- 关键词:APOA5
; //www.sciencedirect.com/scidirimg/entities/204e.gif"" alt=""low asterisk"" title=""low asterisk"" border=""0"">2 ; Plasma apoAV ; − ; 1131T> ; C ; − ; 3A> ; G ; + 1891T> ; C ; Kozak sequence ; Plasma TG
- 刊名:Biochimica et Biophysica Acta (BBA)/Molecular Basis of Disease
- 出版年:2008
- 出版时间:July-August 2008
- 年:2008
- 卷:1782
- 期:7-8
- 页码:447-452
- 全文大小:340 K
文摘
Plasma triglyceride (TG) and apoAV levels are reported to be positively correlated, yet SNPs defining haplotype APOA5![]()
2 have consistently shown association with elevated plasma triglyceride (TG) but not plasma apoAV levels. We previously reported that individually − 1131T>C, − 3A>G and + 1891T>C did not influence luciferase activity or in vitro translation efficiency. To investigate the combined effect of these SNPs additional constructs were examined. Compared to the wildtype − 1131T/− 3A/+ 1891T (TAT), the triple rare allele construct − 1131C/− 3G/+ 1891C (CGC) conferred 46 % lower luciferase activity (p < 0.0001), showing these SNPs are acting co-operatively. Although only these two combinations occur in vivo, we experimentally altered the TAT construct one site at a time; − 3G (TGT) had the largest effect (94 % lower luciferase), with lesser effects from CAT (− 77 % ) and TAC (− 70.3 % ) (all p < 0.0001). Deletion constructs excluding one site at a time showed that − 3G/1891C ( –GC) in combination, compared to − AT, was having the largest effect on luciferase activity (− 59 % , p = 0.055). Using sequence homology and EMSA analysis no transcription factor binding at − 1131 or + 1891 was identified, though + 1891 lies within a putative mRNA stability motif. Taken together, these data identify − 3A>G in the Kozak sequence as functional, affecting translation initiation and driving the haplotype effects, while showing interaction with + 1891T>C and to a lesser extent − 1131T>C. A paradox arises since these results predict that APOA5![]()
2 will lead to reduced apoAV with concomitant reduced LPL activation or lipoprotein-receptor interaction, resulting in higher plasma TG levels. We conclude that APOA5 expression, and not circulating plasma apoAV levels, is causatively associated with plasma TG levels.