Integrative analysis of hepatic transcriptional profiles reveals genetic regulation of atherosclerosis in hyperlipidemic Diversity Outbred-F1 mice

Myungsuk Kim; M Nazmul Huda; Levi W Evans; Excel Que; Erik R Gertz; Nobuyo Maeda-Smithies; Brian J Bennett

doi:10.1038/s41598-023-35917-8

Integrative analysis of hepatic transcriptional profiles reveals genetic regulation of atherosclerosis in hyperlipidemic Diversity Outbred-F1 mice

Sci Rep. 2023 Jun 10;13(1):9475. doi: 10.1038/s41598-023-35917-8.

Authors

Myungsuk Kim^{1

2

3}, M Nazmul Huda^{1

4}, Levi W Evans⁴, Excel Que⁴, Erik R Gertz⁴, Nobuyo Maeda-Smithies⁵, Brian J Bennett^{6

7}

Affiliations

¹ Department of Nutrition, University of California, Davis, CA, USA.
² Korea Institute of Science and Technology (KIST), Gangneung, Gangwon-Do, Republic of Korea.
³ Division of Bio-Medical Science and Technology, KIST School, University of Science and Technology (UST), Seoul, 02792, Republic of Korea.
⁴ Western Human Nutrition Research Center, Agricultural Research Service, US Department of Agriculture, Davis, CA, USA.
⁵ Department of Pathology and Laboratory Medicine, University of North Carolina at Chapel Hill, Chapel Hill, NC, USA.
⁶ Department of Nutrition, University of California, Davis, CA, USA. brian.bennett@usda.gov.
⁷ Western Human Nutrition Research Center, Agricultural Research Service, US Department of Agriculture, Davis, CA, USA. brian.bennett@usda.gov.

Abstract

Atherogenesis is an insipidus but precipitating process leading to serious consequences of many cardiovascular diseases (CVD). Numerous genetic loci contributing to atherosclerosis have been identified in human genome-wide association studies, but these studies have limitations in the ability to control environmental factors and to decipher cause/effect relationships. To assess the power of hyperlipidemic Diversity Outbred (DO) mice in facilitating quantitative trait loci (QTL) analysis of complex traits, we generated a high-resolution genetic panel of atherosclerosis susceptible (DO-F1) mouse cohort by crossing 200 DO females with C57BL/6J males carrying two human genes: encoding apolipoprotein E3-Leiden and cholesterol ester transfer protein. We examined atherosclerotic traits including plasma lipids and glucose in the 235 female and 226 male progeny before and after 16 weeks of a high-fat/cholesterol diet, and aortic plaque size at 24 weeks. We also assessed the liver transcriptome using RNA-sequencing. Our QTL mapping for atherosclerotic traits identified one previously reported female-specific QTL on Chr10 with a narrower interval of 22.73 to 30.80 Mb, and one novel male-specific QTL at 31.89 to 40.25 Mb on Chr19. Liver transcription levels of several genes within each QTL were highly correlated with the atherogenic traits. A majority of these candidates have already known atherogenic potential in humans and/or mice, but integrative QTL, eQTL, and correlation analyses further pointed Ptprk as a major candidate of the Chr10 QTL, while Pten and Cyp2c67 of the Chr19 QTL in our DO-F1 cohort. Finally, through additional analyses of RNA-seq data we identified genetic regulation of hepatic transcription factors, including Nr1h3, contributes to atherogenesis in this cohort. Thus, an integrative approach using DO-F1 mice effectively validates the influence of genetic factors on atherosclerosis in DO mice and suggests an opportunity to discover therapeutics in the setting of hyperlipidemia.

Publication types

Research Support, N.I.H., Extramural
Research Support, U.S. Gov't, Non-P.H.S.

MeSH terms

Animals
Atherosclerosis* / genetics
Collaborative Cross Mice* / genetics
Female
Genome-Wide Association Study
Humans
Liver
Male
Mice
Mice, Inbred C57BL

Grants and funding

R01 HL049277/HL/NHLBI NIH HHS/United States