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Knockout rat models mimicking human atherosclerosis created by Cpf1-mediated gene targeting

  • Jong Geol Lee
  • , Chang Hoon Ha
  • , Bohyun Yoon
  • , Seung A. Cheong
  • , Globinna Kim
  • , Doo Jae Lee
  • , Dong Cheol Woo
  • , Young Hak Kim
  • , Sang Yoon Nam
  • , Sang wook Lee
  • , Young Hoon Sung
  • , In Jeoung Baek
  • University of Ulsan
  • Chungbuk National University

Research output: Contribution to journalArticlepeer-review

39 Scopus citations

Abstract

The rat is a time-honored traditional experimental model animal, but its use is limited due to the difficulty of genetic modification. Although engineered endonucleases enable us to manipulate the rat genome, it is not known whether the newly identified endonuclease Cpf1 system is applicable to rats. Here we report the first application of CRISPR-Cpf1 in rats and investigate whether Apoe knockout rat can be used as an atherosclerosis model. We generated Apoe- and/or Ldlr-deficient rats via CRISPR-Cpf1 system, characterized by high efficiency, successful germline transmission, multiple gene targeting capacity, and minimal off-target effect. The resulting Apoe knockout rats displayed hyperlipidemia and aortic lesions. In partially ligated carotid arteries of rats and mice fed with high-fat diet, in contrast to Apoe knockout mice showing atherosclerotic lesions, Apoe knockout rats showed only adventitial immune infiltrates comprising T lymphocytes and mainly macrophages with no plaque. In addition, adventitial macrophage progenitor cells (AMPCs) were more abundant in Apoe knockout rats than in mice. Our data suggest that the Cpf1 system can target single or multiple genes efficiently and specifically in rats with genetic heritability and that Apoe knockout rats may help understand initial-stage atherosclerosis.

Original languageEnglish
Article number2628
JournalScientific Reports
Volume9
Issue number1
DOIs
StatePublished - 1 Dec 2019

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