4.3 Article

Generation of viable PDX1 gene-edited founder pigs as providers of nonmosaics

Journal

MOLECULAR REPRODUCTION AND DEVELOPMENT
Volume 87, Issue 4, Pages 471-481

Publisher

WILEY
DOI: 10.1002/mrd.23335

Keywords

CRISPR; Cas9; diabetes mellitus; electroporation; IVF; PDX1-mutant pigs

Funding

  1. Research Clusters program of Tokushima University [1701001]
  2. JSPS KAKENHI [JP17H03938, JP19K16014]
  3. Funds for the Development of Human Resources in Science and Technology under MEXT, through the Home for Innovative Researchers and Academic Knowledge Users (HIRAKU)
  4. Program of Open Innovation Platform with Enterprises, Research Institute and Academia (OPERA) [JPMJOP1613]

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Pancreatic duodenal homeobox 1 (PDX1) is a crucial gene for pancreas development during the fetal period. PDX1-modified pigs have the potential to be used as a model of diabetes mellitus. However, the severe health problems caused by the PDX1 mutation limit phenotypic studies of PDX1-modified pigs as diabetes models. In this study, we generated PDX1-modified pigs by the CRISPR/Cas9 system introduced into zygotes via electroporation and investigated the mosaicism, phenotypes, and inheritance of the resulting pigs. After the embryo transfer of PDX1-modified zygotes, nine mutant piglets were delivered. Two piglets were apancreatic biallelic mutants. For the other seven piglets, the ratio of mutant alleles to total alleles was 17.5-79.7%. Two mutant piglets with high mutation rates (67.7% and 79.7%) exhibited hypoplasia of the pancreas, whereas the other five piglets were healthy. One of the male mutant piglets was further analyzed. The ejaculated semen from the pig contained PDX1-mutant spermatozoa and the pig showed normal reproductive ability. In conclusion, the frequency of the PDX1 mutation is presumed to relate to pancreas formation, and PDX1 mutant founder pigs generated from zygotes introduced to the CRISPR/Cas9 system can serve as providers of nonmosaics to contribute to medical research on diabetes mellitus.

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