Conditionally mutant animal model for investigating the invasive trophoblast cell lineage

Author:

Iqbal Khursheed12ORCID,Dominguez Esteban M.12,Nixon Brandon12,Moreno-Irusta Ayelen12ORCID,Crnkovich Benjamin12,Scott Regan L.12ORCID,Vu Ha T. H.34,Tuteja Geetu34ORCID,Vivian Jay L.125ORCID,Soares Michael J.1267ORCID

Affiliation:

1. Institute for Reproductive and Developmental Sciences, University of Kansas Medical Center 1 , Kansas City, KS 66160 , USA

2. University of Kansas Medical Center 2 Department of Pathology and Laboratory Medicine , , Kansas City, KS 66160 , USA

3. Iowa State University 3 Department of Genetics, Development, and Cell Biology , , Ames, IA 50011 , USA

4. Iowa State University 4 Bioinformatics and Computational Biology Interdepartmental Graduate Program , , Ames, IA 50011 , USA

5. Children's Mercy Research Institute, Children's Mercy Kansas City 5 Division of Clinical Genetics, Department of Pediatrics , , Kansas City, MO 64018 , USA

6. University of Kansas Medical Center 6 Department of Obstetrics and Gynecology , , Kansas City, KS 66160 , USA

7. Center for Perinatal Research, Children's Mercy Research Institute, Children's Mercy Kansas City 7 , Kansas City, MO 64108 , USA

Abstract

ABSTRACT Placental development involves coordinated expansion and differentiation of trophoblast cell lineages possessing specialized functions. Among the differentiated trophoblast cell lineages are invasive trophoblast cells, which exit the placenta and invade the uterus, where they restructure the uterine parenchyma and facilitate remodeling of uterine spiral arteries. The rat exhibits deep intrauterine trophoblast cell invasion, a feature shared with human placentation, and is also amenable to gene manipulation using genome-editing techniques. In this investigation, we generated a conditional rat model targeting the invasive trophoblast cell lineage. Prolactin family 7, subfamily b, member 1 (Prl7b1) is uniquely and abundantly expressed in the rat invasive trophoblast cell lineage. Disruption of Prl7b1 did not adversely affect placental development. We demonstrated that the Prl7b1 locus could be effectively used to drive the expression of Cre recombinase in invasive trophoblast cells. Our rat model represents a new tool for investigating candidate genes contributing to the regulation of invasive trophoblast cells and their roles in trophoblast-guided uterine spiral artery remodeling.

Funder

Kansas IdeA Network of Biomedical Research Excellence

Lalor Foundation

National Institutes of Health

Sosland Foundation

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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