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Publication : Cardiometabolic Consequences of Deleting the Regulator of G protein Signaling-2 (Rgs2) From Cells Expressing Agouti-Related Peptide or the ANG (Angiotensin) II Type 1A Receptor in Mice.

First Author  Ritter ML Year  2022
Journal  Hypertension Volume  79
Issue  12 Pages  2843-2853
PubMed ID  36259376 Mgi Jnum  J:352970
Mgi Id  MGI:7707536 Doi  10.1161/HYPERTENSIONAHA.122.20169
Citation  Ritter ML, et al. (2022) Cardiometabolic Consequences of Deleting the Regulator of G protein Signaling-2 (Rgs2) From Cells Expressing Agouti-Related Peptide or the ANG (Angiotensin) II Type 1A Receptor in Mice. Hypertension 79(12):2843-2853
abstractText  BACKGROUND: RGS (regulator of G protein signaling) family members catalyze the termination of G protein signaling cascades. Single nucleotide polymorphisms in the RGS2 gene in humans have been linked to hypertension, preeclampsia, and anxiety disorders. Mice deficient for Rgs2 (Rgs2(Null)) exhibit hypertension, anxiety, and altered adipose development and function. METHODS: To study cell-specific functions of RGS2, a novel gene-targeted mouse harboring a conditional allele for the Rgs2 gene (Rgs2(Flox)) was developed. These mice were bred with mice expressing Cre-recombinase via the Agouti-related peptide locus (Agrp-Cre) to cause deletion of Rgs2 from all cells expressing Agrp (Rgs2(Agrp-KO)), or a novel transgenic mouse expressing Cre-recombinase via the ANG (angiotensin) type 1A receptor (Agtr1a/ AT(1A)) promoter encoded in a bacterial artificial chromosome (BAC-AT(1A)-Cre) to delete Rgs2 in all Agtr1a-expressing cells (Rgs2(AT1A-KO)). RESULTS: Whereas Rgs2(Flox), Rgs2(Agrp-KO), and BAC-AT(1A)-Cre mice exhibited normal growth and survival, Rgs2(AT1A-KO) exhibited pre-weaning lethality. Relative to littermates, Rgs2(Agrp-KO) exhibited reduced fat gains when maintained on a high fat diet, associated with increased energy expenditure. Similarly, surviving adult Rgs2(AT1A-KO) mice also exhibited increased energy expenditure. Surprisingly, given the hypertensive phenotype previously reported for Rgs2(Null) mice and evidence supporting a role for RGS2 in terminating AT(1A) signaling in various cell types, Rgs2(AT1A-KO) mice exhibited normal blood pressure, ingestive behaviors, and renal functions, both before and after chronic infusion of ANG (490 ng/kg/min, sc). CONCLUSIONS: These results demonstrate the development of a novel mouse with conditional expression of Rgs2 and illustrate the role of Rgs2 within selected cell types for cardiometabolic control.
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