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Publication : In Vivo Renin Activity Imaging in the Kidney of Progeroid Ercc1 Mutant Mice.

First Author  van Thiel BS Year  2021
Journal  Int J Mol Sci Volume  22
Issue  22 PubMed ID  34830315
Mgi Jnum  J:333269 Mgi Id  MGI:6828169
Doi  10.3390/ijms222212433 Citation  van Thiel BS, et al. (2021) In Vivo Renin Activity Imaging in the Kidney of Progeroid Ercc1 Mutant Mice. Int J Mol Sci 22(22)
abstractText  Changes in the renin-angiotensin system, known for its critical role in the regulation of blood pressure and sodium homeostasis, may contribute to aging and age-related diseases. While the renin-angiotensin system is suppressed during aging, little is known about its regulation and activity within tissues. However, this knowledge is required to successively treat or prevent renal disease in the elderly. Ercc1 is involved in important DNA repair pathways, and when mutated causes accelerated aging phenotypes in humans and mice. In this study, we hypothesized that unrepaired DNA damage contributes to accelerated kidney failure. We tested the use of the renin-activatable near-infrared fluorescent probe ReninSense680 in progeroid Ercc1(d/-) mice and compared renin activity levels in vivo to wild-type mice. First, we validated the specificity of the probe by detecting increased intrarenal activity after losartan treatment and the virtual absence of fluorescence in renin knock-out mice. Second, age-related kidney pathology, tubular anisokaryosis, glomerulosclerosis and increased apoptosis were confirmed in the kidneys of 24-week-old Ercc1(d/-) mice, while initial renal development was normal. Next, we examined the in vivo renin activity in these Ercc1(d/-) mice. Interestingly, increased intrarenal renin activity was detected by ReninSense in Ercc1(d/-) compared to WT mice, while their plasma renin concentrations were lower. Hence, this study demonstrates that intrarenal RAS activity does not necessarily run in parallel with circulating renin in the aging mouse. In addition, our study supports the use of this probe for longitudinal imaging of altered RAS signaling in aging.
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