AI Article Synopsis
- Research shows that SGLT1 contributes to cognitive impairment associated with small vessel disease, and the study aims to investigate if SGLT1 inhibitors can improve this impairment.
- The study used two SGLT1 inhibitors, mizagliflozin and phlorizin, on mice with induced small vessel disease, revealing that phlorizin improved cerebral blood flow while both inhibitors enhanced cognitive function in tests.
- Findings indicate that both inhibitors can reduce negative effects of small vessel disease on cognition, with phlorizin also normalizing certain gene expressions related to inflammation and cell death.
Article Abstract
Previously, we showed that sodium/glucose cotransporter 1 (SGLT1) participates in vascular cognitive impairment in small vessel disease. We hypothesized that SGLT1 inhibitors can improve the small vessel disease induced-vascular cognitive impairment. We examined the effects of mizagliflozin, a selective SGLT1 inhibitor, and phlorizin, a non-selective SGLT inhibitor, on vascular cognitive impairment in a mouse model of small vessel disease. Small vessel disease was created using a mouse model of asymmetric common carotid artery surgery (ACAS). Two and/or 4 weeks after ACAS, all experiments were performed. Cerebral blood flow (CBF) was decreased in ACAS compared with sham-operated mice. Phlorizin but not mizagliflozin reversed the decreased CBF of ACAS mice. Both mizagliflozin and phlorizin reversed the ACAS-induced decrease in the latency to fall in a wire hang test of ACAS mice. Moreover, they reversed the ACAS-induced longer escape latencies in the Morris water maze test of ACAS mice. ACAS increased SGLT1 and proinflammatory cytokine gene expressions in mouse brains and phlorizin but not mizagliflozin normalized all gene expressions in ACAS mice. Hematoxylin/eosin staining demonstrated that they inhibited pyknotic cell death in the ACAS mouse hippocampus. In PC12HS cells, IL-1β increased SGLT1 expression and decreased survival rates of cells. Both mizagliflozin and phlorizin increased the survival rates of IL-1β-treated PC12HS cells. These results suggest that mizagliflozin and phlorizin can improve vascular cognitive impairment through the inhibition of neural SGLT1 and phlorizin also does so through the improvement of CBF in a mouse model of small vessel disease.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8480397 | PMC |
| http://dx.doi.org/10.1002/prp2.869 | DOI Listing |
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