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Dietary Phosphate Reduces Hypertension, Inflammation and End Organ Damage

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dc.contributor.advisor Itani, Hana
dc.contributor.advisor Obeid, Omar
dc.contributor.author El Atie, Yara
dc.date.accessioned 2021-09-08T09:53:56Z
dc.date.available 2021-09-08T09:53:56Z
dc.date.issued 9/8/2021
dc.date.submitted 9/8/2021
dc.identifier.uri http://hdl.handle.net/10938/22994
dc.description.abstract Hypertension remains an increasing global health burden. Previous research has shown that dietary phosphate can modulate cardiovascular disease (CVD), yet the precise mechanism of how dietary phosphate contributes to blood pressure (BP), renal injury, and CVD remains unclear. Thus, we hypothesized that phosphate (P) reduces BP, inflammation, and end-organ damage. To this end, male C57bL/6 mice were either infused with four weeks of saline or Angiotensin II (490ng/kg/min) using a subcutaneous mini-osmotic pump. Over these 4 weeks, mice were fed a control diet for 2 weeks, followed by 2 weeks of phosphate-rich diet (0.15%, control (0.3%), and 1.5%P). Tail-cuff BP recordings were measured throughout the study protocol. To assess kidney damage, albumin in 24-hour urine samples, Masson’s trichrome staining, and DHE staining were performed. Flow cytometry was performed to examine immune cells infiltration in the kidney. Strikingly, our results show that control (0.3%P) and 1.5%P significantly reduced the SBP by 6.1 and 24.8 mmHg, respectively. In addition, CD4+T and CD8+T cell infiltration was dramatically reduced in the kidneys of the Angiotensin II-infused mice fed a 0.15%, control (0.3%P), 1.5%P diet compared to sham mice. Finally, Angiotensin II-infused mice fed a 0.15%, control (0.3%P), 1.5%P diet were protected from kidney glomerular damage, fibrosis, and ROS formation. We conclude that containing dietary phosphate mitigates hypertension and its end-organ damage.
dc.language.iso en_US
dc.subject Phosphate, Inflammation, Hypertension, Kidney
dc.title Dietary Phosphate Reduces Hypertension, Inflammation and End Organ Damage
dc.type Thesis
dc.contributor.department Department of Pharmacology and Toxicology
dc.contributor.faculty Faculty of Medicine
dc.contributor.institution American University of Beirut
dc.contributor.commembers Sabra, Ramzi
dc.contributor.commembers El Sabban, Marwan
dc.contributor.commembers Abou Kheir, Wassim
dc.contributor.degree MS
dc.contributor.AUBidnumber 202022445


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