Litcius/Paper detail

Angiotensin-[1–7] attenuates kidney injury in experimental Alport syndrome

Hong Sang Choi, In Jin Kim, Chang Seong Kim, Seong Kwon, James W. Scholey, Soo Wan Kim, Eun Hui Bae

2020Scientific Reports38 citationsDOIOpen Access PDF

Abstract

Abstract Angiotensin-[1–7] (Ang-[1–7]) antagonize the actions of the renin-angiotensin-system via the Mas receptor and thereby exert renoprotective effects. Murine recombinant angiotensin-converting enzyme (ACE)2 was reported to show renoprotective effects in an experimental Alport syndrome model; however, the protective effect of direct administration of Ang-[1–7] is unknown. Here, we used Col4a3 −/− mice as a model of Alport syndrome, which were treated with saline or Ang- [1–7]; saline-treated wild-type mice were used as a control group. The mice were continuously infused with saline or Ang-[1–7] (25 μg/kg/h) using osmotic mini-pumps. Col4a3 −/− mice showed increased α-smooth muscle actin (SMA), collagen, and fibronectin expression levels, which were attenuated by Ang-[1–7] treatment. Moreover, Ang-[1–7] alleviated activation of transforming growth factor-β/Smad signaling, and attenuated the protein expression of ED-1 and heme oxygenase-1, indicating reduction of renal inflammation. Ang-[1–7] treatment further reduced the expression levels of inflammatory cytokines and adhesion molecules and attenuated apoptosis in human kidney cells. Finally, Ang-[1–7] downregulated TNF-α converting enzyme and upregulated ACE2 expression. Thus, treatment with Ang-[1–7] altered the ACE2-Ang-[1–7]-Mas receptor axis in the kidneys of Col4a3 −/− mice to attenuate the nephropathy progression of Alport syndrome.

Topics & Concepts

Alport syndromeMedicineKidneyRenin–angiotensin systemAngiotensin IIAcute kidney injuryInternal medicineGlomerulonephritisBlood pressureRenin-Angiotensin System StudiesBlood Coagulation and Thrombosis MechanismsPulmonary Hypertension Research and Treatments