The Absence of the ACE N-Domain Decreases Renal Inflammation and Facilitates Sodium Excretion during Diabetic Kidney Disease

Author:

Eriguchi Masahiro,Bernstein Ellen A.,Veiras Luciana C.,Khan Zakir,Cao Duo Yao,Fuchs Sebastien,McDonough Alicia A.ORCID,Toblli Jorge E.,Gonzalez-Villalobos Romer A.,Bernstein Kenneth E.,Giani Jorge F.

Abstract

BackgroundRecent evidence emphasizes the critical role of inflammation in the development of diabetic nephropathy. Angiotensin-converting enzyme (ACE) plays an active role in regulating the renal inflammatory response associated with diabetes. Studies have also shown that ACE has roles in inflammation and the immune response that are independent of angiotensin II. ACE’s two catalytically independent domains, the N- and C-domains, can process a variety of substrates other than angiotensin I.MethodsTo examine the relative contributions of each ACE domain to the sodium retentive state, renal inflammation, and renal injury associated with diabetic kidney disease, we used streptozotocin to induce diabetes in wild-type mice and in genetic mouse models lacking either a functional ACE N-domain (NKO mice) or C-domain (CKO mice).ResultsIn response to a saline challenge, diabetic NKO mice excreted 32% more urinary sodium compared with diabetic wild-type or CKO mice. Diabetic NKO mice also exhibited 55% less renal epithelial sodium channel cleavage (a marker of channel activity), 55% less renal IL-1β, 53% less renal TNF-α, and 53% less albuminuria than diabetic wild-type mice. This protective phenotype was not associated with changes in renal angiotensin II levels. Further, we present evidence that the anti-inflammatory tetrapeptide N-acetyl-seryl-asparyl-lysyl-proline (AcSDKP), an ACE N-domain–specific substrate that accumulates in the urine of NKO mice, mediates the beneficial effects observed in the NKO.ConclusionsThese data indicate that increasing AcSDKP by blocking the ACE N-domain facilitates sodium excretion and ameliorates diabetic kidney disease independent of intrarenal angiotensin II regulation.

Publisher

American Society of Nephrology (ASN)

Subject

Nephrology,General Medicine

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