Angiotensin-converting Enzyme Overexpression in Myelomonocytes Prevents Alzheimer's-like Cognitive Decline

Overview

Journal J Clin Invest

Specialty General Medicine

Date 2014 Feb 4

PMID 24487585

Citations 58

Authors

Kenneth E Bernstein

Yosef Koronyo

Brenda C Salumbides

Julia Sheyn

Lindsey Pelissier

Dahabada H J Lopes

Kandarp H Shah

Ellen A Bernstein

Dieu-Trang Fuchs

Jeff J-Y Yu

Michael Pham

Keith L Black

Xiao Z Shen

Sebastien Fuchs

Maya Koronyo-Hamaoui

Affiliations

Soon will be listed here.

Abstract

Cognitive decline in patients with Alzheimer's disease (AD) is associated with elevated brain levels of amyloid β protein (Aβ), particularly neurotoxic Aβ(1-42). Angiotensin-converting enzyme (ACE) can degrade Aβ(1-42), and ACE overexpression in myelomonocytic cells enhances their immune function. To examine the effect of targeted ACE overexpression on AD, we crossed ACE(10/10) mice, which overexpress ACE in myelomonocytes using the c-fms promoter, with the transgenic APP(SWE)/PS1(ΔE9) mouse model of AD (AD⁺). Evaluation of brain tissue from these AD⁺ACE(10/10) mice at 7 and 13 months revealed that levels of both soluble and insoluble brain Aβ(1-42) were reduced compared with those in AD⁺ mice. Furthermore, both plaque burden and astrogliosis were drastically reduced. Administration of the ACE inhibitor ramipril increased Aβ levels in AD⁺ACE(10/10) mice compared with the levels induced by the ACE-independent vasodilator hydralazine. Overall, AD⁺ACE(10/10) mice had less brain-infiltrating cells, consistent with reduced AD-associated pathology, though ACE-overexpressing macrophages were abundant around and engulfing Aβ plaques. At 11 and 12 months of age, the AD⁺ACE(10/WT) and AD⁺ACE(10/10) mice were virtually equivalent to non-AD mice in cognitive ability, as assessed by maze-based behavioral tests. Our data demonstrate that an enhanced immune response, coupled with increased myelomonocytic expression of catalytically active ACE, prevents cognitive decline in a murine model of AD.

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