Natriuretic peptides system in the pulmonary tissue of rats with heart failure: potential involvement in lung edema and inflammation.

Emad E Khoury,Natalia Volinsky,Doron Aronson,Safa Kinaneh,Zaid Abassi,Zaher Azzam,Diab Ghanim,Offer Amir

doi:10.18632/oncotarget.24922

Abstract

Congestive heart failure (CHF) often leads to progressive cardiac hypertrophy and salt/water retention as evident by peripheral and lung edema. Although the pathogenesis of CHF remains largely unclarified, it is widely accepted that neurohormonal changes and inflammatory processes are profoundly involved in structural and functional deterioration of vital organs including, heart, kidney and lungs. Corin, a cardiac serine protease, is responsible for converting pro-ANP and pro-BNP to biologically active natriuretic peptides (NPs). Although the involvement of corin in cardiac hypertrophy and heart failure was extensively studied, the alterations in corin and PCSK6, a key enzyme in the conversion of procorin to corin, have not been studied in the pulmonary tissue. Thus, this study aims at examining the status of PCSK6/Corin in the lung of rats with CHF induced by the creation of aorto-caval fistula (ACF) between the abdominal aorta and vena cava in SD rats. Rats with ACF were divided into 2 subgroups based on the pattern of their daily sodium excretion, compensated and decompensated CHF. Placement of ACF led to cardiac hypertrophy, pulmonary congestion, and renal dysfunction, which were more severe in the decompensated subgroup, despite remarkable elevation of circulatory ANP and BNP levels. Corin mRNA and immunoreactive peptide were detected in pulmonary tissue of all experimental groups. However, the expression and abundance of pulmonary corin significantly increased in the decompensated animals, but not in the compensated ones. Noteworthy, the expression of PCSK6 and ANP/BNP in the pulmonary tissue followed a similar pattern as corin. The upregulation of pulmonary Corin/PCSK6 and NPs were accompanied by local activation of cathepsin L and certain cytokines including IL-6. In light of the anti-inflammatory role of NPs, we postulate that the obtained upregulation of pulmonary PCSK6/Corin along NPs in rats with decompensated CHF may represent a counterbalance response to the inflammatory milieu characterizing CHF especially in severe cases.

Highlights

Heart failure (HF) is endemic in the Western world with continuously rising incidence estimated to affect more than 23 million patients worldwide, especially among aging population [1, 2]
The expression of proprotein convertase subtilisin/kexin-6 (PCSK6) and Atrial natriuretic peptide (ANP)/brain natriuretic peptide (BNP) in the pulmonary tissue followed a similar pattern as corin
The present study provides novel information concerning the status of corin and PCSK6 in the pulmonary tissue of rats with Congestive heart failure (CHF)

Summary

Introduction

Heart failure (HF) is endemic in the Western world with continuously rising incidence estimated to affect more than 23 million patients worldwide, especially among aging population [1, 2]. Besides its cardiac, renal, pulmonary and fluid imbalance manifestations, CHF is considered as inflammatory disease where proinflammatory substances are detected at high concentrations in several vital organs, including heart, kidney, and lung, as well as the circulation [12,13,14,15,16]. These inflammatory processes are profoundly involved in the structural and functional deterioration that occurs in heart failure [11, 12, 15, 16]. While the exact underlying causes of inflammation are not clear, it most likely instigated by intrinsic injury to end target organs, which recruits and activates immune cells of both the innate and adaptive systems

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