Effects of elevation of ANP and its deficiency on cardiorenal function
Daria V. Ilatovskaya, Vladislav Levchenko, Kristen Winsor, Gregory R. Blass, Denisha R. Spires, Elizaveta Sarsenova, Iuliia Polina, Adrian Zietara, Mark Paterson, Alison J. Kriegel, Alexander Staruschenko
Daria V. Ilatovskaya, Vladislav Levchenko, Kristen Winsor, Gregory R. Blass, Denisha R. Spires, Elizaveta Sarsenova, Iuliia Polina, Adrian Zietara, Mark Paterson, Alison J. Kriegel, Alexander Staruschenko
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Research Article Nephrology

Effects of elevation of ANP and its deficiency on cardiorenal function

Abstract

Atrial natriuretic peptide (ANP), encoded by Nppa, is a vasodilatory hormone that promotes salt excretion. Genome-wide association studies identified Nppa as a causative factor of blood pressure development, and in humans, ANP levels were suggested as an indicator of salt sensitivity. This study aimed to provide insights into the effects of ANP on cardiorenal function in salt-sensitive hypertension. To address this question, hypertension was induced in SSNPPA–/– (KO of Nppa in the Dahl salt-sensitive [SS] rat background) or SSWT (WT Dahl SS) rats by a high-salt (HS) diet challenge (4% NaCl for 21 days). Chronic infusion of ANP in SSWT rats attenuated the increase in blood pressure and cardiorenal damage. Overall, the SSNPPA–/– strain demonstrated higher blood pressure and intensified cardiac fibrosis (with no changes in ejection fraction) compared with SSWT rats. Furthermore, SSNPPA–/– rats exhibited kidney hypertrophy and higher glomerular injury scores, reduced diuresis, and lower sodium and chloride excretion than SSWT when fed a HS diet. Additionally, the activity of epithelial Na+ channel (ENaC) was found to be increased in the collecting ducts of the SSNPPA–/– rats. Taken together, these data show promise for the therapeutic benefits of ANP and ANP-increasing drugs for treating salt-sensitive hypertension.

Authors

Daria V. Ilatovskaya, Vladislav Levchenko, Kristen Winsor, Gregory R. Blass, Denisha R. Spires, Elizaveta Sarsenova, Iuliia Polina, Adrian Zietara, Mark Paterson, Alison J. Kriegel, Alexander Staruschenko

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Figure 5

Male SSNPPA–/– rats exhibit aggravated cardiac fibrosis and hypertrophy following a HS diet challenge.

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Male SSNPPA–/– rats exhibit aggravated cardiac fibrosis and hypertrophy ...
(A) Masson trichrome–stained cardiac tissues. (B) Summary of heart/body weight ratio obtained from the 11-week-old SSWT rats on NS and HS, and SSNPPA–/– rats on NS and HS; n = 8, 9, 8, 8. (C) Continuous heart rate recorded with telemetry from the SSWT (n = 6) and SSNPPA–/– (n = 7) rats throughout the protocol (each point shows daily averages from 9 a.m. to 12 p.m.). (D and E) Representative images of Masson trichrome–stained hearts and analysis of cardiac interstitial fibrosis assessed in the 11-week-old SSWT rats on NS and HS, and SSNPPA–/– rats on NS and HS; n = 6, 9, 5, and 8 rats (independent tissues analyzed). Fibrosis was calculated as percentage of the total area of the tissue section. (F) Perivascular cardiac fibrosis assessed in the 11-week-old SSWT rats on NS and HS, and SSNPPA–/– rats on NS and HS, presented as percentage of fibrotic area versus whole vessel area; n = 6, 9, 5, 8 (each point represents an average of 25–30 randomly selected vessels per tissue section). Data were analyzed with 2-way ANOVA, followed by a Holm-Sidak post hoc test; if significant, P values are shown on the graphs. Male animals were used.