To test these hypotheses, we first studied the pro-fibrotic activity of MBG in salt-loaded rats with diabetes type 2 (DM), in which stimulation of MBG and cardiac remodeling were observed in the absence of BP elevation. DM was induced by early postnatal administration of streptozotocin, and 8-week old DM rats were salt loaded (1.8% NaCl instead of water) for 4 weeks, following which BP did not change, MBG levels increased 2-fold and erythrocyte NKA was inhibited vs. control group. During the last week of salt loading, rats were administered anti-MBG mAb or vehicle. Isolated aortic rings from NaCl-loaded DM rats exhibited reduced sensitivity to sodium nitroprusside (SNP; a donor of NO). Collagen-1 abundance in rat aortae increased in parallel to decline in Fli1 level. Increase in collagen-5 levels indicated that another pro-fibrotic pathway is involved in DM. We detected an increase of TGFβ and other proteins, implicated in TGFβ pro-fibrotic pathway (fibronectin, SMAD-5) in aortae from DM rats. Anti-MBG mAb administration did not affect BP, and restored erythrocyte NKA, which was inhibited following high salt intake. Importantly, aortic rings from DM rats, treated with 3E9 mAb, demonstrated restored responsiveness to SNP to control parameters, and decreased levels of aortic proteins implicated in pro-fibrotic TGFβ-signaling protein levels vs. vehicle-treated DM rats. Next, we studied effects of MR antagonist canrenone (10 μM), an active metabolite of spironolactone, on MBG-induced synthesis of collagen-1 in vitro in the explants of rat thoracic aortae. Incubation of aortic rings with 100 nM MBG for 24 h resulted in a reduction of Fli1 level and a concomitant increase in collagen-1 levels, accompanied by reduced sensitivity of aortae to the vasorexation effect of SNP. Addition of canrenone to the incubation media reversed the pro-fibrotic effect of MBG, and restored the vasorelaxation of aortae. In a pilot study in patients with RH (7 men and 9 women, 562 years) we assessed BP, vascular stiffness as a pulse wave velocity (PWV), plasma levels of MBG and activity of erythrocyte NKA before and after a six-month of addition of placebo or spironolactone (50 mg/day) to the conventional triple therapy (lisinopril/amlodipine/hydrochlorothiazide). RH patients demonstrated greater BP and PWV, higher serum creatinine, reduced GFR, elevated plasma MBG, and decreased erythrocyte NKA activity vs. normotensive control. Administration of spironolactone to RH patients for 6 months was associated with restoration of NKA activity even in the presence of unchanged MBG levels. Spironolactone treatment, unlike placebo, decreased systolic and diastolic BP, and significantly reduced PWV. Thus, MR antagonists reversed MBG-induced vascular collagen deposition that may compromise relaxation of rat aortae. These data together with the clinical finding that spironolactone can reduce arterial stiffness in RH patients and restore NKA in the presence of increased MBG levels, indicate the deep relation between MBG and arterial stiffness. Thus MBG and MBG-induced arterial remodeling and arterial stiffness are novel targets for MR antagonists. Conclusion: Thus, both immunoneutralization of heightened MBG levels and modulation of NKA/MBG interaction by aldosterone antagonists demonstrated anti-fibroric effects in various pathological conditions, when increased MBG levels participate in development of vascular stiffness via activation of Fli-1 and/or TGFβ signaling.

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Investigator-Initiated Intramural Research Projects (ZIA)
Project #
1ZIAAG000609-23
Application #
9147309
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
23
Fiscal Year
2015
Total Cost
Indirect Cost
Name
Aging
Department
Type
DUNS #
City
State
Country
Zip Code
Chirinos, Julio A; Sardana, Mayank; Oldland, Garrett et al. (2018) Association of arginine vasopressin with low atrial natriuretic peptide levels, left ventricular remodelling, and outcomes in adults with and without heart failure. ESC Heart Fail 5:911-919
Strauss, Michél; Smith, Wayne; Kruger, Ruan et al. (2018) Marinobufagenin and left ventricular mass in young adults: The African-PREDICT study. Eur J Prev Cardiol 25:1587-1595
Chirinos, Julio A; Sardana, Mayank; Syed, Amer Ahmed et al. (2018) Aldosterone, inactive matrix gla-protein, and large artery stiffness in hypertension. J Am Soc Hypertens 12:681-689
Strauss, Michél; Smith, Wayne; Wei, Wen et al. (2018) Marinobufagenin is related to elevated central and 24-h systolic blood pressures in young black women: the African-PREDICT Study. Hypertens Res 41:183-192
AlGhatrif, Majd; Wang, Mingyi; Fedorova, Olga V et al. (2017) The Pressure of Aging. Med Clin North Am 101:81-101
Gable, Marjorie E; Ellis, Linda; Fedorova, Olga V et al. (2017) Comparison of Digitalis Sensitivities of Na(+)/K(+)-ATPases from Human and Pig Kidneys. ACS Omega 2:3610-3615
Fedorova, Olga V; Zernetkina, Valentina I; Shilova, Victoria Y et al. (2015) Synthesis of an Endogenous Steroidal Na Pump Inhibitor Marinobufagenin, Implicated in Human Cardiovascular Diseases, Is Initiated by CYP27A1 via Bile Acid Pathway. Circ Cardiovasc Genet 8:736-45
Fedorova, Olga V; Lakatta, Edward G; Bagrov, Alexei Y et al. (2015) Plasma level of the endogenous sodium pump ligand marinobufagenin is related to the salt-sensitivity in men. J Hypertens 33:534-41; discussion 541
Kennedy, David J; Shrestha, Kevin; Sheehey, Brendan et al. (2015) Elevated Plasma Marinobufagenin, An Endogenous Cardiotonic Steroid, Is Associated With Right Ventricular Dysfunction and Nitrative Stress in Heart Failure. Circ Heart Fail 8:1068-76
Fedorova, Olga V; Emelianov, Igor V; Bagrov, Konstantin A et al. (2015) Marinobufagenin-induced vascular fibrosis is a likely target for mineralocorticoid antagonists. J Hypertens 33:1602-10

Showing the most recent 10 out of 23 publications