Literature DB >> 22902873

Submaximal suppression of parathyroid hormone ameliorates calcitriol-induced aortic calcification and remodeling and myocardial fibrosis in uremic rats.

Susanne Jung1, Uwe Querfeld, Dominik Müller, Birgit Rudolph, Harm Peters, Stephanie Krämer.   

Abstract

BACKGROUND AND
OBJECTIVE: In subtotally nephrectomized rats, we studied to what extent high-dose calcitriol-induced cardiovascular disease can be modulated by almost complete suppression of parathyroid hormone (PTH), mediated by either cinacalcet (CINA) or parathyroidectomy (PTX).
METHODS: Five groups were studied: sham-operated controls, uremic (U), uremic with calcitriol (U+1,25D), uremic and calcitriol with CINA (U+1,25D+CINA) and uremic and calcitriol with PTX (U+1,25D+PTX). Treatments lasted 14 weeks.
RESULTS: Compared with U group animals, PTH was significantly lower with calcitriol treatment and almost completely suppressed in animals treated with either PTX or CINA. Serum calcium and phosphorus levels were similarly elevated in all groups receiving calcitriol. Renal function in uremic animals was significantly more impaired in the U+1,25D group. Aortic calcifications were pronounced in U+1,25D animals and reduced by more than 50% by concomittant treatment with CINA or PTX. Chondrocytes were observed near areas of calcification (>90%) and endochondral bone formation was confirmed by positive immunofluorescence for chondrocytic transcription factor sox9 and matrix protein collagen X. Altered arterial (aneurysmatic) geometry with a significant increase in wall/lumen and lumen/body weight ratio was found only in the U+1,25D group. Myocardial fibrosis was present in all uremic groups with a significant increase in the U+1,25D group. Connective tissue growth factor messenger RNA was significantly upregulated only in the U+1,25D group.
CONCLUSION: Submaximal suppression of PTH by either CINA or PTX reduced vascular calcifications, arterial remodeling and myocardial fibrosis to a similar degree and independent of the serum calcium and phosphorus levels. These data do not indicate vasculotropic effects of calcimimetics independent of PTH suppression.

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Year:  2012        PMID: 22902873     DOI: 10.1097/HJH.0b013e328357c049

Source DB:  PubMed          Journal:  J Hypertens        ISSN: 0263-6352            Impact factor:   4.844


  12 in total

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Authors:  Justine Bacchetta
Journal:  Pediatr Nephrol       Date:  2019-11-06       Impact factor: 3.714

2.  Cinacalcet ameliorates cardiac fibrosis in uremic hearts through suppression of endothelial-to-mesenchymal transition.

Authors:  Min Wu; Ri-Ning Tang; Hong Liu; Ming-Ming Pan; Lin-Li Lv; Jian-Dong Zhang; Steven D Crowley; Bi-Cheng Liu
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3.  Cinacalcet ameliorates aortic calcification in uremic rats via suppression of endothelial-to-mesenchymal transition.

Authors:  Min Wu; Ri-Ning Tang; Hong Liu; Ming-Ming Pan; Bi-Cheng Liu
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Review 4.  Vitamin D and Calcimimetics in Cardiovascular Disease.

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6.  Clinical outcomes and survival in pediatric patients initiating chronic dialysis: a report of the NAPRTCS registry.

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Review 7.  Calcimimetics and outcomes in CKD.

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Review 8.  Vascular calcification and renal bone disorders.

Authors:  Kuo-Cheng Lu; Chia-Chao Wu; Jen-Fen Yen; Wen-Chih Liu
Journal:  ScientificWorldJournal       Date:  2014-07-17

9.  Acid-base balance in uremic rats with vascular calcification.

Authors:  Alan Peralta-Ramírez; Ana Isabel Raya; Carmen Pineda; Mariano Rodríguez; Escolástico Aguilera-Tejero; Ignacio López
Journal:  Nephron Extra       Date:  2014-07-02

10.  PTH suppression by calcitriol does not predict off-target actions in experimental CKD.

Authors:  Bruno A Svajger; Cynthia M Pruss; Kimberly J Laverty; Jason G E Zelt; Glenville Jones; Martin Kaufmann; Martin Petkovich; Rachel M Holden; Michael A Adams
Journal:  Pharmacol Res Perspect       Date:  2020-06
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