Literature DB >> 33130676

Recovery of Renal Function following Kidney-Specific VEGF Therapy in Experimental Renovascular Disease.

Jason E Engel1, Maxx L Williams1, Erika Williams1, Camille Azar1, Erin B Taylor1, Gene L Bidwell2,3,4, Alejandro R Chade5,6,7.   

Abstract

BACKGROUND: Chronic renovascular disease (RVD) can lead to a progressive loss of renal function, and current treatments are inefficient. We designed a fusion of vascular endothelial growth factor (VEGF) conjugated to an elastin-like polypeptide (ELP) carrier protein with an N-terminal kidney-targeting peptide (KTP). We tested the hypothesis that KTP-ELP-VEGF therapy will effectively recover renal function with an improved targeting profile. Further, we aimed to elucidate potential mechanisms driving renal recovery.
METHODS: Unilateral RVD was induced in 14 pigs. Six weeks later, renal blood flow (RBF) and glomerular filtration rate (GFR) were quantified by multidetector CT imaging. Pigs then received a single intrarenal injection of KTP-ELP-VEGF or vehicle. CT quantification of renal hemodynamics was repeated 4 weeks later, and then pigs were euthanized. Ex vivo renal microvascular (MV) density and media-to-lumen ratio, macrophage infiltration, and fibrosis were quantified. In parallel, THP-1 human monocytes were differentiated into naïve macrophages (M0) or inflammatory macrophages (M1) and incubated with VEGF, KTP-ELP, KTP-ELP-VEGF, or control media. The mRNA expression of macrophage polarization and angiogenic markers was quantified (qPCR).
RESULTS: Intrarenal KTP-ELP-VEGF improved RBF, GFR, and MV density and attenuated MV media-to-lumen ratio and renal fibrosis compared to placebo, accompanied by augmented renal M2 macrophages. In vitro, exposure to VEGF/KTP-ELP-VEGF shifted M0 macrophages to a proangiogenic M2 phenotype while M1s were nonresponsive to VEGF treatment.
CONCLUSIONS: Our results support the efficacy of a new renal-specific biologic construct in recovering renal function and suggest that VEGF may directly influence macrophage phenotype as a possible mechanism to improve MV integrity and function in the stenotic kidney.
© 2020 S. Karger AG, Basel.

Entities:  

Keywords:  Angiogenesis; Drug-delivery technology; Macrophage; Microcirculation; Renovascular disease; Vascular endothelial growth factor

Year:  2020        PMID: 33130676      PMCID: PMC7750286          DOI: 10.1159/000511260

Source DB:  PubMed          Journal:  Am J Nephrol        ISSN: 0250-8095            Impact factor:   3.754


  49 in total

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2.  Systemic biopolymer-delivered vascular endothelial growth factor promotes therapeutic angiogenesis in experimental renovascular disease.

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6.  Reversal of renal dysfunction by targeted administration of VEGF into the stenotic kidney: a novel potential therapeutic approach.

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Journal:  Am J Physiol Renal Physiol       Date:  2012-02-22

7.  Renal Therapeutic Angiogenesis Using a Bioengineered Polymer-Stabilized Vascular Endothelial Growth Factor Construct.

Authors:  Alejandro R Chade; Nathan A Tullos; Taylor W Harvey; Fakhri Mahdi; Gene L Bidwell
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Review 8.  Current Concepts in the Treatment of Renovascular Hypertension.

Authors:  Sandra M Herrmann; Stephen C Textor
Journal:  Am J Hypertens       Date:  2018-01-12       Impact factor: 2.689

9.  Conservation and divergence in Toll-like receptor 4-regulated gene expression in primary human versus mouse macrophages.

Authors:  Kate Schroder; Katharine M Irvine; Martin S Taylor; Nilesh J Bokil; Kim-Anh Le Cao; Kelly-Anne Masterman; Larisa I Labzin; Colin A Semple; Ronan Kapetanovic; Lynsey Fairbairn; Altuna Akalin; Geoffrey J Faulkner; John Kenneth Baillie; Milena Gongora; Carsten O Daub; Hideya Kawaji; Geoffrey J McLachlan; Nick Goldman; Sean M Grimmond; Piero Carninci; Harukazu Suzuki; Yoshihide Hayashizaki; Boris Lenhard; David A Hume; Matthew J Sweet
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