Lysyl oxidase inhibitors attenuate cyclosporin A-induced nephropathy in mouse

Lysyl oxidase inhibitors attenuate cyclosporin A-induced nephropathy in mouse

Abstract Calcineurin inhibitors, such as Cyclosporin (CsA), are the mainstay of anti-rejection therapy in solid organ transplants but can paradoxically induce progressive nephropathy characterised by renal dysfunction and interstitial fibrosis. Lysyl oxidases (LOXs), a group of enzymes that catalyse...

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Main Authors: Long T. Nguyen, Sonia Saad, Ying Shi, Rosy Wang, Angela S. Y. Chou, Anthony Gill, Yimin Yao, Wolfgang Jarolimek, Carol A. Pollock
Format: Article
Language:English
Published: Nature Publishing Group 2021-06-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-021-91772-5
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spelling doaj-1d8b0be6924f440380930771f436d6c42021-06-20T11:34:16ZengNature Publishing GroupScientific Reports2045-23222021-06-0111111210.1038/s41598-021-91772-5Lysyl oxidase inhibitors attenuate cyclosporin A-induced nephropathy in mouseLong T. Nguyen0Sonia Saad1Ying Shi2Rosy Wang3Angela S. Y. Chou4Anthony Gill5Yimin Yao6Wolfgang Jarolimek7Carol A. Pollock8Renal Medicine, Kolling Institute, Royal North Shore Hospital, University of SydneyRenal Medicine, Kolling Institute, Royal North Shore Hospital, University of SydneyRenal Medicine, Kolling Institute, Royal North Shore Hospital, University of SydneyRenal Medicine, Kolling Institute, Royal North Shore Hospital, University of SydneyCancer Diagnosis and Pathology Research Group, Kolling Institute, Royal North Shore Hospital, University of SydneyCancer Diagnosis and Pathology Research Group, Kolling Institute, Royal North Shore Hospital, University of SydneyDrug Discovery Department, Pharmaxis Ltd.Drug Discovery Department, Pharmaxis Ltd.Renal Medicine, Kolling Institute, Royal North Shore Hospital, University of SydneyAbstract Calcineurin inhibitors, such as Cyclosporin (CsA), are the mainstay of anti-rejection therapy in solid organ transplants but can paradoxically induce progressive nephropathy characterised by renal dysfunction and interstitial fibrosis. Lysyl oxidases (LOXs), a group of enzymes that catalyse extracellular matrix (ECM) crosslinking, were shown to implicate in tissue scarring. It is hypothesized that inhibition of these enzymes may render therapeutic effects against CsA-induced nephropathy. In this study, 6-to-8 weeks old C57BL/6 J mice were administered saline or CsA (30 mg/kg/day s.c) for 16 weeks. At 8 weeks, CsA-treated animals were divided into 5 groups respectively treated with: (1) vehicle, (2) PXS-5505 (Pan-LOX inhibitor), (3) PXS-5382 (LOX-like 2 inhibitor), (4) PXS-5505 for 4 weeks then PXS-5382 for 4 weeks (sequential therapy), and (5) Telmisartan (standard therapy). Our results indicate that CsA administration significantly increased the levels of blood urea nitrogen, glomerular and tubular injury, tubulointerstitial fibrosis, inflammation and oxidative stress in mouse kidney. These changes were associated with upregulated mRNA expression of LOX and LOXL2. Administration of Pan-LOX or LOXL2 inhibitors or the sequential therapy suppressed the expression of ECM proteins (α-SMA, FN and COL1A), matrix metalloproteases (MMP)2 and 9, inflammatory markers (TNFα and MCP-1) and TGF-β1-Smad3 signalling. Among all regimens including telmisartan, only Pan-LOX inhibitor PXS-5505 was able to attenuate uraemia. Collectively, our study suggests that Pan-LOX and LOXL2 inhibition can attenuate progressive nephropathy due to CsA administration.https://doi.org/10.1038/s41598-021-91772-5
collection DOAJ
language English
format Article
sources DOAJ
author Long T. Nguyen
Sonia Saad
Ying Shi
Rosy Wang
Angela S. Y. Chou
Anthony Gill
Yimin Yao
Wolfgang Jarolimek
Carol A. Pollock
spellingShingle Long T. Nguyen
Sonia Saad
Ying Shi
Rosy Wang
Angela S. Y. Chou
Anthony Gill
Yimin Yao
Wolfgang Jarolimek
Carol A. Pollock
Lysyl oxidase inhibitors attenuate cyclosporin A-induced nephropathy in mouse
Scientific Reports
author_facet Long T. Nguyen
Sonia Saad
Ying Shi
Rosy Wang
Angela S. Y. Chou
Anthony Gill
Yimin Yao
Wolfgang Jarolimek
Carol A. Pollock
author_sort Long T. Nguyen
title Lysyl oxidase inhibitors attenuate cyclosporin A-induced nephropathy in mouse
title_short Lysyl oxidase inhibitors attenuate cyclosporin A-induced nephropathy in mouse
title_full Lysyl oxidase inhibitors attenuate cyclosporin A-induced nephropathy in mouse
title_fullStr Lysyl oxidase inhibitors attenuate cyclosporin A-induced nephropathy in mouse
title_full_unstemmed Lysyl oxidase inhibitors attenuate cyclosporin A-induced nephropathy in mouse
title_sort lysyl oxidase inhibitors attenuate cyclosporin a-induced nephropathy in mouse
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2021-06-01
description Abstract Calcineurin inhibitors, such as Cyclosporin (CsA), are the mainstay of anti-rejection therapy in solid organ transplants but can paradoxically induce progressive nephropathy characterised by renal dysfunction and interstitial fibrosis. Lysyl oxidases (LOXs), a group of enzymes that catalyse extracellular matrix (ECM) crosslinking, were shown to implicate in tissue scarring. It is hypothesized that inhibition of these enzymes may render therapeutic effects against CsA-induced nephropathy. In this study, 6-to-8 weeks old C57BL/6 J mice were administered saline or CsA (30 mg/kg/day s.c) for 16 weeks. At 8 weeks, CsA-treated animals were divided into 5 groups respectively treated with: (1) vehicle, (2) PXS-5505 (Pan-LOX inhibitor), (3) PXS-5382 (LOX-like 2 inhibitor), (4) PXS-5505 for 4 weeks then PXS-5382 for 4 weeks (sequential therapy), and (5) Telmisartan (standard therapy). Our results indicate that CsA administration significantly increased the levels of blood urea nitrogen, glomerular and tubular injury, tubulointerstitial fibrosis, inflammation and oxidative stress in mouse kidney. These changes were associated with upregulated mRNA expression of LOX and LOXL2. Administration of Pan-LOX or LOXL2 inhibitors or the sequential therapy suppressed the expression of ECM proteins (α-SMA, FN and COL1A), matrix metalloproteases (MMP)2 and 9, inflammatory markers (TNFα and MCP-1) and TGF-β1-Smad3 signalling. Among all regimens including telmisartan, only Pan-LOX inhibitor PXS-5505 was able to attenuate uraemia. Collectively, our study suggests that Pan-LOX and LOXL2 inhibition can attenuate progressive nephropathy due to CsA administration.
url https://doi.org/10.1038/s41598-021-91772-5
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