Low-dose hydralazine during gestation reduces renal fibrosis in rodent offspring exposed to maternal high fat diet

Larkin, BP; Saad, S; Glastras, SJ; Nguyen, LT; Hou, M; Chen, H; Wang, R; Pollock, CA

Low-dose hydralazine during gestation reduces renal fibrosis in rodent offspring exposed to maternal high fat diet

Larkin, BP Saad, S Glastras, SJ Nguyen, LT Hou, M Chen, H

Wang, R Pollock, CA

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Publisher:: PUBLIC LIBRARY SCIENCE
Publication Type:: Journal Article
Citation:: PLOS ONE, 2021, 16, (3), pp. e0248854
Issue Date:: 2021-03-18

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Field	Value	Language
dc.contributor.author	Larkin, BP
dc.contributor.author	Saad, S
dc.contributor.author	Glastras, SJ
dc.contributor.author	Nguyen, LT
dc.contributor.author	Hou, M
dc.contributor.author	Chen, H https://orcid.org/0000-0001-6883-3752
dc.contributor.author	Wang, R
dc.contributor.author	Pollock, CA
dc.date.accessioned	2022-01-12T04:57:46Z
dc.date.available	2021-03-08
dc.date.available	2022-01-12T04:57:46Z
dc.date.issued	2021-03-18
dc.identifier.citation	PLOS ONE, 2021, 16, (3), pp. e0248854
dc.identifier.issn	1932-6203
dc.identifier.issn	1932-6203
dc.identifier.uri	http://hdl.handle.net/10453/152976
dc.description.abstract	BACKGROUND: Maternal high fat diet (HFD) promotes chronic kidney disease (CKD) in offspring. This is in accordance with the theory of fetal programming, which suggests adverse conditions occurring in utero predispose offspring to chronic conditions later in life. DNA methylation has been proposed as a key mechanism by which fetal programming occurs and is implicated in CKD progression. DNA demethylating drugs may interrupt the fetal programming of CKD by maternal obesity. Hydralazine, an antihypertensive agent, demethylates DNA at low doses which do not reduce blood pressure. We used a mouse model of maternal obesity to determine whether gestational administration of low-dose hydralazine to mothers can prevent CKD in offspring. METHODS: C57BL/6 dams received HFD or chow from 6 weeks prior to mating and were administered subcutaneous hydralazine (5mg/kg) or saline thrice weekly during gestation. Male offspring were weaned to chow and were sacrificed at either postnatal week 9 or week 32. Biometric and metabolic parameters, renal global DNA methylation, renal structural and functional changes and markers of fibrosis, oxidative stress and inflammation were measured in offspring at weeks 9 and 32. RESULTS: In week 9 offspring, maternal HFD consumption did not significantly alter anthropometric or metabolic parameters, or renal global DNA methylation. Week 32 offspring had increased renal global DNA methylation, together with albuminuria, glomerulosclerosis, renal fibrosis and oxidative stress. Administration of low-dose hydralazine to obese mothers during gestation reduced renal global DNA methylation and renal fibrotic markers in week 32 offspring. CONCLUSION: Gestational hydralazine reduced renal global DNA methylation in offspring of obese mothers and attenuated maternal obesity-induced renal fibrosis. These data support the use of low-dose hydralazine as a demethylating agent to prevent CKD arising in offspring due to maternal HFD consumption.
dc.format	Electronic-eCollection
dc.language	eng
dc.publisher	PUBLIC LIBRARY SCIENCE
dc.relation.ispartof	PLOS ONE
dc.relation.isbasedon	10.1371/journal.pone.0248854
dc.rights	info:eu-repo/semantics/openAccess
dc.subject.classification	General Science & Technology
dc.subject.mesh	Albuminuria
dc.subject.mesh	Animals
dc.subject.mesh	Biomarkers
dc.subject.mesh	Body Weight
dc.subject.mesh	Collagen
dc.subject.mesh	DNA Methylation
dc.subject.mesh	Diet, High-Fat
dc.subject.mesh	Female
dc.subject.mesh	Fibronectins
dc.subject.mesh	Fibrosis
dc.subject.mesh	Hydralazine
dc.subject.mesh	Inflammation
dc.subject.mesh	Kidney
dc.subject.mesh	Kidney Glomerulus
dc.subject.mesh	Mice, Inbred C57BL
dc.subject.mesh	Necrosis
dc.subject.mesh	Obesity
dc.subject.mesh	Oxidative Stress
dc.subject.mesh	Pregnancy
dc.title	Low-dose hydralazine during gestation reduces renal fibrosis in rodent offspring exposed to maternal high fat diet
dc.type	Journal Article
utslib.citation.volume	16
utslib.location.activity	United States
pubs.organisational-group	/University of Technology Sydney
pubs.organisational-group	/University of Technology Sydney/Faculty of Science
pubs.organisational-group	/University of Technology Sydney/Strength - CHT - Health Technologies
pubs.organisational-group	/University of Technology Sydney/Faculty of Science/School of Life Sciences
pubs.organisational-group	/University of Technology Sydney/Centre for Health Technologies (CHT)
utslib.copyright.status	open_access	*
dc.date.updated	2022-01-12T04:57:40Z
pubs.issue	3
pubs.publication-status	Published online
pubs.volume	16
utslib.citation.issue	3

Abstract:

BACKGROUND: Maternal high fat diet (HFD) promotes chronic kidney disease (CKD) in offspring. This is in accordance with the theory of fetal programming, which suggests adverse conditions occurring in utero predispose offspring to chronic conditions later in life. DNA methylation has been proposed as a key mechanism by which fetal programming occurs and is implicated in CKD progression. DNA demethylating drugs may interrupt the fetal programming of CKD by maternal obesity. Hydralazine, an antihypertensive agent, demethylates DNA at low doses which do not reduce blood pressure. We used a mouse model of maternal obesity to determine whether gestational administration of low-dose hydralazine to mothers can prevent CKD in offspring. METHODS: C57BL/6 dams received HFD or chow from 6 weeks prior to mating and were administered subcutaneous hydralazine (5mg/kg) or saline thrice weekly during gestation. Male offspring were weaned to chow and were sacrificed at either postnatal week 9 or week 32. Biometric and metabolic parameters, renal global DNA methylation, renal structural and functional changes and markers of fibrosis, oxidative stress and inflammation were measured in offspring at weeks 9 and 32. RESULTS: In week 9 offspring, maternal HFD consumption did not significantly alter anthropometric or metabolic parameters, or renal global DNA methylation. Week 32 offspring had increased renal global DNA methylation, together with albuminuria, glomerulosclerosis, renal fibrosis and oxidative stress. Administration of low-dose hydralazine to obese mothers during gestation reduced renal global DNA methylation and renal fibrotic markers in week 32 offspring. CONCLUSION: Gestational hydralazine reduced renal global DNA methylation in offspring of obese mothers and attenuated maternal obesity-induced renal fibrosis. These data support the use of low-dose hydralazine as a demethylating agent to prevent CKD arising in offspring due to maternal HFD consumption.

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http://hdl.handle.net/10453/152976