Functional MRI for characterization of renal perfusion impairment and edema formation due to acute kidney injury in different mouse strains

Functional MRI for characterization of renal perfusion impairment and edema formation due to acute kidney injury in different mouse strains

The purpose was to characterize acute kidney injury (AKI) in C57BL/6 (B6)- and 129/Sv (Sv)-mice by noninvasive measurement of renal perfusion and tissue edema using functional MRI. Different severities of AKI were induced in B6- and Sv-mice by renal ischemia reperfusion injury (IRI). Unilateral clam...

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Bibliographic Details
Published in:PloS one Vol. 12; no. 3; p. e0173248
Main Authors: Tewes, Susanne, Gueler, Faikah, Chen, Rongjun, Gutberlet, Marcel, Jang, Mi-Sun, Meier, Martin, Mengel, Michael, Hartung, Dagmar, Wacker, Frank, Rong, Song, Hueper, Katja
Format: Journal Article
Language:English
Published: United States Public Library of Science 20-03-2017
Public Library of Science (PLoS)
Subjects:
Acute kidney failure
Acute Kidney Injury - diagnostic imaging
Acute Kidney Injury - pathology
Acute Kidney Injury - physiopathology
Analysis
Animals
Biology and Life Sciences
Collagen (type IV)
Diagnosis
Disease Models, Animal
Disease Progression
Edema
Edema - diagnostic imaging
Edema - pathology
Edema - physiopathology
Fibrosis
Fibrosis - diagnostic imaging
Fibrosis - pathology
Fibrosis - physiopathology
Functional magnetic resonance imaging
Health aspects
Histology
Hypertension
Immunohistochemistry
Impairment
Injuries
Ischemia
Kidney - diagnostic imaging
Kidney - pathology
Kidney - physiopathology
Kidney diseases
Kidneys
Laboratory animals
Macrophages - pathology
Macrophages - physiology
Magnetic Resonance Imaging
Male
Medical schools
Medicine and Health Sciences
Mice
Mice, 129 Strain
Mice, Inbred C57BL
Morphology
Nephrology
NMR
Nuclear magnetic resonance
Organ Size
Perfusion
Relaxation time
Renal cortex
Reperfusion
Reperfusion Injury
Research and Analysis Methods
Severity of Illness Index
Species Specificity
Spin labeling
Studies
Surgery
Time Factors
Transplants & implants
United States
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Summary:The purpose was to characterize acute kidney injury (AKI) in C57BL/6 (B6)- and 129/Sv (Sv)-mice by noninvasive measurement of renal perfusion and tissue edema using functional MRI. Different severities of AKI were induced in B6- and Sv-mice by renal ischemia reperfusion injury (IRI). Unilateral clamping of the renal pedicle for 35 min (moderate AKI) or 45 min (severe AKI) was done. MRI (7-Tesla) was performed 1, 7 and 28 days after surgery using a flow alternating inversion recovery (FAIR) arterial spin labeling (ASL) sequence. Maps of perfusion and T1-relaxation time were calculated. Relative MRI-parameters of the IRI kidney compared to the contralateral not-clipped kidney were compared between AKI severities and between mouse strains using unpaired t-tests. In addition, fibrosis was assessed by Masson Trichrome and collagen IV staining. After moderate AKI relative perfusion impairment was significantly higher in B6- than in Sv-mice at d7 (55±7% vs. 82±8%, p<0.05) and d28 (76±7% vs. 102±3%, p<0.01). T1-values increased in the early phase after AKI in both mouse strains. T1-increase was more severe after prolonged ischemia times of 45 min compared to 35 min in both mouse strains, measured in the renal cortex and outer stripe of outer medulla. Kidney volume loss (compared to the contralateral kidney) occurred already after 7 days but proceeded markedly towards 4 weeks in severe AKI. Early renal perfusion impairment was predictive for later kidney volume loss. The progression to chronic kidney disease (CKD) in the severe AKI model was similar in both mouse strains as revealed by histology. Quantification of renal perfusion and tissue edema by functional MRI allows characterization of strain differences upon AKI. Renal perfusion impairment was stronger in B6- compared to Sv-animals following moderate AKI. Prolonged ischemia times were associated with more severe perfusion impairment and edema formation in the early phase and progression to CKD within 4 weeks of observation.
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Conceptualization: FG KH ST.Data curation: KH FG.Formal analysis: KH FG ST M. Mengel.Funding acquisition: KH FG ST.Investigation: SR M. Meier M. Mengel RC MJ.Methodology: FG RC KH SR ST M. Meier M. Mengel.Project administration: KH FG.Resources: M. Meier KH FG.Software: MG.Supervision: FG KH FW.Validation: M. Meier M. Mengel FG KH ST.Visualization: KH FG ST.Writing – original draft: KH FG ST.Writing – review & editing: ST FG RC MG MJ M. Meier M. Mengel DH FW SR KH.
These authors also contributed equally to this work.
Competing Interests: KH and MG have a research collaboration with Siemens Healthcare outside the work submitted. FW receives institutional grants from Siemens Healthcare and Promedicus Ltd and Delcath Systems Inc. outside the work submitted. FG is consulting for A1M Pharma not related to the work submitted. This does not alter our adherence to PLOS ONE policies on sharing data and materials.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0173248