A synthetic epoxyeicosatrienoic acid analogue prevents the initiation of ischemic acute kidney injury

Hoff, Uwe; Bubalo, Gordana; Fechner, Mandy; Blum, M; Zhu, Ye; Pohlmann, Andreas; Hentschel, Jan; Arakelyan, Karen; Seeliger, Erdmann; Flemming, Bert; Gürgen, Dennis; Rothe, Michael; Niendorf, Thoralf; Manthati, Vijaya L.; Falck, John R.; Haase, Michael; Schunck, Wolf Hagen; Dragun, Duska

doi:10.1111/apha.13297

Cited by 25 publications

(34 citation statements)

References 77 publications

(183 reference statements)

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“…13,14 Renal MRI is noninvasive, affords full kidney coverage, excellent soft tissue contrast, high temporal resolution, and longitudinal studies without ionizing radiation, 15,16 as illustrated by Figure 1 showing multi-parametric MRI for probing different physiological parameters at different spatial scales using T 1 , T 2 , T 2 *, blood oxygenation level dependent, apparent water diffusion and renal blood volume contrast. 13,14 Renal MRI is noninvasive, affords full kidney coverage, excellent soft tissue contrast, high temporal resolution, and longitudinal studies without ionizing radiation, 15,16 as illustrated by Figure 1 showing multi-parametric MRI for probing different physiological parameters at different spatial scales using T 1 , T 2 , T 2 *, blood oxygenation level dependent, apparent water diffusion and renal blood volume contrast.…”

Section: Validation With Quantitative Physiological Measurementsmentioning

confidence: 99%

“…Functional MRI of the kidney may serve as a striking example: state-of-the-art renal MRI allows investigators to qualitatively assess physiological parameters such as renal blood flow, GFR and oxygenation. 13,14 Renal MRI is noninvasive, affords full kidney coverage, excellent soft tissue contrast, high temporal resolution, and longitudinal studies without ionizing radiation, 15,16 as illustrated by Figure 1 showing multi-parametric MRI for probing different physiological parameters at different spatial scales using T 1 , T 2 , T 2 *, blood oxygenation level dependent, apparent water diffusion and renal blood volume contrast. Yet, the validity of functional MRI techniques for renal parameters for various (patho-)physiological scenarios remains to be established.…”

Section: Validation With Quantitative Physiological Measurementsmentioning

confidence: 99%

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Google maps for tissues: Multiscale imaging of biological systems and disease

et al. 2019

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kidneys: A) photograph of freshly excised kidney, B) T 1 -weighted anatomical MR microscopy acquired ex vivo using an in-plane spatial resolution of 50 μm (cortex COR; outer medulla OM; inner medulla IM), C) T 2 * sensitized MR image acquired ex vivo using an in-plane spatial resolution of 50 μm, D) Mesoscopic in vivo parametric map of the MRI relaxation time T 2 which represents the blood oxygenation level at the more capillary level (in-plane spatial resolution 300 μm), E) In vivo map of the MRI relaxation parameter T 2 * (in-plane spatial resolution of 300 μm) which is a surrogate for blood oxygenation of large venous vessels, F) Apparent water diffusion coefficient (ADC) map with a spatial resolution of 300 μm showing Brownian water motion at the scale of 50 μm, G) In vivo map of renal cortical and outer medullary renal blood volume fraction (BVf) obtained from T 2 * mapping using an intravascular contrast agent (4 mg Fe/kg USPIO). The 1 cm scale bar illustrates the size of the rat kidney. MRI, magnetic resonance imaging | 5 of 5 EXACTA Centre for Cardiovascular Research, BER 6.1, partner site Berlin) and by the Federal Ministry

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Section: Validation With Quantitative Physiological Measurementsmentioning

confidence: 99%

Section: Validation With Quantitative Physiological Measurementsmentioning

confidence: 99%

Google maps for tissues: Multiscale imaging of biological systems and disease

et al. 2019

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“…2 EETs by contrast are mainly derived from the vascular endothelium, and some may act as vasodilators that attenuate inflammation and hypertension. 1 Notably, at 48-hours follow-up, the EET-treated rats displayed plasma creatinine and urea concentrations and thus creatinine clearance values not different from control rats. 3 The authors exploited previous data showing that (a) modification of the 14,15-EET into a more stable urea bioisostere still yielded potent vascular relaxation, 4 and (b) 14,15-EET is a vasodilator in the perfused kidney.…”

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confidence: 91%

“…Arachidonic acid can be metabolized by 3 distinct pathways: lipoxygenase, cyclooxygenase and CYPs. The investigators of the Acta Physiologica study 1 have shown previously in mice that deletion of the enzyme responsible for degradation and inactivation of EET, soluble epoxide hydrolase (sEH), elevated EET expectedly but did not exert the predicted protective effect on GFR and tissue injury after 22 minutes kidney ischaemia insult and 2-day follow-up. Both fatty acid derivatives are short lived; they are produced by the kidneys, and substantial data show that 20-HETE is a vasoconstrictor in the renal vascular bed involved in autoregulation of blood flow by myogenic and tubuloglomerular feedback mechanisms and as an amplifier of the vasoconstrictor action of endothelin and angiotensin II (reviewed by Fan and Roman).…”

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confidence: 99%

“…CYP enzymes synthesize EET regioisomers: 5,6-EET, 8,9-EET, 11,12-EET and 14,15-EET, and this is of functional relevance since diameter responses to regioisomers differ in kidneys. 1 It was concluded that detrimental upregulation of 20-HETE formation in response to ischaemia-reperfusion could be mitigated by pre-treatment with a more stable EET analog in an animal model of kidney injury. 3 While 20-HETE has been tested in numerous studies for a negative role in ischaemia-reperfusion injury, surprisingly few studies have addressed the potential protective effect of selected EETs in ischaemia-reperfusion injury in kidneys.…”

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Protection against acute kidney injury is afforded by a 14,15‐epoxy‐eicosatrienoic acid (EET) analog—A potential druggable pathway

Jensen

2019

Acta Physiologica

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Subsegmentation of the Kidney in Experimental MR Images Using Morphology-Based Regions-of-Interest or Multiple-Layer Concentric Objects

Riazy

Milani

Periquito

et al. 2021

Methods in Molecular Biology

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Functional renal MRI promises access to a wide range of physiologically relevant parameters such as blood oxygenation, perfusion, tissue microstructure, pH, and sodium concentration. For quantitative comparison of results, representative values must be extracted from the parametric maps obtained with these different MRI techniques. To improve reproducibility of results this should be done based on regions-of-interest (ROIs) that are clearly and objectively defined.Semiautomated subsegmentation of the kidney in magnetic resonance images represents a simple but very valuable approach for the quantitative analysis of imaging parameters in multiple ROIs that are associated with specific anatomic locations. Thereby, it facilitates comparing MR parameters between different kidney regions, as well as tracking changes over time.Here we provide detailed step-by-step instructions for two recently developed subsegmentation techniques that are suitable for kidneys of small rodents: i) the placement of ROIs in cortex, outer and the inner medulla based on typical kidney morphology and ii) the division of the kidney into concentrically oriented layers.This chapter is based upon work from the COST Action PARENCHIMA, a community-driven network funded by the European Cooperation in Science and Technology (COST) program of the European Union, which aims to improve the reproducibility and standardization of renal MRI biomarkers.

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A synthetic epoxyeicosatrienoic acid analogue prevents the initiation of ischemic acute kidney injury

Cited by 25 publications

References 77 publications

Google maps for tissues: Multiscale imaging of biological systems and disease

Google maps for tissues: Multiscale imaging of biological systems and disease

Protection against acute kidney injury is afforded by a 14,15‐epoxy‐eicosatrienoic acid (EET) analog—A potential druggable pathway

Subsegmentation of the Kidney in Experimental MR Images Using Morphology-Based Regions-of-Interest or Multiple-Layer Concentric Objects

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