Mammalian Fetal Cardiac Regeneration After Myocardial Infarction Is Associated With Differential Gene Expression Compared With the Adult

Zgheib, Carlos; Allukian, Myron; Xu, Jie; Morris, Michael W.; Caskey, Robert C.; Herdrich, Benjamin J.; Hu, Junyi; Gorman, Joseph H.; Gorman, Robert C.; Liechty, Kenneth W.

doi:10.1016/j.athoracsur.2014.01.013

Cited by 22 publications

(40 citation statements)

References 21 publications

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“…The healing and repair process following MI differs in the fetus compared to the adult. Injured fetal hearts can recover from a MI event via proliferation of cardiomyocytes at the site of the infarction and surrounding border zone, and this involves low‐grade inflammation . While the fetal heart does not form a permanent collagenous scar, considerable extracellular matrix deposition occurs in the first week following MI in neonatal rodents .…”

Section: Introductionmentioning

confidence: 99%

Label‐free imaging of healthy and infarcted fetal sheep hearts by two‐photon microscopy

Sorvina

Bader

Lock

et al. 2017

Journal of Biophotonics

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Coronary heart disease is one of the largest causes of death worldwide, making this a significant health care issue. A critical problem for the adult human heart is that it does not undergo effective repair in response to damage, leaving patients with a poor prognosis. Unlike the adult, fetal hearts have the ability to repair after myocardial damage. Using two-photon microscopy, we have visualised the morphological and metabolic changes following myocardial infarction in sheep fetuses, to characterise response to cardiac injury in a mammalian model. Following myocardial infarction, fetal hearts showed no significant increase in collagen deposition in the region of the infarction, when compared to either the surrounding tissue or shams. In contrast, metabolic activity (i. e. NAD(P)H and FAD) was significantly reduced in the region of myocardial infarction, when compared to either the surrounding tissue or sham hearts. For comparison, we also imaged two hearts from preadolescent sheep (sham and myocardial infarction) and showed highly ordered collagen deposition with decreased metabolic activity within the infarcted area. Therefore, two-photon imaging had the capacity to image both morphological and metabolic changes in response to myocardial infarction and showed differences in the response with age. Picture: Two-photon imaging of myocardial infarction (b and d) enabled the visualisation of increased collagen (blue; Em = 431 nm) and changes in other tissue autofluorescence (green; Em = 489-606 nm) in fetal (a and b) and preadolescent (c and d) hearts, compared to shams (a and c). The excitation wavelength was 840 nm. Scale bars: 10 mm.

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Section: Introductionmentioning

confidence: 99%

Label‐free imaging of healthy and infarcted fetal sheep hearts by two‐photon microscopy

Sorvina

Bader

Lock

et al. 2017

Journal of Biophotonics

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“…Sheep are one of the most commonly used large animals for research into perinatal cardiac physiology because of the similarities with humans in terms of the timing of development relative to birth, fetal size and the number of foetuses [ 13 – 15 , 22 ]. Unlike the adult heart, the fetal heart responds to MI with a different gene expression profile, better recovery of cardiac function, diminished inflammatory response and no fibrosis [ 13 – 15 ]. Understanding the mechanism of fetal cardiac regeneration could help us develop ways to regenerate the myocardium in the injured adult heart.…”

Section: Discussionmentioning

confidence: 99%

“…However, after acute irreversible myocardial injury, contrast enters the intracellular space due to disruptions in cell membranes and becomes trapped for a period of time in reperfused cardiac tissue. The fetal myocardium has different cardiomyocyte characteristics, extracellular matrix components, and response to MI, compared with the adult heart [ 13 – 15 , 43 ]. For example, fetal cardiomyocytes are mononucleated and proliferative [ 44 , 45 ].…”

Section: Discussionmentioning

confidence: 99%

“…A fetal sheep model of MI has allowed researchers to investigate the mechanisms involved in fetal myocardial regeneration. The fetal response to MI is characterized by a distinct gene expression profile, elevated myocardial proliferation, diminished inflammation, lack of fibrosis, and better restoration of cellularity and cardiac function within 30 days when compared to adults [ 13 – 15 ]. Developing a method of detecting and monitoring the post-MI fetal heart could therefore help researchers study the mechanisms of cardiac regeneration in fetuses post-MI by promoting or inhibiting repair.…”

Section: Introductionmentioning

confidence: 99%

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Feasibility of detecting myocardial infarction in the sheep fetus using late gadolinium enhancement CMR imaging

Duan

Lock

Perumal

et al. 2016

Journal of Cardiovascular Magnetic Resonance

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BackgroundLate gadolinium enhancement (LGE) cardiovascular magnetic resonance (CMR) imaging has enabled the accurate assessment of myocardial infarction (MI). However, LGE CMR has not been performed successfully in the fetus, where it could be useful for animal studies of interventions to promote cardiac regeneration. We believe that LGE imaging could allow us to document the presence, extent and effect of MI in utero and would thereby expand our capacity for conducting fetal sheep MI research. We therefore aimed to investigate the feasibility of using LGE to detect MI in sheep fetuses.MethodsSix sheep fetuses underwent a thoracotomy and ligation of a left anterior descending (LAD) coronary artery branch; while two fetuses underwent a sham surgery. LGE CMR was performed in a subset of fetuses immediately after the surgery and three days later. Early gadolinium enhancement (EGE) CMR was also performed in a subset of fetuses on both days. Cine imaging of the heart was performed to measure ventricular function.ResultsThe imaging performed immediately after LAD ligation revealed no evidence of infarct on LGE (n=3). Two of four infarcted fetuses (50%) showed hypoenhancement at the infarct site on the EGE images. Three days after the ligation, LGE images revealed a clear, hyper-enhanced infarct zone in four of the five infarcted fetuses (80%). No hyper-enhanced infarct zone was seen on the one sham fetus that underwent LGE CMR. No hypoenhancement could be seen in the EGE images in either the sham (n=1) or the infarcted fetus (n=1). No regional wall motion abnormalities were apparent in two of the five infarcted fetuses.ConclusionLGE CMR detected the MI three days after LAD ligation, but not immediately after. Using available methods, EGE imaging was less useful for detecting deficits in perfusion. Our study provides evidence for the ability of a non-invasive tool to monitor the progression of cardiac repair and damage in fetuses with MI. However, further investigation into the optimal timing of LGE and EGE scans and improvement of the sequences should be pursued with the aim of expanding our capacity to monitor cardiac regeneration after MI in fetal sheep.Electronic supplementary materialThe online version of this article (10.1186/s12968-017-0383-1) contains supplementary material, which is available to authorized users.

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“…Recent studies support the notion that tissue injury and the regenerative response are associated with the activation of embryonic/fetal gene regulatory pathways during regeneration [ 33 , 34 ]. Regeneration is marked by distinct stages of architectural restoration including: wound healing, blastema formation, cellular proliferation and differentiation ( Figure 1 B) [ 11 , 19 , 35 , 36 , 37 , 38 ].…”

Section: Introductionmentioning

confidence: 86%

Hedgehog Signaling during Appendage Development and Regeneration

Singh

Koyano-Nakagawa

Donaldson

et al. 2015

Genes

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Regulatory networks that govern embryonic development have been well defined. While a common hypothesis supports the notion that the embryonic regulatory cascades are reexpressed following injury and tissue regeneration, the mechanistic regulatory pathways that mediate the regenerative response in higher organisms remain undefined. Relative to mammals, lower vertebrates, including zebrafish and newts, have a tremendous regenerative capacity to repair and regenerate a number of organs including: appendages, retina, heart, jaw and nervous system. Elucidation of the pathways that govern regeneration in these lower organisms may provide cues that will enhance the capacity for the regeneration of mammalian organs. Signaling pathways, such as the hedgehog pathway, have been shown to play critical functions during development and during regeneration in lower organisms. These signaling pathways have been shown to modulate multiple processes including cellular origin, positional identity and cellular maturation. The present review will focus on the cellular and molecular regulation of the hedgehog (HH) signaling pathway and its interaction with other signaling factors during appendage development and regeneration.

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Mammalian Fetal Cardiac Regeneration After Myocardial Infarction Is Associated With Differential Gene Expression Compared With the Adult

Cited by 22 publications

References 21 publications

Label‐free imaging of healthy and infarcted fetal sheep hearts by two‐photon microscopy

Label‐free imaging of healthy and infarcted fetal sheep hearts by two‐photon microscopy

Feasibility of detecting myocardial infarction in the sheep fetus using late gadolinium enhancement CMR imaging

Hedgehog Signaling during Appendage Development and Regeneration

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