Bone Marrow Characteristics Associated With Changes in Infarct Size After STEMI

Schutt, Robert C.; Trachtenberg, Barry; Cooke, John P.; Traverse, Jay H.; Henry, Timothy D.; Pepine, Carl J.; Willerson, James T.; Perin, Emerson C.; Ellis, Stephen G.; Zhao, David; Bhatnagar, Aruni; Johnstone, Brian H.; Lai, Dejian; Resende, Micheline; Ebert, Ray F.; Wu, Joseph C.; Sayre, Shelly L.; Orozco, Aaron; Zierold, Claudia; Simari, Robert D.; Moyé, Lem; Cogle, Christopher R.

doi:10.1161/circresaha.116.304710

Cited by 60 publications

(37 citation statements)

References 45 publications

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“…Regenerative therapies through exogenous stem cell administration hold promising potential [1, 2, 4, 22, 25, 31], but may be limited by excessive cell death after transplantation into an oxidative environment [17]. Since mitochondria are a major source of reactive oxygen species (ROS) in the cell, reductions in mitochondrial metabolism may reduce both the oxidative burden and cell death under oxidative stress.…”

Section: Introductionmentioning

confidence: 99%

Novel thiazolidinedione mitoNEET ligand-1 acutely improves cardiac stem cell survival under oxidative stress

et al. 2015

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Ischemic heart disease (IHD) is a leading cause of death worldwide, and regenerative therapies through exogenous stem cell delivery hold promising potential. One limitation of such therapies is the vulnerability of stem cells to the oxidative environment associated with IHD. Accordingly, manipulation of stem cell mitochondrial metabolism may be an effective strategy to improve survival of stem cells under oxidative stress. MitoNEET is a redox-sensitive, mitochondrial target of thiazolidinediones (TZDs), and influences cellular oxidative capacity. Pharmacological targeting of mitoNEET with the novel TZD, mitoNEET Ligand-1 (NL-1), improved cardiac stem cell (CSC) survival compared to vehicle (0.1 % DMSO) during in vitro oxidative stress (H2O2). 10 μM NL-1 also reduced CSC maximal oxygen consumption rate (OCR) compared to vehicle. Following treatment with dexamethasone, CSC maximal OCR increased compared to baseline, but NL-1 prevented this effect. Smooth muscle α-actin expression increased significantly in CSC following differentiation compared to baseline, irrespective of NL-1 treatment. When CSCs were treated with glucose oxidase for 7 days, NL-1 significantly improved cell survival compared to vehicle (trypan blue exclusion). NL-1 treatment of cells isolated from mitoNEET knockout mice did not increase CSC survival with H2O2 treatment. Following intramyocardial injection of CSCs into Zucker obese fatty rats, NL-1 significantly improved CSC survival after 24 h, but not after 10 days. These data suggest that pharmacological targeting of mitoNEET with TZDs may acutely protect stem cells following transplantation into an oxidative environment. Continued treatment or manipulation of mitochondrial metabolism may be necessary to produce long-term benefits related to stem cell therapies.

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Section: Introductionmentioning

confidence: 99%

Novel thiazolidinedione mitoNEET ligand-1 acutely improves cardiac stem cell survival under oxidative stress

et al. 2015

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“…10,11 It is noteworthy that BM and circulating endothelial cells and monocytes expressing high levels of CD31 have been shown to have proangiogenic and vasculogenic activities 12,13 ; however, in the study by Shutt et al, 1 BM CD31 + cells that exhibit a positive correlation with the decrease in infarct size are lymphocytes (ie, CD45 + CD31 low ). Given that T cells are the major lymphocyte subset in BMC, and that CD31 + T lymphocytes decrease while CD31 -increase during life, 14 the results by Shutt et al 1 of diminished myocardial healing in individuals with low frequency of CD31 + lymphocytes among BMC strengthen the hypothesis that aging of the immune system plays an important role in the lack of myocardial regeneration.…”

Section: Article See P 99mentioning

confidence: 99%

“…8 Despite these previous studies on circulating BMC in acute MI, a detailed evaluation of resident BMC in humans with MI was missing. The work by Shutt et al 1 analyzes the cells in the BM of patients with acute MI for their ability to give rise to endothelial, mesenchymal, and proangiogenic cell colonies, assessed in vitro by endothelial colony-forming cells, colonyforming units (CFU)-fibroblasts, and CFU-Hill assays as surrogate markers of the healing potential of regenerative cells. Furthermore, the authors evaluate BMC composition by the use of multiparametric flow cytometry.…”

Section: Article See P 99mentioning

confidence: 99%

“…I n this issue of Circulation Research, Shutt et al 1 explore the characteristics of resident bone marrow cells (BMC) in patients enrolled in the Timing In Myocardial infarction Evaluation (TIME) clinical trial, in search of cellular correlates of reduction of the infarcted area 6 months after acute myocardial infarction (MI). The central hypothesis is that endogenous BM properties could affect the clinical outcome.…”

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confidence: 99%

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Bone Good to the Heart

Picozza

Pompilio

Capogrossi

2015

Circulation Research

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Editorial In this issue of Circulation Research, Shutt et al 1 explore the characteristics of resident bone marrow cells (BMC) in patients enrolled in the Timing In Myocardial infarction Evaluation (TIME) clinical trial, in search of cellular correlates of reduction of the infarcted area 6 months after acute myocardial infarction (MI). The central hypothesis is that endogenous BM properties could affect the clinical outcome. They found both phenotypic and biological BMC correlates of infarct size reduction, and the emerging picture is quite interesting. Article, see p 99Why should subset composition and functional status of BMC affect recovery after acute MI? One explanation relates to the fact that specific populations of BMC have been shown to mobilize from the BM into the peripheral blood (PB) after MI and to have prognostic and therapeutic values. The first clue of a cross talk between the human ischemic heart and the BM came more than a decade ago with the work of Shintani et al, 2 which reported a peak in BM-derived, circulating CD34 + cells 7 days after MI, a trend that correlated with the rise in the number of putative endothelial cell clusters under in vitro angiogenic conditions (ie, in medium supplemented with endothelial cell growth factors). Mobilization of precursor cells after MI was confirmed by subsequent studies: Wojakowski et al 3 showed that, immediately after admission, blood mononuclear cells of patients with ST-segment-elevation myocardial infarction are enriched in transcripts for early myocardial, muscle, and endothelial markers; Leone et al 4 properly. Subsequently, enhanced mobilization of CD34 + hematopoietic stem cell cells in MI was confirmed, and these cells were shown to express the receptor for stromal-derived factor-1, CXCR4, and the adhesion molecule very late antigen-4; expression of these proteins, without being unique, is characteristic of hematopoietic stem cells and probably instrumental in the recruitment of these regenerative populations into the infarcted myocardium.7 Of note, the blockade of both stromal-derived factor-1/CXCR4 axes and very late antigen-4 through the chemical reversible inhibitor AMD3100 and the humanized monoclonal antibody Natalizumab, respectively, results in enhanced mobilization of CD34 + cells from the BM. Furthermore, enhanced levels of circulating CD34 + CXCR4 + precursor cells, accompanied by increased levels of plasmatic G-CSF but reduced stromal-derived factor-1, was recently found to correlate with recovery of left ventricular ejection fraction in patients with MI. 8Despite these previous studies on circulating BMC in acute MI, a detailed evaluation of resident BMC in humans with MI was missing. The work by Shutt et al 1 analyzes the cells in the BM of patients with acute MI for their ability to give rise to endothelial, mesenchymal, and proangiogenic cell colonies, assessed in vitro by endothelial colony-forming cells, colonyforming units (CFU)-fibroblasts, and CFU-Hill assays as surrogate markers of the healing potential of regenerative ...

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“…2 There is a growing interest in the BM status in patients with cardiovascular disease or risk factors. 11,12 For instance, acute myocardial infarction induces BM metabolic activation, 13 and failure of the BM to mobilize CD34 + cells post-acute myocardial infarction is associated with a poor outcome. 14 In diabetes mellitus, especially with vascular disease, the BM undergoes extensive remodeling and stem cell mobilization is impaired.…”

Section: Cd34 + Cells Predict Mortality 233mentioning

confidence: 99%

A Look at the Bone Marrow Predicts the Global Outcome

Fadini

2015

Circulation Research

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Bone Marrow Characteristics Associated With Changes in Infarct Size After STEMI

Cited by 60 publications

References 45 publications

Novel thiazolidinedione mitoNEET ligand-1 acutely improves cardiac stem cell survival under oxidative stress

Novel thiazolidinedione mitoNEET ligand-1 acutely improves cardiac stem cell survival under oxidative stress

Bone Good to the Heart

A Look at the Bone Marrow Predicts the Global Outcome

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