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Query: UMLS:C0151744 (
myocardial ischemia
)
31,282
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
We present in this article main theories of development of atherosclerosis and modern views of the role of inflammation in atherogenesis. We have conducted a review of studies of the role of endothelial local factors such as accumulation of smooth muscle cells, T and B lymphocytes, macrophages, matrix metalloproteinase (MMP), high sensitivity C reactive protein (CRP). It has been shown that low oxidative stress modulates expression of endothelial gene which induces atherogenic factor formatting early atherosclerotic plaque (FP). CRP and oxidized low density lipoproteins (OxLDL) are directly linked with oxidative damage of arteries in
ischemic heart disease
. Monocytes activated in areas of inflammation by monocyte chemoattractant protein (MCP) 1 and MMP 1 play pivotal role in AP rupture. CRP and OxLDL augment synthesis of MMP, tumor necrosis factor alpha (TNF alpha) and granulocyte macrophage colony stimulating factor (GM
CSF
). Moreover addition of exogenous MCP 1 and prostaglandin E2 elevates synthesis of MMP 1, TNF alpha, and GM
CSF
by monocytes. Apoptosis of smooth muscle cells of AP fibrous cap combined with destruction of extracellular matrix proteins by MMP 1 eventually leads to AP rupture.
...
PMID:[Contemporary concepts of the role of inflammation in atherosclerosis]. 2065 35
Cell based therapy for
ischemic heart disease
has the potential to reduce post infarct heart failure and chronic ischemia. Treatment with granulocyte-colony stimulating factor (G-CSF) mobilizes cells from the bone marrow to the peripheral blood. Some of these cells are putative stem or progenitor cells. G-
CSF
is injected subcutaneously. This therapy is intuitively attractive compared to other cell based techniques since repeated catheterizations and ex vivo cell purification and expansion are avoided. Previous preclinical and early clinical trials have indicated that treatment with G-
CSF
leads to improved myocardial perfusion and function in acute or chronic ischemic heart disease. The hypothesis of this thesis is that patient with
ischemic heart disease
will benefit from G-
CSF
therapy. We examined this hypothesis in two clinical trials with G-
CSF
treatment to patients with either acute myocardial infarction or severe chronic ischemic heart disease. In addition, we assed a number of factors that could potentially affect the effect of cell based therapy. Finally, we intended to develop a method for in vivo cell tracking in the heart. Our research showed that subcutaneous G-
CSF
along with gene therapy do not improve myocardial function in patients with chronic ischemia despite a large increase in circulation bone marrow-derived cells. Also, neither angina pectoris nor exercise capacity was improved compared to placebo treatment. We could not identify differences in angiogenic factors or bone marrow-derived cells in the blood that could explain the neutral effect of G-
CSF
. Next, we examined G-
CSF
as adjunctive therapy following ST segment elevation myocardial infarction. We did not find any effect of G-
CSF
neither on the primary endpoint--regional myocardial function--nor on left ventricular ejection fraction (secondary endpoint) compared to placebo treatment. In subsequent analyses, we found significant differences in the types of cells mobilized from the bone marrow by G-
CSF
. This could explain why intracoronary injections of unfractionated bone marrow-derived cells have more effect that mobilization with G-
CSF
. A number of other factors could explain the neutral effect of G-
CSF
in our trial compared to previous studies. These factors include timing of the treatment, G-
CSF
dose, and study population. It is however, remarkable that the changes in our G-
CSF
group are comparable to the results of previous non-blinded studies, whereas the major differences are in the control/placebo groups. We found that ejection fraction, wall motion, edema, perfusion, and infarct size all improve significantly in the first month following ST-segment myocardial infarction with standard guideline treatment (including acute mechanical revascularization), but without cell therapy. This is an important factor to take into account when assessing the results of non-controlled trials. Finally, we found that ex vivo labeling of cells with indium-111 for in vivo cell tracking after intramyocardial injection is problematic. In our hand, a significant amount of indium-111 remained in the myocardium despite cell death. It is difficult to determine viability of the cells after injection in human trials, and it is thus complicated to determine if the activity in the myocardium tracks viable cells. Cell based therapy is still in the explorative phase, but based on the intense research within this field it is our hope that the clinical relevance of the therapy can be determined in the foreseeable future. Ultimately, this will require large randomized, double-blind and placebo-controlled trials with "hard" clinical endpoints like mortality and morbidity.
...
PMID:Granulocyte-colony stimulating factor therapy to induce neovascularization in ischemic heart disease. 2238 Oct 94
Myocardial infarction (MI) elicits massive inflammatory leukocyte recruitment to the heart. Here, we hypothesized that excessive leukocyte invasion leads to heart failure and death during acute
myocardial ischemia
. We found that shortly and transiently after onset of ischemia, human and mouse cardiac fibroblasts produce granulocyte/macrophage colony-stimulating factor (GM-CSF) that acts locally and distally to generate and recruit inflammatory and proteolytic cells. In the heart, fibroblast-derived GM-
CSF
alerts its neighboring myeloid cells to attract neutrophils and monocytes. The growth factor also reaches the bone marrow, where it stimulates a distinct myeloid-biased progenitor subset. Consequently, hearts of mice deficient in either GM-
CSF
or its receptor recruit fewer leukocytes and function relatively well, whereas mice producing GM-
CSF
can succumb from left ventricular rupture, a complication mitigated by anti-GM-
CSF
therapy. These results identify GM-
CSF
as both a key contributor to the pathogenesis of MI and a potential therapeutic target, bolstering the idea that GM-
CSF
is a major orchestrator of the leukocyte supply chain during inflammation.
...
PMID:The infarcted myocardium solicits GM-CSF for the detrimental oversupply of inflammatory leukocytes. 2897 34
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