Metallothionein Enhances Angiogenesis and Arteriogenesis by Modulating Smooth Muscle Cell and Macrophage Function

Zbinden, Stephan; Wang, Jinsong; Adenika, Remi; Schmidt, Marcel; Tilan, Justin; Najafi, Amir H.; Peng, XinZhi; Lassance‐Soares, Roberta M.; Iantorno, Micaela; Morsli, Hakim; Gercenshtein, Leonid; Jang, Gwang Cheon; Epstein, Stephen E.; Burnett, Mary Susan

doi:10.1161/atvbaha.109.200949

Cited by 38 publications

(35 citation statements)

References 39 publications

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“…As a result, effective angiogenesis in vivo following MT-I knockdown is hampered. This was confirmed by Zbinden et al [9], who found decreased vessel density and less EC migration in matrigel plugs implanted in MTI/II knockout mice as compared to wild-type animals. …”

Section: Introductionsupporting

confidence: 63%

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Expression, Regulation and Function of Human Metallothioneins in Endothelial Cells

et al. 2014

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Metallothioneins (MTs) are small cysteine-rich proteins which are involved in e.g. metal homeostasis, metal detoxification and protection against oxidative stress. In addition, several MTs have been shown to regulate expression of proangiogenic growth factors like vascular endothelial growth factor. Detailed information about the expression and regulation of specific MT isoforms in endothelial cells (EC) is limited. We therefore performed extensive mRNA expression profiling of all known human MTs in EC. We found that the basal endothelial expression is restricted to MT1E, MT1X, MT2A, and MT3. Physiological activation of EC by exposure to serum increased the expression of MT1E and MT2A and induced the expression of MT1M. Furthermore, exposure to zinc or copper induced the expression of most MT1 isoforms, while hypoxia specifically increased the expression of MT1E, MT1M, MT1X, and MT3. Finally, knockdown of the dominant MT isoform in EC, i.e. MT2A, resulted in decreased proliferation and sprouting as well as in increased migration of human umbilical vein EC. Together, these findings provide a link between MTs and angiogenesis.

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Section: Introductionsupporting

confidence: 63%

“…At the same time, MTs have been shown to be involved in neovessel formation, i.e. angiogenesis, both in vitro and in vivo [8,9]. By inducing angiogenesis, MTs could provide a possible feedback mechanism to counteract oxidative stress.…”

Section: Introductionmentioning

confidence: 99%

Expression, Regulation and Function of Human Metallothioneins in Endothelial Cells

et al. 2014

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“…Genome-wide transcriptome analysis of satellite cells overexpressing Bmi1 revealed significantly increased expression of MT1, which has been shown to be necessary to maintain proliferation and normal cellular functions under stress conditions, including when cells reenter the cell cycle from a quiescent state (Zbinden et al, 2010). In keeping with this notion, improvement of muscle strength is seen only in those mdx mice in which up-regulation of MT1 occurred concomitantly with overexpression of Bmi1 in satellite cells.…”

Section: Bmi1 Expression Is Reduced In Patients Affected By Dmdmentioning

confidence: 86%

Bmi1 enhances skeletal muscle regeneration through MT1-mediated oxidative stress protection in a mouse model of dystrophinopathy

Foggia¹,

Zhang²,

Licastro³

et al. 2014

J Cell Biol

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The Polycomb group (PcG) protein Bmi1 is an essential epigenetic regulator of stem cell function during normal development and in adult organ systems. We show that mild upregulation of Bmi1 expression in the adult stem cells of the skeletal muscle leads to a remarkable improvement of muscle function in a mouse model of Duchenne muscular dystrophy. The molecular mechanism underlying enhanced physiological function of Bmi1 depends on the injury context and it is mediated by metallothionein 1 (MT1)-driven modulation of resistance to oxidative stress in the satellite cell population. These results lay the basis for developing Bmi1 pharmacological activators, which either alone or in combination with MT1 agonists could be a powerful novel therapeutic approach to improve regeneration in muscle wasting conditions.

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“…Indeed, there was a Ͼ600-fold increase in MT3 mRNA level, although such an apparently large response reflects, to some extent, the fact that expression is minimal in adipocytes incubated under normoxic conditions (208). The metallothioneins are low molecular weight (ϳ6,000 M r ) cysteine-rich, metal-binding proteins, with several presumed functions which include angiogenesis and antioxidant defense (129,150,230). A proangiogenic role in adipose tissue would be consistent with the major induction of MT3 expression by hypoxia.…”

Section: Hypoxia and Global Gene Expressionmentioning

confidence: 99%

Hypoxia and Adipose Tissue Function and Dysfunction in Obesity

Trayhurn

2013

Physiological Reviews

707

539

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The rise in the incidence of obesity has led to a major interest in the biology of white adipose tissue. The tissue is a major endocrine and signaling organ, with adipocytes, the characteristic cell type, secreting a multiplicity of protein factors, the adipokines. Increases in the secretion of a number of adipokines occur in obesity, underpinning inflammation in white adipose tissue and the development of obesity-associated diseases. There is substantial evidence, particularly from animal studies, that hypoxia develops in adipose tissue as the tissue mass expands, and the reduction in Po2is considered to underlie the inflammatory response. Exposure of white adipocytes to hypoxic conditions in culture induces changes in the expression of >1,000 genes. The secretion of a number of inflammation-related adipokines is upregulated by hypoxia, and there is a switch from oxidative metabolism to anaerobic glycolysis. Glucose utilization is increased in hypoxic adipocytes with corresponding increases in lactate production. Importantly, hypoxia induces insulin resistance in fat cells and leads to the development of adipose tissue fibrosis. Many of the responses of adipocytes to hypoxia are initiated at Po2levels above the normal physiological range for adipose tissue. The other cell types within the tissue also respond to hypoxia, with the differentiation of preadipocytes to adipocytes being inhibited and preadipocytes being transformed into leptin-secreting cells. Overall, hypoxia has pervasive effects on the function of adipocytes and appears to be a key factor in adipose tissue dysfunction in obesity.

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Metallothionein Enhances Angiogenesis and Arteriogenesis by Modulating Smooth Muscle Cell and Macrophage Function

Cited by 38 publications

References 39 publications

Expression, Regulation and Function of Human Metallothioneins in Endothelial Cells

Expression, Regulation and Function of Human Metallothioneins in Endothelial Cells

Bmi1 enhances skeletal muscle regeneration through MT1-mediated oxidative stress protection in a mouse model of dystrophinopathy

Hypoxia and Adipose Tissue Function and Dysfunction in Obesity

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