Small Artery Remodeling Depends on Tissue-Type Transglutaminase

Bakker, Erik N. T. P.; Buus, C. L.; Spaan, Jos A. E.; Perree, Jop; Ganga, A; Rolf, T. M.; Sorop, Oana; Bramsen, Linda H.; Mulvany, Michael J.; VanBavel, Ed

doi:10.1161/01.res.0000151333.56089.66

Cited by 163 publications

(195 citation statements)

References 37 publications

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“…Inhibitors of TG2 block inward remodeling that was induced by endothelin-1. Enhanced expression of endogenous TG2 or the application of exogenous TG2 increases inward remodeling in several animal models (94). In a porcine model of renal artery stenosis, simvastatin inhibited the inward remodeling of the intrarenal microvasculature, partly by decreasing the upregulation of TG2 expression in the ischemic kidney (95).…”

Section: Transglutaminases and Arterial Remodelingmentioning

confidence: 99%

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Roles of transglutaminases in cardiac and vascular diseases

Sane

Kontos²,

Greenberg³

2007

Front Biosci

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All transglutaminases share the common enzymatic activity of transamidation, or the cross-linking of glutamine and lysine residues to form N epsilon (gamma-glutamyl) lysyl isopeptide bonds. The plasma proenzyme factor XIII is responsible for stabilizing the fibrin clot against physical and fibrinolytic disruption. Another member of the transglutaminase family, tissue transglutaminase or TG2 is abundantly expressed in cardiomyocytes, vascular cells and macrophages. The transglutaminases have a variety of functions independent of their transamidating activity. For example, TG2 binds and hydrolyzes GTP, thereby fostering signal transduction by several G protein coupled receptors. Accumulating evidence points to novel roles for factor XIII and TG2 in cardiovascular biology including: (a) modulating platelet activity, (b) regulating glucose control, (c) contributing to the development of hypertension, (d) influencing the progression of atherosclerosis, (e) regulating vascular permeability and angiogenesis (f) and contributing to myocardial signaling, contractile activity and ischemia/reperfusion injury. In this review, we summarize the cardiovascular biology of two members of the family of transglutaminases, Factor XIII and TG2.

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Section: Transglutaminases and Arterial Remodelingmentioning

confidence: 99%

“…Interestingly, the activity of TG2 appears to be regulated, in part, by the application of pressure to the arterial wall (94). Both TG2 and FXIII transglutaminase activities are also regulated by nitric oxide.…”

Section: Transglutaminases and Arterial Remodelingmentioning

confidence: 99%

Roles of transglutaminases in cardiac and vascular diseases

Sane

Kontos²,

Greenberg³

2007

Front Biosci

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“…20,22,23,32,33,37 In addition to being a model that mimics the remodeling that occurs in hypoperfused tissues, LF remodeling has been shown to be equivalent to the eutrophic inward remodeling observed in several types of hypertension, such as endothelin-1-dependent hypertension and L-NAME-induced hypertension. 10 The main finding of this study is that the diameter reduction because of a decrease in blood flow in RAs was prevented by perindopril and candesartan, but not by hydralazine, suggesting selective involvement of angiotensin II and of its AT1R. The AT2R was not involved in this remodeling (see Supplementary information).…”

Section: Discussionmentioning

confidence: 61%

“…This contraction is then stabilized by the activation of tissuetransglutaminases. 10 Using mice lacking tissue angiotensin I-converting enzyme, Hilgers et al 11 showed that this enzyme has a major role in hyperplasic inward remodeling of the carotid artery after blood flow cessation. In mesenteric RAs, we have previously shown that acute stimulation of the endothelium by flow (shear stress) induces vasodilation, which is modulated by the local production of angiotensin II.…”

Section: Introductionmentioning

confidence: 99%

Involvement of angiotensin II in the remodeling induced by a chronic decrease in blood flow in rat mesenteric resistance arteries

et al. 2010

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Blood flow reduction induces inward remodeling of resistance arteries (RAs). This remodeling occurs in ischemic diseases, diabetes and hypertension. Nonetheless, the effect of flow reduction per se, independent of the effect of pressure or metabolic influences, is not well understood in RA. As angiotensin II is involved in the response to flow in RA, we hypothesized that angiotensin II may also be involved in the remodeling induced by a chronic flow reduction. We analyzed the effect of angiotensin I-converting enzyme inhibition (perindopril) and angiotensin II type 1 receptor blockade (candesartan) on inward remodeling induced by blood flow reduction in vivo in rat mesenteric RAs (low flow (LF) arteries). After 1 week, diameter reduction in LF arteries was associated with reduced endothelium-dependent relaxation and lower levels of eNOS expression. Superoxide production and extracellular signal-regulated kinases 1/2 (ERK1/2 phosphorylation were higher in LF than in normal flow arteries. Nevertheless, the absence of eNOS or superoxide level reduction (tempol or apocynin) did not prevent LF remodeling. Perindopril and candesartan prevented inward remodeling in LF arteries. Contractility to angiotensin II was reduced in LF vessels by perindopril, candesartan and the ERK1/2 blocker PD98059. ERK1/2 activation (ratio phospho-ERK/ERK) was higher in LF arteries, and this activation was prevented by perindopril and candesartan. ERK1/2 inhibition in vivo (U0126) prevented LF-induced diameter reduction. Thus, inward remodeling because of blood flow reduction in mesenteric RA depends on unopposed angiotensin II-induced contraction and ERK1/2 activation, independent of superoxide production. These findings might be of importance in the treatment of vascular disorders.

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“…Understanding the mechanisms which may modulate resistance arterial eutrophic remodelling is thus important, but these remain poorly understood. Prolonged vasoconstriction appears important, which, in itself may modulate re-organisation via the activities of cross-linking enzymes such as tissue-type transglutaminase and/ or integrins (Bakker et al, 2002(Bakker et al, , 2005Heerkens et al, 2006). It has been proposed that initial eutrophic remodelling may be an energetically favourable adaptive mechanism to normalise wall stress to maintain adequate blood flow, whilst a growth response, which may be observed in advanced or secondary hypertension, is related to a greater adverse prognosis (Izzard et al, 2006;Heagerty et al, 2010).…”

Section: Resistance Artery Structure and Hypertensionmentioning

confidence: 99%

Plasma membrane calcium ATPases (PMCAs) as potential targets for the treatment of essential hypertension

Little

Cartwright

Neyses

et al. 2016

Pharmacology & Therapeutics

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The incidence of hypertension, the major modifiable risk factor for cardiovascular disease, is increasing. Thus, there is a pressing need for the development of new and more effective strategies to prevent and treat hypertension. Development of these relies on a continued evolution of our understanding of the mechanisms which control blood pressure (BP). Resistance arteries are important in the regulation of total peripheral resistance and BP; changes in their structure and function are strongly associated with hypertension. Anti-hypertensives which both reduce BP and reverse changes in resistance arterial structure reduce cardiovascular risk more than therapies which reduce BP alone. Hence, identification of novel potential vascular targets which modify BP is important. Hypertension is a multifactorial disorder which may include a genetic component. Genome wide association studies have identified ATP2B1, encoding the calcium pump plasma membrane calcium ATPase 1 (PMCA1), as having a strong association with BP and hypertension. Knockdown or reduced PMCA1 expression in mice has confirmed a physiological role for PMCA1 in BP and resistance arterial regulation. Altered expression or inhibition of PMCA4 has also been shown to modulate these parameters. The mechanisms whereby PMCA1 and 4 can modulate vascular function remain to be fully elucidated but may involve regulation of intracellular calcium homeostasis and/or comprise a structural role. However, clear physiological links between PMCA and BP, coupled with experimental studies directly linking PMCA1 and 4 to changes in BP and arterial function, suggest that they may be important targets for the development of new pharmacological modulators of BP.

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Small Artery Remodeling Depends on Tissue-Type Transglutaminase

Cited by 163 publications

References 37 publications

Roles of transglutaminases in cardiac and vascular diseases

Roles of transglutaminases in cardiac and vascular diseases

Involvement of angiotensin II in the remodeling induced by a chronic decrease in blood flow in rat mesenteric resistance arteries

Plasma membrane calcium ATPases (PMCAs) as potential targets for the treatment of essential hypertension

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