Transglutaminase 2 Accelerates Vascular Calcification in Chronic Kidney Disease

Chen, Neal X.; O’Neill, Kalisha D.; Chen, Xianming; Kiattisunthorn, Kraiwiporn; Gattone, Vincent H.; Moe, Sharon M.

doi:10.1159/000347031

Cited by 38 publications

(35 citation statements)

References 55 publications

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“…Although the methods of activation and inhibition of transglutaminase used in our experiments have been used extensively in the past (1, 10, 17, 31, 37-39), a limitation of our study rests on the potential nonspecific effects of DTT and cystamine. Nonetheless, our results are consistent with an increasing body of evidence that indicates intracellular transglutaminase activation participates in vascular pathology (6,7,23,30). A better understanding of the pathways associated with transglutaminase-dependent cytoskeletal changes should provide new therapeutic avenues for controlling vascular remodeling and the adverse cardiovascular events associated with it.…”

Section: Discussionsupporting

confidence: 90%

The obligatory role of the actin cytoskeleton on inward remodeling induced by dithiothreitol activation of endogenous transglutaminase in isolated arterioles

Castorena‐Gonzalez

Staiculescu

Foote

et al. 2014

American Journal of Physiology-Heart and Circulatory Physiology

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The obligatory role of the actin cytoskeleton on inward remodeling induced by dithiothreitol activation of endogenous transglutaminase in isolated arterioles. Am J Physiol Heart Circ Physiol 306: H485-H495, 2014. First published December 13, 2013 doi:10.1152/ajpheart.00557.2013.-Inward remodeling is the most prevalent structural change found in the resistance arteries and arterioles of hypertensive individuals. Separate studies have shown that the inward remodeling process requires transglutaminase activation and the polymerization of actin. Therefore, we hypothesize that inward remodeling induced via endogenous transglutaminase activation requires and depends on actin cytoskeletal structures. To test this hypothesis, isolated and cannulated rat cremaster arterioles were exposed to dithiothreitol (DTT) to activate endogenous transglutaminases. DTT induced concentration-dependent vasoconstriction that was suppressed by coincubation with cystamine or cytochalasin-D to inhibit tranglutaminase activity or actin polymerization, respectively. Prolonged (4 h) exposure to DTT caused arteriolar inward remodeling that was also blocked by the presence of cystamine or cytochalasin-D. DTT inwardly remodeled arterioles had reduced passive diameters, augmented wall thickness-to-lumen ratios and altered elastic characteristics that were reverted upon disruption of the actin cytoskeleton with mycalolide-B. In freshly isolated arterioles, exposure to mycalolide-B caused no changes in their passive diameters or their elastic characteristics. These results suggest that, in arterioles, the early stages of the inward remodeling process induced by prolonged endogenous transglutaminase activation require actin dynamics and depend on changes in actin cytoskeletal structures.hypertension; vasoconstriction; stiffness; elasticity; passive diameter INWARD REMODELING OF ARTERIOLES is the most prevalent structural change of the resistance vasculature observed in patients with hypertension and diabetes (14, 28). Its presence is associated with an increased risk for life-threatening cardiovascular events including stroke and myocardial infarction (22,27). However, despite its clinical importance, the mechanism(s) responsible for its development have not been completely elucidated.Cumulative evidence indicates that prolonged exposure to vasoconstrictor agonists causes inward remodeling of arterioles. Ex vivo, prolonged vasoconstriction induced by exposure of isolated arterioles to endothelin-1, angiotensin II, norepinephrine, or serum causes inward remodeling (4,5,19). In vivo, vasoconstriction also appears to be the primary stimulus causing inward remodeling in hypertension, as vasodilation and not a mere reduction in blood pressure is needed to prevent or revert inward remodeling in hypertensive individuals (8,21). The mechanism(s) responsible for inducing remodeling during prolonged vasoconstriction, however, remain elusive.A series of recent studies indicates that inward remodeling of arterioles requires transglutaminase activity. In 2005 B...

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Section: Discussionsupporting

confidence: 90%

The obligatory role of the actin cytoskeleton on inward remodeling induced by dithiothreitol activation of endogenous transglutaminase in isolated arterioles

Castorena‐Gonzalez

Staiculescu

Foote

et al. 2014

American Journal of Physiology-Heart and Circulatory Physiology

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“…This observation is consistent with many other demonstrations in the literature showing that the in vivo effects of inhibitors are often less intense than those observed in vitro. 32 Taken as a whole, these results suggest that the decrease of VSMC and aortic ring calcification induced by DP8 is mainly related to the inhibition of osteogenic marker expression.…”

Section: Discussionmentioning

confidence: 73%

Oligogalacturonic Acid Inhibits Vascular Calcification by Two Mechanisms

Hodroge

Trecherel

Cornu

et al. 2017

ATVB

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Objective— Cardiovascular diseases constitute the leading cause of mortality worldwide. Calcification of the vessel wall is associated with cardiovascular morbidity and mortality in patients having many diseases, including diabetes mellitus, atherosclerosis, and chronic kidney disease. Vascular calcification is actively regulated by inductive and inhibitory mechanisms (including vascular smooth muscle cell adaptation) and results from an active osteogenic process. During the calcification process, extracellular vesicles (also known as matrix vesicles) released by vascular smooth muscle cells interact with type I collagen and then act as nucleating foci for calcium crystallization. Our primary objective was to identify new, natural molecules that inhibit the vascular calcification process. Approach and Results— We have found that oligogalacturonic acids (obtained by the acid hydrolysis of polygalacturonic acid) reduce in vitro inorganic phosphate–induced calcification of vascular smooth muscle cells by 80% and inorganic phosphate–induced calcification of isolated rat aortic rings by 50%. A specific oligogalacturonic acid with a degree of polymerization of 8 (DP8) was found to inhibit the expression of osteogenic markers and, thus, prevent the conversion of vascular smooth muscle cells into osteoblast-like cells. We also evidenced in biochemical and immunofluorescence assays a direct interaction between matrix vesicles and type I collagen via the GFOGER sequence (where single letter amino acid nomenclature is used, O=hydroxyproline) thought to be involved in interactions with several pairs of integrins. Conclusions— DP8 inhibits vascular calcification development mainly by inhibition of osteogenic marker expression but also partly by masking the GFOGER sequence—thereby, preventing matrix vesicles from binding to type I collagen.

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“…In a recent study based on a novel rat model of progressive CKD-MBD (Cy/+ rat) displaying arterial calcification on a normal phosphorus diet (Moe et al 2009), increased TG2 expression and activity was detected in Cy/+ rat-vascular smooth muscle cells and in pathological matrix vesicles ex vivo. Furthermore, the general TG inhibitor cystamine slowed down calcification in cells, matrix vesicles and aorta rings from the CKD rats (Chen et al 2013).…”

Section: Tg Expression and Activity In Experimental Kidney Fibrosismentioning

confidence: 91%

“…From all these investigations in experimental models of fibrosis (summarized in Table 11.1), it has become clear that TG2 serves as a crosslinker predominantly in Table 11.1 Studies of transglutaminase in CKD Experimental models Subtotal nephrectomy (SNx) in rat Johnson et al (1997Johnson et al ( , 1999Johnson et al ( , 2007 and Burhan et al (2011) Unilateral ureteric obstruction (UUO) in rat Chen et al (2005) Unilateral ureteric obstruction (UUO) in mouse Chen et al (2013) the interstitial space, and its action site is both tubular and glomerular with variations depending on the type of kidney damage.…”

Section: Tg Expression and Activity In Experimental Kidney Fibrosismentioning

confidence: 99%