CD73-TNAP crosstalk regulates the hypertrophic response and cardiomyocyte calcification due to α1 adrenoceptor activation

Gan, Xiaohong Tracey; Taniai, Seiichi; Zhao, Gan-Jian; Huang, Cathy; Velenosi, Thomas J.; Xue, Jenny Y.; Urquhart, Bradley L.; Karmazyn, Morris

doi:10.1007/s11010-014-2100-9

Cited by 25 publications

(19 citation statements)

References 31 publications

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“…Here we analysed two different models of fibrosis: rapid-onset cardiac fibrosis induced by the hypertensive molecule Ang II, and chronic skeletal muscle fibrosis in the Sgca null mice. We confirm earlier evidence showing that TNAP is upregulated in tissue fibrosis (Herencia et al, 2015) (Gan et al, 2014), but also show here that the number of cells expressing TNAP increases in both heart and skeletal muscle. Furthermore, as the abrogation of TGF-β signaling in TNAP positive cells dramatically reduces vascular and interstitial fibrosis, we can conclude that TNAP is actively expressed in cells driving tissue fibrosis.…”

Section: Discussionsupporting

confidence: 92%

TNAP limits TGF-β-dependent cardiac and skeletal muscle fibrosis by inactivating SMAD2/3 transcription factors

Arnò

Galli

Roostalu

et al. 2019

Preprint

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2Fibrosis is associated with almost all forms of chronic cardiac and skeletal muscle diseases. The accumulation of extracellular matrix impairs the contractility of muscle cells contributing to organ failure. Transforming growth factor beta (TGF-β) plays a pivotal role in fibrosis, activating pro-fibrotic gene programs via phosphorylation of SMAD2/3 transcription factors. However, the mechanisms that control dephosphorylation of SMAD2/3 have remained poorly characterized. Here we show that tissue non-specific alkaline phosphatase (TNAP) is highly upregulated in hypertrophic hearts and in dystrophic skeletal muscles, and the abrogation of TGF-β signalling in TNAP positive cells reduces vascular and interstitial fibrosis. We show that TNAP co-localizes and interacts with SMAD2. TNAP inhibitor MLS-0038949 increases SMAD2/3 phosphorylation, while TNAP overexpression reduces SMAD2/3 phosphorylation and the expression of downstream fibrotic genes. Overall our data demonstrate that TNAP negatively regulates TGF-β signalling and likely represents a mechanism to limit fibrosis.

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Section: Discussionsupporting

confidence: 92%

TNAP limits TGF-β-dependent cardiac and skeletal muscle fibrosis by inactivating SMAD2/3 transcription factors

Arnò

Galli

Roostalu

et al. 2019

Preprint

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“…These effects are abolished by TNAP inhibition. This proves that the CD73 activity, and thus CD73-derived adenosine may act as endogenous negative regulators of hypertrophy and also calcification -possibly via inhibiting of TNAP [45].…”

Section: Cd73 and Arterial Calcificationsmentioning

confidence: 63%

“…There are also data on individual roles of CD73 and TNAP, as well as on the link between them, in the regulation of myocyte response to the a 1 -adrenoreceptor agonist-phenylephrine in the context of calcification and hypertrophy [45]. These studies clearly shows that cardiomyocyte hypertrophy in the response to phenylephrine is associated with TNAP stimulation and at the same time -CD73 inhibition, both in terms of expression and enzyme activity.…”

Section: Cd73 and Arterial Calcificationsmentioning

confidence: 97%

The role of ecto-5′-nucleotidase in endothelial dysfunction and vascular pathologies

Zukowska

Kutryb–Zajac

Toczek

et al. 2015

Pharmacological Reports

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Ecto-5'-nucleotidase (e5NT, CD73) is an enzyme that is highly expressed in endothelium and is involved in the extracellular nucleotide catabolism. CD73 converts AMP to adenosine that via specific subtypes of P1 receptor mediates cytoprotection involving diverse mechanisms such as vasodilatation, suppression of inflammation, inhibition of thrombosis and anti-adrenergic effect. Physiological intravascular concentration of adenosine is in nanomolar range, but could become micromolar in response to various forms of stress. Endothelium is a major site for both CD73 mediated production of adenosine and its cytoprotective effect. Nucleotides (predominantly ATP or ADP) that could be released from different cells via controlled specific of unspecific mechanisms constitute a major source of substrate for adenosine production via CD73. Direct effects of extracellular nucleotides (mediated by P2 receptors) are typically opposite to adenosine P1 mediated activities. Retention of nucleotides and decreased adenosine production due to loss of CD73 function may have negative implications and could be important cause of various pathologies. Protective role of CD73 was indicated in ectopic calcification, atherosclerosis, rejection after xenotransplantation and thrombosis. Reduced activity of CD73 due to lymphocyte contact with endothelium increases its permeability that leads to enhanced leukocyte transmigration. Upregulation of endothelial CD73 may therefore be protective in a number of cardiovascular pathologies. Such effect has been confirmed for some common drugs such as statins and it could be part of its pleiotropic portfolio. Activation of CD73 could be a new target for specific treatment strategy that in particular will enhance endothelial protection.

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“…9 One of the many functions of adenosine is to suppress the activity of tissue nonspecific alkaline phosphatase, an enzyme important in regulating extracellular matrix calcification. 17 p.Arg463X is a nonsense mutation, so it will cause a truncated, and often nonfunctional protein product. By protein structural modeling, we showed that p.Gly454Arg in our family may influence the folding of β-pleated sheet and make the protein unstable, thus leading to an impaired CD73 enzymatic activity.…”

Section: Discussionmentioning

confidence: 99%

Calcification of joints and arteries: second report with novel NT5E mutations and expansion of the phenotype

Zeng

et al. 2015

J Hum Genet

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Calcification of joints and arteries (CALJA; MIM 211800) is an extremely rare mendelian disorder of isolated calcification that is characterized by late onset calcification of the extremity arteries and hand and foot joint capsules. Mutations of NT5E, encoding cluster of differentiation 73, have been implicated in CALJA. Here we report on a Chinese family with CALJA and novel compound heterozygous mutations (c.1360G>A (p.Gly454Arg) and c.1387C>T (p.Arg463X)) in NT5E. Our study represents the second report on patients with CALJA associated with NT5E mutations. The clinical features expand the previously reported phenotype of NT5E mutations. The propositus has calcification of the lower extremity arteries and hand and foot joint capsules similar to those previously reported patients. However, he also has calcification of the upper extremity arteries. By protein structural modeling, we found the mutation p.Gly454Arg may disrupt the folding of β-pleated sheet and destabilize the protein structure. Our findings will provide clues to the phenotype-genotype relations and may assist not only in the clinical diagnosis but also in the interpretation of genetic information used for prenatal diagnosis and genetic counseling.

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CD73-TNAP crosstalk regulates the hypertrophic response and cardiomyocyte calcification due to α1 adrenoceptor activation

Cited by 25 publications

References 31 publications

TNAP limits TGF-β-dependent cardiac and skeletal muscle fibrosis by inactivating SMAD2/3 transcription factors

TNAP limits TGF-β-dependent cardiac and skeletal muscle fibrosis by inactivating SMAD2/3 transcription factors

The role of ecto-5′-nucleotidase in endothelial dysfunction and vascular pathologies

Calcification of joints and arteries: second report with novel NT5E mutations and expansion of the phenotype

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