Transgenic A
            <sub>1</sub>
            adenosine receptor overexpression increases myocardial resistance to ischemia

Matherne, G. Paul; Linden, Joel; Byford, Anne M.; Gauthier, Naomi; Headrick, John P.

doi:10.1073/pnas.94.12.6541

Cited by 150 publications

(191 citation statements)

References 42 publications

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“…GLUT4 is an important transporter for the entry of glucose into myocardial cells, and NADH dehydrogenase is a mitochondrial enzyme involved in the first step of the electron transport chain. The role of these proteins in cellular ATP production supports the hypothesis that their overexpression could contribute to the preservation of ATP stores during ischemia (7) and possibly the overall tolerance to ischemia-reperfusion injury afforded by A 1 AR overexpression (12,13,25). Another previous finding in transgenic mice is the observation of altered adrenergic responsiveness of Ltype calcium channel current in myocytes isolated from transgenic hearts (unpublished results).…”

Section: Discussionsupporting

confidence: 63%

“…85-23, revised 1996) and the work was approved by the Institutional Animal Care and Use committee. Transgenic mice overexpressing the rat A1AR cDNA were produced as described previously (12). Briefly, the full-length rat A1 cDNA was subcloned into a construct containing the ␣-MHC promoter with a MEF-2 mutation and the human growth hormone polyadenylation signal.…”

Section: Methodsmentioning

confidence: 99%

“…Since the degree of protection is limited by the availability of A 1 ARs, we have developed lines of transgenic mice with 20-to 200-fold overexpression of cardiac A 1 ARs to optimize the cardioprotective effect (12). Transgenic mouse hearts demonstrate better functional tolerance and diminished cell necrosis, compared with wild-type controls, in response to global ischemia in isolated perfused heart studies (13).…”

mentioning

confidence: 99%

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Gene expression profile of mouse myocardium with transgenic overexpression of A₁adenosine receptors

Lankford

Byford

Ashton

et al. 2002

Physiological Genomics

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Section: Discussionsupporting

confidence: 63%

Section: Methodsmentioning

confidence: 99%

mentioning

confidence: 99%

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Gene expression profile of mouse myocardium with transgenic overexpression of A₁adenosine receptors

Lankford

Byford

Ashton

et al. 2002

Physiological Genomics

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“…A 1 AR signaling has also been shown to protect cells from damage. Deletion of adenosine deaminase leads to elevated adenosine levels and protects the heart from ischemic/ reperfusion injury (18,19). Overexpression of A 1 AR also helps to protect the heart from ischemic/reperfusion injury and conversely the loss of A 1 AR impairs ischemic tolerance (18,19).…”

mentioning

confidence: 99%

A1 adenosine receptors play an essential role in protecting the embryo against hypoxia

Wendler

Amatya

McClaskey

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

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Embryos can be exposed to environmental factors that induce hypoxia. Currently, our understanding of the effects of hypoxia on early mammalian development is modest. Potential mediators of hypoxia action include the nucleoside adenosine, which acts through A 1 adenosine receptors (A1ARs) and mediates adverse effects of hypoxia on the neonatal brain. We hypothesized that A 1ARs may also play a role in mediating effects of hypoxia on the embryo. When pregnant dams were exposed to hypoxia (10% O2) beginning at embryonic day (E) 7.5 or 8.5 and continued for 24 -96 h, A 1AR؉/؉ embryos manifested growth inhibition and a disproportionate reduction in heart size, including thinner ventricular walls. Yet, when dams were exposed to hypoxia, embryos lacking A 1ARs (A1AR؊/؊) had much more severe growth retardation than A 1AR؉/؉ or ؉/؊ embryos. When levels of hypoxia-inducible factor 1␣ (HIF1␣) were examined, A1AR؊/؊ embryos had less stabilized HIF1␣ protein than A1AR؉/؊ littermates. Normal patterns of cardiac gene expression were also disturbed in A1AR؊/؊ embryos exposed to hypoxia. These results show that short periods of hypoxia during early embryogenesis can result in intrauterine growth retardation. We identify adenosine and A1ARs as playing an essential role in protecting the embryo from hypoxia.cardiac ͉ heart development ͉ hypoxia-inducible factor ͉ intrauterine growth retardation

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“…2) [45][46][47]; it also showed somewhat reduced affinity and potency. In contrast, several of the mutants displayed increased potency of adenine up to 14 [48,49].…”

Section: Discussionmentioning

confidence: 88%

The rat adenine receptor: pharmacological characterization and mutagenesis studies to investigate its putative ligand binding site

Knospe

Müller

Rosa

et al. 2013

Purinergic Signalling

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The rat adenine receptor (rAdeR) was the first member of a family of G protein-coupled receptors (GPCRs) activated by adenine and designated as P0-purine receptors. The present study aimed at gaining insights into structural aspects of ligand binding and function of the rAdeR. We exchanged amino acid residues predicted to be involved in ligand binding (Phe110 3.24 47 , were found to be crucial for activation since their alanine mutants did not respond to adenine. Moreover we showed that-in contrast to most other rhodopsin-like GPCRs-the rAdeR does not contain essential disulfide bonds since preincubation with dithiothreitol neither altered adenine binding in Sf9 cell membranes, nor adenineinduced inhibition of adenylate cyclase in 1321N1 astrocytoma cells transfected with the rAdeR. To detect rAdeRs by Western blot analysis, we developed a specific antibody. Finally, we were able to show that the extended N-terminal sequence of the rAdeR constitutes a putative signal peptide of unknown function that is cleaved off in the mature receptor. Our results provide important insights into this new, poorly investigated family of purinergic receptors.

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Transgenic A ₁ adenosine receptor overexpression increases myocardial resistance to ischemia

Cited by 150 publications

References 42 publications

Gene expression profile of mouse myocardium with transgenic overexpression of A₁adenosine receptors

Gene expression profile of mouse myocardium with transgenic overexpression of A₁adenosine receptors

A1 adenosine receptors play an essential role in protecting the embryo against hypoxia

The rat adenine receptor: pharmacological characterization and mutagenesis studies to investigate its putative ligand binding site

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Transgenic A 1 adenosine receptor overexpression increases myocardial resistance to ischemia

Cited by 150 publications

References 42 publications

Gene expression profile of mouse myocardium with transgenic overexpression of A1adenosine receptors

Gene expression profile of mouse myocardium with transgenic overexpression of A1adenosine receptors

A1 adenosine receptors play an essential role in protecting the embryo against hypoxia

The rat adenine receptor: pharmacological characterization and mutagenesis studies to investigate its putative ligand binding site

Contact Info

Product

Resources

About

Transgenic A ₁ adenosine receptor overexpression increases myocardial resistance to ischemia

Gene expression profile of mouse myocardium with transgenic overexpression of A₁adenosine receptors

Gene expression profile of mouse myocardium with transgenic overexpression of A₁adenosine receptors