Effects of adenosine deaminase and A1 receptor deficiency in normoxic and ischaemic mouse hearts

Willems, Laura; Reichelt, Melissa E.; Molina, Jose G.; Sun, Chunxiao; Chunn, Janci L.; Ashton, Kevin J.; Schnermann, Jürgen; Blackburn, Michael R.; Headrick, John P.

doi:10.1016/j.cardiores.2006.03.006

Cited by 26 publications

(27 citation statements)

References 53 publications

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“…Adenosine deaminase (ADA)-deficient mice (Blackburn et al, 1998) were maintained on ADA enzyme therapy as described previously (Blackburn et al, 2000) until the age of 6 weeks. An increase in adenosine levels in the hearts was induced by withdrawing mice from enzyme therapy for 15 days before experiments (Willems et al, 2006). The H-2K b -tsA58 transgenic mice on a C57BL/6 genetic background (Immortomouse) were purchased from Charles River Laboratories International, Inc. (Wilmington, MA).…”

Section: Methodsmentioning

confidence: 99%

“…A considerable increase in the stromal to endothelial cell ratio ؊ Stromal and Sca-1 ؉ CD31 ؉ Endothelial Cells Induced by Adenosine In Vivo. Withdrawal from ADA enzyme replacement therapy for 2 weeks has been reported to increase adenosine levels in hearts of ADA-deficient mice (Willems et al, 2006). We used this model to evaluate in vivo the effects of adenosine on VEGF production by cardiac stromal and endothelial cells.…”

Section: Cd31mentioning

confidence: 99%

“…Concentrations of extracellular adenosine were demonstrated to increase in ischemic hearts, where it becomes a part of the pathological environment (Martin et al, 1997;Willems et al, 2006). Adenosine exerts its actions via cell surface receptors of the G protein-coupled receptor family, namely A 1 , A 2A , A 2B , and A 3 (Fredholm et al, 2001).…”

Section: Introductionmentioning

confidence: 99%

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Role of A_2BAdenosine Receptors in Regulation of Paracrine Functions of Stem Cell Antigen 1-Positive Cardiac Stromal Cells

Ryzhov

Goldstein

Novitskiy

et al. 2012

J Pharmacol Exp Ther

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Section: Methodsmentioning

confidence: 99%

Section: Cd31mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Role of A_2BAdenosine Receptors in Regulation of Paracrine Functions of Stem Cell Antigen 1-Positive Cardiac Stromal Cells

Ryzhov

Goldstein

Novitskiy

et al. 2012

J Pharmacol Exp Ther

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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%

“…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). In addition, adenosine signaling through the A 2a receptor has shown to be protective under hypoxic conditions in the lung by inhibiting the immune response (8).…”

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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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Anti-adipogenesis by 6-thioinosine is mediated by downregulation of PPAR γ through JNK-dependent upregulation of iNOS

Lee

Jung

Lee

et al. 2009

Cell. Mol. Life Sci.

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Adipocyte dysfunction is associated with the development of obesity. This study shows that 6-thioinosine inhibits adipocyte differentiation. The mRNA levels of PPAR gamma and C/EBPalpha, but not C/EBPbeta and delta, were reduced by 6-thioinosine. Moreover, the mRNA levels of PPAR gamma target genes (LPL, CD36, aP2, and LXRalpha) were down-regulated by 6-thioinosine. We also demonstrated that 6-thioinosine inhibits the transactivation activity and the mRNA level of PPAR gamma. Additionally, attempts to elucidate a possible mechanism underlying the 6-thioinosine-mediated effects revealed that 6-thioinosine induced iNOS gene expression without impacting eNOS expression, and that this was mediated through activation of AP-1, especially, JNK. In addition, 6-thioinosine was found to operate upstream of MEKK-1 in JNK activation signaling. Taken together, these findings suggest that the inhibition of adipocyte differentiation by 6-thioinosine occurs primarily through the reduced expression of PPAR gamma, which is mediated by upregulation of iNOS via the activation of JNK.

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Effects of adenosine deaminase and A1 receptor deficiency in normoxic and ischaemic mouse hearts

Cited by 26 publications

References 53 publications

Role of A_2BAdenosine Receptors in Regulation of Paracrine Functions of Stem Cell Antigen 1-Positive Cardiac Stromal Cells

Role of A_2BAdenosine Receptors in Regulation of Paracrine Functions of Stem Cell Antigen 1-Positive Cardiac Stromal Cells

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

Anti-adipogenesis by 6-thioinosine is mediated by downregulation of PPAR γ through JNK-dependent upregulation of iNOS

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Effects of adenosine deaminase and A1 receptor deficiency in normoxic and ischaemic mouse hearts

Cited by 26 publications

References 53 publications

Role of A2BAdenosine Receptors in Regulation of Paracrine Functions of Stem Cell Antigen 1-Positive Cardiac Stromal Cells

Role of A2BAdenosine Receptors in Regulation of Paracrine Functions of Stem Cell Antigen 1-Positive Cardiac Stromal Cells

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

Anti-adipogenesis by 6-thioinosine is mediated by downregulation of PPAR γ through JNK-dependent upregulation of iNOS

Contact Info

Product

Resources

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Role of A_2BAdenosine Receptors in Regulation of Paracrine Functions of Stem Cell Antigen 1-Positive Cardiac Stromal Cells

Role of A_2BAdenosine Receptors in Regulation of Paracrine Functions of Stem Cell Antigen 1-Positive Cardiac Stromal Cells