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Dive into the research topics where Joel Linden is active.

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Featured researches published by Joel Linden.


Biochemical Journal | 2001

Gene dose effect reveals no Gs-coupled A2A adenosine receptor reserve in murine T-lymphocytes: studies of cells from A2A-receptor-gene-deficient mice.

John Armstrong; Jiang-Fan Chen; Michael A. Schwarzschild; Sergey Apasov; Patrick Smith; Charles C. Caldwell; Pearl Chen; Heidi Figler; Gail W. Sullivan; Steven Fink; Joel Linden; Michail Sitkovsky

Agonist binding to extracellular A2A adenosine receptors (A2ARs) inhibits the activation of virtually all tested functions of T-cells and can induce apoptosis in thymocytes. The evaluation of levels of expression of these immunosuppressive receptors is expected to clarify whether the absence of spare A2ARs (no receptor reserve) might be one of the mechanisms of attenuation of the effects of extracellular adenosine on T-cells. A2A transcript is found in T-cells and functional receptors can be demonstrated, but the density of receptor on T-cells is too low to be detected by radioligand binding. Studies of direct radioligand binding to murine brain with the selective A2AR agonist [3H]CGS21680 (2-(4-[(2-carboxyethyl)-phenyl]ethylamino)-5-N-ethylcarboxamidoadenosine) established that striata levels of A2AR are virtually absent from A2A knock-out mice. Mice that are heterozygous (A2AR+/-) for the A2AR express significantly decreased levels of A2AR. To test for the presence of spare receptors in T-cells we took advantage of this gene dose effect and examined whether the decrease in the number of receptors in thymocytes from A2AR+/- mice was proportionately reflected in a decrease in the functional cAMP response of T-cells to adenosine. cAMP accumulation and apoptosis induced by adenosine and by A2AR agonist are of a lower magnitude in T-cells from A2AR+/- heterozygous mice than in T-cells from A2AR+/+ littermate control mice. These results indicate that there is no A2AR reserve in murine T-cells. Strongly decreased adenosine-triggered cAMP increases were detected in thymocytes from A2AR-/- mice, suggesting that A2B adenosine receptors cannot fully compensate for the loss of A2ARs in murine T-cells. We conclude that the number of A2ARs is the limiting factor in determining the maximal cAMP response of T-lymphocytes to extracellular adenosine, thereby minimizing the immunosuppressive effects of extracellular adenosine.


Archive | 2000

Substituted 8-phenylxanthines useful as antagonists of A2B adenosine receptors

Joel Linden; Kenneth A. Jacobson; Yong-Chul Kim


Archive | 2000

Method for treating restenosis with A2A adenosine receptor agonists

Joel Linden; Gail W. Sullivan; Ian J. Sarembock; W. Michael Sheld


Archive | 2003

Use of a2a adenosine receptor agonists for the treatment of inflammatory diseases

Joel Linden; Gail W. Sullivan; Timothy L. Macdonald; W. Michael Scheld; Tom G. Obrig; Jayson M. Rieger


Archive | 2011

Pharmacology of purine and pyrimidine receptors

Kenneth A. Jacobson; Joel Linden


Archive | 2005

2-polycyclic propynyl adenosine analogs with modified 5'-ribose groups having a2a agonist activity

Jayson M. Rieger; Joel Linden; Timothy L. Macdonald; Gail W. Sullivan; Lauren Murphree; Robert A. Figler; Robert D. Thompson


Archive | 2009

A Novel Neutrophil-Specific PET Imaging Agent: cFLFLFK-PEG- 64 Cu

Landon W. Locke; Mahendra D. Chordia; Yi Zhang; Bijoy Kundu; Dylan Kennedy; Jessica Landseadel; Li Xiao; Karen D. Fairchild; Stuart S. Berr; Joel Linden; Dongfeng Pan


Archive | 2003

2-aminothiazole allosteric enhancers of a1 adenosine receptors

Joel Linden; Timothy L. Macdonald; Lauren Murphree; Mahendra D. Chordia


Archive | 2010

INTERLACED METHOD FOR TREATING CANCER OR A PRECANCEROUS CONDITION

Andrew J. Krouse; Lloyd S. Gray; Timothy L. Macdonald; Joel Linden


Archive | 2016

COMBINATION METHOD FOR TREATING CANCER OR PRECANCEROUS CONDITION

Andrew J. Krouse; Lloyd S. Gray; Timothy L. Macdonald; Joel Linden

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Gail W. Sullivan

National Institutes of Health

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Irving L. Kron

Memorial Hospital of South Bend

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Lauren Murphree

National Institutes of Health

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Kenneth A. Jacobson

Case Western Reserve University

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