Historical and Current Adenosine Receptor Agonists in Preclinical and Clinical Development

Jacobson, Kenneth A.; Tosh, Dilip K.; Jain, Shanu; Gao, Zhan‐Guo

doi:10.3389/fncel.2019.00124

Cited by 154 publications

(191 citation statements)

References 157 publications

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“…Regadenoson (CVT-3146, Lexiscan) is a synthetic AR agonist currently approved for clinical use as a pharmacologic stress agent for myocardial perfusion imaging (MPI). It demonstrates non-inferiority to adenosine for detecting reversible myocardial perfusion defects, although it is a moderately selective (K i = 290 nM), short acting A 2A AR agonist with low affinity for the remaining adenosine receptors [22,25,26]. In addition to its diagnostic application, regadenoson was considered for the treatment of inflammation and sickle cell disease, and was involved in the development of brain tumor-targeted drug delivery systems [27][28][29].…”

Section: Discussionmentioning

confidence: 99%

Adenosine Receptor Agonists Exhibit Anti-Platelet Effects and the Potential to Overcome Resistance to P2Y12 Receptor Antagonists

et al. 2019

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Large inter-individual variation in platelet response to endogenous agonists and pharmacological agents, including resistance to antiplatelet therapy, prompts a search for novel platelet inhibitors and development new antithrombotic strategies. The present in vitro study evaluates the beneficial effects of three adenosine receptor (AR) agonists (regadenoson, LUF 5835 and NECA), different in terms of their selectivity for platelet adenosine receptors, when used alone and in combination with P2Y 12 inhibitors, such as cangrelor or prasugrel metabolite. The anti-platelet effects of AR agonists were evaluated in healthy subjects (in the whole group and after stratification of individuals into high-and low-responders to P2Y 12 inhibitors), using whole blood techniques, under flow (thrombus formation) and static conditions (study of platelet activation and aggregation). Compared to P2Y 12 antagonists, AR agonists were much less or not effective under static conditions, but demonstrated similar antiplatelet activity in flow. In most cases, AR agonists significantly enhanced the anti-platelet effect of P2Y 12 antagonists, despite possessing different selectivity profiles and antiplatelet activities. Importantly, their inhibitory effects in combination with P2Y 12 antagonists were similar in high-and low-responders to P2Y 12 inhibitors. In conclusion, a combination of anti-platelet agents acting via the P1 and P2 purinergic receptors represents a promising alternative to existing antithrombotic therapy.Molecules 2020, 25, 130 2 of 17 ADP is one of the key mediators of both physiological haemostasis and thrombosis, being not only a direct agonist of platelets, but also an important factor released from platelet intracellular structures, enhancing the platelet response initially induced by other activators. Platelets have two ADP receptors on their surface: the P2Y 1 receptor initiates platelet aggregation, while the P2Y 12 receptor enhances this process, eventually leading to the formation of a clot. Due to this fact, the P2Y 12 receptor is the main therapeutic target in anti-platelet therapy targeted at the ADP-dependent activation pathway [5]. Generally, the most commonly used clinically approved P2Y 12 inhibitors include the thienopyridine-class inhibitors (ticlopidine, clopidogrel and prasugrel), the ATP analogue cangrelor, and the cyclo-pentyl-triazolo-pyrimidine derivative ticagrelor [3,5]. Thienopyridines are prodrugs: their short-lived active metabolites irreversibly inactivate the receptor and consequently inhibit ADP-induced platelet activation. Cangrelor is the first (recently approved) intravenous P2Y 12 receptor inhibitor that reversibly and non-competitively blocks ADP signalling [6].Adenosine is an important purine metabolite, serving not only as a component of nucleic acids and ATP, the most important energy carrier in the cell, but also as a signalling molecule regulating many cell processes [7,8]. Adenosine receptors (AR) are a subfamily of highly conserved G protein-coupled receptors located in the membr...

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Section: Discussionmentioning

confidence: 99%

Adenosine Receptor Agonists Exhibit Anti-Platelet Effects and the Potential to Overcome Resistance to P2Y12 Receptor Antagonists

et al. 2019

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“…Moreover, this agonist also stimulated A 2B AR, promoting cardioprotection and modulating cardiac fibrosis in heart disease [122]. Unfortunately, the clinical trial of capadenoson was discontinued [123]. A clinical trial using the partial agonist neladenoson (BAY 1067197) for the treatment of heart failure was safe without atrioventricular conduction disorders or neurological adverse effects [124].…”

Section: A 1 Ar In the Cardiovascular Systemsmentioning

confidence: 99%

“…A clinical trial using the partial agonist neladenoson (BAY 1067197) for the treatment of heart failure was safe without atrioventricular conduction disorders or neurological adverse effects [124]. A multiple-dose study of neladenoson in heart failure is still ongoing [123].…”

Section: A 1 Ar In the Cardiovascular Systemsmentioning

confidence: 99%

“…At present, several full A 1 AR agonists have been used in clinical trials as antiarrhythmic agents. An optimal dose of a new A 1 AR selective agonist, tecadenoson (CVT-510), was successful in the conversion of paroxysmal supraventricular tachycardia (PSVT) into sinus rhythm [128], but its development for PSVT and atrial fibrillation (AF) was discontinued in 2009 [123]. Other agonists, such as selodenoson and PJ-875, have started in early phase evaluations for the treatment of AF [129].…”

Section: A 1 Ar In the Cardiovascular Systemsmentioning

confidence: 99%

“…It was assumed that prolonged activation of A 1 AR increased A 2A AR expression, which generated global damage and neurodegeneration in ischemic stroke [135]. Recently, an A 1 AR selective agonist, NNC-21-0136, was designed for neuroprotection in stroke models [123].…”

Section: A 1 Ar In Cnsmentioning

confidence: 99%

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Focusing on Adenosine Receptors as a Potential Targeted Therapy in Human Diseases

Effendi

Nagano

Kobayashi

et al. 2020

Cells

104

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Adenosine is involved in a range of physiological and pathological effects through membrane-bound receptors linked to G proteins. There are four subtypes of adenosine receptors, described as A1AR, A2AAR, A2BAR, and A3AR, which are the center of cAMP signal pathway-based drug development. Several types of agonists, partial agonists or antagonists, and allosteric substances have been synthesized from these receptors as new therapeutic drug candidates. Research efforts surrounding A1AR and A2AAR are perhaps the most enticing because of their concentration and affinity; however, as a consequence of distressing conditions, both A2BAR and A3AR levels might accumulate. This review focuses on the biological features of each adenosine receptor as the basis of ligand production and describes clinical studies of adenosine receptor-associated pharmaceuticals in human diseases.

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Importance of Structure and Dynamics in the Rational Drug Design of G Protein‐Coupled Receptor ( GPCR ) Modulators

Lazim¹,

Lee²,

Nakliang³

et al. 2022

GPCRs as Therapeutic Targets

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Historical and Current Adenosine Receptor Agonists in Preclinical and Clinical Development

Cited by 154 publications

References 157 publications

Adenosine Receptor Agonists Exhibit Anti-Platelet Effects and the Potential to Overcome Resistance to P2Y12 Receptor Antagonists

Adenosine Receptor Agonists Exhibit Anti-Platelet Effects and the Potential to Overcome Resistance to P2Y12 Receptor Antagonists

Focusing on Adenosine Receptors as a Potential Targeted Therapy in Human Diseases

Importance of Structure and Dynamics in the Rational Drug Design of G Protein‐Coupled Receptor ( GPCR ) Modulators

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