Adenine nucleotide metabolism in human blood – important roles for leukocytes and erythrocytes

Heptinstall, S; Johnson, Andrew; Glenn, J. R.; White, Ann E.

doi:10.1111/j.1538-7836.2005.01489.x

Cited by 61 publications

(53 citation statements)

References 27 publications

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“…1), indicating that the H12-(ADP)-liposomes circulate in the bloodstream without any leakage of ADP. In addition, we also realized that the nonliposomal ADP was immediately eliminated from blood (unpublished data), because ADP released into blood was metabolized by leukocytes, erythrocytes, and endothelial cells (Marcus et al, 2003;Heptinstall et al, 2005). This means that ADP encapsulated in the vesicle has advantages that are not only specific delivery ADP to injury site but also improvement of the blood retention of ADP.…”

Section: Discussionmentioning

confidence: 94%

Pharmacokinetic Study of the Structural Components of Adenosine Diphosphate-Encapsulated Liposomes Coated with Fibrinogenγ-Chain Dodecapeptide as a Synthetic Platelet Substitute

et al. 2013

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Fibrinogen g-chain (dodecapeptide HHLGGAKQAGDV, H12)-coated, ADP-encapsulated liposomes [H12-(ADP)-liposomes] were developed as a synthetic platelet alternative that specifically accumulates at bleeding sites as the result of interactions with activated platelets via glycoprotein IIb/IIIa and augments platelet aggregation by releasing ADP. The aim of this study is to characterize the pharmacokinetic properties of H12-(ADP)-liposomes and structural components in rats, and to predict the blood retention of H12-(ADP)-liposomes in humans. With use of H12-(ADP)-liposomes in which the encapsulated ADP and liposomal membrane cholesterol were radiolabeled with 14 C and 3 H, respectively, it was found that the time courses for the plasma concentration curves of 14 C and 3 H radioactivity showed that the H12-(ADP)-liposomes remained intact in the blood circulation for up to 24 hours after injection, and were mainly distributed to the liver and spleen. However, the 14 C and 3 H radioactivity of H12-(ADP)-liposomes disappeared from organs within 7 days after injection. The encapsulated ADP was metabolized to allantoin, which is the final metabolite of ADP in rodents, and was mainly eliminated in the urine, whereas the cholesterol was mainly eliminated in feces. In addition, the half-life of the H12-(ADP)-liposomes in humans was predicted to be approximately 96 hours from pharmacokinetic data obtained for mice, rats, and rabbits using an allometric equation. These results suggest that the H12-(ADP)-liposome has potential with proper pharmacokinetic and acceptable biodegradable properties as a synthetic platelet substitute.

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Section: Discussionmentioning

confidence: 94%

Pharmacokinetic Study of the Structural Components of Adenosine Diphosphate-Encapsulated Liposomes Coated with Fibrinogenγ-Chain Dodecapeptide as a Synthetic Platelet Substitute

et al. 2013

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“…Large pools of ATP/ADP are sequestered in secretory granules during platelet formation, and the release of ADP from activated platelets is one of the important signals stimulating their aggregation. Furthermore, ATP coreleased with ADP from dense granules may increase platelet aggregation in whole blood because of its cleavage to ADP by ecto-ATPases present on the surface of leukocytes (11,12). In addition, platelet exocytosis and aggregation require metabolic energy in the form of ATP (13).…”

mentioning

confidence: 99%

Alterations of Adenine Nucleotide Metabolism and Function of Blood Platelets in Patients With Diabetes

et al. 2007

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Increased activity of blood platelets contributes to vascular complications in patients with diabetes. The aim of this work was to investigate whether persisting hyperglycemia in diabetic patients generates excessive accumulation of ATP/ADP, which may underlie platelet hyperactivity. Platelet ATP and ADP levels, thiobarbituric acid-reactive species synthesis, and aggregation of platelets from patients with diabetes were 18 -82% higher than in platelets from healthy participants. In patients with diabetes, platelet stimulation with thrombin caused about two times greater release of ATP and ADP than in the healthy group while decreasing intraplatelet nucleotide content to similar levels in both groups. This indicates that the increased content of adenylate nucleotides in the releasable pool in the platelets of diabetic patients does not affect their level in metabolic cytoplasmic/mitochondrial compartments. Significant correlations between platelet ATP levels and plasma fructosamine, as well as between platelet ATP/ADP and platelet activities, have been found in diabetic patients. In conclusion, chronic hyperglycemia-evoked elevations of ATP/ADP levels and release from blood platelets of patients with diabetes may be important factors underlying platelet hyperactivity in the course of the disease.

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“…ATP can be converted into ADP in the presence of leukocytes (35). ADP is a potent stimulus for platelet aggregation.…”

Section: Pathophysiology Of Vascular Occlusion In Ttpmentioning

confidence: 99%

“…However, not all studies have reported success with ASA plus dipyridamole (51) and, furthermore, these studies have not examined the effect of treatment on troponin levels. From a theoretical standpoint, dipyridamole has several advantages: it exerts antiplatelet activity by inhibiting platelet phosphodiesterase and also has a vasodilating effect by inhibiting the uptake of adenosine into red cells, endothelial cells and platelets by blocking the equilibrative nucleoside transporters (35). Subsequent binding of adenosine to the A2 adenosine receptor leads to elevated intracellular levels of cAMP, which results in anti-platelet activity and vasodilation.…”

Section: Current Adjunctive Therapiesmentioning

confidence: 99%

Myocardial necrosis in patients with thrombotic thrombocytopenic purpura: pathophysiology and rationale for specific therapy

Sane¹,

Streer

Owen

2009

European J of Haematology

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Myocardial necrosis is now recognized as a common feature of thrombotic thrombocytopenic purpura (TTP), usually due to platelet plugging in the microvasculature. Despite reports that TTP patients with myocardial damage have higher morbidity and mortality, there are no established guidelines for managing these high‐risk patients. The universal occurrence of thrombocytopenia and variable findings including renal dysfunction present unique challenges in this setting. Established therapies including plasma exchange and immunosuppression are the mainstay of therapy for all TTP patients. For the subset of patients with myocardial damage, therapy with more potent antiplatelet drugs, agents that enhance NO availability and alleviate vasospasm and drugs that suppress von Willebrand factor levels may have additional benefit. However, clinical trials are needed to optimize therapy for this subset of TTP patients.

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Adenine nucleotide metabolism in human blood – important roles for leukocytes and erythrocytes

Cited by 61 publications

References 27 publications

Pharmacokinetic Study of the Structural Components of Adenosine Diphosphate-Encapsulated Liposomes Coated with Fibrinogenγ-Chain Dodecapeptide as a Synthetic Platelet Substitute

Pharmacokinetic Study of the Structural Components of Adenosine Diphosphate-Encapsulated Liposomes Coated with Fibrinogenγ-Chain Dodecapeptide as a Synthetic Platelet Substitute

Alterations of Adenine Nucleotide Metabolism and Function of Blood Platelets in Patients With Diabetes

Myocardial necrosis in patients with thrombotic thrombocytopenic purpura: pathophysiology and rationale for specific therapy

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