4.6 Article

In Vitro Antithrombotic, Hematological Toxicity, and Inhibitor Studies of Protocatechuic, Isovanillic, and p-Hydroxybenzoic Acids from Maclura tricuspidata (Carr.) Bur

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MOLECULES
卷 27, 期 11, 页码 -

出版社

MDPI
DOI: 10.3390/molecules27113496

关键词

protocatechuic acid; isovanillic acid; p-Hydroxybenzoic acid; antithrombosis; anticoagulation; inhibitor

资金

  1. Korea Forest Service [2021381D10-2223-BD02]
  2. Korea Forestry Promotion Institute (KOFPI) [2021381D10-2223-BD02] Funding Source: Korea Institute of Science & Technology Information (KISTI), National Science & Technology Information Service (NTIS)

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This study explored the antithrombotic activity and hematological toxicity of three compounds (PA, IVA, and 4-HA) isolated from M. tricuspidata. The results showed that these compounds could reduce the formation and degrade existing blood clots, inhibit the activities of coagulation factors, prolong coagulation time, and lower platelet function and activation levels without being toxic to blood cells.
In blood coagulation, circulating platelets and coagulation factors are crucial for the primary process because thrombi are generated by fibrin clotting with fibrinogen, thrombin, FXIIIa, and platelet activation. Therefore, strategies to reduce the activity of key coagulation factors, or interfere with their functions and delay the activation of platelets can be used as important tools to suppress excessive blood clot formation and platelet hyperactivation. This study examined the antithrombotic activity and hematological toxicity of PA, IVA, and 4-HA isolated from M. tricuspidata (Carr.) Bur in several in vitro experiments and inhibitor assays. We found that PA, IVA, and 4-HA attenuated the formation of fibrin polymers/clots and degraded the blood clots. These compounds inhibited the activities of procoagulant proteases and fibrinoligase, and prolonged the coagulation time. There was a significant reduction in platelet function and ATP or serotonin levels in thrombin-activated platelets. An inhibitor study showed that PA exhibited a mixed inhibition type for thrombin, an uncompetitive inhibition type for FXa, and a non-competitive inhibition type for FXIIIa and IVA, while 4-HA exhibited an uncompetitive inhibition type for thrombin and non-competitive inhibition type for FXa and FXIIIa. These three compounds (up to 50 mu g/mL) were not toxic to blood cells.

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