Antiplatelet Aggregation and Antithrombosis Efficiency of Peptides in the Snake Venom ofDeinagkistrodon acutus: Isolation, Identification, and Evaluation

Author:

Ding Bin1,Xu Zhenghong1,Qian Chaodong1,Jiang Fusheng1,Ding Xinghong1,Ruan Yeping1,Ding Zhishan1,Fan Yongsheng1

Affiliation:

1. Zhejiang Chinese Medical University, Hangzhou, Zhejiang 310053, China

Abstract

Two peptides of Pt-A (Glu-Asn-Trp 429 Da) and Pt-B (Glu-Gln-Trp 443 Da) were isolated from venom liquor ofDeinagkistrodon acutus. Their antiplatelet aggregation effects were evaluated with platelet-rich human plasmain vitro; the respective IC50of Pt-A and Pt-B was 66 μM and 203 μM. Both peptides exhibited protection effects on ADP-induced paralysis in mice. After ADP administration, the paralysis time of different concentration of Pt-A and Pt-B lasted as the following: 80 mg/kg Pt-B (152.8 ± 57.8 s) < 40 mg/kg Pt-A (163.5 ± 59.8 s) < 20 mg/kg Pt-A (253.5 ± 74.5 s) < 4 mg/kg clopidogrel (a positive control, 254.5 ± 41.97 s) < 40 mg/kg Pt-B (400.8 ± 35.9 s) < 10 mg/kg Pt-A (422.8 ± 55.4 s), all of which were statistically shorter than the saline treatment (666 ± 28 s). Pulmonary tissue biopsy confirmed that Pt-A and Pt-B prevented the formation of thrombi in the lung. Unlike ADP injection alone, which caused significant reduction of peripheral platelet count, Pt-A treatment prevented the drop of peripheral platelet counts; interestingly, Pt-B could not, even though the same amount of Pt-B also showed protection effects on ADP-induced paralysis and thrombosis. More importantly, intravenous injection of Pt-A and Pt-B did not significantly increase the hemorrhage risks as clopidogrel.

Funder

Qianjiang Talents C and D Scheme of Zhejiang Province

Publisher

Hindawi Limited

Subject

Complementary and alternative medicine

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