Antiplatelet effects of the CEACAM1-derived peptide QDTT.

IF 2.5 3区医学 Q3 CELL BIOLOGY Platelets Pub Date : 2024-12-01 Epub Date: 2024-02-12 DOI:10.1080/09537104.2024.2308635

Yujia Ye, Min Leng, Shengjie Chai, Lihong Yang, Longcheng Ren, Wen Wan, Huawei Wang, Longjun Li, Chaozhong Li, Zhaohui Meng

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Abstract

Carcinoembryonic antigen-related cell adhesion molecule 1 (CEACAM1) restricts platelet activation via platelet collagen receptor GPVI/FcRγ-chain. In this study, screening against collagen-induced platelet aggregation was performed to identify functional CEACAM1 extracellular domain fragments. CEACAM1 fragments, including Ala-substituted peptides, were synthesized. Platelet assays were conducted on healthy donor samples for aggregation, cytotoxicity, adhesion, spreading, and secretion. Mice were used for tail bleeding and FeCl₃-induced thrombosis experiments. Clot retraction was assessed using platelet-rich plasma. Extracellular segments of CEACAM1 and A1 domain-derived peptide QDTT were identified, while N, A2, and B domains showed no involvement. QDTT inhibited platelet aggregation. Ala substitution for essential amino acids (Asp139, Thr141, Tyr142, Trp144, and Trp145) in the QDTT sequence abrogated collagen-induced aggregation inhibition. QDTT also suppressed platelet secretion and "inside-out" GP IIb/IIIa activation by convulxin, along with inhibiting PI3K/Akt pathways. QDTT curtailed FeCl₃-induced mesenteric thrombosis without significantly prolonging bleeding time, implying the potential of CEACAM1 A1 domain against platelet activation without raising bleeding risk, thus paving the way for novel antiplatelet drugs.

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CEACAM1 衍生肽 QDTT 的抗血小板作用。

癌胚抗原相关细胞粘附分子 1（CEACAM1）通过血小板胶原受体 GPVI/FcRγ-链限制血小板活化。本研究对胶原蛋白诱导的血小板聚集进行了筛选，以确定功能性 CEACAM1 细胞外结构域片段。研究人员合成了 CEACAM1 片段，包括 Ala 取代的多肽。对健康供体样本进行了血小板聚集、细胞毒性、粘附、扩散和分泌试验。用小鼠进行尾部出血和氯化铁诱导血栓形成实验。使用富血小板血浆对血栓回缩进行评估。结果表明，CEACAM1的胞外片段和A1结构域衍生肽QDTT被鉴定出来，而N、A2和B结构域则没有参与。QDTT 可抑制血小板聚集。用 Ala 取代 QDTT 序列中的必需氨基酸（Asp139、Thr141、Tyr142、Trp144 和 Trp145）可减弱胶原诱导的聚集抑制作用。QDTT 还能抑制血小板分泌和旋覆花苷对 GP IIb/IIIa 的 "内向外 "激活，同时抑制 PI3K/Akt 通路。QDTT能抑制FeCl3诱导的肠系膜血栓形成，而不会明显延长出血时间，这意味着CEACAM1 A1结构域具有抗血小板活化的潜力，而不会增加出血风险，从而为新型抗血小板药物的开发铺平了道路。

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来源期刊

Platelets 医学-细胞生物学

CiteScore

6.70

自引率

3.00%

发文量

审稿时长

1 months

期刊介绍： Platelets is an international, peer-reviewed journal covering all aspects of platelet- and megakaryocyte-related research. Platelets provides the opportunity for contributors and readers across scientific disciplines to engage with new information about blood platelets. The journal’s Methods section aims to improve standardization between laboratories and to help researchers replicate difficult methods. Research areas include: Platelet function Biochemistry Signal transduction Pharmacology and therapeutics Interaction with other cells in the blood vessel wall The contribution of platelets and platelet-derived products to health and disease The journal publishes original articles, fast-track articles, review articles, systematic reviews, methods papers, short communications, case reports, opinion articles, commentaries, gene of the issue, and letters to the editor. Platelets operates a single-blind peer review policy. Authors can choose to publish gold open access in this journal.