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Antitumor properties of a new non-anticoagulant heparin analog from the mollusk Nodipecten nodosus: Effect on P-selectin, heparanase, metastasis and cellular recruitment

机译:软体动物Nodipecten nodosus的新型非抗凝肝素类似物的抗肿瘤特性:对P-选择素,乙酰肝素酶,转移和细胞募集的影响

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Inflammation and cancer are related pathologies acting synergistically to promote tumor progression. In both, hematogenous metastasis and inflammation, P-selectin participates in interactions involving tumor cells, platelets, leukocytes and endothelium. Heparin has been shown to inhibit P-selectin and as a consequence it blunts metastasis and inflammation. Some heparin analogs obtained from marine invertebrates are P-selectin inhibitors and do not induce bleeding effects. The present work focuses on the P-selectin blocking activity of a unique heparan sulfate (HS) from the bivalve mollusk Nodipecten nodosus. Initially, we showed that the mollusk HS inhibited LS180 colon carcinoma cell adhesion to immobilized P-selectin in a dose-dependent manner. In addition, we demonstrated that this glycan attenuates leukocyte rolling on activated endothelium and inflammatory cell recruitment in thioglycollate-induced peritonitis in mice. Biochemical analysis indicated that the invertebrate glycan also inhibits heparanase, a key player in cell invasion and metastasis. Experimental metastasis of Lewis lung carcinoma cells was drastically attenuated by the mollusk HS through a mechanism involving inhibition of platelet-tumor-cell complex formation in blood vessels. These data suggest that the mollusk HS is a potential alternative to heparin for inhibiting P-selectin-mediated events such as metastasis and inflammatory cell recruitment.
机译:炎症和癌症是协同作用以促进肿瘤进展的相关病理。在血源性转移和炎症中,P-选择蛋白均参与涉及肿瘤细胞,血小板,白细胞和内皮的相互作用。肝素已显示出抑制P-选择素的作用,并因此抑制了转移和炎症。从海洋无脊椎动物获得的一些肝素类似物是P-选择素抑制剂,不会引起出血作用。目前的工作集中在双壳贝类软体动物Nodipecten nodosus独特的硫酸乙酰肝素(HS)的P-选择素阻断活性。最初,我们显示了软体动物HS以剂量依赖的方式抑制LS180结肠癌细胞对固定化P-选择素的粘附。此外,我们证明了这种聚糖可减轻白细胞在激活的内皮细胞上的滚动以及在硫代乙醇酸酯诱导的小鼠腹膜炎中炎症细胞募集的过程。生化分析表明,无脊椎动物聚糖还抑制乙酰肝素酶,乙酰肝素酶是细胞入侵和转移的关键因素。软体动物HS通过抑制血管中血小板-肿瘤-细胞复合物形成的机制,使Lewis肺癌细胞的实验转移大大减弱。这些数据表明,软体动物HS是肝素的潜在替代品,可抑制P-选择素介导的事件(如转移和炎症细胞募集)。

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