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无副作用的凝血酶抑制类肝素模拟物的合成。

Synthesis of thrombin-inhibiting heparin mimetics without side effects.

作者信息

Petitou M, Hérault J P, Bernat A, Driguez P A, Duchaussoy P, Lormeau J C, Herbert J M

机构信息

Sanofi Recherche, Toulouse, France.

出版信息

Nature. 1999 Apr 1;398(6726):417-22. doi: 10.1038/18877.

Abstract

Unwanted side effects of pharmacologically active compounds can usually be eliminated by structural modifications. But the complex heterogeneous structure of the polysaccharide heparin has limited this approach to fragmentation, leading to slightly better-tolerated heparin preparations of low molecular mass. Despite this improvement, heparin-induced thrombocytopaenia (HIT), related to an interaction with platelet factor 4 (PF4) and, to a lesser extent, haemorrhages, remain significant side effects of heparinotherapy. Breakthroughs in oligosaccharide chemistry made possible the total synthesis of the pentasaccharide antithrombin-binding site of heparin. This pentasaccharide represents a new family of potential antithrombotic drugs, devoid of thrombin inhibitory properties, and free of undesired interactions with blood and vessel components. To obtain more potent and well-tolerated antithrombotic drugs, we wished to synthesize heparin mimetics able to inhibit thrombin, that is, longer oligosaccharides. Like thrombin inhibition, undesired interactions are directly correlated to the charge and the size of the molecules, so we had to design structures that were able to discriminate between thrombin and other proteins, particularly PF4. Here we describe the use of multistep converging synthesis to obtain sulphated oligosaccharides that meet these requirements.

摘要

药理活性化合物的不良副作用通常可以通过结构修饰来消除。但多糖肝素复杂的异质结构限制了这种碎片化方法,仅得到了耐受性稍好的低分子质量肝素制剂。尽管有了这种改进,与血小板因子4(PF4)相互作用相关的肝素诱导的血小板减少症(HIT)以及程度较轻的出血,仍然是肝素治疗的显著副作用。寡糖化学的突破使肝素的五糖抗凝血酶结合位点的全合成成为可能。这种五糖代表了一类新的潜在抗血栓药物,没有凝血酶抑制特性,也没有与血液和血管成分的不良相互作用。为了获得更有效且耐受性良好的抗血栓药物,我们希望合成能够抑制凝血酶的肝素模拟物,即更长的寡糖。与凝血酶抑制一样,不良相互作用与分子的电荷和大小直接相关,因此我们必须设计出能够区分凝血酶和其他蛋白质,特别是PF4的结构。在此我们描述了使用多步汇聚合成法来获得满足这些要求的硫酸化寡糖。

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