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首页> 外文期刊>Glycobiology >Delta inulin: a novel, immunologically active, stable packing structure comprising β-d-[2 → 1] poly(fructo-furanosyl) α-d-glucosen polymers
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Delta inulin: a novel, immunologically active, stable packing structure comprising β-d-[2 → 1] poly(fructo-furanosyl) α-d-glucosen polymers

机译:三角菊粉:一种新颖的,具有免疫活性的稳定包装结构,包含β-d-[2→1]聚(果糖呋喃糖基)α-d-葡萄糖苷聚合物

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摘要

We report a novel isoform of β-d-[2 → 1] poly(fructo-furanosyl) α-d-glucose termed delta inulin (DI), comparing it with previously described alpha (AI), beta (BI) and gamma (GI) isoforms. In vitro, DI is the most immunologically active weight/weight in human complement activation and in binding to monocytes and regulating their chemokine production and cell surface protein expression. In vivo, this translates into potent immune adjuvant activity, enhancing humoral and cellular responses against co-administered antigens. As a biocompatible polysaccharide particle, DI is safe and well tolerated by subcutaneous or intramuscular injection. Physico-chemically, DI forms as an insoluble precipitate from an aqueous solution of suitable AI, BI or GI held at 37–48°C, whereas the precipitate from the same solution at lower temperatures has the properties of AI or GI. DI can also be produced by heat conversion of GI suspensions at 56°C, whereas GI is converted from AI at 45°C. DI is distinguished from GI by its higher temperature of solution in dilute aqueous suspension and by its lower solubility in dimethyl sulfoxide, both consistent with greater hydrogen bonding in DI's polymer packing structure. DI suspensions can be dissolved by heat, re-precipitated by cooling as AI and finally re-converted back to DI by repeated heat treatment. Thus, DI, like the previously described inulin isoforms, reflects the formation of a distinct polymer aggregate packing structure via reversible noncovalent bonding. DI forms the basis for a potent new human vaccine adjuvant and further swells the growing family of carbohydrate structures with immunological activity.
机译:我们报告了一种新型的β-d-[2→1]聚果糖呋喃糖基α-d-葡萄糖同种型,称为δ菊粉(DI),并将其与先前描述的alpha(AI),beta(BI)和γ( GI)亚型。在体外,DI是人类补体激活以及与单核细胞结合并调节其趋化因子产生和细胞表面蛋白表达方面最具免疫活性的重量/重量。在体内,这转化为有效的免疫佐剂活性,增强了针对共同施用的抗原的体液和细胞应答。作为一种生物相容性多糖颗粒,DI是安全的,并且可以通过皮下或肌内注射耐受。物理化学上,DI是在适当的AI,BI或GI水溶液(保持于37-48°C)下以不溶性沉淀形式形成的,而同一溶液在较低温度下的沉淀具有AI或GI的性质。 DI也可以通过在56°C下对GI悬浮液进行热转化来生产,而GI在45°C下由AI转化而来。 DI与GI的区别在于其在稀水悬浮液中的较高溶液温度和在二甲基亚砜中的较低溶解度,这两者都与DI的聚合物堆积结构中的氢键更大有关。 DI悬浮液可以通过加热溶解,通过冷却以AI的形式重新沉淀,最后通过重复热处理将其重新转化为DI。因此,DI,如先前所述的菊粉同工型一样,通过可逆的非共价键反映了独特的聚合物聚集体堆积结构的形成。 DI构成了有效的新型人类疫苗佐剂的基础,并进一步扩大了具有免疫活性的碳水化合物结构家族。

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  • 来源
    《Glycobiology》 |2011年第5期|p.595-606|共12页
  • 作者

    Nikolai Petrovsky;

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    Vaxine Pty Ltd, Flinders Medical Centre, @%@, Australia @%@, Australian National University Medical School, The Canberra Hospital, @%@ (P.D.C.);

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