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多糖-抗体缀合物对细胞因子的结合。

Cytokine binding by polysaccharide-antibody conjugates.

机构信息

Departments of Biomedical Engineering and Chemistry, Carnegie Mellon University, Pittsburgh, PA 15213, USA.

出版信息

Mol Pharm. 2010 Oct 4;7(5):1769-77. doi: 10.1021/mp100150z. Epub 2010 Sep 1.

Abstract

Cytokine-neutralizing antibodies are used in treating a broad range of inflammatory conditions. We demonstrate that monoclonal antibodies against interleukin-1β and tumor necrosis factor-α were still active when conjugated to high molecular weight polysaccharides. These polysaccharides are hydrophilic, but their size makes them unable to circulate in the bloodstream when delivered to tissues, opening up the possibility of localized treatment of inflammatory conditions. To explore this new class of protein-polysaccharide conjugates, we covalently modified interleukin-1β and tumor necrosis factor-α monoclonal antibodies with high molecular weight hyaluronic acid and carboxymethylcellulose. Rigorous purification using dialysis with a 300 kDa-cutoff membrane removed unconjugated monoclonal antibodies. We characterized the composition of the constructs and demonstrated using molecular binding affinity measurements and cell assays that the conjugates were capable of binding proinflammatory cytokines. The binding affinities of both the unconjugated antibodies for their cytokines were measured to be approximately 120 pM. While all conjugates had pM-level binding constants, they ranged from 40 pM for the hyaluronic acid-(anti-interleukin-1β) conjugate to 412 pM for the carboxymethylcellulose-(anti-interleukin-1β) conjugate. Interestingly, the dissociation time constants varied more than the association time constants, suggesting that conjugation to a high molecular weight polysaccharide did not interfere with the formation of the antibody-cytokine complex but could stabilize or destabilize it once formed. Conjugation of cytokine-neutralizing antibodies to high molecular weight polymers represents a novel method of delivering anticytokine therapeutics that may avoid many of the complications associated with systemic delivery.

摘要

细胞因子中和抗体被广泛用于治疗各种炎症性疾病。我们证明,当与高分子量多糖结合时,针对白细胞介素-1β和肿瘤坏死因子-α的单克隆抗体仍然具有活性。这些多糖具有亲水性,但由于其尺寸较大,当递送到组织时无法在血液中循环,从而为炎症性疾病的局部治疗开辟了可能性。为了探索这种新的蛋白-多糖缀合物,我们用高分子量透明质酸和羧甲基纤维素对白细胞介素-1β和肿瘤坏死因子-α单克隆抗体进行了共价修饰。使用 300 kDa 截止膜进行透析的严格纯化去除了未结合的单克隆抗体。我们对构建物的组成进行了表征,并通过分子结合亲和力测量和细胞测定证明,缀合物能够结合促炎细胞因子。测量了未缀合的抗体与其细胞因子的结合亲和力,结果表明,两种抗体的亲和力约为 120 pM。虽然所有缀合物的结合常数都在 pM 级,但范围从透明质酸-(抗白细胞介素-1β)缀合物的 40 pM 到羧甲基纤维素-(抗白细胞介素-1β)缀合物的 412 pM。有趣的是,解离时间常数的变化大于结合时间常数的变化,这表明与高分子量多糖的缀合不会干扰抗体-细胞因子复合物的形成,但一旦形成,可能会稳定或不稳定该复合物。将细胞因子中和抗体与高分子量聚合物缀合代表了一种递送抗细胞因子治疗剂的新方法,这种方法可能会避免与全身递送相关的许多并发症。

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