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重组II型胶原蛋白的特性:DBA/1小鼠中的致关节炎性和耐受性

Characterization of recombinant type II collagen: arthritogenicity and tolerogenicity in DBA/1 mice.

作者信息

Myers L K, Brand D D, Ye X J, Cremer M A, Rosloniec E F, Bodo M, Myllyharju J, Helaakoski T, Nokelainen M, Pihlajaniemi T, Kivirikko K, Yang C L, Ala-Kokko L, Prockop D J, Notbohm H, Fietzek P, Stuart J M, Kang A H

机构信息

Departments of Pediatrics and Medicine, University of Tennessee, Memphis, TN, USA.

出版信息

Immunology. 1998 Dec;95(4):631-9. doi: 10.1046/j.1365-2567.1998.00637.x.

Abstract

Recombinant human type II collagen (rhCII) was produced using both the HT1080 mammalian cell expression system (rhCIIht) and a baculovirus expression system (rhCIIbac). The biosynthesis of CII requires extensive post-translational modifications, such as the hydroxylation of prolyl and lysyl residues and glycosylation of hydroxylysyl residues. Amino acid analyses indicated that the rhCIIbac was adequately hydroxylated at prolyl residues but underhydroxylated at lysyl residues and underglycosylated compared with tissue-derived hCII, while rhCIIht was hyperhydroxylated and hyperglycosylated at lysyl residues. When the murine collagen-induced arthritis (CIA) model was used to investigate the immunological properties of the two forms of recombinant CII, each induced a high incidence of arthritis following immunization of susceptible mice when emulsified with complete Freund's adjuvant (CFA). However, the severity of the arthritis, as assessed by the number of affected limbs, was significantly higher in mice immunized with rhCIIht than in mice immunized with rhCIIbac. These data indicate that the degree of hydroxylysine glycosylation may play a role in the induction of the arthritogenic response to CII. Each of the recombinant collagens was comparable to tissue-derived hCII in their ability to induce tolerance and suppress arthritis when given as intravenous or oral tolerogens. Taken together, our data suggest that recombinant CII can be prepared in adequate amounts for therapeutic uses and that the material is immunologically comparable to tissue-derived hCII when used to induce tolerance.

摘要

重组人II型胶原蛋白(rhCII)通过HT1080哺乳动物细胞表达系统(rhCIIht)和杆状病毒表达系统(rhCIIbac)生产。II型胶原蛋白的生物合成需要广泛的翻译后修饰,如脯氨酰和赖氨酰残基的羟基化以及羟赖氨酰残基的糖基化。氨基酸分析表明,与组织来源的hCII相比,rhCIIbac脯氨酰残基的羟基化程度足够,但赖氨酰残基的羟基化不足且糖基化不足,而rhCIIht在赖氨酰残基上过度羟基化和过度糖基化。当使用小鼠胶原诱导性关节炎(CIA)模型研究两种形式的重组CII的免疫学特性时,每种与完全弗氏佐剂(CFA)乳化后免疫易感小鼠,均诱导出高发病率的关节炎。然而,通过受影响肢体的数量评估,用rhCIIht免疫的小鼠的关节炎严重程度明显高于用rhCIIbac免疫的小鼠。这些数据表明,羟赖氨酰糖基化程度可能在对CII的致关节炎反应诱导中起作用。当作为静脉内或口服耐受原给予时,每种重组胶原蛋白在诱导耐受和抑制关节炎的能力方面与组织来源的hCII相当。综上所述,我们的数据表明,可以制备足够量的重组CII用于治疗用途,并且当用于诱导耐受时,该材料在免疫学上与组织来源的hCII相当。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/449c/1364363/1a939c6017d0/immunology00039-0135-a.jpg

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