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含有与人类绒毛膜促性腺激素β羧基末端的β亚基嵌合体的重组促甲状腺素具有生物活性,血浆半衰期延长:碳水化合物在生物活性和代谢清除中的作用。

Recombinant thyrotropin containing a beta-subunit chimera with the human chorionic gonadotropin-beta carboxy-terminus is biologically active, with a prolonged plasma half-life: role of carbohydrate in bioactivity and metabolic clearance.

作者信息

Joshi L, Murata Y, Wondisford F E, Szkudlinski M W, Desai R, Weintraub B D

机构信息

Molecular and Cellular Endocrinology Branch, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

Endocrinology. 1995 Sep;136(9):3839-48. doi: 10.1210/endo.136.9.7544273.

Abstract

Recombinant TSH is now successfully being used in clinical studies of thyroid cancer. Because of its therapeutic potential, we have constructed a longer acting analog of TSH by fusing the carboxy-terminal extension peptide (CTEP) of hCG beta onto TSH beta. When coexpressed either with alpha-subunit complementary DNA or alpha minigene in African green monkey (COS-7) and human embryonic kidney (293) cells, the chimera was fully bioactive in vitro and exhibited enhanced in vivo potency associated with a prolonged plasma half-life. The addition of 25 amino acids with 4 O-linked oligosaccharide chains did not affect the assembly and secretion of chimeric TSH. Wild-type (WT) and chimeric TSH secreted by COS-7 and 293 cells displayed wide differences in their plasma half-lives, presumably due to the presence of terminal sialic acid and SO4 on their oligosaccharide chains, respectively. Chimeric and WT TSH secreted by both cell lines demonstrated similar bioactivity in cAMP production, with some differences in [3H]thymidine incorporation. Chimeric TSH appears to be more effective in COS-7 cells than in 293 cells, as judged by growth assay. COS-7-produced chimeric TSH showed the maximum increase in half-life, indicating the importance of sialic acid in prolonging half-life and in vivo potency. Sulfation of both subunits, predominantly beta and to a lesser extent alpha, appears to be responsible at least in part for the increased metabolic clearance of WT and chimeric TSH secreted by 293 cells. Apart from its therapeutic potential, chimeric TSH produced in various cell lines can be used as a tool to delineate the roles of sulfate and sialic acid in the in vivo clearance and, thereby, the in vivo bioactivity.

摘要

重组促甲状腺激素(TSH)目前已成功应用于甲状腺癌的临床研究。鉴于其治疗潜力,我们通过将人绒毛膜促性腺激素β亚基的羧基末端延伸肽(CTEP)与TSHβ亚基融合,构建了一种作用时间更长的TSH类似物。当与α亚基互补DNA或α小基因在非洲绿猴(COS-7)和人胚肾(293)细胞中共表达时,该嵌合体在体外具有完全的生物活性,并且在体内表现出增强的效力以及延长的血浆半衰期。添加带有4条O-连接寡糖链的25个氨基酸并不影响嵌合TSH的组装和分泌。COS-7和293细胞分泌的野生型(WT)和嵌合TSH在血浆半衰期上表现出很大差异,推测分别是由于其寡糖链上存在末端唾液酸和硫酸根。两种细胞系分泌的嵌合TSH和WT TSH在cAMP产生方面表现出相似的生物活性,但在[3H]胸苷掺入方面存在一些差异。通过生长试验判断,嵌合TSH在COS-7细胞中似乎比在293细胞中更有效。COS-7产生的嵌合TSH半衰期增加最大,表明唾液酸在延长半衰期和体内效力方面的重要性。两个亚基的硫酸化,主要是β亚基,α亚基程度较轻,似乎至少部分负责293细胞分泌的WT和嵌合TSH代谢清除率的增加。除了其治疗潜力外,在各种细胞系中产生的嵌合TSH可作为一种工具,用于阐明硫酸根和唾液酸在体内清除以及体内生物活性中的作用。

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