衰变加速因子
基因亚型
生物
选择性拼接
互补DNA
分子生物学
内含子
转染
糖基化
RNA剪接
克隆(编程)
中国仓鼠卵巢细胞
补体系统
分子克隆
基因
细胞生物学
遗传学
细胞培养
核糖核酸
抗体
计算机科学
程序设计语言
作者
Fumihiko Osuka,Yuichi Endo,Mitsunori Higuchi,Hiroyuki Suzuki,Yutaka Shio,Koichi Fujiu,Ryuzo Kanno,Akio Oishi,Masanori Terashima,Teizo Fujita,Mitsukazu Gotoh
出处
期刊:Genomics
[Elsevier]
日期:2006-09-01
卷期号:88 (3): 316-322
被引量:17
标识
DOI:10.1016/j.ygeno.2006.01.006
摘要
Decay-accelerating factor (DAF) is one of the complement regulatory proteins. Two isoforms of DAF have been identified in humans. In this study, we isolated novel cDNAs encoding five isoforms of DAF from the human lung, which were generated by insertion of new exonic sequences. RT-PCR revealed that all isoforms were expressed in almost all tissues tested, although the expression patterns and levels differed among the tissues. Transfection of isoform vDAF1, 2, and 3 cDNAs into CHO cells showed that these molecules are soluble forms secreted after glycosylation. Isoform vDAF4 and vDAF5 cDNAs included a part of and the entire intron 7 sequence, respectively, and the transfection of vDAF4 cDNA produced a large, glycosylated, membrane-bound form. These results suggest that more than seven isoforms of human DAF are involved in the regulation of complement activation under physiological conditions through their specific structures and localization.
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