效应器
配对
细胞生物学
基因亚型
生物
计算机科学
计算生物学
基因
遗传学
物理
超导电性
量子力学
作者
Aida S. Hansen,Bettina Bundgaard,Bjarne Kuno Møller,Per Höllsberg
摘要
CD46 is a glycoprotein with important functions in innate and adaptive immune responses. Functionally different isoforms are generated by alternative splicing at exons 7-9 (BC and C isoforms) and exon 13 (CYT-1 and CYT-2 isoforms) giving rise to BC1, BC2, C1 and C2. We developed a novel real-time PCR assay that allows quantitative comparisons between these isoforms. Their relative frequency in CD4 +T cells from 100 donors revealed a distribution with high interpersonally variability. Importantly, the distribution between the isoforms was not random and although splicing favoured inclusion of exon 8 (BC isoforms), exclusion of exon 8 (C isoforms) was significantly linked to exclusion of exon 13 (CYT-2 isoforms). Despite inter-individual differences, CD4 + and CD8 +T cells, B cells, NK cells and monocytes expressed similar isoform profiles intra-individually. However, memory/effector CD4 +T cells had a significantly higher frequency of CYT-2 when compared with naïve CD4 +T cells. Likewise, in vitro activation of naïve and total CD4 +T cells increased the expression of CYT-2. This indicates that although splicing factors determine a certain expression profile in an individual, the profile can be modulated by external stimuli. This suggests a mechanism by which alterations in CD46 isoforms may temporarily regulate the immune response.
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