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首页> 外文期刊>Molecular and Biochemical Parasitology >Selection for activation of a new variant surface glycoprotein gene expression site in Trypanosoma brucei can result in deletion of the old one.
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Selection for activation of a new variant surface glycoprotein gene expression site in Trypanosoma brucei can result in deletion of the old one.

机译:在布鲁氏锥虫中选择激活一个新的变异表面糖蛋白基因表达位点可以导致旧的缺失。

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摘要

The African trypanosome Trypanosoma brucei expresses the active variant surface glycoprotein (VSG) gene in a telomeric VSG gene expression site. We have generated trypanosomes with a neomycin resistance gene inserted behind an active VSG gene expression site promoter, and a hygromycin resistance gene behind a silent one. By alternating drug selection, we could select for trypanosomes that had switched between the two marked VSG gene expression sites. Surprisingly, trypanosomes that had activated a new VSG gene expression site had often lost the old one. Using polymerase chain reaction (PCR), we screened large numbers of switched trypanosomes and found that sequences lost invariably included the drug marker near the promoter, as well as the telomeric VSG gene many tens of kilobases away. We postulate that stable activation of a new expression site requires silencing of the old one. If silencing does not occur at a sufficient rate by normal switch-off, stable activation of the new site can only occur if the old site is lost in random deletion events. The fact that we pick up these normally infrequent deletions, indicates that inactivation of the old VSG expression site could be rate limiting during switching in our strain of T. brucei.
机译:非洲锥虫锥虫锥虫在端粒VSG基因表达位点表达活性变异表面糖蛋白(VSG)基因。我们已经产生了锥虫体,其中的新霉素抗性基因插入了活跃的VSG基因表达位点启动子后,而潮霉素抗性基因插入了沉默后的锥虫。通过交替选择药物,我们可以选择在两个标记的VSG基因表达位点之间切换的锥虫。令人惊讶的是,已经激活了新的VSG基因表达位点的锥虫常常丢失了旧的锥虫。使用聚合酶链反应(PCR),我们筛选了许多转换后的锥虫,发现丢失的序列总是包括启动子附近的药物标记,以及数十公里外的端粒VSG基因。我们假设新表达位点的稳定激活需要沉默旧表达位点。如果通过正常关闭无法以足够的速率进行沉默,则只有在随机删除事件中丢失了旧站点的情况下,才可以稳定激活新站点。我们挑选出这些通常不常见的缺失这一事实表明,在切换布鲁氏杆菌菌株期间,旧的VSG表达位点的失活可能是速率限制。

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