首页> 美国卫生研究院文献>Nucleic Acids Research >Position independent expression and developmental regulation is directed by the beta myosin heavy chain genes 5 upstream region in transgenic mice.
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Position independent expression and developmental regulation is directed by the beta myosin heavy chain genes 5 upstream region in transgenic mice.

机译:β肌球蛋白重链基因在转基因小鼠中的5上游区域指导位置无关的表达和发育调控。

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摘要

Transgenic mice generated with constructs containing 5.6 kb of the beta myosin heavy chain (MyHC) gene's 5' flanking region linked to the cat reporter gene express the transgene at high levels. In all 47 lines analyzed, tissue-specific accumulation of chloramphenicol acetyltransferase was found at levels proportional to the number of integrated transgene copies. Deletion constructs containing only 0.6 kb of 5' upstream region showed position effects in transgenic mice and did not demonstrate copy number dependence although transgene expression remained muscle-specific. The 5.6 kb 5' upstream region conferred appropriate developmental control of the transgene to the cardiac compartment and directs copy number dependent and position independent expression. Lines generated with a construct in which three proximal cis-acting elements were mutated showed reduced levels of transgene expression, but all maintained their position independence and copy number dependence, suggesting the presence of distinct regulatory mechanisms.
机译:用含有5.6 kbβ肌球蛋白重链(MyHC)基因与猫报道基因相连的5'侧翼区域的构建体产生的转基因小鼠高水平表达转基因。在所分析的所有47个品系中,发现氯霉素乙酰转移酶的组织特异性积累水平与整合的转基因拷贝数成正比。仅含有0.6kb的5'上游区域的缺失构建体在转基因小鼠中显示出位置效应,尽管转基因表达仍然是肌肉特异性的,但并未显示出拷贝数依赖性。 5.6kb 5′上游区域赋予转基因适当的发育控制到心脏区室,并指导拷贝数依赖性和位置依赖性表达。用其中三个近端顺式作用元件被突变的构建体产生的品系显示降低的转基因表达水平,但是全部维持其位置独立性和拷贝数依赖性,表明存在不同的调节机制。

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