Cloning, developmental expression, and evidence for alternative splicing of the murine tuberous sclerosis (TSC2) gene product.

K K Kim, L Pajak, H Wang, L J Field
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Abstract

Tuberous sclerosis (TS) is a genetically heterogeneous disease characterized by the widespread appearance of nonmalignant growths that affect multiple organ systems. A TS disease-determining gene, located at 16p13.3 and designated TSC2, has recently been cloned. In this report, the murine TSC2 homologue was cloned and characterized. cDNA clones encompassing the entire murine TSC2 transcript were isolated. Sequence analysis revealed a high degree of homology between the deduced amino acid sequence of the murine and human gene products. Northern blot surveys demonstrated widespread TSC2 expression which was subject to developmental regulation in a tissue-specific manner. Although high levels of TSC2 transcripts were observed in many adult tissues, protein analyses are required to determine whether functional tuberin protein is synthesized. Reverse transcription-polymerase chain reaction analyses identified at least six regions of alternative splicing, several of which modified putative regulatory motifs in the deduced amino acid structure of the TSC2 protein.

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小鼠结节性硬化症(TSC2)基因产物的克隆、发育表达和选择性剪接证据。
结节性硬化症(TS)是一种遗传异质性疾病,其特点是广泛出现影响多器官系统的非恶性生长。最近克隆出了位于16p13.3的TS疾病决定基因TSC2。本报告克隆并鉴定了小鼠TSC2同源基因。分离了包含整个小鼠TSC2转录物的cDNA克隆。序列分析表明,推导出的小鼠基因产物的氨基酸序列与人类基因产物具有高度的同源性。Northern blot调查显示,TSC2广泛表达,受组织特异性发育调节的影响。虽然在许多成人组织中观察到高水平的TSC2转录本,但需要进行蛋白质分析以确定是否合成了功能性结核菌素蛋白。逆转录-聚合酶链反应分析发现了至少6个选择性剪接区域,其中一些修改了推测的TSC2蛋白氨基酸结构中的调节基序。
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