Myc基本结构域高度保守的天冬酰胺在DNA结合、转化和细胞凋亡中是必不可少的

Stephan Bodis , Timothy Hemesath , David E. Fisher
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引用次数: 1

摘要

c-Myc和其他含有基本螺旋-环-螺旋(b-HLH)的蛋白质的基本区域与回文DNA序列CANNTG结合。对于肌生成因子MyoD, b-HLH家族的一员,几个基本区域残基的突变会消除肌肉分化,但不会消除DNA结合。MyoD中显示这种行为的一个氨基酸位置与Myc中高度保守的天冬酰胺一致。这种保守的天冬酰胺表现出完全耐受丙氨酸取代的DNA结合测量。为了验证Myc基本区是否编码第二种生物学功能的可能性,我们将c-Myc中保守的天冬酰胺(N360)突变为丙氨酸,并测试了Myc依赖的细胞转化和凋亡功能。与MyoD中此类突变的有害影响相反,丙氨酸突变体在myc依赖性细胞转化和诱导凋亡方面功能正常。因此,与DNA结合不同的基本区域功能可能不是HLH转录因子的一般特征。
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Highly Conserved Asparagine in the Basic Domain of Myc Is Dispensable for DNA Binding, Transformation, and Apoptosis

The basic region of c-Myc and other basic helix–loop–helix (b-HLH)-containing proteins bind to the palindromic DNA sequences CANNTG. For the myogenic factor MyoD, a member of the b-HLH family, mutation of several basic region residues abrogates muscle differentiation, but not DNA binding. One of the amino acid positions displaying this behavior in MyoD aligns with a highly conserved asparagine in Myc. This conserved asparagine displays complete tolerance for alanine substitution as measured by DNA binding. To test the possibility of whether the basic region of Myc encodes a second biological function, the conserved asparagine in c-Myc (N360) was mutated to alanine and tested for the Myc-dependent functions of cellular transformation and apoptosis. In contrast to the deleterious effects of such mutations in MyoD, the alanine mutant functions normally for both Myc-dependent cellular transformation and apoptosis induction. Therefore, a basic region function distinct from DNA binding may not be a general feature of HLH transcription factors.

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