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MCM1的DNA结合和寡聚化结构域足以使其与其他调控蛋白相互作用。

The DNA binding and oligomerization domain of MCM1 is sufficient for its interaction with other regulatory proteins.

作者信息

Primig M, Winkler H, Ammerer G

机构信息

Research Institute of Molecular Pathology, Vienna, Austria.

出版信息

EMBO J. 1991 Dec;10(13):4209-18. doi: 10.1002/j.1460-2075.1991.tb04999.x.

Abstract

The MCM1 gene encodes an essential DNA binding protein that, in cooperation with the transactivators alpha 1 and STE12 and the repressor alpha 2, confers mating specificity to haploid yeast cells. We show that the amino-terminal third of the MCM1 protein is sufficient for the physical interaction with these factors. A strain expressing just 98 amino acids encompassing the oligomerization and DNA binding domains of MCM1 is viable and mating competent. This motif exhibits considerable similarity to a domain of the mammalian transcription factor SRF. A 98 amino acid hybrid gene coding for the MCM1 DNA binding domain and SRF dimerization domain is sufficient for viability but not for the expression of mating type specific genes. In vitro binding studies suggest that a region of approximately 50 amino acids of MCM1 is essential for providing contacts with alpha 1, alpha 2 and STE12.

摘要

MCM1基因编码一种必需的DNA结合蛋白,该蛋白与反式激活因子α1和STE12以及阻遏因子α2协同作用,赋予单倍体酵母细胞交配特异性。我们发现,MCM1蛋白氨基末端的三分之一足以与这些因子进行物理相互作用。仅表达包含MCM1寡聚化和DNA结合结构域的98个氨基酸的菌株是有活力的且具有交配能力。该基序与哺乳动物转录因子SRF的一个结构域具有相当大的相似性。编码MCM1 DNA结合结构域和SRF二聚化结构域的98个氨基酸的杂交基因足以维持细胞活力,但不足以用于交配型特异性基因的表达。体外结合研究表明,MCM1大约50个氨基酸的区域对于与α1、α2和STE12建立联系至关重要。

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