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Evolutionarily conserved domains required for activation and repression functions of the Drosophila Hox protein Ultrabithorax.

机译:果蝇Hox蛋白Ultrabithorax的激活和阻遏功能所需的进化保守结构域。

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While testing the functions of deletion mutants in the Hox protein Ultrabithorax (Ubx), we found that the embryonic repression function of Ubx on Distal-less transcription in limb primordia is highly concentration dependent. The steep sigmoidal relationship between in vivo Ubx concentration and Distal-less repression is dependent on the Ubx YPWM motif. This suggests that Ubx cooperatively assembles a multi-protein repression complex on Distal-less regulatory DNA with the YPWM motif as a key protein-protein interface in this complex. Our deletion mutants also provide evidence for a transcriptional activation domain in the N-terminal 19 amino acids of Ubx. This proposed activation domain contains a variant of the SSYF motif that is found at the N termini of many Hox proteins, and is conserved in the activation domain of another Hox protein, Sex combs reduced. These results suggest that the N-terminal region containing the SSYF motif has been conserved in many Hox proteins for its role in transcriptional activation.
机译:在测试Hox蛋白Ultrabithorax(Ubx)中缺失突变体的功能时,我们发现Ubx对肢原基中的Distal-less转录的胚胎抑制功能高度依赖浓度。体内Ubx浓度与无远端抑制之间的陡峭S形关系取决于Ubx YPWM基序。这表明Ubx在无远距离的调控DNA上协同组装了多蛋白阻遏复合物,其中YPWM基序是该复合物中关键的蛋白-蛋白界面。我们的缺失突变体还提供了Ubx N末端19个氨基酸中转录激活域的证据。该提议的激活结构域包含SSYF基序的变体,该变体存在于许多Hox蛋白的N末端,并且在另一个Hox蛋白的激活结构域中保守,即性梳减少。这些结果表明,含有SSYF基序的N末端区域在许多Hox蛋白中由于其在转录激活中的作用而被保守。

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