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抗生素AGPM生物合成途径的初步研究 总被引:5,自引:0,他引:5
采用前体添加实验法、静息细胞培养法以及酶抑制剂法对藤黄灰链霉菌中抗生素AG PM生物合成途径进行了初步探讨。研究表明能转化成聚酮合成所需活性前体的氨基酸如异亮氨酸、缬氨酸、蛋氨酸、谷氨酸等以及短链脂肪酸乙酸、丙酸、丁酸盐对抗生素AGPM合成均有明显促进作用 ;另外 ,在培养基中添加脂肪酸和聚酮生物合成途径的专一性抑制剂浅蓝菌素 (2 5μg mL)或脂肪酸合成抑制剂碘乙酰胺 (0 5mmol L)时 ,菌体生长不受影响 ,而抗生素AGPM合成受到强烈抑制 ,分别为对照的 35 3 %和 2 6 2 % ; 相似文献
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Christian Laing Segun Jung Abdul Iqbal Tamar Schlick 《Journal of molecular biology》2009,393(1):67-82
RNA junctions are secondary-structure elements formed when three or more helices come together. They are present in diverse RNA molecules with various fundamental functions in the cell. To better understand the intricate architecture of three-dimensional (3D) RNAs, we analyze currently solved 3D RNA junctions in terms of base-pair interactions and 3D configurations. First, we study base-pair interaction diagrams for solved RNA junctions with 5 to 10 helices and discuss common features. Second, we compare these higher-order junctions to those containing 3 or 4 helices and identify global motif patterns such as coaxial stacking and parallel and perpendicular helical configurations. These analyses show that higher-order junctions organize their helical components in parallel and helical configurations similar to lower-order junctions. Their sub-junctions also resemble local helical configurations found in three- and four-way junctions and are stabilized by similar long-range interaction preferences such as A-minor interactions. Furthermore, loop regions within junctions are high in adenine but low in cytosine, and in agreement with previous studies, we suggest that coaxial stacking between helices likely forms when the common single-stranded loop is small in size; however, other factors such as stacking interactions involving noncanonical base pairs and proteins can greatly determine or disrupt coaxial stacking. Finally, we introduce the ribo-base interactions: when combined with the along-groove packing motif, these ribo-base interactions form novel motifs involved in perpendicular helix-helix interactions. Overall, these analyses suggest recurrent tertiary motifs that stabilize junction architecture, pack helices, and help form helical configurations that occur as sub-elements of larger junction networks. The frequent occurrence of similar helical motifs suggest nature's finite and perhaps limited repertoire of RNA helical conformation preferences. More generally, studies of RNA junctions and tertiary building blocks can ultimately help in the difficult task of RNA 3D structure prediction. 相似文献
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