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In vitro selection of ribozymes dependent on peptides for activity

机译:取决于活性的肽的核酶的体外选择

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A peptide-dependent ribozyme ligase (aptazyme ligase) has been selected from a random sequence population based on the small L1 ligase. The aptazyme ligase is activated > 18,000-fold by its cognate peptide effector, the HIV-1 Rev arginine-rich motif (ARM), and specifically recognizes the Rev ARM relative to other peptides containing arginine-rich motifs. Moreover, the aptazyme ligase can preferentially recognize the Rev ARM in the context of the full-length HIV-1 Rev protein. The only cross-reactivity exhibited by the aptazyme is toward the Tat ARM. Reselection of peptide- and protein-dependent aptazymes from a partially randomized population yielded aptazymes that could readily discriminate against the Tat ARM. These results have important implications for the development of aptazymes that can be used in arrays for the detection and quantitation of multiple cellular proteins (proteome arrays). [References: 42]
机译:基于小L1连接酶,从随机序列群体中选择了肽依赖性核酶连接酶(aptazyme连接酶)。 aptazyme连接酶被其同源肽效应物HIV-1 Rev富含精氨酸的基序(ARM)激活> 18,000倍,并且相对于其他含有富含精氨酸的基序的肽,可以特异性识别Rev ARM。此外,在全长HIV-1 Rev蛋白的背景下,适酶连接酶可以优先识别Rev ARM。 aptazyme表现出的唯一交叉反应是针对Tat ARM。从部分随机的群体中重新选择肽和蛋白质依赖性的aptazymes产生的aptazymes可以很容易地区别于Tat ARM。这些结果对可在阵列中用于检测和定量多种细胞蛋白(蛋白质组阵列)的aptazyme的开发具有重要意义。 [参考:42]

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