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Parallel dimerization of a PrrC-anticodon nuclease region implicated in tRNALys recognition

机译:牵连tRNALys识别的PrrC-反噬核酸酶区域的平行二聚化

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The optional Escherichia coli restriction tRNase PrrC represents a family of potential antiviral devices widespread among bacteria. PrrC comprises a functional C-domain of unknown structure and regulatory ABC/ATPase-like N-domain. The possible involvement of a C-domain sequence in tRNALys recognition was investigated using a matching end-protected 11-meric peptide. This mimic, termed here LARP (Lys-anticodon recognizing peptide) UV-cross-linked tRNALys anticodon stem-loop (ASL) analogs and inhibited their PrrC-catalyzed cleavage. Trimming LARP or introducing in it inactivating PrrC missense mutations impaired these activities. LARP appeared to mimic its matching protein sequence in ability to dimerize in parallel, as inferred from the following results. First, tethering Cys to the amino- or carboxy-end of LARP dramatically enhanced the ASL-cross-linking and PrrC-inhibiting activities under suitable redox conditions. Second, Cys-substitutions in a C-domain region containing the sequence corresponding to LARP elicited specific intersubunit cross-links. The parallel dimerization of PrrC's C-domains and expected head-to-tail dimerization of its N-domains further suggest that the NTPase and tRNALys-binding sites of PrrC arise during distinct assembly stages of its dimer of dimers form.
机译:可选的大肠杆菌限制性tRNase PrrC代表了在细菌中广泛分布的潜在抗病毒设备家族。 PrrC包含未知结构的功能性C结构域和调控性ABC / ATPase样N结构域。使用匹配的末端保护的11位肽,研究了C域序列可能参与tRNA Lys 识别的可能。该模拟物在这里称为LARP(Lys-反弓形虫识别肽)UV交联的tRNA Lys 反密码子茎环(ASL)类似物,并抑制了其PrrC催化的裂解。修剪LARP或将失活的PrrC错义突变引入其中会损害这些活性。 LARP似乎在平行二聚的能力上模仿了其匹配的蛋白质序列,如以下结果所示。首先,在合适的氧化还原条件下,将Cys束缚在LARP的氨基或羧基末端会大大增强ASL交联和PrrC抑制活性。第二,包含对应于LARP的序列的C结构域区域中的Cys取代引起特定的亚基交联。 PrrC的C结构域的平行二聚化和N结构域的预期的从头到尾的二聚化进一步表明,PrrC的NTPase和tRNA Lys 结合位点在其二聚体的不同组装阶段出现。二聚体形式。

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