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Solution structure of the TatB component of the twin-arginine translocation system

  • 影响因子:
    0.0
  • 发表刊物:
    Biochim Biophys Acta
  • 关键字:
    Membrane protein; NMR; Protein dynamics; Protein structure; Protein transport; Twin-arginine translocation (Tat)
  • 摘要:
    The twin-arginine protein transport (Tat) system translocates fully folded proteins across lipid membranes. In Escherichia coli, the Tat system comprises three essential components: TatA, TatB and TatC. The protein translocation process is proposed to initiate by signal peptide recognition and substrate binding to the TatBC complex. Upon formation of the TatBC-substrate protein complex, the TatA subunits are recruited and form the protein translocation pore. Experimental evidences suggest that TatB forms a tight complex with TatC at 1:1 molar ratio and the TatBC complex contains multiple copies of both proteins. Cross-linking experiments demonstrate that TatB functions in tetrameric units and interacts with both TatC and substrate proteins. However, structural information of the TatB protein is still lacking, and its functional mechanism remains elusive. Herein, we report the solution structure of TatB in DPC micelles determined by Nuclear Magnetic Resonance (NMR) spectroscopy. Overall, the structure shows an extended 'L-shape' conformation comprising four helices: a transmembrane helix (TMH) α1, an amphipathic helix (APH) α2, and two solvent exposed helices α3 and α4. The packing of TMH and APH is relatively rigid, whereas helices α3 and α4 display notably higher mobility. The observed floppiness of helices α3 and α4 allows TatB to sample a large conformational space, thus providing high structural plasticity to interact with substrate proteins of different sizes and shapes.
  • 论文类型:
    期刊论文
  • 论文编号:
    44
  • 卷号:
    1838
  • 期号:
    7
  • 页面范围:
    1881-1888
  • 是否译文:
  • 发表时间:
    2014-07-01
  • 收录刊物:
    SCI
  • 发布期刊链接:
  • 第一作者:
    Zhang Yi
  • 通讯作者:
    Jin Changwen
  • 全部作者:
    Wang Lei,Hu Yunfei