4.8 Article

N-terminus-independent activation of c-Src via binding to a tetraspan(in) TM4SF5 in hepatocellular carcinoma is abolished by the TM4SF5 C-terminal peptide application

THERANOSTICS (2021)

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Journal

THERANOSTICS
Volume 11, Issue 16, Pages 8092-8111

Publisher

IVYSPRING INT PUBL
DOI: 10.7150/thno.58739

Keywords

c-Src; metastasis; protein-protein interaction; PTPIB; TM4SF5

Categories

Medicine, Research & Experimental

Funding

  1. Basic Science Research Program through the National Research Foundation of Korea (NRF) - Ministry of Science, ICT & Future Planning [NRF-2020R1I1A1A01070020, NRF-2018 M3A9C8020027, NRF2020R1A2C3008993, NRF-2021M3A9D3024752]
  2. Mid-career Researcher Program - Ministry of Science and ICT (MSIT) [NRF2020R1A2C2101636]
  3. Medical Research Center (MRC) grant - Ministry of Science and ICT (MSIT) [2018R1A5A2025286]
  4. Bio & Medical Technology Development Program - Ministry of Science and ICT (MSIT) [NRF-2019M3E5D4065251]
  5. Ministry of Health and Welfare (MOHW) through the National Research Foundation of Korea (NRF)
  6. National Research Foundation of Korea [2021M3A9D3024752] Funding Source: Korea Institute of Science & Technology Information (KISTI), National Science & Technology Information Service (NTIS)

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The study revealed that the binding of the TM4SF5 C-terminus to the kinase domain of inactive c-Src leads to its activation. Cell-penetrating peptides containing the TM4SF5 C-terminus can block the interaction of TM4SF5 with c-Src, preventing the initiation and progression of hepatocellular carcinoma.
Active c-Src non-receptor tyrosine kinase localizes to the plasma membrane via N-terminal lipid modification. Membranous c-Src causes cancer initiation and progression. Even though transmembrane 4 L six family member 5 (TM4SF5), a tetraspan(in), can be involved in this mechanism, the molecular and structural influence of TM4SF5 on c-Src remains unknown. Methods: Here, we investigated molecular and structural details by which TM4SF5 regulated c-Src devoid of its N-terminus and how cell-penetrating peptides were able to interrupt c-Src activation via interference of c-Src-TM4SF5 interaction in hepatocellular carcinoma models. Results: The TM4SF5 C-terminus efficiently bound the c-Src SH1 kinase domain, efficiently to the inactively-closed form. The complex involved protein tyrosine phosphatase 1B able to dephosphorylate Tyr530. The c-Src SH1 domain alone, even in a closed form, bound TM4SF5 to cause c-Src Tyr419 and FAK Y861 phosphorylation. Homology modeling and molecular dynamics simulation studies predicted the directly interfacing residues, which were further validated by mutational studies. Cell penetration of TM4SF5 C-terminal peptides blocked the interaction of TM4SF5 with c-Src and prevented c-Src-dependent tumor initiation and progression in vivo. Conclusions: Collectively, these data demonstrate that binding of the TM4SF5 C-terminus to the kinase domain of inactive c-Src leads to its activation. Because this binding can be abolished by cell-penetrating peptides containing the TM4SF5 C-terminus, targeting this direct interaction may be an effective strategy for developing therapeutics that block the development and progression of hepatocellular carcinoma.

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