Plecstatin inhibits hepatocellular carcinoma tumorigenesis and invasion through cytolinker plectin

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Abstract

Plecstatin (PST) is a potent anticancer agent in preclinical models, yet its precise mechanism of action and molecular specificity regarding its main targets, plectin and outer dense fiber protein 2 (ODF2), remain incompletely understood. Here, we dissected PST's mode of action using knockouts of plectin (PLEC) and ODF2 in SNU-475 hepatocellular carcinoma (HCC) cells. PST suppressed anchorage-independent growth and impaired 2D and 3D migration in a dose-dependent manner in both wild-type and ODF2-deficient cells, but not in PLEC-deficient cells, establishing plectin as the principal effector of PST's antitumor activity. Proteomic and functional analyses revealed that PST primarily disrupts cytoskeletal remodeling through plectin, while selectively affecting ciliogenesis-related pathways linked to ODF2 loss. Deletion of either protein attenuated PST-induced Ser51 phosphorylation of eIF2α, ATF4/GADD34 induction, and cytochrome c release, indicating cooperative involvement in integrated stress response (ISR). Correlative analysis of patient datasets confirmed associations between PLEC/ODF2 expression and ISR-related gene signatures, supporting the clinical relevance of this pathway. Together, these findings identify plectin as a key target of PST in disrupting cytoskeletal integrity and establish plectin/ODF2 axis in PST-driven stress adaptation in HCC.

Original languageEnglish
JournalMolecular Oncology
DOIs
Publication statusE-pub ahead of print - Dec 2025

Funding

FundersFunder number
Grant Agency of the Czech RepublicGA21-21736S, GA25-15690S
Czech Academy of SciencesRVO 68378050
European Union Next Generation EULX22NPO5102

    UN SDGs

    This output contributes to the following UN Sustainable Development Goals (SDGs)

    1. SDG 3 - Good Health and Well-being
      SDG 3 Good Health and Well-being

    Austrian Fields of Science 2012

    • 301306 Medical molecular biology
    • 302055 Oncology
    • 301904 Cancer research

    Keywords

    • hepatocellular carcinoma
    • ODF2
    • organometallic compounds
    • plecstatin
    • plectin
    • therapeutic target

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