Plectin-mediated cytoskeletal crosstalk as a target for inhibition of hepatocellular carcinoma growth and metastasis

Zuzana Outla; Gizem Oyman-Eyrilmez; Katerina Korelova; Magdalena Prechova; Lukas Frick; Lenka Sarnova; Piyush Bisht; Petra Novotna; Jan Kosla; Patricia Janker-Bortel; Yasmin Borutzki; Andrea Bileck; Christopher Gerner; Mohammad Rahbari; Nuh Rahbari; Emrullah Birgin; Bibiana Kvasnicova; Andrea Galisova; Katerina Sulkova; Andreas Bauer; Njainday Jobe; Ondrej Tolde; Eva Sticova; Daniel Rösel; Tracy O'Connor; Martin Otahal; Daniel Jirak; Mathias Heikenwälder; Gerhard Wiche; Samuel M. Meier-Menches; Martin Gregor

doi:10.7554/eLife.102205

Plectin-mediated cytoskeletal crosstalk as a target for inhibition of hepatocellular carcinoma growth and metastasis

Zuzana Outla
, Gizem Oyman-Eyrilmez
, Katerina Korelova
, Magdalena Prechova
, Lukas Frick
, Lenka Sarnova
, Piyush Bisht
, Petra Novotna
, Jan Kosla
, Patricia Janker-Bortel
, Yasmin Borutzki
, Andrea Bileck
, Christopher Gerner
, Mohammad Rahbari
, Nuh Rahbari
, Emrullah Birgin
, Bibiana Kvasnicova
, Andrea Galisova
, Katerina Sulkova
, Andreas Bauer

Njainday Jobe, Ondrej Tolde, Eva Sticova, Daniel Rösel, Tracy O'Connor, Martin Otahal, Daniel Jirak, Mathias Heikenwälder, Gerhard Wiche, Samuel M. Meier-Menches, Martin Gregor (Corresponding author)

Publications: Contribution to journal › Article › Peer Reviewed

Abstract

The most common primary malignancy of the liver, hepatocellular carcinoma (HCC), is a heterogeneous tumor entity with high metastatic potential and complex pathophysiology. Increasing evidence suggests that tissue mechanics plays a critical role in tumor onset and progression. Here, we show that plectin, a major cytoskeletal crosslinker protein, plays a crucial role in mechanical homeostasis and mechanosensitive oncogenic signaling that drives hepatocarcinogenesis. Our expression analyses revealed elevated plectin levels in liver tumors, which correlated with poor prognosis for HCC patients. Using autochthonous and orthotopic mouse models we demonstrated that genetic and pharmacological inactivation of plectin potently suppressed the initiation and growth of HCC. Moreover, plectin targeting potently inhibited the invasion potential of human HCC cells and reduced their metastatic outgrowth in the lung. Proteomic and phosphoproteomic profiling linked plectin-dependent disruption of cytoskeletal networks to attenuation of oncogenic FAK, MAPK/Erk, and PI3K/Akt signatures. Importantly, by combining cell line-based and murine HCC models, we show that plectin inhibitor plecstatin-1 (PST) is well-tolerated and potently inhibits HCC progression. In conclusion, our study demonstrates that plectin-controlled cytoarchitecture is a key determinant of HCC development and suggests that pharmacologically induced disruption of mechanical homeostasis may represent a new therapeutic strategy for HCC treatment.

Original language	English
Journal	eLife
Volume	13
DOIs	https://doi.org/10.7554/eLife.102205
Publication status	Published - 7 Mar 2025

UN SDGs

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

SDG 3 Good Health and Well-being

Austrian Fields of Science 2012

301904 Cancer research
301303 Medical biochemistry
301306 Medical molecular biology

Keywords

cancer biology
cell biology
cytoskeletal crosstalk
hepatocellular carcinoma
metastasis
mouse
plecstatin
plectin
therapeutic strategy

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10.7554/eLife.102205

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Outla, Z., Oyman-Eyrilmez, G., Korelova, K., Prechova, M., Frick, L., Sarnova, L., Bisht, P., Novotna, P., Kosla, J., Janker-Bortel, P., Borutzki, Y., Bileck, A., Gerner, C., Rahbari, M., Rahbari, N., Birgin, E., Kvasnicova, B., Galisova, A., Sulkova, K., ... Gregor, M. (2025). Plectin-mediated cytoskeletal crosstalk as a target for inhibition of hepatocellular carcinoma growth and metastasis. eLife, 13. https://doi.org/10.7554/eLife.102205

@article{ed1ad16092ae4851bfb82eac8f078a02,

title = "Plectin-mediated cytoskeletal crosstalk as a target for inhibition of hepatocellular carcinoma growth and metastasis",

abstract = "The most common primary malignancy of the liver, hepatocellular carcinoma (HCC), is a heterogeneous tumor entity with high metastatic potential and complex pathophysiology. Increasing evidence suggests that tissue mechanics plays a critical role in tumor onset and progression. Here, we show that plectin, a major cytoskeletal crosslinker protein, plays a crucial role in mechanical homeostasis and mechanosensitive oncogenic signaling that drives hepatocarcinogenesis. Our expression analyses revealed elevated plectin levels in liver tumors, which correlated with poor prognosis for HCC patients. Using autochthonous and orthotopic mouse models we demonstrated that genetic and pharmacological inactivation of plectin potently suppressed the initiation and growth of HCC. Moreover, plectin targeting potently inhibited the invasion potential of human HCC cells and reduced their metastatic outgrowth in the lung. Proteomic and phosphoproteomic profiling linked plectin-dependent disruption of cytoskeletal networks to attenuation of oncogenic FAK, MAPK/Erk, and PI3K/Akt signatures. Importantly, by combining cell line-based and murine HCC models, we show that plectin inhibitor plecstatin-1 (PST) is well-tolerated and potently inhibits HCC progression. In conclusion, our study demonstrates that plectin-controlled cytoarchitecture is a key determinant of HCC development and suggests that pharmacologically induced disruption of mechanical homeostasis may represent a new therapeutic strategy for HCC treatment.",

keywords = "cancer biology, cell biology, cytoskeletal crosstalk, hepatocellular carcinoma, metastasis, mouse, plecstatin, plectin, therapeutic strategy",

author = "Zuzana Outla and Gizem Oyman-Eyrilmez and Katerina Korelova and Magdalena Prechova and Lukas Frick and Lenka Sarnova and Piyush Bisht and Petra Novotna and Jan Kosla and Patricia Janker-Bortel and Yasmin Borutzki and Andrea Bileck and Christopher Gerner and Mohammad Rahbari and Nuh Rahbari and Emrullah Birgin and Bibiana Kvasnicova and Andrea Galisova and Katerina Sulkova and Andreas Bauer and Njainday Jobe and Ondrej Tolde and Eva Sticova and Daniel R{\"o}sel and Tracy O'Connor and Martin Otahal and Daniel Jirak and Mathias Heikenw{\"a}lder and Gerhard Wiche and Meier-Menches, \{Samuel M.\} and Martin Gregor",

note = "Publisher Copyright: {\textcopyright} 2024, Outla et al. Accession Number WOS:001439805900001 PubMed ID 40052672",

year = "2025",

month = mar,

day = "7",

doi = "10.7554/eLife.102205",

language = "English",

volume = "13",

journal = "eLife",

issn = "2050-084X",

publisher = "ELIFE SCIENCES PUBLICATIONS LTD",

}

Outla, Z, Oyman-Eyrilmez, G, Korelova, K, Prechova, M, Frick, L, Sarnova, L, Bisht, P, Novotna, P, Kosla, J, Janker-Bortel, P, Borutzki, Y, Bileck, A , Gerner, C, Rahbari, M, Rahbari, N, Birgin, E, Kvasnicova, B, Galisova, A, Sulkova, K, Bauer, A, Jobe, N, Tolde, O, Sticova, E, Rösel, D, O'Connor, T, Otahal, M, Jirak, D, Heikenwälder, M, Wiche, G, Meier-Menches, SM & Gregor, M 2025, 'Plectin-mediated cytoskeletal crosstalk as a target for inhibition of hepatocellular carcinoma growth and metastasis', eLife, vol. 13. https://doi.org/10.7554/eLife.102205

TY - JOUR

T1 - Plectin-mediated cytoskeletal crosstalk as a target for inhibition of hepatocellular carcinoma growth and metastasis

AU - Outla, Zuzana

AU - Oyman-Eyrilmez, Gizem

AU - Korelova, Katerina

AU - Prechova, Magdalena

AU - Frick, Lukas

AU - Sarnova, Lenka

AU - Bisht, Piyush

AU - Novotna, Petra

AU - Kosla, Jan

AU - Janker-Bortel, Patricia

AU - Borutzki, Yasmin

AU - Bileck, Andrea

AU - Gerner, Christopher

AU - Rahbari, Mohammad

AU - Rahbari, Nuh

AU - Birgin, Emrullah

AU - Kvasnicova, Bibiana

AU - Galisova, Andrea

AU - Sulkova, Katerina

AU - Bauer, Andreas

AU - Jobe, Njainday

AU - Tolde, Ondrej

AU - Sticova, Eva

AU - Rösel, Daniel

AU - O'Connor, Tracy

AU - Otahal, Martin

AU - Jirak, Daniel

AU - Heikenwälder, Mathias

AU - Wiche, Gerhard

AU - Meier-Menches, Samuel M.

AU - Gregor, Martin

PY - 2025/3/7

Y1 - 2025/3/7

N2 - The most common primary malignancy of the liver, hepatocellular carcinoma (HCC), is a heterogeneous tumor entity with high metastatic potential and complex pathophysiology. Increasing evidence suggests that tissue mechanics plays a critical role in tumor onset and progression. Here, we show that plectin, a major cytoskeletal crosslinker protein, plays a crucial role in mechanical homeostasis and mechanosensitive oncogenic signaling that drives hepatocarcinogenesis. Our expression analyses revealed elevated plectin levels in liver tumors, which correlated with poor prognosis for HCC patients. Using autochthonous and orthotopic mouse models we demonstrated that genetic and pharmacological inactivation of plectin potently suppressed the initiation and growth of HCC. Moreover, plectin targeting potently inhibited the invasion potential of human HCC cells and reduced their metastatic outgrowth in the lung. Proteomic and phosphoproteomic profiling linked plectin-dependent disruption of cytoskeletal networks to attenuation of oncogenic FAK, MAPK/Erk, and PI3K/Akt signatures. Importantly, by combining cell line-based and murine HCC models, we show that plectin inhibitor plecstatin-1 (PST) is well-tolerated and potently inhibits HCC progression. In conclusion, our study demonstrates that plectin-controlled cytoarchitecture is a key determinant of HCC development and suggests that pharmacologically induced disruption of mechanical homeostasis may represent a new therapeutic strategy for HCC treatment.

AB - The most common primary malignancy of the liver, hepatocellular carcinoma (HCC), is a heterogeneous tumor entity with high metastatic potential and complex pathophysiology. Increasing evidence suggests that tissue mechanics plays a critical role in tumor onset and progression. Here, we show that plectin, a major cytoskeletal crosslinker protein, plays a crucial role in mechanical homeostasis and mechanosensitive oncogenic signaling that drives hepatocarcinogenesis. Our expression analyses revealed elevated plectin levels in liver tumors, which correlated with poor prognosis for HCC patients. Using autochthonous and orthotopic mouse models we demonstrated that genetic and pharmacological inactivation of plectin potently suppressed the initiation and growth of HCC. Moreover, plectin targeting potently inhibited the invasion potential of human HCC cells and reduced their metastatic outgrowth in the lung. Proteomic and phosphoproteomic profiling linked plectin-dependent disruption of cytoskeletal networks to attenuation of oncogenic FAK, MAPK/Erk, and PI3K/Akt signatures. Importantly, by combining cell line-based and murine HCC models, we show that plectin inhibitor plecstatin-1 (PST) is well-tolerated and potently inhibits HCC progression. In conclusion, our study demonstrates that plectin-controlled cytoarchitecture is a key determinant of HCC development and suggests that pharmacologically induced disruption of mechanical homeostasis may represent a new therapeutic strategy for HCC treatment.

KW - cancer biology

KW - cell biology

KW - cytoskeletal crosstalk

KW - hepatocellular carcinoma

KW - metastasis

KW - mouse

KW - plecstatin

KW - plectin

KW - therapeutic strategy

UR - https://www.scopus.com/pages/publications/86000695128

U2 - 10.7554/eLife.102205

DO - 10.7554/eLife.102205

M3 - Article

C2 - 40052672

AN - SCOPUS:86000695128

SN - 2050-084X

VL - 13

JO - eLife

JF - eLife

ER -

Plectin-mediated cytoskeletal crosstalk as a target for inhibition of hepatocellular carcinoma growth and metastasis

Abstract

UN SDGs

Austrian Fields of Science 2012

Keywords

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