Trip13 Depletion in Liver Cancer Induces a Lipogenic Response Contributing to Plin2-Dependent Mitotic Cell Death

Marcos Rios Garcia; Bettina Meissburger; Jessica Chan; Roldan M. de Guia; Frits Mattijssen; Stephanie Roessler; Andreas L. Birkenfeld; Nathanael Raschzok; Fabien Riols; Janina Tokarz; Maude Giroud; Manuel Gil Lozano; Goetz Hartleben; Peter Nawroth; Mark Haid; Miguel López; Stephan Herzig; Mauricio Berriel Diaz

doi:10.1002/advs.202104291

Trip13 Depletion in Liver Cancer Induces a Lipogenic Response Contributing to Plin2-Dependent Mitotic Cell Death

Marcos Rios Garcia
, Bettina Meissburger
, Jessica Chan
, Roldan M. de Guia
, Frits Mattijssen
, Stephanie Roessler
, Andreas L. Birkenfeld
, Nathanael Raschzok
, Fabien Riols
, Janina Tokarz
, Maude Giroud
, Manuel Gil Lozano
, Goetz Hartleben
, Peter Nawroth
, Mark Haid
, Miguel López
, Stephan Herzig
, Mauricio Berriel Diaz

Life Sciences

Helmholtz Zentrum München German Research Center for Environmental Health
University Hospital Heidelberg
German Centre for Diabetes Research (DZD)
University of Santiago de Compostela
German Cancer Research Center
Institute of Diabetes and Metabolic Disease at the Helmholtz Center Munich
King's College London
Charite Universitätsmedizin Berlin
Heidelberg University
(CIBERobn)

Research output: Contribution to journal › Article › peer-review

28 Scopus citations

Abstract

Aberrant energy metabolism and cell cycle regulation both critically contribute to malignant cell growth and both processes represent targets for anticancer therapy. It is shown here that depletion of the AAA+-ATPase thyroid hormone receptor interacting protein 13 (Trip13) results in mitotic cell death through a combined mechanism linking lipid metabolism to aberrant mitosis. Diminished Trip13 levels in hepatocellular carcinoma cells result in insulin-receptor-/Akt-pathway-dependent accumulation of lipid droplets, which act as functional acentriolar microtubule organizing centers disturbing mitotic spindle polarity. Specifically, the lipid-droplet-coating protein perilipin 2 (Plin2) is required for multipolar spindle formation, induction of DNA damage, and mitotic cell death. Plin2 expression in different tumor cells confers susceptibility to cell death induced by Trip13 depletion as well as treatment with paclitaxel, a spindle-interfering drug commonly used against different cancers. Thus, assessment of Plin2 levels enables the stratification of tumor responsiveness to mitosis-targeting drugs, including clinically approved paclitaxel and Trip13 inhibitors currently under development.

Original language	English
Article number	2104291
Journal	Advanced Science
Volume	9
Issue number	29
DOIs	https://doi.org/10.1002/advs.202104291
State	Published - 14 Oct 2022

UN SDGs

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

SDG 3 Good Health and Well-being

Keywords

MTOCs
Plin2
Trip13
hepatocellular carcinoma
lipogenesis
mitosis
spindle assembly checkpoint

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10.1002/advs.202104291

Cite this

Rios Garcia, M., Meissburger, B., Chan, J., de Guia, R. M., Mattijssen, F., Roessler, S., Birkenfeld, A. L., Raschzok, N., Riols, F., Tokarz, J., Giroud, M., Gil Lozano, M., Hartleben, G., Nawroth, P., Haid, M., López, M., Herzig, S., & Berriel Diaz, M. (2022). Trip13 Depletion in Liver Cancer Induces a Lipogenic Response Contributing to Plin2-Dependent Mitotic Cell Death. Advanced Science, 9(29), Article 2104291. https://doi.org/10.1002/advs.202104291

@article{af874034364c4355b4ef54549e8ba389,

title = "Trip13 Depletion in Liver Cancer Induces a Lipogenic Response Contributing to Plin2-Dependent Mitotic Cell Death",

abstract = "Aberrant energy metabolism and cell cycle regulation both critically contribute to malignant cell growth and both processes represent targets for anticancer therapy. It is shown here that depletion of the AAA+-ATPase thyroid hormone receptor interacting protein 13 (Trip13) results in mitotic cell death through a combined mechanism linking lipid metabolism to aberrant mitosis. Diminished Trip13 levels in hepatocellular carcinoma cells result in insulin-receptor-/Akt-pathway-dependent accumulation of lipid droplets, which act as functional acentriolar microtubule organizing centers disturbing mitotic spindle polarity. Specifically, the lipid-droplet-coating protein perilipin 2 (Plin2) is required for multipolar spindle formation, induction of DNA damage, and mitotic cell death. Plin2 expression in different tumor cells confers susceptibility to cell death induced by Trip13 depletion as well as treatment with paclitaxel, a spindle-interfering drug commonly used against different cancers. Thus, assessment of Plin2 levels enables the stratification of tumor responsiveness to mitosis-targeting drugs, including clinically approved paclitaxel and Trip13 inhibitors currently under development.",

keywords = "MTOCs, Plin2, Trip13, hepatocellular carcinoma, lipogenesis, mitosis, spindle assembly checkpoint",

author = "\{Rios Garcia\}, Marcos and Bettina Meissburger and Jessica Chan and \{de Guia\}, \{Roldan M.\} and Frits Mattijssen and Stephanie Roessler and Birkenfeld, \{Andreas L.\} and Nathanael Raschzok and Fabien Riols and Janina Tokarz and Maude Giroud and \{Gil Lozano\}, Manuel and Goetz Hartleben and Peter Nawroth and Mark Haid and Miguel L{\'o}pez and Stephan Herzig and \{Berriel Diaz\}, Mauricio",

note = "Publisher Copyright: {\textcopyright} 2022 The Authors. Advanced Science published by Wiley-VCH GmbH.",

year = "2022",

month = oct,

day = "14",

doi = "10.1002/advs.202104291",

language = "English",

volume = "9",

journal = "Advanced Science",

issn = "2198-3844",

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Rios Garcia, M, Meissburger, B, Chan, J, de Guia, RM, Mattijssen, F, Roessler, S, Birkenfeld, AL, Raschzok, N, Riols, F, Tokarz, J, Giroud, M, Gil Lozano, M, Hartleben, G, Nawroth, P, Haid, M, López, M, Herzig, S & Berriel Diaz, M 2022, 'Trip13 Depletion in Liver Cancer Induces a Lipogenic Response Contributing to Plin2-Dependent Mitotic Cell Death', Advanced Science, vol. 9, no. 29, 2104291. https://doi.org/10.1002/advs.202104291

TY - JOUR

T1 - Trip13 Depletion in Liver Cancer Induces a Lipogenic Response Contributing to Plin2-Dependent Mitotic Cell Death

AU - Rios Garcia, Marcos

AU - Meissburger, Bettina

AU - Chan, Jessica

AU - de Guia, Roldan M.

AU - Mattijssen, Frits

AU - Roessler, Stephanie

AU - Birkenfeld, Andreas L.

AU - Raschzok, Nathanael

AU - Riols, Fabien

AU - Tokarz, Janina

AU - Giroud, Maude

AU - Gil Lozano, Manuel

AU - Hartleben, Goetz

AU - Nawroth, Peter

AU - Haid, Mark

AU - López, Miguel

AU - Herzig, Stephan

AU - Berriel Diaz, Mauricio

PY - 2022/10/14

Y1 - 2022/10/14

N2 - Aberrant energy metabolism and cell cycle regulation both critically contribute to malignant cell growth and both processes represent targets for anticancer therapy. It is shown here that depletion of the AAA+-ATPase thyroid hormone receptor interacting protein 13 (Trip13) results in mitotic cell death through a combined mechanism linking lipid metabolism to aberrant mitosis. Diminished Trip13 levels in hepatocellular carcinoma cells result in insulin-receptor-/Akt-pathway-dependent accumulation of lipid droplets, which act as functional acentriolar microtubule organizing centers disturbing mitotic spindle polarity. Specifically, the lipid-droplet-coating protein perilipin 2 (Plin2) is required for multipolar spindle formation, induction of DNA damage, and mitotic cell death. Plin2 expression in different tumor cells confers susceptibility to cell death induced by Trip13 depletion as well as treatment with paclitaxel, a spindle-interfering drug commonly used against different cancers. Thus, assessment of Plin2 levels enables the stratification of tumor responsiveness to mitosis-targeting drugs, including clinically approved paclitaxel and Trip13 inhibitors currently under development.

AB - Aberrant energy metabolism and cell cycle regulation both critically contribute to malignant cell growth and both processes represent targets for anticancer therapy. It is shown here that depletion of the AAA+-ATPase thyroid hormone receptor interacting protein 13 (Trip13) results in mitotic cell death through a combined mechanism linking lipid metabolism to aberrant mitosis. Diminished Trip13 levels in hepatocellular carcinoma cells result in insulin-receptor-/Akt-pathway-dependent accumulation of lipid droplets, which act as functional acentriolar microtubule organizing centers disturbing mitotic spindle polarity. Specifically, the lipid-droplet-coating protein perilipin 2 (Plin2) is required for multipolar spindle formation, induction of DNA damage, and mitotic cell death. Plin2 expression in different tumor cells confers susceptibility to cell death induced by Trip13 depletion as well as treatment with paclitaxel, a spindle-interfering drug commonly used against different cancers. Thus, assessment of Plin2 levels enables the stratification of tumor responsiveness to mitosis-targeting drugs, including clinically approved paclitaxel and Trip13 inhibitors currently under development.

KW - MTOCs

KW - Plin2

KW - Trip13

KW - hepatocellular carcinoma

KW - lipogenesis

KW - mitosis

KW - spindle assembly checkpoint

UR - https://www.scopus.com/pages/publications/85136967355

U2 - 10.1002/advs.202104291

DO - 10.1002/advs.202104291

M3 - Article

C2 - 36031387

AN - SCOPUS:85136967355

SN - 2198-3844

VL - 9

JO - Advanced Science

JF - Advanced Science

IS - 29

M1 - 2104291

ER -

Trip13 Depletion in Liver Cancer Induces a Lipogenic Response Contributing to Plin2-Dependent Mitotic Cell Death

Abstract

UN SDGs

Keywords

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