Targeting LINC00673 expression triggers cellular senescence in lung cancer

Anna Roth; Karine Boulay; Matthias Groß; Maria Polycarpou-Schwarz; Frédérick A. Mallette; Marine Regnier; Or Bida; Doron Ginsberg; Arne Warth; Philipp A. Schnabel; Thomas Muley; Michael Meister; Heike Zabeck; Hans Hoffmann; Sven Diederichs

doi:10.1080/15476286.2018.1553481

Targeting LINC00673 expression triggers cellular senescence in lung cancer

Anna Roth
, Karine Boulay
, Matthias Groß
, Maria Polycarpou-Schwarz
, Frédérick A. Mallette
, Marine Regnier
, Or Bida
, Doron Ginsberg
, Arne Warth
, Philipp A. Schnabel
, Thomas Muley
, Michael Meister
, Heike Zabeck
, Hans Hoffmann
, Sven Diederichs

Department of Surgery

German Cancer Research Center
Université de Montréal
Bar Ilan University
University Hospital Heidelberg
member of the German Centre for lung Research (DZL)
Saarland University Medical Center
Thoraxklinik at the University Hospital Heidelberg
University of Freiburg

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

28 Scopus citations

Abstract

Aberrant expression of noncoding RNAs plays a critical role during tumorigenesis. To uncover novel functions of long non-coding RNA (lncRNA) in lung adenocarcinoma, we used a microarray-based screen identifying LINC00673 with elevated expression in matched tumor versus normal tissue. We report that loss of LINC00673 is sufficient to trigger cellular senescence, a tumor suppressive mechanism associated with permanent cell cycle arrest, both in lung cancer and normal cells in a p53-dependent manner. LINC00673-depleted cells fail to efficiently transit from G1- to S-phase. Using a quantitative proteomics approach, we confirm the modulation of senescence-associated genes as a result of LINC00673 knockdown. In addition, we uncover that depletion of p53 in normal and tumor cells is sufficient to overcome LINC00673-mediated cell cycle arrest and cellular senescence. Furthermore, we report that overexpression of LINC00673 reduces p53 translation and contributes to the bypass of Ras-induced senescence. In summary, our findings highlight LINC00673 as a crucial regulator of proliferation and cellular senescence in lung cancer.

Original language	English
Pages (from-to)	1499-1511
Number of pages	13
Journal	RNA Biology
Volume	15
Issue number	12
DOIs	https://doi.org/10.1080/15476286.2018.1553481
State	Published - 2 Dec 2018

UN SDGs

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

SDG 3 Good Health and Well-being

Keywords

LINC00673
long noncoding RNA
lung cancer
p53
senescence

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10.1080/15476286.2018.1553481

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title = "Targeting LINC00673 expression triggers cellular senescence in lung cancer",

abstract = "Aberrant expression of noncoding RNAs plays a critical role during tumorigenesis. To uncover novel functions of long non-coding RNA (lncRNA) in lung adenocarcinoma, we used a microarray-based screen identifying LINC00673 with elevated expression in matched tumor versus normal tissue. We report that loss of LINC00673 is sufficient to trigger cellular senescence, a tumor suppressive mechanism associated with permanent cell cycle arrest, both in lung cancer and normal cells in a p53-dependent manner. LINC00673-depleted cells fail to efficiently transit from G1- to S-phase. Using a quantitative proteomics approach, we confirm the modulation of senescence-associated genes as a result of LINC00673 knockdown. In addition, we uncover that depletion of p53 in normal and tumor cells is sufficient to overcome LINC00673-mediated cell cycle arrest and cellular senescence. Furthermore, we report that overexpression of LINC00673 reduces p53 translation and contributes to the bypass of Ras-induced senescence. In summary, our findings highlight LINC00673 as a crucial regulator of proliferation and cellular senescence in lung cancer.",

keywords = "LINC00673, long noncoding RNA, lung cancer, p53, senescence",

author = "Anna Roth and Karine Boulay and Matthias Gro{\ss} and Maria Polycarpou-Schwarz and Mallette, \{Fr{\'e}d{\'e}rick A.\} and Marine Regnier and Or Bida and Doron Ginsberg and Arne Warth and Schnabel, \{Philipp A.\} and Thomas Muley and Michael Meister and Heike Zabeck and Hans Hoffmann and Sven Diederichs",

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T1 - Targeting LINC00673 expression triggers cellular senescence in lung cancer

AU - Roth, Anna

AU - Boulay, Karine

AU - Groß, Matthias

AU - Polycarpou-Schwarz, Maria

AU - Mallette, Frédérick A.

AU - Regnier, Marine

AU - Bida, Or

AU - Ginsberg, Doron

AU - Warth, Arne

AU - Schnabel, Philipp A.

AU - Muley, Thomas

AU - Meister, Michael

AU - Zabeck, Heike

AU - Hoffmann, Hans

AU - Diederichs, Sven

PY - 2018/12/2

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N2 - Aberrant expression of noncoding RNAs plays a critical role during tumorigenesis. To uncover novel functions of long non-coding RNA (lncRNA) in lung adenocarcinoma, we used a microarray-based screen identifying LINC00673 with elevated expression in matched tumor versus normal tissue. We report that loss of LINC00673 is sufficient to trigger cellular senescence, a tumor suppressive mechanism associated with permanent cell cycle arrest, both in lung cancer and normal cells in a p53-dependent manner. LINC00673-depleted cells fail to efficiently transit from G1- to S-phase. Using a quantitative proteomics approach, we confirm the modulation of senescence-associated genes as a result of LINC00673 knockdown. In addition, we uncover that depletion of p53 in normal and tumor cells is sufficient to overcome LINC00673-mediated cell cycle arrest and cellular senescence. Furthermore, we report that overexpression of LINC00673 reduces p53 translation and contributes to the bypass of Ras-induced senescence. In summary, our findings highlight LINC00673 as a crucial regulator of proliferation and cellular senescence in lung cancer.

AB - Aberrant expression of noncoding RNAs plays a critical role during tumorigenesis. To uncover novel functions of long non-coding RNA (lncRNA) in lung adenocarcinoma, we used a microarray-based screen identifying LINC00673 with elevated expression in matched tumor versus normal tissue. We report that loss of LINC00673 is sufficient to trigger cellular senescence, a tumor suppressive mechanism associated with permanent cell cycle arrest, both in lung cancer and normal cells in a p53-dependent manner. LINC00673-depleted cells fail to efficiently transit from G1- to S-phase. Using a quantitative proteomics approach, we confirm the modulation of senescence-associated genes as a result of LINC00673 knockdown. In addition, we uncover that depletion of p53 in normal and tumor cells is sufficient to overcome LINC00673-mediated cell cycle arrest and cellular senescence. Furthermore, we report that overexpression of LINC00673 reduces p53 translation and contributes to the bypass of Ras-induced senescence. In summary, our findings highlight LINC00673 as a crucial regulator of proliferation and cellular senescence in lung cancer.

KW - LINC00673

KW - long noncoding RNA

KW - lung cancer

KW - p53

KW - senescence

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DO - 10.1080/15476286.2018.1553481

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SP - 1499

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JO - RNA Biology

JF - RNA Biology

IS - 12

ER -

Targeting LINC00673 expression triggers cellular senescence in lung cancer

Abstract

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Keywords

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