NOTCH1 mediates a switch between two distinct secretomes during senescence

Matthew Hoare; Yoko Ito; Tae Won Kang; Michael P. Weekes; Nicholas J. Matheson; Daniel A. Patten; Shishir Shetty; Aled J. Parry; Suraj Menon; Rafik Salama; Robin Antrobus; Kosuke Tomimatsu; William Howat; Paul J. Lehner; Lars Zender; Masashi Narita

doi:10.1038/ncb3397

NOTCH1 mediates a switch between two distinct secretomes during senescence

Matthew Hoare, Yoko Ito, Tae Won Kang, Michael P. Weekes, Nicholas J. Matheson, Daniel A. Patten, Shishir Shetty, Aled J. Parry, Suraj Menon, Rafik Salama, Robin Antrobus, Kosuke Tomimatsu, William Howat, Paul J. Lehner, Lars Zender, Masashi Narita

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

282 Citations (Scopus)

Abstract

Senescence, a persistent form of cell-cycle arrest, is often associated with a diverse secretome, which provides complex functionality for senescent cells within the tissue microenvironment. We show that oncogene-induced senescence is accompanied by a dynamic fluctuation of NOTCH1 activity, which drives a TGF-β-rich secretome, while suppressing the senescence-associated pro-inflammatory secretome through inhibition of C/EBPβ. NOTCH1 and NOTCH1-driven TGF-β contribute to 'lateral induction of senescence' through a juxtacrine NOTCH-JAG1 pathway. In addition, NOTCH1 inhibition during senescence facilitates upregulation of pro-inflammatory cytokines, promoting lymphocyte recruitment and senescence surveillance in vivo. As enforced activation of NOTCH1 signalling confers a near mutually exclusive secretory profile compared with typical senescence, our data collectively indicate that the dynamic alteration of NOTCH1 activity during senescence dictates a functional balance between these two distinct secretomes: one representing TGF-β and the other pro-inflammatory cytokines, highlighting that NOTCH1 is a temporospatial controller of secretome composition.

Original language	English
Pages (from-to)	979-992
Number of pages	14
Journal	Nature Cell Biology
Volume	18
Issue number	9
DOIs	https://doi.org/10.1038/ncb3397
Publication status	Published - Sept 1 2016
Externally published	Yes

All Science Journal Classification (ASJC) codes

Cell Biology

Access to Document

10.1038/ncb3397

Cite this

@article{567abdfb640a46f690f791e5795a7d19,

title = "NOTCH1 mediates a switch between two distinct secretomes during senescence",

abstract = "Senescence, a persistent form of cell-cycle arrest, is often associated with a diverse secretome, which provides complex functionality for senescent cells within the tissue microenvironment. We show that oncogene-induced senescence is accompanied by a dynamic fluctuation of NOTCH1 activity, which drives a TGF-β-rich secretome, while suppressing the senescence-associated pro-inflammatory secretome through inhibition of C/EBPβ. NOTCH1 and NOTCH1-driven TGF-β contribute to 'lateral induction of senescence' through a juxtacrine NOTCH-JAG1 pathway. In addition, NOTCH1 inhibition during senescence facilitates upregulation of pro-inflammatory cytokines, promoting lymphocyte recruitment and senescence surveillance in vivo. As enforced activation of NOTCH1 signalling confers a near mutually exclusive secretory profile compared with typical senescence, our data collectively indicate that the dynamic alteration of NOTCH1 activity during senescence dictates a functional balance between these two distinct secretomes: one representing TGF-β and the other pro-inflammatory cytokines, highlighting that NOTCH1 is a temporospatial controller of secretome composition.",

author = "Matthew Hoare and Yoko Ito and Kang, {Tae Won} and Weekes, {Michael P.} and Matheson, {Nicholas J.} and Patten, {Daniel A.} and Shishir Shetty and Parry, {Aled J.} and Suraj Menon and Rafik Salama and Robin Antrobus and Kosuke Tomimatsu and William Howat and Lehner, {Paul J.} and Lars Zender and Masashi Narita",

note = "Publisher Copyright: {\textcopyright} 2016 Macmillan Publishers Limited, part of Springer Nature.",

year = "2016",

month = sep,

day = "1",

doi = "10.1038/ncb3397",

language = "English",

volume = "18",

pages = "979--992",

journal = "Nature Cell Biology",

issn = "1465-7392",

publisher = "Nature Publishing Group",

number = "9",

}

TY - JOUR

T1 - NOTCH1 mediates a switch between two distinct secretomes during senescence

AU - Hoare, Matthew

AU - Ito, Yoko

AU - Kang, Tae Won

AU - Weekes, Michael P.

AU - Matheson, Nicholas J.

AU - Patten, Daniel A.

AU - Shetty, Shishir

AU - Parry, Aled J.

AU - Menon, Suraj

AU - Salama, Rafik

AU - Antrobus, Robin

AU - Tomimatsu, Kosuke

AU - Howat, William

AU - Lehner, Paul J.

AU - Zender, Lars

AU - Narita, Masashi

PY - 2016/9/1

Y1 - 2016/9/1

N2 - Senescence, a persistent form of cell-cycle arrest, is often associated with a diverse secretome, which provides complex functionality for senescent cells within the tissue microenvironment. We show that oncogene-induced senescence is accompanied by a dynamic fluctuation of NOTCH1 activity, which drives a TGF-β-rich secretome, while suppressing the senescence-associated pro-inflammatory secretome through inhibition of C/EBPβ. NOTCH1 and NOTCH1-driven TGF-β contribute to 'lateral induction of senescence' through a juxtacrine NOTCH-JAG1 pathway. In addition, NOTCH1 inhibition during senescence facilitates upregulation of pro-inflammatory cytokines, promoting lymphocyte recruitment and senescence surveillance in vivo. As enforced activation of NOTCH1 signalling confers a near mutually exclusive secretory profile compared with typical senescence, our data collectively indicate that the dynamic alteration of NOTCH1 activity during senescence dictates a functional balance between these two distinct secretomes: one representing TGF-β and the other pro-inflammatory cytokines, highlighting that NOTCH1 is a temporospatial controller of secretome composition.

AB - Senescence, a persistent form of cell-cycle arrest, is often associated with a diverse secretome, which provides complex functionality for senescent cells within the tissue microenvironment. We show that oncogene-induced senescence is accompanied by a dynamic fluctuation of NOTCH1 activity, which drives a TGF-β-rich secretome, while suppressing the senescence-associated pro-inflammatory secretome through inhibition of C/EBPβ. NOTCH1 and NOTCH1-driven TGF-β contribute to 'lateral induction of senescence' through a juxtacrine NOTCH-JAG1 pathway. In addition, NOTCH1 inhibition during senescence facilitates upregulation of pro-inflammatory cytokines, promoting lymphocyte recruitment and senescence surveillance in vivo. As enforced activation of NOTCH1 signalling confers a near mutually exclusive secretory profile compared with typical senescence, our data collectively indicate that the dynamic alteration of NOTCH1 activity during senescence dictates a functional balance between these two distinct secretomes: one representing TGF-β and the other pro-inflammatory cytokines, highlighting that NOTCH1 is a temporospatial controller of secretome composition.

UR - http://www.scopus.com/inward/record.url?scp=84982133301&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=84982133301&partnerID=8YFLogxK

U2 - 10.1038/ncb3397

DO - 10.1038/ncb3397

M3 - Article

C2 - 27525720

AN - SCOPUS:84982133301

SN - 1465-7392

VL - 18

SP - 979

EP - 992

JO - Nature Cell Biology

JF - Nature Cell Biology

IS - 9

ER -

NOTCH1 mediates a switch between two distinct secretomes during senescence

Abstract

All Science Journal Classification (ASJC) codes

Access to Document

Other files and links

Fingerprint

Cite this