Compressive stress-mediated p38 activation required for ERα + phenotype in breast cancer

Pauliina M. Munne; Lahja Martikainen; Iiris Räty; Kia Bertula; null Nonappa; Janika Ruuska; Hanna Ala-Hongisto; Aino Peura; Babette Hollmann; Lilya Euro; Kerim Yavuz; Linda Patrikainen; Maria Salmela; Juho Pokki; Mikko Kivento; Juho Väänänen; Tomi Suomi; Liina Nevalaita; Minna Mutka; Panu Kovanen; Marjut Leidenius; Tuomo Meretoja; Katja Hukkinen; Outi Monni; Jeroen Pouwels; Biswajyoti Sahu; Johanna Mattson; Heikki Joensuu; Päivi Heikkilä; Laura L. Elo; Ciara Metcalfe; Melissa R. Junttila; Olli Ikkala; Juha Klefström

doi:10.1038/s41467-021-27220-9

Compressive stress-mediated p38 activation required for ERα + phenotype in breast cancer

Pauliina M. Munne, Lahja Martikainen, Iiris Räty, Kia Bertula, Nonappa, Janika Ruuska, Hanna Ala-Hongisto, Aino Peura, Babette Hollmann, Lilya Euro, Kerim Yavuz, Linda Patrikainen, Maria Salmela, Juho Pokki, Mikko Kivento, Juho Väänänen, Tomi Suomi, Liina Nevalaita, Minna Mutka, Panu KovanenMarjut Leidenius, Tuomo Meretoja, Katja Hukkinen, Outi Monni, Jeroen Pouwels, Biswajyoti Sahu, Johanna Mattson, Heikki Joensuu, Päivi Heikkilä, Laura L. Elo, Ciara Metcalfe, Melissa R. Junttila, Olli Ikkala, Juha Klefström^*

^*Tämän työn vastaava kirjoittaja

Tutkimustuotos: Lehtiartikkeli › Article › Scientific › vertaisarvioitu

13 Sitaatiot (Scopus)

43 Lataukset (Pure)

Abstrakti

Breast cancer is now globally the most frequent cancer and leading cause of women’s death. Two thirds of breast cancers express the luminal estrogen receptor-positive (ERα + ) phenotype that is initially responsive to antihormonal therapies, but drug resistance emerges. A major barrier to the understanding of the ERα-pathway biology and therapeutic discoveries is the restricted repertoire of luminal ERα + breast cancer models. The ERα + phenotype is not stable in cultured cells for reasons not fully understood. We examine 400 patient-derived breast epithelial and breast cancer explant cultures (PDECs) grown in various three-dimensional matrix scaffolds, finding that ERα is primarily regulated by the matrix stiffness. Matrix stiffness upregulates the ERα signaling via stress-mediated p38 activation and H3K27me3-mediated epigenetic regulation. The finding that the matrix stiffness is a central cue to the ERα phenotype reveals a mechanobiological component in breast tissue hormonal signaling and enables the development of novel therapeutic interventions. Subject terms: ER-positive (ER + ), breast cancer, ex vivo model, preclinical model, PDEC, stiffness, p38 SAPK.

Alkuperäiskieli	Englanti
Artikkeli	6967
Sivut	1-17
Sivumäärä	17
Julkaisu	Nature Communications
Vuosikerta	12
Numero	1
DOI - pysyväislinkit	https://doi.org/10.1038/s41467-021-27220-9
Tila	Julkaistu - 29 marrask. 2021
OKM-julkaisutyyppi	A1 Julkaistu artikkeli, soviteltu

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10.1038/s41467-021-27220-9Lisenssi: CC BY

Compressive stress-mediated p38 activation required for ERα + phenotype in breast cancerFinal published version, 29,5 MBLisenssi: CC BY

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PreClinica: Novel Preclinical Model for Breast Cancer Theraphy
Nonappa, N., Bertula, K. & Heilala, M.
01/09/2017 → 30/09/2020
Projekti: Business Finland: New business from research ideas (TUTLI)
HYBER: Suomen Akatemian Biosynteettisten hybridimateriaalien molekyylimuokkauksen huippuyksikkö (2014-2019)
Ikkala, O., Morits, M., Rissanen, S., Nonappa, N., Sanchez Sanchez, A., Bertula, K., Cherian, T., Haataja, J., Toivonen, M., Poutanen, M., Sohrabi, F., Hynninen, V. & Myllymäki, T.
01/01/2017 → 31/12/2019
Projekti: Academy of Finland: Other research funding

OtaNano
Anna Rissanen (Manager)
Aalto-yliopisto
Laitteistot/tilat: Facility
OtaNano Nanomikroskopiakeskus
Jani Seitsonen (Manager)
OtaNano
Laitteistot/tilat: Facility

University of Helsinki: Finnish Researchers Developed Mini-Breast Cancer as a New Weapon Against the Most Common Type of Breast Cancer
Olli Ikkala & Juho Pokki
29/11/2021 → 30/11/2021
2 kohdetta/ Medianäkyvyys
Lehdistö/media: Esiintyminen mediassa
Finnish researchers developed mini-breast cancer as new weapon against most common type of breast cancer
Juho Pokki
29/11/2021
1 kohde/ Medianäkyvyys
Lehdistö/media: Esiintyminen mediassa

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Munne, P. M., Martikainen, L., Räty, I., Bertula, K., Nonappa, Ruuska, J., Ala-Hongisto, H., Peura, A., Hollmann, B., Euro, L., Yavuz, K., Patrikainen, L., Salmela, M., Pokki, J., Kivento, M., Väänänen, J., Suomi, T., Nevalaita, L., Mutka, M., ... Klefström, J. (2021). Compressive stress-mediated p38 activation required for ERα + phenotype in breast cancer. Nature Communications, 12(1), 1-17. [6967]. https://doi.org/10.1038/s41467-021-27220-9

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title = "Compressive stress-mediated p38 activation required for ERα + phenotype in breast cancer",

abstract = "Breast cancer is now globally the most frequent cancer and leading cause of women{\textquoteright}s death. Two thirds of breast cancers express the luminal estrogen receptor-positive (ERα + ) phenotype that is initially responsive to antihormonal therapies, but drug resistance emerges. A major barrier to the understanding of the ERα-pathway biology and therapeutic discoveries is the restricted repertoire of luminal ERα + breast cancer models. The ERα + phenotype is not stable in cultured cells for reasons not fully understood. We examine 400 patient-derived breast epithelial and breast cancer explant cultures (PDECs) grown in various three-dimensional matrix scaffolds, finding that ERα is primarily regulated by the matrix stiffness. Matrix stiffness upregulates the ERα signaling via stress-mediated p38 activation and H3K27me3-mediated epigenetic regulation. The finding that the matrix stiffness is a central cue to the ERα phenotype reveals a mechanobiological component in breast tissue hormonal signaling and enables the development of novel therapeutic interventions. Subject terms: ER-positive (ER + ), breast cancer, ex vivo model, preclinical model, PDEC, stiffness, p38 SAPK.",

author = "Munne, {Pauliina M.} and Lahja Martikainen and Iiris R{\"a}ty and Kia Bertula and Nonappa and Janika Ruuska and Hanna Ala-Hongisto and Aino Peura and Babette Hollmann and Lilya Euro and Kerim Yavuz and Linda Patrikainen and Maria Salmela and Juho Pokki and Mikko Kivento and Juho V{\"a}{\"a}n{\"a}nen and Tomi Suomi and Liina Nevalaita and Minna Mutka and Panu Kovanen and Marjut Leidenius and Tuomo Meretoja and Katja Hukkinen and Outi Monni and Jeroen Pouwels and Biswajyoti Sahu and Johanna Mattson and Heikki Joensuu and P{\"a}ivi Heikkil{\"a} and Elo, {Laura L.} and Ciara Metcalfe and Junttila, {Melissa R.} and Olli Ikkala and Juha Klefstr{\"o}m",

note = "| openaire: EC/H2020/742829/EU//DRIVEN | openaire: EC/H2020/847912/EU//RESCUER ",

year = "2021",

month = nov,

day = "29",

doi = "10.1038/s41467-021-27220-9",

language = "English",

volume = "12",

pages = "1--17",

journal = "Nature Communications",

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Munne, PM, Martikainen, L, Räty, I, Bertula, K, Nonappa, Ruuska, J, Ala-Hongisto, H, Peura, A, Hollmann, B, Euro, L, Yavuz, K, Patrikainen, L, Salmela, M, Pokki, J, Kivento, M, Väänänen, J, Suomi, T, Nevalaita, L, Mutka, M, Kovanen, P, Leidenius, M, Meretoja, T, Hukkinen, K, Monni, O, Pouwels, J, Sahu, B, Mattson, J, Joensuu, H, Heikkilä, P, Elo, LL, Metcalfe, C, Junttila, MR, Ikkala, O & Klefström, J 2021, 'Compressive stress-mediated p38 activation required for ERα + phenotype in breast cancer', Nature Communications, Vuosikerta 12, Nro 1, 6967, Sivut 1-17. https://doi.org/10.1038/s41467-021-27220-9

TY - JOUR

T1 - Compressive stress-mediated p38 activation required for ERα + phenotype in breast cancer

AU - Munne, Pauliina M.

AU - Martikainen, Lahja

AU - Räty, Iiris

AU - Bertula, Kia

AU - Nonappa, null

AU - Ruuska, Janika

AU - Ala-Hongisto, Hanna

AU - Peura, Aino

AU - Hollmann, Babette

AU - Euro, Lilya

AU - Yavuz, Kerim

AU - Patrikainen, Linda

AU - Salmela, Maria

AU - Pokki, Juho

AU - Kivento, Mikko

AU - Väänänen, Juho

AU - Suomi, Tomi

AU - Nevalaita, Liina

AU - Mutka, Minna

AU - Kovanen, Panu

AU - Leidenius, Marjut

AU - Meretoja, Tuomo

AU - Hukkinen, Katja

AU - Monni, Outi

AU - Pouwels, Jeroen

AU - Sahu, Biswajyoti

AU - Mattson, Johanna

AU - Joensuu, Heikki

AU - Heikkilä, Päivi

AU - Elo, Laura L.

AU - Metcalfe, Ciara

AU - Junttila, Melissa R.

AU - Ikkala, Olli

AU - Klefström, Juha

N1 - | openaire: EC/H2020/742829/EU//DRIVEN | openaire: EC/H2020/847912/EU//RESCUER

PY - 2021/11/29

Y1 - 2021/11/29

N2 - Breast cancer is now globally the most frequent cancer and leading cause of women’s death. Two thirds of breast cancers express the luminal estrogen receptor-positive (ERα + ) phenotype that is initially responsive to antihormonal therapies, but drug resistance emerges. A major barrier to the understanding of the ERα-pathway biology and therapeutic discoveries is the restricted repertoire of luminal ERα + breast cancer models. The ERα + phenotype is not stable in cultured cells for reasons not fully understood. We examine 400 patient-derived breast epithelial and breast cancer explant cultures (PDECs) grown in various three-dimensional matrix scaffolds, finding that ERα is primarily regulated by the matrix stiffness. Matrix stiffness upregulates the ERα signaling via stress-mediated p38 activation and H3K27me3-mediated epigenetic regulation. The finding that the matrix stiffness is a central cue to the ERα phenotype reveals a mechanobiological component in breast tissue hormonal signaling and enables the development of novel therapeutic interventions. Subject terms: ER-positive (ER + ), breast cancer, ex vivo model, preclinical model, PDEC, stiffness, p38 SAPK.

AB - Breast cancer is now globally the most frequent cancer and leading cause of women’s death. Two thirds of breast cancers express the luminal estrogen receptor-positive (ERα + ) phenotype that is initially responsive to antihormonal therapies, but drug resistance emerges. A major barrier to the understanding of the ERα-pathway biology and therapeutic discoveries is the restricted repertoire of luminal ERα + breast cancer models. The ERα + phenotype is not stable in cultured cells for reasons not fully understood. We examine 400 patient-derived breast epithelial and breast cancer explant cultures (PDECs) grown in various three-dimensional matrix scaffolds, finding that ERα is primarily regulated by the matrix stiffness. Matrix stiffness upregulates the ERα signaling via stress-mediated p38 activation and H3K27me3-mediated epigenetic regulation. The finding that the matrix stiffness is a central cue to the ERα phenotype reveals a mechanobiological component in breast tissue hormonal signaling and enables the development of novel therapeutic interventions. Subject terms: ER-positive (ER + ), breast cancer, ex vivo model, preclinical model, PDEC, stiffness, p38 SAPK.

UR - http://www.scopus.com/inward/record.url?scp=85120080419&partnerID=8YFLogxK

U2 - 10.1038/s41467-021-27220-9

DO - 10.1038/s41467-021-27220-9

M3 - Article

AN - SCOPUS:85120080419

SN - 2041-1723

VL - 12

SP - 1

EP - 17

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 6967

ER -

Compressive stress-mediated p38 activation required for ERα + phenotype in breast cancer

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Projektit

PreClinica: Novel Preclinical Model for Breast Cancer Theraphy

HYBER: Suomen Akatemian Biosynteettisten hybridimateriaalien molekyylimuokkauksen huippuyksikkö (2014-2019)

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Lehtileikkeet

University of Helsinki: Finnish Researchers Developed Mini-Breast Cancer as a New Weapon Against the Most Common Type of Breast Cancer

Finnish researchers developed mini-breast cancer as new weapon against most common type of breast cancer

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