The intracellular domain of β-dystroglycan mediates the nucleolar stress response by suppressing UBF transcriptional activity

Paulina Margarita Azuara-Medina; Ariana María Sandoval-Duarte; Sara L. Morales-Lázaro; Ricardo Modragón-González; Griselda Vélez-Aguilera; Juan de Dios Gómez-López; Guadalupe Elizabeth Jiménez-Gutiérrez; Reynaldo Tiburcio-Félix; Ivette Martínez-Vieyra; Rocío Suárez-Sánchez; Gernot Längst; Jonathan Javier Magaña; Steve J. Winder; Arturo Ortega; Rita de Cassia Ramos Perlingeiro; Laura A. Jacobs; Bulmaro Cisneros

doi:10.1038/s41419-019-1454-z

The intracellular domain of β-dystroglycan mediates the nucleolar stress response by suppressing UBF transcriptional activity

Paulina Margarita Azuara-Medina, Ariana María Sandoval-Duarte, Sara L. Morales-Lázaro, Ricardo Modragón-González, Griselda Vélez-Aguilera, Juan de Dios Gómez-López, Guadalupe Elizabeth Jiménez-Gutiérrez, Reynaldo Tiburcio-Félix, Ivette Martínez-Vieyra, Rocío Suárez-Sánchez, Gernot Längst, Jonathan Javier Magaña, Steve J. Winder, Arturo Ortega, Rita de Cassia Ramos Perlingeiro, Laura A. Jacobs, Bulmaro Cisneros

Escuela Nacional de Medicina y Homeopatía (ENMH)

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

3 Scopus citations

Abstract

β-dystroglycan (β-DG) is a key component of multiprotein complexes in the plasma membrane and nuclear envelope. In addition, β-DG undergoes two successive proteolytic cleavages that result in the liberation of its intracellular domain (ICD) into the cytosol and nucleus. However, stimuli-inducing ICD cleavage and the physiological relevance of this proteolytic fragment are largely unknown. In this study we show for the first time that β-DG ICD is targeted to the nucleolus where it interacts with the nuclear proteins B23 and UBF (central factor of Pol I-mediated rRNA gene transcription) and binds to rDNA promoter regions. Interestingly DG silencing results in reduced B23 and UBF levels and aberrant nucleolar morphology. Furthermore, β-DG ICD cleavage is induced by different nucleolar stressors, including oxidative stress, acidosis, and UV irradiation, which implies its participation in the response to nucleolar stress. Consistent with this idea, overexpression of β-DG elicited mislocalization and decreased levels of UBF and suppression of rRNA expression, which in turn provoked altered ribosome profiling and decreased cell growth. Collectively our data reveal that β-DG ICD acts as negative regulator of rDNA transcription by impeding the transcriptional activity of UBF, as a part of the protective mechanism activated in response to nucleolar stress.

Original language	English
Article number	196
Journal	Cell Death and Disease
Volume	10
Issue number	3
DOIs	https://doi.org/10.1038/s41419-019-1454-z
State	Published - 1 Mar 2019

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Azuara-Medina, P. M., Sandoval-Duarte, A. M., Morales-Lázaro, S. L., Modragón-González, R., Vélez-Aguilera, G., Gómez-López, J. D. D., Jiménez-Gutiérrez, G. E., Tiburcio-Félix, R., Martínez-Vieyra, I., Suárez-Sánchez, R., Längst, G., Magaña, J. J., Winder, S. J., Ortega, A., Ramos Perlingeiro, R. D. C., Jacobs, L. A., & Cisneros, B. (2019). The intracellular domain of β-dystroglycan mediates the nucleolar stress response by suppressing UBF transcriptional activity. Cell Death and Disease, 10(3), Article 196. https://doi.org/10.1038/s41419-019-1454-z

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title = "The intracellular domain of β-dystroglycan mediates the nucleolar stress response by suppressing UBF transcriptional activity",

abstract = "β-dystroglycan (β-DG) is a key component of multiprotein complexes in the plasma membrane and nuclear envelope. In addition, β-DG undergoes two successive proteolytic cleavages that result in the liberation of its intracellular domain (ICD) into the cytosol and nucleus. However, stimuli-inducing ICD cleavage and the physiological relevance of this proteolytic fragment are largely unknown. In this study we show for the first time that β-DG ICD is targeted to the nucleolus where it interacts with the nuclear proteins B23 and UBF (central factor of Pol I-mediated rRNA gene transcription) and binds to rDNA promoter regions. Interestingly DG silencing results in reduced B23 and UBF levels and aberrant nucleolar morphology. Furthermore, β-DG ICD cleavage is induced by different nucleolar stressors, including oxidative stress, acidosis, and UV irradiation, which implies its participation in the response to nucleolar stress. Consistent with this idea, overexpression of β-DG elicited mislocalization and decreased levels of UBF and suppression of rRNA expression, which in turn provoked altered ribosome profiling and decreased cell growth. Collectively our data reveal that β-DG ICD acts as negative regulator of rDNA transcription by impeding the transcriptional activity of UBF, as a part of the protective mechanism activated in response to nucleolar stress.",

author = "Azuara-Medina, {Paulina Margarita} and Sandoval-Duarte, {Ariana Mar{\'i}a} and Morales-L{\'a}zaro, {Sara L.} and Ricardo Modrag{\'o}n-Gonz{\'a}lez and Griselda V{\'e}lez-Aguilera and G{\'o}mez-L{\'o}pez, {Juan de Dios} and Jim{\'e}nez-Guti{\'e}rrez, {Guadalupe Elizabeth} and Reynaldo Tiburcio-F{\'e}lix and Ivette Mart{\'i}nez-Vieyra and Roc{\'i}o Su{\'a}rez-S{\'a}nchez and Gernot L{\"a}ngst and Maga{\~n}a, {Jonathan Javier} and Winder, {Steve J.} and Arturo Ortega and {Ramos Perlingeiro}, {Rita de Cassia} and Jacobs, {Laura A.} and Bulmaro Cisneros",

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doi = "10.1038/s41419-019-1454-z",

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Azuara-Medina, PM, Sandoval-Duarte, AM, Morales-Lázaro, SL, Modragón-González, R, Vélez-Aguilera, G, Gómez-López, JDD, Jiménez-Gutiérrez, GE, Tiburcio-Félix, R, Martínez-Vieyra, I, Suárez-Sánchez, R, Längst, G, Magaña, JJ, Winder, SJ, Ortega, A, Ramos Perlingeiro, RDC, Jacobs, LA & Cisneros, B 2019, 'The intracellular domain of β-dystroglycan mediates the nucleolar stress response by suppressing UBF transcriptional activity', Cell Death and Disease, vol. 10, no. 3, 196. https://doi.org/10.1038/s41419-019-1454-z

TY - JOUR

T1 - The intracellular domain of β-dystroglycan mediates the nucleolar stress response by suppressing UBF transcriptional activity

AU - Azuara-Medina, Paulina Margarita

AU - Sandoval-Duarte, Ariana María

AU - Morales-Lázaro, Sara L.

AU - Modragón-González, Ricardo

AU - Vélez-Aguilera, Griselda

AU - Gómez-López, Juan de Dios

AU - Jiménez-Gutiérrez, Guadalupe Elizabeth

AU - Tiburcio-Félix, Reynaldo

AU - Martínez-Vieyra, Ivette

AU - Suárez-Sánchez, Rocío

AU - Längst, Gernot

AU - Magaña, Jonathan Javier

AU - Winder, Steve J.

AU - Ortega, Arturo

AU - Ramos Perlingeiro, Rita de Cassia

AU - Jacobs, Laura A.

AU - Cisneros, Bulmaro

PY - 2019/3/1

Y1 - 2019/3/1

N2 - β-dystroglycan (β-DG) is a key component of multiprotein complexes in the plasma membrane and nuclear envelope. In addition, β-DG undergoes two successive proteolytic cleavages that result in the liberation of its intracellular domain (ICD) into the cytosol and nucleus. However, stimuli-inducing ICD cleavage and the physiological relevance of this proteolytic fragment are largely unknown. In this study we show for the first time that β-DG ICD is targeted to the nucleolus where it interacts with the nuclear proteins B23 and UBF (central factor of Pol I-mediated rRNA gene transcription) and binds to rDNA promoter regions. Interestingly DG silencing results in reduced B23 and UBF levels and aberrant nucleolar morphology. Furthermore, β-DG ICD cleavage is induced by different nucleolar stressors, including oxidative stress, acidosis, and UV irradiation, which implies its participation in the response to nucleolar stress. Consistent with this idea, overexpression of β-DG elicited mislocalization and decreased levels of UBF and suppression of rRNA expression, which in turn provoked altered ribosome profiling and decreased cell growth. Collectively our data reveal that β-DG ICD acts as negative regulator of rDNA transcription by impeding the transcriptional activity of UBF, as a part of the protective mechanism activated in response to nucleolar stress.

AB - β-dystroglycan (β-DG) is a key component of multiprotein complexes in the plasma membrane and nuclear envelope. In addition, β-DG undergoes two successive proteolytic cleavages that result in the liberation of its intracellular domain (ICD) into the cytosol and nucleus. However, stimuli-inducing ICD cleavage and the physiological relevance of this proteolytic fragment are largely unknown. In this study we show for the first time that β-DG ICD is targeted to the nucleolus where it interacts with the nuclear proteins B23 and UBF (central factor of Pol I-mediated rRNA gene transcription) and binds to rDNA promoter regions. Interestingly DG silencing results in reduced B23 and UBF levels and aberrant nucleolar morphology. Furthermore, β-DG ICD cleavage is induced by different nucleolar stressors, including oxidative stress, acidosis, and UV irradiation, which implies its participation in the response to nucleolar stress. Consistent with this idea, overexpression of β-DG elicited mislocalization and decreased levels of UBF and suppression of rRNA expression, which in turn provoked altered ribosome profiling and decreased cell growth. Collectively our data reveal that β-DG ICD acts as negative regulator of rDNA transcription by impeding the transcriptional activity of UBF, as a part of the protective mechanism activated in response to nucleolar stress.

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U2 - 10.1038/s41419-019-1454-z

DO - 10.1038/s41419-019-1454-z

M3 - Artículo

C2 - 30814495

SN - 2041-4889

VL - 10

JO - Cell Death and Disease

JF - Cell Death and Disease

IS - 3

M1 - 196

ER -

The intracellular domain of β-dystroglycan mediates the nucleolar stress response by suppressing UBF transcriptional activity

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