Impaired telomere integrity and rRNA biogenesis in PARN‐deficient patients and knock‐out models

Maname Benyelles; Harikleia Episkopou; Marie‐Françoise O'Donohue; Laëtitia Kermasson; Pierre Frange; Florian Poulain; Fatma Burcu Belen; Meltem Polat; Christine Bole‐Feysot; Francina Langa‐Vives; Pierre‐Emmanuel Gleizes; Jean‐Pierre Villartay; Isabelle Callebaut; Anabelle Decottignies; Patrick Revy

doi:10.15252/emmm.201810201

Impaired telomere integrity and rRNA biogenesis in PARN‐deficient patients and knock‐out models

Maname Benyelles, Harikleia Episkopou, Marie‐Françoise O'Donohue, Laëtitia Kermasson, Pierre Frange, Florian Poulain, Fatma Burcu Belen, Meltem Polat, Christine Bole‐Feysot, Francina Langa‐Vives, Pierre‐Emmanuel Gleizes, Jean‐Pierre Villartay, Isabelle Callebaut, Anabelle Decottignies, Patrick Revy

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

Abstract

PARN, poly(A)-specific ribonuclease, regulates the turnover of mRNAs and the maturation and stabilization of the hTR RNA component of telomerase. Biallelic PARN mutations were associated with Høyeraal–Hreidarsson (HH) syndrome, a rare telomere biology disorder that, because of its severity, is likely not exclusively due to hTR down-regulation. Whether PARN deficiency was affecting the expression of telomere-related genes was still unclear. Using cells from two unrelated HH individuals carrying novel PARN mutations and a human PARN knock-out (KO) cell line with inducible PARN complementation, we found that PARN deficiency affects both telomere length and stability and down-regulates the expression of TRF1, TRF2, TPP1, RAP1, and POT1 shelterin transcripts. Down-regulation of dyskerin-encoding DKC1 mRNA was also observed and found to result from p53 activation in PARN-deficient cells. We further showed that PARN deficiency compromises ribosomal RNA biogenesis in patients' fibroblasts and cells from heterozygous Parn KO mice. Homozygous Parn KO however resulted in early embryonic lethality that was not overcome by p53 KO. Our results refine our knowledge on the pleiotropic cellular consequences of PARN deficiency.

Original language	English
Article number	e10201
Journal	EMBO Molecular Medicine
Volume	11
Issue number	7
DOIs	https://doi.org/10.15252/emmm.201810201
Publication status	Published - Jul 2019

Keywords

Høyeraal–Hreidarsson syndrome
PARN
p53
rRNA
shelterin

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10.15252/emmm.201810201

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Benyelles, M., Episkopou, H., O'Donohue, MF., Kermasson, L., Frange, P., Poulain, F., Belen, F. B., Polat, M., Bole‐Feysot, C., Langa‐Vives, F., Gleizes, PE., Villartay, JP., Callebaut, I., Decottignies, A., & Revy, P. (2019). Impaired telomere integrity and rRNA biogenesis in PARN‐deficient patients and knock‐out models. EMBO Molecular Medicine, 11(7), Article e10201. https://doi.org/10.15252/emmm.201810201

@article{44906fde867f43eb82c272920c2d5ad4,

title = "Impaired telomere integrity and rRNA biogenesis in PARN‐deficient patients and knock‐out models",

abstract = "PARN, poly(A)-specific ribonuclease, regulates the turnover of mRNAs and the maturation and stabilization of the hTR RNA component of telomerase. Biallelic PARN mutations were associated with H{\o}yeraal–Hreidarsson (HH) syndrome, a rare telomere biology disorder that, because of its severity, is likely not exclusively due to hTR down-regulation. Whether PARN deficiency was affecting the expression of telomere-related genes was still unclear. Using cells from two unrelated HH individuals carrying novel PARN mutations and a human PARN knock-out (KO) cell line with inducible PARN complementation, we found that PARN deficiency affects both telomere length and stability and down-regulates the expression of TRF1, TRF2, TPP1, RAP1, and POT1 shelterin transcripts. Down-regulation of dyskerin-encoding DKC1 mRNA was also observed and found to result from p53 activation in PARN-deficient cells. We further showed that PARN deficiency compromises ribosomal RNA biogenesis in patients' fibroblasts and cells from heterozygous Parn KO mice. Homozygous Parn KO however resulted in early embryonic lethality that was not overcome by p53 KO. Our results refine our knowledge on the pleiotropic cellular consequences of PARN deficiency.",

keywords = "H{\o}yeraal–Hreidarsson syndrome, PARN, p53, rRNA, shelterin",

author = "Maname Benyelles and Harikleia Episkopou and Marie‐Fran{\c c}oise O'Donohue and La{\"e}titia Kermasson and Pierre Frange and Florian Poulain and Belen, {Fatma Burcu} and Meltem Polat and Christine Bole‐Feysot and Francina Langa‐Vives and Pierre‐Emmanuel Gleizes and Jean‐Pierre Villartay and Isabelle Callebaut and Anabelle Decottignies and Patrick Revy",

note = "Funding Information: We thank the patients and their families for their contribution. We thank Jerry W. Shay and Woodring E. Wright for the kind gift of the Muntjac cells. P.R. is grateful to Prof. Alain Fischer for discussions, advice, and support. We acknowledge the excellent technical assistance of Alicia Fernandez for generating B-LCL (CRB, Imagine Institute, Paris, France) and Nikenza Viceconte for the hTR FISH. This work has been supported by institutional grants from INSERM, Ligue Nationale contre le Cancer (Equipe Labellis{\'e}e La Ligue), Institut National du Cancer INCa, GIS-Institut des maladies rares, and FNRS (Fonds National de la Recherche Scientifique, Belgium). P.E.G. and M.F.O. are supported by Agence Nationale de la Recherche (ANR 2015 AAP g{\'e}n{\'e}rique CE12-0001-DBA Multigenes), and the EuroDBA project is funded by the ERA-NET program E-RAR3 (ANR-15-RAR3-0007-04). P.R. and M.F.O. are scientists from Centre National de la Recherche Scientifique (CNRS). H.E. and F.P. were supported by grants from the T{\'e}l{\'e}vie/FNRS and FRIA/FNRS. A.D. is a scientist from the FNRS. Funding Information: We thank the patients and their families for their contribution. We thank Jerry W. Shay and Woodring E. Wright for the kind gift of the Muntjac cells. P.R. is grateful to Prof. Alain Fischer for discussions, advice, and support. We acknowledge the excellent technical assistance of Alicia Fernandez for generating B-LCL (CRB, Imagine Institute, Paris, France) and Nikenza Viceconte for the hTR FISH. This work has been supported by institutional grants from INSERM, Ligue Nationale contre le Cancer (Equipe Labellis{\'e}e La Ligue), Insti-tut National du Cancer INCa, GIS-Institut des maladies rares, and FNRS (Fonds National de la Recherche Scientifique, Belgium). P.E.G. and M.F.O. are supported by Agence Nationale de la Recherche (ANR 2015 AAP g{\'e}n{\'e}rique CE12-0001-DBA Multigenes), and the EuroDBA project is funded by the ERA-NET program E-RAR3 (ANR-15-RAR3-0007-04). P.R. and M.F.O. are scientists from Centre National de la Recherche Scientifique (CNRS). H.E. and F.P. were supported by grants from the T{\'e}l{\'e}vie/FNRS and FRIA/FNRS. A.D. is a scientist from the FNRS. Publisher Copyright: {\textcopyright} 2019 The Authors. Published under the terms of the CC BY 4.0 license",

year = "2019",

month = jul,

doi = "10.15252/emmm.201810201",

language = "English",

volume = "11",

journal = "EMBO Molecular Medicine",

issn = "1757-4676",

publisher = "Springer Science and Business Media Deutschland GmbH",

number = "7",

}

Benyelles, M, Episkopou, H, O'Donohue, MF, Kermasson, L, Frange, P, Poulain, F, Belen, FB, Polat, M, Bole‐Feysot, C, Langa‐Vives, F, Gleizes, PE, Villartay, JP, Callebaut, I, Decottignies, A & Revy, P 2019, 'Impaired telomere integrity and rRNA biogenesis in PARN‐deficient patients and knock‐out models', EMBO Molecular Medicine, vol. 11, no. 7, e10201. https://doi.org/10.15252/emmm.201810201

TY - JOUR

T1 - Impaired telomere integrity and rRNA biogenesis in PARN‐deficient patients and knock‐out models

AU - Benyelles, Maname

AU - Episkopou, Harikleia

AU - O'Donohue, Marie‐Françoise

AU - Kermasson, Laëtitia

AU - Frange, Pierre

AU - Poulain, Florian

AU - Belen, Fatma Burcu

AU - Polat, Meltem

AU - Bole‐Feysot, Christine

AU - Langa‐Vives, Francina

AU - Gleizes, Pierre‐Emmanuel

AU - Villartay, Jean‐Pierre

AU - Callebaut, Isabelle

AU - Decottignies, Anabelle

AU - Revy, Patrick

N1 - Funding Information: We thank the patients and their families for their contribution. We thank Jerry W. Shay and Woodring E. Wright for the kind gift of the Muntjac cells. P.R. is grateful to Prof. Alain Fischer for discussions, advice, and support. We acknowledge the excellent technical assistance of Alicia Fernandez for generating B-LCL (CRB, Imagine Institute, Paris, France) and Nikenza Viceconte for the hTR FISH. This work has been supported by institutional grants from INSERM, Ligue Nationale contre le Cancer (Equipe Labellisée La Ligue), Institut National du Cancer INCa, GIS-Institut des maladies rares, and FNRS (Fonds National de la Recherche Scientifique, Belgium). P.E.G. and M.F.O. are supported by Agence Nationale de la Recherche (ANR 2015 AAP générique CE12-0001-DBA Multigenes), and the EuroDBA project is funded by the ERA-NET program E-RAR3 (ANR-15-RAR3-0007-04). P.R. and M.F.O. are scientists from Centre National de la Recherche Scientifique (CNRS). H.E. and F.P. were supported by grants from the Télévie/FNRS and FRIA/FNRS. A.D. is a scientist from the FNRS. Funding Information: We thank the patients and their families for their contribution. We thank Jerry W. Shay and Woodring E. Wright for the kind gift of the Muntjac cells. P.R. is grateful to Prof. Alain Fischer for discussions, advice, and support. We acknowledge the excellent technical assistance of Alicia Fernandez for generating B-LCL (CRB, Imagine Institute, Paris, France) and Nikenza Viceconte for the hTR FISH. This work has been supported by institutional grants from INSERM, Ligue Nationale contre le Cancer (Equipe Labellisée La Ligue), Insti-tut National du Cancer INCa, GIS-Institut des maladies rares, and FNRS (Fonds National de la Recherche Scientifique, Belgium). P.E.G. and M.F.O. are supported by Agence Nationale de la Recherche (ANR 2015 AAP générique CE12-0001-DBA Multigenes), and the EuroDBA project is funded by the ERA-NET program E-RAR3 (ANR-15-RAR3-0007-04). P.R. and M.F.O. are scientists from Centre National de la Recherche Scientifique (CNRS). H.E. and F.P. were supported by grants from the Télévie/FNRS and FRIA/FNRS. A.D. is a scientist from the FNRS. Publisher Copyright: © 2019 The Authors. Published under the terms of the CC BY 4.0 license

PY - 2019/7

Y1 - 2019/7

N2 - PARN, poly(A)-specific ribonuclease, regulates the turnover of mRNAs and the maturation and stabilization of the hTR RNA component of telomerase. Biallelic PARN mutations were associated with Høyeraal–Hreidarsson (HH) syndrome, a rare telomere biology disorder that, because of its severity, is likely not exclusively due to hTR down-regulation. Whether PARN deficiency was affecting the expression of telomere-related genes was still unclear. Using cells from two unrelated HH individuals carrying novel PARN mutations and a human PARN knock-out (KO) cell line with inducible PARN complementation, we found that PARN deficiency affects both telomere length and stability and down-regulates the expression of TRF1, TRF2, TPP1, RAP1, and POT1 shelterin transcripts. Down-regulation of dyskerin-encoding DKC1 mRNA was also observed and found to result from p53 activation in PARN-deficient cells. We further showed that PARN deficiency compromises ribosomal RNA biogenesis in patients' fibroblasts and cells from heterozygous Parn KO mice. Homozygous Parn KO however resulted in early embryonic lethality that was not overcome by p53 KO. Our results refine our knowledge on the pleiotropic cellular consequences of PARN deficiency.

AB - PARN, poly(A)-specific ribonuclease, regulates the turnover of mRNAs and the maturation and stabilization of the hTR RNA component of telomerase. Biallelic PARN mutations were associated with Høyeraal–Hreidarsson (HH) syndrome, a rare telomere biology disorder that, because of its severity, is likely not exclusively due to hTR down-regulation. Whether PARN deficiency was affecting the expression of telomere-related genes was still unclear. Using cells from two unrelated HH individuals carrying novel PARN mutations and a human PARN knock-out (KO) cell line with inducible PARN complementation, we found that PARN deficiency affects both telomere length and stability and down-regulates the expression of TRF1, TRF2, TPP1, RAP1, and POT1 shelterin transcripts. Down-regulation of dyskerin-encoding DKC1 mRNA was also observed and found to result from p53 activation in PARN-deficient cells. We further showed that PARN deficiency compromises ribosomal RNA biogenesis in patients' fibroblasts and cells from heterozygous Parn KO mice. Homozygous Parn KO however resulted in early embryonic lethality that was not overcome by p53 KO. Our results refine our knowledge on the pleiotropic cellular consequences of PARN deficiency.

KW - Høyeraal–Hreidarsson syndrome

KW - PARN

KW - p53

KW - rRNA

KW - shelterin

UR - http://www.scopus.com/inward/record.url?scp=85067393765&partnerID=8YFLogxK

U2 - 10.15252/emmm.201810201

DO - 10.15252/emmm.201810201

M3 - Article

SN - 1757-4676

VL - 11

JO - EMBO Molecular Medicine

JF - EMBO Molecular Medicine

IS - 7

M1 - e10201

ER -

Impaired telomere integrity and rRNA biogenesis in PARN‐deficient patients and knock‐out models

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Keywords

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