Mammalian Hbs1L deficiency causes congenital anomalies and developmental delay associated with Pelota depletion and 80S monosome accumulation

Hbs1 has been established as a central component of the cell’s translational quality control pathways in both yeast and prokaryotic models; however, the functional characteristics of its human ortholog (Hbs1L) have not been well-defined. We recently reported a novel human phenotype resulting from a...

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Autores principales: O’Connell, Amy E., Gerashchenko, Maxim V., O’Donohue, Marie-Francoise, Rosen, Samantha M., Huntzinger, Eric, Gleeson, Diane, Galli, Antonella, Ryder, Edward, Cao, Siqi, Murphy, Quinn, Kazerounian, Shideh, Morton, Sarah U., Schmitz-Abe, Klaus, Gladyshev, Vadim N., Gleizes, Pierre-Emmanuel, Séraphin, Bertrand, Agrawal, Pankaj B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6373978/
https://www.ncbi.nlm.nih.gov/pubmed/30707697
http://dx.doi.org/10.1371/journal.pgen.1007917
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author O’Connell, Amy E.
Gerashchenko, Maxim V.
O’Donohue, Marie-Francoise
Rosen, Samantha M.
Huntzinger, Eric
Gleeson, Diane
Galli, Antonella
Ryder, Edward
Cao, Siqi
Murphy, Quinn
Kazerounian, Shideh
Morton, Sarah U.
Schmitz-Abe, Klaus
Gladyshev, Vadim N.
Gleizes, Pierre-Emmanuel
Séraphin, Bertrand
Agrawal, Pankaj B.
author_facet O’Connell, Amy E.
Gerashchenko, Maxim V.
O’Donohue, Marie-Francoise
Rosen, Samantha M.
Huntzinger, Eric
Gleeson, Diane
Galli, Antonella
Ryder, Edward
Cao, Siqi
Murphy, Quinn
Kazerounian, Shideh
Morton, Sarah U.
Schmitz-Abe, Klaus
Gladyshev, Vadim N.
Gleizes, Pierre-Emmanuel
Séraphin, Bertrand
Agrawal, Pankaj B.
author_sort O’Connell, Amy E.
collection PubMed
description Hbs1 has been established as a central component of the cell’s translational quality control pathways in both yeast and prokaryotic models; however, the functional characteristics of its human ortholog (Hbs1L) have not been well-defined. We recently reported a novel human phenotype resulting from a mutation in the critical coding region of the HBS1L gene characterized by facial dysmorphism, severe growth restriction, axial hypotonia, global developmental delay and retinal pigmentary deposits. Here we further characterize downstream effects of the human HBS1L mutation. HBS1L has three transcripts in humans, and RT-PCR demonstrated reduced mRNA levels corresponding with transcripts V1 and V2 whereas V3 expression was unchanged. Western blot analyses revealed Hbs1L protein was absent in the patient cells. Additionally, polysome profiling revealed an abnormal aggregation of 80S monosomes in patient cells under baseline conditions. RNA and ribosomal sequencing demonstrated an increased translation efficiency of ribosomal RNA in Hbs1L-deficient fibroblasts, suggesting that there may be a compensatory increase in ribosome translation to accommodate the increased 80S monosome levels. This enhanced translation was accompanied by upregulation of mTOR and 4-EBP protein expression, suggesting an mTOR-dependent phenomenon. Furthermore, lack of Hbs1L caused depletion of Pelota protein in both patient cells and mouse tissues, while PELO mRNA levels were unaffected. Inhibition of proteasomal function partially restored Pelota expression in human Hbs1L-deficient cells. We also describe a mouse model harboring a knockdown mutation in the murine Hbs1l gene that shared several of the phenotypic elements observed in the Hbs1L-deficient human including facial dysmorphism, growth restriction and retinal deposits. The Hbs1lKO mice similarly demonstrate diminished Pelota levels that were rescued by proteasome inhibition.
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spelling pubmed-63739782019-03-01 Mammalian Hbs1L deficiency causes congenital anomalies and developmental delay associated with Pelota depletion and 80S monosome accumulation O’Connell, Amy E. Gerashchenko, Maxim V. O’Donohue, Marie-Francoise Rosen, Samantha M. Huntzinger, Eric Gleeson, Diane Galli, Antonella Ryder, Edward Cao, Siqi Murphy, Quinn Kazerounian, Shideh Morton, Sarah U. Schmitz-Abe, Klaus Gladyshev, Vadim N. Gleizes, Pierre-Emmanuel Séraphin, Bertrand Agrawal, Pankaj B. PLoS Genet Research Article Hbs1 has been established as a central component of the cell’s translational quality control pathways in both yeast and prokaryotic models; however, the functional characteristics of its human ortholog (Hbs1L) have not been well-defined. We recently reported a novel human phenotype resulting from a mutation in the critical coding region of the HBS1L gene characterized by facial dysmorphism, severe growth restriction, axial hypotonia, global developmental delay and retinal pigmentary deposits. Here we further characterize downstream effects of the human HBS1L mutation. HBS1L has three transcripts in humans, and RT-PCR demonstrated reduced mRNA levels corresponding with transcripts V1 and V2 whereas V3 expression was unchanged. Western blot analyses revealed Hbs1L protein was absent in the patient cells. Additionally, polysome profiling revealed an abnormal aggregation of 80S monosomes in patient cells under baseline conditions. RNA and ribosomal sequencing demonstrated an increased translation efficiency of ribosomal RNA in Hbs1L-deficient fibroblasts, suggesting that there may be a compensatory increase in ribosome translation to accommodate the increased 80S monosome levels. This enhanced translation was accompanied by upregulation of mTOR and 4-EBP protein expression, suggesting an mTOR-dependent phenomenon. Furthermore, lack of Hbs1L caused depletion of Pelota protein in both patient cells and mouse tissues, while PELO mRNA levels were unaffected. Inhibition of proteasomal function partially restored Pelota expression in human Hbs1L-deficient cells. We also describe a mouse model harboring a knockdown mutation in the murine Hbs1l gene that shared several of the phenotypic elements observed in the Hbs1L-deficient human including facial dysmorphism, growth restriction and retinal deposits. The Hbs1lKO mice similarly demonstrate diminished Pelota levels that were rescued by proteasome inhibition. Public Library of Science 2019-02-01 /pmc/articles/PMC6373978/ /pubmed/30707697 http://dx.doi.org/10.1371/journal.pgen.1007917 Text en © 2019 O’Connell et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
O’Connell, Amy E.
Gerashchenko, Maxim V.
O’Donohue, Marie-Francoise
Rosen, Samantha M.
Huntzinger, Eric
Gleeson, Diane
Galli, Antonella
Ryder, Edward
Cao, Siqi
Murphy, Quinn
Kazerounian, Shideh
Morton, Sarah U.
Schmitz-Abe, Klaus
Gladyshev, Vadim N.
Gleizes, Pierre-Emmanuel
Séraphin, Bertrand
Agrawal, Pankaj B.
Mammalian Hbs1L deficiency causes congenital anomalies and developmental delay associated with Pelota depletion and 80S monosome accumulation
title Mammalian Hbs1L deficiency causes congenital anomalies and developmental delay associated with Pelota depletion and 80S monosome accumulation
title_full Mammalian Hbs1L deficiency causes congenital anomalies and developmental delay associated with Pelota depletion and 80S monosome accumulation
title_fullStr Mammalian Hbs1L deficiency causes congenital anomalies and developmental delay associated with Pelota depletion and 80S monosome accumulation
title_full_unstemmed Mammalian Hbs1L deficiency causes congenital anomalies and developmental delay associated with Pelota depletion and 80S monosome accumulation
title_short Mammalian Hbs1L deficiency causes congenital anomalies and developmental delay associated with Pelota depletion and 80S monosome accumulation
title_sort mammalian hbs1l deficiency causes congenital anomalies and developmental delay associated with pelota depletion and 80s monosome accumulation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6373978/
https://www.ncbi.nlm.nih.gov/pubmed/30707697
http://dx.doi.org/10.1371/journal.pgen.1007917
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