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MKRN3 Interacts With Several Proteins Implicated in Puberty Timing but Does Not Influence GNRH1 Expression

Paternally-inherited loss-of-function mutations in makorin ring finger protein 3 gene (MKRN3) underlie central precocious puberty. To investigate the puberty-related mechanism(s) of MKRN3 in humans, we generated two distinct bi-allelic MKRN3 knock-out human pluripotent stem cell lines, Del 1 and Del...

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Autores principales: Yellapragada, Venkatram, Liu, Xiaonan, Lund, Carina, Känsäkoski, Johanna, Pulli, Kristiina, Vuoristo, Sanna, Lundin, Karolina, Tuuri, Timo, Varjosalo, Markku, Raivio, Taneli
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6375840/
https://www.ncbi.nlm.nih.gov/pubmed/30800097
http://dx.doi.org/10.3389/fendo.2019.00048
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author Yellapragada, Venkatram
Liu, Xiaonan
Lund, Carina
Känsäkoski, Johanna
Pulli, Kristiina
Vuoristo, Sanna
Lundin, Karolina
Tuuri, Timo
Varjosalo, Markku
Raivio, Taneli
author_facet Yellapragada, Venkatram
Liu, Xiaonan
Lund, Carina
Känsäkoski, Johanna
Pulli, Kristiina
Vuoristo, Sanna
Lundin, Karolina
Tuuri, Timo
Varjosalo, Markku
Raivio, Taneli
author_sort Yellapragada, Venkatram
collection PubMed
description Paternally-inherited loss-of-function mutations in makorin ring finger protein 3 gene (MKRN3) underlie central precocious puberty. To investigate the puberty-related mechanism(s) of MKRN3 in humans, we generated two distinct bi-allelic MKRN3 knock-out human pluripotent stem cell lines, Del 1 and Del 2, and differentiated them into GNRH1-expressing neurons. Both Del 1 and Del 2 clones could be differentiated into neuronal progenitors and GNRH1-expressing neurons, however, the relative expression of GNRH1 did not differ from wild type cells (P = NS). Subsequently, we investigated stable and dynamic protein-protein interaction (PPI) partners of MKRN3 by stably expressing it in HEK cells followed by mass spectrometry analyses. We found 81 high-confidence novel protein interaction partners, which are implicated in cellular processes such as insulin signaling, RNA metabolism and cell-cell adhesion. Of the identified interactors, 20 have been previously implicated in puberty timing. In conclusion, our stem cell model for generation of GNRH1-expressing neurons did not offer mechanistic insight for the role of MKRN3 in puberty initiation. The PPI data, however, indicate that MKRN3 may regulate puberty by interacting with other puberty-related proteins. Further studies are required to elucidate the possible mechanisms and outcomes of these interactions.
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spelling pubmed-63758402019-02-22 MKRN3 Interacts With Several Proteins Implicated in Puberty Timing but Does Not Influence GNRH1 Expression Yellapragada, Venkatram Liu, Xiaonan Lund, Carina Känsäkoski, Johanna Pulli, Kristiina Vuoristo, Sanna Lundin, Karolina Tuuri, Timo Varjosalo, Markku Raivio, Taneli Front Endocrinol (Lausanne) Endocrinology Paternally-inherited loss-of-function mutations in makorin ring finger protein 3 gene (MKRN3) underlie central precocious puberty. To investigate the puberty-related mechanism(s) of MKRN3 in humans, we generated two distinct bi-allelic MKRN3 knock-out human pluripotent stem cell lines, Del 1 and Del 2, and differentiated them into GNRH1-expressing neurons. Both Del 1 and Del 2 clones could be differentiated into neuronal progenitors and GNRH1-expressing neurons, however, the relative expression of GNRH1 did not differ from wild type cells (P = NS). Subsequently, we investigated stable and dynamic protein-protein interaction (PPI) partners of MKRN3 by stably expressing it in HEK cells followed by mass spectrometry analyses. We found 81 high-confidence novel protein interaction partners, which are implicated in cellular processes such as insulin signaling, RNA metabolism and cell-cell adhesion. Of the identified interactors, 20 have been previously implicated in puberty timing. In conclusion, our stem cell model for generation of GNRH1-expressing neurons did not offer mechanistic insight for the role of MKRN3 in puberty initiation. The PPI data, however, indicate that MKRN3 may regulate puberty by interacting with other puberty-related proteins. Further studies are required to elucidate the possible mechanisms and outcomes of these interactions. Frontiers Media S.A. 2019-02-08 /pmc/articles/PMC6375840/ /pubmed/30800097 http://dx.doi.org/10.3389/fendo.2019.00048 Text en Copyright © 2019 Yellapragada, Liu, Lund, Känsäkoski, Pulli, Vuoristo, Lundin, Tuuri, Varjosalo and Raivio. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Endocrinology
Yellapragada, Venkatram
Liu, Xiaonan
Lund, Carina
Känsäkoski, Johanna
Pulli, Kristiina
Vuoristo, Sanna
Lundin, Karolina
Tuuri, Timo
Varjosalo, Markku
Raivio, Taneli
MKRN3 Interacts With Several Proteins Implicated in Puberty Timing but Does Not Influence GNRH1 Expression
title MKRN3 Interacts With Several Proteins Implicated in Puberty Timing but Does Not Influence GNRH1 Expression
title_full MKRN3 Interacts With Several Proteins Implicated in Puberty Timing but Does Not Influence GNRH1 Expression
title_fullStr MKRN3 Interacts With Several Proteins Implicated in Puberty Timing but Does Not Influence GNRH1 Expression
title_full_unstemmed MKRN3 Interacts With Several Proteins Implicated in Puberty Timing but Does Not Influence GNRH1 Expression
title_short MKRN3 Interacts With Several Proteins Implicated in Puberty Timing but Does Not Influence GNRH1 Expression
title_sort mkrn3 interacts with several proteins implicated in puberty timing but does not influence gnrh1 expression
topic Endocrinology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6375840/
https://www.ncbi.nlm.nih.gov/pubmed/30800097
http://dx.doi.org/10.3389/fendo.2019.00048
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