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Characteristics of Transfer RNA-Derived Fragments Expressed during Human Renal Cell Development: The Role of Dicer in tRF Biogenesis

tRNA-derived fragments participate in the regulation of many processes, such as gene silencing, splicing and translation in many organisms, ranging from bacteria to humans. We were interested to know how tRF abundance changes during the different stages of renal cell development. The research model...

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Autores principales: Kazimierczyk, Marek, Wojnicka, Marta, Biała, Ewa, Żydowicz-Machtel, Paulina, Imiołczyk, Barbara, Ostrowski, Tomasz, Kurzyńska-Kokorniak, Anna, Wrzesinski, Jan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8998818/
https://www.ncbi.nlm.nih.gov/pubmed/35409004
http://dx.doi.org/10.3390/ijms23073644
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author Kazimierczyk, Marek
Wojnicka, Marta
Biała, Ewa
Żydowicz-Machtel, Paulina
Imiołczyk, Barbara
Ostrowski, Tomasz
Kurzyńska-Kokorniak, Anna
Wrzesinski, Jan
author_facet Kazimierczyk, Marek
Wojnicka, Marta
Biała, Ewa
Żydowicz-Machtel, Paulina
Imiołczyk, Barbara
Ostrowski, Tomasz
Kurzyńska-Kokorniak, Anna
Wrzesinski, Jan
author_sort Kazimierczyk, Marek
collection PubMed
description tRNA-derived fragments participate in the regulation of many processes, such as gene silencing, splicing and translation in many organisms, ranging from bacteria to humans. We were interested to know how tRF abundance changes during the different stages of renal cell development. The research model used here consisted of the following human renal cells: hESCs, HEK-293T, HK-2 and A-489 kidney tumor cells, which, together, mimic the different stages of kidney development. The characteristics of the most abundant tRFs, tRFGly(CCC), tRFVal(AAC) and tRFArg(CCU), were presented. It was found that these parental tRNAs present in cells are the source of many tRFs, thus increasing the pool of potential regulatory RNAs. Indeed, a bioinformatic analysis showed the possibility that tRFGly(CCC) and tRRFVal(AAC) could regulate the activity of a range of kidney proteins. Moreover, the distribution of tRFs and the efficiency of their expression is similar in adult and embryonic stem cells. During the formation of tRFs, HK-2 cells resemble A-498 cancer cells more than other cells. Additionally, we postulate the involvement of Dicer nuclease in the formation of tRF-5b in all the analyzed tRNAs. To confirm this, 293T NoDice cells, which in the absence of Dicer activity do not generate tRF-5b, were used.
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spelling pubmed-89988182022-04-12 Characteristics of Transfer RNA-Derived Fragments Expressed during Human Renal Cell Development: The Role of Dicer in tRF Biogenesis Kazimierczyk, Marek Wojnicka, Marta Biała, Ewa Żydowicz-Machtel, Paulina Imiołczyk, Barbara Ostrowski, Tomasz Kurzyńska-Kokorniak, Anna Wrzesinski, Jan Int J Mol Sci Article tRNA-derived fragments participate in the regulation of many processes, such as gene silencing, splicing and translation in many organisms, ranging from bacteria to humans. We were interested to know how tRF abundance changes during the different stages of renal cell development. The research model used here consisted of the following human renal cells: hESCs, HEK-293T, HK-2 and A-489 kidney tumor cells, which, together, mimic the different stages of kidney development. The characteristics of the most abundant tRFs, tRFGly(CCC), tRFVal(AAC) and tRFArg(CCU), were presented. It was found that these parental tRNAs present in cells are the source of many tRFs, thus increasing the pool of potential regulatory RNAs. Indeed, a bioinformatic analysis showed the possibility that tRFGly(CCC) and tRRFVal(AAC) could regulate the activity of a range of kidney proteins. Moreover, the distribution of tRFs and the efficiency of their expression is similar in adult and embryonic stem cells. During the formation of tRFs, HK-2 cells resemble A-498 cancer cells more than other cells. Additionally, we postulate the involvement of Dicer nuclease in the formation of tRF-5b in all the analyzed tRNAs. To confirm this, 293T NoDice cells, which in the absence of Dicer activity do not generate tRF-5b, were used. MDPI 2022-03-26 /pmc/articles/PMC8998818/ /pubmed/35409004 http://dx.doi.org/10.3390/ijms23073644 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Kazimierczyk, Marek
Wojnicka, Marta
Biała, Ewa
Żydowicz-Machtel, Paulina
Imiołczyk, Barbara
Ostrowski, Tomasz
Kurzyńska-Kokorniak, Anna
Wrzesinski, Jan
Characteristics of Transfer RNA-Derived Fragments Expressed during Human Renal Cell Development: The Role of Dicer in tRF Biogenesis
title Characteristics of Transfer RNA-Derived Fragments Expressed during Human Renal Cell Development: The Role of Dicer in tRF Biogenesis
title_full Characteristics of Transfer RNA-Derived Fragments Expressed during Human Renal Cell Development: The Role of Dicer in tRF Biogenesis
title_fullStr Characteristics of Transfer RNA-Derived Fragments Expressed during Human Renal Cell Development: The Role of Dicer in tRF Biogenesis
title_full_unstemmed Characteristics of Transfer RNA-Derived Fragments Expressed during Human Renal Cell Development: The Role of Dicer in tRF Biogenesis
title_short Characteristics of Transfer RNA-Derived Fragments Expressed during Human Renal Cell Development: The Role of Dicer in tRF Biogenesis
title_sort characteristics of transfer rna-derived fragments expressed during human renal cell development: the role of dicer in trf biogenesis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8998818/
https://www.ncbi.nlm.nih.gov/pubmed/35409004
http://dx.doi.org/10.3390/ijms23073644
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