Experimental supporting data on DIS3L2 over nonsense-mediated mRNA decay targets in human cells

In this article, we present supportive data related to the research article “A role for DIS3L2 over natural nonsense-mediated mRNA decay targets in human cells” [1], where interpretation of the data presented here is available. Indeed, here we analyze the impact of the DIS3L2 exoribonuclease over no...

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Detalhes bibliográficos
Autor principal: da Costa, Paulo J. (author)
Outros Autores: Menezes, Juliane (author), Saramago, Margarida (author), García-Moreno, Juan F. (author), Santos, Hugo A. (author), Gama-Carvalho, Margarida (author), Arraiano, Cecília M. (author), Viegas, Sandra C. (author), Romão, Luísa (author)
Formato: other
Idioma:eng
Publicado em: 2020
Assuntos:
DIS3L2
mRNA degradation
mRNA surveillance
NMD
NMD-targets
UPF1
General
Texto completo:http://hdl.handle.net/10362/102671
País:Portugal
Oai:oai:run.unl.pt:10362/102671
Descrição
Resumo:In this article, we present supportive data related to the research article “A role for DIS3L2 over natural nonsense-mediated mRNA decay targets in human cells” [1], where interpretation of the data presented here is available. Indeed, here we analyze the impact of the DIS3L2 exoribonuclease over nonsense-mediated mRNA decay (NMD)-targets. Specifically, we present data on: a) the expression of various reporter human β-globin mRNAs, monitored by Northern blot and RT-qPCR, before and after altering DIS3L2 levels in HeLa cells, and b) the gene expression levels of deregulated transcripts generated by re-analyzing publicly available data from UPF1-depleted HeLa cells that were further cross-referenced with a dataset of transcripts upregulated in DIS3L2-depleted cells. These analyses revealed that DIS3L2 regulates the levels of a subset of NMD-targets. These data can be valuable for researchers interested in the NMD mechanism.

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