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The RNA-Binding Landscape of HAX1 Protein Indicates Its Involvement in Translation and Ribosome Assembly

Autor
Wiśniewska, Marta
Grzybowska, Ewa A.
Kudla, Grzegorz
Tollervey, David
Helwak, Aleksandra
Lyczek, Filip
Szostakowska-Rodzos, Malgorzata
Chmielarczyk, Mateusz
Rydzanicz, Malgorzata
Goryca, Krzysztof
Data publikacji
2022
Abstrakt (EN)

HAX1 is a human protein with no known homologues or structural domains. Mutations in the HAX1 gene cause severe congenital neutropenia through mechanisms that are poorly understood. Previous studies reported the RNA-binding capacity of HAX1, but the role of this binding in physiology and pathology remains unexplained. Here, we report the transcriptome-wide characterization of HAX1 RNA targets using RIP-seq and CRAC, indicating that HAX1 binds transcripts involved in translation, ribosome biogenesis, and rRNA processing. Using CRISPR knockouts, we find that HAX1 RNA targets partially overlap with transcripts downregulated in HAX1 KO, implying a role in mRNA stabilization. Gene ontology analysis demonstrated that genes differentially expressed in HAX1 KO (including genes involved in ribosome biogenesis and translation) are also enriched in a subset of genes whose expression correlates with HAX1 expression in four analyzed neoplasms. The functional connection to ribosome biogenesis was also demonstrated by gradient sedimentation ribosome profiles, which revealed differences in the small subunit:monosome ratio in HAX1 WT/KO. We speculate that changes in HAX1 expression may be important for the etiology of HAX1-linked diseases through dysregulation of translation.

Słowa kluczowe EN
RNA–protein binding
HAX1
RIP-seq
CRAC
translation
ribosome assembly
Dyscyplina PBN
nauki biologiczne
Czasopismo
Cells
Tom
11
Zeszyt
19
Strony od-do
2943 (1-22)
Data udostępnienia w otwartym dostępie
2022-09-20
Licencja otwartego dostępu
Uznanie autorstwa