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Mutations in a broad variety of genes can provoke the severe childhood disorder trichothiodystrophy (TTD) that is classified as a DNA repair disease or a transcription syndrome of RNA polymerase II. In an attempt to identify the common underlying pathomechanism of TTD we performed a knockout/knockdown of the two unrelated TTD factors TTDN1 and RNF113A and investigated the consequences on ribosomal biogenesis and performance. Interestingly, interference with these TTD factors created a nearly uniform impact on RNA polymerase I transcription with downregulation of UBF, disturbed rRNA processing and reduction of the backbone of the small ribosomal subunit rRNA 18S. This was accompanied by a reduced quality of decoding in protein translation and the accumulation of misfolded and carbonylated proteins, indicating a loss of protein homeostasis (proteostasis). As the loss of proteostasis by the ribosome has been identified in the other forms of TTD, here we postulate that ribosomal dysfunction is a common underlying pathomechanism of TTD.

Ribosomal Dysfunction Is a Common Pathomechanism in Different Forms of Trichothiodystrophy

Orioli D
Conceptualization
;
2023

Abstract

Mutations in a broad variety of genes can provoke the severe childhood disorder trichothiodystrophy (TTD) that is classified as a DNA repair disease or a transcription syndrome of RNA polymerase II. In an attempt to identify the common underlying pathomechanism of TTD we performed a knockout/knockdown of the two unrelated TTD factors TTDN1 and RNF113A and investigated the consequences on ribosomal biogenesis and performance. Interestingly, interference with these TTD factors created a nearly uniform impact on RNA polymerase I transcription with downregulation of UBF, disturbed rRNA processing and reduction of the backbone of the small ribosomal subunit rRNA 18S. This was accompanied by a reduced quality of decoding in protein translation and the accumulation of misfolded and carbonylated proteins, indicating a loss of protein homeostasis (proteostasis). As the loss of proteostasis by the ribosome has been identified in the other forms of TTD, here we postulate that ribosomal dysfunction is a common underlying pathomechanism of TTD.
2023
Istituto di Genetica Molecolare "Luigi Luca Cavalli Sforza"
Inglese
CELLS
WOS:001038040000001
12
14
1877
1897
21
2-s2.0-85165958375
https://pmc.ncbi.nlm.nih.gov/articles/PMC10377840/pdf/cells-12-01877.pdf
Esperti anonimi
ribosome
trichothiodystrophy
translational infidelity
loss of proteostasis
L'articolo è stato pubblicato su una rivista internazionale indicizzata e soggetta a revisione da parte di esperti del settore. Lo studio fornisce un importante avanzamento nella comprensione dei meccanismi molecolari e cellulari di una malattia genetica rara caratterizzata da invecchiamento precoce. Apre inoltre una nuova prospettiva di interpretazione che può in parte spiegare le caratteristiche cliniche della patologia.
Internazionale
Elettronico
9
info:eu-repo/semantics/article
262
Zhu, G; Khalid, F; Zhang, D; Cao, Z; Maity, P; Kestler, Ha; Orioli, D; Scharffetterkochanek, K; Iben, S
01 Contributo su Rivista::01.01 Articolo in rivista
open
   Basis of the different skin cancer risk in human disorders caused by mutations in the same gene, XPD
   AIRC
   ID 21737
01.01 Articolo in rivista
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/20.500.14243/457469
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