TFIIH is a complex essential for transcription of protein-coding genes by RNA polymerase II, DNA repair of UV-lesions and transcription of rRNA by RNA polymerase I. Mutations in TFIIH cause the cancer prone DNA-repair disorder xeroderma pigmentosum (XP) and the developmental and premature aging disorders trichothiodystrophy (TTD) and Cockayne syndrome. A total of 50% of the TTD cases are caused by TFIIH mutations. Using TFIIH mutant patient cells from TTD and XP subjects we can show that the stress-sensitivity of the proteome is reduced in TTD, but not in XP. Using three different methods to investigate the accuracy of protein synthesis by the ribosome, we demonstrate that translational fidelity of the ribosomes of TTD, but not XP cells, is decreased. The process of ribosomal synthesis and maturation is affected in TTD cells and can lead to instable ribosomes. Isolated ribosomes from TTD patients show an elevated error rate when challenged with oxidized mRNA, explaining the oxidative hypersensitivity of TTD cells. Treatment of TTD cells with N-acetyl cysteine normalized the increased translational error-rate and restored translational fidelity. Here we describe a pathomechanism that might be relevant for our understanding of impaired development and aging-associated neurodegeneration.

TFIIH mutations can impact on translational fidelity of the ribosome

Orioli D
Conceptualization
;
2023

Abstract

TFIIH is a complex essential for transcription of protein-coding genes by RNA polymerase II, DNA repair of UV-lesions and transcription of rRNA by RNA polymerase I. Mutations in TFIIH cause the cancer prone DNA-repair disorder xeroderma pigmentosum (XP) and the developmental and premature aging disorders trichothiodystrophy (TTD) and Cockayne syndrome. A total of 50% of the TTD cases are caused by TFIIH mutations. Using TFIIH mutant patient cells from TTD and XP subjects we can show that the stress-sensitivity of the proteome is reduced in TTD, but not in XP. Using three different methods to investigate the accuracy of protein synthesis by the ribosome, we demonstrate that translational fidelity of the ribosomes of TTD, but not XP cells, is decreased. The process of ribosomal synthesis and maturation is affected in TTD cells and can lead to instable ribosomes. Isolated ribosomes from TTD patients show an elevated error rate when challenged with oxidized mRNA, explaining the oxidative hypersensitivity of TTD cells. Treatment of TTD cells with N-acetyl cysteine normalized the increased translational error-rate and restored translational fidelity. Here we describe a pathomechanism that might be relevant for our understanding of impaired development and aging-associated neurodegeneration.
2023
Istituto di Genetica Molecolare "Luigi Luca Cavalli Sforza"
Inglese
32
7
1102
1113
12
https://pmc.ncbi.nlm.nih.gov/articles/PMC10026254/pdf/ddac268.pdf
Esperti anonimi
TFIIH mutations, translational fidelity, ribosome
La rivista pubblica studi di alta qualità relativi ai meccanismi molecolari delle malattie genetiche umane, spaziando dagli studi di analisi dei geni mutati alla suscettibilità alle malattie fino alle terapie.
Internazionale
Stampa
11
info:eu-repo/semantics/article
262
Khalid, F; Phan, T; Qiang, M; Maity, P; Lasser, T; Wiese, S; Penzo, M; Alupei, M; 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
   ID21737
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/20.500.14243/431516
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