Tent4a non‐canonical poly(A) polymerase regulates dna‐damage tolerance via multiple pathways that are mutated in endometrial cancer

Umakanta Swain, Gilgi Friedlander, Urmila Sehrawat, Avital Sarusi‐portuguez, Ron Rotkopf, Charlotte Ebert, Tamar Paz‐elizur, Rivka Dikstein, Thomas Carell, Nicholas E. Geacintov, Zvi Livneh

Research output: Contribution to journalArticlepeer-review

8 Scopus citations

Abstract

TENT4A (PAPD7) is a non‐canonical poly(A) polymerase, of which little is known. Here, we show that TENT4A regulates multiple biological pathways and focuses on its multilayer regulation of translesion DNA synthesis (TLS), in which error‐prone DNA polymerases bypass unre-paired DNA lesions. We show that TENT4A regulates mRNA stability and/or translation of DNA polymerase η and RAD18 E3 ligase, which guides the polymerase to replication stalling sites and monoubiquitinates PCNA, thereby enabling recruitment of error‐prone DNA polymerases to damaged DNA sites. Remarkably, in addition to the effect on RAD18 mRNA stability via controlling its poly(A) tail, TENT4A indirectly regulates RAD18 via the tumor suppressor CYLD and via the long non‐coding antisense RNA PAXIP1‐AS2, which had no known function. Knocking down the expression of TENT4A or CYLD, or overexpression of PAXIP1‐AS2 led each to reduced amounts of the RAD18 protein and DNA polymerase η, leading to reduced TLS, highlighting PAXIP1‐AS2 as a new TLS regulator. Bioinformatics analysis revealed that TLS error‐prone DNA polymerase genes and their TENT4A‐related regulators are frequently mutated in endometrial cancer genomes, sug-gesting that TLS is dysregulated in this cancer.

Original languageEnglish
Article number6957
JournalInternational Journal of Molecular Sciences
Volume22
Issue number13
DOIs
StatePublished - 28 Jun 2021
Externally publishedYes

Bibliographical note

Publisher Copyright:
© 2021 by the authors. Licensee MDPI, Basel, Switzerland.

Funding

Funding: This research was funded by the Flight Attendant Medical Research Institute, Florida, USA (FAMRI #032001 to Z.L. and T.P.E.); the Israel Science Foundation (#684/12 to Z.L.), and the Minerva Foundation (#120855) with funding from the Federal German Ministry for Education and Research (to Z.L.). Funding for open access charge: Flight Attendant Medical Research Institute, Florida, USA.

FundersFunder number
Federal German Ministry for Education and Research
Flight Attendant Medical Research Institute032001
Minerva Foundation120855
Israel Science Foundation684/12

    Keywords

    • DNA repair
    • Lesion bypass
    • Poly(A) RNA polymerase
    • TLS
    • Translesion

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