Functional evaluation of germline TP53 variants identified in Brazilian families at-risk for Li–Fraumeni syndrome

Abstract Germline TP53 pathogenic variants can lead to a cancer susceptibility syndrome known as Li–Fraumeni (LFS). Variants affecting its activity can drive tumorigenesis altering p53 pathways and their identification is crucial for assessing individual risk. This study explored the functional impa...

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書誌詳細
出版年:Scientific Reports
主要な著者: Renata B. V. Abreu, Ariane S. Pereira, Marcela N. Rosa, Patricia Ashton-Prolla, Viviane A. O. Silva, Matias E. Melendez, Edenir I. Palmero
フォーマット: 論文
言語:英語
出版事項: Nature Portfolio 2024-07-01
主題:
TP53
Variants of uncertain significance
Functional analysis
Transcription factor
DNA repair
Li–Fraumeni syndrome
オンライン・アクセス:https://doi.org/10.1038/s41598-024-67810-3
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author Renata B. V. Abreu
Ariane S. Pereira
Marcela N. Rosa
Patricia Ashton-Prolla
Viviane A. O. Silva
Matias E. Melendez
Edenir I. Palmero
author_facet Renata B. V. Abreu
Ariane S. Pereira
Marcela N. Rosa
Patricia Ashton-Prolla
Viviane A. O. Silva
Matias E. Melendez
Edenir I. Palmero
author_sort Renata B. V. Abreu
collection DOAJ
container_title Scientific Reports
description Abstract Germline TP53 pathogenic variants can lead to a cancer susceptibility syndrome known as Li–Fraumeni (LFS). Variants affecting its activity can drive tumorigenesis altering p53 pathways and their identification is crucial for assessing individual risk. This study explored the functional impact of TP53 missense variants on its transcription factor activity. We selected seven TP53 missense variants (c.129G > C, c.320A > G, c.417G > T, c.460G > A, c,522G > T, c.589G > A and c.997C > T) identified in Brazilian families at-risk for LFS. Variants were created through site-directed mutagenesis and transfected into SK-OV-3 cells to assess their transcription activation capabilities. Variants K139N and V197M displayed significantly reduced transactivation activity in a TP53-dependent luciferase reporter assay. Additionally, K139N negatively impacted CDKN1A and MDM2 expression and had a limited effect on GADD45A and PMAIP1 upon irradiation-induced DNA damage. Variant V197M demonstrated functional impact in all target genes evaluated and loss of Ser15 phosphorylation. K139N and V197M variants presented a reduction of p21 levels after irradiation. Our data show that K139N and V197M negatively impact p53 functions, supporting their classification as pathogenic variants. This underscores the significance of conducting functional studies on germline TP53 missense variants classified as variants of uncertain significance to ensure proper management of LFS-related cancer risks.
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spelling doaj-art-e45da8d2b79c463587803a601981cdf72025-08-19T23:20:58ZengNature PortfolioScientific Reports2045-23222024-07-0114111010.1038/s41598-024-67810-3Functional evaluation of germline TP53 variants identified in Brazilian families at-risk for Li–Fraumeni syndromeRenata B. V. Abreu0Ariane S. Pereira1Marcela N. Rosa2Patricia Ashton-Prolla3Viviane A. O. Silva4Matias E. Melendez5Edenir I. Palmero6Molecular Oncology Research Center, Barretos Cancer HospitalMolecular Oncology Research Center, Barretos Cancer HospitalMolecular Oncology Research Center, Barretos Cancer HospitalExperimental Research Center, Hospital de Clínicas de Porto AlegreMolecular Oncology Research Center, Barretos Cancer HospitalMolecular Oncology Research Center, Barretos Cancer HospitalMolecular Oncology Research Center, Barretos Cancer HospitalAbstract Germline TP53 pathogenic variants can lead to a cancer susceptibility syndrome known as Li–Fraumeni (LFS). Variants affecting its activity can drive tumorigenesis altering p53 pathways and their identification is crucial for assessing individual risk. This study explored the functional impact of TP53 missense variants on its transcription factor activity. We selected seven TP53 missense variants (c.129G > C, c.320A > G, c.417G > T, c.460G > A, c,522G > T, c.589G > A and c.997C > T) identified in Brazilian families at-risk for LFS. Variants were created through site-directed mutagenesis and transfected into SK-OV-3 cells to assess their transcription activation capabilities. Variants K139N and V197M displayed significantly reduced transactivation activity in a TP53-dependent luciferase reporter assay. Additionally, K139N negatively impacted CDKN1A and MDM2 expression and had a limited effect on GADD45A and PMAIP1 upon irradiation-induced DNA damage. Variant V197M demonstrated functional impact in all target genes evaluated and loss of Ser15 phosphorylation. K139N and V197M variants presented a reduction of p21 levels after irradiation. Our data show that K139N and V197M negatively impact p53 functions, supporting their classification as pathogenic variants. This underscores the significance of conducting functional studies on germline TP53 missense variants classified as variants of uncertain significance to ensure proper management of LFS-related cancer risks.https://doi.org/10.1038/s41598-024-67810-3TP53Variants of uncertain significanceFunctional analysisTranscription factorDNA repairLi–Fraumeni syndrome
spellingShingle Renata B. V. Abreu
Ariane S. Pereira
Marcela N. Rosa
Patricia Ashton-Prolla
Viviane A. O. Silva
Matias E. Melendez
Edenir I. Palmero
Functional evaluation of germline TP53 variants identified in Brazilian families at-risk for Li–Fraumeni syndrome
TP53
Variants of uncertain significance
Functional analysis
Transcription factor
DNA repair
Li–Fraumeni syndrome
title Functional evaluation of germline TP53 variants identified in Brazilian families at-risk for Li–Fraumeni syndrome
title_full Functional evaluation of germline TP53 variants identified in Brazilian families at-risk for Li–Fraumeni syndrome
title_fullStr Functional evaluation of germline TP53 variants identified in Brazilian families at-risk for Li–Fraumeni syndrome
title_full_unstemmed Functional evaluation of germline TP53 variants identified in Brazilian families at-risk for Li–Fraumeni syndrome
title_short Functional evaluation of germline TP53 variants identified in Brazilian families at-risk for Li–Fraumeni syndrome
title_sort functional evaluation of germline tp53 variants identified in brazilian families at risk for li fraumeni syndrome
topic TP53
Variants of uncertain significance
Functional analysis
Transcription factor
DNA repair
Li–Fraumeni syndrome
url https://doi.org/10.1038/s41598-024-67810-3
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