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Development of a method for generating SNP interaction-aware polygenic risk scores for radiotherapy toxicity

AIM: To identify the effect of single nucleotide polymorphism (SNP) interactions on the risk of toxicity following radiotherapy (RT) for prostate cancer (PCa) and propose a new method for polygenic risk score incorporating SNP-SNP interactions (PRSi). MATERIALS AND METHODS: Analysis included the REQ...

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Autores principales: Franco, Nicola Rares, Massi, Michela Carlotta, Ieva, Francesca, Manzoni, Andrea, Paganoni, Anna Maria, Zunino, Paolo, Veldeman, Liv, Ost, Piet, Fonteyne, Valérie, Talbot, Christopher J., Rattay, Tim, Webb, Adam, Johnson, Kerstie, Lambrecht, Maarten, Haustermans, Karin, De Meerleer, Gert, de Ruysscher, Dirk, Vanneste, Ben, Van Limbergen, Evert, Choudhury, Ananya, Elliott, Rebecca M., Sperk, Elena, Veldwijk, Marlon R., Herskind, Carsten, Avuzzi, Barbara, Noris Chiorda, Barbara, Valdagni, Riccardo, Azria, David, Farcy-Jacquet, Marie-Pierre, Brengues, Muriel, Rosenstein, Barry S., Stock, Richard G., Vega, Ana, Aguado-Barrera, Miguel E., Sosa-Fajardo, Paloma, Dunning, Alison M., Fachal, Laura, Kerns, Sarah L., Payne, Debbie, Chang-Claude, Jenny, Seibold, Petra, West, Catharine M.L., Rancati, Tiziana
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8754257/
https://www.ncbi.nlm.nih.gov/pubmed/33838170
http://dx.doi.org/10.1016/j.radonc.2021.03.024
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author Franco, Nicola Rares
Massi, Michela Carlotta
Ieva, Francesca
Manzoni, Andrea
Paganoni, Anna Maria
Zunino, Paolo
Veldeman, Liv
Ost, Piet
Fonteyne, Valérie
Talbot, Christopher J.
Rattay, Tim
Webb, Adam
Johnson, Kerstie
Lambrecht, Maarten
Haustermans, Karin
De Meerleer, Gert
de Ruysscher, Dirk
Vanneste, Ben
Van Limbergen, Evert
Choudhury, Ananya
Elliott, Rebecca M.
Sperk, Elena
Veldwijk, Marlon R.
Herskind, Carsten
Avuzzi, Barbara
Noris Chiorda, Barbara
Valdagni, Riccardo
Azria, David
Farcy-Jacquet, Marie-Pierre
Brengues, Muriel
Rosenstein, Barry S.
Stock, Richard G.
Vega, Ana
Aguado-Barrera, Miguel E.
Sosa-Fajardo, Paloma
Dunning, Alison M.
Fachal, Laura
Kerns, Sarah L.
Payne, Debbie
Chang-Claude, Jenny
Seibold, Petra
West, Catharine M.L.
Rancati, Tiziana
author_facet Franco, Nicola Rares
Massi, Michela Carlotta
Ieva, Francesca
Manzoni, Andrea
Paganoni, Anna Maria
Zunino, Paolo
Veldeman, Liv
Ost, Piet
Fonteyne, Valérie
Talbot, Christopher J.
Rattay, Tim
Webb, Adam
Johnson, Kerstie
Lambrecht, Maarten
Haustermans, Karin
De Meerleer, Gert
de Ruysscher, Dirk
Vanneste, Ben
Van Limbergen, Evert
Choudhury, Ananya
Elliott, Rebecca M.
Sperk, Elena
Veldwijk, Marlon R.
Herskind, Carsten
Avuzzi, Barbara
Noris Chiorda, Barbara
Valdagni, Riccardo
Azria, David
Farcy-Jacquet, Marie-Pierre
Brengues, Muriel
Rosenstein, Barry S.
Stock, Richard G.
Vega, Ana
Aguado-Barrera, Miguel E.
Sosa-Fajardo, Paloma
Dunning, Alison M.
Fachal, Laura
Kerns, Sarah L.
Payne, Debbie
Chang-Claude, Jenny
Seibold, Petra
West, Catharine M.L.
Rancati, Tiziana
author_sort Franco, Nicola Rares
collection PubMed
description AIM: To identify the effect of single nucleotide polymorphism (SNP) interactions on the risk of toxicity following radiotherapy (RT) for prostate cancer (PCa) and propose a new method for polygenic risk score incorporating SNP-SNP interactions (PRSi). MATERIALS AND METHODS: Analysis included the REQUITE PCa cohort that received external beam RT and was followed for 2 years. Late toxicity endpoints were: rectal bleeding, urinary frequency, haematuria, nocturia, decreased urinary stream. Among 43 literature-identified SNPs, the 30% most strongly associated with each toxicity were tested. SNP-SNP combinations (named SNP-allele sets) seen in ≥ 10% of the cohort were condensed into risk (RS) and protection (PS) scores, respectively indicating increased or decreased toxicity risk. Performance of RS and PS was evaluated by logistic regression. RS and PS were then combined into a single PRSi evaluated by area under the receiver operating characteristic curve (AUC). RESULTS: Among 1,387 analysed patients, toxicity rates were 11.7% (rectal bleeding), 4.0% (urinary frequency), 5.5% (haematuria), 7.8% (nocturia) and 17.1% (decreased urinary stream). RS and PS combined 8 to 15 different SNP-allele sets, depending on the toxicity endpoint. Distributions of PRSi differed significantly in patients with/without toxicity with AUCs ranging from 0.61 to 0.78. PRSi was better than the classical summed PRS, particularly for the urinary frequency, haematuria and decreased urinary stream endpoints. CONCLUSIONS: Our method incorporates SNP-SNP interactions when calculating PRS for radiotherapy toxicity. Our approach is better than classical summation in discriminating patients with toxicity and should enable incorporating genetic information to improve normal tissue complication probability models.
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spelling pubmed-87542572022-06-01 Development of a method for generating SNP interaction-aware polygenic risk scores for radiotherapy toxicity Franco, Nicola Rares Massi, Michela Carlotta Ieva, Francesca Manzoni, Andrea Paganoni, Anna Maria Zunino, Paolo Veldeman, Liv Ost, Piet Fonteyne, Valérie Talbot, Christopher J. Rattay, Tim Webb, Adam Johnson, Kerstie Lambrecht, Maarten Haustermans, Karin De Meerleer, Gert de Ruysscher, Dirk Vanneste, Ben Van Limbergen, Evert Choudhury, Ananya Elliott, Rebecca M. Sperk, Elena Veldwijk, Marlon R. Herskind, Carsten Avuzzi, Barbara Noris Chiorda, Barbara Valdagni, Riccardo Azria, David Farcy-Jacquet, Marie-Pierre Brengues, Muriel Rosenstein, Barry S. Stock, Richard G. Vega, Ana Aguado-Barrera, Miguel E. Sosa-Fajardo, Paloma Dunning, Alison M. Fachal, Laura Kerns, Sarah L. Payne, Debbie Chang-Claude, Jenny Seibold, Petra West, Catharine M.L. Rancati, Tiziana Radiother Oncol Article AIM: To identify the effect of single nucleotide polymorphism (SNP) interactions on the risk of toxicity following radiotherapy (RT) for prostate cancer (PCa) and propose a new method for polygenic risk score incorporating SNP-SNP interactions (PRSi). MATERIALS AND METHODS: Analysis included the REQUITE PCa cohort that received external beam RT and was followed for 2 years. Late toxicity endpoints were: rectal bleeding, urinary frequency, haematuria, nocturia, decreased urinary stream. Among 43 literature-identified SNPs, the 30% most strongly associated with each toxicity were tested. SNP-SNP combinations (named SNP-allele sets) seen in ≥ 10% of the cohort were condensed into risk (RS) and protection (PS) scores, respectively indicating increased or decreased toxicity risk. Performance of RS and PS was evaluated by logistic regression. RS and PS were then combined into a single PRSi evaluated by area under the receiver operating characteristic curve (AUC). RESULTS: Among 1,387 analysed patients, toxicity rates were 11.7% (rectal bleeding), 4.0% (urinary frequency), 5.5% (haematuria), 7.8% (nocturia) and 17.1% (decreased urinary stream). RS and PS combined 8 to 15 different SNP-allele sets, depending on the toxicity endpoint. Distributions of PRSi differed significantly in patients with/without toxicity with AUCs ranging from 0.61 to 0.78. PRSi was better than the classical summed PRS, particularly for the urinary frequency, haematuria and decreased urinary stream endpoints. CONCLUSIONS: Our method incorporates SNP-SNP interactions when calculating PRS for radiotherapy toxicity. Our approach is better than classical summation in discriminating patients with toxicity and should enable incorporating genetic information to improve normal tissue complication probability models. 2021-06 2021-04-08 /pmc/articles/PMC8754257/ /pubmed/33838170 http://dx.doi.org/10.1016/j.radonc.2021.03.024 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/ (https://creativecommons.org/licenses/by-nc-nd/4.0/) ).
spellingShingle Article
Franco, Nicola Rares
Massi, Michela Carlotta
Ieva, Francesca
Manzoni, Andrea
Paganoni, Anna Maria
Zunino, Paolo
Veldeman, Liv
Ost, Piet
Fonteyne, Valérie
Talbot, Christopher J.
Rattay, Tim
Webb, Adam
Johnson, Kerstie
Lambrecht, Maarten
Haustermans, Karin
De Meerleer, Gert
de Ruysscher, Dirk
Vanneste, Ben
Van Limbergen, Evert
Choudhury, Ananya
Elliott, Rebecca M.
Sperk, Elena
Veldwijk, Marlon R.
Herskind, Carsten
Avuzzi, Barbara
Noris Chiorda, Barbara
Valdagni, Riccardo
Azria, David
Farcy-Jacquet, Marie-Pierre
Brengues, Muriel
Rosenstein, Barry S.
Stock, Richard G.
Vega, Ana
Aguado-Barrera, Miguel E.
Sosa-Fajardo, Paloma
Dunning, Alison M.
Fachal, Laura
Kerns, Sarah L.
Payne, Debbie
Chang-Claude, Jenny
Seibold, Petra
West, Catharine M.L.
Rancati, Tiziana
Development of a method for generating SNP interaction-aware polygenic risk scores for radiotherapy toxicity
title Development of a method for generating SNP interaction-aware polygenic risk scores for radiotherapy toxicity
title_full Development of a method for generating SNP interaction-aware polygenic risk scores for radiotherapy toxicity
title_fullStr Development of a method for generating SNP interaction-aware polygenic risk scores for radiotherapy toxicity
title_full_unstemmed Development of a method for generating SNP interaction-aware polygenic risk scores for radiotherapy toxicity
title_short Development of a method for generating SNP interaction-aware polygenic risk scores for radiotherapy toxicity
title_sort development of a method for generating snp interaction-aware polygenic risk scores for radiotherapy toxicity
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8754257/
https://www.ncbi.nlm.nih.gov/pubmed/33838170
http://dx.doi.org/10.1016/j.radonc.2021.03.024
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