Genomic profile of pharmacogenetic  markers and fitting prediction models for maintenance doses of warfarin

Detalhes bibliográficos
Autor(a) principal: Neyra, Jennifer Eliana Montoya
Data de Publicação: 2024
Tipo de documento: Tese
Idioma: eng
Título da fonte: Biblioteca Digital de Teses e Dissertações da USP
Texto Completo: https://www.teses.usp.br/teses/disponiveis/95/95131/tde-23082024-202433/
Resumo: The admixed Brazilian population is highly heterogeneous, which has implications in health, disease, and also susceptibility to therapeutic regimens due to the underlying genetic variability from ancestral populations. Genomic data were composed of independent individuals selected from the ISA-Nutrição projects (N = 681), Projeto Coração Baependi (N = 548) and the Trios do project (N = 136). These data were subjected to genetic quality control per individual and polymorphism, identification of the haplotypic phase, imputation of variants not covered by the genotyping, and, filtering of variants with low imputation quality. Then, haplotypes were derived for global and local ancestry and the filtered post-imputation data were used to characterize the distribution of the pharmacogenetic markers of interest. Global ancestry was analyzed using Principal Component Analysis, and the average distribution of each population inferred by clustering with FastStructure was also evaluated. Local ancestry was calculated using RFMix and was explored by the average distribution at each locus, in addition, the polygenic risk score was calculated to compare regions of lower and higher ancestral variability between the studied cohorts. Also, we look for evidence of positive selection in the genome based on the average contribution of local ancestry. Six SNPs (rs10916661, rs10871454, rs749671, rs34707540, rs6897106, and rs2108622) differed from the global population panel. The overall average ancestral composition was 18.3% (SD = 18.5%) African, 5.2% (SD = 6%) Native American, 3.1% (SD = 3%) Asian, and 75.4% (SD = 19.6%) European compared to local ancestry with 22.2% (SD = 1.2), 5.1% (SD = 1.5), 2.1% (SD = 1.0) and 70.4% (SD = 2,3) respectively. The inferred local genetic profile presents heterogeneity between individuals, we have those with homogeneous ancestry (> 99%) and others in different stages of miscegenation, including individuals with a heterogeneous profile with a predominance of a single ancestor of around 30%. It was found that 48.2% of the samples had a polygenic risk greater than zero. Furthermore, no areas with signs of positive selection were found throughout the genome in our data. The variable ancestral profile was identified between our Brazilian admixed samples and genetic variants exhibiting varying frequencies in homogeneous global populations. However, the regression model with variables selected by the Stepwise method (AIC) did not perform well for individuals who required warfarin doses greater than 50 mg/week, possibly due to the absence of a factor capable of controlling dose variability in the model.
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spelling Genomic profile of pharmacogenetic  markers and fitting prediction models for maintenance doses of warfarinPerfil genômico de marcadores farmacogenéticos e ajuste de modelos de predição para doses de manutenção de varfarina.admixed populationancestralidade localFarmacogenéticalocal ancestrymodelos de prediçãoPharmacogeneticspopulação mistaprediction modelsvarfarina.warfarin.The admixed Brazilian population is highly heterogeneous, which has implications in health, disease, and also susceptibility to therapeutic regimens due to the underlying genetic variability from ancestral populations. Genomic data were composed of independent individuals selected from the ISA-Nutrição projects (N = 681), Projeto Coração Baependi (N = 548) and the Trios do project (N = 136). These data were subjected to genetic quality control per individual and polymorphism, identification of the haplotypic phase, imputation of variants not covered by the genotyping, and, filtering of variants with low imputation quality. Then, haplotypes were derived for global and local ancestry and the filtered post-imputation data were used to characterize the distribution of the pharmacogenetic markers of interest. Global ancestry was analyzed using Principal Component Analysis, and the average distribution of each population inferred by clustering with FastStructure was also evaluated. Local ancestry was calculated using RFMix and was explored by the average distribution at each locus, in addition, the polygenic risk score was calculated to compare regions of lower and higher ancestral variability between the studied cohorts. Also, we look for evidence of positive selection in the genome based on the average contribution of local ancestry. Six SNPs (rs10916661, rs10871454, rs749671, rs34707540, rs6897106, and rs2108622) differed from the global population panel. The overall average ancestral composition was 18.3% (SD = 18.5%) African, 5.2% (SD = 6%) Native American, 3.1% (SD = 3%) Asian, and 75.4% (SD = 19.6%) European compared to local ancestry with 22.2% (SD = 1.2), 5.1% (SD = 1.5), 2.1% (SD = 1.0) and 70.4% (SD = 2,3) respectively. The inferred local genetic profile presents heterogeneity between individuals, we have those with homogeneous ancestry (> 99%) and others in different stages of miscegenation, including individuals with a heterogeneous profile with a predominance of a single ancestor of around 30%. It was found that 48.2% of the samples had a polygenic risk greater than zero. Furthermore, no areas with signs of positive selection were found throughout the genome in our data. The variable ancestral profile was identified between our Brazilian admixed samples and genetic variants exhibiting varying frequencies in homogeneous global populations. However, the regression model with variables selected by the Stepwise method (AIC) did not perform well for individuals who required warfarin doses greater than 50 mg/week, possibly due to the absence of a factor capable of controlling dose variability in the model.A população brasileira moderna é altamente heterogênea, tendo implicações para a saúde, doenças e também para a suscetibilidade a regimes terapêuticos devido à variabilidade genética subjacente derivada da miscigenação de populações ancestrais. Os dados genômicos foram compostos por indivíduos independentes selecionados dos projetos do ISA-Nutrição (N = 681), Projeto Coração Baependi (N = 548) e do projeto Trios do Sudeste Brasileiro (N = 136). Esses dados passaram controle de qualidade genético por indivíduo e por polimorfismo, identificação da fase haplotípica, imputação de variantes não cobertas pela genotipagem e, por último, filtragem de variantes com baixa qualidade de imputação. Seguidamente, os haplótipos foram derivados para ancestralidade global e local e os dados filtrados pós-imputação foram utilizados na caracterização da distribuição dos marcadores farmacogenéticos de interesse. A ancestralidade global foi analisada por meio da Análise de Componentes Principais, também foi avaliada a distribuição média de cada população inferida por agrupamento com FastStructure. A ancestralidade local foi calculada usando RFMix e foi explorada pela distribuição média em cada locus. Além disso, foi calculado o escore de risco poligênico para comparar regiões de menor e maior variabilidade ancestral entre as coortes estudadas. Também, procuramos evidências de seleção positiva no genoma em base a contribuição média da ancestralidade local. Foi usado um quarto conjunto de dados (N = 766) contendo amostras do InCor-USP, pacientes com diagnóstico de fibrilação atrial, acidente vascular cerebral, trombose ou prótese valvar cardíaca, e que também hajam obtido valores INR entre dois e três após receberem dose semanal constante de varfarina. Os modelos avaliados foram Regressão Linear Múltipla, Regressão Linear com seleção de características (AIC), com métodos penalizados, Floresta Aleatória e Redes Neurais. As métricas de desempenho foram o erro quadrático médio (MSE), a raiz do erro quadrático médio (RMSE) e o erro médio absoluto (MAE). Seis SNPs (rs10916661, rs10871454, rs749671, rs34707540, rs6897106, e rs2108622) diferiram do painel de populações mundiais. A composição ancestral média global foi de 18,3% (DP = 18,5%) africano, 5,2% (DP = 6%) nativo americano, 3,1 % (DP = 3%) Asiático e 75,4% (DP = 19,6%) Europeu em comparação a ancestralidade local com 22,2% (DP = 1,2), 5,1% (DP = 1,5), 2,1% (DP = 1,0) e 70,4% (DP = 2,3) respectivamente. O perfil genético local inferido apresenta heterogeneidade entre os indivíduos, temos aqueles com ancestralidade homogênea (> 99%) e outros em diferentes estágios de miscigenação, inclusive tem indivíduos com perfil heterogêneo com predominância de um único ancestral ao redor de 30%. Se obteve que 48.2% das amostras tiveram risco poligênico maior de zero. Além disso, não foram encontradas zonas com indícios de seleção positiva ao longo do genoma nos nossos dados. Identificamos um diversidad de estruturas ancestrais entre os indivíduos que compõem nossa amostra miscigenada brasileira e variantes farmacogenéticas com frequências diferenciadas das populações globais. Por outro lado, obtivemos que o modelo de regressão com variáveis selecionadas pelo método Stepwise (AIC) foi de melhor rendimento, mas não teve bom desempenho para indivíduos que precisaram doses de varfarina superiores a 50 mg/semana, isto possivelmente devido à ausência de um marcador capaz de controlar a variabilidade da dose.Biblioteca Digitais de Teses e Dissertações da USPSoler, Julia Maria PavanNeyra, Jennifer Eliana Montoya2024-06-24info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/doctoralThesisapplication/pdfhttps://www.teses.usp.br/teses/disponiveis/95/95131/tde-23082024-202433/reponame:Biblioteca Digital de Teses e Dissertações da USPinstname:Universidade de São Paulo (USP)instacron:USPLiberar o conteúdo para acesso público.info:eu-repo/semantics/openAccesseng2024-10-22T14:37:03Zoai:teses.usp.br:tde-23082024-202433Biblioteca Digital de Teses e Dissertaçõeshttp://www.teses.usp.br/PUBhttp://www.teses.usp.br/cgi-bin/mtd2br.plvirginia@if.usp.br|| atendimento@aguia.usp.br||virginia@if.usp.bropendoar:27212024-10-22T14:37:03Biblioteca Digital de Teses e Dissertações da USP - Universidade de São Paulo (USP)false
dc.title.none.fl_str_mv Genomic profile of pharmacogenetic  markers and fitting prediction models for maintenance doses of warfarin
Perfil genômico de marcadores farmacogenéticos e ajuste de modelos de predição para doses de manutenção de varfarina.
title Genomic profile of pharmacogenetic  markers and fitting prediction models for maintenance doses of warfarin
spellingShingle Genomic profile of pharmacogenetic  markers and fitting prediction models for maintenance doses of warfarin
Neyra, Jennifer Eliana Montoya
admixed population
ancestralidade local
Farmacogenética
local ancestry
modelos de predição
Pharmacogenetics
população mista
prediction models
varfarina.
warfarin.
title_short Genomic profile of pharmacogenetic  markers and fitting prediction models for maintenance doses of warfarin
title_full Genomic profile of pharmacogenetic  markers and fitting prediction models for maintenance doses of warfarin
title_fullStr Genomic profile of pharmacogenetic  markers and fitting prediction models for maintenance doses of warfarin
title_full_unstemmed Genomic profile of pharmacogenetic  markers and fitting prediction models for maintenance doses of warfarin
title_sort Genomic profile of pharmacogenetic  markers and fitting prediction models for maintenance doses of warfarin
author Neyra, Jennifer Eliana Montoya
author_facet Neyra, Jennifer Eliana Montoya
author_role author
dc.contributor.none.fl_str_mv Soler, Julia Maria Pavan
dc.contributor.author.fl_str_mv Neyra, Jennifer Eliana Montoya
dc.subject.por.fl_str_mv admixed population
ancestralidade local
Farmacogenética
local ancestry
modelos de predição
Pharmacogenetics
população mista
prediction models
varfarina.
warfarin.
topic admixed population
ancestralidade local
Farmacogenética
local ancestry
modelos de predição
Pharmacogenetics
população mista
prediction models
varfarina.
warfarin.
description The admixed Brazilian population is highly heterogeneous, which has implications in health, disease, and also susceptibility to therapeutic regimens due to the underlying genetic variability from ancestral populations. Genomic data were composed of independent individuals selected from the ISA-Nutrição projects (N = 681), Projeto Coração Baependi (N = 548) and the Trios do project (N = 136). These data were subjected to genetic quality control per individual and polymorphism, identification of the haplotypic phase, imputation of variants not covered by the genotyping, and, filtering of variants with low imputation quality. Then, haplotypes were derived for global and local ancestry and the filtered post-imputation data were used to characterize the distribution of the pharmacogenetic markers of interest. Global ancestry was analyzed using Principal Component Analysis, and the average distribution of each population inferred by clustering with FastStructure was also evaluated. Local ancestry was calculated using RFMix and was explored by the average distribution at each locus, in addition, the polygenic risk score was calculated to compare regions of lower and higher ancestral variability between the studied cohorts. Also, we look for evidence of positive selection in the genome based on the average contribution of local ancestry. Six SNPs (rs10916661, rs10871454, rs749671, rs34707540, rs6897106, and rs2108622) differed from the global population panel. The overall average ancestral composition was 18.3% (SD = 18.5%) African, 5.2% (SD = 6%) Native American, 3.1% (SD = 3%) Asian, and 75.4% (SD = 19.6%) European compared to local ancestry with 22.2% (SD = 1.2), 5.1% (SD = 1.5), 2.1% (SD = 1.0) and 70.4% (SD = 2,3) respectively. The inferred local genetic profile presents heterogeneity between individuals, we have those with homogeneous ancestry (> 99%) and others in different stages of miscegenation, including individuals with a heterogeneous profile with a predominance of a single ancestor of around 30%. It was found that 48.2% of the samples had a polygenic risk greater than zero. Furthermore, no areas with signs of positive selection were found throughout the genome in our data. The variable ancestral profile was identified between our Brazilian admixed samples and genetic variants exhibiting varying frequencies in homogeneous global populations. However, the regression model with variables selected by the Stepwise method (AIC) did not perform well for individuals who required warfarin doses greater than 50 mg/week, possibly due to the absence of a factor capable of controlling dose variability in the model.
publishDate 2024
dc.date.none.fl_str_mv 2024-06-24
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/doctoralThesis
format doctoralThesis
status_str publishedVersion
dc.identifier.uri.fl_str_mv https://www.teses.usp.br/teses/disponiveis/95/95131/tde-23082024-202433/
url https://www.teses.usp.br/teses/disponiveis/95/95131/tde-23082024-202433/
dc.language.iso.fl_str_mv eng
language eng
dc.relation.none.fl_str_mv
dc.rights.driver.fl_str_mv Liberar o conteúdo para acesso público.
info:eu-repo/semantics/openAccess
rights_invalid_str_mv Liberar o conteúdo para acesso público.
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
dc.coverage.none.fl_str_mv
dc.publisher.none.fl_str_mv Biblioteca Digitais de Teses e Dissertações da USP
publisher.none.fl_str_mv Biblioteca Digitais de Teses e Dissertações da USP
dc.source.none.fl_str_mv
reponame:Biblioteca Digital de Teses e Dissertações da USP
instname:Universidade de São Paulo (USP)
instacron:USP
instname_str Universidade de São Paulo (USP)
instacron_str USP
institution USP
reponame_str Biblioteca Digital de Teses e Dissertações da USP
collection Biblioteca Digital de Teses e Dissertações da USP
repository.name.fl_str_mv Biblioteca Digital de Teses e Dissertações da USP - Universidade de São Paulo (USP)
repository.mail.fl_str_mv virginia@if.usp.br|| atendimento@aguia.usp.br||virginia@if.usp.br
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