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2 résultat(s) recherche sur le mot-clé 'Genomic Surveillance'
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"ANALYSE GÉNOMIQUE DU SARS-COV-2 AU MAROC & IDENTIFICATION DES BIOMARQUEURS DU CANCER DE SEIN CHEZ DES PATIENTES GHANÉENNES " / EL JARJINI Rabab
Titre : "ANALYSE GÉNOMIQUE DU SARS-COV-2 AU MAROC & IDENTIFICATION DES BIOMARQUEURS DU CANCER DE SEIN CHEZ DES PATIENTES GHANÉENNES " Type de document : thèse Auteurs : EL JARJINI Rabab, Auteur Année de publication : 2024 Langues : Anglais (eng) Mots-clés : SARS-CoV-2 genomic surveillance variants Morocco Breast cancer Ghanaian population Genetic mutations whole exome sequencing data SARS-CoV-2 surveillance génomique variants Maroc cancer du sein population ghanéenne mutations génétiques données de séquençage de l'exome complet SARS-CoV-2 المراقبة الجينومية المتغيرات المغرب سرطان الثدي السكان الغانيون الطفرات الجينية بيانات تسلس ل اإلكسوم الكام ل Résumé : This study includes two genomic research initiatives that emphasize the crucial importance of Next generation sequencing and bioinformatics. The first study focused on the genomic surveillance of SARS-CoV-2 in Morocco from 2022 to 2023, employing Ion Torrent technology to sequence viral samples and detect the circulating variants in Morocco. We found that Omicron and Delta variants were present during this period, which impact transmissibility, vaccine efficacy, and disease severity. Variant distribution plots and a phylogenetic tree were generated to provide detailed insights into the genomic landscape of the pathogen.
The second project aimed to characterize the mutations associated with breast cancer within the Ghanaian population using whole exome sequencing data. Significant mutations were identified in key genes, including BRCA1, BARD1, and TP53. The application of bioinformatic tools enabled high-resolution detection and comprehensive analysis of genetic alterations across different types of samples. These findings underscore the importance of incorporating these genes into genetic testing panels for early detection and personalized treatment strategies.Numéro (Thèse ou Mémoire) : MM0222024 Président : OUADGHIRI Mouna, Directeur : RCHIAD Zineb ; DAOUDA Tariq ; CHAOUNI Bouchra Co-encadrante Juge : KANDOUSSI Ilham Juge : OUDGHIRI Amal "ANALYSE GÉNOMIQUE DU SARS-COV-2 AU MAROC & IDENTIFICATION DES BIOMARQUEURS DU CANCER DE SEIN CHEZ DES PATIENTES GHANÉENNES " [thèse] / EL JARJINI Rabab, Auteur . - 2024.
Langues : Anglais (eng)
Mots-clés : SARS-CoV-2 genomic surveillance variants Morocco Breast cancer Ghanaian population Genetic mutations whole exome sequencing data SARS-CoV-2 surveillance génomique variants Maroc cancer du sein population ghanéenne mutations génétiques données de séquençage de l'exome complet SARS-CoV-2 المراقبة الجينومية المتغيرات المغرب سرطان الثدي السكان الغانيون الطفرات الجينية بيانات تسلس ل اإلكسوم الكام ل Résumé : This study includes two genomic research initiatives that emphasize the crucial importance of Next generation sequencing and bioinformatics. The first study focused on the genomic surveillance of SARS-CoV-2 in Morocco from 2022 to 2023, employing Ion Torrent technology to sequence viral samples and detect the circulating variants in Morocco. We found that Omicron and Delta variants were present during this period, which impact transmissibility, vaccine efficacy, and disease severity. Variant distribution plots and a phylogenetic tree were generated to provide detailed insights into the genomic landscape of the pathogen.
The second project aimed to characterize the mutations associated with breast cancer within the Ghanaian population using whole exome sequencing data. Significant mutations were identified in key genes, including BRCA1, BARD1, and TP53. The application of bioinformatic tools enabled high-resolution detection and comprehensive analysis of genetic alterations across different types of samples. These findings underscore the importance of incorporating these genes into genetic testing panels for early detection and personalized treatment strategies.Numéro (Thèse ou Mémoire) : MM0222024 Président : OUADGHIRI Mouna, Directeur : RCHIAD Zineb ; DAOUDA Tariq ; CHAOUNI Bouchra Co-encadrante Juge : KANDOUSSI Ilham Juge : OUDGHIRI Amal Réservation
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Code barre Cote Support Localisation Section Disponibilité MM0222024 WA Thèse imprimé Unité des Thèses et Mémoires Mémoires de Masters Disponible EVOLUTIONARY DYNAMICS OF SARS-COV-2 DELTA AND OMICRON VARIANTS IN MOROCCO: WHOLE GENOME SEQUENCING AND GENOMIC ANALYSIS / EL MAZOURI SAFAE
Titre : EVOLUTIONARY DYNAMICS OF SARS-COV-2 DELTA AND OMICRON VARIANTS IN MOROCCO: WHOLE GENOME SEQUENCING AND GENOMIC ANALYSIS Type de document : thèse Auteurs : EL MAZOURI SAFAE, Auteur Année de publication : 2024 Langues : Anglais (eng) Mots-clés : SARS-CoV-2 Variants Genomic Surveillance Evolutionary Dynamics Spike
Protein Pandemic Variants du SARS-CoV-2 Surveillance Génomique Dynamique Évolutive Protéine Spike Pandémie سالالت فيروس سارس-كوف2- مراقبة جينية ديناميات تطورية بروتين سبايك جائحةRésumé : The COVID-19 pandemic, caused by the novel coronavirus SARS-CoV-2, has posed
unprecedented global health challenges. This thesis provides a comprehensive monitoring of
the genetic characteristics and evolutionary patterns of the Delta and Omicron variants of
SARS-CoV-2 in Morocco. Employing the Ion Torrent S5 Prime for Next Generation
Sequencing, we have sequenced 415 of SARS-CoV-2 genomes, submitted to the GISAID
database, from March 2020 to November 2022. The dataset specifically emphasizes the analysis
of 164 Delta and 937 Omicron genomes originating from Morocco. For the Delta variant, our
research detects at least four separate introductions into Morocco, linked to international
sources. The Delta sub-lineage AY.33 was found to be dominant in the region. This study also
uncovers three mutations in the Spike protein's N-terminal domain (NTD) specific to Moroccan
AY.33 isolates: T29A, T250I, and T299I. These mutations may affect the Spike protein's
function and have implications for the variant's behavior. In studying the Omicron variant, our
analysis identifies a distinctive genetic diversity in Moroccan SARS-CoV-2 genomes,
diverging from other global strains. This variant was introduced into Morocco through multiple
sources, as evidenced by the genomic data. Among the Omicron lineages, certain clades
demonstrated higher transmissibility, with clade 22E becoming globally dominant. Notably,
mutations in the Receptor-Binding Domain (RBD) of the Spike protein, such as K444T and
N460K, were identified. These mutations potentially enhance the variant's ability to evade
immunity conferred by vaccines. The findings from this research emphasize the importance of
continuous genomic surveillance to understand local and global genomic dynamics of SARS-
CoV-2. This approach is vital for effective pandemic response and for preparing public health
measures to mitigate the spread of current and future variants. This thesis not only enhances
our understanding of the COVID-19 pandemic in Morocco but also offers valuable insights for
international public health considerations.Numéro (Thèse ou Mémoire) : D0052024 Président : Abdelilah LARAQUI Directeur : Mouna OUADGHIRI Juge : Abdenbi EL KARKOURI Juge : Hicham EL ANNAZ Juge : Yassir BOUSLIMAN ; Abdelhakim BOUYAHYA ; Tarik AANNIZ EVOLUTIONARY DYNAMICS OF SARS-COV-2 DELTA AND OMICRON VARIANTS IN MOROCCO: WHOLE GENOME SEQUENCING AND GENOMIC ANALYSIS [thèse] / EL MAZOURI SAFAE, Auteur . - 2024.
Langues : Anglais (eng)
Mots-clés : SARS-CoV-2 Variants Genomic Surveillance Evolutionary Dynamics Spike
Protein Pandemic Variants du SARS-CoV-2 Surveillance Génomique Dynamique Évolutive Protéine Spike Pandémie سالالت فيروس سارس-كوف2- مراقبة جينية ديناميات تطورية بروتين سبايك جائحةRésumé : The COVID-19 pandemic, caused by the novel coronavirus SARS-CoV-2, has posed
unprecedented global health challenges. This thesis provides a comprehensive monitoring of
the genetic characteristics and evolutionary patterns of the Delta and Omicron variants of
SARS-CoV-2 in Morocco. Employing the Ion Torrent S5 Prime for Next Generation
Sequencing, we have sequenced 415 of SARS-CoV-2 genomes, submitted to the GISAID
database, from March 2020 to November 2022. The dataset specifically emphasizes the analysis
of 164 Delta and 937 Omicron genomes originating from Morocco. For the Delta variant, our
research detects at least four separate introductions into Morocco, linked to international
sources. The Delta sub-lineage AY.33 was found to be dominant in the region. This study also
uncovers three mutations in the Spike protein's N-terminal domain (NTD) specific to Moroccan
AY.33 isolates: T29A, T250I, and T299I. These mutations may affect the Spike protein's
function and have implications for the variant's behavior. In studying the Omicron variant, our
analysis identifies a distinctive genetic diversity in Moroccan SARS-CoV-2 genomes,
diverging from other global strains. This variant was introduced into Morocco through multiple
sources, as evidenced by the genomic data. Among the Omicron lineages, certain clades
demonstrated higher transmissibility, with clade 22E becoming globally dominant. Notably,
mutations in the Receptor-Binding Domain (RBD) of the Spike protein, such as K444T and
N460K, were identified. These mutations potentially enhance the variant's ability to evade
immunity conferred by vaccines. The findings from this research emphasize the importance of
continuous genomic surveillance to understand local and global genomic dynamics of SARS-
CoV-2. This approach is vital for effective pandemic response and for preparing public health
measures to mitigate the spread of current and future variants. This thesis not only enhances
our understanding of the COVID-19 pandemic in Morocco but also offers valuable insights for
international public health considerations.Numéro (Thèse ou Mémoire) : D0052024 Président : Abdelilah LARAQUI Directeur : Mouna OUADGHIRI Juge : Abdenbi EL KARKOURI Juge : Hicham EL ANNAZ Juge : Yassir BOUSLIMAN ; Abdelhakim BOUYAHYA ; Tarik AANNIZ Réservation
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Exemplaires
Code barre Cote Support Localisation Section Disponibilité D0052024 WA Thèse imprimé Unité des Thèses et Mémoires Doctorat SVS 2024 Disponible