Les défis du séquençage à haut débit dans l'exploration génétique des cancers du sein et de l'ovaire. / Challenges of Next Generation Sequencing in the exploration of genetic predispositions to breast and/or ovarian cancers

Muller, Etienne

12 December 2017

Les cancers du sein et de l’ovaire apparaissent dans 5 à 10% dans un contexte de prédisposition génétique, dont seule une faible part est expliquée par la présence d’un variant pathogène sur les gènes BRCA1, BRCA2 et PALB2. Le séquençage à haut-débit permet d’explorer cette hérédité manquante, mais représente un nouveau défi à la fois informatique, statistique et biologique. Trois approches utilisant cette nouvelle technologie ont été employées pour rechercher de nouveaux facteurs de prédisposition. En premier lieu, les risques associés à 34 gènes connus ou suspectés d’être impliqués dans les prédispositions ont été estimés à partir de l’analyse de 5 131 cas index et le développement d’une nouvelle approche statistique. Aussi la participation des néo-mutations en mosaïque dans le syndrome a été explorée à partir de 1 750 cas index issus de l’étude précédente, avec un logiciel de détection des variants faiblement représentés développé spécifiquement: outLyzer. Enfin, l’exploration par séquençage de l’hérédité manquante a été étendue à un panel de 201 gènes impliqués dans le cancer, à partir de 118 patientes sélectionnées pour la précocité d’apparition de leur maladie, élément fortement évocateur d’un facteur de prédisposition. Les résultats de ces travaux ont permis de valider la pertinence de l’étude de PALB2, RAD51C et RAD51D pour la prise en charge des patients, et suggèrent aussi une implication sous-estimée des variants en mosaïque. Cependant il reste encore très probablement d’autres facteurs génétiques fortement pénétrants à découvrir mais dont la modulation du risque répond à un modèle oligogénique. / Breast and ovarian cancers appear in 5 to 10% of cases in a context of genetic predisposition, of which only a small proportion is explained by the presence of a pathogenic variant on the BRCA1, BRCA2 and PALB2 genes. High throughput sequencing can explore this missing heredity, but represents a new challenge both in computing, statistics and biology. Three approaches using this new technology have been used to investigate new predisposition factors. First, the risks associated with 34 known or suspected genes involved in predispositions were estimated from the analysis of 5,131 index cases and the development of a new statistical approach. Also, the participation of mosaic neo-mutations in the syndrome was explored from 1,750 index cases from the previous study, with a software developed specifically for detecting poorly represented variants: outLyzer. Finally, the exploration by sequencing of the missing heredity was extended to a panel of 201 genes involved in cancer, from 118 patients selected for the early onset of their disease, a highly suggestive element of a predisposition factor. The results of this work validated the relevance of the PALB2, RAD51C and RAD51D study for patient management, and also suggested an underestimated involvement of mosaic variants. However, there are still very likely other highly penetrating genetic factors to be discovered, but whose risk modulation is based on an oligogenic model.

Séquençage de nouvelle génération

Séquençage à haut-débit

Bio-informatique

Mosaïque

Variant-calling

Next Generation Sequencing

High Throughput Sequencing

Bioinformatics

Mosaic

Variant-calling

660.65

Variants rares et analyse d'exomes : application à la maladie d'Alzheimer du sujet jeune / Rare variants and exomes analyses : the example of Early-Onset Alzheimer Disease

Le Guennec, Kilan

07 June 2017

L’avènement du séquençage haut débit permet actuellement d’étudier et d’analyser la part de lacomposante génétique des maladies complexes médiée par les variants rares. Cependant, leurinterprétation représente un défi majeur. En effet, le séquençage de milliers d’exomes et degénomes a révélé la complexité du polymorphisme humain et notamment la surreprésentation devariants rares. Et malgré le développement de logiciels d’analyse ainsi que de différentes bases dedonnées, la priorisation des variants rares reste difficile. Dans le cadre de cette thèse, nous avons focalisé nos analyses sur les variations génétiques rares impliquées dans la maladie d’Alzheimer (MA). D’un point de vue génétique, la MA répond dans une majorité des cas à un déterminisme multifactoriel mais une minorité des cas sont des formes précoces à transmission autosomique dominante. La caractérisation des gènes PSEN1, PSEN2 et APP responsables des formes mendéliennes de MA a permis de formuler l’hypothèse de la cascade amyloïde en plaçant le peptide amyloïde (Aβ) au centre du processus physiopathologique. Afin de détecter de nouveaux facteurs de risque génétique dans la survenue de la MA, nous avons réalisé une étude d’association à partir de données de séquençage d’exomes de 522 cas atteints de formes précoces de MA et 584 contrôles. Les premières analyses ont porté sur les variants mononucléotidiques ainsi que les courtes insertions/délétions et ont permis de mettre en évidence un enrichissement en variants rares prédits délétères dans le gène ABCA7 chez les individus malades. Notre attention s’est ensuite portée sur les variations du nombre de copies (CNVs). L’absence de récurrence à l’échelle d’un gène nous a amené à travailler sur une liste de gènes. En nous focalisant sur l’hypothèse amyloïdergique, nous avons construit une liste de 342 gènes impliqués dans le métabolisme et la toxicité du peptide Aβ. Grâce à cette stratégie, nous avons ainsi réussi à mettre en évidence un enrichissement de CNVs rares intersectant ce réseau centré sur le peptide Aβ. Le résultat majeur de cette étude de CNVs a été la mise en évidence d’une duplication du locus 17q21.31 chez 5 patients atteints d’une maladie neurodégénérative similaire à une maladie d’Alzheimer. Les patients porteurs présentent un diagnostic clinique de MA, des biomarqueurs et une imagerie métabolique en faveur d’une neurodégénérescence de type Alzheimer. En revanche, l’imagerie amyloïde et l’analyse neuropathologique n’ont pas révélé de pathologie amyloïde et sont donc en faveur d’une tauopathie pure. L’étude des CNVs a également révélé une délétion partielle du gène PSEN1, emportant les exons 9 et 10, pour laquelle nous avons pu réaliser des études fonctionnelles. Nous avons ainsi pu déterminer que la protéine mutante favorisait la production de peptides amyloïdes plus longs, ces derniers étant des médiateurs majeurs de la neurotoxicité d’Aβ. / Next-generation sequencing allows studying and analyzing the genetic component part of complexdiseases mediated by rare variants. However, their interpretation represents a major challenge.Indeed, the sequencing of thousands of exomes and genomes revealed the human polymorphismcomplexity and in particular the overrepresentation of rare variants. Despite the development ofsoftwares and variant databases, the prioritization of rare variants remains arduous. My thesis subject was focused on the involvement of rare variants in Alzheimer's disease (AD). From a genetic point of view, AD is caused, in most cases, by a multifactorial determinism, but a minority of cases are autosomal dominant early-onset forms (ADEOAD). The characterization of mutations in the PSEN1, PSEN2 and APP genes as a cause of these Mendelian forms of AD led to the formulationof the amyloid cascade hypothesis, stating that the amyloid-β peptide (Aβ) is triggering the pathophysiological process. In order to detect new genetic risk factors involved in AD, we performed an association study using exome sequencing data from 522 cases with early-onset Alzheimer Disease and 584 controls. The first analyzes focused on single nucleotide variants and short insertions / deletions, and revealed an enrichment in cases of variants that are predicted to be deleterious in the ABCA7 genes. We then then focused on copy number variations (CNVs). The lack of recurrence at the gene-level incited us to work on a gene list. By focusing on the amyloidogenic hypothesis, we built a list of 342 genes involved in the metabolism and toxicity of the Aβ peptide. Thanks to this strategy, we found an enrichment of rare CNVs intersecting this Aβ network in cases.The main result of this CNV study was the identification of a duplication of the 17q21.31 locus in 5patients with a neurodegenerative disease similar to Alzheimer's disease. These patients have aclinical diagnosis of AD, as well as biomarkers and metabolic imaging consistent with an ADneurodegeneration. However, amyloid imaging and neuropathological analysis did not reveal anyamyloid pathology, and were therefore pointing to a pure tauopathy. This CNV study also revealed a partial deletion of the PSEN1 gene, overlapping exons 9 and 10, for which we performed functional studies. We demonstrated that the mutant protein enhanced the production of longer amyloid peptides, the latter being major mediators of Aβ neurotoxicity.

Séquençage haut-débit

Exome

Etudes d'association

Maladie d'Alzheimer du sujet jeune

ABCA7

CNV

MAPT

17q21.31

PSEN1

Next-generation sequencing

Exome

Association study

Early-onset Alzheimer Disease

ABCA7

CNV

MAPT

17q21.31

PSEN1

616.831

Drug resistance genotyping and phylogenetic analysis of HIV in chronically infected antiretroviral naive patients

Baloyi, Tlangelani

18 May 2019

MSc (Microbiology) / Department of Microbiology / Background: Antiretroviral treatment (ART) has grown to be one of the most effective tool in the fight to control HIV/AIDS morbidity and mortality worldwide. However, due to the emergence of drug resistant HIV, ART efficacy can be jeopardized. Drug resistant HIV strain has a potential of becoming a major public threat, as its limit treatment options on people living with HIV. With several findings worldwide reporting drug resistant HIV to be currently being transmitted to ART-naïve persons, measures have been taken to genotype drug resistant HIV prior to treatment initiation. However, in resource limited countries such measures are not executed especially in public sectors due to the costs associated with the required assays for genotyping. Objective: The objectives of the study was to establish a deep sequencing protocol (Next Generation Sequencing-NGS) using an Illumina MiniSeq Platform and subsequently apply it to genotype HIV in chronically infected drug naïve persons for resistance mutations and viral genotypes Methods: HIV positive Individuals without any exposure to ART (Treatment-naive) were recruited. Partial pol fragment (complete protease and ~1104bp reverse transcriptase) were amplified and purified. Libraries were prepared using Nextera XT library preparation kit, fragmented, tagmented, pooled and denatured then sequenced with Illumina MiniSeq instrument. Consensus sequences were derived, aligned and phylogenetically analysed. The Stanford HIV Drug Resistance Algorithm was used to infer the presence of drug resistant mutants, at the viral minority and majority population levels. Results and discussion: An NGS protocol to generate nucleotide sequences for drug resistance inference was established. No major drug resistance mutations were detected against protease, reverse transcriptase inhibitors in the study subjects investigated. Nevertheless, V179D change was observed in one patient (8.3%). V179D has been shown to impact a low-level resistance to NNRTI. On the other hand, several secondary and unusual mutations at known drug sites were detected even at minority threshold level of <20%. Conclusion: No major drug resistance mutations was detected in the drug naïve study population. This finding suggests that there is no risk of treatment failure to the investigated subjects, however it is important to assess the potential phenotypic v | P a g e significance of the identified secondary resistance mutations in the context of HIV-1 subtype C. The established NGS protocol should be applied in subsequent HIV drug resistance studies. / NRF

HIV-1 Subtype C.

Next generation sequencing

Drug resistance mutations

Treatment naive patients

South Africa

616.9792010968

AIDS (Disease) -- South Africa

AIDS (Disease) -- Prevention

HIV-positive persons -- South Africa

Patients -- South Africa

HIV infections -- South Africa

Molekulárně genetické příčiny vývojových onemocnění předního segmentu oka / Anterior segment dysgenesis disorders and their molecular genetic cause

Moravíková, Jana

January 2018

Proper eye development depends on expression and mutual regulation of many genes. Anterior segment dysgenesis (ASD) are a highly heterogeneous group of diseases exhibiting all types of Mendelian inheritance, which manifest as combination of congenital abnormalities of the cornea, iris, anterior chamber angle or lens. Screening of genes associated with ASD does not often lead to the identification of the underlying genetic cause implying that there are still novel variants or genes to be discovered. Molecular genetic analysis in 12 probands with ASD using Sanger and whole-exome sequencing were performed. Functional analysis by Exon trapping assay was provided in variants predicted to effect pre-mRNA splicing. Four PAX6 mutations evaluated as pathogenic or likely pathogenic in a heterozygous state were found in four probands c.183C˃G; p.(Tyr61*), c.1032+1G>A, c.1183+1G>T and c.622C>T; p.(Arg208Trp). One proband was found to be a compound heterozygote for c.244A>G; p.(Met82Val) and c.541delG; p.(Glu181Lysfs*26) mutations in FOXE3. In 7 probands, no potentially pathogenic variants were identified. Exon trapping assay confirmed that mutations c.1032+1G>A and c.1183+1G>T have an effect on pre-mRNA splicing of the PAX6 gene. Detailed molecular-genetic analysis in patients with ASD may contribute to...

Role genu WT1 a dalších molekulárně-biologických abnormalit u germinálních nádorů varlat / The role of WT1 gene and other molecular biological abnormalities in testicular germ cell tumors

Bakardjieva - Mihaylova, Violeta

January 2020

Testicular germinal tumors (TGCT) are relatively rare solid tumors in adults. Even so, they affect more than 700 men a year in the Czech Republic, mostly young patients aged 18- 45 years. A large number of patients are curable by a combination of surgery and chemotherapy, yet about 50 men a year in the Czech Republic succumb to this tumor, in the vast majority of cases due to the development of resistance to chemotherapy containing cisplatin. The rare occurrence and high curability are probably the cause of infrequent molecular and clinical studies carried out in these tumors, and our understanding of the biological processes leading to primary tumor development and the development of cisplatin resistance (CDDP) is still limited. At present, no specific molecular markers that could be used as prognostic or predictive factors and improve patient stratification or treatment tailoring are available in TGCT management. In this work, we studied the molecular-genetic background of TGCT development and CDDP resistance at several levels. To comprehensively study the development of cisplatin resistance, we prepared and analyzed CDDP-exposed TGCT cell lines. Long-term exposure to CDDP increased resistance 10-fold in the NCCIT cell line, while no significant resistance was achieved with Tera-2. The...

Molekulárně genetická analýza pacientů s Usherovým syndromem / Molecular genetic analysis of patients with Usher syndrome

Průšová, Kateřina

January 2020

The work focuses on molecular genetic testing of patients with Usher syndrome to confirm the diagnosis, to determine the causal cause of the disease and describe new mutations causing Usher syndrome in Czech patients. Usher syndrome is a clinically and genetically heterogeneous disease that is the most common cause of hereditary deafblindness. Based on responsible genes and disease onset is classified into three clinical subtypes. Given the fact that there is currently no specific treatment, there is a need to understand the pathophysiology of this disease and to broaden the spectrum of causal mutations. The theoretical part of the thesis deals with the anatomy of the eye, especially the structure of the retina. Attention is also paid to retinal diseases, such as the progressive loss of vision characteristic for retinitis pigmentosa (RP). RP may occur either as an isolated disorder or also affecting other organs, so-called syndromic RP. Classic syndromic RP includes Usher's syndrome, which the work mainly deals with. The theoretical part of the thesis describes mainly the mechanism of the disease, the functions of individual Usher proteins and the genes that encode these proteins. The haplotype analysis has been previously done for the most common mutations causing Usher's syndrome in Europe Based...

Struktura, vývoj a funkce mikrobiálních společenstev v odumřelém dřevě / Assembly, successional development and functioning of microbial communities in deadwood

Bernardová, Natálie

January 2020

Dead wood is one of the most important reservoirs associated with forest ecosystems. In natural forests, its volume is counted in hundreds of m3 ha-1 , whereas it reaches only tens of m3 ha-1 in productive commercial forests. In contrast to soil and plant litter, deadwood is unevenly distributed on the forest floor. The specific physicochemical properties such as high content of recalcitrant polymers, low nitrogen level and impermeability negatively affect the rate of decomposition especially in the initial stages of wood deconstruction. The deadwood decomposition is very slow in comparisons with other substrates, it accumulates and thus it represents the important reservoir of nutrients. This thesis is focused on the structure, development and function of microbial (fungal) community in decomposing deadwood in unmanaged forest. Functional screening of fungi isolated from fruit bodies collected from coarse deadwood was set aside. Physico-chemical properties of deadwood including pH, carbon and nitrogen content and microbial biomass were estimated for four wood decomposition stages and three different tree species. New generation sequencing (Illumina MiSeq platform) was applied for fungal community structure analysis based on ITS2 fragment. Fungal functional screening was based on physico-chemical...

Integrating behavior, hormones and genes associated with the primate HPA-axis

Gutleb, Daria Raffaella

03 December 2018

No description available.

570

stress

aggression

HPA-axis

next-generation sequencing

behavioral genetics

single nucleotide polymorphism

catechol-O-methyltransferase

COMT Val158Met

dominance hierarchy

gene-environment

Macaca assamensis

macaque

non-human primate

rs4680

social rank

Val157Met

social buffering

Biologie (PPN619462639)

Impact des antibiotiques céfprozil et céfoxitine sur le microbiote Eggerthella lenta, lié au métabolisme du cardiotonique digoxine

Auger, Jérémie

12 1900

La digoxine est un cardiotonique largement employé pour contrôler les symptômes de l'insuffisance cardiaque et de la fibrillation auriculaire. Il est connu depuis les années 1980 que le métabolite principal de la digoxine, la dihydrodigoxine, est produit exclusivement par le microbiome intestinal (métabolisme de premier passage) et plus précisément la bactérie Eggerthella lenta. Aux États-Unis, c'est 14% des participants à une étude qui excrétaient 40% et plus de la dose sous la forme de ce métabolite rapidement éliminable et ayant perdu son affinité pour sa cible. De plus, chaque année, la digoxine est le médicament qui engendre le plus d'hospitalisations pour effets secondaires toxiques. Les effets secondaires très problématiques de la digoxine sont souvent déclenchés par l'ajout d'antibiotiques (surtout les macrolides) à la prescription de digoxine. La théorie explorée ici explique les évènements de toxicité chez les patients métabolisateurs. Ces derniers ont une dose quotidienne de maintien de digoxine plus élevée pour compenser l'action de la bactérie et, lorsque ces patients reçoivent un antibiotique pour une infection non reliée à leur condition cardiaque, l'arrêt du métabolisme par le microbiome engendre une augmentation de la biodisponibilité de la digoxine. Si la concentration plasmatique du médicament augmente trop, les effets secondaires peuvent aller jusqu'à causer la mort. Dans le présent projet, nous avons vérifié la sensibilité de E. lenta à deux antibiotiques de la famille des céphalosporines de seconde génération, in vivo et in vitro. Pour les 18 volontaires qui ont été exposés à 2x500mg de céfprozil durant une semaine, il y a une tendance à la baisse de l'abondance de la bactérie d'intérêt (par 58,3% par rapport au niveau initial), mais pas de significativité au niveau des tests statistiques. Pour les échantillons complets de microbiome fécal, mis en culture avec et sans antibiotiques, il y a une différence statistiquement significative avec une valeur-p de 0,0457, alors que la croissance de E. lenta a été impactée négativement par l'ajout de céfprozil au milieu de culture. Les résultats valident une prémisse importante pour la démonstration du rôle du microbiome dans la pharmacocinétique de la digoxine et la gestion clinique du médicament cardiotonique. / Digoxin is a widely used cardiotonic drug in the management of heart failure and atrial fibrillation. It has been known since the early 1980's that the main metabolite of digoxin, dihydrodigoxin, is synthesized by the gut microbiome during first pass metabolism and is exclusively produced by the bacteria Eggerthella lenta. In a clinical study done in the U.S.A., there were 14% of high metabolizers, for whom over 40% of the oral digoxin dose is transformed to the inactive metabolite and rapidly eliminated. Digoxin toxicity is the leading cause of hospitalization from medication's secondary effects. The toxicity events are often associated with the addition of an antibiotic (mostly from the macrolides class) to the patient's drugs regiments. The theory explored in this project could help explain the toxicity events in metabolizers. These patients have a higher daily digoxin maintenance dose to counteract the effects of the microbiome and are then prescribed antibiotics for an infection unrelated to their heart condition. The antibiotic alters E. lenta negatively, which cannot metabolize digoxin anymore and therefore augments the bioavailability of the cardiotonic. If the plasmatic concentration reaches dangerous levels (over 2ng/ml of plasma), the patients face adverse effects that include death. In the present project, we evaluated the susceptibility of E. lenta to two second generation cephalosporins, in vivo and in vitro. With the 18 healthy volunteers that were exposed to 2x500mg of cefprozil daily for 7 days, we observed a diminution of the abundance of the bacteria of interest by 58,3% from the initial levels. This change did not however produce statistically significant tests results. For the complete fecal microbiome that were cultivated in vitro, with or without cefprozil, the difference between the two conditions resulted in a statistically significant p-value of 0.0457, confirming the sensitivity of E. lenta to this cephalosporin. These results validate an important premise for the demonstration of the importance of the gut microbiome in the pharmacokinetics of digoxin and the clinical management of the drug to avoid toxicity events in clinical practice.

Microbiome

Eggerthella lenta

Eubacterium lentum

Next-Generation Sequencing (NGS)

Whole Genome Shotgun (WGS)

Bioinformatique

Pharmacologie

Pharmacocinétique

Médecine personnalisée

Cardiologie

Insuffisance Cardiaque

Bioinformatics

Pharmacology

Pharmacokinetics

Personnalised Medecine

Cardiology

Heart Failure

Adaptivní změny rozšíření populací v odpovědi na klimatické změny / Adaptive population shifts in response to climate change

Horníková, Michaela

January 2021

Adaptive population shifts in response to climate change Ing. Michaela Horníková, Doctoral thesis Abstract Understanding of species' reactions to past climate and environmental changes is a hot topic in many fields of biology as it is relevant also for addressing species' future under the contemporary climate change. Using an emerging model species, the bank vole, I combine genomic phylogeographic data with information on known intraspecific functional variability and environmental niche modelling and aim to elucidate the particular role of intraspecific variation and ultimately selection in shaping the species' response to the climatic and environmental changes after the end of the last glaciation. Based on the mtDNA markers, bank voles exhibit a complex phylogeographic pattern suggesting population replacement events during the postglacial recolonization of Europe and thus possible involvement of selection in the process. An extensive dataset of more than 6000 SNPs was used to search for signs of population replacement in the bank vole genomic DNA and to investigate the species' postglacial recolonization history throughout its European distribution range. The genomic data revealed even more complex population history than previously detected with mtDNA markers, including not only admixture but also...