MicroRNA-21 is an important downstream component of BMP signalling in epidermal keratinocytes

Ahmed, Mohammed I., Mardaryev, Andrei N., Lewis, Christopher J., Sharov, A.A., Botchkareva, Natalia V.

17 June 2011

Yes / Bone morphogenetic proteins (BMPs) play essential roles in the control of skin development, postnatal tissue remodelling and tumorigenesis. To explore whether some of the effects of BMP signalling are mediated by microRNAs, we performed genome-wide microRNA (miRNA) screening in primary mouse keratinocytes after BMP4 treatment. Microarray analysis revealed substantial BMP4-dependent changes in the expression of distinct miRNAs, including miR-21. Real-time PCR confirmed that BMP4 dramatically inhibits miR-21 expression in the keratinocytes. Consistently, significantly increased levels of miR-21 were observed in transgenic mice overexpressing the BMP antagonist noggin under control of the K14 promoter (K14-noggin). By in situ hybridization, miR-21 expression was observed in the epidermis and hair follicle epithelium in normal mouse skin. In K14-noggin skin, miR-21 was prominently expressed in the epidermis, as well as in the peripheral portion of trichofolliculoma-like hair follicle-derived tumours that contain proliferating and poorly differentiated cells. By transfecting keratinocytes with a miR-21 mimic, we identified the existence of two groups of the BMP target genes, which are differentially regulated by miR-21. These included selected BMP-dependent tumour-suppressor genes (Pten, Pdcd4, Timp3 and Tpm1) negatively regulated by miR-21, as well as miR-21-independent Id1, Id2, Id3 and Msx2 that predominantly mediate the effects of BMPs on cell differentiation. In primary keratinocytes and HaCaT cells, miR-21 prevented the inhibitory effects of BMP4 on cell proliferation and migration. Thus, our study establishes a novel mechanism for the regulation of BMP-induced effects in the skin and suggests miRNAs are important modulators of the effects of growth factor signalling pathways on skin development and tumorigenesis.

Animals

Bone morphogenetic protein 4

Carrier proteins

Cell transformation

Cells

Epidermis

Gene expression regulation

Neoplastic

Genes

Tumor suppressor

Genome-wide association study

Keratin-14

Keratinocytes

Mice

Inbred strains

Transgenic

MicroRNAs

Microarray analysis

Morphogenesis

Signal transduction

REF 2014

Identification of Genomic Variants Associated with Adolescent Idiopathic Scoliosis (AIS) in French-Canadian Population

Tang, Qi Lin

12 1900

La scoliose idiopathique est une déformation tridimensionnelle de la colonne vertébrale dont la pathogenèse reste obscure. Cette maladie affecte 2-4% des adolescents de 10-18 ans parmi les garçons et les filles. Il est à noter que les filles sont plus sévèrement affectées et ce en plus grand nombre que les garçons. Les études de jumeaux ont montré que les facteurs génétiques jouent un rôle important dans la scoliose idiopathique de l'adolescent (SIA). Depuis 2010, les études d'association pan génomiques ont été multipliées dans les recherches, visant à trouver des gènes candidats impliqués dans la SIA à travers des examens des polymorphismes nucléotidiques (SNPs). Un test génétique nommé "ScoliScore" a été publié pour essayer de prédire la progression de courbure dans la population caucasienne. Cependant, l'association n'a pas été reproduite dans une grande étude japonaise, soulignant l'importance d'une étude de réplication dans une population caucasienne indépendante. Dans ce contexte, mon projet de maîtrise a permis de génotyper plus de 1,4 millions de SNPs dans une cohorte canadienne-française dans le but: 1) de valider l'association de ScoliScoreTM; et 2) d’identifier les variants génomiques associées à la SIA dans la population québécoise. Notre étude a montré qu’aucun des variants constituant le test ScoliScoreTM n’était associé à la SIA. Ceci suggère que l'absence d'association dans une cohorte japonaise n'est pas due à l'appartenance ethnique. Aussi, nous avons identifié des variants génomiques associés significativement à l’initiation et/ou la progression de SIA dans la population québécoise, suggérant des gènes candidats impliqués dans la pathogenèse de SIA. / Idiopathic scoliosis is a common spinal deformation occurring without clear reason. This disease affects 2-4% adolescents aging from 10-18 years old in both genders. Of note, girls are more affected in number and severity than boys. Twin studies demonstrated that genetic factors play an important role in adolescent idiopathic scoliosis (AIS). Since 2010, Genome-wide association studies (GWAS) have been multiplied in AIS researches, aiming to find out candidate genes involved in the disease by an examination of single nucleotide polymorphisms (SNPs) throughout the entire genome. A genetic test named “ScoliScore” was released for the prediction of curvature progression in Caucasian AIS population using 53 SNPs. However, such association was not replicated in a larger Japanese-population study. Such a discrepancy could be explained by ethnicity, raising the importance of a replication study in an independent Caucasian population of European descent. In that context, we genotyped over 1.4 million SNPs in a French-Canadian cohort: 1) to validate the association in ScoliScoreTM test; and 2) to identify genomic variants associated with AIS in the population of Quebec. As a result, the association of ScoliScoreTM genomic markers could not be reproduced in French-Canadian AIS patients, suggesting that the lack of association of these SNPs in a Japanese cohort is not due to ethnicity. Meanwhile, we identified genome-wide significant variants associated with spinal curve initiation and/or progression in French-Canadian population, suggesting candidate genes involved in AIS pathogenesis.

Scoliose idiopathique de l'adolescent

Polymorphisme d'un seul nucléotide

Variant génomique

Étude d'association pan génomique

ScoliScoreTM

Analyse de l'association

Adolescent idiopathic scoliosis

Single nucleotide polymorphism

Genomic variant

Genome-wide association study

Spinal curve progression

Caucasian

French-Canadian

Association analysis

Genotype

Epidémiologie et génétique humaine de l’ulcère de Buruli / Epidemiology and human genetics of Buruli ulcer

Vincent, Quentin

28 November 2014

L'ulcère de Buruli (UB), infection à Mycobacterium ulcerans, troisième mycobactériose mondiale, connait une émergence rapide depuis 1980, essentiellement dans les pays d'Afrique subsaharienne. Jusqu’ici, les connaissances épidémiologiques sur l’UB étaient fondées sur des séries de cas cliniques non confirmés par laboratoire. Nous avons constitué la plus grande cohorte de cas confirmés à ce jour rassemblant plus de 1200 patients traités au CDTUB de Pobè au Bénin entre 2005 et 2011, afin de décrire l'épidémiologie clinique de la maladie et d'explorer l’architecture génétique de la susceptibilité à cette maladie. Les patients atteints d’UB sont des enfants (âge médian au diagnostic de 12 ans), présentant une lésion unique (96%), large (plus de 15 cm, 36%), ulcérative (66%) du membre inférieur (60%). Nous rapportons une présentation clinique atypique de l’UB, dans laquelle les patients présentent exclusivement une ostéomyélite à M. ulcerans. Le sex-ratio varie avec l’âge : les garçons sont majoritaires parmi les enfants (57% de patients masculins chez les moins de 15 ans), et les femmes parmi les adultes (33% de patients masculins). La présentation clinique dépend de l’âge et du sexe. 9% des patients masculins ont présenté une ostéomyélite contre 4% des patients féminins. Un an après la fin du traitement, 22% des patients présentent des séquelles fonctionnelles fixées. Une présentation clinique comportant une lésion oedémateuse, osseuse, de grande taille ou plusieurs lésions est significativement associée avec le développement de séquelles fonctionnelles (OR 7.64, IC95% [5.29-11.31]). Les patients coinfectés par le VIH ont un risque significativement plus élevé de développer un UB sévère (OR 2.77, IC95% [1.32-6.33]). Nous avons exploré l’architecture génétique de la susceptibilité à l’UB dans une perspective mendélienne et une perspective complexe. Le cas le plus sévère de la maladie observé dans ce centre appartient à une famille consanguine dans laquelle la ségrégation du phénotype suggère un défaut génétique mendélien récessif. Une analyse de liaison génétique par cartographie d'homozygotie suggère l’implication du locus des béta-défensines sur le chromosome 8 dans la pathogénèse de l'UB, et mène à l’identification d’une délétion homozygote ségrégeant parfaitement avec la maladie. Dans une perspective complexe, une étude d’association pangénomique a été réalisée après génotypage d’une cohorte de 400 cas et 400 témoins exposés sur plus de 2 millions de SNPs par la puce Illumina Omni2.5 et a permis l’identification de nombreux signaux d’intérêt. L’étude de réplication est en cours. La compréhension de la physiopathologie de l'infection à M. ulcerans est cruciale pour générer de nouvelles pistes thérapeutiques et vaccinales. La dissection du contrôle génétique de l'infection par l'hôte est en ce sens indispensable. / Buruli ulcer (BU), caused by Mycobacterium ulcerans, is the third most frequent mycobacteriosis worldwide. It has been rapidly emerging in sub-Saharan African countries since 1980. Until now, knowledge of BU epidemiology relied on series of non laboratory-confirmed clinical cases. From 2005-2011, we recruited the current largest cohort of laboratory-confirmed cases (more than 1,200 patients) at the Pobe CDTUB, Benin, to describe the clinical epidemiology of the disease and to explore the genetic architecture of human susceptibility to BU. Typically, patients with BU were children (median age at diagnosis 12 years) presenting with a unique (96%) large (≥15 cm, 36%) ulcerative (66%) lesion of the lower limb (60%). Atypical clinical presentation of BU included osteomyelitis with no identifiable present or past BU skin lesions. The sex ratio of BU widely varied with age, with male patients accounting for 57% of patients aged 15 years and younger, but only 33% of those older than 15 years. Clinical presentation of BU was significantly dependent on age and sex. 9% male patients had BU osteomyelitis, whereas only 4% of female patients did. 1 year after treatment, 22% of patients with follow-up information presented with permanent functional sequelae. Presentation with oedema, osteomyelitis, or large (≥15 cm in diameter), or multifocal lesions was significantly associated with occurrence of permanent functional sequelae (OR 7•64, 95% CI 5•29–11•31) and operationally defines severe BU. When coinfected with HIV, patients had a significantly higher risk to develop severe BU (OR 2.77, IC95% [1.32-6.33]). We explored the genetic architecture of susceptibility to BU in both mendelian and complex genetic frameworks. The most severe case of the disease to have been treated at the Pobe CDTUB belonged to a consanguineous family in which the segregation of the phenotype was indicative of a recessive mendelian genetic defect. Genetic linkage analysis by homozygosity mapping suggested the implication of the beta-defensin locus on chromosome 8 in BU pathogenesis and lead to the identification of a homozygous deletion, which co-segregated perfectly with the disease in the family. In a complex genetics approach, we undertook a genome-wide association study, which involved the genotyping of more than 2 million SNPs (Illumina Omni2.5) in a cohort of 400 cases and 400 exposed controls. We identified many signals of interest. The replication study is ongoing. Understanding BU physiopathology is crucial to the development of efficient vaccines and drugs. Dissection of the genetic control of the infection by M. ulcerans by its human host therefore constitutes an indispensable step.

Maladie infectieuse

Epidémiologie

Mycobactérie

Mycobacterium ulcerans

Ulcère de Buruli

Bénin

Analyse de liaison

Défensine

Analyse d’association pangénomique

GWAS

Infectious disease

Epidemiology

Complex and Mendelian Human Genetic

Mycobacteriosis

Mycobacterium ulcerans

Buruli ulcer

Benin

Linkage analysis

Defensin

Genome-Wide Association Study

616.042

Genetic background and antenatal risk factors of bronchopulmonary dysplasia

Mahlman, M. (Mari)

08 June 2018

Abstract Advances over the past few decades in ante- and neonatal care have led to the survival of a growing number of premature infants of extremely low gestational age. However, the occurrence of serious diseases, particularly those affecting the most immature infants, remains high. Bronchopulmonary dysplasia (BPD), a chronic lung disease of premature infants, is one such disease. Our current understanding of the molecular pathogenesis of BPD is incomplete; consequently, there are few preventive and therapeutic options for BPD. Moreover, it is challenging to predict the risk of BPD. Previous studies of BPD in twins revealed that the heritability of BPD is quite high. However, the individual genes that predispose premature infants to BPD are largely unknown. The aim of this study was to identify and study genes associated with BPD in order to investigate its pathogenesis. An additional aim was to add to knowledge of the risk of BPD in newborn premature infants, with an emphasis on twins. A candidate gene study found no consistent association between common polymorphisms of vascular endothelial growth factor receptor 2 and BPD. A second candidate gene study noted an association between the gene encoding Kit ligand and BPD. A genome-wide association study found a suggestive association between a locus close to the gene encoding C-reactive protein (CRP) and BPD, and in subsequent analyses, plasma levels of CRP during the first week of life predicted BPD. Finally, a nationwide register study found that the risk of BPD was lower in twins than in singletons. The results of this study add to what is known of the genetics and pathogenesis of BPD. They also provide new data on the risk of BPD, which may be used to improve early identification of infants for whom the risk of developing BPD is high. / Tiivistelmä Ennenaikaisen syntymän ja keskoslasten hoidon kehittymisen myötä yhä useammat huomattavan epäkypsinä syntyneet lapset jäävät henkiin. Samalla erityisesti juuri näitä lapsia uhkaavien sairauksien esiintyvyys on pysynyt korkeana. Bronkopulmonaalinen dysplasia (BPD, keskosen krooninen keuhkosairaus) on yksi näistä sairauksista. BPD:n molekyylitasoinen tautimekanismi on vielä osin tuntematon, eikä BPD:tä tehokkaasti estävää tai siitä parantavaa hoitoa ole. Myös BPD riskin arvioiminen vastasyntyneen keskoslapsen kohdalla on vaikeaa. BPD on huomattavan perinnöllinen tauti. BPD:lle altistavista geeneistä on kuitenkin vasta vähän tietoa. Tämän tutkimuksen tavoitteena oli lisätä tietoa BPD:n tautimekanismista tutkimalla BPD:lle altistavia geenejä. Lisäksi tutkimuksessa tarkasteltiin BPD:n esiintyvyyttä ja syntymää edeltäviä riskitekijöitä erityisesti kaksosten osalta. Ehdokasgeenitutkimuksessa verisuonten endoteelikasvutekijää koodaava geeni ei assosioitunut toistuvasti BPD:hen. Kit ligandia koodaava geeni sen sijaan assosioitui. Koko genomin assosiaatiotutkimuksessa C-reaktiivista proteiinia (CRP) koodaavan geenin lähistöltä löydettiin BPD:hen mahdollisesti assosioituva alue. Lisäksi ensimmäisen viikon CRP-arvojen osoitettiin ennakoivan myöhemmin kehittyvää BPD:tä. BPD-riskin todettiin olevan matalampi kaksi- kuin yksisikiöisistä raskauksista syntyneillä lapsilla. Tutkimuksen tulokset lisäävät tietoa BPD:n perinnöllisyydestä ja sitä kautta BPD:n tautimekanismista. Tutkimus toi myös uutta tietoa BPD:n riskitekijöistä parantaen vastasyntyneen keskoslapsen BPD-riskin arviota.

C-reactive protein

Kit ligand

bronchopulmonary dysplasia

candidate gene study

genetic association study

genetic polymorphism

genome-wide association study

premature birth

premature infant

pulmonary inflammation

twins

vascular endothelial growth factor

C-reaktiivinen proteiini

Kit ligandi

bronkopulmonaalinen dysplasia

ehdokasgeenitutkimus

ennenaikainen syntymä

geenipolymorfismi

geneettinen assosiaatiotutkimus

kaksoset

keskosen krooninen keuhkosairaus

keskosuus

keuhkojen tulehdusreaktio

koko genomin assosiaatiotutkimus

verisuonten endoteelikasvutekijä

The International Consortium on Lithium Genetics (ConLiGen): An Initiative by the NIMH and IGSLI to Study the Genetic Basis of Response to Lithium Treatment

Schulze, Thomas G., Alda, Martin, Adli, Mazda, Akula, Nirmala, Ardau, Raffaella, Bui, Elise T., Chillotti, Caterina, Cichon, Sven, Czerski, Piotr, Del Zompo, Maria, Detera-Wadleigh, Sevilla D., Grof, Paul, Gruber, Oliver, Hashimoto, Ryota, Hauser, Joanna, Hoban, Rebecca, Iwata, Nakao, Kassem, Layla, Kato, Tadafumi, Kittel-Schneider, Sarah, Kliwicki, Sebastian, Kelsoe, John R., Kusumi, Ichiro, Laje, Gonzalo, Leckband, Susan G., Manchia, Mirko, MacQueen, Glenda, Masui, Takuya, Ozaki, Norio, Perlis, Roy H., Pfennig, Andrea, Piccardi, Paola, Richardson, Sara, Rouleau, Guy, Reif, Andreas, Rybakowski, Janusz K., Sasse, Johanna, Schumacher, Johannes, Severino, Giovanni, Smoller, Jordan W., Squassina, Alessio, Turecki, Gustavo, Young, L. Trevor, Yoshikawa, Takeo, Bauer, Michael, McMahon, Francis J.

January 2010

For more than half a decade, lithium has been successfully used to treat bipolar disorder. Worldwide, it is considered the first-line mood stabilizer. Apart from its proven antimanic and prophylactic effects, considerable evidence also suggests an antisuicidal effect in affective disorders. Lithium is also effectively used to augment antidepressant drugs in the treatment of refractory major depressive episodes and prevent relapses in recurrent unipolar depression. In contrast to many psychiatric drugs, lithium has outlasted various pharmacotherapeutic ‘fashions’, and remains an indispensable element in contemporary psychopharmacology. Nevertheless, data from pharmacogenetic studies of lithium are comparatively sparse, and these studies are generally characterized by small sample sizes and varying definitions of response. Here, we present an international effort to elucidate the genetic underpinnings of lithium response in bipolar disorder. Following an initiative by the International Group for the Study of Lithium-Treated Patients (www.IGSLI.org) and the Unit on the Genetic Basis of Mood and Anxiety Disorders at the National Institute of Mental Health,lithium researchers from around the world have formed the Consortium on Lithium Genetics (www.ConLiGen.org) to establish the largest sample to date for genome-wide studies of lithium response in bipolar disorder, currently comprising more than 1,200 patients characterized for response to lithium treatment. A stringent phenotype definition of response is one of the hallmarks of this collaboration. ConLiGen invites all lithium researchers to join its efforts. / Dieser Beitrag ist mit Zustimmung des Rechteinhabers aufgrund einer (DFG-geförderten) Allianz- bzw. Nationallizenz frei zugänglich.

info:eu-repo/classification/ddc/610

ddc:610

info:eu-repo/classification/ddc/150

ddc:150

Identification des déterminants génétiques de la tolérance à la sècheresse chez le maïs par l'étude de l'évolution de l'indice foliaire vert au cours du cycle de la plante et le développement d'une méthode de phénotypage innovant / Identification of the genetic determinants of maize drought tolerance by studying the evolution of Green Leaf Area Index over the plant cycle and the development of an innovative method of phenotyping

Blancon, Justin

28 June 2019

D’ici la fin du siècle, les prévisions climatiques prévoient une diminution de la quantité et de la régularité des pluies s’accompagnant d’une augmentation du risque de sècheresse en Europe et dans de nombreuses régions du monde. La création de nouvelles variétés de maïs plus tolérantes au stress hydrique est un levier indispensable pour faire face à ces contraintes futures. L’objectif principal de cette thèse est d’approfondir les connaissances des déterminismes génétiques de la tolérance à la sècheresse chez le maïs. Pour ce faire, il est proposé de disséquer ce caractère complexe en caractères physiologiques sous-jacents dont le déterminisme génétique est a priori plus simple. L’évolution de l’indice foliaire vert (GLAI : Green Leaf Area Index) au cours du cycle de la plante, par son rôle majeur dans l’interception lumineuse, la transpiration et les échanges de CO2, est un caractère secondaire prometteur pour identifier les bases génétiques de la tolérance à la sècheresse et en améliorer la compréhension. Au cours de cette thèse, nous avons développé une méthode de phénotypage haut débit permettant d’estimer la cinétique du GLAI au champ. Cette méthode combine la caractérisation multispectrale par drone et l’utilisation d’un modèle physiologique simple de GLAI. Elle permet d’estimer la cinétique du GLAI de manière continue sur l’ensemble du cycle de la plante avec une bonne précision, tout en divisant par vingt le temps nécessaire au phénotypage. Nous avons utilisé cette méthode lors de deux essais en conditions optimales et deux essais en conditions de stress hydrique pour mesurer l’évolution du GLAI au sein d’un panel de 324 lignées issues d’une population MAGIC (Multi-parent Advanced Generation Inter-Cross). Les cinétiques estimées présentent une forte héritabilité et expliquent une part significative du rendement en conditions optimales et stressées. Afin d’identifier les bases génétiques de la cinétique du GLAI, trois approches de génétique d’association longitudinales ont été comparées : une approche univariée en deux étapes, une approche multivariée en deux étapes et une approche de régression aléatoire en une étape. Ces trois approches, couplées à la forte densité des données de génotypage disponibles (près de 8 millions de marqueurs), ont permis de révéler de nombreux QTL (Quantitative Trait Loci), dont certains colocalisent avec des QTL de rendement. Enfin, nous avons démontré que les QTL de GLAI identifiés lors de cette étude pouvaient expliquer près de 20 % de la variabilité du rendement observée dans un large réseau d’expérimentations sous stress hydrique. Ce travail fournit des méthodes qui permettront une meilleure caractérisation et une meilleure compréhension des déterminismes génétiques de la cinétique du GLAI, un caractère jusqu’ici inaccessible pour les populations de taille importante. Ce caractère présente toutes les caractéristiques requises pour améliorer l’efficacité des programmes de sélection en conditions de stress hydrique. / By the end of the century, climate forecasts predict a decrease in the quantity and regularity of rainfall with an increasing risk of drought in Europe and in many regions of the world. Breeding for more tolerant varieties will be an essential lever to face these future constraints. The main objective of this work is to characterize the genetic determinisms of drought tolerance in maize. To this aim, it is proposed to dissect this complex trait into underlying physiological traits whose genetic determinism is supposed to be simpler. Green Leaf Area Index (GLAI) dynamics throughout the plant cycle, through its major role in light interception, transpiration and CO2 exchange, is a promising secondary trait to identify and better understand the genetic basis of drought tolerance. During this thesis, we developed a high-throughput method for phenotyping maize GLAI dynamics in the field. This method combines UAV multispectral imagery and a simple GLAI model. It makes possible the estimation of the dynamics of GLAI continuously throughout the whole plant cycle with good accuracy, while reducing the phenotyping time twentyfold. This method was used in two well-watered and two water-deficient trials to characterize the GLAI dynamics of 324 lines from a MAGIC population (Multi-parent Advanced Generation Inter-Cross). The estimated dynamics have a high heritability and explain a significant part of grain yield under well-watered and water-stressed conditions. To characterize the genetic basis of GLAI dynamics, three longitudinal GWAS (Genome Wide Association Study) approaches were compared: a univariate two-step approach, a multivariate two-step approach and a random regression one-step approach. These three approaches, combined with the high density of available genotyping data (nearly 8 million markers), have revealed many QTL (Quantitative Trait Loci), some of which were co-localized with yield QTL. Finally, we demonstrated that the GLAI QTL identified in this study could explain nearly 20 % of the grain yield variability observed in a large network of water-stressed experiments. This work provides methods that will enable a better characterization and understanding of the genetic determinisms of GLAI dynamics, a trait that was out of reach in large populations until now. This trait presents all the characteristics required to improve the effectiveness of selection programs under water stress conditions.

Maïs (Zea mays subsp. mays)

Tolérance à la sècheresse

Indice foliaire vert

Cinétique

Phénotypage haut débit au champ

Drone

Génétique d’association

Maize (Zea mays subsp. mays)

Drought tolerance

Green Leaf Area Index

Dynamics

High-throughput field phenotyping

Unmanned Aerial Vehicle

Genome Wide Association Study

Pathways to dementia: genetic predictors of cognitive and brain imaging endophenotypes in Alzheimer's disease

Ramanan, Vijay K

03 January 2014

Indiana University-Purdue University Indianapolis (IUPUI) / Alzheimer's disease (AD) is a national priority, with nearly six million Americans affected at an annual cost of $200 billion and no available cure. A better understanding of the mechanisms underlying AD is crucial to combat its high and rising incidence and burdens. Most cases of AD are thought to have a complex etiology with numerous genetic and environmental factors influencing susceptibility. Recent genome-wide association studies (GWAS) have confirmed roles for several hypothesized genes and have discovered novel loci associated with disease risk. However, most GWAS-implicated genetic variants have displayed modest individual effects on disease risk and together leave substantial heritability and pathophysiology unexplained. As a result, new paradigms focusing on biological pathways have emerged, drawing on the hypothesis that complex diseases may be influenced by collective effects of multiple variants – of a variety of effect sizes, directions, and frequencies – within key biological pathways. A variety of tools have been developed for pathway-based statistical analysis of GWAS data, but consensus approaches have not been systematically determined. We critically review strategies for genetic pathway analysis, synthesizing extant concepts and methodologies to guide application and future development. We then apply pathway-based approaches to complement GWAS of key AD-related endophenotypes, focusing on two early, hallmark features of disease, episodic memory impairment and brain deposition of amyloid-β. Using GWAS and pathway analysis, we confirmed the association of APOE (apolipoprotein E) and discovered additional genetic modulators of memory functioning and amyloid-β deposition in AD, including pathways related to long-term potentiation, cell adhesion, inflammation, and NOTCH signaling. We also identified genetic associations to amyloid-β deposition that have classically been understood to mediate learning and memory, including the BCHE gene and signaling through the epidermal growth factor receptor. These findings validate the use of pathway analysis in complex diseases and illuminate novel genetic mechanisms of AD, including several pathways at the intersection of disease-related pathology and cognitive decline which represent targets for future studies. The complexity of the AD genetic architecture also suggests that biomarker and treatment strategies may require simultaneous targeting of multiple pathways to effectively combat disease onset and progression.

Alzheimer's disease (AD)

Genome-wide association study (GWAS)

Biological pathway analysis

Episodic memory

Amyloid plaque

Senile dementia

Brain -- Pathophysiology -- Research

Cognition -- Pathophysiology -- Research

Memory -- Pathophysiology -- Research

Cell adhesion -- Molecular aspects

Notch genes

Epidermal growth factor -- Research

Inflammation -- Molecular aspects

Phenotype -- Research

Molecular genetics -- Research

GENETIC ARCHITECTURE OF WELFARE INDICATORS AND IMPLEMENTATION OF SINGLE-STEP GENOMIC PREDICTIONS IN BEEF CATTLE POPULATIONS

Amanda Botelho Alvarenga (14221799)

07 December 2022

<p>Breeding for improved animal welfare is paramount for increasing the long-term sustainability of the animal food industry. In this context, the main objectives of this dissertation were to understand the genetic and genomic background of welfare indicators in livestock and evaluate the feasibility of single-step Genomic Best Linear Unbiased Prediction (ssGBLUP) for performing genomic selection in beef cattle. This dissertation includes five studies. First, we aimed to test and identify an optimal ssGBLUP scenario for crossbreeding schemes. We simulated multiple populations differing based on the genetic background of the trait, and then we tested alternative models, such as multiple-trait weighted ssGBLUP. Even though more elaborated scenarios were evaluated, a single-trait ssGBLUP approach was recommended when genetic correlation across populations were higher than 0.70. The goal of the second study was to identify genomic regions controlling behavior traits that are conserved across livestock species. We systematically reviewed genomic regions associated with behavioral indicators in beef and dairy cattle, pigs, and sheep. The genomic regions identified in this study were located in genes previously reported controlling human behavioral, neural, and mental disorders. In the third study we used a large dataset (675,678 records) from North American Angus cattle to investigate the genetic background of temperament, a behavioral indicator, recorded on one-year-old calves, and provide the models and protocols for implementing genomic selection. We reported a heritability estimate equal to 0.38 for yearling temperament, and it was, in general, genetically favorably correlated with other productivity and fertility traits. Candidate genomic regions controlling yearling temperament were also identified. The fourth study was based on temperament recorded on North American Angus cows from 2 to 15 years of age (797,187 records). The goal was to understand the genetic and genomic background of temperament across the animal’s lifetime. By fitting a random regression model, we observed that temperament is highly genetically correlated across time. However, animals have differential learning and behavioral plasticity (LBP; changes of the phenotype overtime), although the LBP heritability is low. In our last study we evaluated foot scores (foot angle, FA; and claw set, CS) in American (US) and Australian (AU) Angus cattle aiming to assess the genetic and genomic background of foot scores and investigate the feasibility of performing an across-country genomic evaluation (~1.15 million animals genotyped). Foot scores are heritable (heritability from 0.22 to 0.27), and genotype-by-environment interaction was observed between US and AU Angus populations (genetic correlation equal to 0.61 for FA and 0.76 for CS). An across-country genomic prediction outperformed within-country evaluations in terms of predictivity ability (bias, dispersion, and validation accuracy) and theoretical accuracies. We have also identified genes associated with FA and CS previously reported in human’s bone structure and repair mechanism. In conclusion, this dissertation presents a comprehensive genetic and genomic characterization of welfare indicators (temperament and foot scores) in (inter)national livestock populations. </p>

Sustainable agricultural development

Animal Welfare

Animal Behavior

Quantitative Genetics

Genomic Prediction

Genome-wide Association Study

Foot Score

Beef Cattle

Angus Cattle

Data Simulation

Statistical Modeling

Random Regression

Genotype-by-Environment Interaction

Across-country Genetic Evaluation

Genetic Diversity

Longitudinal Analysis

Variance Components

Cross-validation