Genetic Studies of Immunological Diseases in Dogs and Humans

Bianchi, Matteo

January 2017

This thesis presents genetic studies aiming at enlarging our knowledge regarding the genetic factors underlying two immune-mediated diseases, hypothyroidism and autoimmune Addison’s disease (AAD), in dogs and humans, respectively. Genetic and environmental factors are indicated to contribute to canine hypothyroidism, which can be considered a model for human Hashimoto’s thyroiditis (HT). In Paper I we performed the first genome-wide association (GWA) study of this disease in three high-risk dog breeds (Gordon Setter, Hovawart and Rhodesian Ridgeback). Using an integrated GWA and meta-analysis strategy, we identified a novel hypothyroidism risk haplotype located on chromosome 12 being shared by the three breeds. The identified haplotype, harboring three genes previously not associated with hypothyroidism, is independent of the dog leukocyte antigen region and significantly enriched across the affected dogs. In Paper II we performed a GWA study in another high-risk breed (Giant Schnauzer) and detected an associated locus located on chromosome 11 and conferring protection to hypothyroidism. After whole genome resequencing of a subset of samples with key haplotypes, we fine mapped the region of association that was subsequently screened for the presence of structural variants. We detected a putative copy number variant overlapping with the upstream region of the IFNA7 gene, which is located in a region of high genomic complexity. Remarkably, perturbed activities of type I Interferons have been extensively associated with HT and general autoimmunity. In Paper III we performed the first large-scale genetic study of human AAD, a rare autoimmune disorder characterized by dysfunction and ultimately destruction of the adrenal cortex. We resequenced 1853 immune-related genes comprising of their coding sequences, untranslated regions, as well as conserved intronic and intergenic regions in extensively characterized AAD patients and control samples, all collected in Sweden. We identified BACH2 gene as a novel risk locus associated with AAD, and we showed its independent association with isolated AAD. In addition, we confirmed the previously established AAD association with the human leukocyte antigen complex. The results of these studies will hopefully help increasing the understanding of such diseases in dogs and humans, eventually promoting their well-being.

complex disease

immunogenetics

autoimmunity

GWAS

NGS

canine model

dog

hypothyroidism

Addison's disease

IFNA

BACH2

Medical Genetics

Medicinsk genetik

Dissecting mechanisms underlying increased TLR7-mediated IFNα production in pDCs in physiological and pathophysiological settings : between sex differences and HIV-1-HCV co-infection / Identification des mécanismes associés à une production élevée d'IFNa par les pDCs en réponse à TLR7 dans des contextes phyiologique et pathophysiologique : entre différences liées au sexe et co-infection par le VIH-1 et le VHC

Griesbeck, Morgane

02 June 2015

Les interférons de type I (IFN-I) peuvent être produits par toutes les cellules mais les rares cellules dendritiques plasmacytoïdes en sont les principales cellules productrices. L’IFNa orchestre de nombreux mécanismes pathogéniques dans l’infection par le virus de l’immunodéficience humaine de type 1 (VIH-1). L’étude de modèles physiologiques et pathophysiologiques peut fournir des informations cruciales sur les moyens d’exploiter la signalisation de l’IFNa dans un but thérapeutique. Les pDCs de femmes produisent plus d’IFNa en réponse à la stimulation du récepteur Toll-like 7 (TLR7) que les pDCs d’hommes. Les mécanismes impliqués dans cette différence n’ont été que partiellement identifiés. Nous démontrons ici un mécanisme par lequel la plus forte expression d’IRF5 dans les pDCs chez les sujets sains féminins, sous le contrôle d’ERa, participe à leur production plus élevée d’IFNa en réponse à TLR7. La co-infection par le virus de l’hépatite C (VHC) est aujourd’hui l’une des principales causes de mortalité parmi les individus infectés par le VIH-1. Nous avons émis l’hypothèse que l’activation immunitaire chronique plus élevée rapportée chez des individus co-infectés par le VIH-1 et VHC pourrait être due à un dysfonctionnement de la voie de TLR7/IFN-I dans les pDCs. Nos données montrent que le VHC entraîne, chez des individus infectés par le VIH-1, des altérations associées aux pDCs et à l’IFNa, qui sont associées ˆ la sévérité de la maladie hépatique. Nos résultats suggèrent que les patients co-infectés par le VIH-1 et le VHC, même à fibrose minime, pourraient bénéficier d’un traitement plus précoce. / Type I interferons (IFN) can be produce by any cell type but plasmacytoid dendritic cells (pDC) are the main producers. IFNa orchestrates multiple pathogenic mechanisms in human immunodeficiency virus 1 (HIV-1). Studying physiological and pathophysiological model scan provide critical informations on how to harness IFNa signaling for therapeutic purposes. pDCs from females produce more IFNa upon Toll-like receptor (TLR) 7 stimulation than pDCs from males. The mechanisms underlying such difference have only been partially identified. We demonstrate here a mechanism by which increased IRF5 expression in females, under the control of the esrogen receptor a, contribute to increased IFN? production upon TLR7 stimulation. HCV co-infection is one of the major cause of mortality among HIV-1 infected individuals. We hypothesized that increased chronic immune activation observed in HCV-HIV-1 co-infected individuals may be related to altered TLR7/IFNa signaling in pDCs. Our data show that HCV triggers alterations in pDCs and IFNa signaling in HIV-1 co-infected individuals, which are associated to hepatic disease severity. Our results suggest that HCV-HIV-1 co-infected individuals, even with minimal fibrosis, may benefit from ealier treatment initiation.

Pdc

IFNa

Tlr7

Différence liée au sexe

Co-infection par le VIH-1 et le VHC

IRF5

HIV-1 and HCV co-infection

Toll-like receptor 7

571.96

The Contribution of IFNα-Stimulated Immune Cell Populations to B6.NbA2 Lupus-likeDisease

Keller, Emma Jean

01 September 2021

No description available.

Animal Diseases

Health Sciences

Immunology

Molecular Biology

SLE

Lupus

IFNa

Interferon alpha

Type I IFN, Interferon

auto-antibodies

IFN, IFN-I

B6Nba2

murine lupus

autoimmunity

autoimmune

B Cells

T Cells

Myeloid Cells

murine autoimmunity