RÉSUMÉ
Folate and vitamin B(12) metabolism are essential for de novo purine synthesis, and several defects in these pathways have been associated with immunodeficiency. Here we describe the occurrence of severe combined immunodeficiency (SCID) with megaloblastic anemia, leukopenia, atypical hemolytic uremic syndrome, and neurologic abnormalities in which hydroxocobalamin and folate therapy provided partial immune reconstitution. Whole exome sequencing identified compound heterozygous mutations in the MTHFD1 gene, which encodes a trifunctional protein essential for processing of single-carbon folate derivatives. We now report the immunologic details of this novel genetic cause of SCID and the response to targeted metabolic supplementation therapies. This finding expands the known metabolic causes of SCID and presents an important diagnostic consideration given the positive impact of therapy.
Sujet(s)
Analyse de mutations d'ADN , Methylenetetrahydrofolate Dehydrogenase (NADP)/génétique , Immunodéficience combinée grave/génétique , 3-Hydroxyacyl-CoA dehydrogenases/déficit , 3-Hydroxyacyl-CoA dehydrogenases/génétique , Anémie mégaloblastique/diagnostic , Anémie mégaloblastique/traitement médicamenteux , Anémie mégaloblastique/génétique , Myélogramme , Cardiomyopathies/diagnostic , Cardiomyopathies/traitement médicamenteux , Cardiomyopathies/génétique , Association thérapeutique , Association médicamenteuse , Association de médicaments , Exome/génétique , Femelle , Dépistage des porteurs génétiques , Humains , Hydroxocobalamine/usage thérapeutique , Immunisation passive , Nourrisson , Nouveau-né , Leucopénie/diagnostic , Leucopénie/traitement médicamenteux , Leucopénie/génétique , Erreurs innées du métabolisme lipidique/diagnostic , Erreurs innées du métabolisme lipidique/traitement médicamenteux , Erreurs innées du métabolisme lipidique/génétique , Antigènes mineurs d'histocompatibilité , Myopathies mitochondriales , Protéine trifonctionnelle mitochondriale/déficit , Maladies du système nerveux , Infections opportunistes/diagnostic , Infections opportunistes/traitement médicamenteux , Infections opportunistes/génétique , Neuropathies périphériques/diagnostic , Neuropathies périphériques/traitement médicamenteux , Neuropathies périphériques/génétique , Pneumonie à Pneumocystis/diagnostic , Pneumonie à Pneumocystis/traitement médicamenteux , Pneumonie à Pneumocystis/génétique , Rétinite pigmentaire/diagnostic , Rétinite pigmentaire/traitement médicamenteux , Rétinite pigmentaire/génétique , Rhabdomyolyse , Analyse de séquence d'ADN , Immunodéficience combinée grave/diagnostic , Immunodéficience combinée grave/traitement médicamenteux , Sulfadoxine/usage thérapeutique , Triméthoprime/usage thérapeutique , Vitamine B12/usage thérapeutiqueRÉSUMÉ
Among previously healthy children with severe influenza, the mechanisms leading to increased pathology are not understood. We hypothesized that children with severe influenza would have high levels of circulating cytokines. To examine this, we recruited patients with severe influenza and examined plasma cytokine levels as well as the ability of peripheral blood cells to respond to stimuli. Ten patients with severe influenza were enrolled during the 2005-2007 influenza seasons. We evaluated plasma cytokine levels, circulating NK cells, and responses to TLR ligands during the illness. We compared these patients with five patients with moderate influenza, six patients with respiratory syncytial virus (RSV), and 24 noninfected controls. Patients with influenza showed depressed responses to TLR ligands when compared with RSV patients and healthy controls (P<0.05). These normalized when retested during a convalescent phase. Plasma levels of IL-6, IL-12, and IFN- were elevated in influenza patients compared with controls (P<0.05). A compromised ability to produce TNF- was reproduced by in vitro infection, and the magnitude of the effect correlated with the multiplicity of infection and induction of IFN regulatory factor 4 expression. Aberrant, systemic, innate responses to TLR ligands during influenza infection may be a consequence of specific viral attributes such as a high inoculum or rapid replication and may underlie the known susceptibility of influenza-infected patients to secondary bacterial infections.
Sujet(s)
Maladies du système immunitaire/immunologie , Maladies du système immunitaire/physiopathologie , Grippe humaine/immunologie , Grippe humaine/physiopathologie , Technique de Western , Enfant d'âge préscolaire , Cytokines/sang , Femelle , Cytométrie en flux , Régulation de l'expression des gènes , Humains , Maladies du système immunitaire/complications , Nourrisson , Grippe humaine/complications , Grippe humaine/génétique , Facteurs de régulation d'interféron/métabolisme , Cellules tueuses naturelles/immunologie , Cellules tueuses naturelles/virologie , Agranulocytes/virologie , Mâle , Récepteur-1 de déclenchement de cytotoxicité naturelle/immunologie , Récepteurs de type Toll/métabolismeRÉSUMÉ
IPEX syndrome is a rare, inherited condition characterized by immune dysfunction, polyendocrinopathy, enteropathy, and X-linked recessive inheritance. Patients typically present in infancy with severe diarrhea and failure to thrive. Most children die by 1 year of age without therapy. The diagnosis is established by genetic analysis, which often takes several weeks to complete and can sometimes delay crucial immunosuppressive treatment. We attempted to develop a screening tool that allows rapid identification of patients with IPEX syndrome using immunocytochemical staining of FOXP3+ cells in bowel biopsies. We found that 2 patients with classic IPEX syndrome due to protein-truncating mutations in FOXP3 had markedly decreased staining of FOXP3+ T cells in the lamina propria and lymphoid aggregates. One patient with a mild, late-onset presentation and a missense mutation in FOXP3 had intact staining of FOXP3+ cells. This screening test provides a valuable tool for diagnosing IPEX syndrome in extremely ill patients who may not tolerate a delay in therapeutic intervention.
Sujet(s)
Facteurs de transcription Forkhead , Maladies génétiques liées au chromosome X/diagnostic , Dépistage génétique , Polyendocrinopathies auto-immunes/diagnostic , Entéropathie exsudative/diagnostic , Études cas-témoins , Enfant , Enfant d'âge préscolaire , Endoscopie , Issue fatale , Études de suivi , Facteurs de transcription Forkhead/génétique , Facteurs de transcription Forkhead/métabolisme , Mutation avec décalage du cadre de lecture , Maladies génétiques liées au chromosome X/génétique , Maladies génétiques liées au chromosome X/immunologie , Maladies génétiques liées au chromosome X/anatomopathologie , Maladies génétiques liées au chromosome X/chirurgie , Maladies génétiques liées au chromosome X/thérapie , Humains , Immunohistochimie , Immunosuppresseurs/usage thérapeutique , Muqueuse intestinale/métabolisme , Muqueuse intestinale/anatomopathologie , Gros intestin/chirurgie , Mâle , Muqueuse/métabolisme , Muqueuse/anatomopathologie , Mutation faux-sens , Polyendocrinopathies auto-immunes/génétique , Polyendocrinopathies auto-immunes/immunologie , Polyendocrinopathies auto-immunes/anatomopathologie , Polyendocrinopathies auto-immunes/chirurgie , Polyendocrinopathies auto-immunes/thérapie , Entéropathie exsudative/génétique , Entéropathie exsudative/immunologie , Entéropathie exsudative/anatomopathologie , Entéropathie exsudative/chirurgie , Entéropathie exsudative/thérapie , Études rétrospectives , Sirolimus/usage thérapeutique , Syndrome , Lymphocytes T/métabolisme , Facteurs temps , Résultat thérapeutiqueRÉSUMÉ
Chronic granulomatous disease is a neutrophil disorder in which phagocytic cells fail to produce a respiratory burst. Five genetic types of chronic granulomatous disease have been described and in each case the clinical manifestations relate to the inability to effectively kill catalase-positive organisms. It is classically described as a pure disorder of intracellular killing, with preservation of other aspects of phagocytic function such as migration and phagocytosis and normal function of nonmyeloid cells. This article describes a heretofore unrecognized feature of chronic granulomatous disease. Fifty-three patients with chronic granulomatous disease and 42 age-matched controls were studied by flow cytometry. Total T cell numbers and CD4 and CD8 T cell numbers were compared between patients and controls. Patients with chronic granulomatous disease had diminished T cell numbers compared to controls after 3 years of age. The difference increased with age. It is not known whether diminished T cell numbers influence the susceptibility to infections in these patients, but T cell effects could represent a significant cofactor for infection.
