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Heterozygous TBK1 mutations impair TLR3 immunity and underlie herpes simplex encephalitis of childhood (2012)

Herman, M., Ciancanelli, M., Ou, Y.-H., Lorenzo, L., Klaudel-Dreszler, M., Pauwels, E., Sancho-Shimizu, V., Perez de Diego, R., Abhyankar, A., Israelsson, E., Guo, Y., Cardon, A., Rozenberg, F., Lebon, P., Tardieu, M., Heropolitanska-Pliszka, E., Chaussabel, D., White, M. A., Abel, L., Zhang, S.-Y., Casanova, J.-L.

Rockefeller University Press

In: Journal of Experimental Medicine

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Publication Date: 2012-08-28

Description: Childhood herpes simplex virus-1 (HSV-1) encephalitis (HSE) may result from single-gene inborn errors of TLR3 immunity. TLR3-dependent induction of IFN-α/β or IFN- is crucial for protective immunity against primary HSV-1 infection in the central nervous system (CNS). We describe here two unrelated children with HSE carrying different heterozygous mutations (D50A and G159A) in TBK1 , the gene encoding TANK-binding kinase 1, a kinase at the crossroads of multiple IFN-inducing signaling pathways. Both mutant TBK1 alleles are loss-of-function but through different mechanisms: protein instability (D50A) or a loss of kinase activity (G159A). Both are also associated with an autosomal-dominant (AD) trait but by different mechanisms: haplotype insufficiency (D50A) or negative dominance (G159A). A defect in polyinosinic-polycytidylic acid–induced TLR3 responses can be detected in fibroblasts heterozygous for G159A but not for D50A TBK1 . Nevertheless, viral replication and cell death rates caused by two TLR3-dependent viruses (HSV-1 and vesicular stomatitis virus) were high in fibroblasts from both patients, and particularly so in G159A TBK1 fibroblasts. These phenotypes were rescued equally well by IFN-α2b. Moreover, the IFN responses to the TLR3-independent agonists and viruses tested were maintained in both patients’ peripheral blood mononuclear cells and fibroblasts. The narrow, partial cellular phenotype thus accounts for the clinical phenotype of these patients being limited to HSE. These data identify AD partial TBK1 deficiency as a new genetic etiology of childhood HSE, indicating that TBK1 is essential for the TLR3- and IFN-dependent control of HSV-1 in the CNS.

Print ISSN: 0022-1007

Electronic ISSN: 1540-9538

Topics: Medicine

Published by Rockefeller University Press

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Torso RTK controls Capicua degradation by changing its subcellular localization [RESEARCH REPORTS] (2012)

Grimm, O., Zini, V. S., Kim, Y., Casanova, J., Shvartsman, S. Y., Wieschaus, E.

The Company of Biologists

In: Development

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Publication Date: 2012-10-10

Description: Oliver Grimm, Victoria Sanchez Zini, Yoosik Kim, Jordi Casanova, Stanislav Y. Shvartsman, and Eric Wieschaus The transcriptional repressor Capicua (Cic) controls multiple aspects of Drosophila embryogenesis and has been implicated in vertebrate development and human diseases. Receptor tyrosine kinases (RTKs) can antagonize Cic-dependent gene repression, but the mechanisms responsible for this effect are not fully understood. Based on genetic and imaging studies in the early Drosophila embryo, we found that Torso RTK signaling can increase the rate of Cic degradation by changing its subcellular localization. We propose that Cic is degraded predominantly in the cytoplasm and show that Torso reduces the stability of Cic by controlling the rates of its nucleocytoplasmic transport. This model accounts for the experimentally observed spatiotemporal dynamics of Cic in the early embryo and might explain RTK-dependent control of Cic in other developmental contexts.

Print ISSN: 0950-1991

Electronic ISSN: 1477-9129

Topics: Biology

Published by The Company of Biologists

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Encoding relativistic potential dynamics into free evolution (2012)

C. Sabín, J. Casanova, J. J. García-Ripoll, L. Lamata, E. Solano, and J. León

American Physical Society (APS)

In: Physical Review A

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Publication Date: 2012-05-03

Description: Author(s): C. Sabín, J. Casanova, J. J. García-Ripoll, L. Lamata, E. Solano, and J. León We propose a method to simulate a Dirac or Majorana equation evolving under particular potentials with the use of the corresponding free evolution, while the potential dynamics is encoded in a static transformation upon the initial state. We extend our results to interacting two-body systems. [Phys. Rev. A 85, 052301] Published Wed May 02, 2012

Keywords: Quantum information

Print ISSN: 1050-2947

Electronic ISSN: 1094-1622

Topics: Physics

Published by American Physical Society (APS)

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New and recurrent gain-of-function STAT1 mutations in patients with chronic mucocutaneous candidiasis from Eastern and Central Europe (2013)

Soltesz, B., Toth, B., Shabashova, N., Bondarenko, A., Okada, S., Cypowyj, S., Abhyankar, A., Csorba, G., Tasko, S., Sarkadi, A. K., Mehes, L., Rozsival, P., Neumann, D., Chernyshova, L., Tulassay, Z., Puel, A., Casanova, J.-L., Sediva, A., Litzman, J., Marodi, L.

BMJ Publishing Group

In: Journal of Medical Genetics

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Publication Date: 2013-08-17

Description: Background Chronic mucocutaneous candidiasis disease (CMCD) may result from various inborn errors of interleukin (IL)-17-mediated immunity. Twelve of the 13 causal mutations described to date affect the coiled-coil domain (CCD) of STAT1 . Several mutations, including R274W in particular, are recurrent, but the underlying mechanism is unclear. Objective To investigate and describe nine patients with CMCD in Eastern and Central Europe, to assess the biochemical impact of STAT1 mutations, to determine cytokines in supernatants of Candida -exposed blood cells, to determine IL-17-producing T cell subsets and to determine STAT1 haplotypes in a family with the c.820C〉T (R274W) mutation. Results The novel c.537C〉A (N179K) STAT1 mutation was gain-of-function (GOF) for -activated factor (GAF)-dependent cellular responses. In a Russian patient, the cause of CMCD was the newly identified c.854 A〉G (Q285R) STAT1 mutation, which was also GOF for GAF-dependent responses. The c.1154C〉T (T385M) mutation affecting the DNA-binding domain (DBD) resulted in a gain of STAT1 phosphorylation in a Ukrainian patient. Impaired Candida -induced IL-17A and IL-22 secretion by leucocytes and lower levels of intracellular IL-17 and IL-22 production by T cells were found in several patients. Haplotype studies indicated that the c.820C〉T (R274W) mutation was recurrent due to a hotspot rather than a founder effect. Severe clinical phenotypes, including intracranial aneurysm, are presented. Conclusions The c.537C〉A and c.854A〉G mutations affecting the CCD and the c.1154C〉T mutation affecting the DBD of STAT1 are GOF. The c.820C〉T mutation of STAT1 in patients with CMCD is recurrent due to a hotspot. Patients carrying GOF mutations of STAT1 may develop multiple intracranial aneurysms by hitherto unknown mechanisms.

Keywords: Open access, Immunology (including allergy), Dermatology, Drugs: endocrine system

Print ISSN: 0022-2593

Electronic ISSN: 1468-6244

Topics: Medicine

Published by BMJ Publishing Group

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IL-12 receptor {beta}1 deficiency alters in vivo T follicular helper cell response in humans (2013)

Schmitt, N., Bustamante, J., Bourdery, L., Bentebibel, S. E., Boisson-Dupuis, S., Hamlin, F., Tran, M. V., Blankenship, D., Pascual, V., Savino, D. A., Banchereau, J., Casanova, J.-L., Ueno, H.

American Society of Hematology (ASH)

In: Blood

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Publication Date: 2013-04-26

Description: Antibody responses represent a key immune protection mechanism. T follicular helper (Tfh) cells are the major CD4 + T-cell subset that provides help to B cells to generate an antibody response. Tfh cells together with B cells form germinal centers (GCs), the site where high-affinity B cells are selected and differentiate into either memory B cells or long-lived plasma cells. We show here that interleukin-12 receptor β1 (IL-12Rβ1)–mediated signaling is important for in vivo Tfh response in humans. Although not prone to B cell-deficient–associated infections, subjects lacking functional IL-12Rβ1, a receptor for IL-12 and IL-23, displayed substantially less circulating memory Tfh and memory B cells than control subjects. GC formation in lymph nodes was also impaired in IL-12Rβ1–deficient subjects. Consistently, the avidity of tetanus toxoid–specific serum antibodies was substantially lower in these subjects than in age-matched controls. Tfh cells in tonsils from control individuals displayed the active form of signal transducer and activator of transcription 4 (STAT4), demonstrating that IL-12 is also acting on Tfh cells in GCs. Thus, our study shows that the IL-12–STAT4 axis is associated with the development and the functions of Tfh cells in vivo in humans.

Keywords: Immunobiology

Print ISSN: 0006-4971

Electronic ISSN: 1528-0020

Topics: Biology , Medicine

Published by American Society of Hematology (ASH)

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Association Study of Genes Controlling IL-12-dependent IFN-{gamma} Immunity: STAT4 Alleles Increase Risk of Pulmonary Tuberculosis in Morocco (2014)

Sabri, A., Grant, A. V., Cosker, K., El Azbaoui, S., Abid, A., Abderrahmani Rhorfi, I., Souhi, H., Janah, H., Alaoui-Tahiri, K., Gharbaoui, Y., Benkirane, M., Orlova, M., Boland, A., Deswarte, C., Migaud, M., Bustamante, J., Schurr, E., Boisson-Dupuis, S., Casanova, J.-L., Abel, L., El Baghdadi, J.

Oxford University Press

In: Journal of Infectious Diseases

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Publication Date: 2014-07-27

Description: Background. Only a minority of individuals infected with Mycobacterium tuberculosis develop clinical tuberculosis. Genetic epidemiological evidence suggests that pulmonary tuberculosis has a strong human genetic component. Previous genetic findings in Mendelian predisposition to more severe mycobacterial infections, including by M. tuberculosis , underlined the importance of the interleukin 12 (IL-12)/interferon (IFN-) circuit in antimycobacterial immunity. Methods. We conducted an association study in Morocco between pulmonary tuberculosis and a panel of single-nucleotide polymorphisms (SNPs) covering 14 core IL-12/IFN- circuit genes. The analyses were performed in a discovery family-based sample followed by replication in a case-control population. Results. Out of 228 SNPs tested in the family-based sample, 6 STAT4 SNPs were associated with pulmonary tuberculosis ( P = .0013–.01). We replicated the same direction of association for 1 cluster of 3 SNPs encompassing the promoter region of STAT4 . In the combined sample, the association was stronger among younger subjects (pulmonary tuberculosis onset 〈25 years) with an odds ratio of developing pulmonary tuberculosis at rs897200 for GG vs AG/AA subjects of 1.47 (1.06–2.04). Previous functional experiments showed that the G allele of rs897200 was associated with lower STAT4 expression. Conclusions. Our present findings in a Moroccan population support an association of pulmonary tuberculosis with STAT4 promoter-region polymorphisms that may impact STAT4 expression.

Print ISSN: 0022-1899

Electronic ISSN: 1537-6613

Topics: Medicine

Published by Oxford University Press on behalf of The Infectious Diseases Society of America (IDSA).

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TLR-Mediated Inflammatory Responses to Streptococcus pneumoniae Are Highly Dependent on Surface Expression of Bacterial Lipoproteins [INNATE IMMUNITY AND INFLAMMATION] (2014)

Tomlinson, G., Chimalapati, S., Pollard, T., Lapp, T., Cohen, J., Camberlein, E., Stafford, S., Periselneris, J., Aldridge, C., Vollmer, W., Picard, C., Casanova, J.-L., Noursadeghi, M., Brown, J.

The American Association of Immunologists (AAI)

In: Journal of Immunology

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Publication Date: 2014-09-20

Description: Streptococcus pneumoniae infections induce inflammatory responses that contribute toward both disease pathogenesis and immunity, but the host–pathogen interactions that mediate these effects are poorly defined. We used the surface lipoprotein-deficient lgt pneumococcal mutant strain to test the hypothesis that lipoproteins are key determinants of TLR-mediated immune responses to S. pneumoniae . We show using reporter assays that TLR2 signaling is dependent on pneumococcal lipoproteins, and that macrophage NF-B activation and TNF-α release were reduced in response to the lgt strain. Differences in TNF-α responses between lgt and wild-type bacteria were abrogated for macrophages from TLR2- but not TLR4-deficient mice. Transcriptional profiling of human macrophages revealed attenuated TLR2-associated responses to lgt S. pneumoniae , comprising many NF-B–regulated proinflammatory cytokine and chemokine genes. Importantly, non-TLR2–associated responses were preserved. Experiments using leukocytes from IL-1R–associated kinase-4–deficient patients and a mouse pneumonia model confirmed that proinflammatory responses were lipoprotein dependent. Our data suggest that leukocyte responses to bacterial lipoproteins are required for TLR2- and IL-1R–associated kinase-4–mediated inflammatory responses to S. pneumoniae .

Print ISSN: 0022-1767

Electronic ISSN: 1550-6606

Topics: Medicine

Published by The American Association of Immunologists (AAI)

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Guidelines for genetic studies in single patients: lessons from primary immunodeficiencies (2014)

Casanova, J.-L., Conley, M. E., Seligman, S. J., Abel, L., Notarangelo, L. D.

Rockefeller University Press

In: Journal of Experimental Medicine

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Publication Date: 2014-10-21

Description: Can genetic and clinical findings made in a single patient be considered sufficient to establish a causal relationship between genotype and phenotype? We report that up to 49 of the 232 monogenic etiologies (21%) of human primary immunodeficiencies (PIDs) were initially reported in single patients. The ability to incriminate single-gene inborn errors in immunodeficient patients results from the relative ease in validating the disease-causing role of the genotype by in-depth mechanistic studies demonstrating the structural and functional consequences of the mutations using blood samples. The candidate genotype can be causally connected to a clinical phenotype using cellular (leukocytes) or molecular (plasma) substrates. The recent advent of next generation sequencing (NGS), with whole exome and whole genome sequencing, induced pluripotent stem cell (iPSC) technology, and gene editing technologies—including in particular the clustered regularly interspaced short palindromic repeats (CRISPR)/Cas9 technology—offer new and exciting possibilities for the genetic exploration of single patients not only in hematology and immunology but also in other fields. We propose three criteria for deciding if the clinical and experimental data suffice to establish a causal relationship based on only one case. The patient’s candidate genotype must not occur in individuals without the clinical phenotype. Experimental studies must indicate that the genetic variant impairs, destroys, or alters the expression or function of the gene product (or two genetic variants for compound heterozygosity). The causal relationship between the candidate genotype and the clinical phenotype must be confirmed via a relevant cellular phenotype, or by default via a relevant animal phenotype. When supported by satisfaction of rigorous criteria, the report of single patient–based discovery of Mendelian disorders should be encouraged, as it can provide the first step in the understanding of a group of human diseases, thereby revealing crucial pathways underlying physiological and pathological processes.

Print ISSN: 0022-1007

Electronic ISSN: 1540-9538

Topics: Medicine

Published by Rockefeller University Press

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Arid3b is essential for second heart field cell deployment and heart patterning [RESEARCH ARTICLES] (2014)

Uribe, V., Badia-Careaga, C., Casanova, J. C., Dominguez, J. N., de la Pompa, J. L., Sanz-Ezquerro, J. J.

The Company of Biologists

In: Development

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Publication Date: 2014-10-22

Description: Veronica Uribe, Claudio Badia-Careaga, Jesus C. Casanova, Jorge N. Dominguez, Jose Luis de la Pompa, and Juan Jose Sanz-Ezquerro Arid3b , a member of the conserved ARID family of transcription factors, is essential for mouse embryonic development but its precise roles are poorly understood. Here, we show that Arid3b is expressed in the myocardium of the tubular heart and in second heart field progenitors. Arid3b -deficient embryos show cardiac abnormalities, including a notable shortening of the poles, absence of myocardial differentiation and altered patterning of the atrioventricular canal, which also lacks epithelial-to-mesenchymal transition. Proliferation and death of progenitors as well as early patterning of the heart appear normal. However, DiI labelling of second heart field progenitors revealed a defect in the addition of cells to the heart. RNA microarray analysis uncovered a set of differentially expressed genes in Arid3b -deficient tissues, including Bhlhb2 , a regulator of cardiomyocyte differentiation, and Lims2 , a gene involved in cell migration. Arid3b is thus required for heart development by regulating the motility and differentiation of heart progenitors. These findings identify Arid3b as a candidate gene involved in the aetiology of human congenital malformations.

Print ISSN: 0950-1991

Electronic ISSN: 1477-9129

Topics: Biology

Published by The Company of Biologists

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Functional characterization of the human dendritic cell immunodeficiency associated with the IRF8K108E mutation (2014)

Salem, S., Langlais, D., Lefebvre, F., Bourque, G., Bigley, V., Haniffa, M., Casanova, J.-L., Burk, D., Berghuis, A., Butler, K. M., Leahy, T. R., Hambleton, S., Gros, P.

American Society of Hematology (ASH)

In: Blood

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Publication Date: 2014-09-19

Description: We have previously reported on a unique patient in whom homozygosity for a mutation at IRF8 (IRF8 K108E ) causes a severe immunodeficiency. Laboratory evaluation revealed a highly unusual myeloid compartment, remarkable for the complete absence of CD14 + and CD16 + monocytes, absence of CD11c + conventional dendritic cells (DCs) and CD11c + /CD123 + plasmacytoid DCs, and striking granulocytic hyperplasia. The patient initially presented with severe disseminated mycobacterial and mucocutaneous fungal infections and was ultimately cured by cord blood transplant. Sequencing RNA from the IRF8 K108E patient’s primary blood cells prior to transplant shows not only depletion of IRF8-bound and IRF8-regulated transcriptional targets, in keeping with the distorted composition of the myeloid compartment, but also a paucity of transcripts associated with activated CD4 + and CD8 + T lymphocytes. This suggests that T cells reared in the absence of a functional antigen-presenting compartment in IRF8 K108E are anergic. Biochemical characterization of the IRF8 K108E mutant in vitro shows that loss of the positively charged side chain at K108 causes loss of nuclear localization and loss of transcriptional activity, which is concomitant with decreased protein stability, increased ubiquitination, increased small ubiquitin-like modification, and enhanced proteasomal degradation. These findings provide functional insight into the molecular basis of immunodeficiency associated with loss of IRF8.

Keywords: Pediatric Hematology, Immunobiology, Free Research Articles, Phagocytes, Granulocytes, and Myelopoiesis

Print ISSN: 0006-4971

Electronic ISSN: 1528-0020

Topics: Biology , Medicine

Published by American Society of Hematology (ASH)

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