Linkage of familial hemophagocytic lymphohistiocytosis (FHL) type-4 to chromosome 6q24 and identification of mutations in syntaxin 11

Stadt, Udo zur; Schmidt, Susanne; Kasper, Brigitte; Beutel, Karin; Diler, A. Sarper; Henter, Jan‐Inge; Kabisch, H; Schneppenheim, Reinhard; Nürnberg, Peter; Janka, Gritta; Hennies, Hans Christian

doi:10.1093/hmg/ddi076

Cited by 497 publications

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“…Defective NK cell degranulation and cytotoxicity have been identified in patients with FHL-4, which correlates with a deficiency in STX11 expression [5,13]. Therefore we investigated whether a constitutive deficiency of STX11 in NK cells and CTL results in dysregulated degranulation and granule exocytosis in both cell types and whether this altered effector function correlates with a specific NK or CD8 + T-cell phenotype.…”

Section: Stx11 −/− Ctls and Nk Cellsmentioning

confidence: 99%

“…MUNC13-4 and Rab27a) and STX11 [10][11][12][13]. The underlying pathology is the familial hemophagocytic lymphohistiocytosis (FHL), a rare autosomal recessive disorder characterised by an increased inflammatory response with abnormal secretion of proinflammatory cytokines TNF,.…”

Section: Introductionmentioning

confidence: 99%

“…This is in concert with previous findings in lymphocytes from healthy donors and FHL type 4 patient samples showing that a deficiency in STX11 leads to an impaired degranulation and cytotoxic activity [4,5]. Thus, Stx11 −/− mice that were found to carry no overt defect in immune system development and immune cell populations in lymphatic tissues could be an ideal in vivo model for further dissecting the Hemophagocytic Lymphohistiocytosis (HLH) pathogenesis, in particular FHL-4 which is caused by a mutated STX11 gene in humans [13]. Nevertheless, Stx11 −/− mice would still represent an important tool for investigating the principles of cytotoxic lymphocyte degranulation and vesicular trafficking.…”

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Syntaxin 11 is required for NK and CD8⁺ T‐cell cytotoxicity and neutrophil degranulation

et al. 2012

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Syntaxin 11 (STX11) controls vesicular trafficking and is a key player in exocytosis. SinceStx11 mutations are causally associated with a familial hemophagocytic lymphohistiocytosis, we wanted to clarify whether STX11 is functionally important for key immune cell populations. This was studied in primary cells obtained from newly generated Stx11 −/− mice. Our data revealed that STX11 is not only widely expressed in different immune cells, but also induced upon LPS or IFN-γ treatment. However, Stx11 deficiency does not affect macrophage phagocytic function and cytokine secretion, mast cell activation, or antigen presentation by DCs. Instead, STX11 selectively controls lymphocyte cytotoxicity in NK and activated CD8 + T cells and degranulation in neutrophils. Stx11 −/− NK cells and CTLs show impaired degranulation, despite a comparable activation, maturation and expression of the complex-forming partners MUNC18-2 and VTI1B. In addition, Stx11 −/− CTLs and NK cells produce abnormal levels of IFN-γ. Since functional reconstitution rescues the defective phenotype of Stx11 −/− CTLs, we suggest a direct, specific and key role of STX11 in controlling lymphocyte cytotoxicity, cytokine production and secretion. Finally, we show that these mice are a very useful tool for dissecting the role of STX11 in vesicular trafficking and secretion. Keywords: CTL r Cytokines r Exocytosis r N-ethylmaleimide-sensitive factor attachment protein receptorSee accompanying Commentary by Lopez and Voskoboinik.Additional supporting information may be found in the online version of this article at the publisher's web-site IntroductionSyntaxin 11 (STX11) belongs to the family of N-ethylmaleimidesensitive factor attachment protein receptor (SNARE) proteins Correspondence: Prof. Silvia Bulfone-Paus e-mail: sbulfone@fz-borstel.de and is involved in intracellular membrane trafficking events by interacting with other family members or by associating with membranes by palmitoylation of cysteine residues [1][2][3]. STX11 is expressed in a wide variety of cells including human monocytes/macrophages, neutrophils, B cells, NK cells and CD8 + T cells [2][3][4][5][6][7][8][9]. STX11 is enriched in immune tissues such as thymus, spleen C 2012 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim www.eji-journal.eu Eur. J. Immunol. 2013. 43: 194-208 Immunomodulation 195 Values represent the mean ± SEM percentage of cell subsets in the spleen (n = 8) and lymph nodes (WT n = 7; Stx11 −/− n = 6) and are the summary of three experiments performed.and lymph nodes, but lower levels of protein are detectable also in heart, kidney and liver [2]. STX11 localizes mainly in the vesicular tubular clusters, an organelle complex between the endoplasmic reticulum and the Golgi, and displays, in addition, a spotted staining pattern throughout the cell periphery [2,9]. While STX11 has been recognized to act as a negative regulator of both phagocytosis and intracellular trafficking between endosomes, lysosomes and the outer membrane in macrophages [6,9], in human NK cells and CTLs, ST...

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Section: Stx11 −/− Ctls and Nk Cellsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Syntaxin 11 is required for NK and CD8⁺ T‐cell cytotoxicity and neutrophil degranulation

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“…Although the cytolytic cells of the patients with FHLH caused by MUNC13-4 mutations produce sufficient amounts of perforin, the poor ability to deliver the content of the cytolytic granules to the immunologic synapse with the target cell leads to profoundly decreased cytolytic activity. More recently, mutations in two other genes encoding proteins that facilitate granule fusion in intracellular trafficking events have been linked to the development of primary HLH: Syntaxin 11, a member of the SNARE protein family, 28 and syntaxin binding protein 2 (STXBP2, also known as MUNC18-2) 27 ( Figure 2).…”

Section: Genetic Factors For Mas In Sjiamentioning

confidence: 99%

“…48 Munc13-4 is likely important in activating Syntaxin 11 that in turn is important for vesicle fusion. 25,28 Absence of any these molecules prevents the release of perforin and therefore destruction of target antigenpresenting cells (Figure 2). Accordingly, mice deficient in the genes encoding Munc13-4 49 and Rab27a 50,51 also develop HLH upon infection with lymphochoriomeningitic virus in an IFNgdependent manner.…”

Section: Proposed Pathophysiology Of Mas In Children With Sjiamentioning

confidence: 99%

Macrophage activation syndrome as part of systemic juvenile idiopathic arthritis: diagnosis, genetics, pathophysiology and treatment

et al. 2012

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Macrophage activation syndrome (MAS) is a severe, frequently fatal complication of systemic juvenile idiopathic arthritis (sJIA) with features of hemophagocytosis leading to coagulopathy, pancytopenia, and liver and central nervous system dysfunction. MAS is overt in 10% of children with sJIA but occurs subclinically in another 30 --40%. It is difficult to distinguish sJIA disease flare from MAS. Development of criteria for establishing MAS as part of sJIA are under way and will hopefully prove sensitive and specific. Mutations in cytolytic pathway genes are increasingly being recognized in children who develop MAS as part of sJIA. Identification of these mutations may someday assist in MAS diagnosis. Defects in cytolytic genes have provided murine models of MAS to study pathophysiology and treatment. Recently, the first mouse model of MAS not requiring infection but rather dependent on repeated stimulation through Toll-like receptors was reported. This provides a model of MAS that may more accurately reflect MAS pathology in the setting of autoinflammation or autoimmunity. This model confirms the importance of a balance between pro-and anti-inflammatory cytokines. There has been remarkable progress in the use of anti-pro-inflammatory cytokine therapy, particularly against interleukin-1, in the treatment of secondary forms of MAS, such as in sJIA.

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Membrane Traffic and Disease

Cláudio

Pereira

Barral

2014

Encyclopedia of Life Sciences

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Membrane traffic is a highly regulated process that ensures the communication between membrane‐bound compartments while maintaining their specific protein and lipid composition. It can be divided into four steps: cargo sorting and budding of a vesicle from a donor compartment, transport along the cytoskeleton, tethering and docking to an acceptor compartment, and finally fusion with the acceptor compartment. Importantly, defects in any of these steps can lead to diseases that affect different tissues and organs. At the subcellular level, several of these diseases affect compartments from specialized cell types known as lysosome‐related organelles. Moreover, the dysfunction of membrane traffic processes required ubiquitously can lead to restricted phenotypes, underscoring the redundancy of these processes and/or the sensitivity of certain cell types to their impairment. Thus, the study of the diseases caused by defects in membrane traffic provides an opportunity to understand its role in normal cell physiology and discover novel therapies. Key Concepts: Defects in any of the steps of vesicular traffic can lead to disease. Vesicular traffic regulation shows redundancy. Defects in ubiquitously‐expressed proteins can result in a tissue‐restricted phenotype. Lysosome‐related organelles are commonly affected upon impairment of vesicular traffic. Several diseases are caused by defects in different proteins involved in the same biological process/pathway.

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Linkage of familial hemophagocytic lymphohistiocytosis (FHL) type-4 to chromosome 6q24 and identification of mutations in syntaxin 11

Cited by 497 publications

References 41 publications

Syntaxin 11 is required for NK and CD8⁺ T‐cell cytotoxicity and neutrophil degranulation

Syntaxin 11 is required for NK and CD8⁺ T‐cell cytotoxicity and neutrophil degranulation

Macrophage activation syndrome as part of systemic juvenile idiopathic arthritis: diagnosis, genetics, pathophysiology and treatment

Membrane Traffic and Disease

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Linkage of familial hemophagocytic lymphohistiocytosis (FHL) type-4 to chromosome 6q24 and identification of mutations in syntaxin 11

Cited by 497 publications

References 41 publications

Syntaxin 11 is required for NK and CD8+ T‐cell cytotoxicity and neutrophil degranulation

Syntaxin 11 is required for NK and CD8+ T‐cell cytotoxicity and neutrophil degranulation

Macrophage activation syndrome as part of systemic juvenile idiopathic arthritis: diagnosis, genetics, pathophysiology and treatment

Membrane Traffic and Disease

Contact Info

Product

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Syntaxin 11 is required for NK and CD8⁺ T‐cell cytotoxicity and neutrophil degranulation

Syntaxin 11 is required for NK and CD8⁺ T‐cell cytotoxicity and neutrophil degranulation