Genetic and functional data identifying Cd101 as a type 1 diabetes (T1D) susceptibility gene in nonobese diabetic (NOD) mice

Mattner, Jochen; Mohammed, Javid P.; Fusakio, Michael E.; Giessler, Claudia; Hackstein, Carl-Philipp; Opoka, Robert; Wrage, Marius; Schey, Regina; Clark, J. Stephen; Fraser, Heather I.; Rainbow, Daniel B.; Wicker, Linda S.

doi:10.1371/journal.pgen.1008178

Cited by 11 publications

(5 citation statements)

References 54 publications

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“…However, in children with T1D, GAL-1 correlated positively with CD25 MFI in Treg cells, as well as with both the number and frequency of CD101 + Treg cells. CD101 has previously been identified as a T1D susceptibility gene and is proposed to restrain the expansion of diabetogenic CD4 and CD8 expressing T lymphocytes and reduce T1D frequency in NOD mice [ 56 ]. It is thus possible that interaction between GAL-1 and CD101 is a shared pathway in the development of T1D.…”

Section: Discussionmentioning

confidence: 99%

Galectin-1 correlates with inflammatory markers and T regulatory cells in children with type 1 diabetes and/or celiac disease

Fryk,

Wilsson,

Tompa

et al. 2023

Clinical and Experimental Immunology

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Type 1 diabetes (T1D) and celiac disease (CeD) are common autoimmune diseases in children where the pathophysiology is not fully characterized. The autoimmune process involves a complex scenario of both inflammatory and regulatory features. Galectin-1 (GAL-1) has a wide range of biological activities e.g., interaction with immune cells. We examined the relationship between GAL-1 and soluble immune markers and T cell subsets in a cohort of children with T1D and/or CeD relative to healthy children. Galectin-1, together with several soluble immune markers (e g interleukins (IL)), tumor necrosis factor (TNF), acute phase proteins and matrix metalloproteinases (MMP) were measured in sera from children with T1D and/or CeD by fluorochrome (Luminex) technique using children without these diseases as a reference. Subgroups of T cells, including T regulatory (Treg) cells, were analyzed by flow cytometry. Association between GAL-1, pro-inflammatory markers and Treg cells differed depending on which illness combination was present. In children with both T1D and CeD, GAL-1 correlated positively with pro-inflammatory markers (IL-1β, -6 and TNF-α). Composite scores increased the strength of correlation between GAL-1 and pro-inflammatory markers, Th1-associated interferon (IFN)-γ, and T1D-associated visfatin. Contrary, in children diagnosed with exclusively T1D, GAL-1 was positively correlated to CD25hi and CD25hiCD101+ Treg cells. For children with only CeD, no association between GAL-1 and other immune markers was observed. In conclusion, the association observed between GAL-1, soluble immune markers and Treg cells may indicate a role for GAL-1 in the pathophysiology of T1D and, to some extent, also in CeD.

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Section: Discussionmentioning

confidence: 99%

Galectin-1 correlates with inflammatory markers and T regulatory cells in children with type 1 diabetes and/or celiac disease

Fryk,

Wilsson,

Tompa

et al. 2023

Clinical and Experimental Immunology

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“…Pathways include metabolism [42], transport of small molecules [43] and immune system [44] are linked with progression of FSGS. PDK4 [45], ALB (albumin) [46], EGR1 [47], RYR3 [48], APOH (apolipoprotein H) [49], CYP27B1 [50], ESM1 [51], GATA6 [52], PCK1 [53], TET2 [54], AFP (alpha fetoprotein) [55], CACNA1D [56], ATF3 [57], EGF (epidermal growth factor) [58], LPL (lipoprotein lipase) [59], PPARGC1A [60], PLG (plasminogen) [61], NR4A1 [62], STRA6 [63], MLXIPL (MLX interacting protein like) [64], PLA2G6 [65], RGS2 [66], GPS2 [67], SOX5 [68], GLUL (glutamate-ammonia ligase) [69], RYK (receptor like tyrosine kinase) [70], NFKBIA (NFKB inhibitor alpha) [71], LGR4 [72], SPRY2 [73], TRPC1 [74], KL (klotho) [75], GCLC (glutamate-cysteine ligase catalytic subunit) [76], NOX4 [77], CD69 [78], SLC19A2 [79], S100A12 [80], MT1A [81], SORCS1 [82], FKBP5 [83], AFM (afamin) [84], CA3 [85], MAOA (monoamine oxidase A) [86], ND1 [87], ATP6 [88], CHGA (chromogranin A) [89], ICOS (inducible T cell costimulator) [90], DBH (dopamine beta-hydroxylase) [91], CD5 [92], LTA (lymphotoxin alpha) [93], IFNG (interferon gamma) [94], MPO (myeloperoxidase) [95], CD70 [96], CD300E [97], COLEC12 [98], TLR10 [99], LCN2 [100], SLAMF7 [101], TREM2 [102], ITGAL (integrin subunit alpha L) [103], CD27 [104], JAK3 [105], CCR5 [106], FCN1 [107], IL1RN [108], CX3CR1 [109], PDCD1 [110], TRPM2 [111], PLEK (pleckstrin) [112], CD101 [113],...…”

Section: Discussionmentioning

confidence: 99%

“…The GO [64], PLA2G6 [65], RGS2 [66], GPS2 [67], SOX5 [68], GLUL (glutamate-ammonia ligase) [69], RYK (receptor like tyrosine kinase) [70], NFKBIA (NFKB inhibitor alpha) [71], LGR4 [102], ITGAL (integrin subunit alpha L) [103], CD27 [104], JAK3 [105], CCR5 [106], FCN1 [107], IL1RN [108], CX3CR1 [109], PDCD1 [110], TRPM2 [111], PLEK (pleckstrin) [112], CD101 [113], TNF (tumor necrosis factor) [114], CD48 [115], ALOX5 [116], TLR7 [117], CCL3 [118], C2 [119], TNFRSF1B [120], CCR2 [121], PLA2G7 [122], TH (tyrosine hydroxylase) [123], WNT7A [124], ADRB3 [125], GPBAR1 [126], SLC6A20 [127], FUT2 [128], ANK1 [129], NOS3 [130], APLNR (apelin receptor) [131], COMP (cartilage oligomeric matrix protein) [132], RETN (resistin) [133], NMU (neuromedin U) [134], S100B [135], IGFBP1 [136], COL1A1 [137], HBB (hemoglobin subunit beta) [138] and PLAC8 [139] genes plays important regulatory roles in diabetes mellitus. Various genes such as PDK4 [140], ALB (albumin) [141], EGR1 [142], RYR3 [48], CYP27B1 [143], GATA6 [144], NR4A3 [145], TET2…”

Section: Discussionmentioning

confidence: 99%

Identification of biomarkers and pathways for focal segmental glomerulosclerosis using next generation sequencing data and bioinformatics analysis

Vastrad¹,

Vastrad²

2022

Preprint

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Focal segmental glomerulosclerosis (FSGS) is a renal disease leading threat to human health around the world. Here we aimed to explore novel molecular and potential therapeutic targets in FSGS through adopting integrated bioinformatics tools. Next generation sequencing (NGS) data of GSE197307 was available from Gene Expression Omnibus (GEO) database. Furthermore, differentially expressed genes (DEGs) were screened using the DESeq2 package in R software. Gene ontology (GO) and REACTOME pathway enrichment analyses of DEGs were performed via g:Profiler. Then, the protein-protein interaction (PPI) network, miRNA- hub gene regulatory network and TF-hub gene regulatory network were constructed using the HIPPIE, miRNet and NetworkAnalyst databases. Hub genes were validated using the receiver operating characteristic curve (ROC) analysis. By performing DEGs analysis, 488 up regulated genes and 488 down regulated genes were successfully identified from GSE197307, respectively. And they were mainly enriched in the terms of multicellular organismal process, cell periphery, protein binding, metabolism, immune system process, signaling receptor binding and immune system. Based on the data of protein-protein interaction (PPI), miRNA-hub gene regulatory network and TF-hub gene regulatory network, the top hub genes were ranked, including ILK, DDX5, MATR3, ALB, FOS, MKI67, PLK1, TNF, LCK and GTSE1. Bioinformatics analysis of NGS data identified signaling pathways and hub genes, potentially representing molecular mechanisms for the occurrence, progression, and risk prediction in FSGS.

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“…Similarly, the frequency of T follicular regulatory (Tfr) cells, a specialized regulatory counterpart of T follicular helper (Tfh) cells, is reduced in PLNs of T1D patients, and re-supplementation of Tfr cells delays T1D development in mice [ 92 ]. The unbalanced immune status of human T1D is featured by functional defects in CD4 + CD25 + Tregs in PLNs but not in peripheral blood [ 93 , 94 ]. PLN Tregs inhibit in situ differentiation of islet-reactive CD8 + T cells, and the suppression is mediated by the TGF-β/TGF-βRII axis, as Treg cells could not control naïve or activated islet-reactive CD8 + T cells bearing a dominant-negative TGF-βRII genotype following adoptive transfer [ 95 ].…”

Section: Pln Remodeling Is Featured By the Perturbation Of Immune Mic...mentioning

confidence: 99%

Pancreatic draining lymph nodes (PLNs) serve as a pathogenic hub contributing to the development of type 1 diabetes

Sun,

Yang,

Wang

et al. 2023

Cell Biosci

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Type 1 diabetes (T1D) is a chronic, progressive autoinflammatory disorder resulting from the breakdown of self-tolerance and unrestrained β cell-reactive immune response. Activation of immune cells is initiated in islet and amplified in lymphoid tissues, especially those pancreatic draining lymph nodes (PLNs). The knowledge of PLNs as the hub of aberrant immune response is continuously being replenished and renewed. Here we provide a PLN-centered view of T1D pathogenesis and emphasize that PLNs integrate signal inputs from the pancreas, gut, viral infection or peripheral circulation, undergo immune remodeling within the local microenvironment and export effector cell components into pancreas to affect T1D progression. In accordance, we suggest that T1D intervention can be implemented by three major ways: cutting off the signal inputs into PLNs (reduce inflammatory β cell damage, enhance gut integrity and control pathogenic viral infections), modulating the immune activation status of PLNs and blocking the outputs of PLNs towards pancreatic islets. Given the dynamic and complex nature of T1D etiology, the corresponding intervention strategy is thus required to be comprehensive to ensure optimal therapeutic efficacy.

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Genetic and functional data identifying Cd101 as a type 1 diabetes (T1D) susceptibility gene in nonobese diabetic (NOD) mice

Cited by 11 publications

References 54 publications

Galectin-1 correlates with inflammatory markers and T regulatory cells in children with type 1 diabetes and/or celiac disease

Galectin-1 correlates with inflammatory markers and T regulatory cells in children with type 1 diabetes and/or celiac disease

Identification of biomarkers and pathways for focal segmental glomerulosclerosis using next generation sequencing data and bioinformatics analysis

Pancreatic draining lymph nodes (PLNs) serve as a pathogenic hub contributing to the development of type 1 diabetes

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