MHC Class II Presentation in Autoimmunity

Ishina, Irina A.; Захарова, М. В.; Kurbatskaia, Inna N.; Mamedov, A. E.; Belogurov, A. A.; Gabibov, Alexander

doi:10.3390/cells12020314

Cited by 21 publications

(11 citation statements)

References 172 publications

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“…All four proteins belong to the MHC II class, which is essential for triggering an effective immune response to CD4 T cells and maintaining autoantigen tolerance. 36 However, we did not find significant differences in the expressions of these four genes in the expression profile analysis of psoriatic lesions based on GEO datasets, which needs more experiments to prove.…”

Section: F I G U R E 3 Multiomics Analysis Of the Underlying Mechanis...mentioning

confidence: 64%

Exploration of the causality of frailty index on psoriasis: A Mendelian randomization study

Lei,

Xing,

Chen

et al. 2024

Skin Research and Technology

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BackgroundFrailty is associated with a variety of diseases, but the relationship between frailty and psoriasis remains unclear.MethodsFirst, we conducted a two‐sample Mendelian randomization based on genome‐wide association studies (GWAS) to investigate genetic causality between frailty index and common diseases in dermatology. Inverse variance weighted was used to estimate causality. Second, expression quantitative trait locus (eQTLs) analysis was conducted to identify the genes affected by Single nucleotide polymorphisms (SNPs). Third, we performed function and pathway enrichment, transcriptome‐wide association studies (TWAS) analysis based on eQTLs.ResultsIt was shown that the rise of frailty index could increase the risk of psoriasis (IVW, beta = 0.916, OR = 2.500, 95%CI:1.418‐4.408, p = 0.002) through Mendelian randomization (MR), and there was no heterogeneity and pleiotropy. There was no causality between the frailty index and other common diseases in dermatology. We found 31 eQTLs based on strongly correlated SNPs in the causality. TWAS analysis found that the expressions of four genes were closely related to psoriasis, including HLA‐DQA1, HLA‐DQA2, HLA‐DRB1 and HLA‐DQB1.ConclusionIt suggested that the frailty index had a significant positive causality on the risk of psoriasis, which was well documented by combined genomic, transcriptome, and proteome analyses.

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Section: F I G U R E 3 Multiomics Analysis Of the Underlying Mechanis...mentioning

confidence: 64%

Exploration of the causality of frailty index on psoriasis: A Mendelian randomization study

Lei,

Xing,

Chen

et al. 2024

Skin Research and Technology

View full text Add to dashboard Cite

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“…However, it has been reported that the genetic implementation of antigenic minigenes can elicit lower reactivity compared to the exogenous loading of antigenic fragments ( Parkhurst et al, 2019 ). Exogenous loading of peptides may also require competitive displacement of the peptide already presented on MHC-II, which can be problematic when exogenous loading is required for low-affinity peptides that may still be presented and elicit T-cell responses under physiological conditions ( Stadinski et al, 2010 ; Yang et al, 2014 ; Ishina et al, 2023 ). In our system, each peptide of interest is covalently bound to the beta chain of the MHC-II molecule, allowing for the presentation of low-affinity peptides.…”

Section: Discussionmentioning

confidence: 99%

Genetically engineered CD80–pMHC-harboring extracellular vesicles for antigen-specific CD4+ T-cell engagement

Ishina,

Kurbatskaia,

Mamedov

et al. 2024

Front. Bioeng. Biotechnol.

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The identification of low-frequency antigen-specific CD4+ T cells is crucial for effective immunomonitoring across various diseases. However, this task still encounters experimental challenges necessitating the implementation of enrichment procedures. While existing antigen-specific expansion technologies predominantly concentrate on the enrichment of CD8+ T cells, advancements in methods targeting CD4+ T cells have been limited. In this study, we report a technique that harnesses antigen-presenting extracellular vesicles (EVs) for stimulation and expansion of antigen-specific CD4+ T cells. EVs are derived from a genetically modified HeLa cell line designed to emulate professional antigen-presenting cells (APCs) by expressing key costimulatory molecules CD80 and specific peptide–MHC-II complexes (pMHCs). Our results demonstrate the beneficial potent stimulatory capacity of EVs in activating both immortalized and isolated human CD4+ T cells from peripheral blood mononuclear cells (PBMCs). Our technique successfully expands low-frequency influenza-specific CD4+ T cells from healthy individuals. In summary, the elaborated methodology represents a streamlined and efficient approach for the detection and expansion of antigen-specific CD4+ T cells, presenting a valuable alternative to existing antigen-specific T-cell expansion protocols.

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“…Moreover, their transcriptomic signature also revealed higher expression levels of MHC class II autoantigens and Aβ binding receptor genes. It was previously reported that MHC class II autoantigen-expressing microglia were associated with various autoimmune-related neurodegenerative diseases and the development of chronic inflammatory lesions [ 116 – 119 ], which hinted at an intrinsic pathological nature of these cells. In addition to these gain-of-function genes, downregulated genes in FDAMic also suggested a loss in phagocytic activities, which may render them ineffective in clearing Aβ and other protein aggregates from the region [ 120 ] despite exhibiting Aβ binding properties.…”

Section: Discussionmentioning

confidence: 99%

Identification of female-enriched and disease-associated microglia (FDAMic) contributes to sexual dimorphism in late-onset Alzheimer’s disease

Wu,

Bi,

Chow

2024

J Neuroinflammation

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Background Late-onset Alzheimer’s disease (LOAD) is the most common form of dementia; it disproportionally affects women in terms of both incidence rates and severity of progression. The cellular and molecular mechanisms underlying this clinical phenomenon remain elusive and ill-defined. Methods In-depth analyses were performed with multiple human LOAD single-nucleus transcriptome datasets to thoroughly characterize cell populations in the cerebral cortex. ROSMAP bulk human brain tissue transcriptome and DNA methylome datasets were also included for validation. Detailed assessments of microglial cell subpopulations and their relevance to sex-biased changes at the tissue level were performed. Clinical trait associations, cell evolutionary trajectories, and transcription regulon analyses were conducted. Results The relative numbers of functionally defective microglia were aberrantly increased uniquely among affected females. Substratification of the microglia into different subtypes according to their transcriptomic signatures identified a group of female-enriched and disease-associated microglia (FDAMic), the numbers of which were positively associated with disease severity. Phenotypically, these cells exhibit transcriptomic signatures that support active proliferation, MHC class II autoantigen presentation and amyloid-β binding, but they are also likely defective in phagocytosis. FDAMic are likely evolved from female activated response microglia (ARMic) with an APOE4 background and compromised estrogen receptor (ER) signaling that is deemed to be active among most subtypes of microglia. Conclusion This study offered important insights at both the cellular and molecular levels into how ER signaling affects microglial heterogeneity and function. FDAMic are associated with more advanced pathologies and severe trends of cognitive decline. Their emergence could, at least in part, explain the phenomenon of greater penetrance of the APOE4 genotype found in females. The biases of FDAMic emergence toward female sex and APOE4 status may also explain why hormone replacement therapy is more effective in APOE4 carriers. The pathologic nature of FDAMic suggests that selective modulations of these cells may help to regain brain neuroimmune homeostasis, serving as a new target for future drug development.

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MHC Class II Presentation in Autoimmunity

Cited by 21 publications

References 172 publications

Exploration of the causality of frailty index on psoriasis: A Mendelian randomization study

Exploration of the causality of frailty index on psoriasis: A Mendelian randomization study

Genetically engineered CD80–pMHC-harboring extracellular vesicles for antigen-specific CD4+ T-cell engagement

Identification of female-enriched and disease-associated microglia (FDAMic) contributes to sexual dimorphism in late-onset Alzheimer’s disease

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