Modulation of CD4+ T Helper Cell Memory Responses in the Human Skin

Padovan, Elisabetta

doi:10.1159/000477728

Cited by 6 publications

(5 citation statements)

References 143 publications

(208 reference statements)

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“…Hence, the modulation of these pathways will not only contribute to maintaining homeostatic regulation of the immune system but may also contribute to reducing cell apoptosis and necrosis. Other pathways involving T-helper cells, cytokine and chemokine signallers are also closely associated to enhance the immune system which could contribute to up-regulating the down-regulated immune system during corona infection [18][19][20].…”

Section: Discussionmentioning

confidence: 99%

In silico screening of JAK-STAT modulators from the antiviral plants of Indian traditional system of medicine with the potential to inhibit 2019 novel coronavirus

Khanal

Duyu

Patil

et al. 2020

Preprint

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Aim. The present study was aimed to identify the lead hits from reported anti-viral Indian medicinal plants to modulate the proteins through the JAK-STAT pathway and to identify the proteins that share the domain with coronavirus (COVID19) associated proteins i.e. 3CLpro, PLpro, and spike protein. Methods. The reported anti-viral plants were screened from the available databases and published literature; their phytoconstituents were retrieved, gene-expression was predicted and the modulated proteins in JAK-STAT pathway were predicted. The interaction between proteins was evaluated using STRING and the network between phytoconstituents and proteins was constructed using Cytoscape. The druglikeness score was predicted using MolSoft and the ADMET profile of phytoconstituents was evaluated using admetSAR2.0. The domain of three proteins i.e. 3CLpro, PLpro, and spike protein of coronavirus was compared using NCBI blastP against the RCSB database. Results. The majority of the phytoconstituents from the anti-viral plants were predicted to target TRAF5 protein in the JAK-STAT pathway; among them, vitexilactone was predicted to possess the highest druglikeness score. Proteins targeted in the JAK-STAT pathways were also predicted to modulate the immune system. Similarly, the docking study identified sesaminol 2-O-β-D-gentiobioside to possess the highest binding affinity with spike protein. Similarly, phylogeny comparison also identified the common protein domains with other stains of microbes like murine hepatitis virus strain A59, avian infectious bronchitis virus, and porcine epidemic diarrhea virus CV777. Conclusion. Although, the present study is based on computer simulations and database mining, it provides two important aspects in identifying the lead hits against coronavirus. First, targeting the JAK-STAT pathway in the corona-infected host by folk anti-viral agents can regulate the immune system which would inhibit spreading the virus inside the subject. Secondly, the well-known targets of coronavirus i.e. 3CLpro, PLpro, and spike protein share some common domains with other proteins of different microbial strains.

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Section: Discussionmentioning

confidence: 99%

In silico screening of JAK-STAT modulators from the antiviral plants of Indian traditional system of medicine with the potential to inhibit 2019 novel coronavirus

Khanal

Duyu

Patil

et al. 2020

Preprint

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“…CD4 + Trm cells typically gather in lymphoid tissue, and they interact with antigen-presenting cells upon re-encounter with pathogens. However, recent investigations have revealed a significant disparity between the numbers of CD4 + and CD8 + T cells within the T-cell population residing in the skin ( 53 ). CD4 + T cells predominantly populate the dermal and epidermal compartments in humans, whereas in mouse skin, CD4 + T cells are primarily concentrated in the dermis ( 54 ).…”

Section: Phenotype and Localization Of Cutaneous Trm Cellsmentioning

confidence: 99%

“…In vitro , TGF-β upregulated the expression of CD103, and TNF-α, IL-33 and IFN-γ upregulated the expression of CD69 ( Figure 1 ). These cytokines and surface markers affect cutaneous CD4 + Trm cell tissue retention more than antigen recognition ( 53 , 60 ). CD4 + Trm cells can supersede innate immunity upon re-exposure to antigens and exert a direct effector effect.…”

Section: Phenotype and Localization Of Cutaneous Trm Cellsmentioning

confidence: 99%

Heterogeneity and plasticity of tissue-resident memory T cells in skin diseases and homeostasis: a review

Liu,

Wang,

2024

Front. Immunol.

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Skin tissue-resident memory T (Trm) cells are produced by antigenic stimulation and remain in the skin for a long time without entering the peripheral circulation. In the healthy state Trm cells can play a patrolling and surveillance role, but in the disease state Trm cells differentiate into various phenotypes associated with different diseases, exhibit different localizations, and consequently have local protective or pathogenic roles, such as disease recurrence in vitiligo and maintenance of immune homeostasis in melanoma. The most common surface marker of Trm cells is CD69/CD103. However, the plasticity of tissue-resident memory T cells after colonization remains somewhat uncertain. This ambiguity is largely due to the variation in the functionality and ultimate destination of Trm cells produced from memory cells differentiated from diverse precursors. Notably, the presence of Trm cells is not stationary across numerous non-lymphoid tissues, most notably in the skin. These cells may reenter the blood and distant tissue sites during the recall response, revealing the recycling and migration potential of the Trm cell progeny. This review focuses on the origin and function of skin Trm cells, and provides new insights into the role of skin Trm cells in the treatment of autoimmune skin diseases, infectious skin diseases, and tumors.

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“…Hence, modulation of these pathways' may contribute to the immune system's homeostatic regulation and reduce cell apoptosis and necrosis. Other pathways involving T-helper cells, cytokine, and chemokine signallers are also closely associated in enhancing the immune system that may contribute towards up-/down-regulation of the immune system during corona infection (Padovan 2017;Simon 2011;Jang et al 2005).…”

Section: Number Of Hydrogen Bondsmentioning

confidence: 99%

Screening of JAK-STAT modulators from the antiviral plants of Indian traditional system of medicine with the potential to inhibit 2019 novel coronavirus using network pharmacology

et al. 2021

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The majority of the bioactives under investigation were predicted to target TNF receptor-associated factor 5 in the Janus kinase/signal transducers and activators of the transcription pathway. Similarly, druglikeness prediction identified vitexilactone to possess the highest druglikeness score, i.e., 0.88. Furthermore, proteins targeted in the Janus kinase/signal transducers and activators of transcription pathway were also predicted to regulate multiple pathways, i.e., ErbB, AGE-RAGE, NF-kappa B, Measles, insulin, mTOR, chemokine, Ras, and pathways associated with infectious and non-infectious pathogenesis, where the immune system is compromised. Similarly, the docking study identified sesaminol 2-O-β-D-gentiobioside to possess the highest binding affinity with 3CL pro , PL pro , and spike proteins. Furthermore, phylogeny comparison identified the common protein domains with other stains of microbes like murine hepatitis virus strain A59, avian infectious bronchitis virus, and porcine epidemic diarrhea virus CV777.

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Modulation of CD4+ T Helper Cell Memory Responses in the Human Skin

Cited by 6 publications

References 143 publications

In silico screening of JAK-STAT modulators from the antiviral plants of Indian traditional system of medicine with the potential to inhibit 2019 novel coronavirus

In silico screening of JAK-STAT modulators from the antiviral plants of Indian traditional system of medicine with the potential to inhibit 2019 novel coronavirus

Heterogeneity and plasticity of tissue-resident memory T cells in skin diseases and homeostasis: a review

Screening of JAK-STAT modulators from the antiviral plants of Indian traditional system of medicine with the potential to inhibit 2019 novel coronavirus using network pharmacology

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