Attenuation of Excess TNF-α Release in Crohn’s Disease by Silencing of iRHOMs 1/2 and the Restoration of TGF-β Mediated Immunosuppression Through Modulation of TACE Trafficking

Louis, Taylor J.; Qasem, Ahmad; Naser, Saleh A.

doi:10.3389/fimmu.2022.887830

Cited by 6 publications

(8 citation statements)

References 42 publications

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“…In the context of chronic or acute inflammation due to injury or infection, cells in the affected tissue produce elevated and high levels of TNF-α cytokine, triggering the production of other inflammatory cytokines, thereby intensifying the inflammatory response. ,, Inhibition of TNF-α has been shown to restore immunosuppressive capabilities, reduce the release of other cytokines, such as IL-1β and IL-6, and attenuate inflammatory damage in IBD. ,, Thus, we further validated gene silencing by evaluating secreted cytokine levels, revealing significant downregulations of TNF-α and its downstream effectors, IL-1β and IL-6 (as shown in Figure B-D), with smGO exhibiting the most pronounced reduction, while bmGO-mediated transfection had no effects compared to the controls. Similar downregulation of TNF-α (4-fold) and IL-6 (3-fold) cytokines has been reported for LPS-induced mouse macrophages upon transfection with TNF-α_siRNA .…”

Section: Resultsmentioning

confidence: 91%

Attenuation of Chronic Inflammation in Intestinal Organoids with Graphene Oxide-Mediated Tumor Necrosis Factor-α_Small Interfering RNA Delivery

Sakib,

Zou

2024

Langmuir

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Inflammatory bowel disease (IBD) is a chronic inflammatory disease of the gastrointestinal tract with a complex and multifactorial etiology, making it challenging to treat. While recent advances in immunomodulatory biologics, such as antitumor necrosis factor-α (TNFα) antibodies, have shown moderate success, systemic administration of antibody therapeutics may lead to several adverse effects, including the risk of autoimmune disorders due to systemic cytokine depletion. Transient RNA interference using exogenous short interfering RNA (siRNA) to regulate target gene expression at the transcript level offers an alternative to systemic immunomodulation. However, siRNAs are susceptible to premature degradation and have poor cellular uptake. Graphene oxide (GO) nanoparticles have been shown to be effective nanocarriers for biologics due to their reduced cytotoxicity and enhanced bioavailability. In this study, we evaluate the therapeutic efficacy of GO mediated TNF-α_siRNA using in vitro models of chronic inflammation generated by treating murine small intestines (enteroids) and large intestines (colonoids) with inflammatory agents IL-1β, TNF-α, and LPS. The organotypic mouse enteroids and colonoids developed an inflammatory phenotype similar to that of IBD, characterized by impaired epithelial homeostasis and an increased production of inflammatory cytokines such as TNF-α, IL-1β, and IL-6. We assessed siRNA delivery to these inflamed organoids using three different GO formulations. Out of the three, small-sized GO with polymer and dendrimer modifications (smGO) demonstrated the highest transfection efficiency, which led to the downregulation of inflammatory cytokines, indicating an attenuation of the inflammatory phenotype. Moreover, the transfection efficiency and inflammation-ameliorating effects could be further enhanced by increasing the TNF-α_siRNA/smGO ratio from 1:1 to 3:1. Overall, the results of this study demonstrate that ex vivo organoids with disease-specific phenotypes are invaluable models for assessing the therapeutic potential of nanocarrier-mediated drug and biologic delivery systems.

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Section: Resultsmentioning

confidence: 91%

Attenuation of Chronic Inflammation in Intestinal Organoids with Graphene Oxide-Mediated Tumor Necrosis Factor-α_Small Interfering RNA Delivery

Sakib,

Zou

2024

Langmuir

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“…We prepared the knockdown transfection mix as described earlier by Vaccaro et al, 2022 [4], and Louis et al, 2022 [22]. Briefly, 5 nmol of Silencer™ pre-designed siRNA (siRNA ID: 4392420) specific to TLR2 was diluted in 50 µL nuclease-free water.…”

Section: Knockdown Of Tlr2 By Sirna Transfectionmentioning

confidence: 99%

“…Caco-2 monolayers were grown at a density of 5 × 10 5 cells/2 mL in Falcon 8-well chambered cell culture slides (ThermoFisher, Waltham, MA, USA) as described earlier [22]. DHE fluorescence staining was performed on the monolayers following 24 h of treatment with supernatant from MAP-infected THP-1 macrophages.…”

Section: Dhe Fluorescence Staining Assay For Caco-2 Monolayersmentioning

confidence: 99%

“…Slides were examined under an Amscope IN480TC-FL-MF603 fluorescence microscope, where blue staining represents nuclei and red indicates oxidative stress. Images were captured on 100× magnification power and analysis was conducted by measuring the average integrated density using NIH Image J 1.39o software as described previously [22]. Merged images of DAPI and DHE stains were generated by the same software.…”

Section: Dhe Fluorescence Staining Assay For Caco-2 Monolayersmentioning

confidence: 99%

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Mycobacterium avium paratuberculosis Infection Suppresses Vitamin D Activation and Cathelicidin Production in Macrophages through Modulation of the TLR2-Dependent p38/MAPK-CYP27B1-VDR-CAMP Axis

Talafha,

Qasem,

Naser

2024

Nutrients

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Background: Vitamin D plays a vital role in modulating both innate and adaptive immune systems. Therefore, vitamin D deficiency has been associated with higher levels of autoimmune response and increased susceptibility to infections. CYP27B1 encodes a member of the cytochrome P450 superfamily of enzymes. It is instrumental in the conversion of circulating vitamin D (calcifediol) to active vitamin D (calcitriol). This is a crucial step for macrophages to express Cathelicidin Anti-microbial Peptide (CAMP), an anti-bacterial factor released during the immune response. Our recent study indicated that a Crohn’s disease (CD)-associated pathogen known as Mycobacterium avium paratuberculosis (MAP) decreases vitamin D activation in macrophages, thereby impeding cathelicidin production and MAP infection clearance. The mechanism by which MAP infection exerts these effects on the vitamin D metabolic axis remains elusive. Methods: We used two cell culture models of THP-1 macrophages and Caco-2 monolayers to establish the effects of MAP infection on the vitamin D metabolic axis. We also tested the effects of Calcifediol, Calcitriol, and SB203580 treatments on the relative expression of the vitamin D metabolic genes, oxidative stress biomarkers, and inflammatory cytokines profile. Results: In this study, we found that MAP infection interferes with vitamin D activation inside THP-1 macrophages by reducing levels of CYP27B1 and vitamin D receptor (VDR) gene expression via interaction with the TLR2-dependent p38/MAPK pathway. MAP infection exerts its effects in a time-dependent manner, with the maximal inhibition observed at 24 h post-infection. We also demonstrated the necessity to have toll-like receptor 2 (TLR2) for MAP infection to influence CYP27B1 and CAMP expression, as TLR2 gene knockdown resulted in an average increase of 7.78 ± 0.88 and 13.90 ± 3.5 folds in their expression, respectively. MAP infection also clearly decreased the levels of p38 phosphorylation and showed dependency on the p38/MAPK pathway to influence the expression of CYP27B1, VDR, and CAMP which was evident by the average fold increase of 1.93 ± 0.28, 1.86 ± 0.27, and 6.34 ± 0.51 in their expression, respectively, following p38 antagonism. Finally, we showed that calcitriol treatment and p38/MAPK blockade reduce cellular oxidative stress and inflammatory markers in Caco-2 monolayers following macrophage-mediated MAP infection. Conclusions: This study characterized the primary mechanism by which MAP infection leads to diminished levels of active vitamin D and cathelicidin in CD patients, which may explain the exacerbated vitamin D deficiency state in these cases.

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“…TACE is also involved in the shedding of many inflammatory cytokines and their receptors including IL-6R, which mediates the trans-signaling on gp130-expressing cells (51). TACE membrane trafficking increases in macrophages during Mycobacterium avium paratuberculosis (MAP) infection and in IBD, which results in an upregulation of proinflammatory cytokine release (51,52). iRhom1 and iRhom2 are to a large extent redundant and must be abolished together to achieve an effect on TACE membrane trafficking (51).…”

Section: Rhomboid Proteases 1 Andmentioning

confidence: 99%

The dual role of interleukin-6 in Crohn’s disease pathophysiology

Alhendi,

Naser

2023

Front. Immunol.

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Interleukin-6 (IL-6) is a key mediator cytokine of the immune response as well as a regulator of many physiological and pathological processes. In Crohn’s disease (CD), cytokine imbalance rules the intestinal microenvironment and leads to chronic inflammation of the gut. Pro-inflammatory cytokines are generally upregulated in inflammatory bowel disease (IBD) including TNFα and IL-6. Consequently, drugs that target these cytokines have been long sought and approved. Despite the short-term success in treating CD patients with anti-TNFα, many patients stopped responding to treatment, which made IL-6 an alternative target to alleviate inflammation in these patients. IL-6 has long been approached as part of the therapeutic strategies to treat CD and other inflammatory disorders. Clinical trials of CD patients have targeted IL-6 signaling in different mechanisms: blocking IL-6, neutralizing IL-6 receptor (IL-6R), or trapping the soluble IL-6/IL-6R complex. These trials have faced challenges and side effects in patients with gastrointestinal perforations and ulcers, for example, all of which highlight the dual role of IL-6 during intestinal inflammation and the need for this cytokine for intestinal tissue integrity. IL-6 is involved in a complex of upstream regulators and downstream signaling cascades and maintaining a physiological level of IL-6 in the blood and in the intestine is key for achieving health and homeostasis. In this review, we describe IL-6 biology and signaling and its involvement in intestinal health and inflammation. We also discuss the current strategies for targeting IL-6 pathways in CD patients, as well as molecular regulators representing potential therapeutic targets for IL-6 attenuation.

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Attenuation of Excess TNF-α Release in Crohn’s Disease by Silencing of iRHOMs 1/2 and the Restoration of TGF-β Mediated Immunosuppression Through Modulation of TACE Trafficking

Cited by 6 publications

References 42 publications

Attenuation of Chronic Inflammation in Intestinal Organoids with Graphene Oxide-Mediated Tumor Necrosis Factor-α_Small Interfering RNA Delivery

Attenuation of Chronic Inflammation in Intestinal Organoids with Graphene Oxide-Mediated Tumor Necrosis Factor-α_Small Interfering RNA Delivery

Mycobacterium avium paratuberculosis Infection Suppresses Vitamin D Activation and Cathelicidin Production in Macrophages through Modulation of the TLR2-Dependent p38/MAPK-CYP27B1-VDR-CAMP Axis

The dual role of interleukin-6 in Crohn’s disease pathophysiology

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