Your search keyword '"trained immunity"' showing total 2,217 results

1. BCG as an Innovative Option for HCC Treatment: Repurposing and Mechanistic Insights.

Author

Vaziri, Farzam, Setayesh, Tahereh, Hu, Ying, Ravindran, Resmi, Wei, Dongguang, and Wan, Yu-Jui

Subjects

bacterial immunotherapy, fibrosis, interferon, liver, trained immunity, Male, Mice, Animals, Female, Carcinoma, Hepatocellular, BCG Vaccine, Proto-Oncogene Proteins c-akt, Liver Neoplasms, Mycobacterium bovis

Abstract

This study investigates Bacillus Calmette-Guérin (BCG) as a potential treatment for hepatocellular carcinoma (HCC), a condition often associated with unfavorable treatment outcomes. Exploiting BCGs recognized immune-boosting properties, preclinical trials are conducted using HCC mice, with a single subcutaneous dose of BCG administered post-tumor formation. Results indicate that BCG treatment effectively diminishes tumor burden and extends survival in both male and female HCC mice. Positive influences on hepatic fibrosis and metabolism are observed, leading to a reduction in lipid levels. Spatial analysis underscores BCGs tumor-specific effects, inducing the enrichment of metabolic pathways and inhibiting various cancer-related pathways. Furthermore, BCG promotes immune cell infiltration, including CD4+, CD8+ T cells, and M1 macrophages, in both v-akt murine thymoma viral oncogene homolog 1(AKT)/neutoblastoma RAS viral oncogene homolog (RAS) and β-catenin positive HCC models. Interestingly, blocking T cells, trained immunity, and Interferon-γ (IFN-γ) function reverses BCGs anti-HCC effects. In conclusion, BCG emerges as a promising treatment option for HCC, characterized by a favorable safety profile and efficacy in inhibiting fibrosis, improving metabolism, and engaging both trained immunity and T cells in therapeutic mechanisms.

Published

2024

2. Oxylipin transport by lipoprotein particles and its functional implications for cardiometabolic and neurological disorders

Author

Liang, Nuanyi, Harsch, Brian A, Zhou, Sitong, Borkowska, Alison, Shearer, Gregory C, Kaddurah-Daouk, Rima, Newman, John W, and Borkowski, Kamil

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Neurosciences, Brain Disorders, 2.1 Biological and endogenous factors, Neurological, Humans, Oxylipins, Apolipoprotein E4, Lipoproteins, Nervous System Diseases, Cardiovascular Diseases, Inflammation, Cardiometabolic disorders, Neurological disorders, Neurodegenerative disorders, Alzheimer's disease, COVID-19, Immune memory, Trained immunity, Medical Biochemistry and Metabolomics, Nutrition and Dietetics, Biochemistry & Molecular Biology, Biochemistry and cell biology, Medical biochemistry and metabolomics

Abstract

Lipoprotein metabolism is critical to inflammation. While the periphery and central nervous system (CNS) have separate yet connected lipoprotein systems, impaired lipoprotein metabolism is implicated in both cardiometabolic and neurological disorders. Despite the substantial investigation into the composition, structure and function of lipoproteins, the lipoprotein oxylipin profiles, their influence on lipoprotein functions, and their potential biological implications are unclear. Lipoproteins carry most of the circulating oxylipins. Importantly, lipoprotein-mediated oxylipin transport allows for endocrine signaling by these lipid mediators, long considered to have only autocrine and paracrine functions. Alterations in plasma lipoprotein oxylipin composition can directly impact inflammatory responses of lipoprotein metabolizing cells. Similar investigations of CNS lipoprotein oxylipins are non-existent to date. However, as APOE4 is associated with Alzheimer's disease-related microglia dysfunction and oxylipin dysregulation, ApoE4-dependent lipoprotein oxylipin modulation in neurological pathologies is suggested. Such investigations are crucial to bridge knowledge gaps linking oxylipin- and lipoprotein-related disorders in both periphery and CNS. Here, after providing a summary of existent literatures on lipoprotein oxylipin analysis methods, we emphasize the importance of lipoproteins in oxylipin transport and argue that understanding the compartmentalization and distribution of lipoprotein oxylipins may fundamentally alter our consideration of the roles of lipoprotein in cardiometabolic and neurological disorders.

Published

2024

3. Epigenetic training of human bronchial epithelium cells by repeated rhinovirus infections.

Author

Risha, Marua Abu, Reddy, Karosham D., Nemani, Sai Sneha Priya, Jakwerth, Constanze, Schmidt‐Weber, Carsten, Bahmer, Thomas, Hansen, Gesine, Mutius, Erika, Rabe, Klaus F., Dittrich, Anna‐Maria, Grychtol, Ruth, Maison, Nicole, Schaub, Bianca, Kopp, Matthias V., Brinkmann, Folke, Meiners, Silke, Jappe, Uta, and Weckmann, Markus

Abstract

Background Methods Results Conclusions Humans are subjected to various environmental stressors (bacteria, viruses, pollution) throughout life. As such, an inherent relationship exists between the effect of these exposures with age. The impact of these environmental stressors can manifest through DNA methylation (DNAm). However, whether these epigenetic effects selectively target genes, pathways, and biological regulatory mechanisms remains unclear. Due to the frequency of human rhinovirus (HRV) infections throughout life (particularly in early development), we propose the use of HRV under controlled conditions can model the effect of multiple exposures to environmental stressors.We generated a prediction model by combining transcriptome and DNAm datasets from human epithelial cells after repeated HRV infections. We applied a novel experimental statistical design and method to systematically explore the multifaceted experimental space (number of infections, multiplicity of infections and duration). Our model included 35 samples, each characterized by the three parameters defining their infection status.Trainable genes were defined by a consistent linear directionality in DNAm and gene expression changes with successive infections. We identified 77 trainable genes which could be further explored in future studies. The identified methylation sites were tracked within a pediatric cohort to determine the relative changes in candidate‐trained sites with disease status and age.Repeated viral infections induce an immune training response in bronchial epithelial cells. Training‐sensitive DNAm sites indicate alternate divergent associations in asthma compared to healthy individuals. Our novel model presents a robust tool for identifying trainable genes, providing a foundation for future studies. [ABSTRACT FROM AUTHOR]

Published

2024

4. Trained innate immunity: Concept, nomenclature, and future perspectives.

Author

Netea, Mihai G. and Joosten, Leo A.B.

Abstract

During the past decade, compelling evidence has accumulated demonstrating that innate immune cells can mount adaptive characteristics, leading to long-term changes in their function. This de facto innate immune memory has been termed trained immunity. Trained immunity, which is mediated through extensive metabolic rewiring and epigenetic modifications, has important effects in human diseases. Although the upregulation of trained immunity by certain vaccines provides heterologous protection against infections, the inappropriate activation of trained immunity by endogenous stimuli contributes to the pathogenesis of inflammatory and neurodegenerative disorders. Development of vaccines that can induce both classical adaptive immunity and trained immunity may lead to a new generation of vaccines with increased efficacy. Activation of trained immunity can also lead to novel strategies for the treatment of cancer, whereas modulation of trained immunity can provide new approaches to the treatment of inflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2024

5. Central trained immunity and its impact on chronic inflammatory and autoimmune diseases.

Author

Hajishengallis, George and Chavakis, Triantafyllos

Published

2024

6. Impact of cooperative or competitive dynamics between the yeast Saccharomyces cerevisiae and lactobacilli on the immune response of the host.

Author

Nenciarini, Stefano, Rivero, Damariz, Ciccione, Alessia, Amoriello, Roberta, Cerasuolo, Benedetta, Pallecchi, Marco, Bartolucci, Gian Luca, Ballerini, Clara, and Cavalieri, Duccio

Subjects

SHORT-chain fatty acids, DIETARY patterns, IMMUNOREGULATION, COOPETITION, YEAST culture

Abstract

Fungi and bacteria can be found coexisting in a wide variety of environments. The combination of their physical and molecular interactions can result in a broad range of outcomes for each partner, from competition to cooperative relationships. Most of these interactions can also be found in the human gastrointestinal tract. The gut microbiota is essential for humans, helping the assimilation of food components as well as the prevention of pathogen invasions through host immune system modulation and the production of beneficial metabolites such as short-chain fatty acids (SCFAs). Several factors, including changes in diet habits due to the progressive Westernization of the lifestyle, are linked to the onset of dysbiosis statuses that impair the correct balance of the gut environment. It is therefore crucial to explore the interactions between commensal and diet-derived microorganisms and their influence on host health. Investigating these interactions through co-cultures between humanand fermented food-derived lactobacilli and yeasts led us to understand how the strains' growth yield and their metabolic products rely on the nature and concentration of the species involved, producing either cooperative or competitive dynamics. Moreover, single cultures of yeasts and lactobacilli proved to be ideal candidates for developing immune-enhancing products, given their ability to induce trained immunity in blood-derived human monocytes in vitro. Conversely, co-cultures as well as mixtures of yeasts and lactobacilli have been shown to induce an anti-inflammatory response on the same immune cells in terms of cytokine profiles and activation surface markers, opening new possibilities in the design of probiotic and dietary therapies. [ABSTRACT FROM AUTHOR]

Published

2024

7. Genetic and epigenetic dysregulation of innate immune mechanisms in autoinflammatory diseases.

Author

Merlo Pich, Laura M., Ziogas, Athanasios, and Netea, Mihai G.

Subjects

*AUTOINFLAMMATORY diseases, *IMMUNE response, *IMMUNE system, *INTERFERONS, *INFLAMMASOMES

Abstract

Dysregulation and hyperactivation of innate immune responses can lead to the onset of systemic autoinflammatory diseases. Monogenic autoinflammatory diseases are caused by inborn genetic errors and based on molecular mechanisms at play, can be divided into inflammasomopathies, interferonopathies, relopathies, protein misfolding, and endogenous antagonist deficiencies. On the other hand, more common autoinflammatory diseases are multifactorial, with both genetic and non‐genetic factors playing an important role. During the last decade, long‐term memory characteristics of innate immune responses have been described (also called trained immunity) that in physiological conditions provide enhanced host protection from pathogenic re‐infection. However, if dysregulated, induction of trained immunity can become maladaptive, perpetuating chronic inflammatory activation. Here, we describe the mechanisms of genetic and epigenetic dysregulation of the innate immune system and maladaptive trained immunity that leads to the onset and perpetuation of the most common and recently described systemic autoinflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2024

8. Trained immunity of intestinal tuft cells during infancy enhances host defense against enteroviral infections in mice.

Author

Chen, Deyan, Wu, Jing, Zhang, Fang, Lyu, Ruining, You, Qiao, Qian, Yajie, Cai, Yurong, Tian, Xiaoyan, Tao, Hongji, He, Yating, Nawaz, Waqas, and Wu, Zhiwei

Abstract

Innate immune cells have been acknowledged as trainable in recent years. While intestinal tuft cells are recognized for their crucial roles in the host defense against intestinal pathogens, there remains uncertainty regarding their trainability. Enterovirus 71 (EV71), a prevalent enterovirus that primarily infects children but rarely infects adults. At present, there is a significant expansion of intestinal tuft cells in the EV71-infected mouse model, which is associated with EV71-induced interleukin-25 (IL-25) production. Further, we found that IL-25 pre-treatment at 2 weeks old mouse enabled tuft cells to acquire immune memory. This was evidenced by the rapid expansion and stronger response of IL-25-trained tuft cells in response to EV71 infection at 6 weeks old, surpassing the reactivity of naïve tuft cells in mice without IL-25-trained progress. Interestingly, IL-25-trained intestinal tuft cells exhibit anti-enteroviral effect via producing a higher level of IL-25. Mechanically, IL-25 treatment upregulates spermidine/spermine acetyl-transferase enzyme (SAT1) expression, mediates intracellular polyamine deficiency, further inhibits enterovirus replication. In summary, tuft cells can be trained by IL-25, which supports faster and higher level IL-25 production in response to EV71 infection and further exhibits anti-enteroviral effect via SAT1-mediated intracellular polyamine deficiency. Given that IL-25 can be induced by multiple gut microbes during human growth and development, including shifts in gut flora abundance, which may partially explain the different susceptibility to enteroviral infections between adults and children. Synopsis: Our present study implies that intestinal tuft cells can be trained by IL-25 and it may explain the different susceptibility in enteroviral infections between adults and children from an immune training perspective. EV71 mediated tuft cell expansion via promoting IL-25 production in EV71-infected mouse model. IL-25-trained tuft cells were quickly increased and displayed a stronger IL-25-SAT1 axis response and exhibited a more powerful antiviral effect as compared to naïve tuft cells. IL-25 supported the host defense via upregulating SAT1 expression, together with a lower polyamine level, which affected a broad enteroviral replication. Our present study implies that intestinal tuft cells can be trained by IL-25 and it may explain the different susceptibility in enteroviral infections between adults and children from an immune training perspective. [ABSTRACT FROM AUTHOR]

Published

2024

9. Inflammatory Trajectory of Type 2 Diabetes: Novel Opportunities for Early and Late Treatment.

Author

Pellegrini, Valeria, La Grotta, Rosalba, Carreras, Francesca, Giuliani, Angelica, Sabbatinelli, Jacopo, Olivieri, Fabiola, Berra, Cesare Celeste, Ceriello, Antonio, and Prattichizzo, Francesco

Subjects

*TYPE 2 diabetes, *LDL cholesterol, *SEDENTARY behavior, *INSULIN resistance, *KIDNEY physiology, *IMMUNOSENESCENCE

Abstract

Low-grade inflammation (LGI) represents a key driver of type 2 diabetes (T2D) and its associated cardiovascular diseases (CVDs). Indeed, inflammatory markers such as hs-CRP and IL-6 predict the development of T2D and its complications, suggesting that LGI already increases before T2D diagnosis and remains elevated even after treatment. Overnutrition, unhealthy diets, physical inactivity, obesity, and aging are all recognized triggers of LGI, promoting insulin resistance and sustaining the pathogenesis of T2D. Once developed, and even before frank appearance, people with T2D undergo a pathological metabolic remodeling, with an alteration of multiple CVD risk factors, i.e., glycemia, lipids, blood pressure, and renal function. In turn, such variables foster a range of inflammatory pathways and mechanisms, e.g., immune cell stimulation, the accrual of senescent cells, long-lasting epigenetic changes, and trained immunity, which are held to chronically fuel LGI at the systemic and tissue levels. Targeting of CVD risk factors partially ameliorates LGI. However, some long-lasting inflammatory pathways are unaffected by common therapies, and LGI burden is still increased in many T2D patients, a phenomenon possibly underlying the residual inflammatory risk (i.e., having hs-CRP > 2 mg/dL despite optimal LDL cholesterol control). On the other hand, selected disease-modifying drugs, e.g., GLP-1RA, seem to also act on the pathogenesis of T2D, curbing the inflammatory trajectory of the disease and possibly preventing it if introduced early. In addition, selected trials demonstrated the potential of canonical anti-inflammatory therapies in reducing the rate of CVDs in patients with this condition or at high risk for it, many of whom had T2D. Since colchicine, an inhibitor of immune cell activation, is now approved for the prevention of CVDs, it might be worth exploring a possible therapeutic paradigm to identify subjects with T2D and an increased LGI burden to treat them with this drug. Upcoming studies will reveal whether disease-modifying drugs reverse early T2D by suppressing sources of LGI and whether colchicine has a broad benefit in people with this condition. [ABSTRACT FROM AUTHOR]

Published

2024

10. Factors affecting neutrophil functions during sepsis: human microbiome and epigenetics.

Author

Ma, Yina, Zhao, Yu, and Zhang, Xin

Subjects

LEUCOCYTES, HUMAN microbiota, CELL-free DNA, BLOOD circulation, NATURAL immunity

Abstract

Sepsis is a severe disease that occurs when the body's immune system reacts excessively to infection. The body's response, which includes an intense antibacterial reaction, can damage its tissues and organs. Neutrophils are the major components of white blood cells in circulation, play a vital role in innate immunity while fighting against infections, and are considered a feature determining sepsis classification. There is a plethora of basic research detailing neutrophil functioning, among which, the study of neutrophil extracellular traps is providing novel insights into mechanisms and treatments of sepsis. This review explores their functions, dysfunctions, and influences in the context of sepsis. The interplay between neutrophils and the human microbiome and the impact of DNA methylation on neutrophil function in sepsis are crucial areas of study. The interaction between neutrophils and the human microbiome is complex, particularly in the context of sepsis, where dysbiosis may occur. We highlight the importance of deciphering neutrophils' functional alterations and their epigenetic features in sepsis because it is critical for defining sepsis endotypes and opening up the possibility for novel diagnostic methods and therapy. Specifically, epigenetic signatures are pivotal since they will provide a novel implication for a sepsis diagnostic method when used in combination with the cell-free DNA. Research is exploring how specific patterns of DNA methylation in neutrophils, detectable in cell-free DNA, could serve as biomarkers for the early detection of sepsis. [ABSTRACT FROM AUTHOR]

Published

2024

11. Host heterogeneity in humoral bactericidal activity can be complement independent.

Author

Ryuichiro Abe, Ram-Mohan, Nikhil, Zudock, Elizabeth Jordan, Lewis, Shawna, Carroll, Karen C., and Yang, Samuel

Subjects

INDUCTIVELY coupled plasma mass spectrometry, PEARSON correlation (Statistics), COMPLEMENT inhibition, COMPLEMENT activation, NATURAL immunity, IMMUNOGLOBULIN M, SAPONINS

Abstract

Background: Humoral bactericidal activity was first recognized nearly a century ago. However, the extent of inter-individual heterogeneity and the mechanisms underlying such heterogeneity beyond antibody or complement systems have not been well studied. Methods: The plasma bactericidal activity of five healthy volunteers were tested against 30 strains of Gram-negative uropathogens, Klebsiella pneumoniae and Escherichia coli, associated with bloodstream infections. IgG and IgM titers specific to K. pneumoniae strains KP13883 and KPB1 were measured by ELISA, and complement inhibitor was used to measure the contribution of complementinduced killing. Furthermore, MALDI-TOF mass spectrometry was conducted to determine the metabolomic components of plasma with bactericidal properties in 25 healthy individuals using Bayesian inference of Pearson correlation between peak intensity and colony counts of surviving bacteria. Results: Plasma bactericidal activity varied widely between individuals against various bacterial strains. While individual plasma with higher IgM titers specific to K. pneumoniae strain KP13883 showed more efficient killing of the strain, both IgM and IgG titers for K. pneumoniae strain KPB1 did not correlate well with the killing activity. Complement inhibition assays elucidated that the complement-mediated killing was not responsible for the inter-individual heterogeneity in either isolate. Subsequently, using MALDI-TOF mass spectrometry on plasmas of 25 healthy individuals, we identified several small molecules including gangliosides, pediocins, or saponins as candidates that showed negative correlation between peak intensities and colony forming units of the test bacteria. Conclusion: This is the first study to demonstrate the inter-individual heterogeneity of constitutive innate humoral bactericidal function quantitatively and that the heterogeneity can be independent of antibody or the complement system. [ABSTRACT FROM AUTHOR]

Published

2024

12. New progress in pediatric allergic rhinitis.

Author

Miao Cheng, Qianqian Dai, Zhi Liu, Yulin Wang, and Cuiyun Zhou

Subjects

ALLERGY desensitization, ALLERGIC rhinitis, QUALITY of life, CHILDREN'S health, ALLERGENS

Abstract

The prevalence of allergic rhinitis (AR) in children is steadily increasing, and its onset is closely associated with genetic factors, living environment, and exposure to allergens. In recent years, an increasing number of diagnostic methods have been employed to assist in diagnosing AR. In addition to pharmaceutical treatments, personalized approaches such as environmental control and allergen-specific immunotherapy are gradually gaining popularity. In this article, we reviewed recent research on the etiology, diagnostic classification, treatment methods, and health management of AR in children. These insights will benefit the implementation of personalized diagnosis and treatment for children with AR, promoting health management strategies that improve symptoms and quality of life. [ABSTRACT FROM AUTHOR]

Published

2024

13. Vaccine induced mucosal and systemic memory NK/ILCs elicit decreased risk of SIV/SHIV acquisition.

Author

Rahman, Mohammad Arif, Silva de Castro, Isabela, Schifanella, Luca, Bissa, Massimiliano, and Franchini, Genoveffa

Subjects

KILLER cells, AIDS vaccines, HIV infections, VIRAL load, GRANZYMES

Abstract

SIV and HIV-based envelope V1-deleted (ΔV1) vaccines, delivered systemically by the DNA/ALVAC/gp120 platform, decrease the risk of mucosal SIV or SHIV acquisition more effectively than V1-replete vaccines. Here we investigated the induction of mucosal and systemic memory-like NK cells as well as antigenreactive ILC response by DNA/ALVAC/gp120-based vaccination and their role against SIV/SHIV infection. DV1 HIV vaccination elicited a higher level of mucosal TNF-a+ and CD107+ memory-like NK cells than V1-replete vaccination, suggesting immunogen dependence. Mucosal memory-like NK cells, systemic granzyme B+ memory NK cells, and vaccine-induced mucosal envelope antigenreactive IL-17+ NKp44+ ILCs, IL-17+ ILC3s, and IL-13+ ILC2 subsets were linked to a lower risk of virus acquisition. Additionally, mucosal memory-like NK cells and mucosal env-reactive IFN-g+ ILC1s and env-reactive IL-13+ ILC2 subsets correlated with viral load control. We further observed a positive correlation between post-vaccination systemic and mucosal memory-like NK cells, suggesting vaccination enhances the presence of these cells in both compartments. Mucosal and systemic memory-like NK cells positively correlated with V2-specific ADCC responses, a reproducible correlate of reduced risk of SIV/HIV infection. In contrast, an increased risk was associated with the level of mucosal PMA/Ionomycin-induced IFN-γ+ and CD107+ NKG2ANKp44- ILCs. Plasma proteomic analyses demonstrated that suppression of mucosal memory-like NK cells was linked to the level of CCL-19, LT-α, TNFSF-12, and IL-15, suppression of systemic env-reactive granzyme B+ memory-like NK cells was associated with the level of OLR1, CCL-3, and OSM, and suppression of IL-17+ ILCs immunity was correlated with the level of IL-6 and CXCL-9. In contrast, FLT3 ligand was associated with promotion of protective mucosal env-reactive IL-17+ responses. These findings emphasize the importance of mucosal memory-like NK cell and envelope-reactive ILC responses for protection against mucosal SIV/SHIV acquisition. [ABSTRACT FROM AUTHOR]

Published

2024

14. Candida albicans N-Linked Mannans Potentiate the Induction of Trained Immunity via Dectin-2.

Author

Rosati, Diletta, Pradhan, Arnab, Heck, Julia I P van, Helder, Leonie, Jaeger, Martin, Gow, Neil A R, Joosten, Leo A B, Williams, David L, Brown, Alistair J P, Bruno, Mariolina, and Netea, Mihai G

Subjects

*PATTERN perception receptors, *IMMUNOLOGIC memory, *CANDIDA albicans, *IMMUNE response, *PATHOGENIC fungi

Abstract

The interaction between the Candida albicans cell wall and pattern recognition receptors is crucial for the initiation of host immune responses, which, ultimately, contribute to the clearance of this pathogenic fungus. In the present study, we investigate the ability of C. albicans mannans to modulate immune response and induce innate immune memory (also termed trained immunity). Using mutants of C. albicans that are defective in or lack mannosyl residues, we show that alterations in the mannosylation of the C. albicans cell wall affect the innate cytokine response and strongly reduce the secretion of T-cell–derived cytokines. Subsequently, we demonstrate that the branching of N -linked mannan, but not O -linked mannan, is essential to potentiate the induction of trained immunity, a process mediated by dectin 2. In conclusion, N -linked mannan is needed, in addition to β-glucans, for an effective induction of trained immunity by C. albicans. [ABSTRACT FROM AUTHOR]

Published

2024

15. Early transcriptomic response of innate immune cells to subcutaneous BCG vaccination of mice.

Author

Kondratyeva, Liya, Kuzmich, Alexey, Linge, Irina, Pleshkan, Victor, Rakitina, Olga, Kondratieva, Sofia, Snezhkov, Eugene, Sass, Alexander, and Alekseenko, Irina

Subjects

*BCG vaccines, *NATURAL immunity, *RNA sequencing, *CELL populations, *IMMUNE response

Abstract

Objectives: Current data suggests that Bacille Calmette-Guerin (BCG) vaccination contributes to nonspecific enhancement of resistance to various infections. Thus, BCG vaccination induces both specific immunity against mycobacteria and non-specific "trained immunity" against various pathogens. To understand the fundamental mechanisms of "trained" immunity, studies of transcriptome changes occurring during BCG vaccination in innate immunity cells, as well as in their precursors, are necessary. Furthermore, this data possesses important significance for practical applications associated with the development of recombinant BCG strains aimed to enhance innate immunity against diverse infectious agents. Data description: We performed RNA sequencing of innate immune cells derived from murine bone marrow and spleen three days after subcutaneous BCG vaccination. Using fluorescence-activated cell sorting we obtained three cell populations for each mouse from both control and BCG vaccinated groups: bone marrow monocytes and neutrophils and splenic NK-cells. Then double-indexed cDNA libraries for Illumina sequencing from the collected samples were prepared, the resulting cDNA library mix was subjected to NovaSeq 6000 sequencing. This paper describes the collection of 24 RNA sequencing samples comprising 4 sets of immune cell populations obtained from subcutaneously BCG-vaccinated and control mice [ABSTRACT FROM AUTHOR]

Published

2024

16. Innate immune response in acute critical illness: a narrative review.

Author

Stiel, Laure, Gaudet, Alexandre, Thietart, Sara, Vallet, Hélène, Bastard, Paul, Voiriot, Guillaume, Oualha, Mehdi, Sarton, Benjamine, Kallel, Hatem, Brechot, Nicolas, Kreitmann, Louis, Benghanem, Sarah, Joffre, Jérémie, and Jouan, Youenn

Subjects

*MITOCHONDRIA, *IMMUNOSUPPRESSIVE agents, *CATASTROPHIC illness, *DECISION making, *IMMUNE system, *AGING, *IMMUNOLOGIC receptors, *NATURAL immunity, *INDIVIDUALIZED medicine, *INFLAMMATION, *CRITICAL care medicine, *THROMBOSIS, *PHENOTYPES, *IMMUNOMODULATORS

Abstract

Background: Activation of innate immunity is a first line of host defense during acute critical illness (ACI) that aims to contain injury and avoid tissue damages. Aberrant activation of innate immunity may also participate in the occurrence of organ failures during critical illness. This review aims to provide a narrative overview of recent advances in the field of innate immunity in critical illness, and to consider future potential therapeutic strategies. Main text: Understanding the underlying biological concepts supporting therapeutic strategies modulating immune response is essential in decision-making. We will develop the multiple facets of innate immune response, especially its cellular aspects, and its interaction with other defense mechanisms. We will first describe the pathophysiological mechanisms of initiation of innate immune response and its implication during ACI. We will then develop the amplification of innate immunity mediated by multiple effectors. Our review will mainly focus on myeloid and lymphoid cellular effectors, the major actors involved in innate immune-mediated organ failure. We will third discuss the interaction and integration of innate immune response in a global view of host defense, thus considering interaction with non-immune cells through immunothrombosis, immunometabolism and long-term reprogramming via trained immunity. The last part of this review will focus on the specificities of the immune response in children and the older population. Conclusions: Recent understanding of the innate immune response integrates immunity in a highly dynamic global vision of host response. A better knowledge of the implicated mechanisms and their tissue-compartmentalization allows to characterize the individual immune profile, and one day eventually, to develop individualized bench-to-bedside immunomodulation approaches as an adjuvant resuscitation strategy. [ABSTRACT FROM AUTHOR]

Published

2024

17. Ischemia does not provoke the full immune training repertoire in human cardiac fibroblasts.

Author

Mann, Constantin, van Alst, Carolin, Gorressen, Simone, Nega, Rachel, Dobrev, Dobromir, Grandoch, Maria, and Fender, Anke C.

Subjects

TOLL-like receptor agonists, MYELOID cells, PHOSPHOGLYCERATE kinase, MYOCARDIAL ischemia, HYPOXIA-inducible factors

Abstract

Trained immunity of monocytes, endothelial, and smooth muscle cells augments the cytokine response to secondary stimuli. Immune training is characterized by stabilization of hypoxia-inducible factor (HIF)-1α, mTOR activation, and aerobic glycolysis. Cardiac fibroblast (CF)-myofibroblast transition upon myocardial ischemia/reperfusion (I/R) features epigenetic and metabolic adaptations reminiscent of trained immunity. We assessed the impact of I/R on characteristics of immune training in human CF and mouse myocardium. I/R was simulated in vitro with transient metabolic inhibition. CF primed with simulated I/R or control buffer were 5 days later re-stimulated with Pam3CSK for 24 h. Mice underwent transient left anterior descending artery occlusion or sham operation with reperfusion for up to 5 days. HIF-regulated metabolic targets and cytokines were assessed by qPCR, immunoblot, and ELISA and glucose consumption, lactate release, and lactate dehydrogenase (LDH) by chromogenic assay. Simulated I/R increased HIF-1α stabilization, mTOR phosphorylation, glucose consumption, lactate production, and transcription of PFKB3 and F2RL3, a HIF-regulated target gene, in human CF. PGK1 and LDH mRNAs were suppressed. Intracellular LDH transiently increased after simulated I/R, and extracellular LDH showed sustained elevation. I/R priming increased abundance of pro-caspase-1, auto-cleaved active caspase-1, and the expression and secretion of interleukin (IL)-1β, but did not augment Pam3CSK-stimulated cytokine transcription or secretion. Myocardial I/R in vivo increased abundance of HIF-1 and the precursor and cleaved forms of caspase-1, caspase-11, and caspase-8, but not of LDH-A or phospho-mTOR. I/R partially reproduces features of immune training in human CF, specifically HIF-1α stabilization, aerobic glycolysis, mTOR phosphorylation, and PFKB3 transcription. I/R does not augment PGK1 or LDH expression or the cytokine response to Pam3CSK. Regulation of PAR4 and inflammasome caspases likely occurs independently of an immune training repertoire. Ischemia provokes only part of the immune training repertoire in cardiac fibroblasts. Trained immunity in myeloid and non-myeloid cells is triggered by certain infectious and sterile triggers like β-glucan or oxidized LDL, respectively. Key characteristics of immune training are as follows: stabilization of hypoxia-inducible factor (HIF)-1α, mTOR activation, transcriptional induction of lactate dehydrogenase (LDH), phosphoglycerate kinase (PGK)1 and 6-phosphofructo-2-kinase/fructose-2,6-biphosphatase 3 (PFKFB3), increased glycolysis and lactate production, and enhanced cytokine response to a secondary stimulus such as the toll-like receptor agonist Pam3CSK4. Simulated ischemia/reperfusion (SI/R) reproduces some but not all of these features in human cardiac fibroblasts (CF) as indicated with asterisk (*). [ABSTRACT FROM AUTHOR]

Published

2024

18. Non-Coding RNAs and Innate Immune Responses in Cancer.

Author

Díaz, Carlos Romero, Hernández-Huerta, María Teresa, Mayoral, Laura Pérez-Campos, Villegas, Miriam Emily Avendaño, Zenteno, Edgar, Cruz, Margarito Martínez, Mayoral, Eduardo Pérez-Campos, del Socorro Pina Canseco, María, Andrade, Gabriel Mayoral, Castellanos, Manuel Ángeles, Matías Salvador, José Manuel, Cruz Parada, Eli, Martínez Barras, Alexis, Cruz Fernández, Jaydi Nora, Scott-Algara, Daniel, and Pérez-Campos, Eduardo

Subjects

SMALL interfering RNA, LINCRNA, NON-coding RNA, GENE expression, NATURAL immunity

Abstract

Non-coding RNAs (ncRNAs) and the innate immune system are closely related, acting as defense mechanisms and regulating gene expression and innate immunity. Both are modulators in the initiation, development and progression of cancer. We aimed to review the major types of ncRNAs, including small interfering RNAs (siRNAs), microRNAs (miRNAs), piwi-interacting RNAs (piRNAs), and long non-coding RNAs (lncRNAs), with a focus on cancer, innate immunity, and inflammation. We found that ncRNAs are closely related to innate immunity, epigenetics, chronic inflammation, and cancer and share properties such as inducibility, specificity, memory, and transfer. These similarities and interrelationships suggest that ncRNAs and modulators of trained immunity, together with the control of chronic inflammation, can be combined to develop novel therapeutic approaches for personalized cancer treatment. In conclusion, the close relationship between ncRNAs, the innate immune system, and inflammation highlights their importance in cancer pathways and their potential as targets for novel therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2024

19. Trained immunity of intestinal tuft cells during infancy enhances host defense against enteroviral infections in mice

Author

Deyan Chen, Jing Wu, Fang Zhang, Ruining Lyu, Qiao You, Yajie Qian, Yurong Cai, Xiaoyan Tian, Hongji Tao, Yating He, Waqas Nawaz, and Zhiwei Wu

Subjects

Trained Immunity, Tuft Cells, IL-25, SAT1, Anti-Enteroviral Response, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Innate immune cells have been acknowledged as trainable in recent years. While intestinal tuft cells are recognized for their crucial roles in the host defense against intestinal pathogens, there remains uncertainty regarding their trainability. Enterovirus 71 (EV71), a prevalent enterovirus that primarily infects children but rarely infects adults. At present, there is a significant expansion of intestinal tuft cells in the EV71-infected mouse model, which is associated with EV71-induced interleukin-25 (IL-25) production. Further, we found that IL-25 pre-treatment at 2 weeks old mouse enabled tuft cells to acquire immune memory. This was evidenced by the rapid expansion and stronger response of IL-25-trained tuft cells in response to EV71 infection at 6 weeks old, surpassing the reactivity of naïve tuft cells in mice without IL-25-trained progress. Interestingly, IL-25-trained intestinal tuft cells exhibit anti-enteroviral effect via producing a higher level of IL-25. Mechanically, IL-25 treatment upregulates spermidine/spermine acetyl-transferase enzyme (SAT1) expression, mediates intracellular polyamine deficiency, further inhibits enterovirus replication. In summary, tuft cells can be trained by IL-25, which supports faster and higher level IL-25 production in response to EV71 infection and further exhibits anti-enteroviral effect via SAT1-mediated intracellular polyamine deficiency. Given that IL-25 can be induced by multiple gut microbes during human growth and development, including shifts in gut flora abundance, which may partially explain the different susceptibility to enteroviral infections between adults and children.

Published

2024

20. Early transcriptomic response of innate immune cells to subcutaneous BCG vaccination of mice

Author

Liya Kondratyeva, Alexey Kuzmich, Irina Linge, Victor Pleshkan, Olga Rakitina, Sofia Kondratieva, Eugene Snezhkov, Alexander Sass, and Irina Alekseenko

Subjects

RNA-seq, Transcriptomes, Immune cells, Innate immunity, Trained immunity, BCG, Medicine, Biology (General), QH301-705.5, Science (General), Q1-390

Abstract

Abstract Objectives Current data suggests that Bacille Calmette-Guerin (BCG) vaccination contributes to nonspecific enhancement of resistance to various infections. Thus, BCG vaccination induces both specific immunity against mycobacteria and non-specific “trained immunity” against various pathogens. To understand the fundamental mechanisms of “trained” immunity, studies of transcriptome changes occurring during BCG vaccination in innate immunity cells, as well as in their precursors, are necessary. Furthermore, this data possesses important significance for practical applications associated with the development of recombinant BCG strains aimed to enhance innate immunity against diverse infectious agents. Data description We performed RNA sequencing of innate immune cells derived from murine bone marrow and spleen three days after subcutaneous BCG vaccination. Using fluorescence-activated cell sorting we obtained three cell populations for each mouse from both control and BCG vaccinated groups: bone marrow monocytes and neutrophils and splenic NK-cells. Then double-indexed cDNA libraries for Illumina sequencing from the collected samples were prepared, the resulting cDNA library mix was subjected to NovaSeq 6000 sequencing. This paper describes the collection of 24 RNA sequencing samples comprising 4 sets of immune cell populations obtained from subcutaneously BCG-vaccinated and control mice

Published

2024

21. Innate immune response in acute critical illness: a narrative review

Author

Laure Stiel, Alexandre Gaudet, Sara Thietart, Hélène Vallet, Paul Bastard, Guillaume Voiriot, Mehdi Oualha, Benjamine Sarton, Hatem Kallel, Nicolas Brechot, Louis Kreitmann, Sarah Benghanem, Jérémie Joffre, Youenn Jouan, and la Commission de Recherche Translationnelle de la Société de Réanimation en Langue Française

Subjects

Innate immunity, Immunothrombosis, Immunosenescence, Trained immunity, Acute critical illness, Medical emergencies. Critical care. Intensive care. First aid, RC86-88.9

Abstract

Abstract Background Activation of innate immunity is a first line of host defense during acute critical illness (ACI) that aims to contain injury and avoid tissue damages. Aberrant activation of innate immunity may also participate in the occurrence of organ failures during critical illness. This review aims to provide a narrative overview of recent advances in the field of innate immunity in critical illness, and to consider future potential therapeutic strategies. Main text Understanding the underlying biological concepts supporting therapeutic strategies modulating immune response is essential in decision-making. We will develop the multiple facets of innate immune response, especially its cellular aspects, and its interaction with other defense mechanisms. We will first describe the pathophysiological mechanisms of initiation of innate immune response and its implication during ACI. We will then develop the amplification of innate immunity mediated by multiple effectors. Our review will mainly focus on myeloid and lymphoid cellular effectors, the major actors involved in innate immune-mediated organ failure. We will third discuss the interaction and integration of innate immune response in a global view of host defense, thus considering interaction with non-immune cells through immunothrombosis, immunometabolism and long-term reprogramming via trained immunity. The last part of this review will focus on the specificities of the immune response in children and the older population. Conclusions Recent understanding of the innate immune response integrates immunity in a highly dynamic global vision of host response. A better knowledge of the implicated mechanisms and their tissue-compartmentalization allows to characterize the individual immune profile, and one day eventually, to develop individualized bench-to-bedside immunomodulation approaches as an adjuvant resuscitation strategy.

Published

2024

22. Induction of trained immunity in broiler chickens following delivery of oligodeoxynucleotide containing CpG motifs to protect against Escherichia coli septicemia

Author

Iresha Subhasinghe, Khawaja Ashfaque Ahmed, Lisanework E. Ayalew, Hemlata Gautam, Shelly Popowich, Ayumi Matsuyama-Kato, Betty Chow-Lockerbie, Suresh K. Tikoo, Philip Griebel, and Susantha Gomis

Subjects

CpG-ODN, Trained immunity, Innate immune memory, Mitochondrial OXPHOS, Cellular glycolysis, Broiler chicken, Medicine, Science

Abstract

Abstract Oligodeoxynucleotides containing CpG motifs (CpG-ODN) can promote antimicrobial immunity in chickens by enriching immune compartments and activating immune cells. Innate memory, or trained immunity, has been demonstrated in humans and mice, featuring the absence of specificity to the initial stimulus and subsequently cross-protection against pathogens. We hypothesize that CpG-ODN can induce trained immunity in chickens. We delivered single or multiple administrations of CpG-ODN to birds and mitochondrial oxidative phosphorylation (OXPHOS) and glycolysis of peripheral blood mononuclear cells were quantified using Seahorse XFp. Next, chickens were administered with CpG-ODN twice at 1 and 4 day of age and challenged with Escherichia coli at 27 days of age. The CpG-ODN administered groups had significantly higher mitochondrial OXPHOS until 21 days of age while cellular glycolysis gradually declined by 14 days of age. The group administered with CpG-ODN twice at 1 and 4 days of age had significantly higher survival, lower clinical score and bacterial load following challenge with E. coli at 27 d of age. This study demonstrated the induction of trained immunity in broiler chickens following administration of CpG-ODN twice during the first 4 days of age to protect birds against E. coli septicemia at 27 days of age.

Published

2024

23. Modulation of Human Macrophages by Plasma from COVID-19 Patients Following BCG Vaccination: BATTLE Trial

Author

Buosi K, Jalalizadeh M, Maia AR, Morari J, Velloso LA, and Reis LO

Subjects

covid, bcg, trained immunity, gender, age, healthcare worker, ifns, ace2., Medicine (General), R5-920

Abstract

Keini Buosi,1,* Mehrsa Jalalizadeh,1,* Aline Rosa Maia,2 Joseane Morari,2 Licio Augusto Velloso,2 Leonardo Oliveira Reis1,3 1Uroscience, School of Medical Sciences, University of Campinas, UNICAMP, Campinas, Sao Paulo, 13083-872, Brazil; 2Laboratory of Cell Signaling, Obesity and Comorbidities Research Center, University of Campinas, Campinas, 13083-864, Brazil; 3Immunoncology, Pontifical Catholic University of Campinas, PUC-Campinas, Campinas, Sao Paulo, 13087-571, Brazil*These authors contributed equally to this workCorrespondence: Leonardo Oliveira Reis, PUC-Campinas, Pontifical Catholic University of Campinas, ImmunOncology, Av. John Boyd Dunlop - Jardim Ipaussurama, Campinas, Sao Paulo, 13034-685, Brazil, Tel/Fax +55 019 35217481, Email Reisleo@unicamp.brPurpose: To analyze the interfering effect of plasma from COVID-19 convalescent adults vaccinated or not with intradermal Bacillus Calmette-Guérin (BCG) on human macrophages.Methods: The BATTLE clinical trial (NCT04369794) was initiated in the 2020 SARS-CoV-2 pandemic to study the safety and efficacy of BCG revaccination of COVID-19 convalescent adults. We measured the expression induction of eleven COVID-19-related genes in human macrophages cultured in plasma taken from 22 BCG vaccinated and 17 placebo patients at baseline and 45 days post-intervention. Subgroup analysis was based on gender, age, job type (healthcare worker [HCW] vs non-HCW), and the presence of anosmia/dysgeusia.Results: Compared to plasma from placebo counterparts, the plasma of BCG vaccinated patients increased the expression induction of interferon (IFN)β-1b (p = 0.042) in human macrophages. This increase was more pronounced in females and in healthcare workers (HCW) (p = 0.007 and 0.001, respectively). Interferon-induced transmembrane protein 3 (IFITM3) expression induction was increased by plasma from BCG vaccinated females, young age group, and HCWs (p = 0.004, 0.011, and 0.040, respectively). Interleukin (IL)-10 induction increased by the plasma of young BCG recipients (p = 0.008). Induction of IL-6 expression increased by non-HCW BCG recipients plasma but decreased by HCW BCG recipients plasma (p = 0.005). Baseline plasma of patients who presented with anosmia/dysgeusia at the time of admission induced lower angiotensin-converting enzyme 2 (ACE2) compared to those without the symptom (0.76 vs 0.97, p = 0.004). ACE2 expression induction significantly increased by plasma of BCG recipients if they had anosmia/dysgeusia on admission (p = 0.028).Conclusion: The expressions of IFNβ-1b, IFITM3, IL-6, and IL-10 in human macrophages incubated with the plasma of COVID-19 convalescent patients were modulated by BCG. These modulations depended on subject-specific characteristics, including gender, age, clinical presentation (anosmia/dysgeusia), job type, and previous exposure to mycobacteria.Keywords: COVID, BCG, trained immunity, gender, age, healthcare worker, IFNs, ACE2

Published

2024

24. The role of trained immunity in sepsis.

Author

Wenjuan Wang, Lisi Ma, Bin Liu, and Liangliang Ouyang

Subjects

IMMUNOLOGIC memory, SEPSIS, IMMUNE response, INFLAMMATION, IMMUNOTHERAPY

Abstract

Sepsis is defined as a life-threatening organ dysfunction syndrome caused by dysregulated host response to infection, characterized by a systemic inflammatory response to infection. The use of antibiotics, fluid resuscitation, and organ support therapy has limited prognostic benefit in patients with sepsis, and its incidence is not diminishing, which is attracting increased attention in medicine. Sepsis remains one of the most debilitating and expensive illnesses. One of the main reasons of septic mortality is now understood to be disruption of immune homeostasis. Immunotherapy is revolutionizing the treatment of illnesses in which dysregulated immune responses play a significant role. This "trained immunity", which is a potent defense against infection regardless of the type of bacteria, fungus, or virus, is attributed to the discovery that the innate immune cells possess immune memory via metabolic and epigenetic reprogramming. Here we reviewed the immunotherapy of innate immune cells in sepsis, the features of trained immunity, and the relationship between trained immunity and sepsis. [ABSTRACT FROM AUTHOR]

Published

2024

25. Induction of trained immunity in broiler chickens following delivery of oligodeoxynucleotide containing CpG motifs to protect against Escherichia coli septicemia.

Author

Subhasinghe, Iresha, Ahmed, Khawaja Ashfaque, Ayalew, Lisanework E., Gautam, Hemlata, Popowich, Shelly, Matsuyama-Kato, Ayumi, Chow-Lockerbie, Betty, Tikoo, Suresh K., Griebel, Philip, and Gomis, Susantha

Subjects

*POULTRY growth, *BROILER chickens, *CHICKEN diseases, *SEPSIS, *MONONUCLEAR leukocytes, *ESCHERICHIA coli, *CPG nucleotides, *IMMUNITY

Abstract

Oligodeoxynucleotides containing CpG motifs (CpG-ODN) can promote antimicrobial immunity in chickens by enriching immune compartments and activating immune cells. Innate memory, or trained immunity, has been demonstrated in humans and mice, featuring the absence of specificity to the initial stimulus and subsequently cross-protection against pathogens. We hypothesize that CpG-ODN can induce trained immunity in chickens. We delivered single or multiple administrations of CpG-ODN to birds and mitochondrial oxidative phosphorylation (OXPHOS) and glycolysis of peripheral blood mononuclear cells were quantified using Seahorse XFp. Next, chickens were administered with CpG-ODN twice at 1 and 4 day of age and challenged with Escherichia coli at 27 days of age. The CpG-ODN administered groups had significantly higher mitochondrial OXPHOS until 21 days of age while cellular glycolysis gradually declined by 14 days of age. The group administered with CpG-ODN twice at 1 and 4 days of age had significantly higher survival, lower clinical score and bacterial load following challenge with E. coli at 27 d of age. This study demonstrated the induction of trained immunity in broiler chickens following administration of CpG-ODN twice during the first 4 days of age to protect birds against E. coli septicemia at 27 days of age. [ABSTRACT FROM AUTHOR]

Published

2024

26. Metabolic Regulation in the Induction of Trained Immunity.

Author

Ferreira, Anaisa V., Domínguez-Andrés, Jorge, Merlo Pich, Laura M., Joosten, Leo A. B., and Netea, Mihai G.

Abstract

The innate immune system exhibits features of memory, termed trained immunity, which promote faster and more robust responsiveness to heterologous challenges. Innate immune memory is sustained through epigenetic modifications, affecting gene accessibility, and promoting a tailored gene transcription for an enhanced immune response. Alterations in the epigenetic landscape are intertwined with metabolic rewiring. Here, we review the metabolic pathways that underscore the induction and maintenance of trained immunity, including glycolysis, oxidative phosphorylation, the tricarboxylic acid cycle, and amino acid and lipid metabolism. The intricate interplay of these pathways is pivotal for establishing innate immune memory in distinct cellular compartments. We explore in particular the case of resident lung alveolar macrophages. We propose that leveraging the memory of the innate immune system may present therapeutic potential. Specifically, targeting the metabolic programs of innate immune cells is an emerging strategy for clinical interventions, either to boost immune responses in immunosuppressed conditions or to mitigate maladaptive activation in hyperinflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2024

27. Maternal Innate Immune Reprogramming After Complicated Pregnancy.

Author

Lodge‐Tulloch, Nakeisha A., Paré, Jean‐François, Couture, Camille, Bernier, Elsa, Cotechini, Tiziana, Girard, Sylvie, and Graham, Charles H.

Subjects

*FETAL growth retardation, *RNA sequencing, *MYELOID cells, *IMMUNOLOGICAL tolerance, *MONOCYTES

Abstract

Problem: Preeclampsia (PE) and fetal growth restriction (FGR) are often associated with maternal inflammation and an increased risk of cardiovascular and metabolic disease in the affected mothers. The mechanism responsible for this increased risk of subsequent disease may involve reprogramming of innate immune cells, characterized by epigenetic modifications. Method of Study: Circulating monocytes from women with PE, FGR, or uncomplicated pregnancies (control) were isolated before labor. Cytokine release from monocytes following exposure to lipopolysaccharide (LPS) and the presence of lysine 4‐trimethylated histone 3 (H3K4me3) within TNF promoter sequences were evaluated. Single‐cell transcriptomic profiles of circulating monocytes from women with PE or uncomplicated pregnancies were assessed. Results: Monocytes from women with PE or FGR exhibited increased IL‐10 secretion and decreased IL‐1β and GM‐CSF secretion in response to LPS. While TNFα secretion was not significantly different in cultures of control monocytes versus those from complicated pregnancies with or without LPS exposure, monocytes from complicated pregnancies had significantly decreased levels of H3K4me3 associated with TNF promoter sequences. Cluster quantification and pathway analysis of differentially expressed genes revealed an increased proportion of anti‐inflammatory myeloid cells and a lower proportion of inflammatory non‐classical monocytes among the circulating monocyte population in women with PE. Conclusions: Monocytes from women with PE and FGR exhibit an immune tolerance phenotype before initiation of labor. Further investigation is required to determine whether this tolerogenic phenotype persists after the affected pregnancy and contributes to increased risk of subsequent disease. [ABSTRACT FROM AUTHOR]

Published

2024

28. Evidence of innate training in bovine γδ T cells following subcutaneous BCG administration.

Author

Samuel, Beulah Esther Rani, Diaz, Fabian E., Maina, Teresia W., Corbett, Ryan J., Tuggle, Christopher K., and McGill, Jodi L.

Subjects

MONONUCLEAR leukocytes, TRANSCRIPTION factors, IMMUNOLOGIC memory, T cells, BCG vaccines

Abstract

The Bacillus Calmette Guerin (BCG) vaccine has been shown to induce nonspecific protection against diseases other than tuberculosis in vaccinated individuals, attributed to the induction of trained immunity. We have previously demonstrated that BCG administration induces innate immune training in mixed peripheral blood mononuclear cells and monocytes in calves. Gamma Delta (gd) T cells are non-conventional T cells that exhibit innate and adaptive immune system features. They are in higher proportion in the peripheral blood of cattle than humans or rodents and play an essential role in bovine immune response to pathogens. In the current study, we determined if BCG administration induced innate immune training in bovine gd T cells. A group of 16 pre-weaned Holstein calves (2-4 d age) were enrolled in the study and randomly assigned to vaccine and control groups (n=8/group). The vaccine group received two doses of 106 colony forming units (CFU) BCG Danish strain subcutaneously, separated by 2 weeks. The control group remained unvaccinated. Gamma delta T cells were purified from peripheral blood using magnetic cell sorting three weeks after receiving the 1st BCG dose. We observed functional changes in the gd T cells from BCG-treated calves shown by increased IL-6 and TNF-a cytokine production in response to in vitro stimulation with Escherichia coli LPS and PAM3CSK4. ATAC-Seq analysis of 78,278 regions of open chromatin (peaks) revealed that gd T cells fromBCGtreated calves had an altered epigenetic status compared to cells from the control calves. Differentially accessible peaks (DAP) found near the promoters of innate immunity-related genes like Siglec14, Irf4, Ifna2, Lrrfip1, and Tnfrsf10d were 1 to 4-fold more accessible in cells from BCG-treated calves. MOTIF enrichment analysis of the sequences within DAPs, which explores transcription factor binding motifs (TFBM) upstream of regulatory elements, revealed TFBM for Eomes and IRF-5 were among the most enriched transcription factors. GO enrichment analysis of genes proximal to the DAPs showed enrichment of pathways such as regulation of IL-2 production, T-cell receptor signaling pathway, and other immune regulatory pathways. In conclusion, our study shows that subcutaneous BCG administration in preweaned calves can induce innate immune memory in the form of trained immunity in gd T cells. This memory is associated with increased chromatin accessibility of innate immune response-related genes, thereby inducing a functional trained immune response evidenced by increased IL-6 and TNF-α cytokine production. [ABSTRACT FROM AUTHOR]

Published

2024

29. Trained immunity inducers in cancer immunotherapy.

Author

Yongjun Sui and Berzofsky, Jay A.

Subjects

IMMUNOLOGIC memory, T cells, CANCER vaccines, TUMOR microenvironment, VACCINE effectiveness

Abstract

While most of the cancer immunotherapy strategies engage adaptive immunity, especially tumor-associated T cells, the small fraction of responding patients and types of cancers amenable, and the possibility of severe adverse effects limit its usage. More effective and general interventions are urgently needed. Recently, a de facto innate immune memory, termed 'trained immunity', has become a new research focal point, and promises to be a powerful tool for achieving long-term therapeutic benefits against cancers. Trained immunity-inducing agents such as BCG and fungal glucan have been shown to be able to avert the suppressive tumor microenvironment (TME), enhance T cell responses, and eventually lead to tumor regression. Here, we review the current understating of trained immunity induction and highlight the critical roles of emergency granulopoiesis, interferon g and tissue-specific induction. Preclinical and clinical studies that have exploited trained immunity inducers for cancer immunotherapy are summarized, and repurposed trained immunity inducers from other fields are proposed. We also outline the challenges and opportunities for trained immunity in future cancer immunotherapies. We envisage that more effective cancer vaccines will combine the induction of trained immunity with T cell therapies. [ABSTRACT FROM AUTHOR]

Published

2024

30. Emerging opportunities to target inflammation: myocardial infarction and type 2 diabetes.

Author

Kufazvinei, Tafadzwa T J, Chai, Jason, Boden, Katherine A, Channon, Keith M, and Choudhury, Robin P

Subjects

*TYPE 2 diabetes, *MYOCARDIAL infarction, *CORONARY artery disease, *OVERALL survival, *HEALING

Abstract

After myocardial infarction (MI), patients with type 2 diabetes have an increased rate of adverse outcomes, compared to patients without. Diabetes confers a 1.5–2-fold increase in early mortality and, importantly, this discrepancy has been consistent over recent decades, despite advances in treatment and overall survival. Certain assumptions have emerged to explain this increased risk, such as differences in infarct size or coronary artery disease severity. Here, we re-evaluate that evidence and show how contemporary analyses using state-of-the-art characterization tools suggest that the received wisdom tells an incomplete story. Simultaneously, epidemiological and mechanistic biological data suggest additional factors relating to processes of diabetes-related inflammation might play a prominent role. Inflammatory processes after MI mediate injury and repair and are thus a potential therapeutic target. Recent studies have shown how diabetes affects immune cell numbers and drives changes in the bone marrow, leading to pro-inflammatory gene expression and functional suppression of healing and repair. Here, we review and re-evaluate the evidence around adverse prognosis in patients with diabetes after MI, with emphasis on how targeting processes of inflammation presents unexplored, yet valuable opportunities to improve cardiovascular outcomes in this vulnerable patient group. [ABSTRACT FROM AUTHOR]

Published

2024

31. High-throughput screen identifies non inflammatory small molecule inducers of trained immunity.

Author

Knight, Hannah Riley, Ketter, Ellen, Ung, Trevor, Weiss, Adam, Ajit, Jainu, Qing Chen, Jingjing Shen, Ka Man Ip, Chun-Yi Chiang, Barreiro, Luis, and Esser-Kahn, Aaron

Subjects

*IMMUNOLOGIC memory, *METABOLIC reprogramming, *SMALL molecules, *NATURAL immunity, *CLINICAL medicine

Abstract

Trained immunity is characterized by epigenetic and metabolic reprogramming in response to specific stimuli. This rewiring can result in increased cytokine and effector responses to pathogenic challenges, providing nonspecific protection against disease. It may also improve immune responses to established immunotherapeutics and vaccines. Despite its promise for next-generation therapeutic design, most current understanding and experimentation is conducted with complex and heterogeneous biologically derived molecules, such as ß-glucan or the Bacillus Calmette-Guérin (BCG) vaccine. This limited collection of training compounds also limits the study of the genes most involved in training responses as each molecule has both training and nontraining effects. Small molecules with tunable pharmacokinetics and delivery modalities would both assist in the study of trained immunity and its future applications. To identify small molecule inducers of trained immunity, we screened a library of 2,000 drugs and drug-like compounds. Identification of well-defined compounds can improve our understanding of innate immune memory and broaden the scope of its clinical applications. We identified over two dozen small molecules in several chemical classes that induce a training phenotype in the absence of initial immune activation--a current limitation of reported inducers of training. A surprising result was the identification of glucocorticoids, traditionally considered immunosuppressive, providing an unprecedented link between glucocorticoids and trained innate immunity. We chose seven of these top candidates to characterize and establish training activity in vivo. In this work, we expand the number of compounds known to induce trained immunity, creating alternative avenues for studying and applying innate immune training. [ABSTRACT FROM AUTHOR]

Published

2024

32. Systemic versus localized Bacillus Calmette Guérin immunotherapy of bladder cancer promotes an anti‐tumoral microenvironment: Novel role of trained immunity.

Author

Atallah, Aline, Grossman, Arielle, Nauman, Richard W., Paré, Jean‐François, Khan, Adam, Siemens, D. Robert, Cotechini, Tiziana, and Graham, Charles H.

Subjects

BLADDER cancer, NON-muscle invasive bladder cancer, MYELOID-derived suppressor cells, IMMUNOLOGIC memory, CYTOTOXIC T cells, BACILLUS (Bacteria)

Abstract

Treatment for higher‐risk non‐muscle invasive bladder cancer (NMIBC) involves intravesical immunotherapy with Bacillus Calmette Guérin (BCG); however, disease recurrence and progression occur frequently. Systemic immunity is critical for successful cancer immunotherapy; thus, recurrence of NMIBC may be due to suboptimal systemic activation of anti‐tumor immunity after local immunotherapy. We previously reported that systemically acquired trained immunity (a form of innate immune memory) in circulating monocytes is associated with increased time‐to‐recurrence in patients with NMIBC treated with BCG. Herein, we used a mouse model of NMIBC to compare the effects of intravesical versus intravenous (systemic) BCG immunotherapy on the local and peripheral immune microenvironments. We also assessed whether BCG‐induced trained immunity modulates anti‐tumor immune responses. Compared with intravesical BCG, which led to a tumor‐promoting immune microenvironment, intravenous BCG resulted in an anti‐tumoral bladder microenvironment characterized by increased proportions of cytotoxic T lymphocytes (CTLs), and decreased proportions of myeloid‐derived suppressor cells. Polarization toward anti‐tumoral immunity occurred in draining lymph nodes, spleen, and bone marrow following intravenous versus intravesical BCG treatment. Pre‐treatment with intravesical BCG was associated with increased rate of tumor growth compared with intravenous BCG pre‐treatment. Trained immunity contributed to remodeling of the tumor immune microenvironment, as co‐instillation of BCG‐trained macrophages with ovalbumin‐expressing bladder tumor cells increased the proportion of tumor‐specific CTLs. Furthermore, BCG‐trained dendritic cells exhibited enhanced antigen uptake and presentation and promoted CTL proliferation. Our data support the concept that systemic immune activation promotes anti‐tumor responses, and that BCG‐induced trained immunity is important in driving anti‐tumor adaptive immunity. [ABSTRACT FROM AUTHOR]

Published

2024

33. Probiotic bacteria can modulate immune responses to paratuberculosis vaccination.

Author

Oyanguren, Maddi, Molina, Elena, Mugica, Maitane, Ladero-Auñon, Iraia, Fuertes, Miguel, Fernández, Miguel, Benavides, Julio, and Elguezabal, Natalia

Subjects

MYCOBACTERIUM avium paratuberculosis, IMMUNE response, PARATUBERCULOSIS, PROBIOTICS, HUMORAL immunity, VACCINATION

Abstract

Mycobacterium avium subsp. paratuberculosis (Map) is the etiological agent of paratuberculosis (PTB), a chronic intestinal inflammatory disease that causes high economical losses in dairy livestock worldwide. Due to the absence of widely available preventive or therapeutical treatments, new alternative therapies are needed. In this study, the effect of a probiotic alone or in combination with a commercial vaccine has been evaluated in a rabbit model. Vaccination enhanced the humoral response, exerted a training effect of peripheral polymorphonuclear neutrophils (PMNs) against homologous and heterologous stimuli, stimulated the release of pro-inflammatory cytokines by gut-associated lymphoid tissue (GALT) macrophages, and reduced the bacterial burden in GALT as well. However, the administration of the probiotic after vaccination did not affect the PMN activity, increased metabolic demand, and supressed pro-inflammatory cytokines, although humoral response and bacterial burden decrease in GALT was maintained similar to vaccination alone. The administration of the probiotic alone did not enhance the humoral response or PMN activity, and the bacterial burden in GALT was further increased compared to the only challenged group. In conclusion, the probiotic was able to modulate the immune response hampering the clearance of the infection and was also able to affect the response of innate immune cells after vaccination. This study shows that the administration of a probiotic can modulate the immune response pathways triggered by vaccination and/or infection and even exacerbate the outcome of the disease, bringing forward the importance of verifying treatment combinations in the context of each particular infectious agent. [ABSTRACT FROM AUTHOR]

Published

2024

34. Sarcoidosis immunopathogenesis – a new concept of maladaptive trained immunity.

Author

Robert, Marie, Yatim, Nader, Sacré, Karim, and Duffy, Darragh

Subjects

*SARCOIDOSIS, *MYELOID cells, *IMMUNOLOGIC memory, *IMMUNITY, *GENETIC variation, *ENVIRONMENTAL exposure

Abstract

Sarcoidosis results from a combination of genetic variants and environmental factors but its exact cause remains unknown. Evidence highlights a major role of monocytes as important drivers of sarcoidosis immunopathogenesis. The emerging concept of trained immunity opens new perspectives for the comprehension of sarcoidosis pathology, with a particular presumed role played by immune metabolism and epigenetics. We posit that maladaptive innate immune training may drive sarcoidosis pathogenesis. The confirmation of maladaptive innate immune training in sarcoidosis might allow the development of new candidate therapeutic strategies. The pathogenesis of sarcoidosis, an immune-mediated granulomatous disease, has long remained elusive. Recent discoveries on trained immunity might help decipher immunological mechanisms underlying the disease which in turn may inform novel putative treatment options. Sarcoidosis is a chronic immune disease of unknown origin for which we still lack an immunological framework unifying causal agents, host factors, and natural history of disease. Here, we discuss the initial triggers of disease, and how myeloid cells drive granuloma formation and contribute to immunopathogenesis. We highlight recent advances in our understanding of innate immune memory and propose the hypothesis that maladaptive innate immune training connects previous environmental exposure to granuloma maintenance and expansion. Lastly, we consider how this hypothesis may open novel therapeutic avenues, while corticosteroids remain the front-line treatment. [ABSTRACT FROM AUTHOR]

Published

2024

35. Trained Immunity and Trained Tolerance: The Case of Helicobacter pylori Infection.

Author

Dore, Maria Pina and Pes, Giovanni Mario

Subjects

*HELICOBACTER pylori infections, *HELICOBACTER pylori, *IMMUNITY, *GASTRIC mucosa, *MUCOSA-associated lymphoid tissue lymphoma

Abstract

Trained immunity is a concept in immunology in which innate immune cells, such as monocytes and macrophages, exhibit enhanced responsiveness and memory-like characteristics following initial contact with a pathogenic stimulus that may promote a more effective immune defense following subsequent contact with the same pathogen. Helicobacter pylori, a bacterium that colonizes the stomach lining, is etiologically associated with various gastrointestinal diseases, including gastritis, peptic ulcer, gastric adenocarcinoma, MALT lymphoma, and extra gastric disorders. It has been demonstrated that repeated exposure to H. pylori can induce trained immunity in the innate immune cells of the gastric mucosa, which become more responsive and better able to respond to subsequent H. pylori infections. However, interactions between H. pylori and trained immunity are intricate and produce both beneficial and detrimental effects. H. pylori infection is characterized histologically as the presence of both an acute and chronic inflammatory response called acute-on-chronic inflammation, or gastritis. The clinical outcomes of ongoing inflammation include intestinal metaplasia, gastric atrophy, and dysplasia. These same mechanisms may also reduce immunotolerance and trigger autoimmune pathologies in the host. This review focuses on the relationship between trained immunity and H. pylori and underscores the dynamic interplay between the immune system and the pathogen in the context of gastric colonization and inflammation. [ABSTRACT FROM AUTHOR]

Published

2024

36. Immunogenicity and efficacy of CNA25 as a potential whole-cell vaccine against systemic candidiasis.

Author

Sahu, Satya Ranjan, Dutta, Abinash, Peroumal, Doureradjou, Kumari, Premlata, Utakalaja, Bhabasha Gyanadeep, Patel, Shraddheya Kumar, and Acharya, Narottam

Abstract

Disseminated fungal infections account for ~1.5 million deaths per year worldwide, and mortality may increase further due to a rise in the number of immunocompromised individuals and drug-resistance fungal species. Since an approved antifungal vaccine is yet to be available, this study explored the immunogenicity and vaccine efficacy of a DNA polymerase mutant strain of Candida albicans. CNA25 is a pol32ΔΔ strain that exhibits growth defects and does not cause systemic candidiasis in mice. Immunized mice with live CNA25 were fully protected against C. albicans and C. parapsilosis but partially against C. tropicalis and C. glabrata infections. CNA25 induced steady expression of TLR2 and Dectin-1 receptors leading to a faster recognition and clearance by the immune system associated with the activation of protective immune responses mostly mediated by neutrophils, macrophages, NK cells, B cells, and CD4+ and CD8+ T cells. Molecular blockade of Dectin-1, IL-17, IFNγ, and TNFα abolished resistance to reinfection. Altogether, this study suggested that CNA25 collectively activates innate, adaptive, and trained immunity to be a promising live whole-cell vaccine against systemic candidiasis. Synopsis: CNA25 is a DNA polymerase subunit knockout strain of pathogenic yeast Candida albicans. Immunization with live CNA25 prevents systemic candidiasis in mice. It is recognised by innate immune cells leading to its clearance. Activation of CD4+ and CD8 + T cells in vaccinated mice prevents fungal reinfection. Trained innate cells are also involved in protective immune responses. CNA25 is a DNA polymerase subunit knockout strain of pathogenic yeast Candida albicans. Immunization with live CNA25 prevents systemic candidiasis in mice. [ABSTRACT FROM AUTHOR]

Published

2024

37. BCG Vaccination Suppresses Glucose Intolerance Progression in High-Fat-Diet-Fed C57BL/6 Mice.

Author

Arakawa, Haruna and Inafuku, Masashi

Subjects

BCG vaccines, GLUCOSE intolerance, B cells, LABORATORY mice, TYPE 2 diabetes

Abstract

Background and Objectives: Mycobacterium bovis Bacillus Calmette–Guérin (BCG) vaccine administration has been suggested to prevent glucose metabolism abnormalities and fatty liver in genetically obese ob/ob mice; however, it is not clear whether the beneficial effects of BCG are also observed in the progression of glucose intolerance induced by a high-fat diet (HFD). Therefore, the effects of BCG vaccination on changes in glucose tolerance and insulin response were investigated in HFD-fed C57BL/6 mice. Materials and Methods: We used the BCG Tokyo 172 strain to determine effects on abnormalities in glucose metabolism. For vaccination, five-week-old male mice were injected intraperitoneally with BCG and maintained on a HFD for three weeks. The mice were regularly subjected to intraperitoneal glucose tolerance and insulin tolerance tests (IGTTs and ITTs). These tests were also performed in mice transplanted with bone marrow cells from BCG-vaccinated donor mice. Results: Significant effects of BCG vaccination on blood glucose levels in the IGTTs and ITTs were observed from week 12 of the experiment. BCG vaccination significantly improved changes in fasting glucose and insulin levels, insulin resistance indexes, and glucagon-to-insulin ratios in conjunction with the HFD at the end of the experiment. Significant inhibitory effects in the IGTTs and ITTs on glucose intolerance were also observed with transplantation with bone marrow cells derived from BCG-vaccinated donor mice. Conclusions: BCG vaccination significantly delayed glucose intolerance progression, suggesting a beneficial effect of BCG on the pathogenesis of type 2 diabetes. It has also been suggested that the effects of BCG vaccination may be at least partially due to an immune memory (trained immunity) for hematopoietic stem and progenitor cells of the bone marrow. [ABSTRACT FROM AUTHOR]

Published

2024

38. The helminth‐derived peptide, FhHDM‐1, reverses the trained phenotype of NOD bone‐marrow‐derived macrophages and regulates proinflammatory responses.

Author

Quinteros, Susel Loli, Snyder, Nathaniel W., Chatoff, Adam, Ryan, Fiona, O'Brien, Bronwyn, and Donnelly, Sheila

Subjects

PEPTIDES, MACROPHAGES, PHENOTYPES, BONE marrow cells, MACROPHAGE inflammatory proteins

Abstract

This article explores the concept of "trained immunity" in bone-marrow-derived macrophages and its role in the development of type 1 diabetes. The study focuses on macrophages from nonobese diabetic (NOD) mice and finds that they exhibit characteristics of trained immunity, such as increased histone methylation, glycolysis, and proinflammatory cytokine production. The authors suggest that previous infections or changes in gut microbiota may train myeloid cells in the bone marrow, leading to an amplified proinflammatory response and the initiation of autoimmunity in type 1 diabetes. The article also discusses the potential therapeutic effects of a peptide called FhHDM-1, secreted by the parasitic worm Fasciola hepatica, in preventing type 1 diabetes in mice. Administering FhHDM-1 to mice resulted in a reduction in histone methylation, a shift in macrophage metabolism, and a decrease in proinflammatory responses. These findings suggest that FhHDM-1 may alter the epigenetic imprint of macrophages, regulating immune responses and potentially preventing type 1 diabetes and other autoimmune/inflammatory disorders. [Extracted from the article]

Published

2024

39. Effects of Bacillus Calmette-Guérin on immunometabolism, microbiome and liver diseases⋆.

Author

Ijaz, Muhammad, Vaziri, Farzam, and Wan, Yu-Jui

Subjects

Bacillus Calmette-Guérin (BCG), Diabetes, Gut microbiota, Liver disease, Metabolic diseases, Trained immunity, Vaccination

Abstract

Metabolic diseases have overtaken infectious diseases as the most serious public health issue and economic burden in most countries. Moreover, metabolic diseases increase the risk of having infectious diseases. The treatment of metabolic disease may require a long-term strategy of taking multiple medications, which can be costly and have side effects. Attempts to expand the therapeutic use of vaccination to prevent or treat metabolic diseases have attracted significant interest. A growing body of evidence indicates that Bacillus Calmette-Guérin (BCG) offers protection against non-infectious diseases. The non-specific effects of BCG occur likely due to the induction of trained immunity. In this regard, understanding how BCG influences the development of chronic metabolic health including liver diseases would be important. This review focuses on research on BCG, the constellation of disorders associated with metabolic health issues including liver diseases and diabetes as well as how BCG affects the gut microbiome, immunity, and metabolism.

Published

2023

40. Vaccine induced mucosal and systemic memory NK/ILCs elicit decreased risk of SIV/SHIV acquisition

Author

Mohammad Arif Rahman, Isabela Silva de Castro, Luca Schifanella, Massimiliano Bissa, and Genoveffa Franchini

Subjects

memory-like NK cells, antigen-reactive ILCs, V2-specific ADCC, innate memory, trained immunity, SIV/SHIV, Immunologic diseases. Allergy, RC581-607

Abstract

SIV and HIV-based envelope V1-deleted (ΔV1) vaccines, delivered systemically by the DNA/ALVAC/gp120 platform, decrease the risk of mucosal SIV or SHIV acquisition more effectively than V1-replete vaccines. Here we investigated the induction of mucosal and systemic memory-like NK cells as well as antigen-reactive ILC response by DNA/ALVAC/gp120-based vaccination and their role against SIV/SHIV infection. ΔV1 HIV vaccination elicited a higher level of mucosal TNF-α+ and CD107+ memory-like NK cells than V1-replete vaccination, suggesting immunogen dependence. Mucosal memory-like NK cells, systemic granzyme B+ memory NK cells, and vaccine-induced mucosal envelope antigen-reactive IL-17+ NKp44+ ILCs, IL-17+ ILC3s, and IL-13+ ILC2 subsets were linked to a lower risk of virus acquisition. Additionally, mucosal memory-like NK cells and mucosal env-reactive IFN-γ+ ILC1s and env- reactive IL-13+ ILC2 subsets correlated with viral load control. We further observed a positive correlation between post-vaccination systemic and mucosal memory-like NK cells, suggesting vaccination enhances the presence of these cells in both compartments. Mucosal and systemic memory-like NK cells positively correlated with V2-specific ADCC responses, a reproducible correlate of reduced risk of SIV/HIV infection. In contrast, an increased risk was associated with the level of mucosal PMA/Ionomycin-induced IFN-γ+ and CD107+ NKG2A-NKp44- ILCs. Plasma proteomic analyses demonstrated that suppression of mucosal memory-like NK cells was linked to the level of CCL-19, LT-α, TNFSF-12, and IL-15, suppression of systemic env-reactive granzyme B+ memory-like NK cells was associated with the level of OLR1, CCL-3, and OSM, and suppression of IL-17+ ILCs immunity was correlated with the level of IL-6 and CXCL-9. In contrast, FLT3 ligand was associated with promotion of protective mucosal env-reactive IL-17+ responses. These findings emphasize the importance of mucosal memory-like NK cell and envelope- reactive ILC responses for protection against mucosal SIV/SHIV acquisition.

Published

2024

41. Covid lockdown and repaying the immunity debt in children

Author

Peng Han and Kunling Shen

Subjects

SARS-CoV-2, Non-pharmaceutical interventions, Immunity debt, Trained immunity, Children, Pediatrics, RJ1-570

Abstract

Non-pharmaceutical interventions (NPIs) implemented during the SARS-CoV-2 pandemic have been proven effective. While reducing SARS-CoV-2 transmission, NPIs also reduced children's exposure to other pathogens, leading to a decline in the incidence of many viral and bacterial infections. The reduction in contact with viruses and bacteria could result in insufficient immune stimulation of pathogens in the population, leading to an increase in susceptible populations and a decline in herd immunity, which form the immunity debt during the SARS-CoV-2 pandemic. Immunity debt can impact the pattern of seasonal pathogens, increase the incidence and severity of invasive infections, and potentially raise the risk of allergic diseases in children. Immunization, continuing to implement NPIs, pathogen monitoring, and health education are important measures to repay immunity debt. Besides, trained immunity, referring to the memory immunity produced by the innate immune system upon re-stimulation, can be employed as a non-specific measure to prevent the spread of pathogens. The protective effect of trained immunity can be used as a temporary preventive measure for emerging infectious diseases and create conditions for vaccine development.

Published

2024

42. Mucosal trained immunity–based vaccines: Cutting recurrent infections in autoimmune patients on immunosuppression.

Author

Candelas, Gloria, Villegas, Ángela, and Sánchez-Ramón, Silvia

Published

2024

43. Mechanisms involved in the transmission of trained immunity to offspring.

Author

Dulfer, Elisabeth A. and Domínguez-Andrés, Jorge

Published

2024

44. Navigating the crossroads: asthma, trained immunity, and infection susceptibility.

Author

Al Meslamani, Ahmad Z. and Merghani Ali, Eman

Subjects

TH2 cells, TYPE I interferons, T helper cells, RESPIRATORY infections, ASTHMA in children, ENTEROVIRUS diseases, WHEEZE

Abstract

This article discusses the concept of "trained immunity" and its potential implications for asthma and infection susceptibility. Trained immunity refers to the enhanced response of innate immune cells to subsequent encounters with antigens, and it can be adjusted to either amplify immune responses or inhibit reactions contributing to autoimmune disorders. The article explores the complex relationship between asthma, trained immunity, and infection, highlighting the role of various immunological pathways, genetic and environmental factors, and interactions with the microbiome. While trained immunity may have beneficial effects against pathogens, it can also worsen inflammatory diseases like asthma. The article suggests that further research is needed to understand the mechanisms through which trained immunity influences asthma pathogenesis and infection dynamics in order to develop targeted interventions. [Extracted from the article]

Published

2024

45. Epigenetics and Immunity

Author

Carlberg, Carsten and Carlberg, Carsten

Published

2024

46. Immunity and Aging

Author

Carlberg, Carsten, Ulven, Stine M., Velleuer, Eunike, Carlberg, Carsten, Ulven, Stine M., and Velleuer, Eunike

Published

2024

47. Trained immunity of synovial macrophages is associated with exacerbated joint inflammation and damage after Staphylococcus aureus infection

Author

Rocha, Peter Silva, Silva, Adryan Aparecido, Queiroz-Junior, Celso Martins, Braga, Amanda Dias, Moreira, Thaiane Pinto, Teixeira, Mauro Martins, and Amaral, Flávio Almeida

Published

2024

48. Do respiratory epithelial cells 'remember' early life microbial exposure through epigenetic changes?

Author

Janas, Piotr, Drake, Mandy, McSorley, Henry, and Schwarze, Jurgen

Subjects

respiratory epithelial cells, early life microbial exposure, epigenetic changes, adaptive immune system, epigenetic imprinting, metabolomic imprinting, trained immunity, airway epithelial cells, AECs, pathogen-associated molecular patterns, PAMPs, major histocompatibility complex class I, major histocompatibility complex class II, MHC-I, MHC-II

Abstract

The adaptive immune system was considered to be the sole arm of immunity that can form a memory of past infections. In recent years this paradigm has been contested, following discoveries that many innate immune cells display lasting changes in their responses to challenges as a consequence of previous infections. It was determined that these long-term changes in immune responses were possible due to epigenetic or metabolomic imprinting. This phenomenon was also observed in plants and invertebrates and termed 'trained immunity'. Several cohort studies have linked severe respiratory syncytial virus (RSV) bronchiolitis in infancy with a higher risk of developing recurrent wheeze or childhood asthma, yet the pathomechanism behind this phenomenon remains undetermined. Here I hypothesise that RSV infection can epigenetically imprint airway epithelial cells (AECs), thus changing how these cells respond to subsequent challenges, which in turn provides a potential link between RSV infection and asthma development. First, I established in vitro and in vivo AEC experimental systems that would allow us to test the presented hypothesis. Using an assortment of pathogen-associated molecular patterns (PAMPs) as stimuli, I established that a monolayer-based cell line system might not be suitable; however, an airliquid interface (ALI) culture system utilising primary human bronchial epithelial cells proved to be a promising experimental system. Next, I used an in vivo murine model to investigate whether an RSV infection results in long-lasting changes in the responses of AECs to subsequent microbial stimuli. Despite promising cytokine/chemokine gene expression results of isolated murine AECs, I was unable to definitely confirm RSV-induced changes in response to subsequent stimulation at the transcriptional or protein level. ivNevertheless, using the murine model, I observed that RSV infection causes lasting changes in the levels of major histocompatibility complex class I (MHC-I) and II (MHC-II) on the surface of AECs. Furthermore, as seen through histone modifications, I confirmed that RSV infection causes lasting epigenetic changes in AECs, including in the promoters of genes related to MHC biology. Our results lay the basis for future investigation of trained immunity in AECs both in vitro and in vivo. I identified the limitations and benefits of several experimental systems. Importantly, I observed that RSV infection leads to lasting epigenetic and transcriptional changes of AECs that result in a prolonged increase in the levels of both MHC-I and MHC-II.

Published

2023

49. Immunogenicity and efficacy of CNA25 as a potential whole-cell vaccine against systemic candidiasis

Author

Satya Ranjan Sahu, Abinash Dutta, Doureradjou Peroumal, Premlata Kumari, Bhabasha Gyanadeep Utakalaja, Shraddheya Kumar Patel, and Narottam Acharya

Subjects

Antifungal Vaccine, Cytokines, Neutrophils, Dectin-1, Trained Immunity, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Disseminated fungal infections account for ~1.5 million deaths per year worldwide, and mortality may increase further due to a rise in the number of immunocompromised individuals and drug-resistance fungal species. Since an approved antifungal vaccine is yet to be available, this study explored the immunogenicity and vaccine efficacy of a DNA polymerase mutant strain of Candida albicans. CNA25 is a pol32ΔΔ strain that exhibits growth defects and does not cause systemic candidiasis in mice. Immunized mice with live CNA25 were fully protected against C. albicans and C. parapsilosis but partially against C. tropicalis and C. glabrata infections. CNA25 induced steady expression of TLR2 and Dectin-1 receptors leading to a faster recognition and clearance by the immune system associated with the activation of protective immune responses mostly mediated by neutrophils, macrophages, NK cells, B cells, and CD4+ and CD8+ T cells. Molecular blockade of Dectin-1, IL-17, IFNγ, and TNFα abolished resistance to reinfection. Altogether, this study suggested that CNA25 collectively activates innate, adaptive, and trained immunity to be a promising live whole-cell vaccine against systemic candidiasis.

Published

2024

50. Establishment of an in vitro model of monocyte-like THP-1 cells for trained immunity induced by bacillus Calmette-Guérin

Author

Jin-Chuan Xu, Kang Wu, Rui-qing Ma, Jian-hui Li, Jie Tao, Zhidong Hu, and Xiao-Yong Fan

Subjects

Monocyte, THP-1, Bacillus Calmette-Guérin (BCG), Trained immunity, Microbiology, QR1-502

Abstract

Abstract Background Mycobacteria bloodstream infections are common in immunocompromised people and usually have disastrous consequences. As the primary phagocytes in the bloodstream, monocytes and neutrophils play critical roles in the fight against bloodstream mycobacteria infections. In contrast to macrophages, the responses of monocytes infected with the mycobacteria have been less investigated. Results In this study, we first established a protocol for infection of non-adherent monocyte-like THP-1 cells (i.e. without the differentiation induced by phorbol 12-myristate 13-acetate (PMA) by bacillus Calmette-Guérin (BCG). Via the protocol, we were then capable of exploring the global transcriptomic profiles of non-adherent THP-1 cells infected with BCG, and found that NF-κB, MAPK and PI3K-Akt signaling pathways were enhanced, as well as some inflammatory chemokine/cytokine genes (e.g. CCL4, CXCL10, TNF and IL-1β) were up-regulated. Surprisingly, the Akt-HIF-mTOR signaling pathway was also activated, which induces trained immunity. In this in vitro infection model, increased cytokine responses to lipopolysaccharides (LPS) restimulation, higher cell viability, and decreased Candida albicans loads were observed. Conclusions We have first characterized the transcriptomic profiles of BCG-infected non-adherent THP-1 cells, and first developed a trained immunity in vitro model of the cells.

Published

2024