Your search keyword '"cd14"' showing total 10,408 results

1. Platelet and Monocyte Microvesicles as Potential Biomarkers of COVID-19 Severity: A Cross-Sectional Analysis.

Author

Nunki, Nastasya, Hernaningsih, Yetti, Wardhani, Puspa, Herawati, Asih, Yusoff, Narazah Mohd, Moses, Emmanuel Jairaj, and Semedi, Bambang Pujo

Subjects

COVID-19, COVID-19 pandemic, EXTRACELLULAR vesicles, CROSS-sectional method, BLOOD platelets

Abstract

Background: Coronavirus disease (COVID-19) induces inflammation, coagulopathy following platelet and monocyte activation, and fibrinolysis, resulting in elevated D-dimer levels. Activated platelets and monocytes produce microvesicles (MVs). We analyzed the differences in platelet and monocyte MV counts in mild, moderate, and severe COVID-19, as well as their correlation with D-dimer levels. Methods: In this cross-sectional study, blood specimens were collected from 90 COVID-19 patients and analyzed for D-dimers using SYSMEX CS-2500. Platelet MVs (PMVs; PMVCD42b+ and PMVCD41a+), monocyte MVs (MMVs; MMVCD14+), and phosphatidylserinebinding annexin V (PS, AnnV+) were analyzed using a BD FACSCalibur instrument. Results: PMV and MMV counts were significantly increased in COVID-19 patients. AnnV+ PMVCD42b+ and AnnV+ PMVCD41a+ cell counts were higher in patients with severe COVID-19 than in those with moderate clinical symptoms. The median (range) of AnnV+ PMVCD42b+ (MV/μL) in mild, moderate, and severe COVID-19 was 1,118.3 (328.1-1,910.5), 937.4 (311.4-2,909.5), and 1,298.8 (458.2-9,703.5), respectively (P =0.009). The median (range) for AnnV+ PMVCD41a+ (MV/μL) in mild, moderate, and severe disease was 885.5 (346.3-1,682.7), 663.5 (233.8-2,081.5), and 1,146.3 (333.3-10,296.6), respectively (P =0.007). D-dimer levels (ng/mL) weak correlated with AnnV+ PMVCD41a+ (P =0.047, r=0.258). Conclusions: PMV PMVCD42b+ and PMVCD41a+ counts were significantly increased in patients with severe clinical symptoms, and PMVCD41a+ counts correlated with D-dimer levels. Therefore, MV counts can be used as a potential biomarker of COVID-19 severity. [ABSTRACT FROM AUTHOR]

Published

2024

2. Soluble CD14 produced by bovine mammary epithelial cells modulates their response to full length LPS

Author

Mégane Védrine, Florence B. Gilbert, Sarah Maman, Christophe Klopp, Christophe Gitton, Pascal Rainard, and Pierre Germon

Subjects

Mammary epithelial cell, LPS, CD14, mastitis, inflammation, Escherichia coli, Veterinary medicine, SF600-1100

Abstract

Abstract Bovine mastitis remains a major disease in cattle world-wide. In the mammary gland, mammary epithelial cells (MEC) are sentinels equipped with receptors allowing them to detect and respond to the invasion by bacterial pathogens, in particular Escherichia coli. Lipopolysaccharide (LPS) is the major E. coli motif recognized by MEC through its interaction with the TLR4 receptor and the CD14 co-receptor. Previous studies have highlighted the role of soluble CD14 (sCD14) in the efficient recognition of LPS molecules possessing a full-length O-antigen (LPSS). We demonstrate here that MEC are able to secrete CD14 and are likely to contribute to the presence of sCD14 in milk. We then investigated how sCD14 modulates and is required for the response of MEC to LPSS. This study highlights the key role of sCD14 for the full activation of the Myd88-independent pathway by LPSS. We also identified several lncRNA that are activated in MEC in response to LPS, including one lncRNA showing homologies with the mir-99a-let-7c gene (MIR99AHG). Altogether, our results show that a full response to LPS by mammary epithelial cells requires sCD14 and provide detailed information on how milk sCD14 can contribute to an efficient recognition of LPS from coliform pathogens.

Published

2024

3. The Pivotal Role of Presepsin in Assessing Sepsis-Induced Cholestasis.

Author

Ghenu, Maria Iuliana, Dragoș, Dorin, Manea, Maria Mirabela, Balcangiu-Stroescu, Andra-Elena, Ionescu, Dorin, Negreanu, Lucian, and Vlad, Adelina

Subjects

*FISHER exact test, *LEUKOCYTE count, *BLOOD pressure, *ALKALINE phosphatase, *BONFERRONI correction

Abstract

Background: The serum levels of presepsin correlate with parameters indicating cholestasis in sepsis; however, the probability and significance of this association remain uncertain. We aimed to ascertain whether infection, as signaled by presepsin levels, is the primary determinant of elevated biliary parameters in sepsis. Methods: A unicenter, retrospective study included 396 COVID-free emergency-admitted patients, in which presepsin level was determined. Presepsin, neutrophil count, leukocyte count, C reactive protein, and fibrinogen evaluated the septic/inflammatory state. The statistically significant factors associated with cholestasis, ALT, and AST were analyzed by Fisher's exact test and Spearman regression with Bonferroni's correction. Results: Presepsin emerged as the most likely variable correlated with all cholestasis markers: alkaline phosphatase (p = 7 × 10−8), gamma-glutamyl transferase (p = 5 × 10−10), and conjugated bilirubin (p = 4 × 10−15). Thrombocyte count, C reactive protein, age, creatinine, urea, lactate, and blood pressure, were associated with only one or two of these markers. Conclusions: In a sepsis setting, the increase in cholestasis-related parameters is associated with presepsin with a higher probability than hemodynamic, inflammatory, or coagulation-related variables. Determining this robust link between sepsis and cholestasis could eliminate unnecessary imaging procedures in critically ill patients, enabling clinicians to focus efforts on addressing the primary infectious cause. [ABSTRACT FROM AUTHOR]

Published

2024

4. The activation of cGAS‐STING pathway causes abnormal uterine receptivity in aged mice.

Author

Chen, Si‐Ting, Shi, Wen‐Wen, Ran, Feng, Liu, Cheng‐Kan, Luo, Hui‐Na, Wu, Li‐Juan, Wu, Ying, Zhang, Tong‐Tong, and Yang, Zeng‐Ming

Subjects

*EMBRYO implantation, *NUCLEAR DNA, *PROGERIN, *OLDER women, *EPITHELIAL cells, *MATERNAL age

Abstract

Maternal age is one of the most important factors affecting the success of maternal pregnancy. Uterine aging is the leading cause of pregnancy failure in older women. However, how uterine aging affects uterine receptivity and decidualization is unclear. In this study, naturally aged one‐year‐old female mice were used to investigate effects of maternal age on embryo implantation during early pregnancy. In our study, we found abnormal uterine receptivity in aged mice. Aged mouse uterus indicates a decrease in nuclear LAMIN A, and an increase in PRELAMIN A and PROGERIN. In aged mouse uterus, double‐stranded DNA (dsDNA) in cytoplasmic fraction is significantly increased. PROGERIN overexpression in mouse uterine epithelial cells and epithelial organoids leads to nuclear DNA leakage and impaired uterine receptivity. DNase I, DNase II, and TREX1 are obviously reduced in aged mouse uterus. Treatments with foreign DNA or STING agonist significantly downregulate uterine receptivity markers and activate cGAS‐STING pathway. Uterine estrogen (E2) concentration is significantly increased in aged mice. After ovariectomized mice are treated with a high level of E2, there are significant increase of PROGERIN and cytoplasmic DNA, and activation of cGAS‐STING pathway. CD14 is significantly increased in aged uterus. Intrauterine CD14 injection inhibits embryo implantation. In vitro CD14 treatment of cultured epithelial cells or epithelial organoids decreases uterine receptivity. Uterine abnormality in aged mouse can be partially rescued by STING inhibitor. In conclusion, uterine PROGERIN increase in aged mouse uterus results in cytoplasmic DNA accumulation and cGAS‐STING pathway activation. CD14 secretion in aged uterus impairs uterine receptivity. [ABSTRACT FROM AUTHOR]

Published

2024

5. Single and Mixed Strains of Probiotics Reduced Hepatic Fat Accumulation and Inflammation and Altered Gut Microbiome in a Nonalcoholic Steatohepatitis Rat Model.

Author

Chayanupatkul, Maneerat, Machchimapiro, Panrawee, Chuaypen, Natthaya, Wanpiyarat, Natcha, Tumwasorn, Somying, Siriviriyakul, Prasong, and Werawatganon, Duangporn

Subjects

STAINS & staining (Microscopy), LABORATORY rats, LACTOBACILLUS rhamnosus, FREE fatty acids, LACTOBACILLUS plantarum

Abstract

As gut dysbiosis has been implicated in the pathogenesis of nonalcoholic steatohepatitis (NASH), probiotic supplementation might be a potential treatment for this condition. The aim of this study was to evaluate the effects of single- and mixed-strain probiotics on the severity of NASH induced by a high-fat, high-fructose (HFHF) diet and their mechanisms of action. Male Sprague–Dawley rats were divided into four groups (n = 7 per group): control group, NASH group, NASH + single-strain group, and NASH + mixed-strain group. In the single-strain and mixed-strain groups, rats received Lactobacillus plantarum B7 and Lactobacillus rhamnosus L34 + Lactobacillus paracasei B13 by oral gavage once daily, respectively. The duration of the study was 6 weeks. Liver tissue was used for histopathology, hepatic fat content was assessed by Oil Red O staining and hepatic free fatty acid (FFA), and hepatic TLR4 and CD14 expression were assessed by immunohistochemistry. Fresh feces was collected for gut microbiota analysis. Liver histology revealed a higher degree of fat accumulation, hepatocyte ballooning, and lobular inflammation in the NASH group, which improved in probiotics-treated groups. The amounts of hepatic fat droplets and hepatic FFA levels were more pronounced in the NASH group than in the control and treatment groups. Serum TNF- α levels were significantly higher in the NASH group than in control and probiotic groups. The expression of CD14 and TLR4 increased in the NASH group as compared with the control and probiotics-treated groups. Alpha diversity was reduced in the NASH group, but increased in both treatment groups. The relative abundance of Lactobacillus significantly decreased in the NASH group, but increased in both treatment groups. The relative abundance of Akkermansia significantly increased in the NASH group, but decreased in both treatment groups. In conclusion, both single-strain and mixed-strain probiotics could improve NASH histology by suppressing inflammatory responses in the liver, with this improvement potentially being associated with changes in the gut microbiota. [ABSTRACT FROM AUTHOR]

Published

2024

6. Soluble CD14 produced by bovine mammary epithelial cells modulates their response to full length LPS.

Author

Védrine, Mégane, Gilbert, Florence B., Maman, Sarah, Klopp, Christophe, Gitton, Christophe, Rainard, Pascal, and Germon, Pierre

Abstract

Bovine mastitis remains a major disease in cattle world-wide. In the mammary gland, mammary epithelial cells (MEC) are sentinels equipped with receptors allowing them to detect and respond to the invasion by bacterial pathogens, in particular Escherichia coli. Lipopolysaccharide (LPS) is the major E. coli motif recognized by MEC through its interaction with the TLR4 receptor and the CD14 co-receptor. Previous studies have highlighted the role of soluble CD14 (sCD14) in the efficient recognition of LPS molecules possessing a full-length O-antigen (LPSS). We demonstrate here that MEC are able to secrete CD14 and are likely to contribute to the presence of sCD14 in milk. We then investigated how sCD14 modulates and is required for the response of MEC to LPSS. This study highlights the key role of sCD14 for the full activation of the Myd88-independent pathway by LPSS. We also identified several lncRNA that are activated in MEC in response to LPS, including one lncRNA showing homologies with the mir-99a-let-7c gene (MIR99AHG). Altogether, our results show that a full response to LPS by mammary epithelial cells requires sCD14 and provide detailed information on how milk sCD14 can contribute to an efficient recognition of LPS from coliform pathogens. [ABSTRACT FROM AUTHOR]

Published

2024

7. Increased expression of complement C3c, iC3b, and cells containing CD11b or CD14 in experimentally induced psoriatic lesion.

Author

Rahkola, Dina, Harvima, Rauno J, and Harvima, Ilkka T

Subjects

*CD14 antigen, *IMMUNOSTAINING, *COMPLEMENT receptors, *SKIN biopsy, *SKIN diseases

Abstract

Psoriasis is a chronic inflammatory skin disease with a characteristic isomorphic reaction, i.e. the Köbner reaction, induced by slight epidermal trauma. In this study, the tape-stripping technique was used to induce the development of Köbner reaction in 18 subjects with psoriasis. Eight subjects developed a positive reaction. To study the early cellular changes, skin biopsies were taken at the baseline and subsequent time points of 2 h, 1 d, 3 d, and 7 d for the immunostaining of complement C3c, iC3b, and cells expressing complement receptor 3 (CD11b/CD18; a receptor of iC3b) or CD14. The results show that the positive Köbner reaction is associated with rapid (2 h–1 d) and sustained (3–7 d) increase in the expression of epidermal C3c and iC3b and dermal C3c. In addition, there was a positive correlation between CD11b+ and CD14+ cells in baseline and 2 h–1 d biopsies with a subsequent increase in CD11b+ and CD14+ cells in 3–7 d biopsies in the Köbner-positive group. In the Köbner-negative group, only a transient increase in epidermal iC3b at 2 h–1 d, as well as rapid (2 h–1 d) and sustained increase (3–7 d) in dermal iC3b and CD14+ cells, was observed. In experiments with cultured monolayer keratinocytes, a slight cell damage already at 30 mJ/cm2 ultraviolet B irradiation led to increased expression of C3c, but not iC3b. Therefore, there are marked differences between Köbner groups in respect to the expression of C3c, iC3b, and cells expressing CD11b or CD14. Of note is the rapid and sustained increase in epidermal C3c and iC3b in the positive Köbner reaction. The isomorphic psoriatic reaction is especially associated with rapid and sustained increase in the expression of epidermal C3c and iC3b and dermal C3c. In addition, the significant correlation between CD11b+ and CD14+ cells in 0 d and 2 h–1 d biopsies, as well as the subsequent increase in CD11b+ and CD14+ cells in 3–7 d biopsies, in the Köbner-positive group suggests that there are differences between Köbner groups in respect to dermal cellular environment already before the induction of the isomorphic psoriatic reaction. The expression of C3c immunoreactivity in cryosections from a representative Köbner-positive patient with psoriasis on day 0 (a), day 1 (b), and day 7 (c).The immunohistochemical staining of CD11b+ cells in cryosections from a Köbner-positive patient with psoriasis on day 0 (d) and day 7 (e). Graphical Abstract [ABSTRACT FROM AUTHOR]

Published

2024

8. Rosuvastatin Intervention in Patients with Chronic Hepatitis B (CHB) Expands CD14+ CD16− Classical Monocytes via Aryl Hydrocarbon Receptor (AHR).

Author

Rahmati, Mina, Zare Ebrahimabad, Mojtaba, Langari, Alale, Najafi, Ali, Taziki, Shohreh, Norouzi, Alireza, Teimoorian, Mehrdad, Khorasani, Milad, and Mohammadi, Saeed

Subjects

*CHRONIC hepatitis B, *ARYL hydrocarbon receptors, *CD14 antigen, *MONOCYTES, *MACROPHAGES

Abstract

Chronic hepatitis B (CHB) poses treatment challenges, with treatment response and disease outcome often determined by the immune response, particularly mononuclear phagocytes. Monocytes can differentiate into various subpopulations influenced by AHR. Statins, known for inflammation modulation, may impact monocyte function via AHR activation. This study explored rosuvastatin (RSV)'s effects on monocyte subtypes, inflammatory markers, and AHR in CHB patients. Fifteen CHB patients were randomly assigned to receive either 20 mg RSV or a placebo daily for three months. Flow cytometry assessed CD14+ CD16− (classical), CD14+ CD16+ (intermediate), and CD14dim CD16+ (patrolling) monocyte subtypes, along with AHR levels in each subset. ELISA quantified cytokines IL-6, IFN-γ, IL-12, IL-10, TNF-α, TGF-β, and IL-1β. RSV expanded CD14+ CD16− classical and reduced CD14+ CD16+ intermediate monocytes in CHB patients while increasing AHR+ cell percentages in all subsets. RSV treatment upregulated key AHR target genes (Cyp1a1, Cyp1b1, and ARNT), indicating robust AHR signaling activation. It also reduced pro-inflammatory cytokine levels (IL-6, IFNγ, IL-12, TNF-α) and elevated anti-inflammatory cytokines (IL-10, TGF-β). Thus, RSV may modulate the immune response by altering monocyte subtypes in CHB patients via AHR activation. [ABSTRACT FROM AUTHOR]

Published

2024

9. Melatonin alleviates aging-related heart failure through melatonin receptor 1A/B knockout in mice

Author

Zhenyu Feng, Yang Liu, Yijin Yang, Jie Bai, Qiu-yue Lin, Yun-long Xia, and Yunpeng Xie

Subjects

Cardiovascular disease, Melatonin receptor, Heart failure, CD14, Science (General), Q1-390, Social sciences (General), H1-99

Abstract

Age-related cardiovascular diseases continue to be important issues that contribute to the societal burden. Unveiling the molecular mechanisms underlying age-related cardiovascular diseases provides novel opportunities to delay aging and facilitate early disease diagnosis and treatment. This study utilized knockout mice lacking melatonin receptors type 1A (MT1) and 1B (MT2). Ultrasonography, pathological staining, and transcriptomics were used to investigate the role of MT1/2 in the hearts of aging mice. Knockout of both receptors decreased ejection fraction and exacerbated fibrosis, inflammation, oxidative stress, and apoptosis levels in aging mice. Our findings indicated that the cardiac function of MT1 knockout mice was more severely affected than that of MT2 knockout mice. Additionally, we observed that intraperitoneal administration of melatonin (20 mg/kg/day for 90 days) ameliorated abnormal cardiac function in aging mice. However, the absence of MT1/2 resulted in the inability of melatonin to improve cardiac function. Our study, utilizing an aging polymerase chain reaction assay and cell experiments, revealed that melatonin receptors potentially influence cardiac function in aging mice through their effects on leukocyte differentiation antigen 14 (CD14) expression. Consequently, melatonin receptors, particularly MT1, are key contributors to cardiac aging, and therapeutic interventions targeting this receptor are promising for delaying the progression of cardiac aging.

Published

2024

10. Rosuvastatin Intervention in Patients with Chronic Hepatitis B (CHB) Expands CD14+ CD16− Classical Monocytes via Aryl Hydrocarbon Receptor (AHR)

Author

Mina Rahmati, Mojtaba Zare Ebrahimabad, Alale Langari, Ali Najafi, Shohreh Taziki, Alireza Norouzi, Mehrdad Teimoorian, Milad Khorasani, and Saeed Mohammadi

Subjects

chronic hepatitis B (CHB), monocytes, aryl hydrocarbon receptor (AHR), rosuvastatin (RSV), CD14, CD16, Medicine

Abstract

Chronic hepatitis B (CHB) poses treatment challenges, with treatment response and disease outcome often determined by the immune response, particularly mononuclear phagocytes. Monocytes can differentiate into various subpopulations influenced by AHR. Statins, known for inflammation modulation, may impact monocyte function via AHR activation. This study explored rosuvastatin (RSV)’s effects on monocyte subtypes, inflammatory markers, and AHR in CHB patients. Fifteen CHB patients were randomly assigned to receive either 20 mg RSV or a placebo daily for three months. Flow cytometry assessed CD14+ CD16− (classical), CD14+ CD16+ (intermediate), and CD14dim CD16+ (patrolling) monocyte subtypes, along with AHR levels in each subset. ELISA quantified cytokines IL-6, IFN-γ, IL-12, IL-10, TNF-α, TGF-β, and IL-1β. RSV expanded CD14+ CD16− classical and reduced CD14+ CD16+ intermediate monocytes in CHB patients while increasing AHR+ cell percentages in all subsets. RSV treatment upregulated key AHR target genes (Cyp1a1, Cyp1b1, and ARNT), indicating robust AHR signaling activation. It also reduced pro-inflammatory cytokine levels (IL-6, IFNγ, IL-12, TNF-α) and elevated anti-inflammatory cytokines (IL-10, TGF-β). Thus, RSV may modulate the immune response by altering monocyte subtypes in CHB patients via AHR activation.

Published

2024

11. The Inflammatory Response Induced by Aspergillus fumigatus Conidia Is Dependent on Complement Activation: Insight from a Whole Blood Model

Author

Beatrice Fageräng, Maximilian Peter Götz, Leon Cyranka, Corinna Lau, Per H. Nilsson, Tom Eirik Mollnes, and Peter Garred

Subjects

aspergillus fumigatus, inflammatory response, complement, toll-like receptors, cd14, cytokines, Medicine, Internal medicine, RC31-1245

Abstract

Introduction: We aimed to elucidate the inflammatory response of Aspergillus fumigatus conidia in a whole-blood model of innate immune activation and to compare it with the well-characterized inflammatory reaction to Escherichia coli. Methods: Employing a human lepirudin whole-blood model, we analyzed complement and leukocyte activation by measuring the sC5b-9 complex and assessing CD11b expression. A 27-multiplex system was used for quantification of cytokines. Selective cell removal from whole blood and inhibition of C3, C5, and CD14 were also applied. Results: Our findings demonstrated a marked elevation in sC5b-9 and CD11b post-A. fumigatus incubation. Thirteen cytokines (TNF, IL-1β, IL-1ra, IL-4, IL-6, IL-8, IL-17, IFNγ, MCP-1, MIP-1α, MIP-1β, FGF-basic, and G-CSF) showed increased levels. A generally lower level of cytokine release and CD11b expression was observed with A. fumigatus conidia than with E. coli. Notably, monocytes were instrumental in releasing all cytokines except MCP-1. IL-1ra was found to be both monocyte and granulocyte-dependent. Pre-inhibiting with C3 and CD14 inhibitors resulted in decreased release patterns for six cytokines (TNF, IL-1β, IL-6, IL-8, MIP-1α, and MIP-1β), with minimal effects by C5-inhibition. Conclusion: A. fumigatus conidia induced complement activation comparable to E. coli, whereas CD11b expression and cytokine release were lower, underscoring distinct inflammatory responses between these pathogens. Complement C3 inhibition attenuated cytokine release indicating a C3-level role of complement in A. fumigatus immunity.

Published

2024

12. Lysophosphatidylcholine Acetyltransferase 2 (LPCAT2) Influences the Gene Expression of the Lipopolysaccharide Receptor Complex in Infected RAW264.7 Macrophages, Depending on the E. coli Lipopolysaccharide Serotype.

Author

Poloamina, Victory Ibigo, Alrammah, Hanaa, Abate, Wondwossen, Avent, Neil D., Fejer, Gyorgy, and Jackson, Simon K.

Subjects

*ESCHERICHIA coli, *GENE expression, *LIPID rafts, *CELL membranes, *MACROPHAGES, *MYELOID differentiation factor 88, *LIPOPOLYSACCHARIDES

Abstract

Simple Summary: E. coli harms over 100 million patients worldwide annually. Its toxin component is lipopolysaccharide, which has various forms, referred to as smooth or rough, based on their structure. Macrophages' main function is to eat up foreign organisms through phagocytosis. This process requires membrane fluidity, which means the phospholipid in the macrophage plasma membrane needs to be regularly remodelled. A lipid-modifying enzyme known as LPCAT2 performs phospholipid remodelling and participates in inflammation. Here, we studied how this enzyme influences the gene expression of receptors that recognise and bind to lipopolysaccharides. These receptors are TLR4, CD14, and MD2. Our results show that LPCAT2 only influenced these receptors when macrophages were infected with smooth lipopolysaccharides. We conclude that LPCAT2 does not influence the gene expression of the receptors in macrophages infected with rough lipopolysaccharides because they do not require lipid-raft microdomains to mediate inflammation, but smooth lipopolysaccharides do. Escherichia coli (E. coli) is a frequent gram-negative bacterium that causes nosocomial infections, affecting more than 100 million patients annually worldwide. Bacterial lipopolysaccharide (LPS) from E. coli binds to toll-like receptor 4 (TLR4) and its co-receptor's cluster of differentiation protein 14 (CD14) and myeloid differentiation factor 2 (MD2), collectively known as the LPS receptor complex. LPCAT2 participates in lipid-raft assembly by phospholipid remodelling. Previous research has proven that LPCAT2 co-localises in lipid rafts with TLR4 and regulates macrophage inflammatory response. However, no published evidence exists of the influence of LPCAT2 on the gene expression of the LPS receptor complex induced by smooth or rough bacterial serotypes. We used RAW264.7—a commonly used experimental murine macrophage model—to study the effects of LPCAT2 on the LPS receptor complex by transiently silencing the LPCAT2 gene, infecting the macrophages with either smooth or rough LPS, and quantifying gene expression. LPCAT2 only significantly affected the gene expression of the LPS receptor complex in macrophages infected with smooth LPS. This study provides novel evidence that the influence of LPCAT2 on macrophage inflammatory response to bacterial infection depends on the LPS serotype, and it supports previous evidence that LPCAT2 regulates inflammatory response by modulating protein translocation to lipid rafts. [ABSTRACT FROM AUTHOR]

Published

2024

13. Virion-incorporated CD14 enables HIV-1 to bind LPS and initiate TLR4 signaling in immune cells.

Author

Persaud, Arvin T., Khela, Jasmin, Fernandes, Claire, Chaphekar, Deepa, Burnie, Jonathan, Tang, Vera A., Colpitts, Che C., and Guzzo, Christina

Subjects

*HIV, *CD14 antigen, *TUMOR necrosis factors, *TOLL-like receptors, *HOST-virus relationships, *LIPOPOLYSACCHARIDES

Abstract

HIV-1 has a broad range of nuanced interactions with the immune system, and the incorporation of cellular proteins by nascent virions continues to redefine our understanding of the virus-host relationship. Proteins located at the sites of viral egress can be selectively incorporated into the HIV-1 envelope, imparting new functions and phenotypes onto virions, and impacting viral spread and disease. Using virion capture assays and western blot, we show that HIV-1 can incorporate the myeloid antigen CD14 into its viral envelope. Virion-incorporated CD14 remained biologically active and able to bind its natural ligand, bacterial lipopolysaccharide (LPS), as demonstrated by flow virometry and immunoprecipitation assays. Using a Toll-like receptor 4 (TLR4) reporter cell line, we also demonstrated that virions with bound LPS can trigger TLR4 signaling to activate transcription factors that regulate inflammatory gene expression. Complementary assays with THP-1 monocytes demonstrated enhanced secretion of inflammatory cytokines like tumor necrosis factor alpha (TNF-α) and the C-C chemokine ligand 5 (CCL5), when exposed to LPS-loaded virus. These data highlight a new type of interplay between HIV-1 and the myeloid cell compartment, a previously well-established cellular contributor to HIV-1 pathogenesis and inflammation. Persistent gut inflammation is a hallmark of chronic HIV-1 infection, and contributing to this effect is the translocation of microbes across the gut epithelium. Our data herein provide proof of principle that virion-incorporated CD14 could be a novel mechanism through which HIV-1 can drive chronic inflammation, facilitated by HIV-1 particles binding bacterial LPS and initiating inflammatory signaling in TLR4-expressing cells. [ABSTRACT FROM AUTHOR]

Published

2024

14. Controversies associated with the identification of the true origins of human neutrophils.

Author

Silvestre-Roig, Carlos and Brandau, Sven

Subjects

NEUTROPHILS, HUMAN origins, BONE marrow cells, MYELOID cells, GRANULOCYTE-colony stimulating factor

Abstract

This article discusses the controversies surrounding the identification of the true origins of human neutrophils. Neutrophils and monocytes are important components of the innate immune system and play a crucial role in responding to foreign microorganisms and tissue perturbations. The article explores two alternative scenarios for the regulation of neutrophil and monocyte production, and discusses the use of novel technologies to better understand the developmental steps and lineage commitment of these cells. The study presented in the article provides evidence that human neutrophil-committed progenitors are indeed committed to neutrophil production and do not give rise to monocytic cells. The article emphasizes the phenotypic plasticity of human myeloid cells and the importance of using multiple experimental approaches to study their development. [Extracted from the article]

Published

2024

15. The Potential Role of Presepsin in Predicting Severe Infection in Patients with Diabetic Foot Ulcers.

Author

Ha, Eun Yeong, Park, Il Rae, Chung, Seung Min, Roh, Young Nam, Park, Chul Hyun, Kim, Tae-Gon, Kim, Woong, and Moon, Jun Sung

Subjects

*DIABETIC foot, *FOOT diseases, *PEOPLE with diabetes, *FOOT amputation, *LEUCOCYTES, *DIABETES complications

Abstract

Background/Objectives: Diabetic foot ulcers are one of the complications in patients with diabetes, which can be caused by infection, neuropathy, and blood vessel disorder. Among them, infection is the most common cause, and if it becomes worse, amputation may be necessary. So, it is important to detect and treat infections early, and determining indicators that can confirm infection is also important. Known infection markers include white blood cells (WBCs), the erythrocyte sediment rate (ESR), C-reactive protein (CRP), and procalcitonin, but they are not specific to diabetic foot ulcers. Presepsin, also known as soluble CD14, is known to be an early indicator of sepsis. Recent studies have reported that presepsin can be used as an early indicator of infection. This study investigated whether presepsin could be used as an early marker of severe infection in patients with diabetic foot ulcers. Methods: We retrospectively studied 73 patients who were treated for diabetic foot ulcerations from January 2021 to June 2023 at Yeungnam University Hospital. Results: Out of a total of 73 patients, 46 patients underwent amputations with severe infections, and the WBC level, ESR, and CRP, procalcitonin, and presepsin levels were significantly higher in the group of patients who underwent amputations. The cutoff of presepsin, which can predict serious infections that need amputation, was 675 ng/mL. A regression analysis confirmed that presepsin, HbA1c, and osteomyelitis significantly increased the risk of severe infections requiring amputation. Conclusions: Presepsin will be available as an early predictor of patients with severe infections requiring amputations for diabetic foot ulcerations. [ABSTRACT FROM AUTHOR]

Published

2024

16. Association analysis between CD14 gene polymorphisms and peri‐implantitis susceptibility in a Chinese population.

Author

Li, Jie, Qiao, Xiao, and Shang, Jin

Subjects

*GENETIC polymorphisms, *CHINESE people, *CD14 antigen, *PERI-implantitis, *PERIODONTAL pockets, *GENETIC correlations

Abstract

Objective: The goal of the study was to examine the genetic correlation of cluster of differentiation 14 (CD14) gene polymorphisms with peri‐implantitis (PI) predisposition in a Chinese Han population. Methods: In the case‐control study, blood samples were collected from PI patients and healthy individuals (n = 120/group), who were admitted to the Affiliated Hospital of Yangzhou University from 2021 to 2023. One‐way analysis of variance (ANOVA) was applied to compare differences of continuous variables among different groups. Genotype and allele distributions of CD14 gene rs2569190 and rs2915863 polymorphisms were analyzed between groups via χ2 test. Results: A high percentage of rs2569190 GG genotype or G allele carriers were identified in PI group compared with control group (p <.01). Rs2569190 GG genotype carriers had high risk to develop PI (odds ratio: 2.545, 95% confidence interval: 1.257–5.156, p =.009). The rs2569190 AA genotype carriers had the lowest values of gingival index, plaque index, calculus index, peri‐implant pocket depth, and clinical attachment level, which were the highest in cases with GG genotype. Conclusion: Rs2569190 polymorphism of CD14 gene was significantly associated with PI predisposition in the Chinese Han population, and the GG genotype and G allele were risk factors for the development of PI. [ABSTRACT FROM AUTHOR]

Published

2024

17. The Prognostic Impact of Tumor Microenvironment and Checkpoint Blockade-Associated Molecules (PD-1, PD-L1, CD163 and CD14) in Nodal Diffuse Large B-cell Lymphoma, NOS.

Author

Atmış, Ömer, Neşe, Nalan, Aydoğdu, İsmet, Alaca, İlknur, Mavili, Hanife Seda, and İşisağ, Aydın

Abstract

It is aimed to determine expression of programmed cell death-1 (PD-1), programmed cell death ligand-1 (PD-L1), CD163 and CD14 in diffuse large B-cell lymphomas (DLBCL), and whether these markers may predict prognosis in DLBCL cases. A total of 52 nodal DLBCL, NOS cases with no known extranodal involvement at the time of diagnosis were evaluated. PD-1, PD-L1, CD163, and CD14 were studied by immunohistochemistry. The relationships between the results and clinical and laboratory prognostic markers were investigated. It was observed that patients with PD-1 expression < 5 positive cells/HPF had worse overall survival. No significant relationship was found between survival and PD-L1, CD163 and CD14 expressions. In addition, cases that are > 60 years of age, that have Eastern Cooperative Oncology Group (ECOG) performance score ≥ 2, stage IV disease, high International Prognostic Index score score (≥ 3), elevation of LDH, low albumin level, low hemoglobin level, low peripheral blood lymphocyte count, high peripheral blood neutrophil/lymphocyte ratio, high peripheral blood platelet/lymphocyte ratio were found to have worse overall survival. It was concluded that in patients with low number of PD-1 positive tumor-infiltrating lymphocytes have low survival rates and therefore PD-1 expression may be useful in indicating prognosis. [ABSTRACT FROM AUTHOR]

Published

2024

18. Homodimeric Granzyme A Opsonizes Mycobacterium tuberculosis and Inhibits Its Intracellular Growth in Human Monocytes via Toll-Like Receptor 4 and CD14.

Author

Rasi, Valerio, Phelps, Kathleen R, Paulson, Keegan R, Eickhoff, Christopher S, Chinnaraj, Mathivanan, Pozzi, Nicola, Gioia, Marco Di, Zanoni, Ivan, Shakya, Shubha, Carlson, Haley L, Ford, David A, Kolar, Grant R, and Hoft, Daniel F

Abstract

Mycobacterium tuberculosis (Mtb)-specific γ9δ2 T cells secrete granzyme A (GzmA) protective against intracellular Mtb growth. However, GzmA-enzymatic activity is unnecessary for pathogen inhibition, and the mechanisms of GzmA-mediated protection remain unknown. We show that GzmA homodimerization is essential for opsonization of mycobacteria, altered uptake into human monocytes, and subsequent pathogen clearance within the phagolysosome. Although monomeric and homodimeric GzmA bind mycobacteria, only homodimers also bind cluster of differentiation 14 (CD14) and Toll-like receptor 4 (TLR4). Without access to surface-expressed CD14 and TLR4, GzmA fails to inhibit intracellular Mtb. Upregulation of Rab11FIP1 was associated with inhibitory activity. Furthermore, GzmA colocalized with and was regulated by protein disulfide isomerase AI (PDIA1), which cleaves GzmA homodimers into monomers and prevents Mtb inhibitory activity. These studies identify a previously unrecognized role for homodimeric GzmA structure in opsonization, phagocytosis, and elimination of Mtb in human monocytes, and they highlight PDIA1 as a potential host-directed therapy for prevention and treatment of tuberculosis, a major human disease. [ABSTRACT FROM AUTHOR]

Published

2024

19. Predictive accuracy of histopathological profile and immunohistochemical markers for the aging of abrasion: an autopsy-based study.

Author

Pan, Arpan Kumar, Chaudhari, Vinod Ashok, Das, Siddhartha, Gochhait, Debasis, Sontakke, Yogesh Ashok, and Harichandrakumar, K. T.

Subjects

*HEMATOXYLIN & eosin staining, *FORENSIC pathologists, *HISTOPATHOLOGY, *IMMUNOHISTOCHEMISTRY, *GRANULATION tissue, *POSTMORTEM changes

Abstract

Wound age estimation is a crucial medicolegal task for forensic pathologists. The main objective of the current study was to evaluate the ability of the histopathological profile and immunohistochemical markers (CD14 and IL-8) to predict the age of abrasion and, furthermore, identify the relationship between the histopathological profile and immunohistochemical markers in abrasion aging. The study involved postmortem cases (n = 246) of abrasion injuries in which the injury infliction time was known. The test skin samples were taken from the abrasion site, and an adjacent area of uninjured skin was sampled for control. Hematoxylin and eosin stain was applied to tissue sections for the histopathological analysis. The semi-quantitative evaluation was made for expressing immunohistochemical markers CD14 and IL-8 on the infiltrating inflammatory cells. The study showed that the age of abrasion was significantly higher (p < 0.05) among the cases with positive staining than those with negative staining for both CD14 and IL-8. Additionally, the study found a significant association between the age of the abrasion and the IHC staining for IL-8. However, no significant association was seen between the age of abrasion and the CD-14 IHC staining. The odds ratio (95% confidence interval) for more than 72 h of the age of abrasion was compared to 0 to 72 h of the age of abrasion. The odds ratios were 39.00 (4.177–364.13) for the predominant mononuclear cell infiltration and 84.50 (9.287–768.814) for cases with the appearance of fibroblast, granulation tissue, and collagen deposition when compared to an unremarkable change on histopathological examination. Positive staining of immunohistochemical markers CD14 and IL-8 for the age of abrasion of more than 72 h showed a sensitivity of 40% and 80.95%, respectively, and specificity of 71.6% and 52.5%, respectively. The quantification of the histopathological changes of predominant mononuclear cell infiltration and the appearance of fibroblast, granulation tissue formation, and collagen deposition showed a significant correlation for the age of abrasion of more than 72 h. The immunohistochemical analysis revealed IL-8 as a more accurate marker than CD14 in identifying abrasions older than 72 h. [ABSTRACT FROM AUTHOR]

Published

2024

20. The impact of glycosylation on the structure, function, and interactions of CD14.

Author

Quintana, Jon Imanol, Delgado, Sandra, Rábano, Miriam, Azkargorta, Mikel, Florencio-Zabaleta, Mirane, Unione, Luca, Vivanco, Maria dM, Elortza, Félix, Jiménez-Barbero, Jesús, and Ardá, Ana

Subjects

*CD14 antigen, *PROTEIN folding, *CELL differentiation, *FUCOSYLATION, *GLYCOSIDASES

Abstract

CD14 is an innate immune receptor that senses pathogen-associated molecular patterns, such as lipopolysaccharide, to activate the innate immune response. Although CD14 is known to be glycosylated, detailed understanding about the structural and functional significance of this modification is still missing. Herein, an NMR and MS-based study, assisted by MD simulations, has provided a 3D-structural model of glycosylated CD14. Our results reveal the existence of a key N-glycosylation site at Asn282 that exclusively contains unprocessed oligomannnose N-glycans that perfectly fit the concave cavity of the bent-solenoid shaped protein. This site is not accessible to glycosidases and is fundamental for protein folding and secretion. A second N-site at Asn151 displays mostly complex N-glycans, with the typical terminal epitopes of the host cell-line expression system (i.e. βGal, α2,3 and α2,6 sialylated βGal, here), but also particularities, such as the lack of core fucosylation. The glycan at this site points outside the protein surface, resulting in N-glycoforms fully exposed and available for interactions with lectins. In fact, NMR experiments show that galectin-4, proposed as a binder of CD14 on monocytes to induce their differentiation into macrophages-like cells, interacts in vitro with CD14 through the recognition of the terminal glycoepitopes on Asn151. This work provides key information about CD14 glycosylation, which helps to better understand its functional roles and significance. Although protein glycosylation is known to be dynamic and influenced by many factors, some of the features found herein (presence of unprocessed N-glycans and lack of core Fuc) are likely to be protein specific. [ABSTRACT FROM AUTHOR]

Published

2024

21. HDAC6 inhibitor ACY-1215 protects from nonalcoholic fatty liver disease via inhibiting CD14/TLR4/MyD88/MAPK/NFκB signal pathway

Author

Shifeng Fu, Mengmeng Xu, Jianglei Li, Meihong Yu, Siyi Wang, Liu Han, Rong Li, Feihong Deng, Hailing Peng, Deliang Liu, and Yuyong Tan

Subjects

Nonalcoholic fatty liver disease, Histone deacetylation 6, ACY-1215, CD14, TLR4, Science (General), Q1-390, Social sciences (General), H1-99

Abstract

Background & aims: Nonalcoholic fatty liver disease (NAFLD) is a chronic liver disease characterized by hepatic steatosis, for which there is currently no effective treatment. ACY-1215 is a selective inhibitor of histone deacetylation 6, which has shown therapeutic potential in many tumors, as well as acute liver injury. However, no research about ACY-1215 on NAFLD has been published. Therefore, our study aims to explore the role and mechanism of ACY-1215 in the experimental model of NAFLD, to propose a new treatment strategy for NAFLD. Methods: We established cell and animal models of NAFLD and verified the effect of ACY-1215 on NAFLD. The mechanism of ACY-1215 on NAFLD was preliminarily explored through TMT relative quantitative proteomics, and then we verify the mechanism discovered in the experimental model of NAFLD. Results: ACY-1215 can reduce lipid aggregation, IL-1β, and TNF α mRNA levels in liver cells in vitro. ACY-1215 can reduce the weight gain and steatosis in the liver of the NAFLD mouse model, alleviate the deterioration of liver function, and reduce IL-1βs and TNF α mRNA levels in hepatocytes. TMT relative quantitative proteomics found that ACY-1215 decreased the expression of CD14 in hepatocytes. It was found that ACY-1215 can inhibit the activation level of CD14/TLR4/MyD88/MAPK/NFκB pathway in the NAFLD experimental model. Conclusions: ACY-1215 has a protective effect on the cellular model of NAFLD induced by fatty acids and lipopolysaccharide, as well as the C57BL/6J mouse model induced by a high-fat diet. ACY-1215 may play a protective role by inhibiting CD14/TLR4/MyD88/MAPK/NFκB signal pathway.

Published

2024

22. Bovine CD14 gene polymorphism and its association with milk yield, milk constituents and somatic cell count in holstein friesian crossbred and gir cows

Author

Parashar, Raghav, Tomar, Satyendra Singh, Nagoriya, Sunil Kumar, Khan, Zeeshan Ahmed, and Jha, Amit Kumar

Published

2023

23. <italic>IL-18</italic> and <italic>CD14</italic> variants in chronic HBV predisposition: a case-control study with <italic>in silico</italic> analyses focused on transcription and splicing.

Author

Sarhadi, Mohammad, Pahlavani, Elham, Hosseini Razavi, Niloufar, Ghadyani, Fatemeh, Abdollahi, Zahra, Sarhadi, Somayeh, Sabeti Akbar Abad, Mahboobeh, Shahriari, Hossein, and Majidpour, Mahdi

Abstract

AbstractHepatitis B virus (HBV), a vaccine-avoidable infection, is a health concern worldwide, leading to liver disorders such as acute self-constraint and chronic hepatitis, liver failure, hepatic cirrhosis, and even hepatocellular carcinoma if untreated. ‘Immunogeneticprofiling’, genetic variations of the pro- and anti-inflammatory cytokines responsible for regulating the immune responses, cause person-to-person differences and impact the clinical manifestation of the disease. The current experimental–bioinformatics research was conducted to examine whether promoteric IL-18–rs187238 C > G and –rs1946518 T > G and intronic CD14–rs2569190 A > G variations are associated with chronic HBV. A total of 400 individuals (200 in each case and control group) participated in the study and were genotyped using the polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) technique. The data was also assessed bioinformatics-wise for conservation, genomic transcription and splicing, and protein interactions. Findings proposed that unlike the IL-18–rs1946518 T > G and CD14–rs2569190 A > G, the IL-18–rs187238 C > G is a protector against chronic HBV (odds ratio [OR] = 0.62, 95% confidence intervals [CI]: 0.46–0.83, and p = 0.002). The TG/CC/AA, TG/CC/AG, TT/CC/AG, and GG/CC/AA combined genotypes significantly increased chronic HBV risk (p < 0.05), while the IL-18 G/T and G/G haplotypes lessened it (p < 0.05). Moreover, IL-18–rs1946518 T > G is in the protected genomic regions across mammalian species. In contrast to the IL-18–rs1946518 T > G, IL-18–rs187238 C > G is likely to create novel binding sites for transcription factors, and the CD14–rs2569190 A > G presumably changed the ribonucleic acid splicing pattern. More research on larger populations and other ethnicities is required to authenticate these results. [ABSTRACT FROM AUTHOR]

Published

2024

24. CD14 down‐modulation as a real‐time biomarker in Kawasaki disease.

Author

Inada, Yutaro, Sonoda, Motoshi, Mizuno, Yumi, Yamamura, Kenichiro, Motomura, Yoshitomo, Takuma, Aoba, Murata, Kenji, Furuno, Kenji, Tezuka, Junichiro, Sakai, Yasunari, Ohga, Shouichi, Kishimoto, Junji, Hosaka, Koki, Sakata, Satomi, and Hara, Toshiro

Abstract

Objectives: The objectives of this study were to investigate the pathophysiology of Kawasaki disease (KD) from immunological and oxidative stress perspectives, and to identify real‐time biomarkers linked to innate immunity and oxidative stress in KD. Methods: We prospectively enrolled 85 patients with KD and 135 patients with diverse conditions including immune, infectious and non‐infectious diseases for this investigation. Flow cytometry was used to analyse the surface expression of CD14, CD38 and CD62L on monocytes, along with a quantitative assessment of CD14 down‐modulation. Additionally, oxidative stress levels were evaluated using derivatives of reactive oxygen metabolites (d‐ROMs) and antioxidant capacity measured by a free radical elective evaluator system. Results: During the acute phase of KD, we observed a prominent CD14 down‐modulation on monocytes, reflecting the indirect detection of circulating innate immune molecular patterns. Moreover, patients with KD showed a significantly higher CD14 down‐modulation compared with infectious and non‐infectious disease controls. Notably, the surface expression of CD14 on monocytes was restored concurrently with responses to intravenous immunoglobulin and infliximab treatment in KD. Furthermore, d‐ROM levels in patients with KD were significantly elevated compared with patients with infectious and non‐infectious diseases. Following intravenous immunoglobulin treatment, oxidative stress levels decreased in patients with KD. Conclusion: Monitoring CD14 down‐modulation on monocytes in real‐time is a valuable strategy for assessing treatment response, distinguishing KD relapse from concomitant infections and selecting second‐line therapy after IVIG treatment in KD patients. The interplay between inflammation and oxidative stress likely plays a crucial role in the development of KD. [ABSTRACT FROM AUTHOR]

Published

2024

25. Multifaceted role of CD14 in innate immunity and tissue homeostasis.

Author

Na, Kunhee, Oh, Byung-Chul, and Jung, YunJae

Subjects

*CD14 antigen, *NATURAL immunity, *INFLAMMATORY bowel diseases, *PHOSPHOINOSITIDES, *DENDRITIC cells, *GASTROINTESTINAL system

Abstract

CD14 is a co-receptor of Toll-like receptor (TLR)− 4, with a critical role in innate immune responses. CD14 recognizes bacterial lipopolysaccharides, pathogen-, and damage-associated molecular patterns, thereby facilitating inflammatory immune responses. In addition to its well-established association with TLR4, CD14 is also implicated in TLR4-independent signaling, which leads to the apoptotic death of differentiated dendritic cells and activation of the noncanonical inflammasome pathway. CD14 also has a role beyond that of the immune responses. It contributes to tissue homeostasis by promoting the clearance of various apoptotic cells via recognizing externalized phosphatidylinositol phosphates. CD14 also has context-dependent roles, particularly in barrier tissues that include the skin and gastrointestinal tract. For example, CD14+ dendritic cells in the skin can induce immunostimulatory or immunosuppressive responses. In the gastrointestinal system, CD14 is involved in producing inflammatory cytokines in inflammatory bowel disease and maintaining of intestinal integrity. This review focuses on the multifaceted roles of CD14 in innate immunity and its potential regulatory functions in barrier tissues characterized by rapid cell renewal. By providing insights into the diverse functions of CD14, this review offers potential therapeutic implications for this versatile molecule in immune modulation and tissue homeostasis. • CD14, a co-receptor for TLR4, recognizes LPS, PAMPs, and DAMPs in innate immunity. • CD14 has a role in TLR4-dependent and TLR4-independent signaling pathways. • CD14 helps clear apoptotic cells by recognizing phospholipids externalized on the cell surface. • In barrier tissues, CD14 can mediate inflammatory and tolerogenic responses. • Knowledge of CD14 ligand interactions will inform specifically directed therapies. [ABSTRACT FROM AUTHOR]

Published

2023

26. Association of serum CD14 level and functional polymorphism C-159T in the promoter region of CD14 gene with allergic rhinitis.

Author

Kamel, Mai A., Selim, Elham S., Tantawy, Enas A., Elgendy, Aya, Abdulmageed, Alsayed, and Anis, Reham H.

Subjects

*CD14 antigen, *ALLERGIC rhinitis, *PROMOTERS (Genetics), *NASAL mucosa, *EGYPTIANS, *LIPOPOLYSACCHARIDES

Abstract

Allergic rhinitis (AR) is an inflammatory disease of the upper respiratory tract affecting a significant number of the world's population. It occurs as an IgE-mediated immune response of the nasal mucosa to inhaled allergens. The human Cluster of Differentiation 14 (CD14) is a glycosyl-phosphatidylinositol-anchored molecule expressed on the surface of monocytes and macrophages and functions as a receptor to lipopolysaccharides and inhaled endotoxins that may stimulate interleukins production by antigen-presenting cells. Consequently, CD14 plays a substantial role in allergic diseases and may become one of their etiological causes. This study aimed to determine the association between C-159T polymorphism in the CD14 gene promoter region and serum CD14 levels and the risk of Allergic rhinitis Egyptian patients and to test the validity of serum CD14 level measurement in predicting AR. This case–control study included 45 patients with AR referred to Allergy and Immunology Unit, Zagazig University Hospital, Zagazig, Egypt, and 45 healthy subjects as controls. Serum CD14 levels were measured by ELISA. The polymerase chain reaction-restriction fragment length polymorphism technique was used to detect C-159T gene polymorphism in the CD14 promoter region. There was a significant association between CD14 serum levels and AR incidence (P < 0.001), with patients having higher serum CD14 levels than controls. In addition, a significant association (P < 0.001) was detected between serum CD14 levels and the severity of AR, as well as elevated serum CD14 levels in severe and the most severe cases. On the molecular level, there was a statistically significant relationship between patients and the control group regarding the CD14 genotype (P < 0.001), where CT and TT genotypes and T allele were primarily associated with the cases group, indicating that the risk of AR was significantly associated with the inheritance of the TT genotype. Additionally, a statistically significant association was found between the severity of AR and CD14 genotype (P < 0.001), where TT genotypes were mainly associated with severe and the most severe cases. In the studied groups, there was a statistically significant difference (P < 0.05) between the CD14 genotype and serum CD14 levels, with TT genotypes being associated with higher CD14 levels. The results obtained in this study revealed that serum CD14 level is a potential biomarker for the diagnosis of AR and, at the genetic level, a potential predictor of disease. [ABSTRACT FROM AUTHOR]

Published

2023

27. Non‐invasive omics analysis delineates molecular changes in water‐only fasting and its sex‐discriminating features in metabolic syndrome patients.

Author

Jiang, Yanyu, Tang, Zhimei, Zhu, Xiaogang, Xiao, Biying, Tian, Hechuan, Lei, Xingxing, Peng, Huan, Qin, Jun, Zhang, Yanmei, Hoffman, Robert M., Hu, Xiaorong, Chen, Qiu, Ji, Guang, and Jia, Lijun

Subjects

METABOLIC syndrome, FASTING, KREBS cycle, CD14 antigen, PATHOLOGICAL physiology

Abstract

Fasting has been grown in popularity with multiple potential benefits. However, very few studies dynamically monitor physiological and pathological changes during long‐term fasting using noninvasive methods. In the present study, we recruited 37 individuals with metabolic syndrome to engage in a 5‐day water‐only fasting regimen, and simultaneously captured the molecular alterations through urinary proteomics and metabolomics. Our findings reveal that water‐only fasting significantly mitigated metabolic syndrome‐related risk markers, such as body weight, body mass index, abdominal circumference, blood pressure, and fasting blood glucose levels in metabolic syndrome patients. Indicators of liver and renal function remained within the normal range, with the exception of uric acid. Notably, inflammatory response was inhibited during the water‐only fasting period, as evidenced by a decrease in the human monocyte differentiation antigen CD14. Intriguingly, glycolysis, tricarboxylic acid cycle, and oxidative phosphorylation underwent a sex‐dependent reprogramming throughout the fasting period, whereby males exhibited a greater upregulation of carbohydrate metabolism‐related enzymes than females. This disparity may be attributed to evolutionary pressures. Collectively, our study sheds light on the beneficial physiological effects and novel dynamic molecular features associated with fasting in individuals with metabolic syndrome using noninvasive methods. [ABSTRACT FROM AUTHOR]

Published

2023

28. CD14 facilitates perinatal human cytomegalovirus infection in biliary epithelial cells via CD55

Author

Liang Su, Yan Chen, Ming Fu, Hezhen Wang, Yanlu Tong, Zefeng Lin, Hongjiao Chen, Huiting Lin, Yi Chen, Bing Zhu, Sige Ma, Yiyi Xiao, Junyu Huang, Ziyang Zhao, Fenjie Li, Rongchen Ye, Hongguang Shi, Zhe Wang, Jixiao Zeng, Zhe Wen, Minhua Luo, Huimin Xia, and Ruizhong Zhang

Subjects

Cytomegalovirus, Perinatal period, CD14, CD55, Biliary epithelial cells, PARP-1, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Background & Aims: A high human cytomegalovirus (HCMV) infection rate accompanied by an increased level of bile duct damage is observed in the perinatal period. The possible mechanism was investigated. Methods: A total of 1,120 HCMV-positive and 9,297 HCMV-negative children were recruited, and depending on age, their liver biochemistry profile was compared. Fetal and infant biliary epithelial cells (F-BECs and I-BECs, respectively) were infected with HCMV, and the differences in cells were revealed by proteomic analysis. Protein–protein interactions were examined by coimmunoprecipitation and mass spectrometry analyses. A murine cytomegalovirus (MCMV) infection model was established to assess treatment effects. Results: Perinatal HCMV infection significantly increased the level of bile duct damage. Neonatal BALB/c mice inoculated with MCMV showed obvious inflammation in the portal area with an abnormal bile duct structure. Proteomics analysis showed higher CD14 expression in F-BECs than in I-BECs. CD14 siRNA administration hindered HCMV infection, and CD14-knockout mice showed lower MCMV-induced bile duct damage. HCMV infection upregulated CD55 and poly ADP-ribose polymerase-1 (PARP-1) expression in F-BECs. Coimmunoprecipitation and mass spectrometry analyses revealed formation of the CD14–CD55 complex. siRNA-mediated inhibition of CD55 expression reduced sCD14-promoted HCMV replication in F-BECs. In MCMV-infected mice, anti-mouse CD14 antibody and PARP-1 inhibitor treatment diminished cell death, ameliorated bile duct damage, and reduced mortality. Conclusions: CD14 facilitates perinatal HCMV infection in BECs via CD55, and PARP-1-mediated cell death was detected in perinatal cytomegalovirus-infected BECs. These results provide new insight into the treatment of perinatal HCMV infection with bile duct damage. Impact and implications: Perinatal human cytomegalovirus (HCMV) infection is associated with bile duct damage, but the underlying mechanism is still unknown. We discovered that CD14 expression is increased in biliary epithelial cells during perinatal HCMV infection and facilitates viral entry through CD55. We also detected PARP-1-mediated cell death in perinatal HCMV-infected biliary epithelial cells. We showed that blocking CD14 or inhibiting PARP-1 reduced bile duct damage and mortality in a mouse model of murine cytomegalovirus infection. Our findings provide a new insight into therapeutic strategies for perinatal HCMV infection.

Published

2024

29. Association analysis between CD14 gene polymorphisms and peri‐implantitis susceptibility in a Chinese population

Author

Jie Li, Xiao Qiao, and Jin Shang

Subjects

CD14, peri‐implantitis, polymorphism, susceptibility, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Objective The goal of the study was to examine the genetic correlation of cluster of differentiation 14 (CD14) gene polymorphisms with peri‐implantitis (PI) predisposition in a Chinese Han population. Methods In the case‐control study, blood samples were collected from PI patients and healthy individuals (n = 120/group), who were admitted to the Affiliated Hospital of Yangzhou University from 2021 to 2023. One‐way analysis of variance (ANOVA) was applied to compare differences of continuous variables among different groups. Genotype and allele distributions of CD14 gene rs2569190 and rs2915863 polymorphisms were analyzed between groups via χ2 test. Results A high percentage of rs2569190 GG genotype or G allele carriers were identified in PI group compared with control group (p

Published

2024

30. Severity of Schistosoma haematobium co-infection with malaria in school-children is potentially modulated by host CD14 gene variants

Author

Mary A. Oboh-Imafidon, Sabrina M. Torbit, Swathi Jacob, Marissa N. Schroeter, Ashley R. Tucker, Olusola Ojurongbe, and Bolaji N. Thomas

Subjects

Schistosomiasis, Co-infection, Malaria, CD14, Innate immunity, Variants, Medicine, Biology (General), QH301-705.5, Science (General), Q1-390

Abstract

Abstract Objective Schistosomiasis remains a chronic disease of global importance, especially in many rural areas of the world where co-infection with Plasmodium falciparum is common. It is critical to decipher the role of single or co-infected disease scenarios on immune system regulation in such individuals and how such co-infections can either ameliorate or complicate immune response and the consequent disease outcome. First, 10 ml of urine samples, collected between 10:00 am and 2:00 pm, was filtered for diagnosis of schistosomiasis, while egg count, indicative of disease severity, was determined by microscopy. Furthermore, genomic DNA samples extracted from dried blood spots collected on filter paper from one hundred and forty-four Schistosoma haematobium-infected school-children was tested for P. falciparum parasite positivity by an allele-specific nested-PCR analysis of merozoite surface protein (msp)-1 and -2 genes and a real-time PCR assay. In addition, among P. falciparum parasite-positive individuals, we carried out a Taqman SNP genotyping assay to extrapolate the effect of host CD14 (-159 C/T; rs2569190) genetic variants on schistosome egg count. Results Of the 144 individuals recruited, P. falciparum parasite positivity with msp-1 gene were 34%, 43% and 55% for MAD20, RO33 and K1 alleles respectively. Of the co-infected individuals, CD14 genetic variants ranged from 18.8% vs 21.5%, 33.3% vs 44.4%, 9.7% vs 11.8% for single versus schistosome co-infection for the wild type (CC), heterozygous (CT) and mutant (TT) variants respectively. Though the mean egg count for co-infected individuals with CD14 wild type (33.7 eggs per 10 ml of urine) and heterozygote variants (37.5 eggs per 10 ml of urine) were lower than that of schistosome infection alone (52.48 and 48.08 eggs/10 ml of urine respectively), it lacked statistical significance (p-value 0.12 and 0.29), possibly reflecting the benefit of the CD14 activation in schistosome plus malaria co-infection and not schistosome infection alone. In addition, the lower mean egg count in co-infected individuals reveal the benefit of downstream Th1 immune response mitigated by CD14 innate activation that is absent in schistosome infection alone.

Published

2023

31. Single and Mixed Strains of Probiotics Reduced Hepatic Fat Accumulation and Inflammation and Altered Gut Microbiome in a Nonalcoholic Steatohepatitis Rat Model

Author

Maneerat Chayanupatkul, Panrawee Machchimapiro, Natthaya Chuaypen, Natcha Wanpiyarat, Somying Tumwasorn, Prasong Siriviriyakul, and Duangporn Werawatganon

Subjects

probiotics, nonalcoholic steatohepatitis, gut microbiota, TLR4, CD14, Biology (General), QH301-705.5

Abstract

As gut dysbiosis has been implicated in the pathogenesis of nonalcoholic steatohepatitis (NASH), probiotic supplementation might be a potential treatment for this condition. The aim of this study was to evaluate the effects of single- and mixed-strain probiotics on the severity of NASH induced by a high-fat, high-fructose (HFHF) diet and their mechanisms of action. Male Sprague–Dawley rats were divided into four groups (n = 7 per group): control group, NASH group, NASH + single-strain group, and NASH + mixed-strain group. In the single-strain and mixed-strain groups, rats received Lactobacillus plantarum B7 and Lactobacillus rhamnosus L34 + Lactobacillus paracasei B13 by oral gavage once daily, respectively. The duration of the study was 6 weeks. Liver tissue was used for histopathology, hepatic fat content was assessed by Oil Red O staining and hepatic free fatty acid (FFA), and hepatic TLR4 and CD14 expression were assessed by immunohistochemistry. Fresh feces was collected for gut microbiota analysis. Liver histology revealed a higher degree of fat accumulation, hepatocyte ballooning, and lobular inflammation in the NASH group, which improved in probiotics-treated groups. The amounts of hepatic fat droplets and hepatic FFA levels were more pronounced in the NASH group than in the control and treatment groups. Serum TNF- α levels were significantly higher in the NASH group than in control and probiotic groups. The expression of CD14 and TLR4 increased in the NASH group as compared with the control and probiotics-treated groups. Alpha diversity was reduced in the NASH group, but increased in both treatment groups. The relative abundance of Lactobacillus significantly decreased in the NASH group, but increased in both treatment groups. The relative abundance of Akkermansia significantly increased in the NASH group, but decreased in both treatment groups. In conclusion, both single-strain and mixed-strain probiotics could improve NASH histology by suppressing inflammatory responses in the liver, with this improvement potentially being associated with changes in the gut microbiota.

Published

2024

32. The Pivotal Role of Presepsin in Assessing Sepsis-Induced Cholestasis

Author

Maria Iuliana Ghenu, Dorin Dragoș, Maria Mirabela Manea, Andra-Elena Balcangiu-Stroescu, Dorin Ionescu, Lucian Negreanu, and Adelina Vlad

Subjects

presepsin, sepsis, sepsis-induced cholestasis, cholestasis-related parameters, inflammation, CD14, Medicine (General), R5-920

Abstract

Background: The serum levels of presepsin correlate with parameters indicating cholestasis in sepsis; however, the probability and significance of this association remain uncertain. We aimed to ascertain whether infection, as signaled by presepsin levels, is the primary determinant of elevated biliary parameters in sepsis. Methods: A unicenter, retrospective study included 396 COVID-free emergency-admitted patients, in which presepsin level was determined. Presepsin, neutrophil count, leukocyte count, C reactive protein, and fibrinogen evaluated the septic/inflammatory state. The statistically significant factors associated with cholestasis, ALT, and AST were analyzed by Fisher’s exact test and Spearman regression with Bonferroni’s correction. Results: Presepsin emerged as the most likely variable correlated with all cholestasis markers: alkaline phosphatase (p = 7 × 10−8), gamma-glutamyl transferase (p = 5 × 10−10), and conjugated bilirubin (p = 4 × 10−15). Thrombocyte count, C reactive protein, age, creatinine, urea, lactate, and blood pressure, were associated with only one or two of these markers. Conclusions: In a sepsis setting, the increase in cholestasis-related parameters is associated with presepsin with a higher probability than hemodynamic, inflammatory, or coagulation-related variables. Determining this robust link between sepsis and cholestasis could eliminate unnecessary imaging procedures in critically ill patients, enabling clinicians to focus efforts on addressing the primary infectious cause.

Published

2024

33. Non‐invasive omics analysis delineates molecular changes in water‐only fasting and its sex‐discriminating features in metabolic syndrome patients

Author

Yanyu Jiang, Zhimei Tang, Xiaogang Zhu, Biying Xiao, Hechuan Tian, Xingxing Lei, Huan Peng, Jun Qin, Yanmei Zhang, Robert M. Hoffman, Xiaorong Hu, Qiu Chen, Guang Ji, and Lijun Jia

Subjects

CD14, integrative omics analyses, metabolic profiling, metabolic syndrome, sex‐discriminating molecular feature, water‐only fasting, Medicine

Abstract

Abstract Fasting has been grown in popularity with multiple potential benefits. However, very few studies dynamically monitor physiological and pathological changes during long‐term fasting using noninvasive methods. In the present study, we recruited 37 individuals with metabolic syndrome to engage in a 5‐day water‐only fasting regimen, and simultaneously captured the molecular alterations through urinary proteomics and metabolomics. Our findings reveal that water‐only fasting significantly mitigated metabolic syndrome‐related risk markers, such as body weight, body mass index, abdominal circumference, blood pressure, and fasting blood glucose levels in metabolic syndrome patients. Indicators of liver and renal function remained within the normal range, with the exception of uric acid. Notably, inflammatory response was inhibited during the water‐only fasting period, as evidenced by a decrease in the human monocyte differentiation antigen CD14. Intriguingly, glycolysis, tricarboxylic acid cycle, and oxidative phosphorylation underwent a sex‐dependent reprogramming throughout the fasting period, whereby males exhibited a greater upregulation of carbohydrate metabolism‐related enzymes than females. This disparity may be attributed to evolutionary pressures. Collectively, our study sheds light on the beneficial physiological effects and novel dynamic molecular features associated with fasting in individuals with metabolic syndrome using noninvasive methods.

Published

2023

34. 早期开髓减压引流术联合氢氧化钙对牙髓炎患者咀嚼功能 及血清 CD14、HIF-1琢、CX3CL1 水平的影响.

Author

刘亚文, 吴 更, 孟虹良, 何洪立, and 周 玭

Subjects

*SURGICAL decompression, *CALCIUM hydroxide, *PULPITIS

Abstract

Objective: To investigate the effect of calcium hydroxide combined with early myelotomy decompression and drainage surgery on serum leukocyte differentiation antigen-14 (CD14), hypoxia inducible factor-1α (HIF-1α) and CX3C chemokine ligand 1 (CX3CL1) levels and masticatory function in patients with pulpitis. Methods: 174 patients with pulpitis who were treated in Lianyungang Hospital affiliated to Xuzhou Medical University were selected from January 2020 to April 2022, the patients were divided into control group and study group according to the double chromosphere method, 87 cases each. Both groups underwent early myelotomy decompression and drainage surgery, the control group was filled with zinc oxide eugenol cement, the study group was filled with calcium hydroxide paste filling. The efficacy, visual analog score of pain (VAS), bite force, chewing efficiency, CD14, HIF-1α and CX3CL1 levels in two groups were observed. Results: Compared with the control group, the clinical total effective rate was further increased in the study group (P＜0.05) . Compared with the control group, the VAS score decreased, bite force increased, chewing efficiency increased and serum CD14, HIF-1α and CX3CL1 levels decreased in the study group 7 d after treatment (P＜0.05) . Conclusion: Early pulp opening decompression and drainage of pulpitis was treated with calcium hydroxide filling, can effectively reduce the pain in the patient, improve the chewing function, lift the bite force, regulation of the serum CD14, HIF-1α and CX3CL1 levels, improve the clinical treatment effect. [ABSTRACT FROM AUTHOR]

Published

2023

35. Białko CD14 jako modulator odpowiedzi zapalnej.

Author

Ciesielska, Anna, Amor, Ichrak Ben, and Kwiatkowska, Katarzyna

Abstract

Copyright of Advances in Biochemistry / Postepy Biochemii is the property of Polish Biochemical Society / Acta Biochimica Polonica and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

36. 急性牙髓炎患儿血清 CD14、HIF-1α、CX3CL1 水平与根管治疗期间急症发生的关系.

Author

宋旭, 肖海鹰, 王富金, and 孔雪

Abstract

目的　探讨急性牙髓炎患儿血清脂多糖信号受体（CD14）、缺氧诱导因子1α（HIF-1α）、趋化因子CX3C配 体1（CX3CL1）与根管治疗期间急症（EIAE）发生的关系。方法　选择急性牙髓炎患儿100例（牙髓炎组）、健康体检 儿童100例（对照组），采用酶联免疫吸附法检测两组血清CD14、HIF-1α、CX3CL1水平；对牙髓炎组进行常规一次性 根管治疗，记录 EIAE的发生情况。采用 Logistic回归分析血清 CD14、HIF-1α、CX3CL1水平与 EIAE发生的关系，采 用ROC曲线分析相关指标对EIAE发生的预测价值。结果　牙髓炎组治疗前血清CD14、HIF-1α、CX3CL1水平均高 于对照组（P均<0. 05）。牙髓炎组发生EIAE 23例，其中前牙2例、前磨牙8例、磨牙13例。Logistic逐步回归分析结 果显示，根尖 X线阴影及术前血清 CD14、HIF-1α、CX3CL1水平升高是 EIAE发生的独立危险因素（P均<0. 05）。术 前血清 CD14、HIF-1α、CX3CL1 及有根尖 X 线阴影联合对急性牙髓炎患儿 EIAE 发生具有较好的预测价值（AUC= 0. 837）。结论　急性牙髓炎患儿血清CD14、HIF-1α、CX3CL1水平明显升高，与EIAE发生密切相关；根管治疗前检 测上述指标有助于早期预测EIAE发生。 [ABSTRACT FROM AUTHOR]

Published

2023

37. Severity of Schistosoma haematobium co-infection with malaria in school-children is potentially modulated by host CD14 gene variants.

Author

Oboh-Imafidon, Mary A., Torbit, Sabrina M., Jacob, Swathi, Schroeter, Marissa N., Tucker, Ashley R., Ojurongbe, Olusola, and Thomas, Bolaji N.

Subjects

*SCHISTOSOMA haematobium, *MIXED infections, *CD14 antigen, *GENETIC variation, *MALARIA, *INSECTICIDE resistance, *SCHISTOSOMIASIS, *FILTER paper

Abstract

Objective: Schistosomiasis remains a chronic disease of global importance, especially in many rural areas of the world where co-infection with Plasmodium falciparum is common. It is critical to decipher the role of single or co-infected disease scenarios on immune system regulation in such individuals and how such co-infections can either ameliorate or complicate immune response and the consequent disease outcome. First, 10 ml of urine samples, collected between 10:00 am and 2:00 pm, was filtered for diagnosis of schistosomiasis, while egg count, indicative of disease severity, was determined by microscopy. Furthermore, genomic DNA samples extracted from dried blood spots collected on filter paper from one hundred and forty-four Schistosoma haematobium-infected school-children was tested for P. falciparum parasite positivity by an allele-specific nested-PCR analysis of merozoite surface protein (msp)-1 and -2 genes and a real-time PCR assay. In addition, among P. falciparum parasite-positive individuals, we carried out a Taqman SNP genotyping assay to extrapolate the effect of host CD14 (-159 C/T; rs2569190) genetic variants on schistosome egg count. Results: Of the 144 individuals recruited, P. falciparum parasite positivity with msp-1 gene were 34%, 43% and 55% for MAD20, RO33 and K1 alleles respectively. Of the co-infected individuals, CD14 genetic variants ranged from 18.8% vs 21.5%, 33.3% vs 44.4%, 9.7% vs 11.8% for single versus schistosome co-infection for the wild type (CC), heterozygous (CT) and mutant (TT) variants respectively. Though the mean egg count for co-infected individuals with CD14 wild type (33.7 eggs per 10 ml of urine) and heterozygote variants (37.5 eggs per 10 ml of urine) were lower than that of schistosome infection alone (52.48 and 48.08 eggs/10 ml of urine respectively), it lacked statistical significance (p-value 0.12 and 0.29), possibly reflecting the benefit of the CD14 activation in schistosome plus malaria co-infection and not schistosome infection alone. In addition, the lower mean egg count in co-infected individuals reveal the benefit of downstream Th1 immune response mitigated by CD14 innate activation that is absent in schistosome infection alone. [ABSTRACT FROM AUTHOR]

Published

2023

38. Innate Immune Gene Polymorphisms and COVID-19 Prognosis.

Author

Bakaros, Evangelos, Voulgaridi, Ioanna, Paliatsa, Vassiliki, Gatselis, Nikolaos, Germanidis, Georgios, Asvestopoulou, Evangelia, Alexiou, Stamatia, Botsfari, Elli, Lygoura, Vasiliki, Tsachouridou, Olga, Mimtsoudis, Iordanis, Tseroni, Maria, Sarrou, Styliani, Mouchtouri, Varvara A., Dadouli, Katerina, Kalala, Fani, Metallidis, Simeon, Dalekos, George, Hadjichristodoulou, Christos, and Speletas, Matthaios

Subjects

*GENETIC polymorphisms, *COVID-19, *PROGNOSIS, *RESPIRATORY distress syndrome, *SYMPTOMS

Abstract

COVID-19 is characterized by a heterogeneous clinical presentation and prognosis. Risk factors contributing to the development of severe disease include old age and the presence of comorbidities. However, the genetic background of the host has also been recognized as an important determinant of disease prognosis. Considering the pivotal role of innate immunity in the control of SARS-CoV-2 infection, we analyzed the possible contribution of several innate immune gene polymorphisms (including TLR2-rs5743708, TLR4-rs4986790, TLR4-rs4986791, CD14-rs2569190, CARD8-rs1834481, IL18-rs2043211, and CD40-rs1883832) in disease severity and prognosis. A total of 249 individuals were enrolled and further divided into five (5) groups, according to the clinical progression scale provided by the World Health Organization (WHO) (asymptomatic, mild, moderate, severe, and critical). We identified that elderly patients with obesity and/or diabetes mellitus were more susceptible to developing pneumonia and respiratory distress syndrome after SARS-CoV-2 infection, while the IL18-rs1834481 polymorphism was an independent risk factor for developing pneumonia. Moreover, individuals carrying either the TLR2-rs5743708 or the TLR4-rs4986791 polymorphisms exhibited a 3.6- and 2.5-fold increased probability for developing pneumonia and a more severe disease, respectively. Our data support the notion that the host's genetic background can significantly affect COVID-19 clinical phenotype, also suggesting that the IL18-rs1834481, TLR2-rs5743708, and TLR4-rs4986791 polymorphisms may be used as molecular predictors of COVID-19 clinical phenotype. [ABSTRACT FROM AUTHOR]

Published

2023

39. Bear Bile Powder Ameliorates LPS-Induced Acute Lung Injury by Inhibiting CD14 Pathway and Improving Intestinal Flora: Exploration of “Fei (Lung)–Dachang (Large Intestine) Interaction”

Author

Cheng, Long, Tian, Hui-ling, Lei, Hong-yuan, Wang, Ying-zhou, Jiao, Ma-jing, Liang, Yun-hui, Wu, Zhi-zheng, Deng, Xu-kun, and Ren, Yong-shen

Published

2024

40. Regulation of the expression and lysine acetylation of pro-inflammatory molecules by lipid-modifying enzyme (LPCAT2) in RAW264.7 cells

Author

Poloamina, Victory Ibigo

Subjects

616.9, LPCAT2, Macrophage, Signalling, Phospholipid, CD14, RNF19B, TLR, Lipopeptide, Lipopolysaccharide, PolyIC

Abstract

Lysophosphatidylcholine Acyltransferases (LPCATs) are Lipid modifying enzymes that significantly regulate changes in the glycerophospholipid components of the macrophage membrane phospholipid bilayer. LPCAT2 is a subtype of LPCAT that regulates inflammatory responses to infection by lipopolysaccharides and lipopeptides. LPCAT2 co-localises with TLR4 and prevents its translocation to the signalling site (lipid rafts) of macrophage membranes. The first response to inflammation involves infiltration of macrophages to the infected site, where they fight infection by phagocytosing the microbial pathogen. Changes in the macrophage membrane phospholipid bilayer are essential for phagocytosis and receptor signalling. Regulation of protein acylation is also an integral mechanism for macrophage function. LPCAT2 influences acylation of proteins such as RNF19B - An E3 Ubiquitin Ligase. This research aims to understand further the molecular mechanisms of the enzyme - LPCAT2, that leads to its involvement in regulating macrophage inflammatory responses. Building on pre-existing work on the role of LPCAT2 in inflammation, the primary research question is - "How Does LPCAT2 regulate the expression and function of receptors that mediate macrophage inflammatory responses?" Comparison of the expression of proteins and genes in RAW264.7 cells with or without LPCAT2 silenced determined the possible mechanisms by which LPCAT2 regulates inflammation in macrophages. This study analysed the expression of TLR4 and its co-receptors (CD14 and MD2) - which play a significant role in macrophage inflammatory responses to infection by gram-negative bacteria. The expression of inflammatory cytokines such as IL6, TNFα, IP10, and IFNβ, which are synthesised following activation of TLR4, was also studied. Furthermore, the influence of LPCAT2 in the expression and function of acylated proteins such as RNF19B was studied. Analysis of the regulation of lysine acetylation by LPCAT2 helps to understand the role of LPCAT2 in protein acylation. The results show that LPCAT2 regulates the expression of CD14 and RNF19B. It also influences the expression of lysine-acetylated proteins. Finally, LPCAT2 and RNF19B could modulate macrophage inflammatory responses to both bacterial and viral infection. This study shows that LPCAT2 modulates macrophage inflammatory responses by influencing CD14 and RNF19B expression. It also suggests a novel basis for further studies on the role of LPCAT2 in lysine acetylation of proteins during macrophage inflammatory responses. This thesis contributes novel knowledge to the fields of molecular immunology and biochemistry. The future establishment of the role of LPCAT2 in regulating inflammation can lead to its discovery as a biomarker or a drug-target for various immunological diseases.

Published

2021

41. Transcriptomic analysis: the protection of over-expression thioredoxin reductase 1 in Parkinson’s disease

Author

Zihua Liu, Qiang Ye, and Ying Jiang

Subjects

Parkinson's disease, Thioredoxin reductase 1, Na+-K+-ATP, TLR2, CD14, Surgery, RD1-811, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Parkinson’s disease (PD) is the second most common neurodegenerative disease. The pathologic characteristic feature is the loss of dopaminergic neurons in the substantia nigra (SN). However, the biochemical mechanisms are unclear. A large number of studies have shown that oxidative damage is the primary cause of PD. Hence, antioxidants could become a suitable option to treat PD. The thioredoxin (Trx) system represents a useful, potentially disease-relevant oxidation–reduction system. Thioredoxin reductase 1 (TR1) is a significant component of the Trx system. Methods The overexpression lentivirus (LV) or LV-TR1 in the TR1-A53T model of PD by the stereotactic brain, and successful overexpression of LV or LV-TR1 in the MPP+-induced cellular model by LV or LV-TR1 transfection. Results We confirmed that interleukin-7 mRNA levels increased in MPP+ compared to that in the control and MPP+-TR1 groups using quantitative polymerase chain reaction. The γ-H2AX level was increased in the Tg-A53T group compared to that in the TR1-A53T group by western blotting. The expression of Na+-K+-ATP was decreased in the MPP+ group compared to that in the control and MPP+-TR1 groups by high content screening. Tg-A53T(the C57BL/6 mice transferred with mutant human a-syn); TR1-A53T(A53T mice which were injected TR1-LV 2 µl in SNc on two sides with minipump).The mice were fed for 10 months. control (the N2a cells cultivated with DMEM); MPP+(the N2a cells dealt with MPP+(1 mM) 48 h), MPP+-LV (the N2a cells over-expressed LV for 24 h then dealt with MPP+(1 mM) 48 h). MPP+-TR1(the N2a cell over-expressed TR1-LV for 24 h then dealt with MPP+(1 mM) 48 h). From the Kyoto Encyclopedia of Genes and Genomes (KEGG) analysis, we confirmed that the overexpression of TR1 in SN pars compacta cells decreased oxidative stress, apoptosis, DNA damage, and inflammatory response and increased NADPH, Na+-K+-ATP, and immune response in this PD model. Conclusions Our study shows that overexpressed TR1 can be developed as a neuroprotective agent for PD. Therefore, our findings demonstrate a new targeted protein for the treatment of PD.

Published

2023

42. Structural characterization and biological function annotation of cluster of differentiation 14 gene of crossbred cattle - An In silico approach

Author

Selvan, Arumugam Sakthivel, Karthikeyan, Anbazhgan, and Udhayavel, Shanmugasundaram

Published

2023

43. Lysophosphatidylcholine Acetyltransferase 2 (LPCAT2) Influences the Gene Expression of the Lipopolysaccharide Receptor Complex in Infected RAW264.7 Macrophages, Depending on the E. coli Lipopolysaccharide Serotype

Author

Victory Ibigo Poloamina, Hanaa Alrammah, Wondwossen Abate, Neil D. Avent, Gyorgy Fejer, and Simon K. Jackson

Subjects

CD14, TLR4, MD2, LPCAT2, gene, lipid raft, Biology (General), QH301-705.5

Abstract

Escherichia coli (E. coli) is a frequent gram-negative bacterium that causes nosocomial infections, affecting more than 100 million patients annually worldwide. Bacterial lipopolysaccharide (LPS) from E. coli binds to toll-like receptor 4 (TLR4) and its co-receptor’s cluster of differentiation protein 14 (CD14) and myeloid differentiation factor 2 (MD2), collectively known as the LPS receptor complex. LPCAT2 participates in lipid-raft assembly by phospholipid remodelling. Previous research has proven that LPCAT2 co-localises in lipid rafts with TLR4 and regulates macrophage inflammatory response. However, no published evidence exists of the influence of LPCAT2 on the gene expression of the LPS receptor complex induced by smooth or rough bacterial serotypes. We used RAW264.7—a commonly used experimental murine macrophage model—to study the effects of LPCAT2 on the LPS receptor complex by transiently silencing the LPCAT2 gene, infecting the macrophages with either smooth or rough LPS, and quantifying gene expression. LPCAT2 only significantly affected the gene expression of the LPS receptor complex in macrophages infected with smooth LPS. This study provides novel evidence that the influence of LPCAT2 on macrophage inflammatory response to bacterial infection depends on the LPS serotype, and it supports previous evidence that LPCAT2 regulates inflammatory response by modulating protein translocation to lipid rafts.

Published

2024

44. Co-Activation of Human Whole Blood Cells with Lipopolysaccharides and an Allergen.

Author

Zubova, Svetlana V., Kosyakova, Ninel I., Grachev, Sergey V., and Prokhorenko, Isabella R.

Subjects

*BLOOD cells, *LIPOPOLYSACCHARIDES, *ALLERGENS, *MEDICAL sciences, *ESCHERICHIA coli, *ENDOTOXINS, *CHEMOKINE receptors, *MONOCYTES, *NEUTROPHILS

Abstract

The investigation of common inflammation mechanisms caused by exogenic compounds of microbial origin and allergens is one of the most important tasks in current biomedical science. The main manifestations of immune cell activation caused by pro-inflammatory agents are changes in receptor quantity on the surface of immune cells and the production of cytokines and chemokines by blood cells. The levels of expression of TLR4, CD14, and CD11b in the monocytes and neutrophils of human whole blood in response to LPS E. coli, Der p 2 allergen, or their combination reflect different functional activities in these cells, while the composition and amount of produced cytokines reflect the biological activity of the studied agonists. The activity of Der p 2 allergen in ex vivo experiments on whole blood samples is significantly lower compared with its activity in vitro in isolated PBMC cells, which should be taken into account when transferring the results obtained for isolated cells to whole blood cells. LPS R. capsulatus PG significantly decreases the synthesis of MyD88-dependent NF-κB-regulated cytokines activated by LPS E. coli, Der p 2, or their combination. This indirectly indicates the general mechanisms of cell activation caused by these structures and the unified mechanism of the protective action of LPS R. capsulatus PG against both endotoxin and a combination of endotoxin and the allergen. [ABSTRACT FROM AUTHOR]

Published

2023

45. Apoptotic Cell-Derived CD14(+) Microparticles Promote the Phagocytic Activity of Neutrophilic Precursor Cells in the Phagocytosis of Apoptotic Cells.

Author

Lin, Yu-Chieh, Tsai, Wen-Hui, Chang, Shao-Chi, and Hsu, Hui-Chi

Subjects

*CD14 antigen, *PHAGOCYTOSIS, *CELL communication, *HARVESTING

Abstract

Membranous CD14 is crucial in the phagocytic activity of neutrophils. However, the role of CD14(+) microparticles (MPs) derived from apoptotic neutrophils (apo-MP) during the phagocytic process is not clear. All trans-retinoic acid (ATRA) induces acute promyelocytic leukemic NB4 cells along granulocytic differentiation. In this study, we investigated the role of CD14(+)apo-MP in the cell–cell interaction during the phagocytic process of apoptotic cells by viable ATRA-NB4 cells. We firstly demonstrate that CD14 expression and phagocytic activity of NB4 cells were upregulated simultaneously after ATRA treatment in a time-dependent manner, and both were significantly enhanced via concurrent lipopolysaccharide treatment. The phagocytic activity of ATRA-NB4 cells and lipopolysaccharide-treated ATRA-NB4 cells were both significantly attenuated by pre-treating cells with an antibody specific to either CD14 or TLR4. Further flow cytometric analysis demonstrates that apoptotic ATRA-NB4 cells release CD14(+)apo-MP in an idarubicin dosage-dependent manner. Both CD14 expression and the phagocytic activity of viable ATRA-NB4 cells were significantly enhanced after incubation with apo-MP harvested from apoptotic ATRA-NB4 cells, and the apo-MP-enhanced phagocytic activity was significantly attenuated by pre-treating apo-MP with an anti-CD14 antibody before incubation with viable cells. We conclude that CD14(+)apo-MP derived from apoptotic ATRA-NB4 cells promotes the phagocytic activity of viable ATRA-NB4 cells in engulfing apoptotic cells. [ABSTRACT FROM AUTHOR]

Published

2023

46. Exosomal PPARγ derived from macrophages suppresses LPS-induced peritonitis by negative regulation of CD14/TLR4 axis.

Author

Meng, Meng, Lu, Meizhi, Feng, Junxia, Zhou, Xiaoying, Meng, Ping, Chen, Luxuan, Zou, Xunliang, Liu, Xiaohui, Liu, Langxia, Gao, Xuejuan, and Zhang, Yunfang

Subjects

*CARRIER proteins, *PERITONEAL macrophages, *EXOSOMES, *PERITONITIS, *PEROXISOME proliferator-activated receptors, *SALMONELLA enterica serovar Typhi, *MACROPHAGE inflammatory proteins

Abstract

Background: Intercellular communication between macrophages and peritoneal mesothelial cells (PMCs) has been suggested as a key factor regulating peritonitis development. Here, we explored whether PPARγ (peroxisome proliferator-activated receptor gamma) can be packaged into macrophage exosomes to mediate intercellular communication and regulate peritonitis. Methods: Macrophage exosomes were isolated by ultracentrifugation and identified by nanoparticle tracking analysis and transmission electron microscopy. Proteomic analysis of macrophage-derived exosomes was performed using mass spectrometry. Co-culture models of supernatants or exosomes with PMCs, as well as a mouse peritonitis model induced by lipopolysaccharide (LPS), were employed. Results: In this study, using stable Raw264.7 cells overexpressing GFP-FLAG-PPARγ (OE-PPARγ), we found that PPARγ inhibited LPS-induced inflammatory responses in Raw264.7 cells and that PPARγ was incorporated into macrophage exosomes during this process. Overexpression of PPARγ mainly regulated the secretion of differentially expressed exosomal proteins involved in the biological processes of protein transport, lipid metabolic process, cell cycle, apoptotic process, DNA damage stimulus, as well as the KEGG pathway of salmonella infection. Using co-culture models and mouse peritonitis model, we showed that exosomes from Raw264.7 cells overexpressing PPARγ inhibited LPS-induced inflammation in co-cultured human PMCs and in mice through downregulating CD14 and TLR4, two key regulators of the salmonella infection pathway. Pretreatment of the PPARγ inhibitor GW9662 abolished the anti-inflammatory effect of exosomes from Raw264.7 OE-PPARγ cells on human PMCs. Conclusions: These results suggested that overexpression of PPARγ largely altered the proteomic profile of macrophage exosomes and that exosomal PPARγ from macrophages acted as a regulator of intercellular communication to suppress LPS-induced inflammatory responses in vitro and in vivo via negatively regulating the CD14/TLR4 axis. [ABSTRACT FROM AUTHOR]

Published

2023

47. CD14 is not required for carbon tetrachloride‐induced hepatic inflammation and fibrosis with or without lipopolysaccharide challenge.

Author

Sharma, Akanksha, Wang, Jiang, and Gandhi, Chandrashekhar R.

Subjects

*HEPATIC fibrosis, *CD14 antigen, *LIVER cells, *CARBON tetrachloride, *TRANSFORMING growth factors-beta, *LIPOPOLYSACCHARIDES

Abstract

Binding of lipopolysaccharide (LPS) to CD14 is required for its cellular effects via TLR4. A role of LPS/TLR4‐mediated signaling in activated hepatic stellate cells (aHSCs), the major fibrogenic cells, in liver fibrosis has been reported. We investigated effects of LPS on carbon tetrachloride (CCl4)‐induced fibrosis in CD14‐knockout (KO) mice in vivo, and culture‐activated HSCs in vitro. CCl4 (biweekly; 4 weeks)‐treated wild type (WT) and CD14‐KO mice were challenged with single LPS administration for 24 h. Liver injury, inflammation and fibrosis were determined. Culture‐activated HSCs from WT or CD14‐KO mice were stimulated with LPS. Parameters of fibrogenic activity (expression of collagen1a1 [Col1a1], α‐smooth muscle actin [αSMA] and TGFβ1) and inflammatory cytokines/chemokines were measured. CCl4 treatment caused similar liver injury and fibrosis in WT and CD14‐KO mice. LPS increased liver injury and inflammation similarly in CCl4‐treated WT and CD14‐KO mice, but downregulated Timp1 and upregulated Mmp13. LPS elicited similar NFκB activation and inflammatory response in WT and CD14‐KO aHSCs. LPS similarly downregulated Acta2 (encodes αSMA), Pdgfrb, Col1a1 and Mmp13 expression but did not affect Timp1 expression in WT and CD14‐KO aHSCs. LPS did not alter Tgfb1 but increased expression of decorin (Dcn) (inhibitor of TGFβ1) expression in WT and CD14‐KO aHSCs. The results indicate that the effects of LPS on HSCs are CD14‐independent, and CD14 is not required for hepatic fibrosis. LPS‐induced down‐modulation of fibrogenic markers in aHSCs is also CD14‐independent. [ABSTRACT FROM AUTHOR]

Published

2023

48. Atheroma-Relevant 7-Oxysterols Differentially Upregulate Cd14 Expression.

Author

Kim, Bo-Young, Son, Yonghae, Kim, Byoung Joon, Chung, Sung Woon, Lee, Dongjun, Eo, Seong-Kug, and Kim, Koanhoi

Subjects

*CD14 antigen, *LIPOPOLYSACCHARIDES, *MATRIX metalloproteinases, *CELL migration

Abstract

The expression of CD14 in monocytic cells is elevated in atherosclerotic lesions where 7-oxyterols are abundant. However, it remains unknown whether atheroma-relevant 7-oxysterols are involved in receptor expression. Therefore, we investigated the effects of 7α-hydroxycholesterol (7αOHChol), 7β-hydroxycholesterol (7βOHChol), and 7-ketocholesterol (7K) on CD14 levels in THP-1 cells. The three 7-oxysterols increased CD14 transcript levels at a distinct time point, elevated cellular CD14 protein levels, and promoted the release of soluble CD (sCD14) from THP-1 cells. Our data revealed that CD14 expression was most strongly induced after treatment with 7αOHChol. Moreover, 7αOHChol alone upregulated membrane-bound CD14 levels and enhanced responses to lipopolysaccharides, as determined by CCL2 production and monocytic cell migration. The 7-oxysterols also increased the gelatinolytic activity of MMP-9, and a cell-permeable, reversible MMP-9 inhibitor, MMP-9 inhibitor I, significantly impaired sCD14 release. These results indicate that 7-oxysterols differentially induce CD14 expression in vascular cells and contribute to the monocytic cell expression of CD14 via overlapping, but distinct, mechanisms. [ABSTRACT FROM AUTHOR]

Published

2023

49. Role of CD14 in human disease.

Author

Sharygin, Daniel, Koniaris, Leonidas G., Wells, Clark, Zimmers, Teresa A., and Hamidi, Tewfik

Subjects

*CELL surface antigens, *CD14 antigen, *TOLL-like receptors, *NATURAL immunity, *ENDOTHELIAL cells

Abstract

The cell surface antigen CD14 is primarily understood to act as a co‐receptor for toll‐like receptors (TLRs) to activate innate immunity responses to pathogens and tissue injury in macrophages and monocytes. However, roles for CD14 are increasingly being uncovered in disease responses in epithelial and endothelial cells. Consistent with these broader functions, CD14 expression is altered in a variety of non‐immune cell types in response to a several of disease states. Moreover, soluble CD14 activated by factors from both pathogens and tissue damage may initiate signalling in a variety of non‐immune cells. This review examined the current understanding CD14 in innate immunity as well as its potential functions in nonimmune cells and associated human diseases. [ABSTRACT FROM AUTHOR]

Published

2023

50. Soluble CD14 and Risk of Heart Failure and Its Subtypes in Older Adults

Author

Al-Kindi, Sadeer G, Buzkova, Petra, Shitole, Sanyog G, Reiner, Alex P, Garg, Parveen K, Gottdiener, John S, Psaty, Bruce M, and Kizer, Jorge R

Subjects

Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Clinical Research, Heart Disease, Prevention, Cardiovascular, Aetiology, 2.1 Biological and endogenous factors, Aged, Biomarkers, Heart Failure, Humans, Incidence, Lipopolysaccharide Receptors, Prognosis, Risk Factors, Stroke Volume, CD14, inlfammation, heart failure, Cardiorespiratory Medicine and Haematology, Nursing, Cardiovascular System & Hematology, Cardiovascular medicine and haematology, Clinical sciences

Abstract

BackgroundCD14 is a membrane glycoprotein primarily expressed by myeloid cells that plays a key role in inflammation. Soluble CD14 (sCD14) levels carry a poor prognosis in chronic heart failure (HF), but whether elevations in sCD14 precede HF is unknown. We tested the hypothesis that sCD14 is associated with HF incidence and its subtypes independent of major inflammatory biomarkers among older adults.Methods and resultsWe included participants in the Cardiovascular Health Study without preexisting HF and available baseline sCD14. We evaluated the associations of sCD14, high-sensitivity C-reactive protein (hsCRP), interleukin (IL)-6, and white blood cell count (WBC) with incident HF and subtypes using Cox regression. Among 5217 participants, 1878 had incident HF over 13.6 years (609 classifiable as HF with preserved ejection fraction [HFpEF] and 419 as HF with reduced ejection fraction [HFrEF]). After adjusting for clinical and laboratory covariates, sCD14 was significantly associated with incident HF (hazard ratio [HR]: 1.56 per doubling, 95% confidence interval [CI]: 1.29-1.89), an association that was numerically stronger than for hsCRP (HR per doubling: 1.10, 95% CI: 1.06-1.15), IL-6 (HR: 1.18, 95% CI: 1.10-1.25), and WBC (HR: 1.24, 95% CI: 1.09-1.42), and that remained significant after adjustment for the other markers of inflammation. This association for sCD14 was observed with HFpEF (HR: 1.50, 95% CI: 1.07-2.10) but not HFrEF (HR: 0.99, 95% CI: 0.67-1.49).ConclusionsPlasma sCD14 was associated with incident HF independently and numerically more strongly than other major inflammatory markers. This association was only observed with HFpEF in the subset with classifiable HF subtypes. Pending replication, these findings have potentially important therapeutic implications.

Published

2020