Your search keyword '"STAT-3"' showing total 459 results

1. MiR‐144/451 attenuates lipopolysaccharide‐induced lung inflammation by downregulating Rac1 and STAT‐3 in macrophages.

Author

He, Sheng, Gao, Xiang, Yang, Lei, Li, Xiuru, Mo, Yan, He, Zhenpeng, Hou, Ruitao, Yuan, Xiaoling, Fang, Lei, and Yu, Duonan

Abstract

MicroRNAs have been shown to play a critical role in lung inflammatory diseases. Here, we report that knocking out miR‐144/451 in mice exacerbates lipopolysaccharide (LPS)‐induced lung inflammation. The lung inflammation in mice was induced by intratracheal instillation of LPS. Loss‐of‐function experiments demonstrated that miR‐144/451 gene knockout (KO) increased LPS‐induced lung inflammation and oxidant stress compared with wild‐type (WT) mice, as manifested by increased total bronchoalveolar lavage fluid cells and neutrophil counts, elevated TNF‐α and IL‐6 levels in bronchoalveolar lavage fluid, enhanced myeloperoxidase activity, and reduced catalase and glutathione peroxidase activity in lung tissues. We also found that LPS significantly decreased miR‐451 expression in lung tissues and macrophages; while miR‐451 overexpression in LPS‐induced RAW264.7 cells remarkably reduced TNF‐α and IL‐6 levels as well as reactive oxygen species (ROS) production, suggesting a feedback loop might exist in inflammatory cells. Rac1 mRNA and protein levels were downregulated in miR‐451‐overexpressed RAW264.7 cells. Ex vivo stimulation experiments, performed using alveolar macrophages isolated from miR‐144/451 KO mice, confirmed that Rac1 inhibitor alleviated levels of TNF‐α and ROS in response to LPS stimulation compared with WT controls. Luciferase reporter assay demonstrated that STAT‐3 is a direct target of miR‐451. STAT‐3 protein levels were elevated in miR‐144/451 KO macrophages. LPS treatment also resulted in higher phosphorylation levels of STAT‐3 in macrophages from KO mice than in WT cells. Our study identified miR‐144/451 as an anti‐inflammatory factor in LPS‐induced lung inflammation that acts by downregulating Rac1 and STAT‐3. [ABSTRACT FROM AUTHOR]

Published

2024

2. Effect of a high dose atorvastatin as added-on therapy on symptoms and serum AMPK/ NLRP3 inflammasome and IL-6/ STAT3 axes in patients with major depressive disorder: randomized controlled clinical study.

Author

Aldossary, Khlood Mohammad, Ali, Lashin Saad, Abdallah, Mahmoud S., Bahaa, Mostafa M., Elmasry, Thanaa A., Elberri, Eman I., Kotkata, Fedaa A., El Sabaa, Ramy M., Elmorsi, Yasmine M., Kamel, Mostafa M., Negm, Walaa A., Elberri, Aya Ibrahim, Hamouda, Amir O., AlRasheed, Hayam Ali, Salahuddin, Muhammed M., Yasser, Mohamed, and Hamouda, Manal A.

Subjects

HAMILTON Depression Inventory, MENTAL depression, ADENOSINE monophosphate, AMP-activated protein kinases, PROTEIN kinases

Abstract

Background: Neuroinflammation pathways have been associated with the development of major depressive disorders (MDD). The anti-inflammatory characteristics of statins have been demonstrated to have significance in the pathophysiology of depression. Aim: To investigate the mechanistic pathways of high dose atorvastatin in MDD. Patients and methods: This trial included 60 patients with MDD who met the eligibility requirements. Two groups of patients (n = 30) were recruited by selecting patients from the Psychiatry Department. Group 1 received 20 mg of fluoxetine plus a placebo once daily. Group 2 received fluoxetine and atorvastatin (80 mg) once daily. All patients were assessed by a psychiatrist using the Hamilton Depression Rating Scale (HDRS). A HDRS score of ≤7 indicates remission or partial remission [HDRS<17 and>7]. Response was defined as ≥ 50% drop in the HDRS score. The serum concentrations of nucleotide-binding domain, leucine-richcontaining family, pyrin domain-containing-3 (NLRP-3), interleukin-6 (IL-6), adenosine monophosphate activated protein kinase (AMPK), and signal transducer and activator of transcription factor-3 (STAT-3) were measured. Results: The atorvastatin group showed a significant reduction in the levels of all measured markers along with a statistical increase in the levels of AMPK when compared to the fluoxetine group. The atorvastatin group displayed a significant decrease in HDRS when compared to its baseline and the fluoxetine group. The response rate and partial remission were higher in the atorvastatin group than fluoxetine (p = 0.03, and p = 0.005), respectively. Conclusion: These results imply that atorvastatin at high doses may be a promising adjuvant therapy for MDD patients by altering the signaling pathways for AMPK/ NLRP3 and IL-6/STAT-3. [ABSTRACT FROM AUTHOR]

Published

2024

3. Design, Synthesis, and Evaluation of Oleyl-WRH Peptides for siRNA Delivery.

Author

Rai, Mrigank Shekhar, Sajid, Muhammad Imran, Moreno, Jonathan, Parang, Keykavous, and Tiwari, Rakesh Kumar

Subjects

*RNA interference, *CELL-penetrating peptides, *SMALL interfering RNA, *WESTERN immunoblotting, *NUCLEIC acids

Abstract

Delivering nucleic acid therapeutics across cell membranes is a significant challenge. Cell-penetrating peptides (CPPs) containing arginine (R), tryptophan (W), and histidine (H) show promise for siRNA delivery. To improve siRNA delivery and silence a model STAT3 gene, we hypothesized that oleyl acylation to CPPs, specifically (WRH)n, would enhance STAT3 silencing efficiency in breast and ovarian cancer cells. Using Fmoc/tBu solid-phase peptide chemistry, we synthesized, purified, and characterized the oleyl-conjugated (WRH)n (n = 1–4) peptides. The peptide/siRNA complexes were non-cytotoxic at N/P 40 (~20 μM) against MDA-MB-231, MCF-7, SK-OV-3, and HEK-293 cells after 72 h incubation. All peptide/siRNA complexes showed serum stability at N/P ≥ 40. The synthesized conjugates, with a diameter of <100 nm, formed nano-complexes with siRNA and exhibited a stable range of zeta potential values (13–18 mV at N/P = 40). Confocal microscopy and flow cytometry analysis provided qualitative and quantitative evidence of a successful cellular internalization of siRNA. The peptides oleyl-(WRH)3 and oleyl-(WRH)4 showed ~60% and ~75% cellular uptake of siRNA, respectively, in both MDA-MB-231 and SK-OV-3 cells. Western blot analysis of oleyl-(WRH)4 demonstrated effective silencing of the STAT-3 gene, with ~75% silencing in MDA-MB-231 cells and ~45% in SK-OV-3 cells. [ABSTRACT FROM AUTHOR]

Published

2024

4. Effect of a high dose atorvastatin as added-on therapy on symptoms and serum AMPK/NLRP3 inflammasome and IL-6/STAT3 axes in patients with major depressive disorder: randomized controlled clinical study.

Author

Aldossary, Khlood Mohammad, Saad Ali, Lashin, Abdallah, Mahmoud S., Bahaa, Mostafa M., Elmasry, Thanaa A., Elberri, Eman I., Kotkata, Fedaa A., El Sabaa, Ramy M., Elmorsi, Yasmine M., Kamel, Mostafa M., Negm, Walaa A., Elberri, Aya Ibrahim, Hamouda, Amir O., Ali AlRasheed, Hayam, Salahuddin, Muhammed M., Yasser, Mohamed, and Hamouda, Manal A.

Subjects

MENTAL depression, ATORVASTATIN, HAMILTON Depression Inventory, SEROTHERAPY, ADENOSINE monophosphate, SERUM

Abstract

Background: Neuroinflammation pathways have been associated with the development of major depressive disorders (MDD). The anti-inflammatory characteristics of statins have been demonstrated to have significance in the pathophysiology of depression. Aim: To investigate the mechanistic pathways of high dose atorvastatin in MDD. Patients and methods: This trial included 60 patients with MDD who met the eligibility requirements. Two groups of patients (n = 30) were recruited by selecting patients from the Psychiatry Department. Group 1 received 20 mg of fluoxetine plus a placebo once daily. Group 2 received fluoxetine and atorvastatin (80 mg) once daily. All patients were assessed by a psychiatrist using the Hamilton Depression Rating Scale (HDRS). A HDRS score of =7 indicates remission or partial remission [HDRS<17 and>7]. Response was defined as = 50% drop in the HDRS score. The serum concentrations of nucleotide-binding domain, leucine-richcontaining family, pyrin domain-containing-3 (NLRP-3), interleukin-6 (IL-6), adenosine monophosphate activated protein kinase (AMPK), and signal transducer and activator of transcription factor-3 (STAT-3) were measured. Results: The atorvastatin group showed a significant reduction in the levels of all measured markers along with a statistical increase in the levels of AMPK when compared to the fluoxetine group. The atorvastatin group displayed a significant decrease in HDRS when compared to its baseline and the fluoxetine group. The response rate and partial remission were higher in the atorvastatin group than fluoxetine (p = 0.03, and p = 0.005), respectively. Conclusion: These results imply that atorvastatin at high doses may be a promising adjuvant therapy for MDD patients by altering the signaling pathways for AMPK/NLRP3 and IL-6/STAT-3. [ABSTRACT FROM AUTHOR]

Published

2024

5. Canagliflozin Pretreatment Attenuates Myocardial Dysfunction and Improves Postcardiac Arrest Outcomes After Cardiac Arrest and Cardiopulmonary Resuscitation in Mice

Author

Ju, Feng, Abbott, Geoffrey W, Li, Jiaxue, Wang, Qifeng, Liu, Ting, Liu, Quanhua, and Hu, Zhaoyang

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Cardiovascular, Diabetes, Heart Disease, Physical Injury - Accidents and Adverse Effects, Aetiology, 2.1 Biological and endogenous factors, Cardiac arrest, Cardiopulmonary resuscitation, Sodium-glucose co-transporter 2 (SGLT-2) inhibitors, Canagliflozin, STAT-3, Pharmacology and Pharmaceutical Sciences, Cardiovascular System & Hematology, Cardiovascular medicine and haematology, Pharmacology and pharmaceutical sciences

Abstract

ObjectiveThe SGLT2 inhibitor, canagliflozin, not only reduces glycemia in patients with type 2 diabetes but also exerts cardioprotective effects in individuals without diabetes. However, its potential beneficial effects in cardiac arrest have not been characterized. The purpose of this study was to examine the protective effect of canagliflozin pretreatment on postresuscitation-induced cardiac dysfunction in vivo.MethodsMale C57/BL6 mice were randomized to vehicle (sham and control) or canagliflozin treatment groups. All mice except for the sham-operated mice were subjected to potassium chloride-induced cardiac arrest followed by chest compressions and intravenous epinephrine for resuscitation. Canagliflozin therapy efficacies were evaluated by electrocardiogram, echocardiography, histological analysis, inflammatory response, serum markers of myocardial injury, protein phosphorylation analysis, and immunohistological assessment.ResultsCanagliflozin-pretreated mice exhibited a higher survival rate (P < 0.05), a shorter return of spontaneous circulation (ROSC) time (P < 0.01) and a higher neurological score (P < 0.01 or P < 0.001) than control mice after resuscitation. Canagliflozin was effective at improving cardiac arrest and resuscitation-associated cardiac dysfunction, indicated by increased left ventricular ejection fraction and fractional shortening (P < 0.001). Canagliflozin reduced serum levels of LDH, CK-MB and α-HBDH, ameliorated systemic inflammatory response, and diminished the incidence of early resuscitation-induced arrhythmia. Notably, canagliflozin promoted phosphorylation of cardiac STAT-3 postresuscitation. Furthermore, pharmacological inhibition of STAT-3 by Ag490 blunted STAT-3 phosphorylation and abolished the cardioprotective actions of canagliflozin.ConclusionsCanagliflozin offered a strong cardioprotective effect against cardiac arrest and resuscitation-induced cardiac dysfunction. This canagliflozin-induced cardioprotection is mediated by the STAT-3-dependent cell-survival signaling pathway.

Published

2023

6. Canagliflozin Pretreatment Attenuates Myocardial Dysfunction and Improves Postcardiac Arrest Outcomes After Cardiac Arrest and Cardiopulmonary Resuscitation in Mice.

Author

Ju, Feng, Abbott, Geoffrey W., Li, Jiaxue, Wang, Qifeng, Liu, Ting, Liu, Quanhua, and Hu, Zhaoyang

Abstract

Objective: The SGLT2 inhibitor, canagliflozin, not only reduces glycemia in patients with type 2 diabetes but also exerts cardioprotective effects in individuals without diabetes. However, its potential beneficial effects in cardiac arrest have not been characterized. The purpose of this study was to examine the protective effect of canagliflozin pretreatment on postresuscitation-induced cardiac dysfunction in vivo. Methods: Male C57/BL6 mice were randomized to vehicle (sham and control) or canagliflozin treatment groups. All mice except for the sham-operated mice were subjected to potassium chloride-induced cardiac arrest followed by chest compressions and intravenous epinephrine for resuscitation. Canagliflozin therapy efficacies were evaluated by electrocardiogram, echocardiography, histological analysis, inflammatory response, serum markers of myocardial injury, protein phosphorylation analysis, and immunohistological assessment. Results: Canagliflozin-pretreated mice exhibited a higher survival rate (P < 0.05), a shorter return of spontaneous circulation (ROSC) time (P < 0.01) and a higher neurological score (P < 0.01 or P < 0.001) than control mice after resuscitation. Canagliflozin was effective at improving cardiac arrest and resuscitation-associated cardiac dysfunction, indicated by increased left ventricular ejection fraction and fractional shortening (P < 0.001). Canagliflozin reduced serum levels of LDH, CK-MB and α-HBDH, ameliorated systemic inflammatory response, and diminished the incidence of early resuscitation-induced arrhythmia. Notably, canagliflozin promoted phosphorylation of cardiac STAT-3 postresuscitation. Furthermore, pharmacological inhibition of STAT-3 by Ag490 blunted STAT-3 phosphorylation and abolished the cardioprotective actions of canagliflozin. Conclusions: Canagliflozin offered a strong cardioprotective effect against cardiac arrest and resuscitation-induced cardiac dysfunction. This canagliflozin-induced cardioprotection is mediated by the STAT-3-dependent cell-survival signaling pathway. [ABSTRACT FROM AUTHOR]

Published

2024

7. Corrigendum: Effect of a high dose atorvastatin as added-on therapy on symptoms and serum AMPK/NLRP3 inflammasome and IL-6/STAT3 axes in patients with major depressive disorder: randomized controlled clinical study

Author

Khlood Mohammad Aldossary, Lashin Saad Ali, Mahmoud S. Abdallah, Mostafa M. Bahaa, Thanaa A. Elmasry, Eman I. Elberri, Fedaa A. Kotkata, Ramy M. El Sabaa, Yasmine M. Elmorsi, Mostafa M. Kamel, Walaa A. Negm, Aya Ibrahim Elberri, Amir O. Hamouda, Hayam Ali AlRasheed, Muhammed M. Salahuddin, Mohamed Yasser, and Manal A. Hamouda

Subjects

atorvastatin, major depressive disorder, neuroinflammation, NLRP-3, STAT-3, Therapeutics. Pharmacology, RM1-950

Published

2024

8. IL-13 neutralization attenuates carotid artery intimal hyperplasia and increases endothelial cell migration via modulating the JAK-1/STAT-3 signaling pathway

Author

Qi Li, Yue Li, Fengjiao Wu, Jingyu Li, Zhongsha Li, Xiaoling Qin, Simeng Wei, and Chang Chen

Subjects

Endothelial cells, IL-13, intimal hyperplasia, reactive oxygen species, STAT-3, Cytology, QH573-671

Abstract

ABSTRACTThe aim of this study was to investigate how the concentration of interleukin-13 (IL-13) affects the regulation of endothelial cell migration after injury. The incubation of recombinant human interleukin-13 (rhIL-13) strongly increased the content of reactive oxygen species (ROS) in HUVECs via the JAK-1/STAT-3/NOX-4 signaling pathway. Antagonizing the high intracellular ROS that was induced by rhIL-13 promoted the migration of HUVECs. Furthermore, IL-13 neutralization not only inhibited intimal hyperplasia, but also promoted the migration of endothelial cells (ECs) after injury. The results suggest that IL-13 inhibition is a potential means of stimulating endothelial cells recovery after injury. Therefore, the attenuation of IL-13 activation may have therapeutic value for vascular disease.

Published

2023

9. Effect of a high dose atorvastatin as added-on therapy on symptoms and serum AMPK/NLRP3 inflammasome and IL-6/STAT3 axes in patients with major depressive disorder: randomized controlled clinical study

Author

Khlood Mohammad Aldossary, Lashin Saad Ali, Mahmoud S. Abdallah, Mostafa M. Bahaa, Thanaa A. Elmasry, Eman I. Elberri, Fedaa A. Kotkata, Ramy M. El Sabaa, Yasmine M. Elmorsi, Mostafa M. Kamel, Walaa A. Negm, Aya Ibrahim Elberri, Amir O. Hamouda, Hayam Ali AlRasheed, Muhammed M. Salahuddin, Mohamed Yasser, and Manal A. Hamouda

Subjects

atorvastatin, major depressive disorder, neuroinflammation, NLRP-3, STAT-3, Therapeutics. Pharmacology, RM1-950

Abstract

BackgroundNeuroinflammation pathways have been associated with the development of major depressive disorders (MDD). The anti-inflammatory characteristics of statins have been demonstrated to have significance in the pathophysiology of depression.AimTo investigate the mechanistic pathways of high dose atorvastatin in MDD.Patients and methodsThis trial included 60 patients with MDD who met the eligibility requirements. Two groups of patients (n = 30) were recruited by selecting patients from the Psychiatry Department. Group 1 received 20 mg of fluoxetine plus a placebo once daily. Group 2 received fluoxetine and atorvastatin (80 mg) once daily. All patients were assessed by a psychiatrist using the Hamilton Depression Rating Scale (HDRS). A HDRS score of ≤7 indicates remission or partial remission [HDRS7]. Response was defined as ≥ 50% drop in the HDRS score. The serum concentrations of nucleotide-binding domain, leucine-rich-containing family, pyrin domain-containing-3 (NLRP-3), interleukin-6 (IL-6), adenosine monophosphate activated protein kinase (AMPK), and signal transducer and activator of transcription factor-3 (STAT-3) were measured.ResultsThe atorvastatin group showed a significant reduction in the levels of all measured markers along with a statistical increase in the levels of AMPK when compared to the fluoxetine group. The atorvastatin group displayed a significant decrease in HDRS when compared to its baseline and the fluoxetine group. The response rate and partial remission were higher in the atorvastatin group than fluoxetine (p = 0.03, and p = 0.005), respectively.ConclusionThese results imply that atorvastatin at high doses may be a promising adjuvant therapy for MDD patients by altering the signaling pathways for AMPK/NLRP3 and IL-6/STAT-3.Clinical Trial Registrationclinicaltrials.gov, identifier NCT05792540.

Published

2024

10. New insights into the role of the CHI3L2 protein in invasive ductal breast carcinoma

Author

Rusak, Agnieszka, Kątnik, Ewa, Górnicki, Tomasz, Schmuttermaier, Christina, Kujawa, Krzysztof, Piotrowska, Aleksandra, Ratajczak-Wielgomas, Katarzyna, Kmiecik, Alicja, Wojnar, Andrzej, Dzięgiel, Piotr, and Kzhyshkowska, Julia

Published

2024

11. Corrigendum: Effect of a high dose atorvastatin as added-on therapy on symptoms and serum AMPK/ NLRP3 inflammasome and IL-6/ STAT3 axes in patients with major depressive disorder: randomized controlled clinical study.

Author

Aldossary, Khlood Mohammad, Ali, Lashin Saad, Abdallah, Mahmoud S., Bahaa, Mostafa M., Elmasry, Thanaa A., Elberri, Eman I., Kotkata, Fedaa A., El Sabaa, Ramy M., Elmorsi, Yasmine M., Kamel, Mostafa M., Negm, Walaa A., Elberri, Aya Ibrahim, Hamouda, Amir O., AlRasheed, Hayam Ali, Salahuddin, Muhammed M., Yasser, Mohamed, and Hamouda, Manal A.

Subjects

MEDICAL sciences, MENTAL depression, SEROTHERAPY, MOLECULAR biology, MEDICAL offices

Abstract

This document is a corrigendum for an article titled "Effect of a high dose atorvastatin as added-on therapy on symptoms and serum AMPK/NLRP3 inflammasome and IL-6/STAT3 axes in patients with major depressive disorder: randomized controlled clinical study." The corrigendum addresses an error in the affiliation of one of the authors, Manal A. Hamouda. The correct affiliation should be "Department of Clinical Pharmacy, Faculty of Pharmacy, Menoufia University, Shebin El-Kom, Menoufia, Egypt." The authors apologize for the error and state that it does not affect the scientific conclusions of the article. [Extracted from the article]

Published

2024

12. A randomized placebo-controlled, double-blind study to investigate the effect of a high oral loading dose of cholecalciferol in non-alcoholic fatty liver disease patients, new insights on serum STAT-3 and hepassocin.

Author

ALARFAJ, S. J., BAHAA, M. M., YASSIN, H. A., EL-KHATEEB, E., KOTKATA, F. A., EL-GAMMAL, M. A., ELBERRI, A. I., HABBA, E., EL-DEEN, E. E. ZIEN, KHRIEBA, M. O., EL-MASRY, T. A., NEGM, W. A., and ELBERRI, E. I.

Abstract

OBJECTIVE: Non-alcoholic fatty liver disease (NAFLD) is a common chronic liver metabolic disease affecting millions globally. This study aimed to assess the safety and efficacy of a high oral loading dose of cholecalciferol supplement on NAFLD patients and to investigate its potential role on serum inflammatory biomarkers. PATIENTS AND METHODS: One hundred patients with NAFLD and type 2 diabetes mellitus were involved in the study. Eligible patients were randomized among two equal groups. Group 1 received the standard conventional therapy in addition to a placebo. Group 2 received the conventional therapy plus cholecalciferol for 4 months. The improvement in the patients' glycaemic control parameters, liver function tests, lipid profile, and serum 25-hydroxy vitamin D at the end of the study was set as a primary outcome. The secondary outcome was the decrease in steatosis grade in the ultrasound and high-sensitivity C-reactive protein (hs-CRP), tumor necrosis factor-alpha (TNF-a), signal transducer and activator of factor-3 (STAT-3), nitric oxide (NO), malondialdehyde (MDA), and hepassocin serum levels at the end of the study. RESULTS: Group 2 revealed a significant reduction in the serum levels of lipid profile measures, hs-CRP, alanine aminotransferase (ALT), STAT-3, NO, hepassocin, and MDA compared to the baseline and group 1 results. Whereas group 1 did not show these significant changes. Both groups observed no significant changes in glycemic index, TNF-a, aspartate aminotransferase (AST), and albumin levels. CONCLUSIONS: Cholecalciferol is recommended as additional therapy to modulate lipid peroxidation and systemic inflammation alongside other NAFLD therapies. [ABSTRACT FROM AUTHOR]

Published

2023

13. Allyl isothiocyanate inhibits invasion and angiogenesis in breast cancer via EGFR-mediated JAK-1/STAT-3 signaling pathway.

Author

Rajakumar, Thangarasu and Pugalendhi, Pachaiappan

Subjects

*CELLULAR signal transduction, *ORAL drug administration, *BREAST cancer, *NEOVASCULARIZATION, *MAMMARY glands, *BREAST, *COLLAGEN

Abstract

Angiogenesis, invasion, and metastasis are the main events of cancer cells. JAK-1/STAT-3 is a key intracellular signaling transduction pathway, which controls the growth, differentiation, apoptosis, invasion, and angiogenesis of various cancer cells. The present study explored the impact of allyl isothiocyanate (AITC) on the JAK-1/STAT-3 pathway in DMBA-induced rat mammary tumorigenesis. The mammary tumor was initiated through a single dose of 25 mg DMBA/rat by a subcutaneous injection administered near the mammary gland. We observed decreased body weight and increased the total number of tumors, tumor incidence, tumor volume, well-developed tumor, and histopathological abnormalities in DMBA-induced rats that were modulated after being treated with AITC. Staining of mammary tissues showed a high accumulation of collagen in DMBA-induced rats and it was normalized by the AITC treatment. Moreover, DMBA-induced mammary tissues showed up-regulated expressions of EGFR, pJAK-1, pSTAT-3, nuclear fraction of STAT-3, VEGF, VEGFR2, HIF-1α, MMP-2, and MMP-9 and the down-regulated expressions of cytosolic fraction of STAT-3 and TIMP-2. Oral administration of AITC on DMBA-induced rats inhibits angiogenesis and invasion by modifying these angiogenic and invasive markers. The finding of the present study was further confirmed by molecular docking analysis that shows a strong binding interaction between AITC with STAT-3 and cocrystal structure of STAT-3 glide energy of −18.123 and −72.246 (kcal/mole), respectively. Overall, the results suggested that AITC inhibits activation of the JAK-1/STAT-3 pathway, which subsequently prevents angiogenesis and invasion. It was recommended that AITC might develop a beneficial effect against breast cancer. [ABSTRACT FROM AUTHOR]

Published

2023

14. Epigenetic programing of cancer stemness by transcription factors-non-coding RNAs interactions.

Author

Alsayed, Reem Khaled M.E., Sheikhan, Khalid Sultan A.M., Alam, Majid Ali, Buddenkotte, Jorg, Steinhoff, Martin, Uddin, Shahab, and Ahmad, Aamir

Subjects

*LINCRNA, *CANCER stem cells, *CIRCULAR RNA, *NON-coding RNA, *RNA

Abstract

Cancer 'stemness' is fundamental to cancer existence. It defines the ability of cancer cells to indefinitely perpetuate as well as differentiate. Cancer stem cell populations within a growing tumor also help evade the inhibitory effects of chemo- as well as radiation-therapies, in addition to playing an important role in cancer metastases. NF-κB and STAT-3 are representative transcription factors (TFs) that have long been associated with cancer stemness, thus presenting as attractive targets for cancer therapy. The growing interest in non-coding RNAs (ncRNAs) in the recent years has provided further insight into the mechanisms by which TFs influence cancer stem cell characteristics. There is evidence for a direct regulation of TFs by ncRNAs, such as, microRNAs (miRNAs), long non-coding RNAs (lncRNAs) as well as circular RNAs (circRNAs), and vice versa. Additionally, the TF-ncRNAs regulations are often indirect, involving ncRNA-target genes or the sponging of other ncRNA species by individual ncRNAs. The information is rapidly evolving and this review provides a comprehensive review of TF-ncRNAs interactions with implications on cancer stemness and in response to therapies. Such knowledge will help uncover the many levels of tight regulations that control cancer stemness, providing novel opportunities and targets for therapy in the process. [ABSTRACT FROM AUTHOR]

Published

2023

15. Histological Study on the Possible Ameliorating Consequence of Blocking STAT-3 Pathway on Psoriasis Model in Adult Male Albino rat.

Author

Yousry, Marwa Mohamed, Farag, Eman Abas, and Omar, Abeer Ibraheem

Subjects

MALE models, ENDOTHELIAL growth factors, PSORIASIS, ALBINISM, INTRAPERITONEAL injections, BULLOUS pemphigoid

Abstract

Background: Psoriasis, autoimmune chronic inflammatory skin disease, affects 2-3% of population. It causes poor lifequality due to its disfiguring lesions and co-morbidities. Interleukin (IL)-23/T-helper (Th)-17 &IL-23/Th-22 axes activation, signal transducer and activator of transcription (STAT)-3 pathway stimulation and proinflammatory cytokines (IL-6, IL-17, IL-22 &TNF-a) overproduction are psoriasis main mechanisms. Psoriasis conventional treatment has many adverse effects as immunosuppression and hepatotoxicity with consequent lack of patients' compliance. Aim of work: Evaluating the probable curative effect of blocking STAT-3 pathway using ochromycinone [an STA-21 (STAT-3 inhibitor)] on Imiquimod (IMQ)-induced psoriasis model in adult male albino rats. Materials &Methods: 1 cm2 back skin was shaved in twenty-four adult male albino rats. They grouped into; control group [group-I], IMQ group [group-II, received 20mg/cm2 IMQ-5% topically on the shaved skin for 17 days] & IMQ/STA-21 group [group-III, given daily 3.5mg/kg ochromycinone intraperitoneal injection for 2 weeks]. Psoriasis Area &Severity Index (PASI)-scoring and biochemical, histological, immunohistochemical [for IL-23, STAT-3, Ki-67, connexin (Cx)-26 &vascular endothelial growth factor (VEGF)] and statistical studies were done. Results: IMQ produced psoriasis-like skin lesions (inflammation, epidermal proliferation & angiogenesis). However, the use of STA-21 marvelously ameliorated these lesions. Conclusion: Topical IMQ provoked psoriasis-like lesions concerning gross, biochemical &histological features. These resulted from IL-23/Th-17 &IL-23/Th-22 axes activation, proinflammatory cytokines production that acted via STAT-3 pathway activation. The use of an STA-21 (STAT-3 inhibitor) as ochromycinone showed amazing improvement of these lesions. Thus, blocking STAT-3 might be a promising treatment for psoriasis instead of the traditional therapy with its marked side-effects. [ABSTRACT FROM AUTHOR]

Published

2023

16. STAT-3 signaling role in an experimental model of nephropathy induced by doxorubicin.

Author

de Oliveira Santos, Thabata Caroline, Pereira, Gabriel, Coutinho, Anna Gabrielle Gomes, Dos Santos Silva, Halison Pereira, Lima, Marcelo M. S., Dias, Fernando Augusto Lavezzo, de Almeida, Danilo Cândido, Resende e Silva, Débora Tavares, Perez, Ricardo Fernandez, and Pereira, Rafael Luiz

Abstract

The focal segmental glomerulosclerosis (FSGS) is one of the most frequent glomerulopathy in the world, being considered a significative public health problem worldwide. The disease is characterized by glomerular loss mainly due to inflammation process and collagen fibers deposition. STAT-3 is a transcription factor associated with cell differentiation, migration and proliferation and in renal cells it has been related with fibrosis, acting on the progression of the lesion. Considering this perspective, the present study evaluated the involvement of STAT-3 molecule in an experimental model of FSGS induced by Doxorubicin (DOX). DOX mimics primary FSGS by causing both glomerular and tubular lesions and the inhibition of the STAT3 pathway leads to a decrease in fibrosis and attenuation of kidney damage. We described here a novel FSGS experimental model in a strain of genetically heterogeneous mice which resembles the reality of FSGS patients. DOX-injected mice presented elevated indices of albuminuria and glycosuria, that were significantly reduced in animals treated with a STAT-3 inhibitor (STATTIC), in addition with a decrease of some inflammatory molecules. Moreover, we detected that SOCS-3 (a regulator of STAT family) was up-regulated only in STATTIC-treated mice. Finally, histopathological analyzes showed that DOX-treated group had a significant increase in a tubulointerstitial fibrosis and tubular necrosis, which were not identified in both control and STATTIC groups. Thus, our results indicate that STAT-3 pathway possess an important role in experimental FSGS induced by DOX and may be an important molecule to be further investigated. [ABSTRACT FROM AUTHOR]

Published

2023

17. The effects of melatonin against atherosclerosis-induced endothelial dysfunction and inflammation in hypercholesterolemic rats.

Author

Sezgin, Dilşad, Aslan, Gülnur, Sahin, Kazım, Tuzcu, Mehmet, İlhan, Necip, and Sahna, Engin

Subjects

*ENDOTHELIUM diseases, *DIETARY cholesterol, *MELATONIN, *ASYMMETRIC dimethylarginine, *CELLULAR signal transduction

Abstract

The aim of this study was to investigate the effects of melatonin on the serum asymmetric dimethylarginine (ADMA) levels and the expressions of vaspin, visfatin, dimethylarginine dimethylaminohydrolase (DDAH), and signal transducer and activator of transcription-3 (STAT-3) for evaluation of endothelial function and inflammation in the hypercholesterolemic rats. Rats were divided into 5 groups: (1) control, (2) hypercholesterolaemia, (3) melatonin administrated concurrently with cholesterol diet, (4) melatonin administrated only last 2 weeks and fed with cholesterol diet, (5) atorvastatin administered only last 2 weeks fed with cholesterol diet. Although an increase was observed in the expressions of visfatin and STAT-3 and the serum ADMA levels, the vaspin and DDAH protein expressions were found to decrease with hypercholesterolemic diets. Melatonin was determined to restore all the parameters to the normal levels. In conclusion, melatonin may have protective and therapeutic effects on hypercholesterolaemia by regulating vaspin, STAT-3, DDAH, and ADMA signalling pathways and create similar effects with atorvastatin. [ABSTRACT FROM AUTHOR]

Published

2023

18. Enhanced Expression of RAGE AXIS Is Associated with Severity of COVID-19 in Patients with Comorbidities.

Author

Waraich, Rizwana Sanaullah, Sohail, Fadieleh Adnan, Khan, Gulnaz, Durr-E-Shahwar, Syeda, Khan, Bushra, Rafi, Sidra, and Nasir, Shumaila

Abstract

Background: There is a limited understanding of molecular and cellular events that derive disease progression in patients with corona virus disease 2019 (COVID-19). Receptor for advanced glycation end products (RAGE) is hyperactive in development and complications of several diseases by mediating oxidative stress and inflammation in the body. The present study aims to explore activation of RAGE signaling in patients infected with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) with preexisting comorbidities, including hypertension and or diabetes. Methods: A total of 442 subjects with COVID-19, were recruited for the study. The molecular mechanism of Covid-19 was explored in blood cells, using ELISA, RT- PCR and Western blot. Results: Enhanced levels of ligands of RAGE, including AGEs, S100, and high-mobility group box-1 (HMGB-1) were observed in COVID-19 patients with severe diseases; however, their level was significantly higher in COVID-19 patients with comorbidities compared to COVID-19 patients without comorbidities. The expression of RAGE in parallel to ligands accumulation was significantly increased in patients with severe disease and comorbidities compared to COVID-19 patients with severe disease without comorbidities. The expression of downstream effectors of RAGE, including STAT-3 and nuclear factor kappa B (NF-kB), was also enhanced and their activity was increased in COVID-19 patients with comorbidities. Levels of inflammatory and oxidative stress biomarkers were markedly increased in COVID-19 patients with comorbidities. Conclusions: We conclude that upregulated RAGE axis plays critical role, to worsen the severity of the SARS-CoV-2 infection in patients with preexisting comorbidities and partly explain inflammatory and oxidative stress storm in severe COVID-19 patients. [ABSTRACT FROM AUTHOR]

Published

2023

19. Modified Linear Peptides Effectively Silence STAT-3 in Breast Cancer and Ovarian Cancer Cell Lines.

Author

Mandal, Dindyal, Lohan, Sandeep, Sajid, Muhammad Imran, Alhazza, Abdulelah, Tiwari, Rakesh Kumar, Parang, Keykavous, and Montazeri Aliabadi, Hamidreza

Subjects

*PEPTIDES, *OVARIAN cancer, *CELL lines, *BREAST cancer, *CANCER cells, *TRYPTOPHAN

Abstract

RNA interference (RNAi) has drawn enormous attention as a powerful tool because of its capability to interfere with mRNA and protein production. However, designing a safe and efficient delivery system in RNAi therapeutics remains challenging. Herein, we have designed and synthesized several linear peptides containing tryptophan (W) and arginine (R) residues separated by the β-alanine (βA) spacer and attached to a lipophilic fatty acyl chain, cholesterol, or PEG. The peptide backbone sequences were: Ac-C-βA-βA-W4-βA-βA-R4-CO-NH2 and Ac-K-βA-βA-W4-βA-βA-R4-CO-NH2, with only a difference in N-terminal amino acid. The cysteine side chain in the first sequence was used for the conjugation with PEG2000 and PEG550. Alternatively, the side chain of lysine in the second sequence was used for conjugation with cholesterol or oleic acid. We hypothesized that amphiphilic peptides and optimum fatty acyl chain or PEG could function as an effective siRNA carrier by complementing each structural component's self-assembly and membrane internalization properties. None of the designed peptides showed cytotoxicity up to 10 µM. Serum stability studies suggested that the newly designed peptides efficiently protected siRNA against early degradation by nucleases. Flow cytometry analysis indicated 50–90% cellular uptake of siRNA using the newly developed modified linear peptides (MLPs). Western blot results revealed more than 90% protein downregulation after targeting STAT3 in MDA-MB-231 and SKOV-3 cell lines. In summary, a new peptide class was developed to safely and efficiently deliver siRNA. [ABSTRACT FROM AUTHOR]

Published

2023

20. An In Vivo Screening Model for Investigation of Pathophysiology of Human Implantation Failure.

Author

Nakamura, Hitomi and Kimura, Tadashi

Subjects

*EMBRYO implantation, *SENDAI virus, *MEDICAL screening, *PATHOLOGICAL physiology, *GENETIC transformation

Abstract

To improve current infertility treatments, it is important to understand the pathophysiology of implantation failure. However, many molecules are involved in the normal biological process of implantation and the roles of each molecule and the molecular mechanism are not fully understood. This review highlights the hemagglutinating virus of Japan (HVJ; Sendai virus) envelope (HVJ-E) vector, which uses inactivated viral particles as a local and transient gene transfer system to the murine uterus during the implantation period in order to investigate the molecular mechanism of implantation. In vivo screening in mice using the HVJ-E vector system suggests that signal transducer and activator of transcription-3 (Stat-3) could be a diagnostic and therapeutic target for women with a history of implantation failure. The HVJ-E vector system hardly induces complete defects in genes; however, it not only suppresses but also transiently overexpresses some genes in the murine uterus. These features may be useful in investigating the pathophysiology of implantation failure in women. [ABSTRACT FROM AUTHOR]

Published

2023

21. Repurposing metformin as adjuvant therapy in patients with ulcerative colitis treated with mesalamine: A randomized controlled double-blinded study.

Author

El‑Haggar, Sahar M., Hegazy, Sahar K., Maher, Maha M, Bahgat, Monir M, and Bahaa, Mostafa M.

Subjects

*ULCERATIVE colitis, *MESALAMINE, *TUMOR necrosis factors, *INFLAMMATORY bowel diseases, *METFORMIN

Abstract

UC is triggered by various stimuli such as oxidative stress, antigens, immunity, and environmental factors. These stimuli release inflammatory cytokines such as IL-6, TNF-α and other mediators such as zonulin and STAT3. These mediators dysregulate tight junction proteins. Metformin and 5-aminosalcylic acid act together to block the action of these mediators and reduced UC symptoms. [Display omitted] • UC is a chronic inflammatory bowel disease associated with mucosal ulceration and bloody diarrhea. • The pathogenesis of UC involved activation of IL-6/STAT-3, S1P/SPHK, and downregulated tight junction proteins such as ZO-1. • Metformin treatment significantly reduced TNF-α, IL-6/STAT-3, SIP, and upregulated ZO-1 pathways. • Metformin could be a promising anti-inflammatory and adjuvant therapy in UC. Ulcerative colitis (UC) is a type of inflammatory bowel disease associated with persistent inflammation. Animal studies proved the efficacy of metformin in UC. To investigate the potential role of metformin and its protective pathways in patients with UC. This is a randomized, controlled, and double-blinded clinical trial that included 60 participants with mild to moderate UC and was divided randomly into two groups (n = 30). For 6 months, the mesalamine group received 1 g of mesalamine three times daily (t.i.d.). For six months, the metformin group received mesalamine 1 g t.i.d. and metformin 500 mg twice daily. A gastroenterologist evaluated patients at baseline and 6 months after starting the treatment in order to measure serum levels of zonulin, sphingosine 1 phosphate (S1P), interleukin-6 (IL-6), and tumor necrosis factor-alpha (TNF-α). Biopsies from the colon were used to measure gene expression of zonula occuldin-1 (ZO-1), signal transducer and activator of factor-3 (STAT-3), and intracellular adhesion molecule-1 (ICAM-1). The numeric pain rating scale (NRS) and partial Mayo score were also assessed for each patient. When compared to the mesalamine group, the metformin group demonstrated a statistical decrease in serum IL-6, zonulin, TNF-α, SIP, gene expression of ICAM-1 and STAT-3, and a significant increase in colonic ZO-1 when compared to the mesalamine group. The metformin group also showed a significant decrease in NRS and partial Mayo score index in comparison with the mesalamine group. Metformin may be a promising additional therapy for UC patients. Trial registration identifier: NCT05553704. [ABSTRACT FROM AUTHOR]

Published

2024

22. Bacteroides fragilis Toxin Coordinates a Pro-carcinogenic Inflammatory Cascade via Targeting of Colonic Epithelial Cells

Author

Chung, Liam, Orberg, Erik Thiele, Geis, Abby L, Chan, June L, Fu, Kai, Shields, Christina E DeStefano, Dejea, Christine M, Fathi, Payam, Chen, Jie, Finard, Benjamin B, Tam, Ada J, McAllister, Florencia, Fan, Hongni, Wu, Xinqun, Ganguly, Sudipto, Lebid, Andriana, Metz, Paul, Van Meerbeke, Sara W, Huso, David L, Wick, Elizabeth C, Pardoll, Drew M, Wan, Fengyi, Wu, Shaoguang, Sears, Cynthia L, and Housseau, Franck

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Digestive Diseases, Colo-Rectal Cancer, Cancer, Adenomatous Polyposis Coli Protein, Animals, Bacterial Toxins, Bacteroides fragilis, Carcinogenesis, Cell Line, Tumor, Colon, Colorectal Neoplasms, Enzyme Activation, Epithelial Cells, Female, Gene Deletion, HT29 Cells, Humans, Inflammation, Interleukin-17, Male, Metalloendopeptidases, Mice, Mice, Inbred C57BL, Mice, Knockout, Myeloid Cells, Receptors, Interleukin-17, Receptors, Interleukin-8B, STAT3 Transcription Factor, Transcription Factor RelA, Nf-κB, STAT-3, colorectal cancer, inflammation, mucosal immunology, myeloid cells, Microbiology, Medical Microbiology, Immunology, Biochemistry and cell biology, Medical microbiology

Abstract

Pro-carcinogenic bacteria have the potential to initiate and/or promote colon cancer, in part via immune mechanisms that are incompletely understood. Using ApcMin mice colonized with the human pathobiont enterotoxigenic Bacteroides fragilis (ETBF) as a model of microbe-induced colon tumorigenesis, we show that the Bacteroides fragilis toxin (BFT) triggers a pro-carcinogenic, multi-step inflammatory cascade requiring IL-17R, NF-κB, and Stat3 signaling in colonic epithelial cells (CECs). Although necessary, Stat3 activation in CECs is not sufficient to trigger ETBF colon tumorigenesis. Notably, IL-17-dependent NF-κB activation in CECs induces a proximal to distal mucosal gradient of C-X-C chemokines, including CXCL1, that mediates the recruitment of CXCR2-expressing polymorphonuclear immature myeloid cells with parallel onset of ETBF-mediated distal colon tumorigenesis. Thus, BFT induces a pro-carcinogenic signaling relay from the CEC to a mucosal Th17 response that results in selective NF-κB activation in distal colon CECs, which collectively triggers myeloid-cell-dependent distal colon tumorigenesis.

Published

2018

23. The association between PI3K, JAK/STAT pathways with the PDL‐1 expression in prostate cancer.

Author

Kazan, Ozgur, Kir, Gozde, Culpan, Meftun, Cecikoglu, Gozde Ecem, Atis, Gokhan, and Yildirim, Asif

Subjects

*PROSTATE cancer, *RADICAL prostatectomy, *PROSTATE cancer prognosis, *PROGRESSION-free survival, *APOPTOSIS, *PHOSPHATIDYLINOSITOL 3-kinases

Abstract

Programmed cell death protein‐1/programmed death‐ligand‐1 (PD‐1/PDL‐1) signalling pathway has gained attention in prostate cancer. The relationship between pSTAT‐1, pSTAT‐3 expressions and PTEN loss with PDL‐1 expression was assessed and the effects of the pathways on prostate cancer prognosis were evaluated. Patients who underwent radical prostatectomy between 2011 and 2017 were included in our study. Prostatectomy materials were evaluated using immunohistochemical staining of pSTAT‐1, pSTAT‐3, PTEN, and PDL‐1. The relationship between PDL‐1 and pSTAT‐1, pSTAT‐3 expressions and PTEN loss was evaluated. Additionally, factors affecting biochemical recurrence‐free survival and clinical progression‐free survival were analysed. Within100 patients, 9 of 11 patients with PDL‐1 expression also had intermediate‐high pSTAT‐1 staining intensity, and those with PDL‐1 expression had higher pSTAT‐1 staining intensity than those without (81.9% vs. 56.2%, p = 0.014). In univariate analysis, pSTAT‐1, pSTAT‐3 and PDL‐1 expressions had significant impact on biochemical recurrence‐free and clinical progression‐free survival. In multivariate analysis, pSTAT‐1 staining intensity with radical prostatectomy ISUP grade in terms of biochemical recurrence‐free survival and the pSTAT‐1 H‐score with radical prostatectomy ISUP grade in terms of clinical progression‐free survival were independent risk factors. Moderate‐high expression of pSTAT‐1 was closely associated with PDL‐1 expression, and pSTAT‐1 was also a predictor of biochemical recurrence and clinical progression. [ABSTRACT FROM AUTHOR]

Published

2022

24. Modulation of STAT-1, STAT-3, and STAT-6 activities in THP-1 derived macrophages infected with two Trypanosoma cruzi strains.

Author

Oliveira, Melissa Martins, Bonturi, Camila Ramalho, Salu, Bruno Ramos, Oliva, Maria Luiza Vilela, Mortara, Renato Arruda, and Orikaza, Cristina Mary

Subjects

TRYPANOSOMA cruzi, CHAGAS' disease, MACROPHAGES, NEGLECTED diseases, MIXED infections, REACTIVE oxygen species, NEMATODE infections

Abstract

Trypanosoma cruzi is the causative protozoan of Chagas' Disease, a neglected tropical disease that affects 6-7 million people worldwide. Interaction of the parasite with the host immune system is a key factor in disease progression and chronic symptoms. Although the human immune system is capable of controlling the disease, the parasite has numerous evasion mechanisms that aim to maintain intracellular persistence and survival. Due to the pronounced genetic variability of T. cruzi, co-infections or mixed infections with more than one parasite strain have been reported in the literature. The intermodulation in such cases is unclear. This study aimed to evaluate the co-infection of T. cruzi strains G and CL compared to their individual infections in human macrophages derived from THP-1 cells activated by classical or alternative pathways. Flow cytometry analysis demonstrated that trypomastigotes were more infective than extracellular amastigotes (EAs) and that strain G could infect more macrophages than strain CL. Classically activated macrophages showed lower number of infected cells and IL-4-stimulated cells displayed increased CL-infected macrophages. However, co-infection was a rare event. CL EAs decreased the production of reactive oxygen species (ROS), whereas G trypomastigotes displayed increased ROS detection in classically activated cells. Co-infection did not affect ROS production. Monoinfection by strain G or CL mainly induced an anti-inflammatory cytokine profile by decreasing inflammatory cytokines (IFN-g, TNF-a, IL-1b) and/or increasing IL-4, IL-10, and TGF-b. Co-infection led to a predominant inflammatory milieu, with reduced IL-10 and TGF-b, and/or promotion of IFN-g and IL-1b release. Infection by strain G reduced activation of intracellular signal transducer and activator of transcription (STAT) factors. In EAs, monoinfections impaired STAT-1 activity and promoted phosphorylation of STAT-3, both changes may prolong cell survival. Coinfected macrophages displayed pronounced activation of all STATs examined. These activations likely promoted parasite persistence and survival of infected cells. The collective results demonstrate that although macrophages respond to both strains, T. cruzi can modulate the intracellular environment, inducing different responses depending on the strain, parasite infective form, and co-infection or monoinfection. The modulation influences parasite persistence and survival of infected cells. [ABSTRACT FROM AUTHOR]

Published

2022

25. NIL10: A New IL10-Receptor Binding Nanoparticle That Induces Cardiac Protection in Mice and Pigs Subjected to Acute Myocardial Infarction through STAT3/NF-κB Activation.

Author

Tesoro, Laura, Hernández, Ignacio, Ramírez-Carracedo, Rafael, Díez-Mata, Javier, Alcharani, Nunzio, Jiménez-Guirado, Beatriz, Ovejero-Paredes, Karina, Filice, Marco, Zamorano, Jose Luis, Saura, Marta, Zaragoza, Carlos, and Botana, Laura

Subjects

*MICE, *KNOCKOUT mice, *MACROPHAGES, *TRANSCRIPTION factors, *SWINE, *INTERLEUKIN-10

Abstract

(1) Background: Early response after acute myocardial infarction (AMI) prevents extensive cardiac necrosis, in which inflammation resolution, including expression of anti-inflammatory interleukin-10 (IL-10), may play a key role. (2) Methods: We synthesized NIL10, a micelle-based nanoparticle, to target IL-10 receptor in mice and pigs subjected to AMI. (3) Results: Administration of NIL10 induced cardiac protection of wild-type and IL-10 knockout mice and pigs subjected to AMI. Cardiac protection was not induced in IL-10-receptor null mice, as shown by a significant recovery of cardiac function, in which inflammatory foci and fibrosis were strongly reduced, together with the finding that resolving M2-like macrophage populations were increased after day 3 of reperfusion. In addition, anti-inflammatory cytokines, including IL-4, IL-7, IL-10, IL-13, IL-16, and IL-27 were also elevated. Mechanistically, NIL10 induced activation of the IL-10 receptor/STAT-3 signaling pathway, and STAT3-dependent inhibition of nuclear translocation of pro-inflammatory NF-ĸB transcription factor. (4) Conclusions: Taken together, we propose using NIL10 as a novel therapeutic tool against AMI-induced cardiac damage. [ABSTRACT FROM AUTHOR]

Published

2022

26. Targeting inflammation and redox perturbations by lisinopril mitigates Freund's adjuvant-induced arthritis in rats: role of JAK-2/STAT-3/RANKL axis, MMPs, and VEGF.

Author

Arab, Hany H., Abd El-Aal, Sarah A., Ashour, Ahmed M., El-Sheikh, Azza A. K., Al Khabbaz, Hana J., Arafa, El-Shaimaa A., Mahmoud, Ayman M., and Kabel, Ahmed M.

Subjects

*ADJUVANT arthritis, *LISINOPRIL, *ACE inhibitors, *MATRIX metalloproteinases, *ANGIOTENSIN II, *RHEUMATOID arthritis

Abstract

Background: Cardiovascular disorders are major complications of rheumatoid arthritis (RA). Hence, finding effective agents that can target RA progression and its cardiovascular consequences is demanding. The present work aimed to explore the potential of lisinopril, an angiotensin-converting enzyme inhibitor, to mitigate adjuvant's-induced arthritis with emphasis on the pro-inflammatory signals, articular degradation cues, and angiogenesis alongside JAK-2/STAT-3 and Nrf2/HO-1 pathways. Methods: Lisinopril (10 mg/kg/day) was administered by oral gavage for 3 weeks and the target signals were examined by biochemical assays, ELISA, histopathology, immunoblotting, and immunohistochemistry. Results: Lisinopril attenuated the progression of arthritis as proven by lowering paw edema, arthritic index, and gait scores alongside diminishing the immune-cell infiltration/aberrant histopathology in the dorsal pouch lining. These favorable actions were associated with curtailing the production of inflammatory cytokines (TNF-α, IL-6, IL-1β, and IL-17) and the pro-inflammatory angiotensin II alongside upregulating the anti-inflammatory angiotensin-(1–7) in the hind paw of arthritic rats. At the molecular level, lisinopril inhibited the upstream JAK-2/STAT-3 pathway by downregulating the protein expression of p-JAK-2/total JAK-2 and p-STAT-3/total STAT-3 ratio and the nuclear levels of NF-κBp65. Meanwhile, lisinopril curbed the downstream cartilage degradation signals matrix metalloproteinases (MMP-3 and MMP-9) and the bone erosion cue RANKL. Equally important, the protein expression of the angiogenesis signal VEGF was downregulated in the hind paw/dorsal lining. With respect to oxidative stress, lisinopril suppressed the paw lipid peroxides and boosted GSH and Nrf-2/HO-1 pathway. Conclusion: Lisinopril attenuated adjuvant-induced arthritis via inhibition of inflammation, articular degradation cues, and angiogenesis. [ABSTRACT FROM AUTHOR]

Published

2022

27. Modulation of STAT-1, STAT-3, and STAT-6 activities in THP-1 derived macrophages infected with two Trypanosoma cruzi strains

Author

Melissa Martins Oliveira, Camila Ramalho Bonturi, Bruno Ramos Salu, Maria Luiza Vilela Oliva, Renato Arruda Mortara, and Cristina Mary Orikaza

Subjects

STAT-1, STAT-3, STAT-6, Trypanosoma cruzi, THP-1, macrophages, Immunologic diseases. Allergy, RC581-607

Abstract

Trypanosoma cruzi is the causative protozoan of Chagas’ Disease, a neglected tropical disease that affects 6−7 million people worldwide. Interaction of the parasite with the host immune system is a key factor in disease progression and chronic symptoms. Although the human immune system is capable of controlling the disease, the parasite has numerous evasion mechanisms that aim to maintain intracellular persistence and survival. Due to the pronounced genetic variability of T. cruzi, co-infections or mixed infections with more than one parasite strain have been reported in the literature. The intermodulation in such cases is unclear. This study aimed to evaluate the co-infection of T. cruzi strains G and CL compared to their individual infections in human macrophages derived from THP-1 cells activated by classical or alternative pathways. Flow cytometry analysis demonstrated that trypomastigotes were more infective than extracellular amastigotes (EAs) and that strain G could infect more macrophages than strain CL. Classically activated macrophages showed lower number of infected cells and IL-4-stimulated cells displayed increased CL-infected macrophages. However, co-infection was a rare event. CL EAs decreased the production of reactive oxygen species (ROS), whereas G trypomastigotes displayed increased ROS detection in classically activated cells. Co-infection did not affect ROS production. Monoinfection by strain G or CL mainly induced an anti-inflammatory cytokine profile by decreasing inflammatory cytokines (IFN-γ, TNF-α, IL-1β) and/or increasing IL-4, IL-10, and TGF-β. Co-infection led to a predominant inflammatory milieu, with reduced IL-10 and TGF-β, and/or promotion of IFN-γ and IL-1β release. Infection by strain G reduced activation of intracellular signal transducer and activator of transcription (STAT) factors. In EAs, monoinfections impaired STAT-1 activity and promoted phosphorylation of STAT-3, both changes may prolong cell survival. Coinfected macrophages displayed pronounced activation of all STATs examined. These activations likely promoted parasite persistence and survival of infected cells. The collective results demonstrate that although macrophages respond to both strains, T. cruzi can modulate the intracellular environment, inducing different responses depending on the strain, parasite infective form, and co-infection or monoinfection. The modulation influences parasite persistence and survival of infected cells.

Published

2022

28. Growth-Suppressive and Apoptosis-Inducing Effects of Tetrandrine in SW872 Human Malignant Liposarcoma Cells via Activation of Caspase-9, Down-Regulation of XIAP and STAT-3, and ER Stress.

Author

Samsuzzaman, Mohammed and Jang, Byeong-Churl

Subjects

*CANCER cells, *CASPASES, *APOPTOSIS, *SOFT tissue tumors, *NUCLEAR DNA, *NUCLEAR fragmentation

Abstract

Liposarcoma is a rare and heterogeneous soft tissue malignant tumor and has a significant impact on mortality with a poor prognosis. To date, there is no effective treatment for liposarcoma, whereas surgical resection is only the gold treatment with numerous adverse effects. Here we investigated whether tetrandrine inhibits the growth of SW872 human malignant liposarcoma cells. Of note, tetrandrine at 10 μM vastly inhibited growth and induced apoptosis, as evidenced by increased nuclear DNA fragmentation and sub-G1 population of SW872 cells. Mechanistically, treatment with tetrandrine led to activation of caspase-9/3 in SW872 cells, and z-VAD-fmk, a pan-caspase inhibitor, attenuated the tetrandrine-induced apoptosis and growth suppression in SW872 cells. In addition, tetrandrine treatment resulted in down-regulation of XIAP andSTAT-3 in SW872 cells, and importantly knockdown of STAT-3 caused a significant reduction of the cell survival. Tetrandrine also had abilities to up-regulate not only the expression of GRP78 and ATF-4 but also the phosphorylation of eIF-2α in SW872 cells. In summary, these results demonstrated that tetrandrine has strong growth-suppressive and apoptosis-inducing effects on SW872 cells, which are mediated through control of the intrinsic caspase pathway, down-regulation of XIAP and STAT-3, and triggering ER stress. [ABSTRACT FROM AUTHOR]

Published

2022

29. Anti-Growth, Anti-Angiogenic, and Pro-Apoptotic Effects by CX-4945, an Inhibitor of Casein Kinase 2, on HuCCT-1 Human Cholangiocarcinoma Cells via Control of Caspase-9/3, DR-4, STAT-3/STAT-5, Mcl-1, eIF-2α, and HIF-1α.

Author

Wang, Saini, Yadav, Anil Kumar, Han, Jin-Yi, Ahn, Keun Soo, and Jang, Byeong-Churl

Subjects

*PROTEIN kinase CK2, *CHOLANGIOCARCINOMA, *NUCLEAR DNA, *NUCLEAR fragmentation, *KINASE inhibitors, *CELL death, *APOPTOSIS

Abstract

Overexpression of casein kinase 2 (CK2) has an oncogenic and pro-survival role in many cancers. CX-4945 (Silmitasertib) is a CK2 inhibitor with anti-cancerous and anti-angiogenic effects. Up to date, the anti-cancer effect and mechanism of CX-4945 on human cholangiocarcinoma (CCA) remain unclear. This study investigated whether CX-4945 inhibits growth and induces apoptosis of HuCCT-1 cells, a human CCA cell line. Of note, treatment with CX-4945 at 20 μM markedly reduced survival and induced apoptosis of HuCCT-1 cells, as evidenced by nuclear DNA fragmentation, PARP cleavage, activation of caspase-9/3, and up-regulation of DR-4. Although CX-4945 did not affect the phosphorylation and expression of CK2, it vastly inhibited the phosphorylation of CK2 substrates, supporting the drug's efficacy in inhibiting CK2 and its downstream pathway. Importantly, knockdown of CK2 that partially suppressed the phosphorylation of CK2 substrates resulted in a significant reduction of HuCCT-1 cell survival. In addition, CX-4945 reduced the phosphorylation and expression of STAT-3 and STAT-5 in HuCCT-1 cells, and pharmacological inhibition or respective knockdown of these proteins resulted in significant growth suppression of HuCCT-1 cells. CX-4945 also had abilities to decrease Mcl-1 expression while increasing eIF-2α phosphorylation in HuCCT-1 cells. Furthermore, there was a time-differential negative regulation of HIF-1α expression by CX-4945 in HuCCT-1 cells, and knockdown of HIF-1α caused a significant reduction of the cell survival. In summary, these results demonstrated that CX-4945 has anti-growth, anti-angiogenic, and pro-apoptotic effects on HuCCT-1 cells, which are mediated through control of CK2, caspase-9/3, DR-4, STAT-3/5, Mcl-1, eIF-2α, and HIF-1α. [ABSTRACT FROM AUTHOR]

Published

2022

30. Oleyl Conjugated Histidine-Arginine Cell-Penetrating Peptides as Promising Agents for siRNA Delivery.

Author

Sajid, Muhammad Imran, Mandal, Dindyal, El-Sayed, Naglaa Salem, Lohan, Sandeep, Moreno, Jonathan, and Tiwari, Rakesh Kumar

Subjects

*CELL-penetrating peptides, *SMALL interfering RNA, *SURFACE charges, *GENE silencing, *PEPTIDES

Abstract

Recent approvals of siRNA-based products motivated the scientific community to explore siRNA as a treatment option for several intractable ailments, especially cancer. The success of approved siRNA therapy requires a suitable and safer drug delivery agent. Herein, we report a series of oleyl conjugated histidine–arginine peptides as a promising nonviral siRNA delivery tool. The conjugated peptides were found to bind with the siRNA at N/P ratio ≥ 2 and demonstrated complete protection for the siRNA from early enzymatic degradation at N/P ratio ≥ 20. Oleyl-conjugated peptide -siRNA complexes were found to be noncytotoxic in breast cancer cells (MCF-7 and MDA-MB-231) and normal breast epithelial cells (MCF 10A) at N/P ratio of ~40. The oleyl-R3-(HR)4 and oleyl-R4-(HR)4 showed ~80-fold increased cellular uptake in MDA-MB-231 cells at N/P 40. Moreover, the conjugated peptides-siRNA complexes form nanocomplexes (~115 nm in size) and have an appropriate surface charge to interact with the cell membrane and cause cellular internalization. Furthermore, this study provides a proof-of-concept that oleyl-R5-(HR)4 can efficiently silence STAT-3 gene (~80% inhibition) in MDA-MB-231 cells with similar effectiveness to Lipofectamine. Further exploration of this approach holds a great promise in discovering a successful in vivo siRNA delivery agent with a favorable pharmacokinetic profile. [ABSTRACT FROM AUTHOR]

Published

2022

31. Urothelial Cancer Stem Cell Heterogeneity

Author

Kripnerova, Michaela, Parmar, Hamendra Singh, Pesta, Martin, Kohoutova, Michaela, Kuncova, Jitka, Drbal, Karel, Rajtmajerova, Marie, Hatina, Jiri, Lambris, John D., Series Editor, Rezaei, Nima, Series Editor, and Birbrair, Alexander, editor

Published

2019

32. Expression of interleukin-6 (IL-6), signal transducer and activator of transcription-3 (STAT-3) and telomerase in choriocarcinomas

Author

Luciana Pietro, Fátima Bottcher-Luiz, Lício Augusto Velloso, Joseane Morari, Marcelo Nomura, and Liliana A. Lucci De Angelo Andrade

Subjects

Trophoblastic disease, Placenta, Choriocarcinoma, Telomerase activity, Cytokines, STAT-3, Surgery, RD1-811, Pathology, RB1-214

Abstract

Abstract Blastocyst implantation and neoplastic invasion have some common properties related to tissue invasion, mediated by various cytokines. Aim To compare the expression of IL-6, STAT-3 and telomerase in material of abortions in the first trimester of pregnancy, at term placentas and in choriocarcinomas. Methods Immunohistochemical reactions were performed on formalin fixed and included in paraffin samples from 3 groups: abortions, normal at term placentas and choriocarcinomas. Western Blot and Real-Time PCR assays were performed on fresh material from BeWo cell line and in primary culture cells of normal placenta. Results Immunohistochemical reactions: IL-6 expression was moderate in the first trimester abortion samples and high in at term placentas and choriocarcinomas. STAT-3 was strongly positive in all groups. Telomerase expression was absent in normal at term placentas but was increased in BeWo cells. Conclusion IL-6 and STAT-3 are present in the invasion process of the normal placental development and they are maintained during the malignant transformation to choriocarcinoma. The intense telomerase expression observed in BeWo cells was strongly associated with the malignant phenotype, confirming it as a good marker for cell transformation and tumor progression.

Published

2020

33. Vagal afferent fibers contribute to the anti-inflammatory reactions by vagus nerve stimulation in concanavalin A model of hepatitis in rats

Author

Byung Gon Jo, Seung-Hyung Kim, and Uk Namgung

Subjects

Vagus nerve stimulation, Inflammatory cytokines, α7 nicotinic acetylcholine receptor, STAT-3, Capsaicin, Cholinergic anti-inflammation, Therapeutics. Pharmacology, RM1-950, Biochemistry, QD415-436

Abstract

Abstract Background Increasing number of studies provide evidence that the vagus nerve stimulation (VNS) dampens inflammation in peripheral visceral organs. However, the effects of afferent fibers of the vagus nerve (AFVN) on anti-inflammation have not been clearly defined. Here, we investigate whether AFVN are involved in VNS-mediated regulation of hepatic production of proinflammatory cytokines. Methods An animal model of hepatitis was generated by intraperitoneal (i.p.) injection of concanavalin A (ConA) into rats, and electrical stimulation was given to the hepatic branch of the vagus nerve. AFVN activity was regulated by administration of capsaicin (CAP) or AP-5/CNQX and the vagotomy at the hepatic branch of the vagus nerve (hVNX). mRNA and protein expression in target tissues was analyzed by RT-PCR, real-time PCR, western blotting and immunofluorescence staining. Hepatic immune cells were analyzed by flow cytometry. Results TNF-α, IL-1β, and IL-6 mRNAs and proteins that were induced by ConA in the liver macrophages were significantly reduced by the electrical stimulation of the hepatic branch of the vagus nerve (hVNS). Alanine transaminase (ALT) and aspartate transaminase (AST) levels in serum and the number of hepatic CD4+ and CD8+ T cells were increased by ConA injection and downregulated by hVNS. CAP treatment deteriorated transient receptor potential vanilloid 1 (TRPV1)-positive neurons and increased caspase-3 signals in nodose ganglion (NG) neurons. Concomitantly, CAP suppressed choline acetyltransferase (ChAT) expression that was induced by hVNS in DMV neurons of ConA-injected animals. Furthermore, hVNS-mediated downregulation of TNF-α, IL-1β, and IL-6 expression was hampered by CAP treatment and similarly regulated by hVNX and AP-5/CNQX inhibition of vagal feedback loop pathway in the brainstem. hVNS elevated the levels of α7 nicotinic acetylcholine receptors (α7 nAChR) and phospho-STAT3 (Tyr705; pY-STAT3) in the liver, and inhibition of AFVN activity by CAP, AP-5/CNQX and hVNX or the pharmacological blockade of hepatic α7 nAChR decreased STAT3 phosphorylation. Conclusions Our data indicate that the activity of AFVN contributes to hepatic anti-inflammatory responses mediated by hVNS in ConA model of hepatitis in rats.

Published

2020

34. Case Report: Large Granular Lymphocyte Leukemia (LGLL)—A Case Series of Challenging Presentations.

Author

Pflug, Natali, Littauer, Annika, Beverungen, David, Sretenovic, Aleksandra, Wahnschaffe, Linus, Braun, Till, Dechow, Annika, Jungherz, Dennis, Otte, Moritz, Monecke, Astrid, Bach, Enrica, Franke, Georg-Nikolaus, Schwind, Sebastian, Jentzsch, Madlen, Platzbecker, Uwe, Herling, Marco, and Vucinic, Vladan

Subjects

KILLER cells, LYMPHOCYTES, LEUKEMIA, CASTLEMAN'S disease, LYMPHOPROLIFERATIVE disorders, T cells

Abstract

Large granular lymphocyte leukemia (LGLL) represents a rare group of diseases with considerable difficulties in their correct diagnostic workup and therapy. The major challenges lie in their distinction from reactive (including autoimmune) lymphoproliferations. Moreover, monoclonal LGL proliferative diseases are in fact a heterogeneous group of disorders, as recognized by the three subtypes in the current WHO classification. It distinguishes two chronic forms (the focus of this case series), namely T-LGLL and chronic lymphoproliferative disorders of Natural Killer cells (CLPD-NK) as well as aggressive NK-cell leukemia. In the clinical routine, the variable presentations and phenotypes of T-LGLL and CLPD-NK are underappreciated. The relevant differential diagnoses range from benign reactive T-cell expansions to other mature T-cell leukemias to highly aggressive γδ-lymphomas. T-LGLL or CLPD-NK patients suffer from a wide variety of symptoms often including, but not limited to, cytopenias or classical autoimmune phenomena. They receive treatments ranging from mere supportive measures (e.g. antibiotics, growth factors, transfusions) over strategies of immunosuppression up to anti-leukemic therapies. The diagnostic pitfalls range from recognition of the subtle T-cell proliferation, repeated establishment of monoclonality, assignment to a descript immunophenotypic pattern, and interpretations of molecular aberrancies. Here, we report a series of selected cases to represent the spectrum of LGLL. The purpose is to raise awareness among the scientifically or practically interested readers of the wide variety of clinical, immunological, and phenotypic features of the various forms of LGLL, e.g. of T-cell type, including its γδ forms or those of NK-lineage. We highlight the characteristics and courses of four unique cases from two academic centers, including those from a prospective nationwide LGLL registry. Each case of this instructive catalogue serves to transport a key message from the areas of (chronic inflammatory) contexts in which LGLL can arise as well as from the fields of differential diagnostics and of various treatment options. Implications for optimization in these areas are discussed. [ABSTRACT FROM AUTHOR]

Published

2022

35. Stat‐3 signaling promotes cell proliferation and metastasis of gastric cancer through PDCD4 downregulation

Author

Yue‐Lou Yang, Pei Liu, Dong Li, Qun Yang, Bin Li, and Xiang‐Jun Jiang

Subjects

gastric cancer, miR‐499‐5p, PDCD4, Stat‐3, Medicine (General), R5-920

Abstract

Abstract The present study explored a new downstream regulator of Stat‐3 signaling, miR‐499‐5p and its target gene programmed cell death 4 (PDCD4) in cell survival and metastasis of gastric cancer. Our results showed that miR‐499‐5p is significantly upregulated in human gastric cancer cell line SGC‐7901. We further demonstrated that miR‐499‐5p promotes gastric cancer cell proliferation and invasion in vitro. Mechanistically, we demonstrated that upregulation of miR‐499‐5p expression associated with inhibition of PDCD4; STAT3 transcriptional activation by IL‐6 is crucial for the upregulation of miR‐499‐5p expression. These results indicate that the STAT3‐miR‐499‐5p‐PDCD4 signaling axis plays an important role in gastric cancer progression and a potentially therapeutic target for gastric cancer treatment.

Published

2020

36. Case Report: Large Granular Lymphocyte Leukemia (LGLL)—A Case Series of Challenging Presentations

Author

Natali Pflug, Annika Littauer, David Beverungen, Aleksandra Sretenovic, Linus Wahnschaffe, Till Braun, Annika Dechow, Dennis Jungherz, Moritz Otte, Astrid Monecke, Enrica Bach, Georg-Nikolaus Franke, Sebastian Schwind, Madlen Jentzsch, Uwe Platzbecker, Marco Herling, and Vladan Vucinic

Subjects

LGL leukemia, STAT-3, immunosuppression, NK, TCR, CLPD-NK, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Large granular lymphocyte leukemia (LGLL) represents a rare group of diseases with considerable difficulties in their correct diagnostic workup and therapy. The major challenges lie in their distinction from reactive (including autoimmune) lymphoproliferations. Moreover, monoclonal LGL proliferative diseases are in fact a heterogeneous group of disorders, as recognized by the three subtypes in the current WHO classification. It distinguishes two chronic forms (the focus of this case series), namely T-LGLL and chronic lymphoproliferative disorders of Natural Killer cells (CLPD-NK) as well as aggressive NK-cell leukemia. In the clinical routine, the variable presentations and phenotypes of T-LGLL and CLPD-NK are underappreciated. The relevant differential diagnoses range from benign reactive T-cell expansions to other mature T-cell leukemias to highly aggressive γδ-lymphomas. T-LGLL or CLPD-NK patients suffer from a wide variety of symptoms often including, but not limited to, cytopenias or classical autoimmune phenomena. They receive treatments ranging from mere supportive measures (e.g. antibiotics, growth factors, transfusions) over strategies of immunosuppression up to anti-leukemic therapies. The diagnostic pitfalls range from recognition of the subtle T-cell proliferation, repeated establishment of monoclonality, assignment to a descript immunophenotypic pattern, and interpretations of molecular aberrancies. Here, we report a series of selected cases to represent the spectrum of LGLL. The purpose is to raise awareness among the scientifically or practically interested readers of the wide variety of clinical, immunological, and phenotypic features of the various forms of LGLL, e.g. of T-cell type, including its γδ forms or those of NK-lineage. We highlight the characteristics and courses of four unique cases from two academic centers, including those from a prospective nationwide LGLL registry. Each case of this instructive catalogue serves to transport a key message from the areas of (chronic inflammatory) contexts in which LGLL can arise as well as from the fields of differential diagnostics and of various treatment options. Implications for optimization in these areas are discussed.

Published

2022

37. Corrigendum: Effect of a high dose atorvastatin as added-on therapy on symptoms and serum AMPK/NLRP3 inflammasome and IL-6/STAT3 axes in patients with major depressive disorder: randomized controlled clinical study.

Author

Aldossary KM, Saad Ali L, Abdallah MS, Bahaa MM, Elmasry TA, Elberri EI, Kotkata FA, El Sabaa RM, Elmorsi YM, Kamel MM, Negm WA, Elberri AI, Hamouda AO, AlRasheed HA, Salahuddin MM, Yasser M, and Hamouda MA

Abstract

[This corrects the article DOI: 10.3389/fphar.2024.1381523.]., (Copyright © 2024 Aldossary, Saad Ali, Abdallah, Bahaa, Elmasry, Elberri, Kotkata, El Sabaa, Elmorsi, Kamel, Negm, Elberri, Hamouda, AlRasheed, Salahuddin, Yasser and Hamouda.)

Published

2024

38. The crystal structure of the domain-swapped dimer of onconase highlights some catalytic and antitumor activity features of the enzyme.

Author

Gotte, Giovanni, Campagnari, Rachele, Loreto, Domenico, Bettin, Ilaria, Calzetti, Federica, Menegazzi, Marta, and Merlino, Antonello

Subjects

*CATALYTIC activity, *CRYSTAL structure, *B cell lymphoma, *CELLULAR signal transduction, *QUATERNARY structure

Abstract

Onconase (ONC) is a monomeric amphibian "pancreatic-type" RNase endowed with remarkable anticancer activity. ONC spontaneously forms traces of a dimer (ONC-D) in solution, while larger amounts can be formed when ONC is lyophilized from mildly acidic solutions. Here, we report the crystal structure of ONC-D and analyze its catalytic and antitumor activities in comparison to ONC. ONC-D forms via the three-dimensional swapping of the N-terminal α-helix between two monomers, but it displays a significantly different quaternary structure from that previously modeled [Fagagnini A et al., 2017, Biochem J 474, 3767-81], and based on the crystal structure of the RNase A N-terminal swapped dimer. ONC-D presents a variable quaternary assembly deriving from a variable open interface, while it retains a catalytic activity that is similar to that of ONC. Notably, ONC-D displays antitumor activity against two human melanoma cell lines, although it exerts a slightly lower cytostatic effect than the monomer. The inhibition of melanoma cell proliferation by ONC or ONC-D is associated with the reduction of the expression of the anti-apoptotic B cell lymphoma 2 (Bcl2), as well as of the total expression and phosphorylation of the Signal Transducer and Activator of Transcription (STAT)-3. Phosphorylation is inhibited in both STAT3 Tyr705 and Ser727 key-residues, as well as in its upstream tyrosine-kinase Src. Consequently, both ONC species should exert their anti-cancer action by inhibiting the pro-tumor pleiotropic STAT3 effects deriving either by its phospho-tyrosine activation or by its non-canonical signaling pathways. Both ONC species, indeed, increase the portion of A375 cells undergoing apoptotic cell death. This study expands the variety of RNase domain-swapped dimeric structures, underlining the unpredictability of the open interface arrangement upon domain swapping. Structural data also offer valuable insights to analyze the differences in the measured ONC or ONC-D biological activities. [ABSTRACT FROM AUTHOR]

Published

2021

39. β‐Caryophyllene induces apoptosis and inhibits cell proliferation by deregulation of STAT‐3/mTOR/AKT signaling in human bladder cancer cells: An in vitro study.

Author

Yu, Xiaodong, Liao, Bo, Zhu, Pingyu, Cheng, Shulin, Du, Zhongbo, and Jiang, Guo

Subjects

INHIBITION of cellular proliferation, BLADDER cancer, CANCER cells, GENE expression, CELLULAR signal transduction

Abstract

The current study aimed to explore the antitumor effect of β‐caryophyllene (BCP) on two different cell lines of T24 and 5637 human bladder cancer (BC) cells and its potential molecular mechanisms in inhibition of STAT‐3/mTOR/AKT signaling pathways and the inductive process of apoptosis mechanism. The results indicated that BCP showed significant cytotoxicity in BC T24 and 5637 cells in a dose‐ and time‐dependent manner, and IC50 values were 40 µg/ml in the BC cells T24 and 5637. Reactive oxygen species (ROS) synthesis and apoptosis induction were significantly developed, but the mitochondrial membrane potential (Δψm) decreased on BCP treatment as detected by the fluorescence method. Moreover, cell migration was markedly reduced in BCP and Bax, Bcl‐2 mRNA expression was modified. Finally, it was found that the STAT‐3, mTOR, and AKT protein expressions were suppressed via inhibition of cytotoxicity in T24 and 5637 cells. Therefore, we finally concluded that BCP is an effective treatment against BC T24 and 5637 cells, and it has great chemotherapeutic potential for further bladder carcinoma treatment. [ABSTRACT FROM AUTHOR]

Published

2021

40. Novel STAT‐3 gain‐of‐function variant with hypogammaglobulinemia and recurrent infection phenotype.

Author

Erdős, Melinda, Tsumura, Miyuki, Kállai, Judit, Lányi, Árpád, Nyul, Zoltán, Balázs, György, Okada, Satoshi, and Maródi, László

Subjects

*DISEASE relapse, *RESPIRATORY infections, *AGAMMAGLOBULINEMIA, *INTERSTITIAL lung diseases, *PHENOTYPES, *RIB fractures, *SHORT stature

Abstract

Signal transducer and activator of transcription 3 (STAT‐3) gain‐of‐function (GOF) syndrome is an early‐onset monogenic inborn error of immunity characterized by multi‐organ autoimmune disorders, growth failure and lymphoproliferation. We describe that STAT‐3 GOF syndrome may be presented with hypogammaglobulinemia and recurrent severe upper and lower respiratory tract infections. In addition, the patient had lymphoproliferation, short stature and interstitial lung disease. Chest computerized tomography examinations showed mild bronchiectasis with areas of non‐fibrosing alveolar‐interstitial disease and maldevelopment of bilateral first ribs. Using Sanger sequencing, we revealed a novel c.508G>C, p.D170H STAT‐3 variant affecting the coiled coil domain of STAT‐3. Functional studies confirmed that p.D170H was a GOF variant, as shown by increased phosphorylated STAT‐3 (pSTAT‐3) and STAT‐3 transcriptional activity. Our observation suggests that STAT‐3 GOF syndrome can manifest in early childhood with hypogammaglobulinemia and recurrent severe respiratory tract infections. We suggest that patients with lymphoproliferation, hypogammaglobulinemia and severe recurrent infections should be screened for STAT‐3 variants, even if autoimmune manifestations are missing. [ABSTRACT FROM AUTHOR]

Published

2021

41. Human tumor necrosis factor alpha-induced protein eight-like 1 exhibited potent anti-tumor effect through modulation of proliferation, survival, migration and invasion of lung cancer cells.

Author

Bordoloi, Devivasha, Padmavathi, Ganesan, Banik, Kishore, Devi, Khwairakpam Amrita, Harsha, Choudhary, Girisa, Sosmitha, Buhrmann, Constanze, Shakibaei, Mehdi, and Kunnumakkara, Ajaikumar B.

Abstract

Lung cancer represents one of the most prevalent neoplasms across the globe. Tobacco smoking, exposure to different occupational and environmental carcinogens, and various dietary factors are strongly implicated in the development of lung cancer. The 5-year survival rate of lung cancer is extremely poor which can be attributed to its propensity for early spread, lack of appropriate biomarkers and proper therapeutic strategies for this aggressive neoplasm. Emerging evidence suggests tumor necrosis factor-α-induced protein eight like 1 (TIPE1 or TNFAIP8L1), which functions as a cell death regulator, to hold high prospect as an important biomarker. Interestingly, this protein was found to be significantly downregulated in human lung cancer tissues compared to normal lung tissues. In addition, this protein exerted marked downregulation in different stages and grades of lung tumor. Further knockout of TIPE1 led to the enhancement in proliferation, survival, migration and invasion of NCIH460 human lung cancer cells through modulation of Akt/mTOR/STAT-3 signaling cascade. In addition, TIPE1 was found to be involved in nicotine, 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanone, N-nitrosonornicotine and benzo[a]pyrene-mediated lung cancer through enhanced proliferation, survival and migration of lung cancer cells. Altogether, this newly identified protein plays a critical role in lung cancer pathogenesis and possess enormous prospect to serve as an important tool in the effective management of this aggressive neoplasm. [ABSTRACT FROM AUTHOR]

Published

2021

42. NIL10: A New IL10-Receptor Binding Nanoparticle That Induces Cardiac Protection in Mice and Pigs Subjected to Acute Myocardial Infarction through STAT3/NF-κB Activation

Author

Laura Tesoro, Ignacio Hernández, Rafael Ramírez-Carracedo, Javier Díez-Mata, Nunzio Alcharani, Beatriz Jiménez-Guirado, Karina Ovejero-Paredes, Marco Filice, Jose Luis Zamorano, Marta Saura, Carlos Zaragoza, and Laura Botana

Subjects

acute myocardial infarction, interleukin-10, nanoparticles, STAT-3, NF-κB, Pharmacy and materia medica, RS1-441

Abstract

(1) Background: Early response after acute myocardial infarction (AMI) prevents extensive cardiac necrosis, in which inflammation resolution, including expression of anti-inflammatory interleukin-10 (IL-10), may play a key role. (2) Methods: We synthesized NIL10, a micelle-based nanoparticle, to target IL-10 receptor in mice and pigs subjected to AMI. (3) Results: Administration of NIL10 induced cardiac protection of wild-type and IL-10 knockout mice and pigs subjected to AMI. Cardiac protection was not induced in IL-10-receptor null mice, as shown by a significant recovery of cardiac function, in which inflammatory foci and fibrosis were strongly reduced, together with the finding that resolving M2-like macrophage populations were increased after day 3 of reperfusion. In addition, anti-inflammatory cytokines, including IL-4, IL-7, IL-10, IL-13, IL-16, and IL-27 were also elevated. Mechanistically, NIL10 induced activation of the IL-10 receptor/STAT-3 signaling pathway, and STAT3-dependent inhibition of nuclear translocation of pro-inflammatory NF-ĸB transcription factor. (4) Conclusions: Taken together, we propose using NIL10 as a novel therapeutic tool against AMI-induced cardiac damage.

Published

2022

43. Punicalagin induces ROS‐mediated apoptotic cell death through inhibiting STAT3 translocation in lung cancer A549 cells.

Author

Fang, Le, Wang, Hong, Zhang, Jie, and Fang, Xiaolei

Subjects

LUNG cancer, CELL death, CANCER cells, OVERALL survival, CANCER chemotherapy

Abstract

Lung cancer is a noxious disease with substandard overall survival. Despite this, there are several treatment strategies for lung cancer include chemotherapy, radiotherapy, surgery; however, the overall survival remains poor. Punicalagin has been documented as a potential phytomedicine to selectively inhibit the progression and expansion of numerous cancers. In the present study, we evaluated the antiproliferative ability of punicalagin against lung cancer A549 cells by inducing apoptosis by inhibiting STAT‐3 activation. Punicalagin induces toxic effects of A549 cells in a dose‐associated manner after 24 h treatment. And we also observed that punicalagin (10, 20, and 30 μM) induced reactive oxygen species generation, alters the mitochondrion membrane potential and apoptotic morphological changes in A549 cells. The STAT‐3 overexpression regulates apoptosis, proliferation, and angiogenesis. Here, the punicalagin inhibited STAT‐3 translocation and thereby induces apoptosis by inhibiting expression Bcl‐2 and enhanced expression of Bax, cytochrome‐c, caspase‐9, and caspase‐3 in A549 cells. Hence, we stated that the punicalagin is a possible therapy for non‐small cell lung, malignancies. Altogether, the punicalagin is a promising phytomedicine in malignancy treatment and further endeavors are needed to unveil the complete potential. [ABSTRACT FROM AUTHOR]

Published

2021

44. Prognostic values and clinical implications of programmed cell death-ligand 1 (PD-L1), fork head transcription factor P-1 (FOXP-1) and signal transducer and activator of transcription-3 (STAT-3) expression in diffuse large B-cell lymphoma (DLBCL); an immunohistochemical study

Author

Ola A. Harb, Randa Mohamed Kaf, Heba F. Taha, Rham Z. Ahmed, Doaa Mandour, Ahmed Z. Al Attar, Ayman Fathy, Abdelwahab S. Almoregy, Gamal Osman, and Loay M. Gertallah

Subjects

DLBCL, PD-L1, FOXP-1, STAT-3, Immunohistochemistry, Prognosis, Surgery, RD1-811, Pathology, RB1-214

Abstract

Abstract Context PD-L1 is an inhibitory ligand that functions as an essential immune checkpoint. FOXP-1 is a member of the FOXP family. STAT-3 plays a critical role in regulation of cell proliferation and survival. The detailed expression of the three markers together in DLBCL tissues and their prognostic value in patients with DLBCL were not fully investigated. Aim was to assess the expression of PD-L1, FOXP-1 and STAT-3 in diffuse large B-cell lymphoma (DLBCL) and to correlate their expression with the pathological findings, prognostic parameters and clinical implications of patients. Methods PD-L1, FOXP-1 and STAT-3 were assessed in DLBCL tissues derived from 50 patients using immunohistochemistry. Patients were followed up for 3 years for response to therapy progression, recurrence and survival. Results High PD-L1 expression was associated with bone marrow involvement (p = 0.004), extra-nodal involvement (p = 0.006) and advanced stage (p = 0.003). High FOXP-1 expression was associated with presence of bone marrow involvement and high risk group (p

Published

2019

45. Growth-Suppressive and Apoptosis-Inducing Effects of Tetrandrine in SW872 Human Malignant Liposarcoma Cells via Activation of Caspase-9, Down-Regulation of XIAP and STAT-3, and ER Stress

Author

Mohammed Samsuzzaman and Byeong-Churl Jang

Subjects

tetrandrine, SW872, apoptosis, caspase-9, STAT-3, ER stress, Microbiology, QR1-502

Abstract

Liposarcoma is a rare and heterogeneous soft tissue malignant tumor and has a significant impact on mortality with a poor prognosis. To date, there is no effective treatment for liposarcoma, whereas surgical resection is only the gold treatment with numerous adverse effects. Here we investigated whether tetrandrine inhibits the growth of SW872 human malignant liposarcoma cells. Of note, tetrandrine at 10 μM vastly inhibited growth and induced apoptosis, as evidenced by increased nuclear DNA fragmentation and sub-G1 population of SW872 cells. Mechanistically, treatment with tetrandrine led to activation of caspase-9/3 in SW872 cells, and z-VAD-fmk, a pan-caspase inhibitor, attenuated the tetrandrine-induced apoptosis and growth suppression in SW872 cells. In addition, tetrandrine treatment resulted in down-regulation of XIAP andSTAT-3 in SW872 cells, and importantly knockdown of STAT-3 caused a significant reduction of the cell survival. Tetrandrine also had abilities to up-regulate not only the expression of GRP78 and ATF-4 but also the phosphorylation of eIF-2α in SW872 cells. In summary, these results demonstrated that tetrandrine has strong growth-suppressive and apoptosis-inducing effects on SW872 cells, which are mediated through control of the intrinsic caspase pathway, down-regulation of XIAP and STAT-3, and triggering ER stress.

Published

2022

46. Anti-Growth, Anti-Angiogenic, and Pro-Apoptotic Effects by CX-4945, an Inhibitor of Casein Kinase 2, on HuCCT-1 Human Cholangiocarcinoma Cells via Control of Caspase-9/3, DR-4, STAT-3/STAT-5, Mcl-1, eIF-2α, and HIF-1α

Author

Saini Wang, Anil Kumar Yadav, Jin-Yi Han, Keun Soo Ahn, and Byeong-Churl Jang

Subjects

CX-4945, CK2, STAT-3, Mcl-1, HIF-1α, HuCCT-1, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Overexpression of casein kinase 2 (CK2) has an oncogenic and pro-survival role in many cancers. CX-4945 (Silmitasertib) is a CK2 inhibitor with anti-cancerous and anti-angiogenic effects. Up to date, the anti-cancer effect and mechanism of CX-4945 on human cholangiocarcinoma (CCA) remain unclear. This study investigated whether CX-4945 inhibits growth and induces apoptosis of HuCCT-1 cells, a human CCA cell line. Of note, treatment with CX-4945 at 20 μM markedly reduced survival and induced apoptosis of HuCCT-1 cells, as evidenced by nuclear DNA fragmentation, PARP cleavage, activation of caspase-9/3, and up-regulation of DR-4. Although CX-4945 did not affect the phosphorylation and expression of CK2, it vastly inhibited the phosphorylation of CK2 substrates, supporting the drug’s efficacy in inhibiting CK2 and its downstream pathway. Importantly, knockdown of CK2 that partially suppressed the phosphorylation of CK2 substrates resulted in a significant reduction of HuCCT-1 cell survival. In addition, CX-4945 reduced the phosphorylation and expression of STAT-3 and STAT-5 in HuCCT-1 cells, and pharmacological inhibition or respective knockdown of these proteins resulted in significant growth suppression of HuCCT-1 cells. CX-4945 also had abilities to decrease Mcl-1 expression while increasing eIF-2α phosphorylation in HuCCT-1 cells. Furthermore, there was a time-differential negative regulation of HIF-1α expression by CX-4945 in HuCCT-1 cells, and knockdown of HIF-1α caused a significant reduction of the cell survival. In summary, these results demonstrated that CX-4945 has anti-growth, anti-angiogenic, and pro-apoptotic effects on HuCCT-1 cells, which are mediated through control of CK2, caspase-9/3, DR-4, STAT-3/5, Mcl-1, eIF-2α, and HIF-1α.

Published

2022

47. Targeting Transcriptional Factors in Gastrointestinal Cancers and Future Prospective

Author

Nagaraju, Ganji Purnachandra, Bramhachari, Pallaval Veera, Pattnaik, Subasini, Nagaraju, Ganji Purnachandra, editor, and Bramhachari, Pallaval Veera, editor

Published

2017

48. Salidroside regulates imbalance of Th17/Treg and promotes ischemic tolerance by targeting STAT-3 in cerebral ischemia-reperfusion injury.

Author

Lele Yin, Dongyun Ouyang, Lihong Lin, Xiufeng Xin, Yuhua Ji, Yin, Lele, Ouyang, Dongyun, Lin, Lihong, Xin, Xiufeng, and Ji, Yuhua

Subjects

*MONONUCLEAR leukocytes, *T helper cells, *MYOCARDIAL reperfusion, *T cells, *BLOOD cells

Abstract

Introduction: The balance between Th17 and Treg cells controls the immune response and is an important regulator of helper T cells acting on autoimmune diseases. Focal cerebral ischemia-reperfusion injury can induce imbalance of Th17/Treg cells in the brain and the peripheral immune system of rats. The aim of this study was to investigate the effect of salidroside (Sal) on the ratio of Th17 and Treg cells in an adult rat model of middle cerebral artery occlusion (MCAO).Material and Methods: Forty rats were divided into 4 groups: normal group, sham group, surgery group, and Sal group. After treatment, the neurological deficits in rats were evaluated. Peripheral blood mononuclear cells were isolated and the count of Th17 and Treg cells was detected by flow cytometry. The infarct size and expression of RORγt and Foxp3 were detected in rat brain tissue. Rat spleen cells were isolated, CD4+ T cells were purified by immunomagnetic beads. Treg cells were induced by adding cytokine TGF-β. Th17 cells were induced by adding cytokine IL-6. The expression of STAT-3 was inhibited by SiRNA, and the effect of Sal on the differentiation of Th17/Treg cells was analyzed. The expression levels of IL-6, TNF-α, MCP-1, STAT-3 and NF-κ-B2 proteins were examined.Results: The results show that MCAO can induce an imbalance of Th17 and Treg cells in peripheral blood of rats. Sal treatment can significantly reduce the neurological deficit and infarct size of MCAO rats, reverse the oxidative stress of rat brain tissue, and inhibit the apoptosis of brain cells in MCAO rats. In the brain tissue of MCAO rats, Sal could significantly inhibit the expression of IL-6, TNF-α, MCP-1, STAT-3 and NF-κ-B2. Down-regulation of STAT-3 significantly reversed the therapeutic effects of Sal treatment.Conclusions: Our results indicate that Sal can increase the tolerance of rat brain tissue to ischemia, inhibit cell apoptosis and reduce oxidative stress by targeting STAT-3. [ABSTRACT FROM AUTHOR]

Published

2021

49. Oleyl Conjugated Histidine-Arginine Cell-Penetrating Peptides as Promising Agents for siRNA Delivery

Author

Muhammad Imran Sajid, Dindyal Mandal, Naglaa Salem El-Sayed, Sandeep Lohan, Jonathan Moreno, and Rakesh Kumar Tiwari

Subjects

siRNA, STAT-3, cell-penetrating peptides, siRNA delivery, RNA interference, Western blotting, Pharmacy and materia medica, RS1-441

Abstract

Recent approvals of siRNA-based products motivated the scientific community to explore siRNA as a treatment option for several intractable ailments, especially cancer. The success of approved siRNA therapy requires a suitable and safer drug delivery agent. Herein, we report a series of oleyl conjugated histidine–arginine peptides as a promising nonviral siRNA delivery tool. The conjugated peptides were found to bind with the siRNA at N/P ratio ≥ 2 and demonstrated complete protection for the siRNA from early enzymatic degradation at N/P ratio ≥ 20. Oleyl-conjugated peptide -siRNA complexes were found to be noncytotoxic in breast cancer cells (MCF-7 and MDA-MB-231) and normal breast epithelial cells (MCF 10A) at N/P ratio of ~40. The oleyl-R3-(HR)4 and oleyl-R4-(HR)4 showed ~80-fold increased cellular uptake in MDA-MB-231 cells at N/P 40. Moreover, the conjugated peptides-siRNA complexes form nanocomplexes (~115 nm in size) and have an appropriate surface charge to interact with the cell membrane and cause cellular internalization. Furthermore, this study provides a proof-of-concept that oleyl-R5-(HR)4 can efficiently silence STAT-3 gene (~80% inhibition) in MDA-MB-231 cells with similar effectiveness to Lipofectamine. Further exploration of this approach holds a great promise in discovering a successful in vivo siRNA delivery agent with a favorable pharmacokinetic profile.

Published

2022

50. Targeting IL‐10, ZO‐1 gene expression and IL‐6/STAT‐3 trans‐signaling by a combination of atorvastatin and mesalazine to enhance anti‐inflammatory effects and attenuates progression of oxazolone‐induced colitis.

Author

El‐Mahdy, Nageh Ahmed, El‐Sayad, Magda El‐Sayed, El‐Kadem, Aya Hassan, and Abu‐Risha, Sally El‐Sayed

Subjects

*COLITIS, *INTERLEUKIN receptors, *MESALAMINE, *TUMOR necrosis factors, *GENE expression, *ULCERATIVE colitis, *INFLAMMATORY bowel diseases

Abstract

Ulcerative colitis (UC) is a chronic inflammatory disease characterized by diffused inflammation of the colon and rectum mucosa. The pathogenesis of UC is multifactorial, and the exact underlying mechanisms remain poorly understood. This study aims to investigate the effect of mesalazine and atorvastatin combination in enhancing anti‐inflammatory effects and attenuates progression of oxazolone colitis in rats. In the present study, male albino rats (N = 60) were divided into six groups (10 rats each), the first two groups served as normal control and a control saline group. Colitis was induced by intra‐rectal administration of oxazolone in the 5th and 7th days after pre‐sensitization. Then, rats were divided into untreated group, groups treated with mesalazine or atorvastatin or their combination. Colitis was assessed by colon length, body weight, and incidence of diarrhea, rectal bleeding, and histopathology of colon tissue. Colon tissues were used for measuring interleukin 6 (IL‐6), tumor necrosis factor alpha (TNF‐α), IL‐13, signal transducer and activator of transcription‐3 (STAT‐3), myeloperoxidase activity (MPO), reduced glutathione(GSH), and tissue expression of IL‐10, tight junction protein zonula occludens (ZO‐1), and caspase‐3 genes. The combination therapy significantly attenuated progression of UC by decreasing incidence of diarrhea, rectal bleeding, weight loss, IL‐13, IL‐6, TNF‐α, STAT‐3, caspase‐3, and MPO activity and significantly increased IL‐10, ZO‐1, colon length, and GSH content, and these effects were more superior to single drugs. These findings showed that combination therapy was able to ameliorate progression of UC and enhance anti‐inflammatory effects possibly by restoring IL‐10 and ZO‐1 levels and limiting IL‐6/STAT‐3 trans‐signaling. [ABSTRACT FROM AUTHOR]

Published

2021