Your search keyword '"AUTOPHAGY"' showing total 196,495 results

201. A Selective Melatonin 2 Receptor Agonist, IIK7, Relieves Blue Light-Induced Corneal Damage by Modulating the Process of Autophagy and Apoptosis.

Author

Yoon, Hyeon-Jeong, Jiang, Enying, Liu, Jingting, Jin, Hui, Yoon, Hee Su, Choi, Ji Suk, Moon, Ja Young, and Yoon, Kyung Chul

Subjects

*BLUE light, *REACTIVE oxygen species, *T cells, *LABORATORY mice, *CORNEA, *TEARS (Body fluid)

Abstract

This study aims to investigate the effect of the selective MT2 receptor agonist, IIK7, on corneal autophagy and apoptosis, aiming to reduce corneal epithelial damage and inflammation from blue light exposure in mice. Eight-week-old C57BL/6 mice were divided into BL-exposed (BL) and BL-exposed with IIK7 treatment (BL + IIK7 group). Mice underwent blue light exposure (410 nm, 100 J) twice daily with assessments at baseline and on days 3, 7, and 14. Corneal samples were analyzed for MT2 receptor expression, autophagy markers (LC3-II and p62), and apoptosis indicators (BAX expression and TUNEL assay). Then, mice were assigned to normal control, BL, and BL + IIK7. Ocular surface parameters, including corneal fluorescein staining scores, tear volume, and tear film break-up time, were evaluated on days 7 and 14. On day 14, reactive oxygen species (ROS) levels and CD4+ IFN-γ+ T cells percentages were measured. The BL group exhibited higher LC3-II and p62 expression, while the BL + IIK7 group showed reduced expression (p < 0.05). The TUNEL assay showed reduced apoptosis in the BL + IIK7 group compared to the BL group. ROS levels were lower in the BL + IIK7 group. The BL + IIK7 group showed improved ocular surface parameters, including decreased corneal fluorescein staining and increased tear volume. The percentages of CD4+ IFN-γ+ T cells indicated reduced inflammatory responses in the BL + IIK7 group. The MT2 receptor agonist IIK7 regulates corneal autophagy and apoptosis, reducing corneal epithelial damage and inflammation from blue light exposure. [ABSTRACT FROM AUTHOR]

Published

2024

202. Interconnection of CD133 Stem Cell Marker with Autophagy and Apoptosis in Colorectal Cancer.

Author

Sipos, Ferenc and Műzes, Györgyi

Subjects

*CANCER stem cells, *COLORECTAL cancer, *PROGENITOR cells, *CANCER cells, *PHOSPHATIDYLINOSITOL 3-kinases

Abstract

CD133 protein expression is observable in differentiated cells, stem cells, and progenitor cells within normal tissues, as well as in tumor tissues, including colorectal cancer cells. The CD133 protein is the predominant cell surface marker utilized to detect cancer cells exhibiting stem cell-like characteristics. CD133 alters common abnormal processes in colorectal cancer, such as the phosphoinositide 3-kinase (PI3K)/protein kinase B (AKT) and Wnt/β-catenin pathways. Autophagy is a cellular self-digestion mechanism that preserves the intracellular milieu and plays a dual regulatory role in cancer. In cancer cells, apoptosis is a critical cell death mechanism that can impede cancer progression. CD133 can modulate autophagy and apoptosis in colorectal cancer cells via several signaling pathways; hence, it is involved in the regulation of these intricate processes. This can be an explanation for why CD133 expression is associated with enhanced cellular self-renewal, migration, invasion, and survival under stress conditions in colorectal cancer. The purpose of this review article is to explain the complex relationship between the CD133 protein, apoptosis, and autophagy. We also want to highlight the possible ways that CD133-mediated autophagy may affect the apoptosis of colorectal cancer cells. Targeting the aforementioned mechanisms may have a significant therapeutic role in eliminating CD133-positive stem cell-phenotype colorectal cancer cells, which can be responsible for tumor recurrence. [ABSTRACT FROM AUTHOR]

Published

2024

203. Targeting Lipid Metabolism in Cancer Stem Cells for Anticancer Treatment.

Author

Singh, Manish Kumar, Han, Sunhee, Kim, Sungsoo, and Kang, Insug

Subjects

*DRUG resistance in cancer cells, *CANCER stem cells, *METABOLIC reprogramming, *LIPID metabolism, *MEMBRANE permeability (Biology), *HOMEOSTASIS

Abstract

Cancer stem cells (CSCs), or tumor-initiating cells (TICs), are small subpopulations (0.0001–0.1%) of cancer cells that are crucial for cancer relapse and therapy resistance. The elimination of each CSC is essential for achieving long-term remission. Metabolic reprogramming, particularly lipids, has a significant impact on drug efficacy by influencing drug diffusion, altering membrane permeability, modifying mitochondrial function, and adjusting the lipid composition within CSCs. These changes contribute to the development of chemoresistance in various cancers. The intricate relationship between lipid metabolism and drug resistance in CSCs is an emerging area of research, as different lipid species play essential roles in multiple stages of autophagy. However, the link between autophagy and lipid metabolism in the context of CSC regulation remains unclear. Understanding the interplay between autophagy and lipid reprogramming in CSCs could lead to the development of new approaches for enhancing therapies and reducing tumorigenicity in these cells. In this review, we explore the latest findings on lipid metabolism in CSCs, including the role of key regulatory enzymes, inhibitors, and the contribution of autophagy in maintaining lipid homeostasis. These recent findings may provide critical insights for identifying novel pharmacological targets for effective anticancer treatment. [ABSTRACT FROM AUTHOR]

Published

2024

204. Crosstalk of Hyperglycaemia and Cellular Mechanisms in the Pathogenesis of Diabetic Kidney Disease.

Author

Efiong, Esienanwan Esien, Bazireh, Homa, Fuchs, Markéta, Amadi, Peter Uchenna, Effa, Emmanuel, Sharma, Sapna, and Schmaderer, Christoph

Subjects

*DIABETIC nephropathies, *RENAL fibrosis, *ADVANCED glycation end-products, *RENAL replacement therapy, *CHRONIC kidney failure

Abstract

Among all nephropathies, diabetic kidney disease (DKD) is the most common cause of kidney impairment advancement to end-stage renal disease (ESRD). Although DKD has no cure, the disease is commonly managed by strict control of blood glucose and blood pressure, and in most of these cases, kidney function often deteriorates, resulting in dialysis, kidney replacement therapy, and high mortality. The difficulties in finding a cure for DKD are mainly due to a poor understanding of the underpinning complex cellular mechanisms that could be identified as druggable targets for the treatment of this disease. The review is thus aimed at giving insight into the interconnection between chronic hyperglycaemia and cellular mechanistic perturbations of nephropathy in diabetes. A comprehensive literature review of observational studies on DKD published within the past ten years, with 57 percent published within the past three years was carried out. The article search focused on original research studies and reviews published in English. The articles were explored using Google Scholar, Medline, Web of Science, and PubMed databases based on keywords, titles, and abstracts related to the topic. This article provides a detailed relationship between hyperglycaemia, oxidative stress, and various cellular mechanisms that underlie the onset and progression of the disease. Moreover, it also shows how these mechanisms affect organelle dysfunction, resulting in fibrosis and podocyte impairment. The advances in understanding the complexity of DKD mechanisms discussed in this review will expedite opportunities to develop new interventions for treating the disease. [ABSTRACT FROM AUTHOR]

Published

2024

205. IFN-γ induces acute graft-versus-host disease by promoting HMGB1-mediated nuclear-to-cytoplasm translocation and autophagic degradation of p53.

Author

Shiyu Wang, Tingting Cheng, Xu Chen, Cong Zeng, Wei Qin, and Yajing Xu

Subjects

*HEMATOPOIETIC stem cell transplantation, *AUTOPHAGY, *T cells, *GRAFT versus host disease, *PROTEOLYSIS

Abstract

Acute graft-versus-host disease (aGVHD) poses a significant impediment to achieving a more favourable therapeutic outcome in allogeneic hematopoietic stem cell transplantation (allo-HSCT). Our prior investigations disclosed a correlation between p53 down-regulation in CD4+ T cells and the occurrence of aGVHD. Notably, the insufficiency of the CCCTC-binding factor (CTCF) emerged as a pivotal factor in repressing p53 expression. However, the existence of additional mechanisms contributing to the reduction in p53 expression remains unclear. Interferon (IFN)-γ, a pivotal proinflammatory cytokine, assumes a crucial role in regulating alloreactive T-cell responses and plays a complex part in aGVHD development. IFN-γ has the capacity to induce autophagy, a vital catabolic process facilitating protein degradation, in various cell types. Presently, whether IFN-γ participates in the development of aGVHD by instigating the autophagic degradation of p53 in CD4+ T cells remains an unresolved question. In the present study, we demonstrated that heightened levels of IFN-γ in the plasma during aGVHD promoted the activation, proliferation, and autophagic activity of CD4+ T cells. Furthermore, IFN-γ induced the nuclear-to-cytoplasm translocation and autophagy-dependent degradation of p53 in CD4+ T cells. The translocation and autophagic degradation of p53 were contingent upon HMGB1, which underwent up-regulation and translocation from the nucleus to the cytoplasm following IFN-γ stimulation. In conclusion, our data unveil a novel mechanism underlying p53 deficiency in CD4+ T cells among aGVHD patients. This deficiency is induced by IFN-γ and relies on autophagy, establishing a link between IFN-γ, HMGB1-mediated translocation, and the autophagic degradation of p53. [ABSTRACT FROM AUTHOR]

Published

2024

206. The autophagy initiation factor ATG13mRNA is stabilized by the RNA‐binding protein YBX3.

Author

Pfuhler, Liva, Awad, Silina, Skipper, William, Lavietes, Jeremy, Sah, Thomas, Ho, Kayla, Ivanova, Radha, and Cooke, Amy

Subjects

*INITIATION factors (Biochemistry), *PROTEIN expression, *AUTOPHAGY, *NEURODEGENERATION, *BREAST cancer

Abstract

Autophagy, a highly conserved form of cellular recycling, is essential for cellular homeostasis. Its dysregulation has been linked to neurodegenerative diseases and various cancers, including breast cancer. We set out to determine if the RNA‐binding protein (RBP) YBX3 regulates autophagy mRNAs, as previous findings suggest YBX3 depletion reduces distinct autophagy transcripts. We found that YBX3 interacts with and stabilizes the mRNA of the autophagy initiation factor ATG13 in HeLa, which in turn increases ATG13 protein expression. We have shown that this requires the 3′ untranslated region (UTR) of ATG13 and occurs in other human cell lines, including HEK293, HepG2, and HCT116. Together, our data suggest a novel regulatory role for YBX3 of autophagy initiation through posttranscriptional control of ATG13 mRNA stability. [ABSTRACT FROM AUTHOR]

Published

2024

207. NIR-II light based combinatorial management of hypertrophic scar by inducing autophagy in fibroblasts.

Author

Dong, Yunxian, Wang, Haibin, Zhang, Youliang, Wu, Yanqun, Lu, Ling, Yu, Hao, Zhou, Lingcong, Zhao, Peng, Ouyang, Sixue, Song, Zibin, Hu, Zhicheng, Lv, Dongming, Rong, Yanchao, Zhao, Zirui, Tao, Jia, Tang, Bing, and Luo, Shengkang

Subjects

*REACTIVE oxygen species, *CHINESE medicine, *CELL death, *FIBROBLASTS, *AUTOPHAGY, *HYPERTROPHIC scars

Abstract

The hypertrophic scar (HS) is a prevalent cutaneous fibrotic disorder that impacts both the aesthetic and functional aspects of the skin, there is an urgent need for a highly safe and effective approach to address the challenge of HS with thick and deep types. Inspired by the superior deep tissue penetrative ability of near-infrared-II (NIR-II) light and potential mitochondria ROS inducing effect of Chinese medicine lycorine (LYC), we fabricated a Cu2Se@LYC (CL) composite by encapsulating LYC on polyvinyl pyrrolidone (PVP) modified Cu2Se nanoparticles. After NIR-II irradiation, CL could induce the generation of reactive oxygen species (ROS) and mitochondrial damage in hypertrophic scar fibroblasts (HSFs). The subsequent release of cytochrome C (cyt-c) from mitochondria into the cytoplasm and upregulation of beclin1 leads to the activation of endogenous apoptosis and autophagy-mediated cell death. The CL + NIR-II treatment exhibited a pronounced anti-scarring effect in both in vitro and in vivo rabbit ear scar models, leading to a significant reduction in the fibrotic markers including Collagen I/III and α-smooth muscle actin (α-SMA). This study comprehensively investigated the crucial role of HSFs' autophagy in scar management and proposed a safe and effective therapy based on NIR-II laser for clinical application. [ABSTRACT FROM AUTHOR]

Published

2024

208. Supplementation of spermidine enhances the quality of postovulatory aged porcine oocytes.

Author

Bai, Jie, Zhang, Yu, Li, Na, Cui, Zhaokang, Zhang, Hanwen, Liu, Yiting, Miao, Yilong, Sun, Shaochen, and Xiong, Bo

Subjects

*HUMAN reproductive technology, *CHROMOSOME structure, *EMBRYOS, *FERTILIZATION in vitro, *REACTIVE oxygen species

Abstract

Background: Spermidine (SPD) is an intermediate compound in the polyamine metabolism which takes critical part in a variety of cellular processes. In particular, it has been reported to exert anti-aging effects, suppress the age-related diseases, and extend lifespan across species. However, whether it has the favorable influence on the quality of postovulatory aged oocytes remains elusive. Methods: Immunostaining and fluorescence intensity measurement were used to evaluate the effects of postovulatory aging and SPD supplementation on the oocyte fragmentation, spindle/chromosome structure, actin polymerization, dynamics of cortical granules (CGs) and ovastacin, mitochondrial distribution and function, as well as autophagy levels. In addition, in vitro sperm binding assay and in vitro fertilization (IVF) experiment were applied to assess the impacts of postovulatory aging and SPD supplementation on the sperm binding ability and fertilization capacity of oocytes. Results: Here, we showed that supplementation of SPD during postovulatory aging could relieve the deterioration of porcine oocytes. Specifically, we found that postovulatory aging impaired the oocyte quality by damaging the morphological integrity of oocytes, maintenance of spindle/chromosome structure, and dynamics of actin cytoskeleton. Postovulatory aging also weakened the sperm binding ability and fertilization capacity of oocytes by compromising the distribution pattern of CGs and their content ovastacin. Notably, supplementation of SPD attenuated these defects in postovulatory aged porcine oocytes via strengthening mitochondrial function, eliminating excessive reactive oxygen species (ROS), inhibiting apoptosis, and enhancing autophagy levels. Conclusion: Altogether, our findings demonstrate that SPD supplementation is a feasible approach to ameliorate the quality of postovulatory aged oocytes, which can be potentially applied to the human assisted reproductive technology (ART) and in vitro production of animal embryos. [ABSTRACT FROM AUTHOR]

Published

2024

209. The N6‐methyladenosine landscape of ovarian development and aging highlights the regulation by RNA stability and chromatin state.

Author

Hu, Xiujuan, Lu, Jiafeng, Ding, Chenyue, Li, Jincheng, Zou, Qinyan, Xia, Wenjuan, Qian, Chunfeng, Li, Hong, and Huang, Boxian

Subjects

*CELLULAR aging, *ENDOGENOUS retroviruses, *KNOCKOUT mice, *DEMETHYLASE, *LABORATORY mice

Abstract

The versatile epigenetic modification known as N6‐methyladenosine (m6A) has been demonstrated to be pivotal in numerous physiological and pathological contexts. Nonetheless, the precise regulatory mechanisms linking m6A to histone modifications and the involvement of transposable elements (TEs) in ovarian development and aging are still not completely understood. First, we discovered that m6A modifications are highly expressed during ovarian aging (OA), with significant contributions from decreased m6A demethylase FTO and overexpressed m6A methyltransferase METTL16. Then, using FTO knockout mouse model and KGN cell line, we also observed that FTO deletion and METTL16 overexpression significantly increased m6A levels. This led to the downregulation of the methyltransferase SUV39H1, resulting in reduced H3K9me3 expression. The downregulation of SUV39H1 and H3K9me3 primarily activated LTR7 and LTR12, subsequently activating ERV1. This resulted in a decrease in cell proliferation, while the levels of apoptosis, cellular aging markers, and autophagy markers significantly increased in OA. In summary, our study offers intriguing insights into the role of m6A in regulating DNA epigenetics, including H3K9me3 and TEs, as well as autophagy, thereby accelerating OA. [ABSTRACT FROM AUTHOR]

Published

2024

210. Autophagy: A New Avenue and Biochemical Mechanisms to Mitigate the Climate Change.

Author

Azmat, Muhammad Abubakkar, Zaheer, Malaika, Shaban, Muhammad, Arshad, Saman, Hasan, Muhammad, Ashraf, Alyan, Naeem, Muhammad, Ahmad, Aftab, Munawar, Nayla, and Lee, Tzong-Shyuan

Subjects

*CELL anatomy, *DEFICIENCY diseases, *ABIOTIC stress, *AUTOPHAGY, *LYSOSOMES

Abstract

Autophagy is a preserved process in eukaryotes that allows large material degeneration and nutrient recovery via vacuoles or lysosomes in cytoplasm. Autophagy starts from the moment of induction during the formation of a phagophore. Degradation may occur in the autophagosomes even without fusion with lysosome or vacuole, particularly in microautophagosomes. This process is arbitrated by the conserved machinery of basic autophagy‐related genes (ATGs). In selective autophagy, specific materials are recruited by autophagosomes via receptors. Selective autophagy targets a vast variety of cellular components for degradation, i.e., old or damaged organelles, aggregates, and inactive or misfolded proteins. In optimal conditions, autophagy in plants ensures cellular homeostasis, proper plant growth, and fitness. Moreover, autophagy is essential during stress responses in plants and aids in survival of plants. Several biotic and abiotic stresses, i.e., pathogen infection, nutrient deficiency, plant senescence, heat stress, drought, osmotic stress, and hypoxia induce autophagy in plants. Cell death is not a stress, which induces autophagy but in contrast, sometimes it is a consequence of autophagy. In this way, autophagy plays a vital role in plant survival during harsh environmental conditions by maintaining nutrient concentration through elimination of useless cellular components. This review discussed the recent advances regarding regulatory functions of autophagy under normal and stressful conditions in plants and suggests future prospects in mitigating climate change. Autophagy in plants offers a viable way to increase plant resilience to climate change by increasing stress tolerance and nutrient usage efficiency. [ABSTRACT FROM AUTHOR]

Published

2024

211. Autophagy and inflammasome activation are associated with poor response to FLT3 inhibitors in patients with FLT3-ITD acute myeloid leukemia.

Author

Santos de Macedo, Brunno Gilberto, Albuquerque de Melo, Manuela, Pereira-Martins, Diego Antonio, Machado-Neto, João Agostinho, and Traina, Fabíola

Subjects

*ACUTE myeloid leukemia, *INFLAMMASOMES, *DRUG resistance, *AUTOPHAGY, *SORAFENIB

Abstract

Beyond its clinical diversity and severity, acute myeloid leukemia (AML) is known for its complex molecular background and for rewiring biological processes to aid disease onset and maintenance. FLT3 mutations are among the most recurring molecular entities that cooperatively drive AML, and their inhibition is a critical molecularly oriented therapeutic strategy. Despite being a promising avenue, it still faces challenges such as intrinsic and acquired drug resistance, which led us to investigate whether and how autophagy and inflammasome interact and whether this interaction could be leveraged to enhance FLT3 inhibition as a therapeutic strategy. We observed a strong and positive correlation between the expression of key genes associated with autophagy and the inflammasome. Gene set enrichment analysis of the FLT3-ITD samples and their ex vivo response to five different FLT3 inhibitors revealed a common molecular signature compatible with autophagy and inflammasome activation across all poor responders. Inflammasome activation was also shown to strongly increase the likelihood of a poor ex vivo response to the FLT3 inhibitors quizartinib and sorafenib. These findings reveal a distinct molecular pattern within FLT3-ITD AML samples that underscores the necessity for further exploration into how approaching these supportive parallel yet altered pathways could improve therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2024

212. A novel ER stress regulator ARL6IP5 induces reticulophagy to ameliorate the prion burden.

Author

Kamble, Kajal, Kumar, Ujjwal, Aahra, Harsh, Yadav, Mohit, Bhola, Sumnil, and Gupta, Sarika

Subjects

*UNFOLDED protein response, *PRION diseases, *AMP-activated protein kinases, *NEURODEGENERATION, *MEDICAL model, *PRIONS

Abstract

Prion disease is a fatal and infectious neurodegenerative disorder caused by the trans-conformation conversion of PRNP/PrPC to PRNP/PrPSc. Accumulated PRNP/PrPSc-induced ER stress causes chronic unfolded protein response (UPR) activation, which is one of the fundamental steps in prion disease progression. However, the role of various ER-resident proteins in prion-induced ER stress is elusive. This study demonstrated that ARL6IP5 is compensatory upregulated in response to chronically activated UPR in the cellular prion disease model (RML-ScN2a). Furthermore, overexpression of ARL6IP5 overcomes ER stress by lowering the expression of chronically activated UPR pathway proteins. We discovered that ARL6IP5 induces reticulophagy to reduce the PRNP/PrPSc burden by releasing ER stress. Conversely, the knockdown of ARL6IP5 leads to inefficient macroautophagic/autophagic flux and elevated PRNP/PrPSc burden. Our study also uncovered that ARL6IP5-induced reticulophagy depends on Ca2+-mediated AMPK activation and can induce 3 MA-inhibited autophagic flux. The detailed mechanistic study revealed that ARL6IP5-induced reticulophagy involves interaction with soluble reticulophagy receptor CALCOCO1 and lysosomal marker LAMP1, leading to degradation in lysosomes. Here, we delineate the role of ARL6IP5 as a novel ER stress regulator and reticulophagy inducer that can effectively reduce the misfolded PRNP/PrPSc burden. Our research opens up a new avenue of selective autophagy in prion disease and represents a potential therapeutic target.Abbreviations: ARL6IP5: ADP ribosylation factor-like GTPase 6 interacting protein 5; AMPK: adenosine 5’-monophosphate (AMP)-activated protein kinase; CALCOCO1: calcium binding and coiled-coil domain 1; CQ: chloroquine; DAPI: 4’6-diamino-2-phenylindole; ER: endoplasmic reticulum; ERPHS: reticulophagy/ER-phagy sites; KD: knockdown; KD-CON: knockdown control; LAMP1: lysosomal-associated membrane protein 1; MAP1LC3/LC3, microtubule-associated protein 1 light chain 3; MTOR: mechanistic target of rapamycin kinase; MβCD: methyl beta cyclodextrin; 3 MA: 3-methyladenine; OE: overexpression; OE-CON: empty vector control; PrDs: prion diseases; PRNP/PrPC: cellular prion protein (Kanno blood group); PRNP/PrPSc: infectious scrapie misfolded PRNP; Tm: tunicamycin; UPR: unfolded protein response; UPS: ubiquitin-proteasome system. [ABSTRACT FROM AUTHOR]

Published

2024

213. Cloning and Expression Analysis of ATG8 (Autophagy-Related 8) Gene Family in Solanaceae.

Author

Chen, Yahan, Lu, Yunshuang, Dong, Shibo, Yang, Chengde, and Yang, Shunyi

Subjects

GENE families, GENE expression, DISEASE resistance of plants, PROTEIN structure, MOLECULAR cloning

Abstract

The autophagy-related gene family ATG8 (Autophagy-related 8) plays an important role in plant growth, development, and stress response. In this study, 15 ATG8 gene family sequences were amplified from Solanaceae, namely tobacco, tomato, and pepper, using RT-PCR to evaluate their basic properties, protein structure, and function, as well as the role of ATG8 in autophagy. The physicochemical properties, the predicted secondary and tertiary protein structures, subcellular localisation, gene structures, conserved motifs, and phylogenetic relationships of the ATG8 genes were analysed using bioinformatic techniques, and their expression patterns under sericin-induced plant disease resistance were investigated by RT-qPCR. The lengths of these proteins ranged from 79 to 120 aa, while their predicted molecular weights and isoelectric points (PI) ranged from 9283.62 to 13,778.74 and 6.32 to 11.44, respectively. The majority of the proteins were localised in the nucleus or chloroplasts. Conserved protein motifs and various cis-regulatory elements in the protein, with a wide range of related functions, were identified. The ATG8 gene family members showed expression changes after treatment with osthole, which induces disease resistance in tobacco, tomato, and pepper. These findings provide a foundation for further analyses of the ATG8 gene family in Solanaceae and the mechanism underlying the response to adverse conditions. [ABSTRACT FROM AUTHOR]

Published

2024

214. CheekAge, a next-generation epigenetic buccal clock, is predictive of mortality in human blood.

Author

Shokhirev, Maxim N., Kramer, Daniel J., Corley, Janie, Cox, Simon R., Cuellar, Trinna L., and Johnson, Adiv A.

Subjects

LIFESTYLES, DEATH, PREDICTION models, RESEARCH funding, AUTOPHAGY, EPIGENOMICS, DESCRIPTIVE statistics, DNA methylation, LONGITUDINAL method, GENE expression profiling, AGING, SKELETAL maturity, BIOMARKERS

Abstract

While earlier first-generation epigenetic aging clocks were trained to estimate chronological age as accurately as possible, more recent next-generation clocks incorporate DNA methylation information more pertinent to health, lifestyle, and/or outcomes. Recently, we produced a non-invasive next-generation epigenetic clock trained using Infinium MethylationEPIC data from more than 8,000 diverse adult buccal samples. While this clock correlated with various health, lifestyle, and disease factors, we did not assess its ability to capture mortality. To address this gap, we applied CheekAge to the longitudinal Lothian Birth Cohorts of 1921 and 1936. Despite missing nearly half of its CpG inputs, CheekAge was significantly associated with mortality in this longitudinal blood dataset. Specifically, a change in one standard deviation corresponded to a hazard ratio (HR) of 1.21 (FDR q = 1.66e-6). CheekAge performed better than all first-generation clocks tested and displayed a comparable HR to the next-generation, blood-trained DNAm PhenoAge clock (HR = 1.23, q = 2.45e-9). To better understand the relative importance of each CheekAge input in blood, we iteratively removed each clock CpG and re-calculated the overall mortality association. The most significant effect came from omitting the CpG cg14386193, which is annotated to the gene ALPK2. Excluding this DNA methylation site increased the FDR value by nearly threefold (to 4.92e-06). We additionally performed enrichment analyses of the top annotated CpGs that impact mortality to better understand their associated biology. Taken together, we provide important validation for CheekAge and highlight novel CpGs that underlie a newly identified mortality association. [ABSTRACT FROM AUTHOR]

Published

2024

215. Dietary Probiotic Pediococcus acidilactici GKA4, Dead Probiotic GKA4, and Postbiotic GKA4 Improves Cisplatin-Induced AKI by Autophagy and Endoplasmic Reticulum Stress and Organic Ion Transporters.

Author

Lin, Jaung-Geng, Jiang, Wen-Ping, Tsai, You-Shan, Lin, Shih-Wei, Chen, Yen-Lien, Chen, Chin-Chu, and Huang, Guan-Jhong

Abstract

Background/Objectives: Acute kidney injury (AKI) syndrome is distinguished by a quick decline in renal excretory capacity and usually diagnosed by the presence of elevated nitrogen metabolism end products and/or diminished urine output. AKI frequently occurs in hospital patients, and there are no existing specific treatments available to diminish its occurrence or expedite recovery. For an extended period in the food industry, Pediococcus acidilactici has been distinguished by its robust bacteriocin production, effectively inhibiting pathogen growth during fermentation and storage. Methods: In this study, the aim is to assess the effectiveness of P. acidilactici GKA4, dead probiotic GKA4, and postbiotic GKA4 against cisplatin-induced AKI in an animal model. The experimental protocol involves a ten-day oral administration of GKA4, dead probiotic GKA4, and postbiotic GKA4 to mice, with a cisplatin intraperitoneal injection being given on the seventh day to induce AKI. Results: The findings indicated the significant alleviation of the renal histopathological changes and serum biomarkers of GKA4, dead probiotic GKA4, and postbiotic GKA4 in cisplatin-induced nephrotoxicity. GKA4, dead probiotic GKA4, and postbiotic GKA4 elevated the expression levels of HO-1 and decreased the expression levels of Nrf-2 proteins. In addition, the administration of GKA4, dead probiotic GKA4, and postbiotic GKA4 significantly reduced the expression of apoptosis-related proteins (Bax, Bcl-2, and caspase 3), autophagy-related proteins (LC3B, p62, and Beclin1), and endoplasmic reticulum (ER) stress-related proteins (GRP78, PERK, ATF-6, IRE1, CHOP, and Caspase 12) in kidney tissues. Notably, GKA4, dead probiotic GKA4, and postbiotic GKA4 also upregulated the levels of proteins related to organic anion transporters and organic cation transporters. Conclusions: Overall, the potential therapeutic benefits of GKA4, dead probiotic GKA4, and postbiotic GKA4 are significant, particularly after cisplatin treatment. This is achieved by modulating apoptosis, autophagy, ER stress, and transporter proteins to alleviate oxidative stress. [ABSTRACT FROM AUTHOR]

Published

2024

216. Effect of natural products on host cell autophagy induced by Influenza A virus infection.

Author

Xiaopan Liu and Qingsen Wang

Subjects

VIRUS diseases, INFLUENZA A virus, PLANT extracts, NATURAL products, INFLUENZA viruses

Abstract

Influenza A virus (IAV) can cause seasonal epidemics and global pandemics, posing serious threats to public health, making a deeper understanding of its biological characteristics and effective countermeasure strategies essential. Autophagy not only maintains cellular homeostasis but also plays an important role in host defense against IAV infection. However, the relationship between IAV and autophagy is complex, and effective antiviral drugs are not yet available. Natural products have shown excellent potential in disease control due to their diversity and multi-targeting. This review focuses on the relationship between IAV and autophagy and discusses the potential of targeting autophagic pathways for the development of new antiviral therapies. Particularly, the use of plant extracts as autophagy modulators has garnered attention due to their non-toxic nature and cost-effectiveness, which provides strong support for the development of future antiviral drugs that can help to inhibit viral infections and slow down disease progression. [ABSTRACT FROM AUTHOR]

Published

2024

217. Autophagy is a promising process for linking inflammation and redox homeostasis in Down syndrome.

Author

Xuehai Ma, Weimin Li, Jun Ma, Zhongcheng Han, Shoulong Deng, and Sutian Wang

Subjects

OXIDATIVE stress, DOWN syndrome, NUCLEOLUS, CELLULAR signal transduction, AUTOPHAGY, HOMEOSTASIS

Abstract

Trisomy 21, characterized by the presence of an additional chromosome 21, leads to a set of clinical features commonly referred to as Down syndrome (DS). The pathological phenotypes observed in DS are caused by a combination of factors, such as mitochondrial dysfunction, neuroinflammation, oxidative stress, disrupted metabolic patterns, and changes in protein homeostasis and signal transduction, and these factors collectively induce neurological alterations. In DS, the triplication of chromosome 21 and the micronuclei arising from the missegregation of chromosomes are closely associated with inflammation and the development of redox imbalance. Autophagy, an essential biological process that affects cellular homeostasis, is a powerful tool to facilitate the degradation of redundant or dysfunctional cytoplasmic components, thereby enabling the recycling of their constituents. Targeting the autophagy process has been suggested as a promising method to balance intracellular inflammation and oxidative stress and improve mitochondrial dysfunction. In this review, we summarize the role of autophagy in regulating inflammation and redox homeostasis in DS and discuss their crosslinks. A comprehensive elucidation of the roles of autophagy in DS offers novel insights for the development of therapeutic strategies aimed at aneuploidy-associated diseases. [ABSTRACT FROM AUTHOR]

Published

2024

218. Apoptosis, autophagy, ferroptosis, and pyroptosis in cisplatin-induced ototoxicity and protective agents.

Author

Dingyuan Dai, Chao Chen, Chen Lu, Yu Guo, Qi Li, and Chen Sun

Subjects

CELL death, PYROPTOSIS, OTOTOXICITY, HEARING disorders, CISPLATIN, INNER ear

Abstract

Cisplatin is widely used to treat various solid tumors. However, its toxicity to normal tissues limits its clinical application, particularly due to its ototoxic effects, which can result in hearing loss in patients undergoing chemotherapy. While significant progress has been made in preclinical studies to elucidate the cellular and molecular mechanisms underlying cisplatin-induced ototoxicity (CIO), the precise mechanisms remain unclear. Moreover, the optimal protective agent for preventing or mitigating cisplatin-induced ototoxicity has yet to be identified. This review summarizes the current understanding of the roles of apoptosis, autophagy, ferroptosis, pyroptosis, and protective agents in cisplatin-induced ototoxicity. A deeper understanding of these cell death mechanisms in the inner ear, along with the protective agents, could facilitate the translation of these agents into clinical therapeutics, help identify new therapeutic targets, and provide novel strategies for cisplatin-based cancer treatment. [ABSTRACT FROM AUTHOR]

Published

2024

219. The role of SIRT1 in autophagy and drug resistance: unveiling new targets and potential biomarkers in cancer therapy.

Author

Yujing Tang, Wantao Ju, Yanjun Liu, and Qin Deng

Subjects

CELL anatomy, SIRTUINS, AMP-activated protein kinases, PROTEIN kinases, TUMOR markers

Abstract

Cancer, the world’s second leading cause of death after cardiovascular diseases, is characterized by hallmarks such as uncontrolled cell growth, metastasis, angiogenesis, hypoxia, and resistance to therapy. Autophagy, a cellular process that can both support and inhibit cancer progression, plays a critical role in cancer development and progression. This process involves the formation of autophagosomes that ultimately fuse with lysosomes to degrade cellular components. A key regulator of this process is Sirtuin 1 (SIRT1), which significantly influences autophagy. This review delves into the role of SIRT1 in modulating autophagy and its broader impacts on carcinogenesis. SIRT1 regulates crucial autophagy mediators, such as AMP-activated protein kinase (AMPK) and mammalian target of rapamycin (mTOR), effectively promoting or suppressing autophagy. Beyond its direct effects on autophagy, SIRT1’s regulatory actions extend to other cell death processes, including apoptosis and ferroptosis, thereby influencing tumor cell proliferation, metastasis, and chemotherapy responses. These insights underscore the complex interplay between SIRT1 and autophagy, with significant implications for cancer therapy. Targeting SIRT1 and its associated pathways presents a promising strategy to manipulate autophagy in cancer treatment. This review underscores the potential of SIRT1 as a therapeutic target, opening new avenues for enhancing cancer treatment efficacy. [ABSTRACT FROM AUTHOR]

Published

2024

220. The role of autophagy in pancreatic diseases.

Author

Wen-Gang Zhang, Qing-Zhen Wu, and Bo-Zong Shao

Subjects

PANCREATIC diseases, PANCREATIC cancer, AUTOPHAGY, PANCREATITIS, DEATH rate

Abstract

Pancreatic diseases such as pancreatitis and pancreatic cancer represent significant health challenges characterized by high mortality rates and limited survival durations. Autophagy, a crucial cellular catabolic process, has emerged as a focal point in understanding various pathological conditions, spanning inflammation-related disorders to malignant neoplasms. This comprehensive review aims to elucidate the biological intricacies of autophagy and its pivotal roles within two extensively researched pancreatic diseases, namely pancreatitis and pancreatic cancer, drawing upon recent scholarly contributions. The discussion will delve into the nuanced mechanisms underlying autophagy’s involvement in these diseases, shedding light on its potential as a therapeutic target. Furthermore, the review will explore cutting-edge therapeutic interventions leveraging autophagy regulation for managing pancreatitis and pancreatic cancer. Through this analysis, we endeavor to offer novel insights into the pathophysiology of pancreatic disorders and contribute to the development of innovative therapeutic modalities in this challenging clinical domain. [ABSTRACT FROM AUTHOR]

Published

2024

221. Anti-inflammatory compounds from the rhizome of Acorus calamus var. angustatus Besser and their mechanism.

Author

Huang, Liping, Feng, Zhenying, Xiang, Jie, Deng, Minzhen, and Zhou, Zhongliu

Subjects

LIPOPOLYSACCHARIDES, ANTI-inflammatory agents, AUTOPHAGY, MEDICINAL plants, INTERLEUKIN-6

Abstract

Seven compounds, named β-sitosterol (1), daucosterol (2), (+)-pinoresinol-β-D-glucoside (3), (−)-syringaresinol 4-O-β-D-apiofuranosyl-(1→2)- β-D-glucopyranoside (4), 4-hydroxybenzoic acid (5), 2-(3', 4'-dihydroxyphenyl)-1, 3-pepper ring-5-aldehyde (6) and spinosin (7) were isolated from the rhizome of Acorus calamus var. angustatus Besser. 3, 4, 6 and 7 were isolated from this medicinal plant for the first time. Structures were elucidated by physicochemical properties and extensive spectroscopic analysis, as well as by comparison with literature data. The anti-inflammatory activity and related mechanisms of the seven compounds showed that compounds 1–7 all increased the levels of GSH-PX and SOD and decreased the levels of MDA, TNF-α, IL-1β and IL-6. Compound 4 showed the best effect of anti-inflammatory and Beclin-1 inhibition. These results suggest that compound 4 has stronger anti-inflammatory effect and provide preliminary evidence that the mechanism of action of compound 4 in attenuating LPS-induced inflammatory damage may be related to the inhibition of Beclin-1-dependent autophagy. [ABSTRACT FROM AUTHOR]

Published

2024

222. Protective Effects of Nettle Tea on SKOV-3 Ovarian Cancer Cells Through ROS Production, Apoptosis Induction, and Motility Inhibition Without Altering Autophagy.

Author

Abi Akl, Maria, Hajj, Roy, Jamati, Georgio, Karam, Louna, Ibrahim, José-Noel, Kobeissy, Philippe H., Younes, Maria, and Rizk, Sandra

Subjects

CANCER cell motility, CELL cycle, STINGING nettle, WESTERN immunoblotting, CELL analysis, CELL death

Abstract

Urtica dioica L. (UD), also known as the stinging nettle, has long been used in traditional medicine for its wide range of health benefits. The current study focuses on the effect of nettle tea on the growth and proliferation of one of the most aggressive ovarian adenocarcinoma cell line, SKOV-3 cells. To examine this, cytotoxicity, cell cycle analysis, and ROS assays were performed, along with Annexin V/PI dual staining, cell death ELISA, Western blot analysis, and motility assays. The results showed that a UD aqueous extract (UDAE) can inhibit the growth and proliferation of SKOV-3 cells in a dose- and time-dependent manner by promoting cellular fragmentation. This was accompanied by an increase in two apoptotic hallmarks, the flipping of phosphatidylserine to the outer membrane leaflet and DNA fragmentation as revealed by cell death ELISA. This aqueous extract showed a pro-oxidant activity while also activating the extrinsic caspase-dependent apoptotic pathway with no alteration in autophagy markers. Furthermore, the extract showed promising inhibitory effect on the migratory capacities of aggressive ovarian cancer cells, in vitro. [ABSTRACT FROM AUTHOR]

Published

2024

223. Artesunate-driven autophagy: a shield against liver hypoxia/reoxygenation insult in rats via modulation of GLP1R, the chief metabolic kinase AMPK, mTOR, ULK1, P70S6K, cyclin D1, Akt, and GSK3β.

Author

Ghoneim, Mai El-Sayed, El-Abhar, Hanan S., and Abdallah, Dalaal M.

Subjects

*LIVER transplantation, *AMP-activated protein kinases, *PROTEIN expression, *AUTOPHAGY, *WESTERN immunoblotting

Abstract

Background: Hepatic hypoxia/reoxygenation (H/R) insult is a critical issue in hepatic transplant and surgeries, profoundly influencing postoperative prognosis. One crucial pathomechanism in this condition is impaired autophagy flux, which disrupts liver homeostasis. Artesunate, an antimalarial drug, has shown potential in providing hepatoprotection against H/R injury; however, whether it can modulate disrupted autophagy to enhance hepatoprotection remains unclear. Purpose of the study: Accordingly, we delved into the potential mechanism(s) through which artesunate modulates the autophagy process in a hepatic H/R injury model. Methods and results: Rats were categorized into three groups, viz. sham operated, H/R, and artesunate-treated (50 mg/kg, i.p). Disease regression was evaluated microscopically, and molecular alternations were assessed biochemically using ELISA and western blotting techniques. Mechanistic analysis revealed that artesunate administration at reperfusion time significantly upregulated the gene expression of GLP1R protein expression of p-AMPK, accompanied by a downregulation in those of p-mTOR, and its target molecule p-ULK1, presenting the first trail to initiate autophagy. Additionally, artesunate reduced H/R-induced hepatic upregulated protein expression of p-mTOR/P70S6K cue, and cyclin D1 content, which positively correlated with the mTOR/P70S6K axis. Moreover, artesunate sharply upregulated active p-Akt, which in turn phosphorylated/inactivated GSK3β, a cascade that indirectly promotes autophagy. Consequently, artesunate increased the hepatic beclin-1 and LC3-II to further uphold its autophagic capacity. The hepato-therapeutic effectiveness of artesunate was further evidenced by reduced serum ALT and AST levels, along with diminished hepatic histopathological alterations. Conclusion: Artesunate protected liver by triggering autophagy partly by modulating the GLP1R/AMPK/mTOR/ULK1, GLP1R/AMPK/mTOR/P70S6K, cyclin D1, and Akt/GSK3β trajectories providing a significant therapeutic potential in managing hepatic H/R insult. [ABSTRACT FROM AUTHOR]

Published

2024

224. Quinoa ameliorates polycystic ovary syndrome via regulating gut microbiota through PI3K/AKT/mTOR pathway and autophagy.

Author

Dou, Jinfang, Wu, Yanxiang, Hu, Rentong, Liu, Jiaxian, Zhang, Yuelin, Zhen, Xianjie, Wu, Tao, Zhang, Chuyue, Liu, Yutong, Zheng, Ruifang, and Jiang, Guangjian

Subjects

*PHYTOTHERAPY, *SEX hormones, *COMPUTER-assisted molecular modeling, *PROTEINS, *AUTOPHAGY, *DATA analysis, *BACTEROIDES, *RESEARCH funding, *GUT microbiome, *UNSATURATED fatty acids, *PHARMACEUTICAL chemistry, *POLYCYSTIC ovary syndrome, *CELLULAR signal transduction, *DESCRIPTIVE statistics, *RATS, *PANCREAS, *DUODENUM, *COLON (Anatomy), *IMMUNOHISTOCHEMISTRY, *MEDICINAL plants, *ANIMAL experimentation, *PAP test, *WESTERN immunoblotting, *STATISTICS, *HUMAN reproduction, *LACTOBACILLUS, *TRANSFERASES, *LETROZOLE, *GRAM-negative anaerobic bacteria, *DATA analysis software, *OVARIES

Abstract

Background: Polycystic ovary syndrome (PCOS) is a unity of endocrine and metabolic disorders, associated with PI3K/AKT/mTOR, autophagy, and gut microbiota. Quinoa is a valuable food source, which contains rich minerals, unsaturated fatty acids, and has a positive modulating effect on metabolic diseases. However, its effects and potential mechanisms on PCOS have not been reported yet. Therefore, the purpose of this study is to investigate the effect of quinoa on PCOS rats by regulating PI3K/AKT/mTOR, autophagy, and gut microbiota. Methods: Ten–week-old female Sprague-Dawley (SD) rats have received letrozole for 24 days for induction of PCOS and subsequently were treated with a quinoa diet for 8 weeks. Vaginal smears were used to analyze the estrous cycle of rats. Hormone and biochemical indexes were analyzed by kit assays and glucometer. The pathological changes of ovary, pancreas, duodenum and colon were observed by HE staining. PI3K, AKT, mTOR and autophagy-related proteins in the ovary and colon were measured by western blot and immunohistochemistry staining. Tight junction proteins in colon were measured by immunohistochemistry staining. 16 s rDNA sequencing was used to detect the changes of intestinal microbiota in rats. Network pharmacology and molecular docking were used to study the possible targets and mechanisms of quinoa on PCOS. Spearman correlation analysis was used to study the relationship between intestinal microbial abundance and hormone levels of PCOS rats at the phylum and genus level. Results: Quinoa significantly improved estrous cycle and biochemical parameters of PCOS-like rats, and the pathological state of ovary, pancreas, duodenum and colon tissues. Especially, quinoa significantly regulated the expression of PI3K, AKT, mTOR and autophagy-related proteins in the ovary. Quinoa may repair the intestinal barrier by upregulating the expression of tight junction proteins in the colon, and regulate autophagy-related factors in colon. Additionally, quinoa increased the abundance of Lactobacillu, Bacteroides and Oscillospira, and decreased the Firmicutes/Bacteroidetes ratio and the Blautia, and Prevotella, reversing the dysregulation of the gut microbiota. Correlation analysis showed that there is a strong correlation between gut microbiota with significant changes in abundance and hormone related to PCOS. Conclusion: Our result indicated that effect of quinoa on PCOS maybe associated with activation of the PI3K/AKT/mTOR signaling pathway, inhibition of autophagy, and regulation of intestinal flora. [ABSTRACT FROM AUTHOR]

Published

2024

225. Cancer cell-selective induction of mitochondrial stress and immunogenic cell death by PT-112 in human prostate cell lines.

Author

Soler-Agesta, R., Moreno-Loshuertos, R., Yim, C. Y., Congenie, M. T., Ames, T. D., Johnson, H. L., Stossi, F., Mancini, M. G., Mancini, M. A., Ripollés-Yuba, C., Marco-Brualla, J., Junquera, C., Martínez-De-Mena, R., Enríquez, J. A., Price, M. R., Jimeno, J., and Anel, A.

Subjects

*ORGANELLE formation, *CASTRATION-resistant prostate cancer, *PROSTATE cancer, *CANCER cells, *CELL death, *CELL lines

Abstract

PT-112 is a novel immunogenic cell death (ICD)-inducing small molecule currently under Phase 2 clinical development, including in metastatic castration-resistant prostate cancer (mCRPC), an immunologically cold and heterogeneous disease state in need of novel therapeutic approaches. PT-112 has been shown to cause ribosome biogenesis inhibition and organelle stress followed by ICD in cancer cells, culminating in anticancer immunity. In addition, clinical evidence of PT-112-driven immune effects has been observed in patient immunoprofiling. Given the unmet need for immune-based therapies in prostate cancer, along with a Phase I study (NCT#02266745) showing PT-112 activity in mCRPC patients, we investigated PT-112 effects in a panel of human prostate cancer cell lines. PT-112 demonstrated cancer cell selectivity, inhibiting cell growth and leading to cell death in prostate cancer cells without affecting the non-tumorigenic epithelial prostate cell line RWPE-1 at the concentrations tested. PT-112 also caused caspase-3 activation, as well as stress features in mitochondria including ROS generation, compromised membrane integrity, altered respiration, and morphological changes. Moreover, PT-112 induced damage-associated molecular pattern (DAMP) release, the first demonstration of ICD in human cancer cell lines, in addition to autophagy initiation across the panel. Taken together, PT-112 caused selective stress, growth inhibition and death in human prostate cancer cell lines. Our data provide additional insight into mitochondrial stress and ICD in response to PT-112. PT-112 anticancer immunogenicity could have clinical applications and is currently under investigation in a Phase 2 mCRPC study. [ABSTRACT FROM AUTHOR]

Published

2024

226. Reticulophagy and viral infection.

Author

Wilson, Alexa and McCormick, Craig

Subjects

*UNFOLDED protein response, *PATTERN perception receptors, *MEMBRANE proteins, *ENDOPLASMIC reticulum, *VIRAL proteins

Abstract

All viruses are obligate intracellular parasites that use host machinery to synthesize viral proteins. In infected eukaryotes, viral secreted and transmembrane proteins are synthesized at the endoplasmic reticulum (ER). Many viruses refashion ER membranes into bespoke factories where viral products accumulate while evading host pattern recognition receptors. ER processes are tightly regulated to maintain cellular homeostasis, so viruses must either conform to ER regulatory mechanisms or subvert them to ensure efficient viral replication. Reticulophagy is a catabolic process that directs lysosomal degradation of ER components. There is accumulating evidence that reticulophagy serves as a form of antiviral defense; we call this defense “xERophagy” to acknowledge its relationship to xenophagy, the catabolic degradation of microorganisms by macroautophagy/autophagy. In turn, viruses can subvert reticulophagy to suppress host antiviral responses and support efficient viral replication. Here, we review the evidence for functional interplay between viruses and the host reticulophagy machinery.Abbreviations: AMFR: autocrine motility factor receptor; ARF4: ADP-ribosylation factor 4; ARL6IP1: ADP-ribosylation factor-like 6 interacting protein 1; ATL3: atlastin GTPase 3; ATF4: activating transcription factor 4; ATF6: activating transcription factor 6; BPIFB3: BPI fold containing family B, member 3; CALCOCO1: calcium binding and coiled coil domain 1; CAMK2B: calcium/calmodulin-dependent protein kinase II, beta; CANX: calnexin; CDV: canine distemper virus; CCPG1: cell cycle progression 1; CDK5RAP3/C53: CDK5 regulatory subunit associated protein 3; CIR: cargo-interacting region; CoV: coronavirus; CSNK2/CK2: casein kinase 2; CVB3: coxsackievirus B3; DAPK1: death associated protein kinase 1; DENV: dengue virus; DMV: double-membrane vesicles; EBOV: Ebola virus; EBV: Epstein-Barr Virus; EIF2AK3/PERK: eukaryotic translation initiation factor 2 alpha kinase 3; EMCV: encephalomyocarditis virus; EMV: extracellular microvesicle; ER: endoplasmic reticulum; ERAD: ER-associated degradation; ERN1/IRE1: endoplasmic reticulum to nucleus signalling 1; EV: extracellular vesicle; EV71: enterovirus 71; FIR: RB1CC1/FIP200-interacting region; FMDV: foot-and-mouth disease virus; HCMV: human cytomegalovirus; HCV: hepatitis C virus; HMGB1: high mobility group box 1; HSPA5/BiP: heat shock protein 5; IFN: interferon; IFNG/IFN-γ: interferon gamma; KSHV: Kaposi’s sarcoma-associated herpesvirus; LIR: MAP1LC3/LC3-interacting region; LNP: lunapark, ER junction formation factor; MAP1LC3: microtubule-associated protein 1 light chain 3; MAP3K5/ASK1: mitogen-activated protein kinase kinase kinase 5; MAPK/JNK: mitogen-activated protein kinase; MeV: measles virus; MHV: murine hepatitis virus; NS: non-structural; PDIA3: protein disulfide isomerase associated 3; PRR: pattern recognition receptor; PRRSV: porcine reproductive and respiratory syndrome virus; RB1CC1/FIP200: RB1-inducible coiled-coil 1; RETREG1/FAM134B: reticulophagy regulator 1; RHD: reticulon homology domain; RTN3: reticulon 3; RTN3L: reticulon 3 long; sAIMs: shuffled Atg8-interacting motifs; SARS-CoV: severe acute respiratory syndrome coronavirus; SINV: Sindbis virus; STING1: stimulator of interferon response cGAMP interactor 1; SVV: Seneca Valley virus; SV40: simian virus 40; TEX264: testis expressed gene 264 ER-phagy receptor; TFEB: transcription factor EB; TRAF2: TNF receptor-associated factor 2; UIM: ubiquitin-interacting motif; UFM1: ubiquitin-fold modifier 1; UPR: unfolded protein response; VAPA: vesicle-associated membrane protein, associated protein A; VAPB: vesicle-associated membrane protein, associated protein B and C; VZV: varicella zoster virus; WNV: West Nile virus; XBP1: X-box binding protein 1; XBP1s: XBP1 spliced; xERophagy: xenophagy involving reticulophagy; ZIKV: Zika virus [ABSTRACT FROM AUTHOR]

Published

2024

227. Asiatic acid impedes NSCLC progression by inhibiting COX‐2 and modulating PI3K signaling.

Author

Singh, Jyoti, Hussain, Yusuf, Meena, Abha, Sinha, Rohit Anthony, and Luqman, Suaib

Subjects

*PROTEIN kinase B, *VASCULAR endothelial growth factors, *CANCER cell growth, *PROTEIN kinases, *CANCER cell proliferation

Abstract

Non‐small cell lung cancer comprises up to 85% of lung cancer cases and has a poor prognosis. At present, there are still no effective treatments for this illness. Evidence suggests that the prostaglandin [cyclooxygenase‐2 (COX‐2)] and leukotriene [lipoxygenase‐5 (5‐LOX)] pathways are involved in lung cancer carcinogenesis. Therefore, novel agents that target COX‐2 and 5‐LOX may have therapeutic potential. In the present study, we examined the role of asiatic acid (AA), a triterpenoid saponin, in targeting the protein kinases responsible for lung cancer proliferation and mobility. The experimental data revealed that AA inhibited the growth of lung cancer cells (> 50%) and it significantly impeded the proliferation of lung cancer cells by inhibiting COX‐2, which results in downregulation of the phosphotidyl inositol‐3 kinase/protein kinase B/mammalian target of rapamycin signaling pathway, leading to an induction of cytotoxic autophagy‐mediated apoptosis. Mechanistically, the expression of mitogen‐activated protein kinase/extracellular signal‐regulated kinase, hypoxia‐inducible factor‐1 and vascular endothelial growth factor is downregulated by AA, thereby reducing cell mobility and invasion. It also shows negative osmotic fragility on healthy human erythrocytes. It is concluded that AA may be a viable therapeutic drug for non‐small cell lung cancer treatment, which opens new opportunities for synthesizing analogues. [ABSTRACT FROM AUTHOR]

Published

2024

228. Regression of postprandial cardiac hypertrophy in burmese pythons is mediated by FoxO1.

Author

Martin, Thomas G., Hunt, Dakota R., Langer, Stephen J., Yuxiao Tan, Ebmeier, Christopher C., and Leinwand, Leslie A.

Subjects

*FORKHEAD transcription factors, *CARDIAC hypertrophy, *VENTRICULAR remodeling, *CELL size, *GROWTH factors

Abstract

As ambush-hunting predators that consume large prey after long intervals of fasting, Burmese pythons evolved with unique adaptations for modulating organ structure and function. Among these is cardiac hypertrophy that develops within three days following a meal (Andersen et al., 2005, Secor, 2008), which we previously showed was initiated by circulating growth factors (Riquelme et al., 2011). Postprandial cardiac hypertrophy in pythons also rapidly regresses with subsequent fasting (Secor, 2008); however, the molecular mechanisms that regulate the dynamic cardiac remodeling in pythons during digestion are largely unknown. In this study, we employed a multiomics approach coupled with targeted molecular analyses to examine remodeling of the python ventricular transcriptome and proteome throughout digestion. We found that forkhead box protein O1 (FoxO1) signaling was suppressed prior to hypertrophy development and then activated during regression, which coincided with decreased and then increased expression, respectively, of FoxO1 transcriptional targets involved in proteolysis. To define the molecular mechanistic role of FoxO1 in hypertrophy regression, we used cultured mammalian cardiomyocytes treated with postfed python plasma. Hypertrophy regression both in pythons and in vitro coincided with activation of FoxO1-dependent autophagy; however, the introduction of a FoxO1-specific inhibitor prevented both regression of cell size and autophagy activation. Finally, to determine whether FoxO1 activation could induce regression, we generated an adenovirus expressing a constitutively active FoxO1. FoxO1 activation was sufficient to prevent and reverse postfed plasma-induced hypertrophy, which was partially prevented by autophagy inhibition. Our results indicate that modulation of FoxO1 activity contributes to the dynamic ventricular remodeling in postprandial Burmese pythons. [ABSTRACT FROM AUTHOR]

Published

2024

229. Puerarin: a hepatoprotective drug from bench to bedside.

Author

He, Yi-Xiang, Liu, Meng-Nan, Wu, Hao, Lan, Qi, Liu, Hao, Mazhar, Maryam, Xue, Jin-Yi, Zhou, Xin, Chen, Hui, and Li, Zhi

Subjects

*THERAPEUTIC use of isoflavones, *CHINESE medicine, *METABOLIC disorders, *AUTOPHAGY, *HERBAL medicine, *APOPTOSIS, *ALCOHOLIC liver diseases, *OXIDATIVE stress, *DRUG delivery systems, *LIVER diseases, *PHARMACY information services, *MEDICINAL plants, *INFLAMMATION, *BIOAVAILABILITY

Abstract

Pueraria is a time-honored food and medicinal plant, which is widely used in China. Puerarin, the main component extracted from pueraria, has a variety of pharmacological characteristics. In recent years, puerarin has received increasing attention for its significant hepatoprotective effects, such as metabolic dysfunction-associated steatotic liver disease, alcohol-related liver disease, and hepatic carcinoma. This paper explores the pharmacological effects of puerarin on various liver diseases through multiple mechanisms, including inflammation factors, oxidative stress, lipid metabolism, apoptosis, and autophagy. Due to its restricted solubility, pharmacokinetic studies revealed that puerarin has a low bioavailability. However, combining puerarin with novel drug delivery systems can improve its bioavailability. Meanwhile, puerarin has very low toxicity and high safety, providing a solid foundation for its further. In addition, this paper discusses puerarin's clinical trials, highlighting its unique advantages. Given its excellent pharmacological effects, puerarin is expected to be a potential drug for the treatment of various liver diseases. [ABSTRACT FROM AUTHOR]

Published

2024

230. Nanomaterial-mediated host directed therapy of tuberculosis by manipulating macrophage autophagy.

Author

Liu, Yilin, Wang, Jiajun, Yang, Jiayi, Xia, Jiaojiao, Yu, Jiaqi, Chen, Dongsheng, Huang, Yuhe, Yang, Fen, Ruan, Yongdui, Xu, Jun-Fa, and Pi, Jiang

Subjects

*MYCOBACTERIUM tuberculosis, *EUKARYOTIC cells, *BACTERIAL diseases, *ANTIMICROBIAL peptides, *PUBLIC health

Abstract

Tuberculosis (TB), induced by Mycobacterium tuberculosis (Mtb) infection, remains a major public health issue worldwide. Mtb has developed complicated strategies to inhibit the immunological clearance of host cells, which significantly promote TB epidemic and weaken the anti-TB treatments. Host-directed therapy (HDT) is a novel approach in the field of anti-infection for overcoming antimicrobial resistance by enhancing the antimicrobial activities of phagocytes through phagosomal maturation, autophagy and antimicrobial peptides. Autophagy, a highly conserved cellular event within eukaryotic cells that is effective against a variety of bacterial infections, has been shown to play a protective role in host defense against Mtb. In recent decades, the introduction of nanomaterials into medical fields open up a new scene for novel therapeutics with enhanced efficiency and safety against different diseases. The active modification of nanomaterials not only allows their attractive targeting effects against the host cells, but also introduce the potential to regulate the host anti-TB immunological mechanisms, such as apoptosis, autophagy or macrophage polarization. In this review, we introduced the mechanisms of host cell autophagy for intracellular Mtb clearance, and how functional nanomaterials regulate autophagy for disease treatment. Moreover, we summarized the recent advances of nanomaterials for autophagy regulations as novel HDT strategies for anti-TB treatment, which may benefit the development of more effective anti-TB treatments. [ABSTRACT FROM AUTHOR]

Published

2024

231. Targeting IGF1/IGF1r signaling relieve pain and autophagic dysfunction in NTG-induced chronic migraine model of mice.

Author

Wang, Tianxiao, Zhu, Chenlu, zhang, Kaibo, Gao, Jinggui, Xu, Yunhao, Duan, Chenyang, Wu, Shouyi, Peng, Cheng, Guan, Jisong, and Wang, Yonggang

Subjects

*BIOLOGICAL models, *AUTOPHAGY, *INTRAPERITONEAL injections, *PHOSPHORYLATION, *T-test (Statistics), *RESEARCH funding, *CELL proliferation, *NEURONS, *POLYMERASE chain reaction, *CELLULAR signal transduction, *NITROGLYCERIN, *ALLERGIES, *CALCITONIN, *FLUORESCENT antibody technique, *MANN Whitney U Test, *DESCRIPTIVE statistics, *GENE expression, *MICE, *MESSENGER RNA, *PAIN, *ANIMAL experimentation, *WESTERN immunoblotting, *SOMATOMEDIN, *DATA analysis software, *MIGRAINE, *ALLODYNIA, *NONPARAMETRIC statistics

Abstract

Background: Chronic migraine is a severe and common neurological disorder, yet its precise physiological mechanisms remain unclear. The IGF1/IGF1r signaling pathway plays a crucial role in pain modulation. Studies have shown that IGF1, by binding to its receptor IGF1r, activates a series of downstream signaling cascades involved in neuronal survival, proliferation, autophagy and functional regulation. The activation of these pathways can influence nociceptive transmission. Furthermore, alterations in IGF1/IGF1r signaling are closely associated with the development of various chronic pain conditions. Therefore, understanding the specific mechanisms by which this pathway contributes to pain is of significant importance for the development of novel pain treatment strategies. In this study, we investigated the role of IGF1/IGF1r and its potential mechanisms in a mouse model of chronic migraine. Methods: Chronic migraine was induced in mice by repeated intraperitoneal injections of nitroglycerin. Mechanical and thermal hypersensitivity responses were assessed using Von Frey filaments and radiant heat, respectively. To determine the role of IGF1/IGF1r in chronic migraine (CM), we examined the effects of the IGF1 receptor antagonist ppp (Picropodophyllin) on pain behaviors and the expression of calcitonin gene-related peptide (CGRP) and c-Fos. Result: In the nitroglycerin-induced chronic migraine model in mice, neuronal secretion of IGF1 is elevated within the trigeminal nucleus caudalis (TNC). Increased phosphorylation of the IGF1 receptor occurs, predominantly co-localizing with neurons. Treatment with ppp alleviated basal mechanical hypersensitivity and acute mechanical allodynia. Furthermore, ppp ameliorated autophagic dysfunction and reduced the expression of CGRP and c-Fos. Conclusion: Our findings demonstrate that in the chronic migraine (CM) model in mice, there is a significant increase in IGF1 expression in the TNC region. This upregulation of IGF1 leads to enhanced phosphorylation of IGF1 receptors on neurons. Targeting and inhibiting this signaling pathway may offer potential preventive strategies for mitigating the progression of chronic migraine. [ABSTRACT FROM AUTHOR]

Published

2024

232. Transcription factor EB (TFEB) promotes autophagy in early brain injury after subarachnoid hemorrhage in rats.

Author

Lu, Wenqi, Chu, Haichao, Yang, Chunchen, and Li, Xiaoxu

Subjects

*TRANSCRIPTION factors, *CEREBRAL edema, *SUBARACHNOID hemorrhage, *HYDROCEPHALUS, *HEMORRHAGIC stroke

Abstract

Subarachnoid hemorrhage (SAH) has high mortality. Early brain injury (EBI) is responsible for unfavorable outcomes for patients with SAH. The protective involvement of autophagy in hemorrhagic stroke has been proposed. The transcription factor EB (TFEB) can increase autophagic flux by promoting autophagosome formation and autophagosome-lysosome fusion, and dysregulation of TFEB activity might induce the development of several diseases. However, the biological functions of TFEB in EBI after SAH remain unknown. We established an animal model of SAH by the modified endovascular perforation method. Expression of TFEB and autophagy required genes was measured by western blotting and immunofluorescence staining. SAH grading, brain water content and neurobehavioral functions were evaluated at 24 h post-SAH. Neuronal apoptosis in cerebral cortex was assessed by TUNEL staining and Fluoro Jade B staining. TFEB was downregulated in SAH rats, and its overexpression reduced brain edema and ameliorated neurological deficits of SAH rats. Additionally, the neuronal apoptosis induced by SAH was inhibited by TFEB overexpression. Moreover, TFEB overexpression promoted autophagy after SAH. TFEB overexpression promotes autophagy to inhibit neuronal apoptosis, brain edema and neurological deficits post-SAH. [ABSTRACT FROM AUTHOR]

Published

2024

233. 二甲双胍预处理诱导心脏自噬减轻脓毒症小鼠的心肌损伤.

Author

田 勇, 周 颖, 古雍翔, and 杨国辉

Abstract

BACKGROUND: Sepsis complicated by myocardial injury is characterized by a high mortality. Metformin can prevent sepsis-induced myocardial dysfunction byexerting anti-inflammatory effects, improving oxidative stress, and reducing apoptosis. However, it is unclear whether metformin-induced autophagy plays an important role in the protective effect against sepsis-induced myocardial injury. OBJECTIVE: To explore the effect of metformin pretreatment on myocardial injury in septic mice. METHODS: A total of 40 male Kunming mice were randomly divided into sham operation group, model group, metformin group, and metformin+ 3-methyladenine group, with 10 mice in each group. The latter two groups were intraperitoneally injected with metformin for 14 days at a fixed time every day, and the metformin+3-methyladenine group was intraperitoneally injected with 3-methyladenine 1 hour before modeling. Twenty-four hours after the last injection of metformin, cecal ligation and perforation were used to construct a model of myocardial injury in septic mice. The sham operation group was not ligated and perforated. All mice were sacrificed 24 hours after surgery, and blood and myocardial specimens were collected. The levels of inflammatory factors and myocardial injury markers in serum were detected by ELISA. The mRNA expression of autophagy markers LC3B and p62 in myocardial tissue was detected by RT-qPCR. The protein expression of LC3B, Beclin-1, p62, p-AMPK, and AMPK in myocardial tissue was detected by western blot. The pathological changes in myocardial tissue were detected by hematoxylin-eosin staining. RESULTS AND CONCLUSION: Autophagy was inhibited in septic mice with myocardial injury. Compared with the sham operation group, the levels of serum tumor necrosis factor-α, interleukin-1β, interleukin-6, creatine kinase isoenzyme, and troponin T were increased in the model group (P < 0.05), but there was no significant difference in p62, LC3II/LC3I, and p-AMPK/AMPK between the two groups (P > 0.05). Compared with the model group, the levels of tumor necrosis factor-α, interleukin-6, creatine kinase isoenzyme, troponin T, and p62 were decreased in the metformin group (P < 0.05), while LC3II/LC3I, p-AMPK/ AMPK and Beclin-1 level were increased (P < 0.05). Compared with the metformin group, the levels of tumor necrosis factor-α, interleukin-6, creatine kinase isoenzyme, troponin T, and p62 were increased in the metformin+3-methyladenine group (P < 0.05), while LC3II/LC3I and Beclin-1 level were decreased (P < 0.05). Myocardial hematoxylin-eosin staining indicated that myocardial fibers arranged normally in the sham operation group, but disorderedly in the model group, with interstitial edema and a large number of infiltrated inflammatory cells. A small amount of vacuolar changes were observed in the metformin group. The arrangement of myocardial fibers in the metformin+3-methyladenine group was slightly disordered, with more vacuolar changes. To conclude, metformin pretreatment may reduce myocardial injury in septic mice by activating the AMPK signaling pathway and inducing autophagy. [ABSTRACT FROM AUTHOR]

Published

2024

234. circCDR1as/miR-7-5p/RAF1 轴参与调控激素性股骨头坏死中的自噬.

Author

翟 生, 艾克热木江 • 阿尔肯, 张 峥, 日夏提 • 帕尔哈提, and 郝飞虎

Abstract

BACKGROUND: Autophagy may be involved in the pathological process of steroid-induced necrosis of the femoral head (SINFH). Some studies have confirmedthat circular RNAs (circRNAs) have a regulatory mechanism in SINFH; however, whether circCDR1as affects autophagy in SINFH has not been investigated. OBJECTIVE: To explore the level of autophagy and the regulatory mechanism of circCDR1as in SINFH. METHODS: Gene expression profiles of SINFH and control rats were extracted from the GSE26316 dataset and differential expression analysis was performed. Subsequently, the biological functions of differentially expressed genes were analyzed. Then, the target miRNAs of circCDR1as and the target genes of target miRNAs were predicted. Further, the target genes were compared with the differentially expressed genes to construct the regulatory network of circCDR1as. In addition, femoral head samples from patients with SINFH and healthy control individuals were collected. Bone marrow mesenchymal stem cells were also applied for cellular experiments and randomly divided into bone marrow mesenchymal stem cell group, model group (methylprednisolone-treated), model+siNC group, and model+si-CDR1as group. RT-qPCR was used to detect the expression of circCDR1as and target genes in cells and tissue samples. Western blot was used to examine the expression of autophagy proteins. The luciferase reporter gene vectors, pmirGLO-CDR1as (WT), pmirGLO-RAF1 (WT), pmirGLOCDR1as (MUT), and pmirGLO-RAF1 (MUT), were constructed and transfected into the cells. miR-7-5p mimic and mimic NC groups were established. The targetregulatory relationship of the circCDR1as network was detected. RESULTS AND CONCLUSION: A total of 1 283 differentially expressed genes were identified between the SINFH and control groups, which were mainly involved in apoptotic and autophagic signaling pathways. Prediction analysis revealed that circCDR1as targeted 6 miRNAs, which in turn regulated 305 target genes. Among these target genes, 31 showed differential expression in SINFH. Among the differentially expressed target genes, RAF1, involved in autophagy, was selected as a key gene, leading to the construction of the circCDR1as/miR-7-5p/RAF1 regulatory network. Compared with the control group, circCDR1as, RAF1, and autophagy levels were upregulated in patients with SINFH and in hormone-induced bone marrow mesenchymal stem cells (P < 0.05), while miR-7-5p expression was downregulated (P < 0.05). Knockdown of circCDR1as significantly decreased cellular autophagy levels (P < 0.05). Dual-luciferase reporter assays confirmed the targeting relationships between circCDR1as and miR-7-5p, as well as between miR-7-5p and RAF1. To conclude, the CircCDR1as/miR-7-5p/RAF1 may potentially promote SINFH through autophagy. Targeting circCDR1as is a potential strategy for partial autophagic repair in the treatment of SINFH. [ABSTRACT FROM AUTHOR]

Published

2024

235. An asymptomatic geminivirus activates autophagy and enhances plant defenses against diverse pathogens.

Author

Wang, Li, Yu, Zijie, Jiang, Mengge, Tian, Mengyuan, Zhou, Hongsheng, Zhao, Wanying, Andika, Ida Bagus, Shang, Qiaoxia, and Sun, Liying

Subjects

POTATO virus X, AUTOPHAGY, CROPS, PLANT diseases, VIRUS diseases

Abstract

Plant viral diseases cause great losses in agricultural production. Virus cross-protection is a strategy in which a mild virus is employed to shield plants against subsequent infections by severe viral strains. However, this approach is restricted to protection against the same viruses. In this study, we observed that pre-inoculation with apple geminivirus (AGV) reduced the accumulation of secondarily infected heterologous viruses, such as cucumber mosaic virus, potato virus X, and tobacco mosaic virus in Nicotiana benthamiana, tomato, and pepper plants. Transcriptional expression analysis showed that autophagy-related genes were transcriptionally up-regulated upon AGV inoculation at an early stage of infection. Accordingly, autophagic activity was observed to be elevated following AGV infection. Interestingly, AGV accumulation was reduced in autophagy-deficient plants, suggesting that autophagy activation promotes AGV infection in the plant. Moreover, pre-inoculation with AGV provided cross-protection against infection with a phytopathogenic bacterium (Pseudomonas syringae) and fungus (Botrytis cinerea) in Nicotiana species. In summary, our study showed that AGV, an asymptomatic virus, could protect plants against severe viral, fungal, and bacterial diseases to some extent through the activation of autophagy pathways, highlighting its potential as a biocontrol agent for managing a wide range of plant crop diseases in the field. [ABSTRACT FROM AUTHOR]

Published

2024

236. Plekhg5 controls the unconventional secretion of Sod1 by presynaptic secretory autophagy.

Author

Hutchings, Amy-Jayne, Hambrecht, Bita, Veh, Alexander, Giridhar, Neha Jadhav, Zare, Abdolhossein, Angerer, Christina, Ohnesorge, Thorben, Schenke, Maren, Selvaraj, Bhuvaneish T., Chandran, Siddharthan, Sterneckert, Jared, Petri, Susanne, Seeger, Bettina, Briese, Michael, Stigloher, Christian, Bischler, Thorsten, Hermann, Andreas, Damme, Markus, Sendtner, Michael, and Lüningschrör, Patrick

Subjects

SECRETION, EXOCYTOSIS, AUTOPHAGY, GUANOSINE triphosphatase, GUANINE

Abstract

Increasing evidence suggests an essential function for autophagy in unconventional protein secretion (UPS). However, despite its relevance for the secretion of aggregate-prone proteins, the mechanisms of secretory autophagy in neurons have remained elusive. Here we show that the lower motoneuron disease-associated guanine exchange factor Plekhg5 drives the UPS of Sod1. Mechanistically, Sod1 is sequestered into autophagosomal carriers, which subsequently fuse with secretory lysosomal-related organelles (LROs). Exocytosis of LROs to release Sod1 into the extracellular milieu requires the activation of the small GTPase Rab26 by Plekhg5. Deletion of Plekhg5 in mice leads to the accumulation of Sod1 in LROs at swollen presynaptic sites. A reduced secretion of toxic ALS-linked SOD1G93A following deletion of Plekhg5 in SOD1G93A mice accelerated disease onset while prolonging survival due to an attenuated microglia activation. Using human iPSC-derived motoneurons we show that reduced levels of PLEKHG5 cause an impaired secretion of ALS-linked SOD1. Our findings highlight an unexpected pathophysiological mechanism that converges two motoneuron disease-associated proteins into a common pathway. Unconventional protein secretion emerges as an important mechanism in aggregate-prone protein removal. Here, the authors demonstrate that Plekhg5 mediates the unconventional secretion of Sod1 by presynaptic secretory autophagy. [ABSTRACT FROM AUTHOR]

Published

2024

237. TERT 调控线粒体氧化应激在疾病中的作用.

Author

田宗源, 李展, and 刘瑞霞

Abstract

Oxidative stress is the result of imbalance between the formation of reactive oxygen species (ROS) and antioxidant level. Mitochondria are important organelles regulating oxidative stress. Telomerase reverse transcriptase (TERT) not only in the nucleus to maintain telomerase activity and telomere length, but also reversibly transits to mitochondria. Improving the activity of oxidative respiratory chain of mitochondria to reduce the production of mitochondrial reactive oxygen species (mtROS) and to activate GSH system as well as autophagy pathway to promote the clearance of mtROS are all important to down-regulate the level of mtROS, which will alleviate oxidative stress and damage and keep the REDOX balance of cells and the normal function of the body. [ABSTRACT FROM AUTHOR]

Published

2024

238. Thyroid Hormone-Mediated Selective Autophagy and Its Implications in Countering Metabolic Dysfunction- Associated Steatotic Liver Disease.

Author

Sinha, Rohit A.

Subjects

*LIVER diseases, *HEPATOCELLULAR carcinoma, *THYROID hormones, *AUTOPHAGY, *METABOLIC disorders

Abstract

The influence of thyroid hormone (TH) on liver metabolism has attracted the attention of pharmacologists seeking new treatments for metabolic dysfunction-associated steatotic liver disease (MASLD), an increasingly common metabolic disorder. In this context, the selective induction of autophagy by TH in preclinical models has been identified as a promising mechanism. In this process, TH clears intrahepatic fat through lipophagy while protecting against inflammation and mitochondrial damage in hepatocytes via mitophagy. Furthermore, TH-induced aggrephagy may represent a protective mechanism to mitigate the development of MASLD-associated hepatocellular carcinoma. Considering the defects in autophagy observed during the progression of human MASLD, the induction of autophagy by TH, its metabolites, and its analogs represent a novel strategy to combat hepatic damage across the MASLD spectrum. [ABSTRACT FROM AUTHOR]

Published

2024

239. Ocular delivery of Pigment Epithelium-Derived Factor (PEDF) as a neuroprotectant for Geographic Atrophy.

Author

Warner, Emily F., Vaux, Laura, Boyd, Kara, Widdowson, Peter S., Binley, Katie M., and Osborne, Andrew

Subjects

*NEUROPROTECTIVE agents, *PIGMENT epithelium-derived factor, *AUTOPHAGY

Abstract

Geographic atrophy (GA) is an advanced form of age-related macular degeneration (AMD), that starts with atrophic lesions in the outer retina that expand to cover the macula and fovea, leading to severe vision loss over time. Pigment Epithelium-Derived Factor (PEDF) has a diverse-range of properties, including its ability to promote cell survival, reduce inflammation, inhibit angiogenesis, combat oxidative stress, regulate autophagy, and stimulate anti-apoptotic pathways, making it a promising therapeutic candidate for GA. However, the relatively short half-life of PEDF protein has precluded its potential as a clinical therapy for GA since it would require frequent injections. Therefore, we describe administration of a PEDF gene, comparing and contrasting delivery routes, viral and nonviral vectors, and consider the critical challenges for PEDF as a neuroprotectant for GA. [ABSTRACT FROM AUTHOR]

Published

2024

240. Protopine regulates oxidative stress, apoptosis and autophagy in H9C2 cardiomyocytes under hypoxic conditions.

Author

Xiaowu Ma, Jing Dong, Yao Wang, and Pingyang Zhang

Subjects

*PTEN protein, *ISOQUINOLINE alkaloids, *MICROTUBULE-associated proteins, *OXIDATIVE stress, *HEART diseases, *ISOQUINOLINE

Abstract

The heart is highly sensitive to oxygen deprivation, and hypoxia can lead to cardiomyocyte damage and subsequent cardiac dysfunction. Protopine Pro), an isoquinoline alkaloid derived from various herbs, exhibits diverse biological activities. However, the protective mechanisms of Pro against hypoxia-induced cardiomyocyte damage are not well understood. In this study, Pro was observed to stimulate cell proliferation in H9C2 cardiomyocytes under hypoxia/reoxygenation (H/R) conditions and mitigate apoptosis typically associated with H/R exposure. Despite a notable increase in oxidative stress following H/R treatment, Pro treatment effectively reduced this effect. Additionally, Pro was found to enhance autophagy in H/R-treated H9C2 cells, as evidenced by higher microtubule-associated protein 1 light chain 3 (LC3)-II/LC3-I ratios and increased LC3B fluorescence intensity. The activation of the phosphatase and tensin homolog deleted on chromosome ten (PTEN)/phosphatidylinositol 3-kinase (PI3K)/protein kinase B (Akt) signaling pathway by Pro was also demonstrated. Overall, Pro influences oxidative stress, apoptosis, and autophagy in H9C2 cardiomyocytes under H/R conditions by activating the PTEN/PI3K/Akt pathway, suggesting it as a promising agent to mitigate hypoxia-induced cardiomyocyte damage. [ABSTRACT FROM AUTHOR]

Published

2024

241. Epigenetic modulation of autophagy pathway by small molecules in colorectal cancer: a systematic review.

Author

Zamani, Mozhdeh, Safari, Farima, Siri, Morvarid, Igder, Somayeh, khatami, Niloofar, Dastghaib, Sanaz, and Mokarram, Pooneh

Abstract

Purpose: Colorectal cancer (CRC) remains a global health challenge with limited treatment success due to drug resistance. Recent research highlights the potential of small molecules to modulate CRC by targeting epigenetics or autophagy pathways. This systematic review explores the epigenetic effect of small molecules on autophagy in CRC, aiming to identify novel therapeutic strategies. Methods: Following PRISMA guidelines, we systematically reviewed 508 studies from PubMed, Scopus, and Web of Science databases until August 13, 2023. Results: Eight studies met inclusion criteria, examining the role of small molecules as epigenetic modulators (Histone acetylation/deacetylation, DNA methylation/demethylation and gene expression regulation by miRNAs) influencing the autophagy pathway in CRC. The studies encompassed in vitro and animal model in vivo studies. Small molecules exhibited diverse effects on autophagy in CRC. For instance, panobinostat promoted autophagy leading to CRC cell death, while aspirin inhibited autophagy flux, reducing aspirin-mediated CRC cell death. The epigenetic modulation of autophagy by various small molecules differently affects their anticancer effect, which underscores the complexity of therapeutic interventions. Conclusion: Understanding the intricate dynamics among small molecules, epigenetic modifications, and autophagy in CRC is crucial for developing targeted therapeutic strategies. Considering the dual role of autophagy in tumorigenesis and tumor suppression, administration of these small molecules may differently affect the cancer cell fate and drug response or resistance based on their effect on the autophagy pathway. Therefore, recognition of the epigenetics mechanism of anticancer small molecules on autophagy may contribute to deciding how to prescribe them for better CRC treatment. [ABSTRACT FROM AUTHOR]

Published

2024

242. TBK1 adaptor AZI2/NAP1 regulates NDP52-driven mitochondrial autophagy.

Author

Ryu Endo, Hiroki Kinefuchi, Momoha Sawada, Reika Kikuchi, Waka Kojima, Noriyuki Matsuda, and Koji Yamano

Subjects

*MITOCHONDRIA, *AUTOPHAGY, *PARKIN (Protein), *UBIQUITIN, *THREONINE

Abstract

Damaged mitochondria are selectively eliminated in a process called mitophagy. PINK1 and Parkin amplify ubiquitin signals on damaged mitochondria, which are then recognized by autophagy adaptors to induce local autophagosome formation. NDP52 and OPTN, two essential mitophagy adaptors, facilitate de novo synthesis of pre-autophagosomal membranes near damaged mitochondria by linking ubiquitinated mitochondria and ATG8 family proteins and by recruiting core autophagy initiation components. The multifunctional serine/threonine kinase TBK1 also plays an important role in mitophagy. OPTN directly binds TBK1 to form a positive feedback loop for isolation membrane expansion. TBK1 is also thought to indirectly interact with NDP52; however, its role in NDP52-driven mitophagy remains largely unknown. Here, we focused on two TBK1 adaptors, AZI2/NAP1 and TBKBP1/SINTBAD, that are thought to mediate the TBK1-NDP52 interaction. We found that both AZI2 and TBKBP1 are recruited to damaged mitochondria during Parkin-mediated mitophagy. Further, a series of AZI2 and TBKBP1 knockout constructs combined with an OPTN knockout showed that AZI2, but not TBKBP1, impacts NDP52-driven mitophagy. In addition, we found that AZI2 at S318 is phosphorylated during mitophagy, the impairment of which slightly inhibits mitochondrial degradation. These results suggest that AZI2, in concert with TBK1, plays an important role in NDP52-driven mitophagy. [ABSTRACT FROM AUTHOR]

Published

2024

243. Promising and challenging phytochemicals targeting LC3 mediated autophagy signaling in cancer therapy.

Author

Rajendran, Peramaiyan, Renu, Kaviyarasi, Ali, Enas M., Genena, Marwa Azmy M., Veeraraghavan, Vishnupriya, Sekar, Ramya, Sekar, Ashok Kumar, Tejavat, Sujatha, Barik, Parthasarathi, and Abdallah, Basem M.

Subjects

*APOPTOSIS, *CELLULAR control mechanisms, *AUTOPHAGY, *TUMOR growth, *CANCER invasiveness

Abstract

Background: Phytochemicals possess a wide range of anti‐tumor properties, including the modulation of autophagy and regulation of programmed cell death. Autophagy is a critical process in cellular homeostasis and its dysregulation is associated with several pathological conditions, such as cancer, neurodegenerative diseases, and diabetes. In cancer, autophagy plays a dual role by either promoting tumor growth or suppressing it, depending on the cellular context. During autophagy, autophagosomes engulf cytoplasmic components such as proteins and organelles. LC3‐II (microtubule‐associated protein 1 light chain 3‐II) is an established marker of autophagosome formation, making it central to autophagy monitoring in mammals. Objective: To explore the regulatory role of phytochemicals in LC3‐mediated autophagy and their potential therapeutic impact on cancer. The review emphasizes the involvement of autophagy in tumor promotion and suppression, particularly focusing on autophagy‐related signaling pathways like oxidative stress through the NRF2 pathway, and its implications for genomic stability in cancer development. Methods: The review focuses on a comprehensive analysis of bioactive compounds including Curcumin, Celastrol, Resveratrol, Kaempferol, Naringenin, Carvacrol, Farnesol, and Piperine. Literature on these compounds was examined to assess their influence on autophagy, LC3 expression, and tumor‐related signaling pathways. A systematic literature search was conducted across databases including PubMed, Scopus, and Web of Science from inception to 2023. Studies were selected from prominent databases, focusing on their roles in cancer diagnosis and therapeutic interventions, particularly in relation to LC3‐mediated mechanisms. Results: Phytochemicals have been shown to modulate autophagy through the regulation of LC3‐II levels and autophagic flux in cancer cells. The interaction between autophagy and other cellular pathways such as oxidative stress, inflammation, and epigenetic modulation highlights the complex role of autophagy in tumor biology. For instance, Curcumin and Resveratrol have been reported to either induce or inhibit autophagy depending on cancer type, influencing tumor progression and therapeutic responses. Conclusion: Targeting autophagy through LC3 modulation presents a promising strategy for cancer therapy. The dual role of autophagy in tumor suppression and promotion, however, necessitates careful consideration of the context in which autophagy is induced or inhibited. Future research should aim to delineate these context‐specific roles and explore how phytochemicals can be optimized for therapeutic efficacy. Novel therapeutic strategies should focus on the use of bioactive compounds to fine‐tune autophagy, thereby maximizing tumor suppression and inducing programmed cell death in cancer cells. [ABSTRACT FROM AUTHOR]

Published

2024

244. Bioinformatics analysis of G protein subunit gamma transduction protein 2‐autophagy axis in CD11b+ dendritic cells as a potential regulator to skew airway neutrophilic inflammation in asthma endotypes.

Author

Ji, Xiaoying, Zhou, Yaoliang, He, Shendong, Chen, Hongda, Zhang, Xianming, Chen, Zhifeng, and Cai, Jinwen

Subjects

*GENE expression, *GENE regulatory networks, *T helper cells, *DENDRITIC cells, *CELL differentiation, *G proteins

Abstract

Background: Asthma is a heterogeneous inflammatory disease with two main clinical endotypes: type 2 (T2) high and low asthma. The plasticity and autophagy in dendritic cells (DCs) influence T helper (Th)2 or Th17 differentiation to regulate asthma endotypes. Enhanced autophagy in DCs fosters Th2 differentiation in allergic environments, while reduced autophagy favors Th17 cell differentiation in sensitized and infected environments. Autophagy regulation in DCs involves interaction with various pathways like G protein‐coupled receptor (GPCR), mammalian target of rapamycin (mTOR), or phosphoinositide 3‐kinase (PI3K) pathway. However, specific molecules within DCs influencing asthma endotypes remain unclear. Methods: Gene expression data series (GSE) 64896, 6858, 2276, and 55247 were obtained from gene expression omnibus (GEO) database. Differentially expressed genes (DEGs) between CD103+ and CD11b+ DCs after induction by ovalbumin (OVA) and lipopolysaccharide (LPS) were analyzed using GEO2R. DEGs were examined through Gene Ontology (GO), Kyoto Encyclopedia of Genes and Genomes (KEGG), and protein–protein interaction (PPI) analyses. The hub gene network was construct with STRING database and Cytoscape. Autophagy differences in DCs and the selected hub gene in GSE6858, GSE2276, and GSE55247 were evaluated using student t tests. Results: Our analysis identified 635 upregulated and 360 downregulated genes in CD11b+ DCs, compared to CD103+ DCs. These DEGs were associated with "PI3K‐AKT signaling pathway," "Ras signaling pathway," and so forth. Thirty‐five hub genes were identified, in which G protein subunit gamma transduction protein 2 (Gngt2) in CD11b+ DCs exhibited a relatively specific increase in expression associated with autophagy defects under the induction environment similar to T2 low asthma model. No significant difference was found in lung Gngt2 expression between T2 high asthma model and control group. Conclusion: Our analysis suggested Gngt2 acted as an adapter molecule that inhibited autophagy, promoting Th17‐mediated airway inflammation via the GPCR pathway in a T2 low asthma mice model. Targeting this pathway provides new asthma treatment strategies in preclinical research. [ABSTRACT FROM AUTHOR]

Published

2024

245. Autophagy plays an antiviral defence role against tomato spotted wilt orthotospovirus and is counteracted by viral effector NSs.

Author

Zhang, Xingwang, Hong, Hao, Yan, Jiaoling, Yuan, Yulong, Feng, Mingfeng, Liu, Qinhai, Zhao, Yanxiao, Yang, Tongqing, Huang, Shen, Wang, Chunli, Zhao, Ruizhen, Zuo, Wenyu, Liu, Suyu, Ding, Zixuan, Huang, Changjun, Zhang, Zhongkai, Kundu, Jiban Kumar, and Tao, Xiaorong

Subjects

*TOMATO spotted wilt virus disease, *PHYTOPATHOGENIC microorganisms, *AUTOPHAGY, *VIRAL replication, *PLANT species

Abstract

Autophagy, an intracellular degradation process, has emerged as a crucial innate immune response against various plant pathogens, including viruses. Tomato spotted wilt orthotospovirus (TSWV) is a highly destructive plant pathogen that infects over 1000 plant species and poses a significant threat to global food security. However, the role of autophagy in defence against the TSWV pathogen, and whether the virus counteracts this defence, remains unknown. In this study, we report that autophagy plays an important role in antiviral defence against TSWV infection; however, this autophagy‐mediated defence is counteracted by the viral effector NSs. Transcriptome profiling revealed the up‐regulation of autophagy‐related genes (ATGs) upon TSWV infection. Blocking autophagy induction by chemical treatment or knockout/down of ATG5/ATG7 significantly enhanced TSWV accumulation. Notably, the TSWV nucleocapsid (N) protein, a major component of the viral replication unit, strongly induced autophagy. However, the TSWV nonstructural protein NSs was able to effectively suppress N‐induced autophagy in a dose‐dependent manner. Further investigation revealed that NSs inhibited ATG6‐mediated autophagy induction. These findings provide new insights into the defence role of autophagy against TSWV, a representative segmented negative‐strand RNA virus, as well as the tospoviral pathogen counterdefence mechanism. [ABSTRACT FROM AUTHOR]

Published

2024

246. Neuroprotective effects of punicalagin and/or micronized zeolite clinoptilolite on manganese‐induced Parkinson's disease in a rat model: Involvement of multiple pathways.

Author

Abu‐Elfotuh, Karema, Abbas, Ashwaq N., Najm, Mazin A. A., Qasim, Qutaiba A., Hamdan, Ahmed M. E., Abdelrehim, Amany B., Gowifel, Ayah M. H., Al‐Najjar, Aya H., Atwa, Ahmed M., Kozman, Magy R., Khalil, Azza S., Negm, Amira M., Mousa, Sara Nagdy Mahmoud, Hamdan, Amira M., Abd El‐Rhman, Rana H., Abdelmohsen, Shaimaa R., Tolba, Amina M. A., Aboelsoud, Heba Abdelnaser, Salahuddin, Ahmad, and Darwish, Alshaymaa

Subjects

*LABORATORY rats, *PARKINSON'S disease, *MANGANESE chlorides, *ENDOPLASMIC reticulum, *CENTRAL nervous system, *BUTYRIC acid

Abstract

Background: Manganism, a central nervous system dysfunction correlated with neurological deficits such as Parkinsonism, is caused by the substantial collection of manganese chloride (MnCl2) in the brain. Objectives: To explore the neuroprotective effects of natural compounds, namely, micronized zeolite clinoptilolite (ZC) and punicalagin (PUN), either individually or in combination, against MnCl2‐induced Parkinson's disease (PD). Methods: Fifty male albino rats were divided into 5 groups (Gps). Gp I was used as the control group, and the remaining animals received MnCl2 (Gp II–Gp V). Rats in Gps III and IV were treated with ZC and PUN, respectively. Gp V received both ZC and PUN as previously reported for the solo‐treated plants. Results: ZC and/or PUN reversed the depletion of monoamines in the brain and decreased acetyl choline esterase activity, which primarily adjusted the animals' behavior and motor coordination. ZC and PUN restored the balance between glutamate/γ‐amino butyric acid content and markedly improved the brain levels of brain‐derived neurotrophic factor and nuclear factor erythroid 2‐related factor 2/heme oxygenase‐1 and decreased glycogen synthase kinase‐3 beta activity. ZC and PUN also inhibited inflammatory and oxidative markers, including nuclear factor kappa‐light‐chain‐enhancer of activated B cells, Toll‐like receptor 4, nucleotide‐binding domain, leucine‐rich‐containing family, pyrin domain‐containing‐3 and caspase‐1. Bcl‐2‐associated X‐protein and B‐cell leukemia/lymphoma 2 protein (Bcl‐2) can significantly modify caspase‐3 expression. ZC and/or PUN ameliorated PD in rats by decreasing the levels of endoplasmic reticulum (ER) stress markers (p‐protein kinase‐like ER kinase (PERK), glucose‐regulated protein 78, and C/EBP homologous protein (CHOP)) and enhancing the levels of an autophagy marker (Beclin‐1). Discussion and Conclusion: ZC and/or PUN mitigated the progression of PD through their potential neurotrophic, neurogenic, anti‐inflammatory, antioxidant, and anti‐apoptotic activities and by controlling ER stress through modulation of the PERK/CHOP/Bcl‐2 pathway. [ABSTRACT FROM AUTHOR]

Published

2024

247. Combination of Diosmetin With Chrysin Against Hepatocellular Carcinoma Through Inhibiting PI3K/AKT/mTOR/NF‐кB Signaling Pathway: TCGA Analysis, Molecular Docking, Molecular Dynamics, In Vitro Experiment.

Author

Yu, Xiang, Zhang, Di, Hu, Chengming, Yu, Zejun, Li, Yang, Fang, Cheng, Qiu, Yinsheng, Mei, Zhinan, and Xu, Lingyun

Subjects

*MOLECULAR docking, *MOLECULAR dynamics, *HEPATOCELLULAR carcinoma, *GENE expression, *INFLAMMATORY mediators

Abstract

Hepatocellular carcinoma (HCC) is the sixth most prevalent malignant tumor. Hepatocellular carcinogenesis is closely linked to apoptosis, autophagy, and inflammation. Diosmetin and chrysin, are two flavonoid compounds, exhibit anti‐inflammatory and anticancer properties. In this study, the TCGA database was utilized to identify differentially expressed genes between normal subjects and HCC patients. Molecular docking and molecular dynamics analyses were employed to assess the binding affinity of chrysin and diosmetin to key proteins in the PI3K/AKT/mTOR/NF‐κB signaling pathway. Western blotting and RT‐qPCR were used to measure the protein and gene expression within this pathway. The results indicated that HCC patients had elevated levels of PI3K, AKT, mTOR, and P65 proteins compared to normal subjects, which adversely affected patient survival. Molecular docking and dynamics studies demonstrated that diosmetin and chrysin are effectively bound to these four proteins. In vitro experiments revealed that the combination of diosmetin and chrysin could induce apoptosis, enhance autophagy, reduce inflammatory mediator production, and improve the tumor cell microenvironment by inhibiting the PI3K/AKT/mTOR/NF‐κB signaling pathway. Notably, the synergy score for the combination of diosmetin (25 μM) and chrysin (10 μM) was 16. Thus, the diosmetin–chrysin combination shows promise as an effective therapeutic approach for hepatocellular carcinoma due to its strong synergistic effect. [ABSTRACT FROM AUTHOR]

Published

2024

248. TaATG8 Is Involved in the Response to Abiotic Stresses and Powdery Mildew in Arabidopsis.

Author

Tian, L. J., Liu, G., Wang, R. N., Wei, F. J., Zhang, F. F., Hou, C. Y., and Wang, D. M.

Subjects

*AMINO acid sequence, *ABIOTIC stress, *DEFICIENCY diseases, *SIGNAL processing, *AUTOPHAGY, *POWDERY mildew diseases

Abstract

ATG8 is a key gene in the process of autophagy. The expression of ATG8 affects many intracellular progresses. Here we report that the amino acid sequence of AtATG8 and TaATG8 protein share a high similarity of 84.03%, we found that TaATG8 involved in the abiotic stresses, such as drought, salt stress and nutrient deficiency. Moreover, TaATG8 plays an important role in the process of Arabidopsis defending against biotic stress caused by the infection of powdery mildew through HR. Hydrogen peroxide acts as an important metabolic product and signaling molecule in the process of TaATG8 resisting to powdery mildew. [ABSTRACT FROM AUTHOR]

Published

2024

249. 葛根素通过AMPK/mTOR 通路激活自噬 治疗小鼠高脂血症.

Author

李蕾, 金妍伶, 吕碧君, 王 月, 陆芝梅, 袁迪芬, 吴月滢, and 袁嘉丽

Abstract

The aim of this study was to investigate the mechanism of therapeutic effect of pucrarin on Hyperlipidemia (HLP) model mice, C57BL/6J mice were randomly divided into blank Control group (Control), disease Model group (Model) and puerarin low-dose, medium-dose and high-dose groups (PUE-L, PUE-M, PUE-H). After the successful construction of the hyperlipidemia model, the mice were treated with puerarin for 4 weeks, and the changes of the lipid profile of the mice were detected by the kit. In addition, pathological changes of mouse liver tissues were observed, and key proteins in liver tissues were detected by Western blot. They included the expression levels of adenylate activated protein kinase (AMPK) and rapamycin mammalian target protein (mTOR) signaling pathway, sterol regulatory element binding protein (SREBP), a key regulatory protein of lipid metabolism, and microtubule-associated protein light chain 3 (LC3) and autophagy substrate (P62) during autophagy, Further, we used quantitative polymerase chain reaction (q-PCR) to detect the mRNA expression of acetyl-CoA carboxylase (ACC), fatty acid synthetase (FAS), sterol regulatory element-binding protein-1c (SREGBP-1C) in liver tissue. And the expression levels of mRNA and inflammatory factors related to AMPK/mTOR signaling pathway. Compared with the model group, the levels of total cholesterol (TC), triglyceride (TG) and low density lipoprotein cholesterol (LDL-C) in the serum of puerarin treated group were significantly decreased, while the levels of high density lipoprotein cholesterol (HDL-C) were significantly increased. In liver tissue, the vacuole-like changes and lipid droplet accumulation were significantly reduced after puerarin intervention, After administration, the relative expression levels of ACC, FAS and SREBP-Ic mRNA in liver tissue decreased, the expression levels of LPS and pro-inflammatory factors TNF-α and II-8 decreased, while the expression levels of antiinflammatory factors 11-4 and 11-10 increased. In addition, the protein levels of mTOR, SREBP and P62 were decreased, while the expression levels of AMPK, p-AMPK and LC3 were increased. In summary, the experimental results show that puerarin can effectively improve the blood lipid profile of hyperlipidemia model mice and reduce the inflammatory response. The mechanism of action may be related to the regulation of AMPK/mTOR signaling pathway by puerarin, which promotes the activation of autophagy. These findings provide a new perspective on the treatment of hyperlipidemia, especially in the use of plant medicine. [ABSTRACT FROM AUTHOR]

Published

2024

250. Anticancer Effects of Weizmannia coagulans MZY531 Postbiotics in CT26 Colorectal Tumor-Bearing Mice by Regulating Apoptosis and Autophagy.

Author

Zhong, Bao, Zhao, Yujuan, Gao, Lei, Yang, Ge, Gao, Yansong, Li, Fenglin, and Li, Shengyu

Subjects

*CYCLIC-AMP-dependent protein kinase, *CANCER cell proliferation, *COLON cancer, *JAK-STAT pathway, *CARCINOEMBRYONIC antigen

Abstract

Weizmannia coagulans has been shown to have anticancer properties. However, there is limited research on the effects of postbiotic W. coagulans on colorectal cancer cell proliferation. Additionally, the exact mechanisms through which it influences apoptosis- and autophagy-related signaling pathways are yet to be thoroughly elucidated. This study explored the role of W. coagulans MZY531 as a postbiotic in inhibiting tumor growth by modulating apoptosis and autophagy in tumor cells. During the experimental period in the model group, tumors proliferated, tumor markers increased significantly, and immunofluorescence results showed that caspase-3 and terminal deoxynucleotidyl transferase dUTP nick-end labeling were significantly decreased. Conversely, supplementation with W. coagulans MZY531 postbiotics significantly reduced the levels of tumor markers carcinoembryonic antigen, colon cancer antigen, and extracellular protein kinase A and promoted cell apoptosis by increasing the caspase-3-positive count and terminal deoxynucleotidyl transferase dUTP nick-end labeling-positive cells in tumor tissue. Mechanistically, W. coagulans MZY531 postbiotics inhibit tumor growth through the modulation of the Bax/Bcl-2/caspase-3 and JAK2/STAT3 apoptosis pathways and PI3K/AKT/mTOR and TGF-β/SMAD4 cell autophagy pathways. W. coagulans MZY531 postbiotics had a more significant effect than that of W. coagulans MZY531 alone. Probiotics are expected to become effective natural functional foods for the treatment of colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2024