Publications by authors named "Ashley VanCleave"
Article Synopsis
- This study investigates how diabetes triggers the activation of the NLRP3 inflammasome, a key player in retinal complications associated with diabetes.
- Researchers found that both NLRP3 and interleukin-1β (IL-1β) levels increased in diabetic mice and cultured Müller cells under hyperglycemic conditions, with the stress response protein REDD1 being essential for this increase.
- The findings suggest that REDD1 influences GSK3β activity, which is crucial for NLRP3 inflammasome activation and IL-1β production in Müller glial cells during diabetes, potentially affecting visual function in diabetic mice.
Background: Skeletal development requires precise extrinsic and intrinsic signals to regulate processes that form and maintain bone and cartilage. Notch1 is a highly conserved signaling receptor that regulates cell fate decisions by controlling the duration of transcriptional bursts. Epigenetic molecular events reversibly modify DNA and histone tails by influencing the spatial organization of chromatin and can fine-tune the outcome of a Notch1 transcriptional response.
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- Inflammation plays a significant role in the development and progression of diabetic retinal complications, with REDD1 being a key protein involved in this process.
- REDD1 promotes the activation of NF-κB, a transcription factor linked to inflammation, by affecting the phosphorylation of GSK3β, particularly under hyperglycemic conditions.
- Inhibiting GSK3β in diabetic models can reduce NF-κB activity and pro-inflammatory cytokine expression, suggesting potential therapeutic avenues for managing diabetic retinal inflammation.
Endoplasmic reticulum (ER) stress and inflammation are hallmarks of myocardial impairment. Here, we investigated the role of the stress response protein regulated in development and DNA damage 1 (REDD1) as a molecular link between ER stress and inflammation in cardiomyocytes. In mice fed a high-fat high-sucrose (HFHS, 42% kcal fat, 34% sucrose by weight) diet for 12 wk, REDD1 expression in the heart was increased in coordination with markers of ER stress and inflammation.
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- Inflammation in the retina is worsened by diabetes, and the study investigates the role of a stress response protein called REDD1 in this process.
- Increased levels of REDD1 were found in the retinas of diabetic mice, and it was essential for the expression of inflammatory cytokines.
- Deleting REDD1 in human retinal cells inhibited these cytokines by affecting the NF-κB signaling pathway, demonstrating that REDD1 is a key player in diabetic retinal inflammation.
Purpose: Neuroglial dysfunction occurs early in the progression of diabetic retinopathy. In response to diabetes or hypoxia, Müller glia secrete cytokines and growth factors that contribute to disease progression. This study was designed to examine common signaling pathways activated in Müller glia by both type 1 and pre-/type 2 diabetes.
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- REDD1, a stress response protein, is linked to visual deficits in diabetes, with increased levels observed in the retinas of diabetic mice, despite no changes in its mRNA or ribosome association.
- Oral antioxidants were found to lower oxidative stress and REDD1 protein levels, indicating a potential therapeutic pathway for managing retinal issues in diabetes.
- The study uncovered that high glucose conditions led to oxidative stress, enhancing REDD1 expression and stability through disulfide bond formation, impacting its degradation and highlighting a complex regulatory mechanism involving redox status.
Article Synopsis
- Clinical studies suggest that the protein REDD1 is involved in retinal issues caused by ischemia and diabetes, particularly in Müller glia cells.
- Researchers used REDD1-specific knockout mice to show that without REDD1, oxidative stress and gliosis (a type of cell reaction in the retina) are reduced in diabetic conditions, which helps preserve retinal health.
- Findings indicate that REDD1 in Müller glia is crucial for the retina's detrimental responses to diabetes, leading to complications like neurodegeneration and vision problems that are not observed in REDD1-deficient mice.
Cancer cachexia is a wasting disorder associated with advanced cancer that contributes to mortality. Cachexia is characterized by involuntary loss of body weight and muscle weakness that affects physical function. Regulated in DNA damage and development 1 (REDD1) is a stress-response protein that is transcriptionally upregulated in muscle during wasting conditions and inhibits mechanistic target of rapamycin complex 1 (mTORC1).
View Article and Find Full Text PDFDysregulation of histone deacetylases (HDACs) is associated with the pathogenesis of human osteosarcoma, which may present an epigenetic vulnerability as well as a therapeutic target. Domatinostat (4SC-202) is a next-generation class I HDAC inhibitor that is currently being used in clinical research for certain cancers, but its impact on human osteosarcoma has yet to be explored. In this study, we report that 4SC-202 inhibits osteosarcoma cell growth in vitro and in vivo.
View Article and Find Full Text PDFObjective: Humpback () mice harbor a pathogenic mutation in the gene and can serve as a beneficial animal model for investigating human myopathy, kyphosis, and developmental disorders, including lateral meningocele syndrome. Detection of the point mutation in mice is important for maintaining strains and scrutinizing genetic rescues, especially considering that homozygous mice are infertile and indistinguishable from their littermates at a young age. This study aimed for the development of a novel, precise, and time-saving genotyping method to identify the mutation in mice.
View Article and Find Full Text PDFOutcomes have not improved for metastatic osteosarcoma for several decades. In part, this failure to develop better therapies stems from a lack of understanding of osteosarcoma biology, given the rarity of the disease and the high genetic heterogeneity at the time of diagnosis. We report here the successful establishment of a new human osteosarcoma cell line, COS-33, from a patient-derived xenograft and demonstrate retention of the biological features of the original tumor.
View Article and Find Full Text PDFAberrant activation of Wnt signaling has been implicated in human osteosarcoma, which may provide a genetic vulnerability that can be targeted in osteosarcoma treatment. To test whether Wnt activation is necessary for osteosarcoma growth, colony formation, invasion, and metastasis, we treated human osteosarcoma cells with a small molecule inhibitor of Wnt/β-catenin, PRI-724, which suppresses Wnt/β-catenin-mediated transcription. We found increased protein levels of endogenous active-β-catenin in five human osteosarcoma cell lines.
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