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5 result(s) for "Gazes, Michael I"
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Apoptosis recognition receptors regulate skin tissue repair in mice
Apoptosis and clearance of apoptotic cells via efferocytosis are evolutionarily conserved processes that drive tissue repair. However, the mechanisms by which recognition and clearance of apoptotic cells regulate repair are not fully understood. Here, we use single-cell RNA sequencing to provide a map of the cellular dynamics during early inflammation in mouse skin wounds. We find that apoptotic pathways and efferocytosis receptors are elevated in fibroblasts and immune cells, including resident Lyve1 + macrophages, during inflammation. Interestingly, human diabetic foot wounds upregulate mRNAs for efferocytosis pathway genes and display altered efferocytosis signaling via the receptor Axl and its ligand Gas6 . During early inflammation in mouse wounds, we detect upregulation of Axl in dendritic cells and fibroblasts via TLR3-independent mechanisms. Inhibition studies in vivo in mice reveal that Axl signaling is required for wound repair but is dispensable for efferocytosis. By contrast, inhibition of another efferocytosis receptor, Timd4, in mouse wounds decreases efferocytosis and abrogates wound repair. These data highlight the distinct mechanisms by which apoptotic cell detection coordinates tissue repair and provides potential therapeutic targets for chronic wounds in diabetic patients. Our skin is constantly exposed to potential damage from the outside world, and it is vital that any injuries are repaired quickly and effectively. Diabetes and many other health conditions can hamper wound healing, resulting in chronic wounds that are both painful and at risk of becoming infected, which can lead to serious illness and death of patients. After an injury to the skin, the wound becomes inflamed as immune cells rush to the site of injury to fight off infection and clear the wound of dead cells and debris. Some of these dead cells will have died by a highly controlled process known as apoptosis. These so-called apoptotic cells display signals on their surface that nearby healthy cells recognize. This triggers the healthy cells to eat the apoptotic cells to remove them from the wound. Previous studies have linked changes in cell death and the removal of dead cells to chronic wounds in patients with diabetes, but it remains unclear how removing dead cells from the wound affects healing. Justynski et al. used a genetic technique called single-cell RNA sequencing to study the patterns of gene activity in mouse skin cells shortly after a wound. The experiments found that, as the area around the wound started to become inflamed, the wounded cells produced signals of apoptosis that in turn triggered nearby healthy cells to remove them. Other signals relating to the removal of dead cells were also widespread in the mouse wounds and treating the wounds with drugs that inhibit these signals resulted in multiple defects in the healing process. Further experiments used the same approach to study samples of tissue taken from foot wounds in human patients with or without diabetes. This revealed that several genes involved in the removal of dead cells were more highly expressed in the wounds of diabetic patients than in the wounds of other individuals. These findings indicate that for wounds to heal properly it is crucial for the body to detect and clear apoptotic cells from the wound site. Further studies building on this work may help to explain why some diabetic patients suffer from chronic wounds and help to develop more effective treatments for them.
Transcriptional heterogeneity in human diabetic foot wounds
Wound repair requires the coordination of multiple cell types including immune cells and tissue resident cells to coordinate healing and return of tissue function. Diabetic foot ulceration is a type of chronic wound that impacts over 4 million patients in the US and over 7 million worldwide (Edmonds et al., 2021). Yet, the cellular and molecular mechanisms that go awry in these wounds are not fully understood. Here, by profiling chronic foot ulcers from non-diabetic (NDFUs) and diabetic (DFUs) patients using single-cell RNA sequencing, we find that DFUs display transcription changes that implicate reduced keratinocyte differentiation, altered fibroblast function and lineages, and defects in macrophage metabolism, inflammation, and ECM production compared to NDFUs. Furthermore, analysis of cellular interactions reveals major alterations in several signaling pathways that are altered in DFUs. These data provide a view of the mechanisms by which diabetes alters healing of foot ulcers and may provide therapeutic avenues for DFU treatments.Wound repair requires the coordination of multiple cell types including immune cells and tissue resident cells to coordinate healing and return of tissue function. Diabetic foot ulceration is a type of chronic wound that impacts over 4 million patients in the US and over 7 million worldwide (Edmonds et al., 2021). Yet, the cellular and molecular mechanisms that go awry in these wounds are not fully understood. Here, by profiling chronic foot ulcers from non-diabetic (NDFUs) and diabetic (DFUs) patients using single-cell RNA sequencing, we find that DFUs display transcription changes that implicate reduced keratinocyte differentiation, altered fibroblast function and lineages, and defects in macrophage metabolism, inflammation, and ECM production compared to NDFUs. Furthermore, analysis of cellular interactions reveals major alterations in several signaling pathways that are altered in DFUs. These data provide a view of the mechanisms by which diabetes alters healing of foot ulcers and may provide therapeutic avenues for DFU treatments.
Classification of the patient population of a podiatric medicine clinic into high rollers (patients keeping clinic visits) and low rollers (patients failing to keep scheduled appointments) and commonly seen conditions
Background: The Foot Center of New York is the oldest podiatric medical facility on the planet treating a large variety of foot related pathologies. Despite how podiatric medicine has existed for over a century, no large study has been performed analyzing patient populations and conditions that lead to patients seeking podiatric medical care. Methodology: A two year study period was chosen for analysis of patient encounters recorded in the Electronic Medical Record (EMR) system in the clinic. 999 patients of the 7,099 who scheduled appointments within the 2 year study period were chosen for examination and classified into high/low roller and compliant/non-compliant patient categories. Patients were further classified by language, insurance type, age, and sex. Common conditions were also briefly reviewed. Results: 71.88% of appointments scheduled were kept. 32.32% of the population were compliant high rollers. 20.49% of the population were compliant low rollers. 25.37% of the population were non-compliant high rollers. 21.83% of the population were non-compliant low rollers. The top 5 most common conditions dissected from the EMR noted in the general population were fungus, onychomycosis, hyperkeratosis, drug prescription, and abnormal vascular status. Results were further classified by language, insurance type, age, and sex. Conclusion: Knowing possible attendance rates, roller statuses, and compliance rates in addition to relating the most common medical conditions with language, insurance type, age, and sex can enable practitioners to provide valuable information and better management of conditions based on expectations from different types of patients.
Transcriptional heterogeneity in diabetic foot wounds
Wound repair requires the coordination of multiple cell types including immune cells and tissue resident cells to coordinate healing and return of tissue function. Diabetic foot ulceration is a type of chronic wound that impacts over 4 million patients in the US and over 7 million worldwide (Edmonds et al., 2021). Yet, the cellular and molecular mechanisms that go awry in these wounds are not fully understood. Here, by profiling chronic foot ulcers from non-diabetic (NDFUs) and diabetic (DFUs) patients using single-cell RNA sequencing, we find that DFUs display transcription changes that implicate reduced keratinocyte differentiation, altered fibroblast function and lineages, and defects in macrophage metabolism, inflammation, and ECM production compared to NDFUs. Furthermore, analysis of cellular interactions reveals major alterations in several signaling pathways that are altered in DFUs. These data provide a view of the mechanisms by which diabetes alters healing of foot ulcers and may provide therapeutic avenues for DFU treatments.Competing Interest StatementThe authors have declared no competing interest.Footnotes* https://skinregeneration.org/data/* https://www.ncbi.nlm.nih.gov/geo/query/acc.cgi?acc=GSE165816
A Low-Cost Solar LED Lighting System Designed for Local Assembly and Repair in Off-Grid Communities
This is about bringing sustainable lighting systems to the world's billion poorest people who live in off-grid, rural communities. The lack of infrastructure presents a distribution challenge that places this market beyond the reach of the companies that address the Base of the Economic Pyramid sector. Addressing this market requires enabling the end-user to set up a local infrastructure for system maintenance. This requires a shift from the traditional consumer electronics paradigm of high-volume automated assembly with no user-serviceable parts. A lighting system is presented for local assembly and repair using locally sourced materials.