697 research outputs found
Evaluation of a Care Management Program on Family Caregivers of Persons with Dementia
Dementia due to Alzheimer’s and other disease is a growing concern for healthcare providers as the number of individuals in the U.S. population ages. Persons with dementia (PWDs) rely on caregivers, primarily family caregivers (FCGs), for basic and instrumental activities of daily living as the disease progresses. There may be negative outcomes, such as depression, strain, and distress for FCGs of PWDs. Routine assessment and intervention by healthcare providers can address needs of FCGs of PWDs. There are multiple interventions that have demonstrated effectiveness in caring for PWDs and FCGs; one such intervention is care management. The University of California, Davis, Health (UCDH) Alzheimer’s and Dementia Care (ADC) Program is a care management program serving PWDs and FCGs since July 2021. This project evaluates the program’s effect on FCG outcomes, specifically depression, strain, and distress. Despite an increase in the severity of dementia and in the number of basic and instrumental activities of daily living requiring caregiving support, FCGs of PWDs experienced decreased levels of depression, strain, and distress following 12 to 18 months in the UCDH ADC Program. Other notable findings include PWDs experiencing reductions in severity of neuropsychiatric symptoms and remaining at home with FCGs. Encounters in the program were primarily unscheduled, non-billable encounters. Despite limitations, primarily small sample size and lack of sample diversity, this project contributes to literature supporting dementia care management for PWDs and FCGs. Future research should address these limitations to understand the experiences of a diverse population and to make dementia care management programs sustainable
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Use of GIS and Remote Sensing Technologies to Study Habitat Requirements of Ocelots, Leopardus pardalis, in south Texas
The goals of this study were to use Geographic Information Systems (GIS) and remote sensing technologies to gain a better understanding of habitat requirements of a population of ocelots in south Texas, and then apply this knowledge to form a predictive model to locate areas of suitable habitat in Willacy and Cameron counties, Texas. Satellite imagery from August 1991 and August 2000 were classified into four land cover types: closed canopy, open canopy, water, and urban/barren. These classified images were converted into digital thematic maps for use in resource utilization studies and modeling. Location estimates (762 from 1991 and 406 from 2000) were entered into a GIS in order to extract information about home range and resource selection. Each animal's home range was calculated using both Minimum Convex Polygon (MCP) and Kernel home range estimators (95% and 50%). Habitat parameters of interest were: soil, land cover, human density, road density, and distance to closest road, city and water body. Ocelots were found to prefer closed canopy and avoid open canopy land cover types. Ocelots preferred soils known to support thorn scrub, an indication of the importance of this habitat. Landscape metrics associated with habitat used by ocelots were determined through the use of Patch Analyst, an extension for ArcView 3.2. Contrary to expectations, ocelots utilized areas with greater fragmentation than random areas available for use. However, this use of highly fragmented areas was an indication of the degree of fragmentation of suitable habitat in the area. Further investigation of patch size selection indicated that ocelots used large sized patches disproportionately to availability, indicating a preference for larger patches. A model was created using the resource selection and habitat preference GIS database from 1991. This model was used to identify areas of “optimal”, ”sub-optimal”, and “unsuitable” habitat for ocelots in 2000. This resultant map was compared to known locations of ocelots in 2000. Ocelots were found to prefer optimal habitat and avoid unsuitable habitat, an indication that the model created was valid
So, You Want to 3D Print a Landscape? An Outline of Some Methods
https://digitalcommons.cedarville.edu/alum_books/1453/thumbnail.jp
So, You Want to 3D Print a Landscape? An Outline of Some Methods
https://digitalcommons.cedarville.edu/alum_books/1435/thumbnail.jp
Lorentz-Violating Electrostatics and Magnetostatics
The static limit of Lorentz-violating electrodynamics in vacuum and in media
is investigated. Features of the general solutions include the need for
unconventional boundary conditions and the mixing of electrostatic and
magnetostatic effects. Explicit solutions are provided for some simple cases.
Electromagnetostatics experiments show promise for improving existing
sensitivities to parity-odd coefficients for Lorentz violation in the photon
sector.Comment: 9 page
Phenformin has anti-tumorigenic effects in human ovarian cancer cells and in an orthotopic mouse model of serous ovarian cancer
Obesity and diabetes have been associated with increased risk and worse outcomes in ovarian cancer (OC). The biguanide metformin is used in the treatment of type 2 diabetes and is also believed to have anti-tumorigenic benefits. Metformin is highly hydrophilic and requires organic cation transporters (OCTs) for entry into human cells. Phenformin, another biguanide, was taken off the market due to an increased risk of lactic acidosis over metformin. However, phenformin is not reliant on transporters for cell entry; and thus, may have increased potency as both an anti-diabetic and anti-tumorigenic agent than metformin. Thus, our goal was to evaluate the effect of phenformin on established OC cell lines, primary cultures of human OC cells and in an orthotopic mouse model of high grade serous OC. In three OC cell lines, phenformin significantly inhibited cellular proliferation, induced cell cycle G1 arrest and apoptosis, caused cellular stress, inhibited adhesion and invasion, and activation of AMPK and inhibition of the mTOR pathway. Phenformin also exerted anti-proliferative effects in seven primary cell cultures of human OC. Lastly, phenformin inhibited tumor growth in an orthotopic mouse model of serous OC, coincident with decreased Ki-67 staining and phosphorylated-S6 expression and increased expression of caspase 3 and phosphorylated-AMPK. Our findings demonstrate that phenformin has anti-tumorigenic effects in OC as previously demonstrated by metformin but it is yet to be determined if it is superior to metformin for the potential treatment of this disease
JQ1 suppresses tumor growth via PTEN/PI3K/AKT pathway in endometrial cancer
Overexpression of c-Myc is associated with worse outcomes in endometrial cancer, indicating that c-Myc may be a promising target for endometrial cancer therapy. A novel small molecule, JQ1, has been shown to block BRD4 resulting in inhibition of c-Myc expression and tumor growth. Thus, we investigated whether JQ1 can inhibit endometrial cancer growth in cell culture and xenograft models. In PTEN-positive endometrial cancer cells, JQ1 significantly suppressed cell proliferation via induction of G1 phase arrest and apoptosis in a dose-dependent manner, accompanied by a sharp decline in cyclin D1 and CDK4 protein expression. However, PTEN-negative endometrial cancer cells exhibited intrinsic resistance to JQ1, despite significant c-Myc inhibition. Moreover, we found that PTEN and its downstream PI3K/AKT signaling targets were modulated by JQ1, as evidenced by microarray analysis. Silencing of PTEN in PTEN-positive endometrial cancer cells resulted in resistance to JQ1, while upregulation of PTEN in PTEN-negative endometrial cancer cells increased sensitivity to JQ1. In xenografts models of PTEN-positive and PTEN-knock-in endometrial cancer, JQ1 significantly upregulated the expression of PTEN, blocked the PI3K/AKT signaling pathway and suppressed tumor growth. These effects were attenuated in PTEN-negative and PTEN-knockdown xenograft models. Thus, JQ1 resistance appears to be highly associated with the status of PTEN expression in endometrial cancer. Our findings suggest that targeting BRD4 using JQ1 might serve as a novel therapeutic strategy in PTEN-positive endometrial cancers
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