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Diseases and Conditions

“Breaking Isolation: How Addressing Hearing Loss Can Preserve Social Connections Among the Elderly”

Providing hearing aids and advice on their use may preserve social connections that often wane as we age, a new study shows. Its authors say that this approach could help ease the loneliness epidemic that older Americans face.

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Breaking Isolation: How Addressing Hearing Loss Can Preserve Social Connections Among the Elderly

A recent study has shown that providing hearing aids and advice on their use may preserve social connections among older Americans. The researchers found that those who received treatment for hearing loss retained one additional social connection on average over a three-year period compared to those who did not receive any hearing therapies.

The study, led by researchers at NYU Langone Health as part of the ACHIEVE clinical trial, revealed that those given hearing aids had more diverse relationships and maintained deeper bonds than those who were not treated for hearing loss. The findings add to evidence that helping aging patients hear better can enrich their social lives and boost their mental and physical well-being.

Experts have linked both loneliness and hearing loss to depression, heart disease, and early death, among other concerns. A 2023 report on the ACHIEVE trial showed that hearing interventions may slow cognitive decline among those at highest risk for dementia.

The research team collected data about older adults with untreated hearing loss across four sites in Maryland, North Carolina, Minnesota, and Mississippi. The study is among the largest to date to explore if hearing care can help prevent weakening of social networks, having included nearly 1,000 men and women ages 70 through 84.

Half of the participants received hearing aids, counseling sessions, and personalized instruction with an audiologist, while the other half received instruction about exercise, strategies for communicating with healthcare providers, and further resources for healthy aging. To measure social isolation, the researchers assessed how regularly participants spent time with others, the size and variety of their social networks, and the depth of their connections.

Among the findings, the study revealed that before treatment, participants in both groups reported feeling equally lonely. Three years after the intervention took place, loneliness scores slightly improved among those who had received hearing care, while scores slightly worsened among those who did not.

Hearing aids and related audiology appointments cost an average of $4,700, which is usually paid out of pocket, notes Coresh, the founding director of the Optimal Aging Institute. The authors plan to continue following the participants for another three years and to repeat the study with a more diverse group of people.

In conclusion, addressing hearing loss may be a crucial step in preserving social connections among older Americans. By providing hearing aids and related care, we can help alleviate loneliness, improve mental and physical well-being, and potentially slow cognitive decline. As the nation’s social isolation epidemic continues to grow, it is essential that we prioritize hearing health and incorporate hearing aid coverage into Medicare as a means of addressing this critical issue.

Diseases and Conditions

Unraveling the Mysteries of Cohesin: A Protein That Forms Loops in the Human Genome

Cohesin is a protein that forms a ring-shaped complex which wraps and alters the DNA molecule shape. It moves through the DNA and creates specific loops in the genetic material which determine the architecture of the genome and gene expression. Some mutations in the genes of the cohesion complex are responsible for rare diseases (cohesinopathies), such as the Cornelia de Lange syndrome (SCdL) or Roberts syndrome, which affect several organs and cause malformations during development.

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Cohesin, a protein complex that forms loops in the human genome, plays a crucial role in determining the architecture of our genetic material and regulating gene expression. However, its function and behavior have remained somewhat mysterious until now.

Researcher Professor Eva Estébanez-Perpiñá from the University of Barcelona, along with her team and international collaborators, has made significant strides in understanding how cohesin works. Their study, published in Nucleic Acids Research, sheds light on the protein’s interaction with chromatin structure and its role in altering gene expression.

Cohesin consists of four subunits: SMC1, SMC3, SCC1/RAD21, and STAG (also known as SA or SCC2). Previous studies had identified 25 proteins that regulate these subunits and their biological function. Estébanez-Perpiñá’s team has now discovered how the NIPBL protein interacts with both MAU2 and the glucocorticoid receptor (GR), a transcription factor essential for cellular functions.

This ternary complex, comprising NIPBL, MAU2, and GR, modulates transcription by facilitating the interaction of GR with these two proteins. When GR interacts with NIPBL and MAU2, it alters chromatin structure and affects gene expression. This discovery has significant implications for understanding Cornelia de Lange syndrome, a rare disease caused by mutations in genes involved in cohesin formation.

The researchers used advanced microscopic techniques to visualize real-time molecular complexes binding to chromatin, as well as biochemical and biophysical methods to analyze the complex from different structural and cellular perspectives.

Their findings not only improve our comprehension of cohesin’s role but also highlight its potential involvement in other diseases, such as asthma and autoimmune pathologies. As research continues, scientists will likely uncover more about this enigmatic protein and its intricate relationships with chromatin structure and gene expression.

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Diseases and Conditions

Unlocking Affordable Clean Energy: A New Method for Discovering Durable Catalysts

Scientists have developed a data-driven method to accelerate the discovery of affordable, stable catalysts for clean hydrogen production. Using a digital platform called DigCat, they identified a low-cost metal oxide that performs both OER and HER in acidic conditions and remains stable over time.

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The quest for clean energy has taken a significant leap forward with the development of a new method to accelerate the discovery of affordable, stable materials that support hydrogen production. A research team has designed a “closed-loop” framework that brings together several stages of catalyst development, including data analysis, testing, and lab experiments, all connected through a digital system for continuous learning and improvement.

“At the core of our work is a data-driven platform called DigCat,” explains Hao Li, a professor at Tohoku University’s Advanced Institute for Materials Research (WPI-AIMR). “It helps us efficiently explore a wide range of materials by predicting how their surfaces behave during water splitting, which is often the key to their effectiveness.”

Using this approach, the researchers identified RbSbWO₆ as a promising catalyst that showed strong performance in both oxygen evolution reaction (OER) and hydrogen evolution reaction (HER) in acidic conditions. Notably, the material remained structurally stable even after extended use, a critical requirement for practical applications.

The team’s framework can be adapted to other important chemical reactions, such as converting carbon dioxide into useful fuels or producing ammonia from nitrogen. These reactions are central to sustainable energy and environmental technologies.

The next phase of the research involves expanding the surface-state database and applying the method to other material systems. “By learning more about how surfaces behave during reactions, we can uncover hidden potential in materials that were previously overlooked,” says Li. The team hopes that this strategy will accelerate progress toward affordable, efficient solutions for the global energy transition.

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Biology

Unraveling Microtubule Mysteries: Scientists Crack Code on Cellular Scaffolding Secrets

Scientists found out how naturally unstable filaments decide whether to grow or to shorten.

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A groundbreaking study has shed new light on the fundamental mechanisms governing microtubule growth within cells. Researchers from Queen Mary University of London and the University of Dundee have made a significant breakthrough by discovering that the ability of tubulin proteins at microtubule ends to connect with each other sideways determines whether a microtubule elongates or shortens.

Microtubules are crucial protein structures that form the internal skeleton of cells, providing structural support and generating dynamic forces that push and pull. These tiny filaments constantly assemble and disassemble by adding or removing tubulin building blocks at their ends. However, the precise rules dictating whether a microtubule grows or shrinks have long remained a mystery due to the complexity and miniature size of their ends.

The collaborative research team has cracked part of this code using advanced computer simulations coupled with innovative imaging techniques. This interdisciplinary approach has allowed them to address this complex biological question from a fresh perspective, bridging physics and biology.

Dr. Vladimir Volkov, co-lead author from Queen Mary University of London, explained the significance of their findings: “Understanding how microtubules grow and shorten is very important – this mechanism underlies division and motility of all our cells. Our results will inform future biomedical research, particularly in areas related to cell growth and cancer.”

Dr. Maxim Igaev, co-lead author from the University of Dundee, highlighted the power of their interdisciplinary approach: “Bridging physics and biology has allowed us to address this complex biological question from a fresh perspective. This synergy not only enriches both fields but also paves the way for discoveries that neither discipline could achieve in isolation.”

This exciting research deepens our understanding of fundamental cellular processes and opens potential new avenues for biomedical research, particularly in areas concerning cell proliferation and the development of treatments for diseases like cancer.

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