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How stimulating the vagus nerve could protect the brain from Alzheimer’s disease

Developing tau tangles doesn’t mean a person has Alzheimer’s disease – in fact, it happens to nearly everyone to varying degrees. But because these changes start in the locus coeruleus, some brain researchers – myself included – see this area as a canary in the coal mine for developing Alzheimer’s disease.

We are exploring whether stopping or slowing down tau tangles in this brain region, or otherwise maintaining its health, may be a way to interrupt how the disease ultimately unfolds and to prevent other aspects of cognitive aging.

Emerging research from my lab and others is investigating the idea that a therapy called vagus nerve stimulation, which is already widely used for other health conditions, could be one way of keeping the locus coeruleus functioning properly.

Effects of Exercise and Intensive Vascular Risk Reduction on Cognitive Function in Older Adults: A Randomized Clinical Trial

In this multicenter randomized clinical trial, 24 months of moderate to vigorous aerobic exercise, intensive pharmacological reduction of blood pressure and serum LDL cholesterol, or the combination of these interventions did not significantly improve global cognitive function compared to usual care in older adults with hypertension and either family history of dementia or subjective cognitive decline.

Exercise and intensive vascular risk reduction each improved cardiovascular parameters, but no group differences were observed for changes in the Preclinical Alzheimer Cognitive Composite or NIH Toolbox Cognition Battery scores.


Question Can exercise, intensive pharmacological reduction of blood pressure (BP) and serum low-density lipoprotein cholesterol (LDL-C), or the combination of these interventions improve cognitive function in older adults with family history of dementia and/or self-reported subjective cognitive decline?

Findings In this randomized clinical trial of 513 participants, moderate to vigorous aerobic exercise training, intensive pharmacological lowering of BP and serum LDL-C, or both did not result in statistically significant differences in improvements in global cognitive function over 24 months.

Meaning The findings do not provide evidence in support of exercise, intensive reduction of BP and serum LDL-C, or both for improving cognitive function in older adults with family history of dementia and/or self-reported subjective cognitive decline.

A new era in childhood obesity

Childhood obesity!

Obesity associated with the melanocortin system can be diagnosed in childhood, including both monogenic and syndromic forms.

Genetic obesity is characterized by early onset and extreme hyperphagia, although there is no precise definition for these features.

Numerous polymalformative syndromes include obesity among their main phenotypic traits. Among these are ciliopathies, in which alterations in the neuronal ciliary system can disrupt hypothalamic proopiomelanocortin neuron signaling, helping to explain the hyperphagia and obesity frequently observed in some of these disorders.

Pharmacological treatment of patients with impairment of the leptin– melanocortin pathway can be classified into specific and nonspecific treatments.

The use of these therapies is expanding to new indications, and additional treatments are under clinical investigation for both monogenic and polygenic obesity sciencenewshighlights ScienceMission https://sciencemission.com/childhood-obesity-19506


New genetic toolkit enables genome-wide analysis

Researchers at Cornell University have developed a powerful new genetic toolkit that allows scientists to study how genes function at the level of individual cells, an advance that could accelerate discoveries in development, neuroscience and disease.

The system builds on MAGIC (Mosaic Analysis by gRNA-Induced Crossing-over), a method originally created by the labs of Chun Han, associate professor in the Department of Molecular Biology and Genetics in the College of Agriculture and Life Sciences (CALS) and the Weill Institute for Cell and Molecular Biology. MAGIC uses CRISPR gene editing to generate individual mutant cells within otherwise normal tissue, enabling precise comparisons within a living organism.

In the new study, graduate researcher Yifan Shen expanded the approach into a genome-wide toolkit for Drosophila melanogaster, creating resources that work across all chromosomes and allow researchers to study genes that were previously difficult, or impossible, to analyze at single-cell resolution.

Tomatidine is a senotherapeutic compound that improves cognitive function and reduces cellular senescence in aged mice

Cellular senescence drives aging and age-related dysfunction across multiple tissues, including the brain. Through a high-content, senescent cell-based phenotypic screen of a small panel of natural products, we identified tomatidine, an aglycone of tomatine found in tomatoes, as a previously unrecognized senotherapeutic agent. In senescent human brain microvascular endothelial cells and fibroblasts, tomatidine selectively suppressed SASP expression without affecting p16Ink4a or p21Cip1 levels consistent with a senomorphic effect. In aged mice, tomatidine reduced frailty and improved motor coordination and cognitive performance. These functional benefits were accompanied by reduced senescence markers (p16 Ink4a, p21 Cip1, and telomere-associated DNA damage foci) in liver, skin, and hippocampal neurons, along with decreased neuroinflammation and microglial activation. Tomatidine also diminished brain endothelial cell senescence while enhancing tight junction protein expression, suggesting preserved blood–brain barrier integrity. Together, these findings identify tomatidine as a promising senescence-targeting compound with beneficial effects in aged mice and support its further evaluation in mechanistic and translational studies.

Brain scans reveal how a woman voluntarily enters a psychedelic-like trance without drugs

A groundbreaking fMRI study has mapped the exact neural shifts of a self-induced visionary state. Researchers discovered that a woman capable of voluntary trance actively disconnects her sensory networks while boosting internal cognitive control.

New ‘Unifying Theory’ May Explain How Alzheimer’s Emerges in The Brain

The origins of Alzheimer’s remain contentious, but a new study suggests the disease may emerge as two key proteins compete inside brain cells.

Alzheimer’s disease, the most common form of dementia, has long been associated with the build-up of two proteins in the brain: amyloid-beta and tau.

This new study ties those two together, offering a “unifying theory” that, according to the team of chemists proposing it, resolves some conflicting ideas about Alzheimer’s.

How the human brain builds our sense of time

How does Jannik Sinner manage to hit the ball at exactly the right moment, with remarkable precision? And how do we, in everyday life, perceive the duration of events around us? The answer lies in how the brain constructs the perception of time, as shown by research published in PLOS Biology by Valeria Centanino, Gianfranco Fortunato, and Domenica Bueti. Starting from what we see—such as an approaching ball—temporal information is processed by the brain through progressively more complex stages: from the occipital visual cortex, to parietal and premotor areas, and finally to frontal regions.

Using high-field functional magnetic resonance imaging (fMRI) and measuring time perception in healthy volunteers, the researchers shed light on what happens in the brain when we estimate the duration of a visual stimulus. “Our results show that time perception is not a unitary process, but the outcome of multiple processing stages distributed across the cerebral cortex,” the authors explain. “Each stage contributes differently, from encoding physical duration to constructing the subjective experience of time.”

In an initial stage, occipital visual areas encode duration through gradual (monotonic) neural responses: the longer the stimulus, the stronger the neural response. This information is then transformed in parietal and premotor regions into selective (unimodal) representations, where distinct neural populations respond preferentially to specific durations, enabling the “readout” of time. Finally, higher-order regions, including the frontal cortex and anterior insula, are involved in the subjective categorization of duration, shaping how time is perceived.

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