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Malicious extensions in Chrome Web store steal user credentials

Two Chrome extensions in the Web Store named ‘Phantom Shuttle’ are posing as plugins for a proxy service to hijack user traffic and steal sensitive data.

Both extensions are still present in Chrome’s official marketplace at the time of writing and have been active since at least 2017, according to a report from researchers at the Socket supply-chain security platform.

Phantom Shuttle’s target audience is users in China, including foreign trade workers who need to test connectivity from various locations in the country.

Alzheimer’s Paper Retracted; Lipoic Acid and MS; Botched Autism Drug Rollout

Science Signaling retracted a 2017 paper that linked a specific amyloid form (amyloid-beta 56) to tau pathology after an investigation into allegations of data manipulation. Author Sylvain Lesné, PhD, who resigned from the University of Minnesota earlier this year, objected to the retraction.

Older adults who were awake more during the night performed worse on cognitive tests no matter how long they slept, data from the Einstein Aging Study showed. (Sleep Health)

Human herpesvirus 7 could be a contributing factor in multiple sclerosis (MS) etiology, a case-control study in Sweden suggested. (Brain Communications)


— News and commentary from the world of neurology and neuroscience.

Professor of Medicine Says Death Appears to Be Reversible

A near-death experience expert insists that one’s heart stopping doesn’t have to be the end, with current medical interventions that can help patients cheat death.

In an interview with The Telegraph, associate professor of medicine at New York University’s Langone Medical Center Sam Parnia insisted that by and large, the medical industry is still very behind on the concepts of death and dying.

According to Parnia, studies from the last five years — including some undertaken by his own eponymous lab at NYU — have suggested that our brains remain “salvageable for not only hours, but possibly days” after death.

Back from the brink: programmed cell revival for regeneration

Yay:3 death can be reversed at a cellular level and then regenerate it back to health.


Therefore, in this issue of The EMBO Journal, Dhar et al sought to improve our understanding of the key molecular mechanisms that regulate the reversal of cell death and apply this knowledge to tissue repair (Dhar et al, 2025). In their study, the authors used a sublethal dose of the lysosomotropic agent L-Leucyl-L-leucine methyl ester (LLOMe) to induce apoptotic cell death (Johansson et al, 2010) in mouse embryonic fibroblasts (MEFs) and characterize the cell revival process. At the initial stage following LLOMe treatment, cells detach from the growth surface and display an apoptotic phenotype, suggesting they are undergoing cell death. However, at later stages, most of the floating cells reattach and regain their typical morphology, with a reduction in the activation of cell death molecules (Fig. 1A). These results indicate that cells can recover from the brink of cell death in response to LLOMe. This phenomenon occurs in multiple non-immune cell types, including primary MEFs and cardiac fibroblasts, as well as several cell lines from hamsters, mice, and humans (Dhar et al, 2025).

At the organellar level, shortly after treatment with LLOMe, microtubules, mitochondria, Golgi, and the endoplasmic reticulum are fragmented; however, these structures progressively recover within 2–3 h and return to near-normal morphology by 16 h post-treatment. Additionally, reviving cells display dramatic changes in endosomes, autophagosomes, and lysosomes, including the formation of abnormally large EEA1-positive early endosomes, LC3-positive autophagosomes, and Rab7/lysotracker-positive acidic vacuoles resembling multivesicular bodies. These large acidic compartments are enzymatically active and frequently surrounded by mitochondrial networks during revival, suggesting a role for metabolic support in driving the recovery.

Advancing Computers to Think Like Humans: Neuromorphic Meshing Explained

#neuromorphic #computing #futuretech


By Chuck Brooks, Skytop Contributor / December 3, 2025

Chuck Brooks serves as President and Consultant of Brooks Consulting International. Chuck also serves as an Adjunct Professor at Georgetown University in the Cyber Risk Management Program, where he teaches graduate courses on risk management, homeland security, and cybersecurity.

Chuck has received numerous global accolades for his work and promotion of cybersecurity. Recently, he was named the top cybersecurity expert to follow on social media, and also as one top cybersecurity leaders for 2024. He has also been named “Cybersecurity Person of the Year” by Cyber Express, Cybersecurity Marketer of the Year, and a “Top 5 Tech Person to Follow” by LinkedIn” where he has 120,000 followers on his profile.

As a thought leader, blogger, and event speaker, he has briefed the G20 on energy cybersecurity, The US Embassy to the Holy See, and the Vatican on global cybersecurity cooperation. He has served on two National Academy of Science Advisory groups, including one on digitalizing the USAF, and another on securing BioTech. He has also addressed USTRANSCOM on cybersecurity and serves on an industry/government Working group for DHS CISA focused on security space systems.

The Incredible Science of Bioprinting

Dive into the remarkable world of bioprinting in this comprehensive video. We’ll be exploring the core concepts of bioprinting — a pioneering technique that uses biological materials to create structures that mimic natural tissues, organs, and even cells. Understand the sophisticated science behind this process, and learn how bio-inks are formulated and layered to build live cells. We’ll also embark on a historical journey, tracing the origins and evolution of bioprinting, and how it is reshaping modern medicine. From overcoming organ shortages to paving the way for personalized treatments, bioprinting is revolutionizing healthcare. Join us as we unpack this fascinating technology and its promising future.

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Tiny Molecule Made by Gut Bacteria Could Cut Type 2 Diabetes Risk

A compound produced by gut bacteria could play a vital role in managing and preventing type 2 diabetes, according to a study led by researchers from Imperial College London (ICL).

The small molecule, called trimethylamine (TMA), is a major type of bacterial metabolite – a class of chemicals produced naturally through processes of transforming nutrients into energy and building blocks.

Scientists have now found evidence in human cell models and lab mice that TMA could protect the body from some of the damage triggered by a high-fat diet. Specifically, it has the effect of dampening down inflammation and improving insulin response, both of which reduce the risk of type 2 diabetes.

Anything-goes “anyons” may be at the root of surprising quantum experiments

In the past year, two separate experiments in two different materials captured the same confounding scenario: the coexistence of superconductivity and magnetism. Scientists had assumed that these two quantum states are mutually exclusive; the presence of one should inherently destroy the other.

Now, theoretical physicists at MIT have an explanation for how this Jekyll-and-Hyde duality could emerge. In a paper appearing today in the Proceedings of the National Academy of Sciences, the team proposes that under certain conditions, a magnetic material’s electrons could splinter into fractions of themselves to form quasiparticles known as “anyons.” In certain fractions, the quasiparticles should flow together without friction, similar to how regular electrons can pair up to flow in conventional superconductors.

If the team’s scenario is correct, it would introduce an entirely new form of superconductivity — one that persists in the presence of magnetism and involves a supercurrent of exotic anyons rather than everyday electrons.

Engineered dendritic cells boost cancer immunotherapy

EPFL researchers have successfully engineered cells of the immune system to more effectively recognize cancer cells. The work, covered in two papers, turns the previously lab-based method into a full-blown immunotherapy strategy.

Cancer immunotherapy is a strategy that turns the patient’s own immune cells into a “search-and-destroy” force that attacks the tumor’s cells. The “search” immune cells are the dendritic cells, which collect and present identifying parts of the cancer cells (antigens) to the “destroy” part (T cells), the immune system’s killer cells.

The problem is that many tumors “learn” how to evade detection by the patient’s dendritic cells. Clinicians address this by collecting dendritic cells from the patient’s blood, loading them in the laboratory with tumor material—antigens that train dendritic cells to better identify the tumor—and then injecting them back into the patient.

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