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Elon Musk UPDATE Neuralink 4.0 Chip Destroy Entire BCI Industry!

Elon Musk UPDATE Neuralink 4.0 Chip introduces Neuralink’s next-generation O1 brain chip developed with Samsung.
This video explores the latest progress of the Neuralink 4.0 chip, including movement restoration, speech recovery, Blindsight vision technology, and how Neuralink patients are using brain-computer interfaces today.
We also examine Samsung’s 4nm partnership, the new R1 surgical robot, and competition from Synchron, Paradromics, and China’s NEO system to understand how the Neuralink 4.0 chip could shape the future of the BCI industry.
If you’re interested in Elon Musk, AI, neuroscience, and future medical technology, this breakdown explains why many experts view the Neuralink 4.0 chip as one of the most important developments in brain-computer interfaces.

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Gary Marcus on AI: How do we bridge the mind with the brain?

Gary Marcus is now one of the loudest skeptics of the AI boom. In 2012, almost nobody was listening.

I have the tape.

That year, I sat down with him for Singularity. FM, right after he published a sharp critique of Ray Kurzweil’s theory of mind in The New Yorker. Marcus was already making the argument that would define his career. Intelligence is not just pattern-matching. The mind is a kluge, a messy evolutionary patch job. And scale alone will not get you to real #AI.

More than a decade later, that argument is everywhere. Labs are chasing the hybrid and neurosymbolic approaches he pointed to back then. The field finally caught up to the conversation.

But here is what makes the interview worth revisiting. He also bet big on neuroscience as the road forward, on projects like Blue Brain and Whole Brain Emulation. The breakthroughs came from somewhere else entirely.

So was he the prophet, or just early on some calls and wrong on others? Watch it and decide for yourself.

How a brainless sea blob still ‘feels’ touch and crawls away in seconds without nerves or muscles

For a flat sea creature just a few millimeters across, a gentle poke is instantly recognized as danger. Trichoplax adhaerens—a translucent blob with no head, brain or muscles—scuttles away in seconds when touched. Imagine a flattened multicellular amoeba moving as a single unit: Trichoplax is only ~20 microns thick and a few millimeters wide. It glides on surfaces by beating tens of thousands of cilia on its lower epithelium (the underside), like microscopic oars dragging against the water.

Yet unlike most animals, Trichoplax has no obvious front or back end, no nerves or muscles at all. How can such a simple “crawling carpet” steer or change direction without a brain?

A new study reveals the remarkable flexibility of this pinhead-sized animal. While in most creatures, the orientation of each cilium is fixed early in development and locked to the body’s axes, Trichoplax achieves its swift escape by reorienting its thousands of hairlike cilia.

Targeting enzyme could block cancer spread to brain with fewer side effects

A new study has identified a more precise and effective way to prevent cancer from spreading to the brain. The paper, published in the Proceedings of the National Academy of Sciences, details the development of novel drug candidates that target a key enzyme implicated in the spread of lung, breast, skin and other cancers to the brain. The work builds on a promising new therapeutic strategy first reported by the same group of researchers last year.

The new drug candidates are designed to intercept rogue cancer cells before they depart from primary tumors and ultimately travel to the brain.

Lead author Sheila Singh, based at both King’s College London and McMaster University, says this type of cancer—called metastatic brain cancer—is the most common type of brain tumor in adults and comes with an extremely grim outlook, with 90% of patients dying within one year of diagnosis.

These tiny genetic fragments may be critical for telling a brain when to rest

The altered presence of tiny fragments of neuronal genes, called microexons, causes hyperarousal in zebrafish. This is the main conclusion of an international study led by Pompeu Fabra University (UPF) and the Center for Genomic Regulation (CRG). An abnormal pattern of neural microexon presence leads to a hyperarousal state characterized by heightened neural activity and insomnia, commonly associated with stress but also with neurodevelopmental disorders.

Arousal regulation is highly conserved in evolution. Therefore, this finding could help researchers understand the mechanism underlying some human neurodevelopmental disorders, such as autism and schizophrenia, conditions associated with microexon mutations.

To survive, animals need to be ready to react to external and internal stimuli. This activation of the central nervous system, arousal, is highly conserved throughout the animal kingdom.

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