this post was submitted on 21 Nov 2024
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In this study, the scientists simulated the process of spaced learning by examining two types of non-brain human cells — one from nerve tissue and one from kidney tissue — in a laboratory setting.

These cells were exposed to varying patterns of chemical signals, akin to the exposure of brain cells to neurotransmitter patterns when we learn new information.

The intriguing part? These non-brain cells also switched on a “memory gene” – the same gene that brain cells activate when they detect information patterns and reorganize their connections to form memories.

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[–] Septimaeus@infosec.pub 18 points 3 days ago* (last edited 3 days ago) (1 children)

Yes, insofar as many reflexive actions, enervation and fiber recruitment thresholds respond to training, such that they “remember“ actions you have performed many times before. There are many clusters of nerves throughout the body called ganglia that are responsible for low-latency control of various functions that would entail too much delay when controlled entirely by the brain.

Generally, the minimum input-process-activation turnaround time of the brain is about 4 hz (240-250 ms) which is too slow for many applications of motor function. But the “co-processing” allowed by the extended nervous system enables the body to, with practice, execute far more rapid and complex action sequences in response to local stimuli. Some actions can be triggered and completed before a signal even makes it to the brain.

[–] homesweethomeMrL@lemmy.world 8 points 3 days ago

Generally, the minimum input-process-activation turnaround time of the brain is about 4 hz (240-250 ms) which is too slow for many motor functions. But the “co-processing” allowed by the extended nervous system enables the body to, with practice, execute far more rapid and complex action sequences in response to local stimuli. Some actions can even be triggered and completed before a signal makes it to the brain.

Thank you. For some reason it makes me happy to know that.