Weekly reads: brain aging, perinatal stem cell clinics, $1M lab meat fine bill

What happens during brain aging and how can we tell if dementia is coming? Are there particular early hallmarks?

There are an increasing number of medical tests for predicting or detecting dementia. Alzheimer’s disease can often be detected early. But what do patients or their doctors do with such information?

Until recently there weren’t any treatments for dementia. Even a new approved drug for Alzheimer’s disease called Aducanumab comes with risks and not much benefit.

Early prevention is even better than trying to detect and treat unhealthy brain again. For that we need to better understand how brains age, normally and on the way to dementia.

With all of this in mind, let’s start our weekly review with two new papers on brain aging.

brain aging
An artistic vision of brain aging. The  image at right is kind of pessimistic I’d say.

Brain aging and dementia

Plasma proteomic profiles predict future dementia in healthy adults, Nat. Aging. GFAP in blood plasma is a strong predictor of all-cause dementia. This is fascinating but why GFAP? Is it related to glial cells? Inflammation? A few other proteins were also strongly linked to dementia. The reasons aren’t yet clear but this is an exciting area of research.

Transcriptional and epigenetic dysregulation impairs generation of proliferative neural stem and progenitor cells during brain aging, Nat. Aging. A long-standing question is whether the aging human brain can make new neural stem cells that have functional meaning for brain health. Overall evidence supports some degree of proliferation and neurogenesis in the adult human brain. It’s less clear how many cells are generated and what those new cells do.

Thinking more interventionally, if you transplanted large numbers of neural precursors into an unhealthy, aging brain, could that improve brain health and function?

This is going to be a major area of research for decades to come.

Paul-Burger-Pic-300x2041
Stem cells making other cells as usual but also being grown into meat or even a burger. Would you eat lab grown meat? Image Paul Knoepfler.

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1 thought on “Weekly reads: brain aging, perinatal stem cell clinics, $1M lab meat fine bill”

  1. Dear Admin:

    In your diagram of the “burger stem cell”, your stem cell is gone after it divides, which is not the case for tissue stem cells that are being used for these “cultured meat” technologies. The diagram would be more accurate if the stem cell divided with an asymmetric self-renewal division – producing another stem cell and a committed meat progenitor cell – or if you drew two stem cells with one dividing like the one you drew and one dividing to produce another two stem cells.

    Why am I bothering you with this seemingly academic minutiae? Because it is not minutiae for one of the biggest hidden problems faced by the cultured meat industry; and most of the companies in this struggling industry don’t even recognize it or understand it when it is explained to them. ALL of their cultures based on natural tissue stem cells eventually stop expanding (Believe me, this they know and are struggling to address it.) no matter what they do, because in cell culture the inherent asymmetric self-renewal program of tissue stem cells leads to their dilution to non-existence among their amplifying committed progeny cells when cultures are expanded by continuous splitting to make more cultures.

    Even if these companies ever figure out how to solve the high cost of media to make producing cultured meat a profitable business with generally affordable products and how to evade political opposition, they will fail if they do not recognize and address this biological limitation of cell production dependent on natural tissue stem cells.

    Conceptually, there are at least two solutions to the tissue stem cell expansion problem.

    1) Controlled suppression of the asymmetric cell kinetics (SACK) of the tissue stem cells responsible for meat cell production. [My past laboratory originated and published the first demonstration the SACK concept in 2003 before racists kicked me out of MIT in 2007.]

    2) An iPSC approach with an with indefinite expansion of iPSCs (they don’t dilute in their undifferentiated cultures because they lack asymmetric cell kinetics) that can be effectively differentiated on demand into the desired meat cells.

    James @ Asymmetrex®

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