Older Adults Grow Just As Many New Brain Cells As Young People

Summary: A new study reveals older adults can generate just as many new hippocampal neurons from progentior cells as young people. The findings confirm neurogenesis does occur in older individuals.

Source: Cell Press.

There has been controversy over whether adult humans grow new neurons, and some research has previously suggested that the adult brain was hard-wired and that adults did not grow new neurons. This study, to appear in the journal Cell Stem Cell on April 5, counters that notion. Lead author Maura Boldrini, associate professor of neurobiology at Columbia University, says the findings may suggest that many senior citizens remain more cognitively and emotionally intact than commonly believed..

“We found that older people have similar ability to make thousands of hippocampal new neurons from progenitor cells as younger people do,” Boldrini says. “We also found equivalent volumes of the hippocampus (a brain structure used for emotion and cognition) across ages. Nevertheless, older individuals had less vascularization and maybe less ability of new neurons to make connections.”

The researchers autopsied hippocampi from 28 previously healthy individuals aged 14-79 who had died suddenly. This is the first time researchers looked at newly formed neurons and the state of blood vessels within the entire human hippocampus soon after death. (The researchers had determined that study subjects were not cognitively impaired and had not suffered from depression or taken antidepressants, which Boldrini and colleagues had previously found could impact the production of new brain cells.)

In rodents and primates, the ability to generate new hippocampal cells declines with age. Waning production of neurons and an overall shrinking of the dentate gyrus, part of the hippocampus thought to help form new episodic memories, was believed to occur in aging humans as well.

The researchers from Columbia University and New York State Psychiatric Institute found that even the oldest brains they studied produced new brain cells. “We found similar numbers of intermediate neural progenitors and thousands of immature neurons,” they wrote. Nevertheless, older individuals form fewer new blood vessels within brain structures and possess a smaller pool of progenitor cells–descendants of stem cells that are more constrained in their capacity to differentiate and self-renew.

hippocampus
The researchers autopsied hippocampi from 28 previously healthy individuals aged 14-79 who had died suddenly. This is the first time researchers looked at newly formed neurons and the state of blood vessels within the entire human hippocampus soon after death. NeuroscienceNews.com image is in the public domain.

Boldrini surmised that reduced cognitive-emotional resilience in old age may be caused by this smaller pool of neural stem cells, the decline in vascularization, and reduced cell-to-cell connectivity within the hippocampus. “It is possible that ongoing hippocampal neurogenesis sustains human-specific cognitive function throughout life and that declines may be linked to compromised cognitive-emotional resilience,” she says.

Boldrini says that future research on the aging brain will continue to explore how neural cell proliferation, maturation, and survival are regulated by hormones, transcription factors, and other inter-cellular pathways.

About this neuroscience research article

Funding: This work was supported by the Stroud Center for Aging Studies at Columbia University, the National Institutes of Health, the American Foundation for Suicide Prevention, the New York Stem Cell Initiative and the Diane Goldberg Foundation.

Source: Joseph Caputo – Cell Press
Publisher: Organized by NeuroscienceNews.com.
Image Source: NeuroscienceNews.com image is in the public domain.
Original Research: Open access research for “Human Hippocampal Neurogenesis Persists throughout Aging” by Maura Boldrini, Camille A. Fulmore, Alexandria N. Tartt, Laika R. Simeon, Ina Pavlova, Verica Poposka, Gorazd B. Rosoklija, Aleksandar Stankov, Victoria Arango, Andrew J. Dwork, René Hen, and J. John Mann in Cell Stem Cell. Published April 5 2018.
doi:10.1016/j.stem.2018.03.015

Cite This NeuroscienceNews.com Article

[cbtabs][cbtab title=”MLA”]Cell Press “Older Adults Grow Just As Many New Brain Cells As Young People.” NeuroscienceNews. NeuroscienceNews, 6 April 2018.
<https://neurosciencenews.com/neurogenesis-aging-8733/>.[/cbtab][cbtab title=”APA”]Cell Press (2018, April 6). Older Adults Grow Just As Many New Brain Cells As Young People. NeuroscienceNews. Retrieved April 6, 2018 from https://neurosciencenews.com/neurogenesis-aging-8733/[/cbtab][cbtab title=”Chicago”]Cell Press “Older Adults Grow Just As Many New Brain Cells As Young People.” https://neurosciencenews.com/neurogenesis-aging-8733/ (accessed April 6, 2018).[/cbtab][/cbtabs]


Abstract

Human Hippocampal Neurogenesis Persists throughout Aging

Highlights
•Pools of quiescent stem cells are smaller in aged human hippocampal dentate gyri
•Proliferating progenitor and immature neuron pools are stable with aging
•Angiogenesis and neuroplasticity decline in older humans
•Granule neurons, glia, and dentate gryus volume are unchanged with aging

Summary
Adult hippocampal neurogenesis declines in aging rodents and primates. Aging humans are thought to exhibit waning neurogenesis and exercise-induced angiogenesis, with a resulting volumetric decrease in the neurogenic hippocampal dentate gyrus (DG) region, although concurrent changes in these parameters are not well studied. Here we assessed whole autopsy hippocampi from healthy human individuals ranging from 14 to 79 years of age. We found similar numbers of intermediate neural progenitors and thousands of immature neurons in the DG, comparable numbers of glia and mature granule neurons, and equivalent DG volume across ages. Nevertheless, older individuals have less angiogenesis and neuroplasticity and a smaller quiescent progenitor pool in anterior-mid DG, with no changes in posterior DG. Thus, healthy older subjects without cognitive impairment, neuropsychiatric disease, or treatment display preserved neurogenesis. It is possible that ongoing hippocampal neurogenesis sustains human-specific cognitive function throughout life and that declines may be linked to compromised cognitive-emotional resilience.

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  1. Body decays and brain slows down not with the passage of time but when the auto renewal process is vitiated. And the auto renewal process is vitiated when brain is not interested (or less interested) in actual functioning, in actual usage, in actual interaction, with possessions, relations, situations, ideas but in seeking stable relief through them or becomes complacent in respect of possessions, relations and so on. It escapes the uneasiness of disturbing the complacency. This escaping conceals the friction (it is uneasiness for the present brain), which is the basis of auto renewal. Becoming aware of this is attunement to the inexhaustible energy, the Original.
    There is renewal every moment. Brain experiences it as friction from moment to moment. The illusion makes one wait for the frictionless state. Friction is experienced as pain, uncertainty, pleasure. To be comfortable with friction (without any idea, explanation) is one’s attunement to supreme relaxation.

  2. You guys have got to tell me that neurogenesis is real for adults..! i need more intelligence! lots of it! i need more memory! i’ve been reading articles telling me that there is no material proof whether neurogenesis in adults exists or not and all research towards that effort is sham because the techniques and technology aren’t good enough. What is going on!? I can’t find anything proving neurogenesis is a fact for adults. A universal fact like 1+1=2 and everybody agrees.

  3. So how do we reverse reduced cognitive-emotional resilience in old age caused by this smaller pool of neural stem cells, decline in vascularization, and reduced cell-to-cell connectivity within the hippocampus?

  4. Actually I think adults grow more new brain cells then juveniles .. I have ZERO craving for Tide pods or shove a condom up my nose. ;)

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