image: Baby neurons -- neuroblasts -- migrate from their birthplace to positions in the olfactory bulb of adult mice thanks to two forces, one pulling from the front, the other pushing from behind. A single protein called DOCK7 helps to orchestrate these two steps. This still is from a video showing a neuroblast's migration. In the movie, one can see how the centrosome (yellow dot) advances, followed by the cell body (green oval), pushed from behind. view more
Credit: Van Aelst Lab, CSHL
Cold Spring Harbor, NY - One of the most hopeful discoveries of modern neuroscience is firm proof that the human brain is not static following birth. Rather, it is continually renewing itself, via a process called postnatal neurogenesis - literally, the birth of new neurons. It begins not long after birth and continues into old age. There is some evidence that when people respond to depression treatment, be it a pill or talk therapy, it has something to do with the wiring up of new neurons.
For reasons still not understood, only two parts of the human brain receive replenishments of neurons postnatally. One is a section of a tiny seahorse-shaped structure called the hippocampus, central in memory and learning. The other is the olfactory bulb, located in a small patch of tissue inside the nose, which receives signals from the environment and helps make them intelligible so they can serve as a basis for action - for instance, to recoil from curdled milk or veer from a stinking skunk.
This week in the Journal of Cell Biology, Professor Linda Van Aelst and colleagues at Cold Spring Harbor Laboratory (CSHL) describe for the first time (in mice) how baby neurons - precursors called neuroblasts, generated from a permanent pocket of stem cells in a brain area called the V-SVZ - make an incredible journey from their place of birth through a special tunnel called the RMS to their target destination in the olfactory bulb. They travel as far as 8 mm, "a huge distance, when you consider how tiny the mouse brain is," Van Aelst says.
The journey is made possible by two forces, one pulling from the front, the other pushing from behind. A single protein called DOCK7 helps to orchestrate these two steps. Ahead of the newborn neuron's soma, or cell body, is a threadlike projection called a process. It stretches forward through the tunnel, guided by various signals. At the same time, the cell body, lagging behind, is powered forward by the activation of tiny molecular motors that push it from the rear. Multiple cells migrate together, one virtually on top of another, somewhat in the manner of a group of tiny worms inching forward by morphing the shape of their bodies.
The Takeaway: Neuroscientists have clarified the mechanism used by newly born neurons in mice to migrate to very specific areas in the olfactory bulb. The bulb must be replenished periodically through life to work properly. Knowing how the replenishment works is part of a much broader effort that aims to enhance natural neurogenesis to repair damaged tissue or treat brain disorders.
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Citation: Nakamuta S et al, "Dual role for DOCK7 in tangential migration of interneuron precursors in the postnatal forebrain" appears in Journal of Cell Biology the week of October 31, 2017
Funding: National Institutes of Health; Uehara Memorial Foundation
About Cold Spring Harbor Laboratory
Founded in 1890, Cold Spring Harbor Laboratory has shaped contemporary biomedical research and education with programs in cancer, neuroscience, plant biology and quantitative biology. Home to eight Nobel Prize winners, the private, not-for-profit Laboratory employs 1,100 people including 600 scientists, students and technicians. The Meetings & Courses Program hosts more than 12,000 scientists from around the world each year on its campuses in Long Island and in Suzhou, China. The Laboratory's education arm also includes an academic publishing house, a graduate school and programs for middle and high school students and teachers. For more information, visit http://www.cshl.edu
Journal
Journal of Cell Biology