We would not expect a baby to join a team or participate in social
situations that require sophisticated communication. Yet, most
developmental biologists have assumed that young cells, only recently
born from stem cells and known as "progenitors," are already competent
at inter-communication with other cells.
New research from Carnegie's Allan Spradling and postdoctoral fellow
Ming-Chia Lee shows that infant cells have to go through a developmental
process that involves specific genes before they can take part in the
group interactions that underlie normal cellular development and keep
our tissues functioning smoothly. The existence of a childhood state
where cells cannot communicate fully has potentially important
implications for our understanding of how gene activity on chromosomes
changes both during normal development and in cancerous cells. The work
is published in Genes and Development.
The way that the molecules that package a cell's chromosomes are
organized in order to control gene activity is known as the cell's
"epigenetic state." The epigenetic state is fundamental to understanding
Spradling and Lee's findings. To developmental biologists, changes in
this epigenetic state ultimately explain how the cell's properties are
altered during tissue maturation.
"In short, acquired epigenetic changes in a developing cell are
reminiscent of the learned changes the brain undergoes during
childhood," Spradling explained. "Just as it remains difficult to map
exactly what happens in a child's brain as it learns, it is still very
difficult to accurately measure epigenetic changes during cellular
development. Not enough cells can usually be obtained that are at
precisely the same stage for scientists to map specific molecules at
specific chromosomal locations."
Lee and Spradling took advantage of the unsurpassed genetic tools
available in the fruit fly to overcome these obstacles and provide new
insight into the epigenetics of cellular development.
Using a variety of tools and techniques, they focused on cells in the
fruit fly ovary and were able identify a specific gene called lsd1 that
is needed for ovarian follicle progenitor cells to mature at their
normal rate. The researchers found that the amount of the protein that
is encoded by this gene, Lsd1, which is present in follicle progenitors
decreases as the cells approach differentiation. What's more, the onset
of differentiation could be shifted by changing the levels of Lsd1
protein that are present. They deduced that differentiation ensues when
Lsd1 levels fall below a critical threshold, and that this likely
corresponds to when genes can be stably expressed.
"The timing of differentiation is very important for normal
development," Lee said. "Differentiation onset determines how many times
progenitors divide, and even small perturbations in Lsd1 levels changed
the number of follicle cells that were ultimately produced, which
reduced ovarian function."
Previously, it was thought that the follicle cell progenitors started
to differentiate based on an external signal they received from another
kind of ovarian cells known as germ cells. Lee and Spradling found that
while this germ cell signal was essential, it was already being
regularly sent even before the progenitors responded. Instead, it was
the Lsd1-mediated change in their epigenetic state that timed when
progenitor cells started to respond to the signal and begun
differentiating. Once they become competent, however, differentiating
follicle cells communicate extensively with their neighbors, and
continued to do so throughout their lives.
As is frequently the case in basic biological research, the molecules
and mechanisms studied here are found in most multicellular animals and
hence the researchers conclusions are likely to apply broadly
throughout the animal kingdom, including in humans.
In addition, to the importance of this research for understanding how
animal chromosomes change during normal development, it may also help
clarify alterations in the epigenetic state that take place in some
cancers. A minority of cells in such cancers begin to express high
levels of Lsd1 and to behave like undifferentiated progenitors.
"Studying fruit fly follicle cell differentiation can teach us at a
deeper level what Lsd1 is doing in both normal and cancerous
progenitors," Lee added.
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