Study Finds Precious Stem Cells Are Assigned ‘Bodyguard’ Cells
Hiding
deep inside our bone marrow — the flexible tissue found in the interior
of bones — are special cells. They wait patiently for the hour of need,
at which point these blood forming stem cells can proliferate and
differentiate into billions of mature blood cells to help the body cope
with infection, for example, or they can turn into extra red blood cells
for low oxygen levels at high altitudes.
Even in emergencies, however, the body sticks to a
long-term plan: It maintains a reserve of undifferentiated stem cells,
meaning cells that have not yet expressed signs of their future specific
type, for eventual needs and crises.
A research team headed by Prof. Tsvee Lapidot of Israel’s Weizmann Institute’s
immunology Department recently discovered a new type of bodyguard that
protects stem cells from over-differentiation. In a paper that appeared
in Nature Immunology, they revealed how this rare, previously unknown
sub-group of activated immune cells keeps the stem cells in the bone
marrow “forever young.”
Blood forming stem cells live in comfort in the bone
marrow, surrounded by an entourage of support cells that cater to their
needs and direct their development – the mesenchymal cells. But the
research team, which included postdoctoral fellow Dr. Aya Ludin, Prof.
Steffen Jung of the Immunology Department and his group, and Ziv Porat
of the Biological Services Unit, discovered another type of support cell
for the stem cells. These are an offshoot of the macrophage family,
literally the “big eaters” of the immune system that are important, for
instance, for bacterial clearance.
The team found, however, that a rare sub-population of the
bone-marrow macrophages has another role to play. Each of these rare
macrophages can take a stem cell under its wing and prevent its
differentiation.
Keeping useful cells alive during chemotherapy
Probing more deeply, the researchers revealed, in precise
detail, how these macrophages guard the stem cells. They secrete
substances called prostaglandins, which are absorbed by the stem cells.
In a chain of biochemical events, these substances delay differentiation
and preserve the youthful state of the stem cells. In addition, the
prostaglandins work on the neighboring mesenchymal cells, activating the
secretion of a delaying substance in them and increasing the production
of receptors for this substance on the stem cells, themselves.
This activity, says Lapidot, may help the non-dividing stem
cells survive chemotherapy – a known phenomenon. Macrophages also live
through the treatment, and they respond by increasing their
prostaglandin output, thus heightening their vigilance in protecting the
stem cells.
The bodyguard macrophages also increase their activity in
times of infection. While other members of the macrophage family are
recruited to fight the pathogens, their cousins in the bone marrow are
hard at work ensuring that a pool of stem cells will resist the urge to
differentiate.
In previous work in Lapidot’s lab, it was discovered that
prostaglandin treatments can improve the number and quality of stem
cells. This insight is currently being tested by doctors in clinical
transplantation trials for the use of stem cells from umbilical cord
blood to treat adult leukemia patients. These trials are showing that
prior treatment with prostaglandins improves migration and repopulation
potential, enabling the small quantities of cord blood stem cells to
better cure the patients.
“The present study hints at the possibility of further
increasing the support for bone marrow stem cells by exploring this
intriguing connection between the immune cells and stem cells,” says
Lapidot. “An understanding of the mechanisms at work in these cells
might improve the success of stem cell transplantation, especially that
of umbilical blood.”
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