IMMUNE SYSTEM OF NEW BORN BABIES STRONGER THAN PREVIOUSLY THOUGHT
Contrary to what was
previously thought, newborn immune T cells may have the ability to trigger an
inflammatory response to bacteria, according to a new study led by King's
College London. Although their immune system works very differently to that of
adults, babies may still be able to mount a strong immune defense, finds the
study published in the journal Nature
Medicine.
Our immune system is
made up of several different types of immune cells, including neutrophils which
play an important role in the frontline defense against infection, and
lymphocytes: B cells which produce antibodies, and T cells that target cells
infected with viruses and microbes.
Up to now, it was
generally believed that babies have an immature immune system that doesn't
trigger the same inflammatory response normally seen in adults. Although babies
need to protect themselves from the harmful pathogens they are exposed to from
birth, it was thought that their T cells were suppressed to some extent to
prevent inflammatory damage to the developing child. Sceptical of this notion,
the King's-led study set out to characterize the properties of T cells,
examining very small samples of blood in twenty-eight highly premature babies,
as they developed over the first few weeks of life.
The team discovered
that whilst T cells in newborn babies are largely different to those in adults,
it is not because they are immunosuppressed; rather, they manufacture a potent
anti-bacterial molecule known as IL8 that has not previously been considered a
major product of T cells, and that activates neutrophils to attack the body's
foreign invaders.
Dr Deena GibbonsDeena
Gibbons, lead author in the Department of Immunobiology at King's College
London, says: "We found that babies have an in-built anti-bacterial
defense mechanism that works differently to adults, but nevertheless may be
effective in protecting them. This may also be a mechanism by which the baby protects
itself in the womb from infections of the mother. The next stage of our work
will be to better understand the pathways that result in the immune cells of
newborns being so different to those in adults."
This T cell activity
could become a target for future treatments aimed at boosting the immune system
of neonates in intensive care, where infection is a major risk for morbidity
and mortality. Premature babies are also at serious risk of developing
inflammatory diseases such as necrotising enterocolitis (NEC), where severe
inflammation destroys tissues in the gut. NEC is the most common
gastrointestinal surgical emergency in preterm babies, with mortality rates of
around 15 to 30 per cent in the UK.
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