Neonatal SEPSIS Clinical Trial
Official title:
Measurement of Neutrophil Membrane CD64 as an Early Indication of Neonatal Infection and Necrotising Enterocolitis (NEC).
Bacterial infections are a major cause of death in newborn infants. And are linked to
complications including: sepsis (an over exaggerated immune response to infection) and
necrotising enterocolitis (a potentially fatal inflammatory bowel disease).
Detecting infections at an early stage is difficult in newborns as the signs and symptoms
can be non-specific, the most commonly used lab test is to culture a sample of blood, urine
or spinal fluid to try and grow and identify any bacteria that is present; however these
tests take 24-48 hours to give results, and this means that neonates who present with signs
of infection are prescribed broad spectrum antibiotics whilst results are obtained.
The lack of a test that can detect infection at an early stage and give rapid results is one
of the major problems in the diagnosis and management of infection in newborns. This study
will investigate neutrophils, which are white blood cells that are important in fighting
infection. When neutrophils detect and infection they become activated, and produce a
protein called CD64 (a cell marker) on their surface, and it is this protein that we want to
measure. Neutrophils produce the CD64 protein within 1 hour of first detecting an infection,
so we could hopefully detect and treat infections much quicker.
The hypothesis this study will test are:
1. Does neutrophil membrane CD64 measurement provide a highly sensitive and specific
marker of infection in neonates AND:
2. Does neutrophil membrane CD64 measurement provide a highly sensitive and specific
marker of NEC in neonates
New born infants (neonates) and particularly premature infants are more at risk of
developing bacterial infections due to a number of different factors including immature
immune systems, and because they are more likely to need invasive procedures such as chest
drains that increase the potential for infection.
The signs of infection in babies can be non-specific and difficult to diagnose. Undetected
infections which are not treated can quickly lead to sepsis, which is an over-exaggerated
response by the immune system which can spread throughout the whole body and attack 'self'
tissue leading to organ failure and death. It is therefore vital that infection in neonates
can be diagnosed quickly in order to administer the best treatment.
The current 'gold standard' laboratory test for detecting infection is to culture samples of
blood, urine or spinal fluid, which allows any bacteria present to be grown in the lab and
identified. However this test can take 24-48 hours to give results, and due to the
devastating consequences of not treating an infection in neonates it is now common practice
to prescribe broad spectrum antibiotics to any neonate who presents with signs of infection
and await test results.
This study will look at what happens to the white blood cells that make up part of the
immune defence against infection when they encounter an infection. One type of white blood
cell that is particularly important in fighting bacterial infections is called the
neutrophil, and when it detects an infection, it becomes activated in order to fight it;
during this activation process it expresses a protein marker called CD64 on its surface. The
CD64 protein is expressed within hours of the onset of bacterial infections, so measuring
the CD64 marker could provide much faster results than laboratory tests that are currently
available.
If we could detect infections in neonates more rapidly then non-infected neonates (with
negative CD64 result) could have antibiotic treatment stopped. This is beneficial as it
reduces unnecessary treatment therefore reducing hospital stays and cost. It also reduces
the use of antibiotics, the overuse of which can promote the development of antibiotic
resistant strains of bacteria, which can colonize entire wards. It would also mean that
infected neonates could receive more appropriate care, for example more specific
antibiotics.
Necrotising enterocolitis (NEC) is another common condition that affects newborn infants.
Exactly how and why some infants develop NEC is still unclear, but is thought to be due to a
number of different factors including bacterial infection. Advanced NEC is characterised by
bowel necrosis, bowel perforation, sepsis and death and remains one of the major causes of
morbidity and death in neonates, with a mortality rate of 30-50%.
The diagnosis of NEC is currently based on X-ray findings and features such as air in the
abdomen are very diagnostic. Other biochemical and haematological parameters are also used
to support X-ray findings. Because we know that one of the 'triggers' for the initiation of
the disease is a bacterial infection: culturing samples of blood, urine or spinal fluid is
important to try and identify/isolate any infection. However these tests all take time, and
current practice means that any neonate who presents with signs of NEC/infection will be
subjected to gut rest i.e. nil by mouth (in order to prevent any further damage to the gut)
and also be prescribed broad spectrum antibiotics. Patients who have suspected NEC will
often be continued on a treatment/monitoring regime, the length of which will be dictated by
clinical judgment: and this may be unnecessary if there is no sign of
infection/inflammation.
One of the greatest challenges in the management/diagnosis of NEC is the lack of an early,
reliable and consistent marker of 'intestinal inflammation' in peripheral blood. This study
will investigate if the CD64 marker can fill this gap.
The inflammatory process seen in NEC is probably initiated by the presence of bacteria. The
bacteria activate cells of the innate immune system which produce a number of inflammatory
mediators causing inflammation. The CD64 marker is not a 'direct' marker of inflammation,
however the cells that are activated in order to produce inflammation i.e. neutrophils will
be positive for CD64 once activated, therefore if CD64 is not present on the cells: they
have not been activated, which means there is no infection and therefore no inflammation.
If the CD64 marker can rule out infection in neonates with suspected NEC, then it also rules
out any ongoing inflammatory process. Clinicians could use the CD64 assay in conjunction
with X-ray findings in order to stop treatment in non affected neonates and restart feeding
sooner, which has many benefits to the neonate's growth and nutritional development, and
also negates the need for prolonged antibiotic treatment and hospital stays. It also means
that affected neonates could receive more appropriate treatment and monitoring.
Taking serial (repeated) measurements from patients with suspected or confirmed NEC at
various intervals (24 48 hours etc.) and seeing how this compares with the clinical picture,
could possibly be used to monitor the disease progression/severity e.g. could a rapid rise
in the expression of CD64 indicate progression to the advanced stage and need for surgery,
and could a reduced expression of CD64 indicate remission or response to treatment.
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