Gene related to brain damage in preterm infants identified
Duke-NUS Graduate Medical School Singapore News Sep 14, 2017
A gene has been identified by a joint study by researchers at KingÂs College London, Duke-NUS Medical School (Duke-NUS), Inserim and Paris Diderot University that is thought to be associated with the types of brain damage that can be caused by preterm birth.
Premature labour is associated with inflammation in the mother or baby, often due to infection. This can cause damage to the brain that could lead to lifelong conditions such as cerebral palsy, autism or learning or behavioural difficulties in up to 30 per cent of pre-term babies.
Published in the journal Nature Communications, a new study investigated the role of microglial cells, which control the immune response in the brain, in responding to this inflammation. Researchers found a gene, known as DLG4, in these cells that is thought to be involved in controlling the inflammatory process.
DLG4 is found in different forms in all humans but previously was thought only to play a role in the function of the nervous system. This new finding suggests it is also involved in the process of brain damage in some pre-term babies and may open doors for research into more effective treatments of these diseases.
The study, which was a collaboration between KingÂs, Duke-NUS, Inserm and Paris Diderot University used an integrative approach which included mouse models of inflammation and a genomic analysis of over 500 infant brain scans. It identified differences in the way DLG4 was expressed in microglia in both the mouse models and brain scans.
This finding suggests a previously unknown mechanism of brain injury caused by pre-term birth. Whilst the association requires further study to confirm the role of microglia and the DLG4 gene, the result contributes to an existing body of evidence that links the gene with both the immune response and neuropsychiatric diseases such as schizophrenia and autism.
Professor David Edwards, Director of the Centre for the Developing Brain at KingÂs College London said: ÂWe have shown that the DLG4 gene is expressed differently in microglia when a brain has been damaged by inflammation.
Associate Professor Enrico Petretto from Duke-NUS said: ÂGiven the previously acknowledged role of the DLG4 gene in brain diseases such as autism and schizophrenia, our study strengthens the link between the immune response and susceptibility to develop these brain disorders.Â
Professor Pierre Gressens from Inserm-Paris Diderot University and KingÂs College London said: ÂThis study identifies for the first time the microglial expression of DLG4, a gene previously considered as expressed in neurons only and highlights the potential role of microglia in different neurodevelopmental disorders.Â
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Premature labour is associated with inflammation in the mother or baby, often due to infection. This can cause damage to the brain that could lead to lifelong conditions such as cerebral palsy, autism or learning or behavioural difficulties in up to 30 per cent of pre-term babies.
Published in the journal Nature Communications, a new study investigated the role of microglial cells, which control the immune response in the brain, in responding to this inflammation. Researchers found a gene, known as DLG4, in these cells that is thought to be involved in controlling the inflammatory process.
DLG4 is found in different forms in all humans but previously was thought only to play a role in the function of the nervous system. This new finding suggests it is also involved in the process of brain damage in some pre-term babies and may open doors for research into more effective treatments of these diseases.
The study, which was a collaboration between KingÂs, Duke-NUS, Inserm and Paris Diderot University used an integrative approach which included mouse models of inflammation and a genomic analysis of over 500 infant brain scans. It identified differences in the way DLG4 was expressed in microglia in both the mouse models and brain scans.
This finding suggests a previously unknown mechanism of brain injury caused by pre-term birth. Whilst the association requires further study to confirm the role of microglia and the DLG4 gene, the result contributes to an existing body of evidence that links the gene with both the immune response and neuropsychiatric diseases such as schizophrenia and autism.
Professor David Edwards, Director of the Centre for the Developing Brain at KingÂs College London said: ÂWe have shown that the DLG4 gene is expressed differently in microglia when a brain has been damaged by inflammation.
Associate Professor Enrico Petretto from Duke-NUS said: ÂGiven the previously acknowledged role of the DLG4 gene in brain diseases such as autism and schizophrenia, our study strengthens the link between the immune response and susceptibility to develop these brain disorders.Â
Professor Pierre Gressens from Inserm-Paris Diderot University and KingÂs College London said: ÂThis study identifies for the first time the microglial expression of DLG4, a gene previously considered as expressed in neurons only and highlights the potential role of microglia in different neurodevelopmental disorders.Â
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