World-first genetic clues point to risk of blindness
The Walter and Eliza Hall Institute of Medical Research News Mar 09, 2017
Australian scientists have discovered the first evidence of genes involved in Macular Telangiectasia type 2 (MacTel), a currently incurable eye disease that can lead to blindness. The teamÂs findings established five key regions  or loci  in the genome most likely to influence a personÂs risk of developing MacTel. The finding will enable researchers to better understand the disease and look for ways to prevent or stop its progression.
The study, published in the journal Nature Genetics, was an international collaboration led by bioinformaticians Professor Melanie Bahlo and Dr Thomas Scerri at MelbourneÂs Walter and Eliza Hall Institute of Medical Research.
MacTel is a rare and complex disease that mainly affects people from the age of 40 onwards. The symptoms begin with patients experiencing a loss of central vision crucial for tasks requiring focus, such as driving or reading.
Professor Bahlo said the study involved detailed genetic analysis of MacTel patients from around the world, including Australia, using genome wide association studies (GWAS).
ÂWe analysed more than six million genetic markers and identified five loci across the genome that had similar patterns in people with the disease, but not in the healthy individuals, Professor Bahlo said.
ÂThese five genetic risk loci are our 'treasure map', telling us where to Âkeep digging in order to discover the specific genes implicated in MacTel, she said.
Professor Bahlo said the team worked with collaborators in London and New York to analyse the genetic data from 476 people with MacTel and 1733 controls people without the disease.
ÂWe were thrilled when our results were corroborated by two further independent validation studies, she said.
The analysis also revealed that people with the MacTel genetic risk loci identified in the study had changes in their metabolism, specifically in their glycine and serine levels.
Professor Bahlo said this meant there could be a significant relationship between the level of glycine and serine in the body, and onset of the disease.
ÂThough the exact link between the disease and glycine and serine is yet to be confirmed, the connection is an exciting clue to help us further explore metabolic abnormalities in people with MacTel, Professor Bahlo said.
Dr Scerri said the teamÂs work highlighted crucial points of interest that, with further investigation, could help researchers find a way to prevent the progression of the disease.
ÂWe are continuing to explore the genetic data to try identify the specific genes involved, and the precise genetic variations that are leading to the disease, Dr Scerri said.
President of the Lowy Medical Research Institute that sponsored the research Professor Martin Friedlander said the work represented a significant advancement in efforts to understand the cause of MacTel.
ÂWe are working towards developing treatments effective in preserving vision in patients with this disease, he said.
Go to Original
The study, published in the journal Nature Genetics, was an international collaboration led by bioinformaticians Professor Melanie Bahlo and Dr Thomas Scerri at MelbourneÂs Walter and Eliza Hall Institute of Medical Research.
MacTel is a rare and complex disease that mainly affects people from the age of 40 onwards. The symptoms begin with patients experiencing a loss of central vision crucial for tasks requiring focus, such as driving or reading.
Professor Bahlo said the study involved detailed genetic analysis of MacTel patients from around the world, including Australia, using genome wide association studies (GWAS).
ÂWe analysed more than six million genetic markers and identified five loci across the genome that had similar patterns in people with the disease, but not in the healthy individuals, Professor Bahlo said.
ÂThese five genetic risk loci are our 'treasure map', telling us where to Âkeep digging in order to discover the specific genes implicated in MacTel, she said.
Professor Bahlo said the team worked with collaborators in London and New York to analyse the genetic data from 476 people with MacTel and 1733 controls people without the disease.
ÂWe were thrilled when our results were corroborated by two further independent validation studies, she said.
The analysis also revealed that people with the MacTel genetic risk loci identified in the study had changes in their metabolism, specifically in their glycine and serine levels.
Professor Bahlo said this meant there could be a significant relationship between the level of glycine and serine in the body, and onset of the disease.
ÂThough the exact link between the disease and glycine and serine is yet to be confirmed, the connection is an exciting clue to help us further explore metabolic abnormalities in people with MacTel, Professor Bahlo said.
Dr Scerri said the teamÂs work highlighted crucial points of interest that, with further investigation, could help researchers find a way to prevent the progression of the disease.
ÂWe are continuing to explore the genetic data to try identify the specific genes involved, and the precise genetic variations that are leading to the disease, Dr Scerri said.
President of the Lowy Medical Research Institute that sponsored the research Professor Martin Friedlander said the work represented a significant advancement in efforts to understand the cause of MacTel.
ÂWe are working towards developing treatments effective in preserving vision in patients with this disease, he said.
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