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Genomic blueprint of heart could help scientists combat fatal diseases
Sep 14, 3:51 pm
Washington, September 14 (ANI): Scientists at the Gladstone Institutes have provided new clues into the genetic basis for some forms of congenital heart disease by revealing the precise order and timing of hundreds of genetic "switches" required to construct a fully functional heart from embryonic heart cells.In a study, researchers in the laboratory of Gladstone Senior Investigator Benoit Bruneau, PhD, employed stem cell technology, next-generation DNA sequencing and computing tools to piece together the instruction manual, or "genomic blueprint" for how a heart becomes a heart. These findings offer renewed hope for combating life-threatening heart defects such as arrhythmias (irregular heart beat) and ventricular septal defects ("holes in the heart")."Congenital heart defects are the most common type of birth defects-affecting more than 35,000 newborn babies in the United States each year," said Dr. Bruneau, who is the associate director of cardiovascular research at Gladstone, an independent and nonprofit biomedical-research organization. "But how these defects develop at the genetic level has been difficult to pinpoint because research has focused on a small set of genes. Here, we approach heart formation with a wide-angle lens by looking at the entirety of the genetic material that gives heart cells their unique identity," he noted.The news comes at a time of emerging importance for the biological process called "epigenetics," in which a non-genetic factor impacts a cell's genetic makeup early during development-but sometimes with longer-term consequences. All of the cells in an organism contain the same DNA, but the epigenetic instructions encoded in specific DNA sequences give the cell its identity. Epigenetics is of particular interest in heart formation, as the incorrect on-and-off switching of genes during fetal development can lead to congenital heart disease-some forms of which may not be apparent until adulthood.In this research-conducted in large part at Gladstone's Roddenberry Center for Stem Cell Biology and Medicine, as well as in collaboration with the laboratory of Laurie Boyer, PhD, at the Massachusetts Institute of Technology-the scientists took embryonic stem cells from mice and reprogrammed them into beating heart cells by mimicking embryonic development in a petri dish. Next, they extracted the DNA from developing and mature heart cells, using an advanced gene-sequencing technique called ChIP-seq that lets scientists "see" the epigenetic signatures written in the DNA."But simply finding these signatures was only half the battle-we next had to decipher which aspects of heart formation they encoded," said Jeffrey Alexander, a Gladstone and UCSF graduate student and one of the paper's lead authors. "To do that, we harnessed the computing power of the Gladstone Bioinformatics Core. This allowed us to take the mountains of data collected from gene sequencing and organize it into a readable, meaningful blueprint for how a heart becomes a heart," he explained.The team made some unexpected discoveries. They found that groups of genes appear to work together in heart cells in a coordinated fashion-switching on and off as a group at designated times during embryonic development. The scientists not only identified a whole host of new genes involved in heart formation, but they also refined exactly how these newly discovered genes interact with previously known genes.The human-health implications of mapping the genomic blueprint of the heart are far reaching. Now that scientists understand how these genes control the heart, they can begin to piece together how heart disease disrupts this regulation. Eventually, they can look for therapies to prevent, interrupt or counteract those disruptions in children who suffer from congenital heart disease."Our findings reveal new clues as to how complex genetic and epigenetic patterns are precisely regulated during heart formation," said Dr. Boyer. "In particular, our identification of key segments of the genome that contribute to this process will hopefully allow us to identify the genetic causes of many forms of congenital heart disease-an important first step in the fight against this devastating disease," he added.The study has been published online in the journal Cell. (ANI)
T. rex cousin fed more like falcon than crocodile
May 22, 12:59 pm
Washington, May 22 (ANI): It is believed that the mighty T. rex may have thrashed its massive head from side to side to dismember prey, but a new study has shown that its smaller cousin Allosaurus was a more dexterous hunter and tugged at prey more like a modern-day falcon.
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14 closely related crocodiles existed around 5mn years ago
May 22, 12:17 pm
Washington, May 22 (ANI): An international team of scientists have revealed that a total of 14 different crocodile species existed and at least seven of them occupied the same area at the same time about five million years ago.
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Potential brain 'switch' responsible for our behavioural change identified
May 22, 11:39 am
Washington, May 22 (ANI): A new study by investigators at the University of Michigan and Eli Lilly may reveal the "switch" that helps our brains to make the shift from current behaviours to new ones.
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Radioactive nanoparticles that target cancer cells developed
May 22, 11:11 am
Washington, May 22 (ANI): Researchers at the University of Missouri have found a way to create radioactive nanoparticles that target lymphoma tumor cells wherever they may be in the body.
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