Insight into brain via 'friend of fragile X' gene
Emory's Woodruff Health Sciences Center News Aug 11, 2017
We can learn a lot about somebody from the friends they hang out with. This applies to people and also to genes and proteins. Emory scientists have been investigating a gene that we will call  spoiler alert – "Friend of fragile X."
Fragile X syndrome is caused by a disruption of the gene FMR1.
In an independent form of inherited intellectual disability found in a small number of Iranian families, a gene called ZC3H14 is mutated. Two papers from Ken Moberg, PhD, associate professor of cell biology, Anita Corbett, PhD, professor of biology and colleagues show that FMR1 and ZC3H14 are, in effect, friends.
The findings provide new insight into the function of FMR1 as well as ZC3H14; the evidence comes from experiments performed in fruit flies and mice. The most recent paper was published in the journal Cell Reports.
The scientists found that the proteins encoded by FMR1 and ZC3H14 stick together in cells and they hang out in the same places. The two proteins have related functions: they both regulate messenger RNA in neurons, which explains their importance for learning and memory.
The fragile X protein (FMRP) was known to control protein production in response to signals arriving in neurons, but the paper shows that FMRP is also regulating the length of "tails" attached to messenger RNAs  something scientists did not realize, even after years of studying FMRP and fragile X, Moberg says.
In fruit flies, ZC3H14 is called dNab2. Mutations in this gene were previously shown to hinder flies' flying and climbing, as well as impair memories formed during courtship.
In the new paper, the researchers show that dNab2 mutant flies also have problems learning to avoid situations when an unpleasant smell is present. In this learning task, dNab2 and the fly version of FMR1 are working together, the researchers showed. However, the set of RNAs they regulate do not overlap completely.
Several labs at Emory contributed to the research, including those of human genetics chair Stephen Warren, PhD, cell biology chair Gary Bassell, PhD and James Zheng, PhD. The first author of the Cell Reports paper is Rick Bienkowski, PhD, a former Genetics and Molecular Biology graduate student.
"We could not have done this work without the strength of the neuroscience and especially, fragile X, community at Emory," Moberg says.
Corbett and Moberg's collaboration on dNab2/ZC3H14 was accelerated in 2009 when German and Iranian researchers contacted them about the link to human intellectual disability. It also pushed Corbett, who had first examined Nab2's function in yeast, into the realm of knockout mice.
Her lab's research on mice lacking ZC3H14, conducted with neuroscientists Paul Garcia, MD, PhD, and Andrew Escayg, PhD, was published in June in the journal Human Molecular Genetics.
Similar to the mutant flies, the mice display impaired working memory and altered brain development. Studies that combine the mutant mice and flies will reveal more about the functions of both RNA–binding proteins in learning and memory, Corbett says.
Go to Original
Fragile X syndrome is caused by a disruption of the gene FMR1.
In an independent form of inherited intellectual disability found in a small number of Iranian families, a gene called ZC3H14 is mutated. Two papers from Ken Moberg, PhD, associate professor of cell biology, Anita Corbett, PhD, professor of biology and colleagues show that FMR1 and ZC3H14 are, in effect, friends.
The findings provide new insight into the function of FMR1 as well as ZC3H14; the evidence comes from experiments performed in fruit flies and mice. The most recent paper was published in the journal Cell Reports.
The scientists found that the proteins encoded by FMR1 and ZC3H14 stick together in cells and they hang out in the same places. The two proteins have related functions: they both regulate messenger RNA in neurons, which explains their importance for learning and memory.
The fragile X protein (FMRP) was known to control protein production in response to signals arriving in neurons, but the paper shows that FMRP is also regulating the length of "tails" attached to messenger RNAs  something scientists did not realize, even after years of studying FMRP and fragile X, Moberg says.
In fruit flies, ZC3H14 is called dNab2. Mutations in this gene were previously shown to hinder flies' flying and climbing, as well as impair memories formed during courtship.
In the new paper, the researchers show that dNab2 mutant flies also have problems learning to avoid situations when an unpleasant smell is present. In this learning task, dNab2 and the fly version of FMR1 are working together, the researchers showed. However, the set of RNAs they regulate do not overlap completely.
Several labs at Emory contributed to the research, including those of human genetics chair Stephen Warren, PhD, cell biology chair Gary Bassell, PhD and James Zheng, PhD. The first author of the Cell Reports paper is Rick Bienkowski, PhD, a former Genetics and Molecular Biology graduate student.
"We could not have done this work without the strength of the neuroscience and especially, fragile X, community at Emory," Moberg says.
Corbett and Moberg's collaboration on dNab2/ZC3H14 was accelerated in 2009 when German and Iranian researchers contacted them about the link to human intellectual disability. It also pushed Corbett, who had first examined Nab2's function in yeast, into the realm of knockout mice.
Her lab's research on mice lacking ZC3H14, conducted with neuroscientists Paul Garcia, MD, PhD, and Andrew Escayg, PhD, was published in June in the journal Human Molecular Genetics.
Similar to the mutant flies, the mice display impaired working memory and altered brain development. Studies that combine the mutant mice and flies will reveal more about the functions of both RNA–binding proteins in learning and memory, Corbett says.
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