First Genome-Wide Study Of Bipolar Disorder Reveals Its Genetic Roots
Main Category: BipolarAlso Included In: Genetics; Psychology / Psychiatry
Article Date: 13 May 2007 - 6:00 PDT
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The likelihood of developing bipolar disorder depends in part on the combined, small effects of variations in many different genes in the brain, none of which is powerful enough to cause the disease by itself, a new study shows. However, targeting the enzyme produced by one of these genes could lead to development of new, more effective medications. The research was conducted by scientists at the National Institutes of Health's National Institute of Mental Health (NIMH), with others from the Universities of Heidelberg and Bonn and a number of U.S. facilities collaborating in a major project called the NIMH Genetics Initiative.
The study is the first to scan virtually all of the variations in human genes to find those associated with bipolar disorder. Results were published online in Molecular Psychiatry by Amber E. Baum, PhD, lead researcher Francis J. McMahon, MD, and colleagues.
"This is an example of how advances in genetics research feed into practical applications. This research would not have been possible a very few years ago. We now have a new molecular target scientists can investigate in their search for better medications for bipolar disorder," said NIH Director Elias A. Zerhouni, MD.
About 5.7 million American adults have bipolar disorder, which also is called manic-depressive illness. Symptoms include extremes in mood, from pronounced over-excitement and elation, often coupled with severe irritability, to depression. Children also may have the condition, usually in a more severe form than adults.
"We're beginning to get a foothold on the genetics of this complex brain disorder," said NIMH Director Thomas R. Insel, MD.
Most people occasionally have mood swings, but the shifts that occur in bipolar disorder, and the changes in behavior and energy level that accompany them, are sometimes disabling. Lithium and the other mood-stabilizing medications used to treat the condition help many patients.
But some people do not respond to these medications, and clinicians need more options so that they can tailor treatments to each patient. People inherit different gene variations, which may influence whether or not they respond to a given medication. Identifying and targeting these variations could help scientists develop additional medication options that take these differences into account.
One of the genes the researchers correlated with the disorder, DGKH, is active in a biochemical pathway through which lithium is thought to exert its therapeutic effects. The gene produces an enzyme (diacylglycerol kinase eta) that functions at a point closer to the root of the lithium-sensitive pathway than does the protein that lithium is thought to target. Scientists can now try to develop more effective medications by focusing on new compounds that act on the DGKH enzyme or regulate how much of the enzyme is produced. The DGKH gene is on chromosome 13.
"Treatments that target just a few of these genes or the proteins they make could yield substantial benefits for patients. Lithium is still the primary treatment for bipolar disorder, but DGKH is a promising target for new treatments that might be more effective and better tolerated," McMahon said.
The finding was enabled by recent genetics technology that allows researchers to scan, in a single experiment, thousands of genes for variations. Everyone has the same genes, but variations in them influence whether or not a person gets a specific disease. In this study, researchers compared variations found in the scans of 413 adults who had bipolar disorder with variations found in the scans of 563 healthy adults.
By pooling the genetic material of the adults with bipolar disorder, the U.S. researchers were able to scan the entire group at a small fraction of the cost of scanning each person's material individually. The genetic material of the healthy group was pooled and scanned separately, again at a fraction of the cost of individual scans. The researchers then zeroed in on the gene variations that occurred more often in the people with bipolar disorder and examined them individually.
An important issue in genetics research is that findings correlating specific genes with specific diseases in one population may not apply to other populations. This study addressed that issue by focusing on US participants of European ancestry, then repeating the study in a large group of patients in Germany. Similar outcomes were found in both populations, strengthening the validity of the results. A subsequent study is examining whether the results apply to other populations, and will look for common variations among them.
The researchers will soon make the results of their scans available, on a website, to other scientists who are pursuing this line of research.
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For more NIMH information about bipolar disorder, visit http://www.nimh.nih.gov/healthinformation/bipolarmenu.cfm.
Coauthors of this report, including contributors from the National Institute on Aging (also part of the National Institutes of Health), are listed below:
Amber E. Baum, Nirmala Akula, Imer Cardona, Michael Cabanero, and Winston Corona
(NIMH Genetic Basis of Mood and Anxiety Disorders Unit, Mood and Anxiety Disorders Program)
Ben Klemens
(NIMH Genetic Basis of Mood and Anxiety Disorders Unit, Mood and Anxiety Disorders Program; The Brookings Institution)
Thomas G Schulze
(University of Heidelberg)
Sven Cichon
( University of Bonn)
Marcella Rietschel
(University of Heidelberg)
Markus Nöthen
(University of Bonn)
A. Georgi
(University of Heidelberg)
Johannes Schumacher
(University of Bonn)
M Schwarz
(University of Heidelberg)
R. Abou Jamra, S. Höfels, and P. Propping
(University of Bonn)
Jaya Satagopan
(Memorial Sloan-Kettering Cancer Center)
NIMH Genetics Initiative Bipolar Disorder Consortium
(Johns Hopkins University School of Medicine, Baltimore, MD; University of California, Irvine and San Diego, CA; University of Chicago, Chicago, IL; University of Pennsylvania, Philadelphia, PA; Laboratory of Clinical Science, National Institute of Mental Health Intramural Research Program, Rush University Medical Center, Chicago, IL; Washington University School of Medicine, St. Louis, MO; University of Iowa Medical School, Iowa City, IA; Indiana University School of Medicine, Indianapolis, IN)
Sevilla Detera-Wadleigh
(NIMH Genetic Basis of Mood and Anxiety Disorders Unit, Mood and Anxiety Disorders Program)
John Hardy
(National Institute on Aging, National Institutes of Health)
McMahon, Francis J.
(NIMH Genetic Basis of Mood and Anxiety Disorders Unit, Mood and Anxiety Disorders Program)
Baum AE, Akula N, Cabanero M, Cardona I, Corona W, Klemens B, Schulze TG, Cichon S, Rietschel M, Nöthen MM, Georgi A, Schumacher J, Schwarz M, Jamra RA, Höfels S, Propping P, Satagopan J, NIMH Genetics Initiative Bipolar Disorder Consortium, Detere-Wadleigh SD, Hardy J, McMahon F. A genome-wide association study implicates diacylglycerol kinase eta (DGKH) and several other genes in the etiology of bipolar disorder. Molecular Psychiatry, online ahead of print, May 8, 2007.
The National Institute of Mental Health (NIMH) mission is to reduce the burden of mental and behavioral disorders through research on mind, brain, and behavior. More information is available at the NIMH website: http://www.nimh.nih.gov/.
The National Institutes of Health (NIH) - The Nation's Medical Research Agency - includes 27 Institutes and Centers and is a component of the U.S. Department of Health and Human Services. It is the primary federal agency for conducting and supporting basic, clinical and translational medical research, and it investigates the causes, treatments, and cures for both common and rare diseases. For more information about NIH and its programs, visit http://www.nih.gov/.
Contact: Susan Cahill
NIH/National Institute of Mental Health
Visit our bipolar section for the latest news on this subject.
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Visitor Opinions In Chronological Order (2)
Basis For Multiple Nutrient Treatment Of Bipolar
posted by Unabelle R. Boggs Ph.D. on 25 May 2007 at 4:34 pmThe finding that numerous genetic defects contribute to bipolar disease in different people shows that a great variety of nutrients are needed to correct the various enzymatic malfunctions. EM Power+ is a multinutrient
formula that has been shown by Bonnie Kaplan et al at the University of Calgary, Canada, to effectively treat bipolar.
Many different genetic dependency diseases have been discovered causing the need for extraordinary levels of vitamins and minerals which are required as cofactors for the functioning of the corresponding enzymes. Many different medications are required for partial control of bipolar in some people. Nutrients increase the potency of the medications causing the need to reduce or eliminate the medications.
In the 1970s and 1980's I successfully treated many different kinds of mental dysfunctions with relatively high levels of individually prescribed multivitamins and minerals.
polar bi name polar bi nature
posted by graham paul ready on 14 Jan 2011 at 8:52 pmI agree with what you are saying but my bi polar is now part of me and i have lernt to live with this illness and in some ways it can even be an advantage to me, but only sometimes!!
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