Genetic Research Related To Ankylosing Spondylitis | Arthritis Information

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Work done in part by researchers at The University of Texas Health Science Center at Houston has led to the discovery of two new genes that are implicated in ankylosing spondylitis (AS), an inflammatory and potentially disabling disease. In addition, the international research team pinpointed two areas along stretches of DNA that play an important role in regulating gene activity associated with the arthritic condition.

The findings, a critical milestone in the understanding of AS, are published in the January issue of Nature Genetics, a journal that emphasizes research on the genetic basis for common and complex diseases. "This helps us better understand what is driving this disease and gives us direction for new treatments and diagnostic tests," said John D. Reveille, M.D., the study's principal investigator and professor and director of the Division of Rheumatology and Clinical Immunogenetics at The University of Texas Medical School at Houston.

Reveille, the university's Linda and Ronny Finger Foundation Distinguished Chair in Neuroimmunologic Disorders, and Matthew A. Brown, M.D., professor of immunogenetics at Australia's University of Queensland, led the research by the Triple "A" Spondylitis Consortium Genetic Study (i.e. the TASC or Australo-Anglo-American Spondylitis Consortium). Based on work from a genome-wide association scan, the team identified genes ANTXR2 and IL1R2 as well as two gene deserts, segments of DNA between genes on chromosomes 2 and 21 that are associated with ankylosing spondylitis. Importantly, the study also confirmed the Triple "A" Australo-Anglo-American Spondylitis Consortium's previously reported associations of genes IL23R and ERAP1, formerly known as ARTS1.

Reveille, chief of rheumatology at Memorial Hermann-Texas Medical Center, said the genetic discoveries bring the scientific community closer to fully understanding AS, a chronic form of
arthritis that attacks the spine and also can target other joints and organs in the body. The Centers for Disease Control and Prevention for the National Arthritis Data Workgroup estimates that AS and its related diseases affect as many as 2.4 million people in the United States. It generally strikes patients in their teens, 20s or 30s and can cause a complete fusion of the spine, leaving patients unable to straighten and bend.

Steve Haskew, who has lived with AS for more than three decades, said these genetic discoveries offer hope to patients, especially those newly diagnosed.

"When I first started experiencing lower
back pain and the aching joints, no one could tell me what was wrong," said Haskew, co-leader of an AS support group. "It's fascinating to see how far we've come and how much has been learned about the disease."

Laurie Savage, co-principal investigator and executive director of the Spondylitis Association of America (SAA) said, "These new breakthroughs are, indeed, good news for those whom we serve. It is very encouraging to know that the health impact and economic consequences of spondyloarthritis in the world eventually will be contained as a direct consequence of the dedication of Drs. Reveille, Brown and colleagues, and that of the many individuals affected by spondyloarthritis who have participated in these studies."

The study, titled "Genomewide association study of ankylosing spondylitis identifies multiple non-MHC susceptibility loci," was supported in part by two grants from the National Institute of Arthritis and Musculoskeletal and Skin Diseases. Other study contributors from the UT Health Science Center at Houston are research associates Laura Diekman and Rui Jin and Xiaodong Zhou, M.D., associate professor of medicine.

Source: Meredith Raine
University of Texas Health Science Center at Houston

 
 
http://www.medicalnewstoday.com/articles/175641.php

Thanks again, Lynn, for another informative article.

People should also know that AS has a close relationship to Psoriatic Arthritis ["PsA"] as they both share the same HLA-B27.
Yes Sam I was wondering if they cross checked PSA and reactive arthritis with those genes. I love the fact that they found something specific. At least now people with AS will not have to wonder if they indeed have AS or if it could be something else.
 
AI diseases are often so alike and leave people confused as to what they may actually have. It would be nice if they could find this in other diseases also. My pc told me when he ordered the anti-ccp test for me that no one would ever question my RA dx again if it was positive. Wow was he wrong. I am RF positive and anti-ccp positive and still the RD's are not exactly sure what I have. Probably RA but my duck has a frog in it's throat.
Milly, as I keep saying, ten years from now we're going to look back and realize how dumb we were about arthritic diseases.  
 
 
[QUOTE=Sam1234]Milly, as I keep saying, ten years from now we're going to look back and realize how dumb we were about arthritic diseases.  
 
 
[/QUOTE]
 
I think that's a very true statement, Sam.
 
how do you get a doc to do the gene testings?? 
 
ETA: my first thought as I began reading this is... There she goes again.. giving us the best info and up to date!! Thanks Lynn!!!
babs102010-01-13 09:43:25

Milly,

The way to get the genetic testing done is to tell your doctor you want the tests for whatever genetic component you want tested.  But here's the sticky part......some doctors are really not up on what latest tests are available or what they're called.
 
For example, I happened to notice from information on a diabetes forum that a particular set of genes is found in those with autoimmune diabetes. I also knew what their test names were [GAD, ICA, and Ig-ICA]. So I asked my endocrinologist to run those tests.
 
I felt absolutely certain I'd come out positive in every single one of them because all the women on my mom's side of the family have Type 2 Diabetes. Well guess what.......I came out negative on every single test. Upon further research I found that only 80% who are positive come out positive, then there are false positives, etc., etc.
 
So nothing's foolproof.
 
In Ankylosing Spondylitis the haplotype HLA-B27 commonly shows up.....as it does in psoriatic arthritis. It appears I've got both diseases and yet I'm negative for both in special testing. In fact, in every genetic test for autoimmune disease I've ever taken, I turn out negative.
 
I think the most comprehensive way would be to go to an immunologist who would be more up-to-date.
 
But all this prompts the question:  How many people who have clear cut signs of Ankylosing Spondylitis, tested negative for HLA-B27, have seronegative RA, and have Type O blood?
 
I think I'll put that on another topic. Will be interesting to see, because I have a hunch that Type O blood might be in back of seronegative test results.
Sam12342010-01-13 12:35:34
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