Genetically Modified Athletes

a book by Professor Andy Miah

Archive for November, 2009

Muscular monkeys prompt sports doping fears (2009, Nov 12)

Posted by Andy Miah on November 13, 2009

Muscular monkeys prompt sports doping fears
Linda Geddes, reporter

A gene therapy that appears to bulk up muscle mass and strength in monkeys – reported today in Science Translational Medicine – will undoubtedly raise fresh concerns about the potential for gene doping in sport.

We already know that some athletes use drugs like erythropoietin to increase the amount of oxygen their blood delivers, and steroids to bulk up muscle mass.

The big advantage with gene doping is that it should be harder to detect. That’s because it’s difficult to test for a protein that the body already produces, especially when its levels naturally vary between individuals – which might explain why some people are inherently better at sports than others.

In the new study, Janaiah Kota and colleagues at Nationwide Children’s Hospital in Columbus, Ohio, used gene therapy to add extra copies of the follistatin gene into the leg muscles of monkeys. Follistatin has been previously shown in mice to block myostatin, a protein that decreases muscle mass, resulting in bulked up “mighty mice”.
Monkeys injected with the gene also seemed to bulk up, and when Kota’s team analyzed their leg muscles with a device that measures force, they found that the muscles injected with the follistatin gene were also stronger than normal muscles.

They hope the approach could eventually be used to treat the severe muscle weakness associated with neuromuscular disorders like muscular dystrophy and multiple sclerosis.

Indeed, the drugs companies Amgen and Wyeth are already experimenting with drugs called myostatin inhibitors in humans, with some promising early results.

Such studies have already prompted fears about the potential for myostatin inhibitors to be abused by athletes hoping to gain the competitive edge. If gene therapy can achieve similar outcomes in humans, such modifications will be even harder to detect.

The World Anti-Doping Authority has already prohibited the use of gene doping within their World Anti-Doping code, and while there is currently no hard evidence of athletes using gene doping to improve performance, there are strong suspicions that they will start doing so soon – unless someone figures out a reliable way of detecting it.

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The Future of Doping – it’s in the Genes! (2009, Oct)

Posted by Andy Miah on November 13, 2009

The Future of Doping – it’s in the Genes! <http://joepapp.blogspot.com/2009/10/future-of-doping.html>

By Duane Corbett with an intro by Joe Papp

Last month here at Pappillon <http://joepapp.blogspot.com/2009/09/armstrongs-blood-values-deemed.html> , we revealed that one of Denmark’s leading blood researchers believed that Lance Armstrong’s blood values from the 2009 Tour de France were suspicious and could be indicative of blood doping <http://joepapp.blogspot.com/2009/09/armstrongs-blood-values-deemed.html> . We followed the story when the main stream media wussed-out (except for cyclingnews.com, where Shane Stokes made a valiant effort <http://www.cyclingnews.com/features/analysis-armstrongs-tour-blood-levels-debated> ), documented what others were saying, shared our own opinions, made scientific fact and proven theory accessible through this site, and, most of all, made it clear that we still believe doping is a problem in pro cycling and that Jakob Mørkebjerg’s claims shouldn’t be dismissed outright.

Not surprisingly, Lance Armstrong didn’t agree, and he lamely offered a four-letter response via Twitter to the serious questions that Mørkebjerg’s insights raised in the eyes of the public: “SSDD <http://www.nydailynews.com/sports/more_sports/2009/10/13/2009-10-13_lance_armstrong.html> “.

But is doping (and the talk of doping) in cycling really just the “same shit, different day,” scenario that The Lance would have us believe? To explore that question more deeply, Pappillon’s newest guest contributor Duane Corbett shares his thoughts on the potential for gene-doping to infect cycling:


With an investigation <http://velonews.com/article/99199/french-open-tour-investigation> into doping at this year’s Tour already underway, and involving the Astana Pro Cycling Team and several others from the Tour’s line-up, anti-doping authorities are likely considering just these scenarios as they try to determine what doping practices are currently en vogue – the same as were popular last year, some forgotten methodologies from the past, or new, as-of-yet unreported cutting-edge techniques.

Since there were no positive drug tests at the 2009 Tour de France it appears no one was doing the same stuff this year. However, several suspicious drugs were recovered at the race including sitagliptin (anti-diabetic), valpromide (anti-convulsant), telmisartan (anti-hypertensive), and quinapril (anti-hypertensive). It is important to note that the latter two may be linked to some of the old stuff as hypertension is a known adverse effect of blood transfusion.

Going into the 2009 Tour de France, many predicted <http://joepapp.blogspot.com/2009/07/2009-tour-de-france-predictions-micro.html> the practice of autologous blood transfusions to be present among riders. And why not? While tests have been developed to test for the use of synthetic EPO and homologous blood transfusions, there is still no definitive test for autologous doping; only the biological passport, which compares riders blood level records to permissible limits. So while the previous implementation of permissible limits may be seen as a green light, the biological passport may be seen as a speed bump.

Let’s quickly remind ourselves what someone’s blood samples would look like if they were transfusing themselves with their own blood. Where you would normally see a decline in red blood cells, hematocrit, and hemoglobin over the period of several days racing, someone transfusing themselves with their own blood would always have that same fresh and replenished baseline they started with. The only problem is so would someone with diarrhea <http://nyvelocity.com/content/features/2009/armstrong-tour-blood-values-suspicious> .

Now that the old stuff and the same stuff have been covered, what are the possibilities of new stuff? With the finding of such drugs like sitagliptin and valpromide, we can’t help but wonder what is, or what could be, going on right now that we don’t know about.

One of the biggest fears of anti-doping authorities is the introduction of gene doping. Dr. Theodore Friedmann, head of the World Anti-Doping Agency’s gene doping panel has been quoted to say, “It will happen, but we don’t know when.” Unfortunately, it may have happened already.

In 2008, scientists discovered orally active agents that genetically switch on an endurance gene signature that was shown to increase running endurance by 44% in sedentary mice. The first target of these drugs is PPARδ, a transcriptional regulator, and the second is AMPK, a serine-threonine kinase. Both PPARδ and AMPK contribute to metabolic reprogramming and are respectively targeted by the drugs GW1516 and AICAR.

A link to a brief video that would make anyone feel like a leading researcher on the topic is available here <http://www.pbs.org/wgbh/nova/sciencenow/0403/03-pill-flash.html> . The research article in its entirety is available here <http://www.sciencedirect.com/science?_ob=MImg&_imagekey=B6WSN-4T3W1NW-1-2&_cdi=7051&_user=10&_coverDate=08%2F08%2F2008&_sk=%23TOC%237051%232008%23998659996%23695566%23FLA%23display%23Volume_134,_Issue_3,_Pages_367-548_%288_August_2008%29%23tagged%23Volume%23first%3D134%23Issue%23first%3D3%23date%23%288_August_2008%29%23&view=c&_gw=y&wchp=dGLzVzz-zSkzV&md5=39775faaea5f20eff1ebb08f614bdf9a&ie=/sdarticle.pdf> .

While these drugs have only been tested in animals, the gap in time since their discovery opens possibility for human interaction. Although we do not know if it is happening now, we do know that the era of gene doping, or new stuff, different day, is uncomfortably close.
Duane Corbett
is a doctoral student in exercise physiology at Kent State University. His research, focused primarily on cycling, has previously examined the relationship between preferred pedal rates and perceived exertion, while current research involvement is examining the effect of cycling on Parkinson’s disease. A former collegiate cyclist, he is the founder of the current Indiana University of Pennsylvania Cycling Team.

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How Fast Can A Human Run The 100 Meter Sprint? (2009, Aug 6)

Posted by Andy Miah on November 13, 2009

How Fast Can A Human Run The 100 Meter Sprint? <http://www.scientificblogging.com/news_articles/how_fast_can_human_run_100_meter_sprint>
By News Staff <http://www.scientificblogging.com/profile/news_staff>  | August 6th 2009 12:00 AM | 6 comments <http://www.scientificblogging.com/news_articles/how_fast_can_human_run_100_meter_sprint#comments>  | Print <http://www.scientificblogging.com/print/56557>  | E-mail <http://www.scientificblogging.com/forward/56557>  | Track Comments <http://www.scientificblogging.com/news_articles/trackarticle/56557?destination=node%2F56557>
Usain Bolt, sprinter from Jamaica, currently holds the world record in the 100 meter sprint with a time of 9.69 seconds.  Whenever new records are set, people ask ‘what is the limit on human performance?’

So how fast can a human run?

Two econometricians from Tilburg University in the Netherlands, Professor of Statistics John Einmahl and former student Sander Smeets, say have calculated the ultimate records for the 100-meter sprint. The good news; there is still room for improvement in both the men’s and women’s times in the near future.

They used extreme value theory <http://en.wikipedia.org/wiki/Extreme_value_theory>  to calculate by how much the current records for the 100 meter sprint could be improved.

Extreme-value theory is a sub-sector of statistics, which tries to answer questions about extreme events (which by definition are uncommon), using information about less extreme events. The theory is normally applied within the financial and insurance world to estimate the risk of extreme damage resulting from storms, earthquakes or the bursting of a dyke, for example, in order to calculate premiums.

With a little modification, they say it can apply to sports as well.

Einmahl and Smeets analyzed the records of 762 male and 479 female athletes. Each athlete was listed once, and the times were recorded between January 1991 and June 2008. Times run before 1991 were discounted on account of the inadequate doping controls before this date. The men’s times varied between 9.72 and 10.30 seconds, and the women’s from 10.65 to 11.38.

According to Smeets and Einmahl, the fastest time that the men are capable of sprinting is 9.51 seconds, which knocks 0.18 seconds off Usain Bolt’s current world record. For female 100m sprinters, another 0.16 seconds can be knocked off the 10.49 run by Florence Griffith-Joyner, which would mean a time of 10.33. In a more cautious estimate (with a 95% confidence interval <http://www.stat.yale.edu/Courses/1997-98/101/confint.htm> ), the predicted times are 9.21 for the men and 9.88 for the women.

Sander Smeets studied Finance and Actuarial Sciences at Tilburg University and now works as a junior actuary at AZL, in Heerlen. John Einmahl is Professor of Statistics at Tilburg University.

Paper: ‘Ultimate 100m world records through extreme-value theory <http://arno.uvt.nl/show.cgi?fid=95436> ‘, CentER Discussion Paper nr. 57


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