No IgNobels here, the 2007 Nobel Prize for Physiology or Medicine has been awarded to Mario R. Capecchi, Martin J. Evans, and Oliver Smithies for a technique that is so incredibly important to modern biomedical research that it's a wonder they didn't get the prize before:
This year's Nobel Laureates have made a series of ground-breaking discoveries concerning embryonic stem cells and DNA recombination in mammals. Their discoveries led to the creation of an immensely powerful technology referred to as gene targeting in mice. It is now being applied to virtually all areas of biomedicine - from basic research to the development of new therapies.
Gene targeting is often used to inactivate single genes. Such gene "knockout" experiments have elucidated the roles of numerous genes in embryonic development, adult physiology, aging and disease. To date, more than ten thousand mouse genes (approximately half of the genes in the mammalian genome) have been knocked out. Ongoing international efforts will make "knockout mice" for all genes available within the near future.
With gene targeting it is now possible to produce almost any type of DNA modification in the mouse genome, allowing scientists to establish the roles of individual genes in health and disease. Gene targeting has already produced more than five hundred different mouse models of human disorders, including cardiovascular and neuro-degenerative diseases, diabetes and cancer.
It's hard to overstate how important this technique has become. Using this genetic engineering technology, it is possible to produce mice with a gene or genes specifically knocked out. It is possible to introduce a gene into stem cells and produce mice with that gene's expression cranked up to high levels. Scientists can then observe the resulting phenotype. The entire process is illustrated below:
I'm actually familiar with Mario Capecchi's work and have read many of his papers. This is because one of my long time research project involves studying homeobox genes, and Capechhi is known for using this gene targeting technique to produce mice with specific HOX genes disrupted in order to demonstrate their function by observing the phenotype of the resulting mice. He played a major role in working out the "HOX code" in vertebrates. Capecchi's work with vertebrate HOX genes demonstrates the power of gene targeting to produce transgenic mice.
In the study of human disease, the applications of this technology range from cancer to heart disease to--well, pretty much any disease with a major genetic component. All I can say after seeing this award is: What took the Nobel Prize committee so long?
I notice that it involves sticking needles into things. Did they adequately control for the fact that the needles might be what's making the mice feel better?
... heh. Just kidding.
I wish I understood this stuff better. I'm glad that there's really smart people out there pushing the boundaries of science while the rest of us push the speed-bumps of stupid.
Orac, given your admiration of Capecchi and work on combating Holocaust denial, I thought you and your readers might be interested in a heartcrushing story by Daniel Cressey at Nature's The Great Beyond blog that I learned from the WSJ Health Blog:
It's a little surprising to me because I'd heard of "knockout mice" a zillion times before, but I'd never heard this described as a "stem cell" technique until I started seeing the articles about this this morning. Looking at the procedure outlined here though that does appear to be the correct way to describe it.
Implanted into a mouse!
What instruments are used to implant a blastocyst into a mouse's uterus?
Is there a diagram or video of this procedure?
What about multiple roles or codes within single genes?
Forgive my ignorance on this subject, but isn't there a complex role that yet needs to be understood within each individual gene? Identifying a so called aging gene for instance is but only a part of that particular genes function?
"Implanted into a mouse! What instruments are used to implant a blastocyst into a mouse's uterus?"
Forceps, a needle, and a pipette.
"Is there a diagram or video of this procedure?"
http://ourworld.compuserve.com/homepages/TheBroons/tnp2.htm
Good point, Coin. To make a genetically altered mouse- i.e., knock out or knock in- the initial DNA recombination occurs in a stem cell and then that cell is used to create a whole animal through blastocyst implantation or tetraploid aggregation. Very neat stuff.
And yet, almost 20 years later, we still have never been able to create a knockout rat. Why? Nobody knows. Still.
May, 2003: the first knockout rat is created. (actually, that's probably the publication date)
What, no word from your pal Egnor?
I thought he said that there was NO connection between evolution and medicine.
Nope, none whatsoever. Not a smidgin'. Totally u.s.e.l.e.s.s.
Maybe he was runner-up for the Prize. Hopefully he'll enlighten us on the travesty of justice in an upcoming essay on the DI's Whine and Cheese site.