And to save the world from this plague brought on by eating cows. :lol:12. The aim of this research is to uncover the science of TSEs, in particular their nature and means of transmission; to develop countermeasures at many points in the food chain; to protect the health of the UK population; and to engage the public in the research and its application.
try explaining this to the 182,583 confirmed cases of UK BSE since 1987 who consumed all the tainted feed and contracted BSE. then maybe you can explain the drastic decline of BSE since the feed ban.
THE TSE agent has been proven beyond a shadow of a doubt to cause death in both man and animal. This is proven science, proven fact. i cannot help if there rkaiser if your pea brain cannot understand this science.
Quote:
12. The aim of this research is to uncover the science of TSEs, in particular their nature and means of transmission; to develop countermeasures at many points in the food chain; to protect the health of the UK population; and to engage the public in the research and its application.
THE BARBs are pretty much self explanatory (for most;-) as well with failed feed ban, old feed stored etc. we saw what can happen with some old beef, it can float around for 23 years, then be passed off as blue
beef;-)
your smoke screens are failing the smell test there rkaiser.
TSS
reader (the Second) said:Jason said:I have to admit I don't read those posts of Flounder's that are 3 miles long. Let me know if this is close.
I think the reduction of BSE cases after a feed ban is proof enough that feeding misfolded prions in high enough concentration to the same species will trigger a TSE. (Britian with BSE and cannibals with Kuru)
CWD confuses me because where is the source of concentrated prions for them?
It also seems to be apperant this feeding has to occur at a young age in cattle at least.
Blood to blood transmission in species seems to be fact.
Cross species transmission through feed seems much harder, 150 cases of vcjd in Britian when thousands of cows had BSE, (Brits have a habit of eating much more SRM than we do) seems to confirm this.
Removal of SRM because of the concentration there of misfolded prions would seem to be the safest way to protect people from the small chance of contracting a TSE from beef.
I understand those that have lost family and crusade about BSE/TSE but in real world terms the risks are so low it is a non issue as long as measures in place are followed.
The benefits of beef for feeding people are higher than the risks of TSEs.
There's that nasty money thing again Randy, ranchers wanting to keep selling beef. :wink:
Jason - you're about 80% correct. Here are the points where what you wrote may not be totally accurate.
-- It's too early to say that the species barrier worked. It appears that it did, thus only 150+ cases in UK, mostly young people. HOWEVER, the incubation for TSEs are 20 - 40 years and so far all the UK cases were the same genotype. People of other genotypes may have LONGER incubation periods. It is certain from some biopsies of tonsils and appendices that there are some asymptomatic carriers of the disease who may yet develop the disease. Until 20 - 30 years have passed, we will not know the full impact of the BSE epidemic on humans.
-- Removing SRMs is not enough for two reasons -- First, they do not remove the central nervous system of cows under 30 months, only the distal ileum, thus putting humans at risk from brain material of under 30 month cows. Second, as you indicate, these diseases are shown to transmit via blood and probably via other bodily fluids (this is how they believe that CWD is spreading among deer). Testing is absolutely necessary to eliminate BSE.
-- The different diseases in the family transmit differently and also, once a disease has crossed the species barrier it appears to transmit more readily. CWD appears to transmit horizontally from deer to deer possibly via saliva, feces, urine ...
-- Read a little of Flounder's recent posting. It explains why TSEs are worrisome, despite the small numbers. They are always fatal, long incubation, and can be transmitted in the blood suppy, via surgical instruments. This leads to silent amplification from just a few cases. I have been coming into contact with a number of cases of CJD that were caused by surgery. Just a teeny bit of contamination can transmit the disease. In the meantime, the person who was infected via surgery is donating blood and having surgery, thus possibly infecting others.
-- Yes, the numbers are small but all life is precious and as I have shown these diseases worry health researchers globally despite the small numbers.
-- I have always said that I believe that the chances of catching vCJD via beef in North America is small but NO ONE knows how small or large the chances are because we haven't done enough testing to understand the numbers and the trend.
The blood brain barrier is the barrier between the brain of some idiot who brags of paying $350,000.00 per validation out of HIS OWN POCKET to help mankind through this BSE issue, and the rest of mankind. Your turn money bags, how do misfolded prions cross the blood brain barrier, or for that matter pass from the gut of a cow to his/her blood muscle tissue, or the infamous SRM?
P.S. - Do cats Fart?.
Prions may hold key to stem cell function
22:00 30 January 2006
NewScientist.com news service
Stu Hutson
The curative properties of stem cells may rely on prions, a new study suggests, the type of protein made infamous by mad cow disease.
Prions are a special class of protein that can change the shape and function of other proteins around them. While these are found throughout any mammal's body, the understanding of their biological role is limited. What is known is that prions that become misshapen, through some unknown process, can result in BSE (bovine spongiform encephalopathy) – mad cow disease – and its equivalents in other animals.
Researchers at the Whitehead Institute in Cambridge, Massachusetts, US, have now found that adult stem cells in bone marrow gradually lose their ability to regenerate without their normal complement of membrane-bound prions. Stem cells are primitive cells which have the potential to divide endlessly, and the ability to differentiate into any cell type in the body – offering hope for future therapies.
First answers
Andrew Steele, Cheng Cheng Zhang and colleagues used radiation to deplete the bone marrow of mice genetically engineered to not produce the prion proteins. The animals' marrow regenerated quickly at first, but eventually slowed to a stop. The marrow also lost its regenerative abilities when transplanted into normal mice.
"For years we've wondered why evolution has preserved this protein, what positive role it could possibly be playing," says Susan Lindquist, one of the team. "With these findings we have our first answer."
The question of how prions sustain stem cell activity remains unanswered, but the finding is a first step to understanding the destructive streak of misshapen prion proteins, Steele says. Similar tests on neural and lung stem cells are underway.
Journal reference: Proceedings of the National Academy of Sciences (DOI: 10.1073/pnas.0510577103)
Just because current tests are not sensitive enough to detect prions in younger animals does not mean that they are not there or that the level they are present is not sufficient to transmit the disease. WHAT is the difference between a 29 month old and a 30 month old?!
How does the food you eat and the oxygen your breathe get to nourish you and that great emptiness between your ears? Is it by some form of voodoo magic or simply having to bang your head against the plate once you lick it clean?? Answer the original question pal and show us your depth of knowledge??
I'll have to go back to this question you are asking and return to my daddy's computer to give you the answer.