aspirin the wonder drug

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    Aspirin continues to amazeFor thousands of years aspirin has been humanity's wonder drug. Extracts from the willow tree

    have been used for pain relief in folk medicine since the time of the ancient Greeks. By 1897 a

    synthetic derivative (acetyl salicylic acid) of the plant's active ingredient (salicin) was created.This allowed aspirin to become the most widely used medicine in the world.

    In recent years its benefits as a blood-thinning drug have led to it being prescribed in

    low doses of around 50mg to reduce deaths from stroke and heart attack. There were

    also hints that aspirin may help prevent some cancers. But these were mostly based on

    observational studies, which can be misleading.

    The gold standard of scientific evidence is the randomised controlled trial, preferably

    one with a lot of peo ple and held over a long time. The results of just such a trial,published in the Lancet, suggest that aspirin is indeed an astonishing drug. Peter

    Rothwell at the John Radcliffe Hospital in Oxford and his colleagues looked at deaths

    due to cancers during and after randomised trials of daily aspirin. The trials had actually

    been started to look at how useful aspirin was for preventing heart attacks and strokes.

    Nevertheless, the data from the 25,570 patients enrolled in eight trials was also

    revealing about cancer.

    In trials lasting between four and eight years, the patients who had been given aspirin

    were 21% less likely to die from cancer than those who had been given a placebo.These results were based on 674 cancer deaths, so are unlikely to represent the kind of

    statistical oddity that can beset studies on cancer risks that sometimes create

    headlines.

    The benefits of aspirin were also apparent many years after the trials had ended. After

    five years, death rates for all cancers fell by 35% and for gastrointestinal cancers by

    54%. A long-term follow-up of patients showed that the 20-year risk of cancer death

    remained 20% lower in those who had taken aspirin.

    The study revealed that the effect takes time to accrue, so aspirin must be taken over a

    long period. The latent period for improving oesophageal, pancreatic, brain and lung

    cancer was about five years of aspirin taken on a daily basis. For stomach and colorectal

    cancer, the effects took ten years and for prostate cancer about 15 years. The means

    by which aspirin prevents cancer is not well understood. It is believed that it inhibits an

    enzyme that promotes cell proliferation in tumours.

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    The researchers also found that small daily doses of aspirin were enough, and that

    taking more than 75mg conferred no additional benefits. Those starting on aspirin in

    their late 40s or 50s benefit most.

    Current guidelines on using aspirin for reducing the chances of a stroke or heart attack

    rightly warn of the small risk of ulcers and of dangerous bleeding in the stomach. These

    guidelines will probably have to be revised given the new findings. However, it remains

    unlikely that popping aspirin will be recommended for everyone like a vitamin

    supplement.

    Aspirin is a highly cost-effective treatment: taking it for five to ten years easily beats

    initiatives to screen for breast and prostate cancers. To put it another way, ask yourself

    what a pharmaceuticals firm might charge for a drug that would reduce the chance ofdeath by cancer by 20% - and then note that 100 days' supply of low-dose aspirin can

    cost less than a dollar. By anyone's measure, that is a bargain.