Drugs are not new. Moreover, the spectacular advances in Molecular Life Sciences
that many would say began after the first field trials of Penicillin,
throughout World War II, and included Watson and Crick's structure for
DNA, Sanger's sequencing of the first protein (the hormone insulin), not
forgetting Kendrew and Perutz's ground-breaking work in protein
crystallography. It was in fact a slightly distracted doctor who during
the Victorian era picked the wrong"potion" from his shelf and
inadvertently, but successfully, administered the first dose of
paracetamol (well a closely related compound), to treat a patient with
fever. In fact apart from the medicinal herbs mixed and formulated by
village "pharmacists" that have their roots (sorry!) in traditional
cures, it was the Victorians and their 20th Century proteges that in my
view laid a formidable foundation for 20th and 21st century medicine. ![]() |
| The antimalarial compound, artemesinin |
In the New Scientist special edition, the emergence of targeted drugs that not only treat the diseased cells and tissues, but also send a digital report on the status of the disease, are suggested to be around the corner! I shall exemplify this with the recent work published in the journal Cell on Photostatins (PST), also covered in a recent article in the Economist. If a molecule could be synthesised that interferes selectively with a Biological process and whose activity can be tuned by a non-invasive pulse of light (hv), then drugs become not only therapeutic but also diagnostics. The term "theranostics" would encompass this type of compound. In the above image, cells are shown as a blue nucleus with green radiating fibres: these are microtubules (take a look here). The addition of the PST molecule, followed by a specific pulse of light, leads to the breakdown in the microtubule network. Since microtubules are central to the cell's many growth and cell division functions, you can see how this approach has enormous potential for precision/personalised medicines. The introduction of a simple test for the over-expression of HER-2 protein: the target for Herceptin, has been approved and marketed by Dako. The company's Hercep Test is one of the earliest examples of a theranostic agent. The combination of these two functions in the form of drugs administered to treat and report on the targeted cells, is a quantum leap in the treatment of complex diseases like cancer and one that offers exciting prospects. It reminds me of the excitement I felt when at the age of around 12, I saw the film "Fantastic Voyage"; a Jules Verne type fantasy, in which a submarine and crew are miniaturised and injected into a scientist's veins to fix a life threatening blood clot. The prospect of controlled nano drones is probably more likely to be the future reality, as we begin to combine targeted intervention, reporting and surveillance. I agree with the New Scientist view that progress across these fronts will begin to transform modern medicine. However, I also believe that the biggest challenge is not whether we can innovate, but how on earth do we pay for it all!
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