The test exploits the fact that the immune system makes antibodies to fight viruses whenever the body becomes infected. These antibodies can live on in the bloodstream for years and even decades.
To develop the test, Elledge engineered batches of harmless viruses to carry bits of proteins from human viruses on their surfaces. In total, they carried proteins from more than 1000 strains of the 206 kinds of viruses known to infect people. Antibodies use these protein fragments to recognise invading viruses and launch their attacks.
When a droplet of blood from a patient is mixed with the modified viruses, any antibodies they have latch on to human virus proteins they recognise as invaders. The scientists then pull out the antibodies and identify the human viruses from the protein fragments they have stuck to.
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Patient selection and profiling would be a very important issue indeed of course. I wonder if it might make sense to try to compare some subgroups within the study? Be able to see how viral load (and virus types) vary with degree of severity (measured somehow ???) and case definitions? I guess you can't go too far with this or you lose statistical power, but I don't really understand the limitations on this aspect of study design, are there any rules of thumb on how far one can go with sub-studies? (And btw the implications of assessing the stats for over 1000 strains sound hairy, but I guess we can handle the necessary error-correction here?).
