Flu Terminology 101
posted Saturday April 25, 2009 under chem-bio, resources-for-wonks by geoffrey_fordenWith the discovery of a new and deadly flu virus in Mexico that might become a worldwide pandemic, I wanted to familiarize myself with the terminology used and bandied about so much in the media. This is the flu naming conventions such as H1N1 or H5N1 strains we are starting to hear so much about. (By the way, this qualifies for armscontrolwonk.com because the public health response to a pandemic is the same whether or not it is caused by human action.)
So here is a quick tutorial on Flu Terminology that I’ve learned:
Flu viruses are categorized by two surface molecules: the neuraminidase (from which the N comes from) and the haemagglutinin molecules (where we get the H). Neuraminidase and haemagglutinin are characterized by the response of antibodies to them. For human influenza viruses the convention is:
—all those in circulation before 1957 are termed H1N1 viruses
—those arising between 1957 and 1968 are known as H2N2
—those present since 1968 (and not previously named) are known as H3N2 (my reference material dates from 2002 so perhaps more have arisen.)
Other strains, such as H5N1, are not originally human viruses though the big danger is that they will jump from birds, swine, or horses to humans.
Neuraminidase has been described as a “mushroom” shaped molecule but with a square head attached to a long thin stalk. It is associated with the release of viruses produced in a host cell. In fact, neuraminidase specific antibodies will prevent their release but will not prevent the original infection of the cell. There are five separate sites on the neuraminidase molecule that antibodies bind to. A single amino acid change at any of these sites makes the virus invisible to the antibodies that had previously attached quite well.
Hemagglutinin is a triangular rod-shaped molecule and is associated with the virus’ binding sites in the host organism. For instance, human and swine haemagglutinin prefer one type of receptor molecules and bird flu viruses prefer a different one.
Interestingly, if a cell is infected with two different flu viruses (such as H1N1 and H2N2) then the virus genetic material can be rearranged in the cell so that the released viruses include mixes like H1N2 and H2N1 surface molecules.
Most of this information comes from the various papers in “Influenza” edited by C.W. Potter. If I’ve made any mistakes, I’m sure biologically oriented wonk-readers will let me know and correct the errors in the comments.
[Geoff takes pains to justify his post about pandemic influenza, but this is a topic we have discussed before. Pandemic influenza is the sort of non-deliberate threat threat that requires “cooperation between potential enemies”, a solution set that encompasses the canonical definition of arms control — Jeffrey]
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Very interesting, but I’m not sure what it has got to do with arms control.
— Major Lemon · Apr 25, 06:25 PM ·
The ease with which infuenza virii recombinate with each other is why flu shots are different from year to year.
As for the Mexican virus being H1N1, what little I’ve read from people who know better leads me to believe that this one really scares them. The 1918 flu pandemic was an H1N1 virus and nobody wants to do that again. Unfortunately, the epidemiology coming from Mexico shows that the death pattern hits the young & healthy instead of the usual flu pattern of infant/elderly. The 1918 virus killed mainly young & healthy because it induced cytokine storms in their fully-active immune systems, essentially causing the immune system to overreact and start attacking the body itself. These cytokine storms led to the widely-observed “drowning in their own lungs” pattern of death. Infants and the elderly escaped because their weakened immune systems didn’t overreact to the virus and cause a cytokine storm.
As for the arms control basis, releasing a 1918 Spanish Flu variant (I’m not saying this current one is) would clearly be a use of WMD. It’s why so many biologists thought it foolhardy beyond belief when the 1918 virus was recently cultured from samples taken from dead Inuit exhumed from the Alaskan permafrost just to see how the virus really worked. Knowledge like that can’t be put back in the can.
— Captain Ned · Apr 25, 07:08 PM ·
Treame to Cyokine storms “..the possibility of preventing a cytokine storm by inhibiting or disabling T-cell response. A few days after T cells are activated, they produce a biologic molecule called OX40, a “survival signal” that keeps activated T-cells working at the site of inflammation during infection with influenza or other pathogens. OX40 binds to receptors on T-cells, preventing them from dying and subsequently increasing cytokine production..while allowing the immune system to fight off the virus successfully.”
[cit. wikipedia]
— etienne monseigneure · Apr 26, 03:55 AM ·
This link will take you to an article published a few years ago. It investigates the possibility of avian (not swine) flu virus being used as a BW agent. Most of the same principles apply to the flu virus in general.
http://www.nti.org/e_research/e3_82.html
I support the posting of public health issues on arms control wonk. Not only for the international cooperation that could be required in dealing with a pandemic, but also for the dual-use nature of many pathogens and biotechnology techniques.
— Amanda Ducasse · Apr 26, 07:29 AM ·