by Anthony F. Hillen
May 12, 2007
from
Scribd Website
The world is on the cusp of a biotech revolution that portends a myriad of salubrious scientific breakthroughs that will undoubtedly change our lives for the better.
Nevertheless, some potentially
catastrophic security concerns are likely to accompany the
development of these otherwise propitious technological
achievements. History suggests that emerging political, business and
social structures are more adept at utilizing nascent technologies
than their more established counterparts.
The biotech revolution stands to
alter the conduct of warfare more dramatically than the infotech
revolution.
Biotechnology affords sub-state groups
the type of destructive power previously available only to the
superpowers. The production of biological weapons has become an
increasingly diffuse scientific enterprise since the end of the Cold
War, and as far as terrorists are concerned, they represent the
ultimate means of sewing political discord and instigating economic
disruption.
Deploying biological weapons has become exceedingly simple, their development is not capital-intensive and they do not require sophisticated delivery systems to be lethally effective.
Unlike
nuclear weapons that destroy everything within a certain
radius, biological weapons are uniquely advantageous in that they
can shutdown vital activity without destroying physical
infrastructure. At the height of its biological weapons program, the
Soviet Union had ICBMs loaded with several kilograms of highly
infectious pathogens processed into a powder finer than bath talc
that can drift in the air for miles at a time.
Pathogens are ideally dispersed in
an aerosol cloud of particles measuring about one to five microns in
diameter (in other words, a line of a hundred particles in a row
would scarcely equal the thickness of a human hair), inhaling just
one of these particles can be lethal.
In general, there are two types of biological weapons:
Modern research efforts aimed at
developing militarily effective biological agents often “weaponize”
certain diseases by increasing their pathogenicity and refining
their deliverability. Genetically altering the pathogenicity of
infectious organisms can boost their lethality and make them more
resistant to treatments and vaccines.
Weaponization can also involve a
refinement of the toxin’s means of delivery and release.
Biological weapons offer a great deal of
flexibility in terms of delivery systems, they can be unleashed on
their targets using missiles with toxin-loaded explosive warheads,
cluster-bombs, crop-dusting aircraft, vehicle-borne improvised
explosive devices, or even simple hand-delivery.
Several pathogens can be used as weapons, but the unique virulence of four toxins in particular suggests that they are the most likely candidates for weaponization.
The United States operated an offensive
biological weapons program at the United States Army Medical
Research Institute of Infectious Diseases (USAMRIID),
in Fort Detrick, Maryland.
President Nixon shut down the
program in 1969, for fear of pioneering weapons that could later be
turned against the United States or its allies. Although some of
them may have been designed to spread disinformation, a significant
number of news articles and journal publications since the 1970s
suggest that biological weapons are ineffective as a strategic
deterrent and operationally impractical at the tactical level.
Logic, however, suggests that those
assertions are incorrect.
Pathogens can be highly effective
weapons, researchers need only,
Alibekov insists that biological weapons
can be effective because he developed one: a durable, highly
infectious, and vaccine-resistant strain of Anthrax.
Should it choose to mount an attack on a densely populated metropolitan area, one of the challenges a rogue state or terrorist organization would face would be to locate individuals with the appropriate scientific background and then convincing (or more likely, coercing) them to support their cause. Very few individuals outside the United States and the former Soviet Union are technically competent enough to dry and process virus and bacteria samples into protectively-coated micro-particles capable of being inhaled.
Monitoring the employment and
international travel habits of scientists with backgrounds in fields
like micro-biology used to be relatively simple when they were
predominantly trained at Western universities and easily
identifiable. But after
the events of September 11, 2001
and the anthrax-letter attacks a month later, the US dramatically
curtailed its acceptance of foreigners to its universities and
research institutions.
International students seeking an
American education have been discouraged from doing so by recently
implemented visa restrictions and steadily increasing tuition costs.
However, it would be a negligent mistake for policy-makers to assume
that the expertise necessary for manipulating pathogens is
exclusively available in the West; there are a number of first-rate
biological science institutions around the world.
Furthermore the widespread availability
of online research data, including step-by-step production
protocols, means that terrorists can clandestinely obtain the
knowledge to produce biological weapons from practically anywhere.
Compared to the task of acquiring rare scientific expertise, obtaining the hardware necessary to produce biological weapons is surprisingly far less daunting. Research involving “hot” viruses (airborne infections without a known cure) like Ebola or Marburg virus, generally require a Bio-Safety Level 4 laboratory, facilities featuring multiple air-locked chambers with closely monitored directed air flow.
Technicians in BSL-4 labs wear
protective suits with individual oxygen supplies and work on samples
enclosed in a specialized cabinet with an air supply of its own.
Although the technical requirements associated with facilities
considered BSL-3 and above have been considered to be too demanding
for their construction in less developed countries, certain
technological breakthroughs allow modular mobile BSL-3 labs to be
constructed on short order and in the most inhospitable
environments.
Another disconcerting fact is that the
virus-propagating flasks known as “bioreactors”
are available for as little as $25 on eBay. Once produced,
delivering the pathogen to its target is relatively simple.
A “line-source laydown” by a modified
commercial helicopter or crop-dusting aircraft could disperse enough
weaponized powder over an open-air stadium or music concert to kill
thousands of people directly and hundreds of thousands indirectly
through contagious infection.
The global diffusion of information pertaining to the production of biological weapons is a serious cause for concern, but even more disconcerting is the relative simplicity of acquiring pathogenic organisms. Before genetically-modified viruses became the pathogen of choice for biological weapons, South African and Iraqi scientists were significantly impressed with the potential military value of naturally occurring and widely available pathogens.
Some of the more promising ones include:
The lethality and widespread
availability of such pathogens suggests that terrorists will likely
attempt to use them at some point in the future.
The small-scale production of pathogens
using cloning technology is another source of biological weapons
that has been negligently underestimated.
Once a disease-causing gene has been
identified and its location published in an academic journal,
scientists or terrorists can use cloning kits (available from
typical lab equipment catalogs) to clone that gene and then splice
it into a common host bacteria.
Emerging Defense Technologies The biotech revolution has spawned a number of cutting-edge technologies; some of which could potentially provide a significant advantage against the threat of biological weapons.
The US Defense Advanced Research
Projects Agency (DARPA)
realized the significance of biotechnology for defense applications
in the mid-1990s. By 1999 the agency funded more than $40 million
dollars worth of bio-defense research projects. That budget grew to
nearly $150 million in 2002, primarily due to DARPA Director
Larry Lynn’s emphasis on pathogen countermeasures. (Marshall)
In 1996 DARPA began funding a project that focused on removing foreign bodies from the bloodstream, a concept originally developed by Dr. Ronald Taylor at Dartmouth University. According to Taylor, a receptor located on the surface of red blood cells known as CR1, is primarily responsible for removing materials that the immune system’s complement-cascade-proteins have tagged as foreign.
The alien substances are then bound to
the CR1 receptor and flushed out of the body through the liver. This
particular technology has the potential to purge any known virus
from the human body in less than two hours.
Another ambitious research effort bankrolled by DARPA in the late 1990s involved manipulating mesenchymal stem cells to detect and respond to biological threats. Mesenchymal stem cells constitute the primary source of bone, cartilage, fat, and muscle tissue. The general idea is that these cells can be “preprogrammed” with a number of transplanted genes, which would then populate the tissues of the recipient into which they are injected.
Theoretically, these cells could
identify specific pathogens and activate certain genes to trigger a
curative biological response. This approach circumvents the
troublesome need for multiple injections, depending instead on cells
engineered to automatically vaccinate the body against pathogens.
The primary drawback of such methods is their dependence on the
pharmaceutical industry.
DARPA may fund their initial research
and development, but it is unlikely to provide the financing
necessary to transform prototype vaccines into functional and
available countermeasures to biological weapons.
According to its FY-2007 budget expenditures, DARPA invested heavily in three specific “bug to drug” research endeavors.
However, DARPA evidently perceives that
to be a surmountable obstacle, investing heavily in its
Accelerated Manufacturing of Pharmaceuticals program, intent on
exploring various challenging but technologically feasible methods
of producing millions of doses of a complex new therapeutic in 12
weeks or less.
Although unrelated to any current DARPA initiatives of which the author is aware, there is another very promising, albeit relatively long term and unconventional, approach to pathogen countermeasures.
This approach would involve the use of
inhibitors to disrupt protein enzymes such as proteases which are
instrumental to pathogenic invasion. For instance, the botulinum
toxin could be effectively neutralized by using inhibitors to
target the zinc endopeptidase in its light chain (the
polypeptide subunit of an antibody). Similarly, anthrax could also
be detoxified with inhibitors, by using them to target the source of
its lethality: zinc protease.
The diffuse applicability of this
approach hinges on the fact that all pathogen invasions are
enzyme-contingent.
The pathogenic enzymes can be inhibited
without the risk of crippling those required for normal functions,
primarily due to the characteristically high substrate specificity
among viral and bacterial enzymes. Although the validity of this
approach has been repeatedly confirmed by the clinical use of
protease inhibitors to successfully treat infections, at present it
must be considered a long-term solution. By today’s technological
standards, it takes about ten years to produce an effective protease
inhibitor.
However, that development time could be
drastically reduced by using advanced supercomputers in the drug
discovery process.
One final emerging technology that may prove to be invaluable against an adversary armed with biological weapons is the Femtosecond Adaptive Spectroscopy Techniques for Remote Agent Detection (FASTREAD).
The FASTREAD program is designed to
detect biological agents at a standoff distance using coherent
nonlinear optical spectroscopy, laser pulse shaping techniques, and
adaptive optics in conjunction with other efforts to better
elucidate the agent under interrogation, such as return signal
optimization strategies.
Primarily based on coherence theory (the
optical effects resulting from partially coherent light and radio
sources), FASTREAD exploits the spectral and temporal information
provided by the backscatter from short-pulse lasers to identify
specific biological agents.
The system is extremely promising but
must first overcome several technological and developmental
challenges before its true potential can be fully realized.
Nuclear vs.
Biological Weapons
A common misconception among technologists is that human beings reached the zenith of their destructive power with the advent of the hydrogen bomb.
When comparing these weapons of mass
destruction, one should keep in mind that the destruction wrought by
a single nuclear weapon is inherently limited by the laws of
physics, whereas a highly contagious biological weapon has neither a
calculated blast radius nor an upper limit death-toll.
At first glance, states seem to have
typically abided by the rules of the 1972 Biological Weapons
Convention (BWC) that categorically banned the production of
biological weapons. The 1968 Nuclear Non-Proliferation Treaty
(NPT), on the other hand, appears to have been somewhat less
successful. However, such perceptions can be misleading; the reality
is that they are probably equally dysfunctional.
The BWC has likely been violated more than the general public will ever know or want to know, but although the NPT is probably violated less often, its occasional infractions are highly publicized due to the compliance watchdog known as the International Atomic Energy Agency, the paladin of the NPT, capable of referring violators to the UN Security Council.
The fact that the BWC lacks a
counterpart institution to the IAEA may suggest a simple and
reasonable explanation for the regimes regulatory weakness. One
might go as far as to say that the evidence supports the efficacy of
institutional oversight mechanisms in enforcing arms control
regimes, but it would be slightly presumptuous to hastily make that
conclusion as it fails to take one important factor into account.
There is a logical reason why more
states do not “go nuclear”, and it has very little to do with the
NPT. Unless motivated by strategic concerns or nationalist impulses,
countries like Uganda, Sri Lanka, or Chile refrain from developing
nuclear arsenals because they would gain nothing (except
international condemnation and notoriety) and it would cost them
everything (politically and economically).
Recent members of the nuclear club, like
Pakistan and India, maneuvered themselves into a security dilemma
destined to result in the mutual development of nuclear weapons,
whereas South Africa geopolitically isolated itself to the point
that it had nothing to lose by building the bomb.
The new “club” members also had a
technological head-start in their nuclear development: the US “Atoms
for Peace” program.
However, it is highly unlikely that a
sub-state actor could obtain the materials and expertise necessary
to manufacture nuclear weapons, especially when one considers that,
even when supported by the resources available to an entire
nation-state, developing nuclear weapons represents a political,
financial, and especially technological feat of the highest order.
Terrorists are unlikely to pursue nuclear weapons when a cheaper and potentially more potent alternative exists. Not only are they technically daunting to manufacture, nuclear weapons generally require elaborate and cost-prohibitive delivery systems.
Thus, for a suicidal sub-state actor
intent on indiscriminately killing as many people as possible, a
nuclear weapon is neither feasible nor desirable.
Conclusion The anthrax attack on Capitol Hill in October 2001 provided stark evidence that biological weapons can allow a single individual with an unknown cause to attack and inflict significant damage on a nation-state.
That particular attack may not have
killed scores of people, but for only a few ounces of anthrax and
postage stamp, the attacker managed to disrupt Congress for several
months, ramp up operating costs for the USPS (and federal
government) by imposing additional screening requirements, and
incurred hundreds of millions of dollars worth of clean up costs.
One could hardly ask for a more cost
effective weapon to advance one’s political agenda. If the
biological weapon enclosed in those envelopes were weaponized
smallpox, a single envelope could have resulted in three times the
casualties on September 11th alone. With the necessary expertise and
equipment, increasing the virus’ pathogenicity would not be
difficult, the complete smallpox genome can be found online in less
than ten minutes.
In 2001, the US DoD conducted an exercise code-named “Dark Winter”, simulating the effect of a smallpox attack against three US metropolitan areas. In less than two weeks, the disease infected 25 states and had already spread to 15 different countries in several epidemiological waves that left several hundred thousand Americans dead.
The exercise was terminated prematurely
when authorities calculated that a fourth generation of the disease
would have resulted in the infection of 3 million people, killing at
least a third of them. Biological weapons are capable of killing
many more people than a nuclear attack. Given the current trend
in biotechnology, small groups or perhaps even individuals may soon
be able to take the sort of virus used in the “Dark Winter”
simulation and increase its lethality three-fold.
Traditional arms control regimes are unlikely to be efficient in preventing the covert development of biological weapons programs by either state or sub-state actors.
The last effort to revise the 1975
Biological and Toxic Weapons Convention was in 2002. A draft
protocol was submitted but the United States rejected it out of
hand, asserting that it did not strengthen existing arms control
strategies, benefited potential proliferators, and compromised
American national security as well as proprietary business
information.
An alternate approach to these antiquated, Cold War-era control strategies could involve categorizing potential threats based on their geographic origin, individually customizing the security resources dedicated to each category.
For example,
The biotech revolution is already
underway, but the risks and dangers which will surely accompany it
have only just begun to reveal themselves.
With the dawning of new technological
eras come new and previously unimaginable threats, often taking the
form of sociopolitical or military challenges. Dual-use emerging
technologies could potentially provide militant organizations or
groups of disaffected individuals with highly effective means of
challenging state-level actors.
The strategically disruptive effect this
could have on the geopolitical environment merits serious
consideration by policy-makers and the scientific community in
general.
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Huwebes, Mayo 31, 2012
BIOLOGICAL WEAPONS
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