DNA Pollution May
Be Spawning Killer Microbes
Copyright Jessica Snyder
Sachs
Originally
published in Discover magazine, March 2008
Rogue genetic
snippets spread antibiotic resistance all over the environment.
On a bright winter morning high in the Colorado Rockies, a slight young woman in oversize hip boots sidles up to a gap of open water in the icy Cache la Poudre River. Heather Storteboom, a 25-year-old graduate student at nearby Colorado State University, is prospecting for clues to an invisible killer.
Heather Storteboom on the Poudre, photo by JSSachsStorteboom snaps
on a pair of latex gloves and stretches over the frozen ledge to fill a sterile
plastic jug with water. Then, setting the container aside, she swings her
rubber-clad legs into the stream. "Ahh, no leaks," she says, standing
upright. She pulls out a clean trowel and attempts to collect some bottom
sediment; in the rapid current, it takes a half dozen tries to fill the small
vial she will take back to the DNA laboratory of her adviser, environmental
engineer Amy Pruden. As Storteboom packs to leave, a curious hiker approaches.
"What were you collecting?" he asks. "Antibiotic resistance
genes," she answers.
Storteboom and
Pruden are at the leading edge of an international forensic investigation into
a potentially colossal new health threat: DNA pollution. Specifically, the
researchers are seeking out snippets of rogue genetic material that transforms
annoying bacteria into unstoppable supergerms, immune to many or all modern
antibiotics. Over the past 60 years, genes for antibiotic resistance have gone
from rare to commonplace in the microbes that routinely infect our bodies. The
newly resistant strains have been implicated in some 90,000 potentially fatal
infections a year in the United States, higher than the number of automobile
and homicide deaths combined.
Among the most
frightening of the emerging pathogens is invasive MRSA, or
methicillin-resistant Staphylococcus aureus. Outbreaks of MRSA in public
schools recently made headlines, but that is just the tip of the iceberg.
Researchers estimate that invasive MRSA kills more than 18,000 Americans a
year, more than AIDS, and the problem is growing rapidly. MRSA caused just 2
percent of staph infections in 1974; in the last few years, that figure has
reached nearly 65 percent. Most reported staph infections stem from MRSA born
and bred in our antibiotic-drenched hospitals and nursing homes. But about 15
percent now involve strains that arose in the general community.
It is not just
MRSA that is causing concern; antibiotic resistance in general is spreading
alarmingly. A 2003 study of the mouths of healthy kindergartners found that 97
percent harbored bacteria with genes for resistance to four out of six tested
antibiotics. In all, resistant microbes made up around 15 percent of the
children's oral bacteria, even though none of the children had taken
antibiotics in the previous three months. Such resistance genes are rare to
nonexistent in specimens of human tissue and body fluid taken 60 years ago,
before the use of antibiotics became widespread.
In part, modern
medicine is paying the price for its own success. "Antibiotics may be the
most powerful evolutionary force seen on this planet in billions of
years," says Tufts University microbiologist Stuart Levy, author of The
Antibiotic Paradox: How the Misuse of Antibiotics Destroys Their Curative
Powers. By their nature, antibiotics support the rise of any bug that can shrug
off their effects, by conveniently eliminating the susceptible competition.
But the rapid
rise of bacterial genes for drug resistance stems from more than lucky
mutation, Levy adds. The vast majority of these genes show a complexity that
could have been achieved only over millions of years. Rather than rising anew
in each species, the genes spread via the microbial equivalent of sexual
promiscuity. Bacteria swap genes, not only among their own kind but also
between widely divergent species, Levy explains. Bacteria can even scavenge the
naked DNA that spills from their dead compatriots out into the environment.
The result is a microbial
arms-smuggling network with a global reach. Over the past 50 years, virtually
every known kind of disease-causing bacterium has acquired genes to survive
some or all of the drugs that once proved effective against it. Analysis of a
strain of vancomycin-resistant enterococcus, a potentially lethal bug that has
invaded many hospitals, reveals that more than one-quarter of its
genome-including virtually all its antibiotic-thwarting genes-is made up of
foreign DNA. One of the newest banes of U.S. medical centers, a supervirulent
and multidrug-resistant strain of Acinetobacter baumannii, likewise appears to
have picked up most of its resistance in gene swaps with other species.
So where in Hades
did this devilishly clever DNA come from? The ultimate source may lie in the
dirt beneath our feet.
For the past
decade, Gerry Wright has been trying to understand the rise of drug resistance
by combing through the world's richest natural source of resistance-enabling
DNA: a clod of dirt. As the head of McMaster University's antibiotic research
center in Hamilton, Ontario, Wright has the most tricked-out laboratory a drug
designer could want, complete with a $15 million high-speed screening facility
for simultaneously testing potential drugs against hundreds of bacterial
targets. Yet he says his technology pales in comparison with the elegant
antibiotic-making abilities he finds encoded in soil bacteria. The vast
majority of the antibiotics stocking our pharmacy shelves-from old standards
like tetracycline to antibiotics of last resort like vancomycin and, most
recently, daptomycin-are derived from soil organisms.
Biologists assume
that soil organisms make antibiotics to beat back the microbial competition and
to establish their territory, Wright says, although the chemicals may also
serve other, less-understood functions. Whatever the case, Wright and his
students began combing through the DNA of soil microbes like streptomyces to
better understand their impressive antibiotic-making powers. In doing so the
researchers stumbled upon three resistance genes embedded in the DNA that
Streptomyces toyocaensis uses to produce the antibiotic teicoplanin. While
Wright was not surprised that the bug would carry such genes as antidotes to
its own weaponry, he was startled to see that the antidote genes were nearly
identical to the resistance genes in vancomycin-resistant enterococcus (VRE),
the scourge of American and European hospitals.
+++
"Yet here
they were in a soil organism, in the exact same orientation as you find in the
genome of VRE," Wright says. "That sure gave us a head-slap moment.
If only we had done this experiment 15 years ago, when vancomycin came into
widespread use, we might have understood exactly what kind of resistance
mechanisms would follow the drug into our clinics and hospitals." If
nothing else, that foreknowledge might have prepared doctors for the inevitable
resistance they would encounter soon after vancomycin was broadly prescribed.
Wright wondered what else he might find in a shovelful of dirt. So he handed out plastic bags to students departing on break, telling them to bring back soil samples. Over two years his lab amassed a collection that spanned the continent. It even included a thawed slice of tundra mailed by Wright's brother, a provincial policeman stationed on the northern Ontario-Manitoba border.
By 2005 Wright's
team had combed through the genes of nearly 500 streptomyces strains and
species, many never before identified. Every one proved resistant to multiple
antibiotics, not just their own signature chemicals. On average, each could
neutralize seven or eight drugs, and many could shrug off 14 or 15. In all, the
researchers found resistance to every one of the 21 antibiotics they tested,
including Ketek and Zyvox, two synthetic new drugs.
"These genes
clearly didn't jump directly from streptomyces into disease-causing
bacteria," Wright says. He had noted subtle variations between the
resistance genes he pulled out of soil organisms and their doppelgangers in
disease-causing bacteria. As in a game of telephone, each time a gene gets
passed from one microbe to another, slight differences develop that reflect the
DNA dialect of its new host. The resistance genes bedeviling doctors had
evidently passed through many intermediaries on their way from soil to
critically ill patients.
Wright suspects
that the antibiotic-drenched environment of commercial livestock operations is
prime ground for such transfer. "You've got the genes encoding for
resistance in the soil beneath these operations," he says, "and we
know that the majority of the antibiotics animals consume get excreted
intact." In other words, the antibiotics fuel the rise of resistant
bacteria both in the animals' guts and in the dirt beneath their hooves, with
ample opportunity for cross-contamination.
Nobody knows how
long free-floating DNA might persist in the water.
A 2001 study by
University of Illinois microbiologist Roderick Mackie documented this flow.
When he looked for tetracycline resistance genes in groundwater downstream from
pig farms, he also found the genes in local soil organisms like Microbacterium
and Pseudomonas, which normally do not contain them. Since then, Mackie has
found that soil bacteria around conventional pig farms, which use antibiotics,
carry 100 to 1,000 times more resistance genes than do the same bacteria around
organic farms.
"These animal operations are real hot spots," he says. "They're glowing red in the concentrations and intensity of these genes." More worrisome, perhaps, is that Mackie pulled more resistance genes from his deepest test wells, suggesting that the genes percolated down toward the drinking water supplies used by surrounding communities.
An even more
direct conduit into the environment may be the common practice of irrigating fields
with wastewater from livestock lagoons. About three years ago, David Graham, a
University of Kansas environmental engineer, was puzzled in the fall by a
dramatic spike in resistance genes in a pond on a Kansas feedlot he was
studying. "We didn't know what was going on until I talked with a
large-animal researcher," he recalls. At the end of the summer, feedlots
receive newly weaned calves from outlying ranches. To prevent the young animals
from importing infections, the feedlot operators were giving them five-day
"shock doses" of antibiotics. "Their attitude had been, cows are
big animals, they're pretty tough, so you give them 10 times what they
need," Graham says.
The operators cut
back on the drugs when Graham showed them that they were coating the next
season's alfalfa crop with highly drug-resistant bacteria. "Essentially,
they were feeding resistance genes back to their animals," Graham says.
"Once they realized that, they started being much more conscious. They
still used antibiotics, but more discriminately."
While livestock
operations are an obvious source of antibiotic resistance, humans also take a
lot of antibiotics-and their waste is another contamination stream. Bacteria
make up about one-third of the solid matter in human stool, and Scott Weber, of
the State University of New York at Buffalo, studies what happens to the
antibiotic resistance genes our nation flushes down its toilets.
Conventional
sewage treatment skims off solids for landfill disposal, then feeds the liquid
waste to sewage-degrading bacteria. The end result is around 5 billion pounds
of bacteria-rich slurry, or waste sludge, each year. Around 35 percent of this
is incinerated or put in a landfill. Close to 65 percent is recycled as
fertilizer, much of it ending up on croplands.
+++
Weber is now investigating how fertilizer derived from human sewage may contribute to the spread of antibiotic-resistant genes. "We've done a good job designing our treatment plants to reduce conventional contaminants," he says. "Unfortunately, no one has been thinking of DNA as a contaminant." In fact, sewage treatment methods used at the country's 18,000-odd wastewater plants could actually affect the resistance genes that enter their systems.
Every tested
strain in a dirt sample proved resistant to multiple antibiotics.
Most treatment
plants, Weber explains, gorge a relatively small number of sludge bacteria with
all the liquid waste they can eat. The result, he found, is a spike in
antibiotic-resistant organisms. "We don't know exactly why," he says,
"but our findings have raised an even more important question." Is
the jump in resistance genes coming from a population explosion in the
resistant enteric, or intestinal, bacteria coming into the sewage plant? Or is
it coming from sewage-digesting sludge bacteria that are taking up the genes
from incoming bacteria? The answer is important because sludge bacteria are
much more likely to thrive and spread their resistance genes once the sludge is
discharged into rivers (in treated wastewater) and onto crop fields (as
slurried fertilizer).
Weber predicts
that follow-up studies will show the resistance genes have indeed made the jump
to sludge bacteria. On a hopeful note, he has shown that an alternative method
of sewage processing seems to decrease the prevalence of bacterial drug
resistance. In this process, the sludge remains inside the treatment plant
longer, allowing dramatically higher concentrations of bacteria to develop. For
reasons that are not yet clear, this method slows the increase of drug-resistant
bacteria. It also produces less sludge for disposal. Unfortunately, the process
is expensive.
Drying sewage
sludge into pellets-which kills the sludge bacteria-is another way to contain
resistance genes, though it may still leave DNA intact. But few municipal
sewage plants want the extra expense of drying the sludge, and so it is instead
exported "live" in tanker trucks that spray the wet slurry onto crop
fields, along roadsides, and into forests.
Trolling the
waters and sediments of the Cache la Poudre, Storteboom and Pruden are
collecting solid evidence to support suspicions that both livestock operations
and human sewage are major players in the dramatic rise of resistance genes in
our environment and our bodies. Specifically, they have found unnaturally high
levels of antibiotic resistance genes in sediments where the river comes into
contact with treated municipal wastewater effluent and farm irrigation runoff
as it flows 126 miles from Rocky Mountain National Park through Fort Collins and
across Colorado's eastern plain, home to some of the country's most densely
packed livestock operations.
"Over the
course of the river, we saw the concentration of resistance genes increase by
several orders of magnitude," Pruden says, "far more than could ever
be accounted for by chance alone." Pruden's team likewise found dangerous
genes in the water headed from local treatment plants toward household taps.
Presumably, most
of these genes reside inside live bacteria, but a microbe doesn't have to be alive
to share its dangerous DNA. As microbiologists have pointed out, bacteria are
known to scavenge genes from the spilled DNA of their dead.
"There's a
lot of interest in whether there's naked DNA in there," Pruden says of the
Poudre's waters. "Current treatment of drinking water is aimed at killing
bacteria, not eliminating their DNA." Nobody even knows exactly how long
such free-floating DNA might persist.
All this makes
resistance genes a uniquely troubling sort of pollution. "At least when
you pollute a site with something like atrazine," a pesticide, "you
can be assured that it will eventually decay," says Graham, the Kansas
environmental engineer, who began his research career tracking chemical
pollutants like toxic herbicides. "When you contaminate a site with
resistance genes, those genes can be transferred into environmental organisms
and actually increase the concentration of contamination."
Taken together,
these findings drive home the urgency of efforts to reduce flagrant antibiotic
overuse that fuels the spread of resistance, whether on the farm, in the home,
or in the hospital.
For years the
livestock pharmaceutical industry has played down its role in the rise of
antibiotic resistance. "We approached this problem many years ago and have
seen all kinds of studies, and there isn't anything definitive to say that
antibiotics in livestock cause harm to people," says Richard Carnevale,
vice president of regulatory and scientific affairs at the Animal Health
Institute, which represents the manufacturers of animal drugs, including those
for livestock. "Antimicrobial resistance has all kinds of sources, people
to animals as well as animals to people."
The institute's
own data testify to the magnitude of antibiotic use in livestock operations,
however. Its members sell an estimated 20 million to 25 million pounds of
antibiotics for use in animals each year, much of it to promote growth. (For
little-understood reasons, antibiotics speed the growth of young animals,
making it cheaper to bring them to slaughter.) The Union of Concerned
Scientists and other groups have long urged the United States to follow the
European Union, which in 2006 completed its ban on the use of antibiotics for
promoting livestock growth. Such a ban remains far more contentious in North
America, where the profitability of factory-farm operations depends on getting
animals to market in the shortest possible time.
+++
On the other
hand, the success of the E.U.'s ban is less than clear-cut. "The studies
show that the E.U.'s curtailing of these compounds in feed has resulted in more
sick animals needing higher therapeutic doses," Carnevale says.
"There are
cases of that," admits Scott McEwen, a University of Guelph veterinary
epidemiologist who advises the Canadian government on the public-health
implications of livestock antibiotics. At certain stressful times in a young
animal's life, as when it is weaned from its mother, it becomes particularly
susceptible to disease. "The lesson," he says, "may be that we
would do well by being more selective than a complete ban."
McEwen and many
of his colleagues see no harm in using growth-promoting livestock antibiotics
known as ionophores. "They have no known use in people, and we see no
evidence that they select for resistance to important medical
antibiotics," he says. "So why not use them? But if anyone tries to
say that we should use such critically important drugs as cephalosporins or
fluoroquinolones as growth promoters, that's a no-brainer. Resistance develops
quickly, and we've seen the deleterious effects in human health."
A thornier issue
is the use of antibiotics to treat sick livestock and prevent the spread of
infections through crowded herds and flocks. "Few people would say we
should deny antibiotics to sick animals," McEwen says, "and often the
only practical way to administer an antibiotic is to give it to the whole
group." Some critics have called for restricting certain classes of
critically important antibiotics from livestock use, even for treating sick
animals. For instance, the FDA is considering approval of cefquinome for
respiratory infections in cattle. Cefquinome belongs to a powerful class of
antibiotic known as fourth-generation cephalosporins, introduced in the 1990s
to combat hospital infections that had grown resistant to older drugs. In the
fall of 2006, the FDA's veterinary advisory committee voted against approving
cefquinome, citing concerns that resistance to this vital class of drug could
spread from bacteria in beef to hospital superbugs that respond to little else.
But the agency's recently adopted guidelines make it difficult to deny approval
to a new veterinary drug unless it clearly threatens the treatment of a
specific foodborne infection in humans. As of press time, the FDA had yet to
reach a decision.
Consumers may
contribute to the problem of DNA pollution whenever they use antibacterial
soaps and cleaning products. These products contain the antibiotic-like
chemicals triclosan and triclocarban and send some 2 million to 20 million
pounds of the compounds into the sewage stream each year. Triclosan and
triclocarban have been shown in the lab to promote resistance to medically
important antibiotics. Worse, the compounds do not break down as readily as do
traditional antibiotics. Rolf Halden, cofounder of the Center for Water and
Health at Johns Hopkins University, has shown that triclosan and triclocarban
show up in many waterways that receive treated wastewater-more than half of the
nation's rivers and streams. He has found even greater levels of these two
chemicals in sewage sludge destined for reuse as crop fertilizer. According to
his figures, a typical sewage treatment plant sends more than a ton of
triclocarban and a slightly lesser amount of triclosan back into the
environment each year.
For consumer
antibacterial soaps the solution is simple, Halden says: "Eliminate them.
There's no reason to have these chemicals in consumer products." Studies
show that household products containing such antibacterials don't prevent the
spread of sickness any better than ordinary soap and water. "If there's no
benefit, then all we're left with is the risk," Halden says. He notes that
many European retailers have already pulled these products from their shelves.
"I think it's only a matter of time before they are removed from U.S.
shelves as well."
Consumers may
contribute to the problem of DNA pollution whenever they use soaps and cleaning
products containing antibiotic-like compounds.
Finally, there is
the complicated matter of the vast quantity of antibiotics that U.S. doctors
prescribe each year: some 3 million pounds, according to the Union of Concerned
Scientists. No doctor wants to ignore an opportunity to save a patient from
infectious disease, yet much of what is prescribed is probably unnecessary-and
all of it feeds the spread of resistance genes in hospitals and apparently
throughout the environment.
"Patients
come in asking for a particular antibiotic because it made them feel better in
the past or they saw it promoted on TV," says Jim King, president of the
American Academy of Family Physicians. The right thing to do is to educate the
patient, he says, "but that takes time, and sometimes it's easier, though
not appropriate, to write the prescription the patient wants."
Curtis Donskey,
chief of infection control at Louis Stokes Cleveland VA Medical Center, adds
that "a lot of antibiotic overuse comes from the mistaken idea that more
is better. Infections are often treated longer than necessary, and multiple
antibiotics are given when one would work as well." In truth, his studies
show, the longer hospital patients remain on antibiotics, the more likely they
are to pick up a multidrug-resistant superbug. The problem appears to lie in
the drugs' disruption of a person's protective microflora-the resident bacteria
that normally help keep invader microbes at bay. "I think the message is
slowly getting through," Donskey says. "I'm seeing the change in
attitude."
Meanwhile,
Pruden's students at Colorado State keep amassing evidence that will make it
difficult for any player-medical, consumer, or agricultural-to shirk
accountability for DNA pollution.
Late in the
afternoon, Storteboom drives past dairy farms and feedlots, meatpacking plants,
and fallow fields, 50 miles downstream from her first DNA sampling site of the
day. Leaving her Jeep at the side of the road, she strides past cow patties and
fast-food wrappers and scrambles down an eroded embankment of the Cache la
Poudre River. She cringes at the sight of two small animal carcasses on the
opposite bank, then wades in, steering clear of an eddy of gray scum.
"Just gross," she mutters, grateful for her watertight hip boots.
Of course, the
invisible genetic pollution is of greater concern. It lends an ironic twist to
the river's name. According to local legend, the appellation comes from the
hidden stashes (cache) of gunpowder (poudre) that French fur trappers once
buried along the banks. Nearly two centuries later, the river's hidden DNA may
pose the real threat.
Jessica Snyder Sachs is the author of Good Germs, Bad Germs: Health and Survival in a Bacterial World, published in fall 2007 by Hill & Wang, a division of Farrar, Strauss and Giroux. Her last feature for Discover looked at how antibiotics affect the body's bacterial ecosystem.
