When a viral infection spread through five genetically identical mice
in a row, the virus replicated faster and became more virulent or
severe. But when the infection spread one-by-one through five
genetically diverse mice, the virus had trouble adapting and became less
virulent. By showing this long-suspected mechanism holds true within a
single species of vertebrate animal, namely, mice, the University of
Utah study suggests that increased genetic diversity should be promoted
in livestock and in captive-bred endangered species so as to limit their
risk of getting deadly infections.
“This study showed a surprising rapid and large effect of genetic
diversity in mice that dramatically reduced the replication of virus
infecting the mice and the severity of disease caused by the virus,”
says biology professor Wayne Potts. He is senior author of the study
published online this month in the British journal Proceedings of the Royal Society B.
“There’s a reason we are not clones of our mom and dad,” says the
study’s first author, Jason Kubinak, a postdoctoral fellow in biology.
“Among other reasons, it’s because mechanisms that promote genetic
differences between us probably protect us from more severe infectious
disease.”Indeed, Potts and Kubinak say their study’s findings support
the “sex-against virulence hypothesis.” It argues that sexual
reproduction, which promotes genetic diversity, may have evolved as a
way to counter the ability of viruses and other pathogens to rapidly
adapt to their hosts and gain virulence.
“The idea is that sexual reproduction produces different genetic
makeups in all the kids so they are different than mom’s and dad’s, and
therefore become more difficult to infect,” Potts says. “Our study
simulates this condition. The inbred mouse strain is like an asexual
line because they all have the same genetic makeup. This is one of the
first empirical demonstrations of how pathogens could make it so that
sexual reproduction had great benefits in providing resistance to
diseases.”(Another hypothesis is that sexual reproduction evolved to
effectively weed out many of the harmful genetic mutations that occur
every generation.)Kubinak and Potts conducted the research with
University of Utah colleagues Douglas Cornwall, a doctoral student in
biology, and Fred Adler, a professor of mathematics and biology, along
with virologist Kim Hasenkrug, of Rocky Mountain Laboratories, a
Hamilton, Montana, lab of the National Institutes of Health. The study
was funded by the National Science Foundation and National Institutes of
Health.
Of Mice and an Unfriendly Virus
Researchers previously showed in plants and insects that a virus
replicates faster and becomes more virulent when it rapidly adapts to
the “host” it infects because the host species has low genetic
diversity. Potts says it hasn’t been shown before in a vertebrate
species, although “it had been theoretically predicted for over two
decades.”“This is the first time that anyone has shown that genetic
variation within a single vertebrate animal species strongly inhibits
replication of a virus and the severity of disease it causes,” Kubinak
says.The virus used in the study is known as the Friend virus complex,
and is often used for studying viral infection. It is a combination of a
mouse leukemia virus named Friend virus and “spleen focus-forming
virus,” which causes a rapid increase in the number of red blood cells
in the mouse spleen, leading to spleen enlargement that can kill
infected mice, Kubinak says.The spleen virus can’t replicate by itself,
but it can if it co-infects a host cell with the Friend virus, borrowing
proteins from it to form new spleen virus particles.The mice used in
the study all belonged to one species, Mus musculus, but were
from seven different strains or breeds, each with numerous genetic
differences, including their colors and their resistance to the Friend
virus complex.In their experiments, the researchers infected mice with
virus from the spleen tissue of a previously infected mouse. They
measured viral fitness by counting how fast the virus replicated (by
counting viral genetic blueprints in the infected spleens), and measured
virulence by weighing the spleens; the more virulent the virus, the
larger the spleen.In a key experiment, the researchers passed the virus
through five mice of one strain, though five mice of another strain,
through five mice of five different strains and through another set of
five mouse strains in different order. In each case, the spleen from the
fifth mouse was used to infect 10 other mice, which were studied 10 to
12 days later for their viral loads (fitness, or how much the virus
replicated) and spleen weights (virulence, or how severely the mice were
harmed by the disease).“We found there was a significant increase in
viral replication and disease severity when a virus was passed through
mice of the same breed,” Kubinak says. “But the virus exposed to
different mouse breeds was unable to increase its reproduction or cause
more severe disease.”Potts says the theory is that the Friend virus
complex, with a small genetic blueprint, mutates rapidly, and variations
in genes are favored that allow the virus to do well in mouse A. But
the virus then infects mouse B, and traits that helped it in mouse A may
hurt it in mouse B.The researchers now are attempting to identify
genetic changes in the virus as it tried to adapt to mice with diverse
genes.
Protecting Livestock and Endangered Species
Kubinak says the
findings impinge on “risks relevant to global food security. We increase
the human population by 80 million people per year, and over the next
century we are expected to increase the global human population to 11
billion or 12 billion. The big question is, how are we going to feed
them all?”Modern society now breeds “large numbers of animals housed in
extremely close proximity to each other, and they have very limited
genetic diversity: cattle, pigs, poultry – any of the major livestock
species,” Kubinak says. “Livestock have been around since the dawn of
agriculture, but high-intensity farming practices really have emerged
within the past few decades, and we are going to become more reliant on
these farming practices in the future to feed 12 billion people.”The
trouble is, experiments like those in the new study “imply that in these
low-diversity, high-density settings, you may promote the emergence of
more virulent infectious diseases, which puts people who work with those
animals at immediate risk and the people who eat that food at indirect
risk.”With diseases like hoof and mouth already a big concern for
livestock, “instead of using a limited set of breeds, maybe using
multibreed herds might limit the ability of a pathogen in that setting
to become highly virulent,” Kubinak says. “This also may reduce
resistance to antibiotics that develops when livestock are given the
drugs to prevent infection and promote growth.”Potts says 25 percent of
all vertebrate species will be endangered by 2050, and “unfortunately,
captive-bred endangered species that are reintroduced into the wild have
a high rate of failure – near 80 percent. There are a number of
hypotheses as to why. One of them is that due to low genetic diversity
created by the collapsing population size that made them endangered,
they make an easier target for parasites and pathogens.”He adds: “This
suggests that the captive-breeding programs and reintroduction programs
should maximize genetic diversity. Once we identify which host genes are
important – and we assume it will be immune system genes –
captive-breeding programs could maximize diversity of these critical
immune system genes.”
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