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9 FEBRUARY 2010
The "secret weapon" of retroviruses that cause cancer
Oncogenic retroviruses are a particular family of viruses that can cause some types of cancer. Thierry Heidmann and his colleagues in the CNRS-Institut Gustave Roussy-Université Paris Sud 11 "Rétrovirus endogènes et éléments rétroïdes des eucaryotes supérieurs" Laboratory have studied these viruses. They have identified a "virulence factor" that inhibits the host immune response and allows the virus to spread throughout the body. This factor is a sequence of amino acids that is located in the envelope protein of the virus. These scientists have also shown that once mutated to lose its immunosuppressive capability, this envelope protein could serve as a basis for the development of vaccines. These findings have been published online in the Proceedings of the National Academy of Sciences USA, monday 8 february 2010.
Retroviruses
are viruses whose genome is made up of RNA. These viruses are unique in
possessing an enzyme that enables synthesis from this RNA of a DNA molecule
capable of integrating into the DNA of a host cell. The retrovirus then
utilizes the cell machinery to replicate. HIV is one of the best-known
retroviruses. Oncogenic retroviruses (or oncoretroviruses) are
cancer-causing viruses. Numerous oncoretroviruses are associated with
animal diseases. In humans, two retroviruses, called HTLV and XMRV, have
been associated with a type of leukemia and with prostate cancer.
Researchers
in the Rétrovirus Endogènes et Eléments Rétroïdes des Eucaryotes Supérieurs
Laboratory (1), headed by Thierry Heidmann, CNRS Senior Researcher at Institut
Gustave Roussy, have been working on the ability of retroviruses to propagate
and persist in their hosts by escaping the immune system. They have
studied the molecular basis of this process, and have shown that it is driven
by the envelope protein of these viruses. First of all, this protein has
an essential "mechanical" role, as it induces the fusion of viral
particles with the target cell membrane, thus allowing them to penetrate into
the cell. Using a mouse model of infection with a murine leukemia virus,
the researchers showed that this envelope protein also has a second role that
is equally essential to viral propagation in the body: it is immunosuppressive,
or in other words it inhibits the host immune response in a radical manner,
affecting both the "innate" and "adaptive" immune
responses.
The
researchers succeeded in locating the domain responsible for this property
within the amino acid sequence of the envelope protein. This domain, an
authentic virulence factor, is a crucial element in the arsenal that enables
retroviruses to invade their host and produce their pathogenic effect. It
thus becomes a target of choice for the design of novel antiretroviral
therapeutic strategies, including vaccines. The results obtained by these
scientists mean it will be possible to follow this path. They were able
to introduce targeted point mutations into the envelope protein that could suppress
its ability to inhibit the immune system which, as expected, reacted much more
effectively than with the non-mutated protein, producing a high level of antibodies
and inducing antiviral cellular immunity. By working on this mutated
protein, it should be possible to develop vaccines for the future.
Indeed, after the mouse model, the researchers were able to show that the HTLV
and XMRV retroviruses associated with human diseases were both endowed with an
immunosuppressive domain in their envelope protein.
Notes:
CNRS/ Université Paris-Sud 11/Institut Gustave Roussy
References:
Schlecht-Louf, G., Renard, M., Mangeney, M., Letzelter, C., Richaud, A., Ducos, B., Bouallaga, I., and Heidmann, T. Retrovirus infection in vivo requires an immune escape virulence factor encrypted in the envelope protein of oncoretroviruses. Proc. Natl. Acad. Sci., published online the week of 8 February 2010.
Contact information:
CNRS researcher l Thierry Heidmann l T 01 42 11 49 70 l heidmann@igr.fr
CNRS press officer l Claire Le Poulennec l T 01 44 96 49 88 l claire.le-poulennec@cnrs-dir.fr
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