Researchers at Moffitt Cancer Center have
developed and tested in mice a synthetic vaccine and found it effective in
killing human papillomavirus-derived cancer, a virus linked to cervical cancers
among others. The research was published in a recent issue of Cancer
Immunology, Immunotherapy.
"Vaccines
for cancer can be good alternatives to conventional therapies that result in
serious side-effects and are rarely effective against advanced disease,"
said Esteban Celis, M.D., Ph.D., senior member and professor in Moffitt's
Immunology Program. "The human papillomavirus,
or HPV, is known to cause 99 percent of cervical cancers and annually causes
more than 250,000 deaths worldwide." In addition, HPV is the causative
agent of a large proportion of head and neck and genital cancers.
Although
two approved prophylactic vaccines against strains of HPV that cause cervical
cancer are now in wide use as a measure to prevent HPV infections, these
vaccines cannot be used to treat HPV-induced cancers. Thus, there is a need to
develop therapeutic vaccines for HPV-related tumors.
In an
effort to find an effective HPV-cancer vaccine that would
eliminate existing HPV-induced cancer, Celis and Kelly Barrios-Marrugo, Ph.D.,
of the University of South Florida College of Medicine's Molecular Medicine
program, designed a peptide vaccination strategy called
TriVax-HPV.
The
TriVax vaccine strategy was designed to generate large numbers of cytotoxic
T-cells that would seek out the proteins preferentially expressed in the
tumors. The HPV16-E6 and E7 proteins function as oncogenic proteins inducing
cancer. Thus, according to Celis and Barrios-Marrugo, a vaccine targeting these viral proteins is
an "ideal candidate" to create strong immune responses, with the
additional benefit of not generating autoimmune-related pathologies.
When
they tested their vaccine in mice with HPV16-induced tumors, they found that
TriVax containing a small synthetic fragment (peptide) of the E7 protein
"induced tumor clearance in 100 percent of the treated mice" while
the unvaccinated mice with HPV-induced tumors had their tumors grow "at a
fast rate."
"Although
the magnitude of the T-cell responses achieved with TriVax in mice is
impressive," Barrios-Marrugo said," we do not know whether similar
effects can be accomplished in humans."
Celis
and Barrios-Marrugo point out that current therapies for cervical cancer can be devastating,
highly toxic and associated with a 10 percent chance of recurrence.
Additionally, a significant proportion of women in the Third World will not
receive the approved prophylactic vaccine to prevent HPV infection and, thus,
will continue at high risk for cervical and other cancers related to HPV.
"We
believe that these studies may help to launch more effective and less invasive
therapeutic vaccines for HPV-caused malignancies," concluded the authors.
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