Cases of one of the world's deadliest
diseases—tuberculosis—are rising at an alarming rate, despite widespread
vaccination. Reasons for the ineffectiveness of the vaccine, especially in
regions where this infectious disease is endemic, as well as arguments for
replacing the existing vaccine with novel synthetic vaccines, are presented in
a review published online August 28th in Trends in Molecular Medicine.
"Tuberculosis is a global health threat, and it is a highly
communicable disease that may influence practically anyone and everyone,"
says senior author Javed Agrewala of the CSIR-Institute of Microbial Technology
in Chandigarh, India. "There is a serious need and challenge for the
scientific community to develop alternative vaccination approaches for the
control of the disease."
Tuberculosis is a bacterial infection caused by Mycobacterium
tuberculosis (Mtb). About one third of the world's population is infected with
Mtb, which causes about two million deaths each year. Vaccines may be the best
strategy for controlling tuberculosis, but the only available vaccine—Bacillus
Calmette-Guerin (BCG)—does not reliably prevent the disease in adults,
especially in regions where tuberculosis is endemic.
In the review, Agrewala explains that BCG does not work well in
these regions because exposure to prevalent mycobacterial strains triggers the
production of antibodies that counteract the vaccine. In addition, infections
with parasitic worms called helminths interfere with protective immune
responses induced by BCG.
To overcome these limitations, Agrewala proposes the use of novel
vaccines called lipidated-promiscuous-peptide vaccines. These synthetic
vaccines are safer than BCG because they do not contain infectious material.
Moreover, they generate long-lasting, protective immune responses and are not
influenced by pre-existing antibodies. This type of vaccine strategy has
already proven to be successful in an animal model of tuberculosis and is being
tested in human clinical trials for other infectious diseases and cancer.
"We believe that lipidated-promiscuous-peptide vaccines have
all the essential qualities that can make them successful in
tuberculosis-endemic countries," Agrewala says. "Such vaccines can
impart better protection than BCG and will have a long-reaching positive impact
on millions of people."
Journal Reference:
1. Gowthaman, Pradeep K Rai, Nargis Khan, David C
Jackson, Javed N Agrewala. Lipidated promiscuous peptides vaccine for
tuberculosis-endemic regions.Trends in Molecular Medicine, 2012 (in
press)
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