Islamabad, Jan 8 :
Scientists from the Florida campus of The Scripps Research Institute, have
developed a novel technology that is able to detect the presence of immune
molecules specific to Alzheimer's disease in patients' blood samples.
While still preliminary, the findings offer clear proof that this
breakthrough technology could be used in the development of biomarkers for a
range of human diseases.
Traditionally, antigens -- a substance such
as a protein from a virus or bacteria that stimulates an immune response -- have
been necessary for the discovery of antibody biomarkers. There has previously
been no way to identify an antibody (a type of targeted immune molecule) without
first knowing the antigen that triggers its production. The new study, however,
challenges conventional wisdom and uses synthetic molecules rather than antigens
to successfully detect signs of disease in patients' blood samples.
These
synthetic compounds have many advantages -- they can be modified easily and can
be produced quickly in relatively large amounts at lower cost.
"Dr.
Kodadek has conceived of a new approach for identifying antibody biomarkers of
human disease that bypasses the conventional, but difficult, step of identifying
the natural antigens or antigen mimics," said James M. Anderson, M.D., Ph.D.,
director of the National Institutes of Health (NIH) Division of Program
Coordination, Planning, and Strategic Initiatives, who helps oversee the NIH
Common Fund's Pioneer Award Program. "The results in the paper suggest great
potential for using this approach to rapidly develop diagnostic biomarkers for a
variety of significant human diseases. Such boldness to challenge conventional
paradigms to achieve important scientific advances is a hallmark of the NIH
Director's Pioneer Award Program, which supported much of this
research."
"This study essentially puts an end to the notion that the
only way to pull a potentially useful antibody from blood samples is with a
specific antigen," said Kodadek. "Because the antigen identification problem has
proven to be so difficult, we decided to take it out of the equation."
A
Focus on the Immune System
To test the concept, Kodadek and his
colleagues used comparative screening of combinatorial libraries of synthetic
molecules -- peptoids -- against serum samples obtained from mice with a
multiple-sclerosis-like condition or healthy controls. Those synthetic molecules
that retained more immunoglobulin (IgG), a major type of antibody, from the
blood samples of the diseased animals were identified as potential agents for
capturing diagnostically useful molecules. This worked well.
The team
next turned to serum samples from six Alzheimer's patients, six healthy
individuals, and six Parkinson's disease patients. Three peptoids were
identified that captured at least three-fold higher levels of IgG antibodies
from all six of the Alzheimer's patients than any of the control or Parkinson's
patients. The results showed that two of the peptoids bind the same IgG
antibodies; a third binds different antibodies, resulting in at least two
candidate biomarkers for the disease.
"We use these peptoids as a lure to
capture the IgG antibodies," Kodadek said. "Some of these synthetic molecules
recognize the antigen-binding sites of disease-specific antibodies well enough
to pull them from blood samples, although they almost certainly don't bind as
well as the native antigens. This ability should make it possible to short
circuit the discovery of the natural
antigens."
Ends
SA/EN
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