New System for
Treating Colorectal
Cancer Can Lead to Complete Cure
Novel three-step pretargeted radioimmunotherapy offers safe, effective treatment
From the Society of Nuclear Medicine and Molecular Imaging (SNMMI)
Cancer Can Lead to Complete Cure
Novel three-step pretargeted radioimmunotherapy offers safe, effective treatment
From the Society of Nuclear Medicine and Molecular Imaging (SNMMI)
RESTON, Va.
– November 2, 2017 -- Researchers at Memorial Sloan Kettering Cancer
Center in New York City and Massachusetts Institute of Technology in Boston
have developed a new, three-step system that uses nuclear medicine to target
and eliminate colorectal cancer. In this study with a mouse model, researchers
achieved a 100-percent cure rate—without any treatment-related toxic
effects. The study is reported in the November featured article in The
Journal of Nuclear Medicine.
Until now,
radioimmunotherapy (targeted therapy) of solid tumors using antibody-targeted
radionuclides has had limited therapeutic success. “This research is novel
because of the benchmarks reached by the treatment regimen, in terms of
curative tumor doses, with non-toxic secondary radiation to the body’s normal
tissues,” explains Steven M. Larson, MD, and Sarah Cheal, PhD, of Memorial
Sloan Kettering Cancer Center. “The success in murine tumor models comes
from the unique quality of the reagents developed by our group, and the
reduction to practice methodology, including a theranostic approach that can be
readily transferred, we believe, to patients.”
Theranostics,
a term derived from therapy and diagnostics, is the use of a single agent
to both diagnose and treat disease. The theranostic agent first finds the
cancer cells, then destroys them, leaving healthy cells unharmed—minimizing
side effects and improving quality of life for patients.
In this study, the
glycoprotein A33 (GPA33), an antigen found on over 95 percent of primary and
metastatic human colorectal cancers, was targeted with a bispecific antibody
for A33 tumor antigen and a second antibody for a small-molecule radioactive
hapten, a complex of lutetium-177 (177Lu) and
S-2-(4-aminobenzyl)1,4,7,10-tetraazacyclododecane tetra-acetic acid (177Lu-DOTA-Bn).
The DOTA-pretargeted
radioimmunotherapy (PRIT) strategy was tested on a mouse model. In randomly
selected mice undergoing treatment, serial SPECT/CT imaging was used to monitor
treatment response and calculate radiation-absorbed doses to tumors. All the
DOTA-PRIT–treated animals tolerated the treatment well, and all 9 assessed mice
had no trace of cancer remaining upon microscopic examination. There was also
no detectable radiation damage to critical organs, including bone marrow and
kidneys.
The 100-percent
cure rate in the mouse model is a promising preliminary finding that suggests
that anti-GPA33-DOTA-PRIT will be a potent radioimmunotherapy regimen for
GPA33-positive colorectal cancer tumors in humans.
According to
the Centers for Disease Control and Prevention, colorectal cancer is the
third most common cancer affecting both men and women. Each year, approximately
140,000 new cases are diagnosed in the United States
The applications
of this nuclear medicine treatment protocol could extend to other cancers as
well. Larson and Cheal state, “If clinically successful, our approach will
expand the repertoire of effective treatments for oncologic patients. The
system is designed as a ‘plug and play’ system, which allows for the use of
many fine antibodies targeting human tumor antigens and is applicable, in
principle, to virtually all solid and liquid tumors in man.” They add, “There
is a huge unmet need in oncology, especially for the solid tumors, for curative
treatments for advanced disease. This includes, colon, breast, pancreas,
melanoma, lung, and esophageal, to name a few.”
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