This article originally posted 23 August, 2005 and appeared in Issue 274
Non-invasive Imaging Helps to Predict Type 1 Diabetes and Response to Treatment
Physicians may be able to identify individuals with preclinical type 1 diabetes, and to assess the effectiveness of therapies.
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A key obstacle to early detection of type 1 diabetes - as well as to rapid
assessment of the effectiveness of therapeutic intervention - has been the lack
of direct, non-invasive technologies to visualize inflammation in the pancreas,
an early manifestation of disease. Instead, clinicians have had to await overt
symptoms before diagnosing an individual, by which time destruction of the insulin-producing
beta cells of the pancreas has already progressed significantly.
Recent proof-of-principle experiments by Joslin Diabetes Center and Massachusetts
General Hospital (MGH) researchers, however, offer hope that physicians may
one day be able to identify individuals with preclinical type 1 diabetes, and
to assess the effectiveness of therapies much earlier than is now possible.
Type 1 diabetes is an autoimmune disease in which the body's immune system
mistakenly attacks its own insulin-producing beta cells and eventually kills
them. Early in this process, white blood cells called T lymphocytes infiltrate
the islets of the pancreas (an inflammatory condition known as insulitis), causing
the blood vessels to become leaky. Over time, this infiltration of lymphocytes
destroys the beta cells, leading to high blood glucose and full-blown diabetes.
Today, the only accurate method for detecting the progression or regression
of insulitis is a biopsy of the pancreas, which is almost never performed because
it is an invasive and potentially risky procedure.
"The most exciting aspect of this study is that it demonstrates that
we can, at least in mice, use a non-invasive imaging method to predict at a
very early time whether a drug will stop the progression of diabetes or not.
In fact, the drug we used in these proof-of-principle experiments is analogous
to one currently being tried in humans with diabetes, and so far showing great
promise," said Diane Mathis, Ph.D., who led the study.
In this study, researchers used a new imaging technique to reveal the otherwise
undetectable inflammation of pancreatic islets in recently diagnosed diabetic
mice. As T lymphocytes invade the pancreas, blood vessels swell, become more
permeable, and leak fluid - as well as small molecules carried in the fluid
- into surrounding tissues. In previous experiments, the researchers demonstrated
that this leakage can be detected with the help of magnetic nanoparticles (MNP)
and magnetic resonance imaging (MRI). After being injected intravenously, these
MNPs, which are minute particles of iron oxide, travel through the blood vessels
of the body including the pancreas. If pancreatic vessels have become leaky
from inflammation, the magnetic particles spill into nearby tissues, where they
are "eaten" by scavenger cells called macrophages. Thus, the MNPs
become concentrated at the inflamed site and can be spotted by high-resolution
MRI.
In their recent study, the researchers applied the MRI-MNP technique to determine
whether they could predict which mice would develop autoimmune diabetes and
monitor the effectiveness of immune therapy aimed at reversing diabetes. The
goal of this study was to gather data on mouse models that could guide the safe
application of the technique in human patients with, or at risk of, type 1 diabetes.
Results of this study suggest that the MRI-MNP imaging technology may be helpful
in identifying people at immediate risk of developing autoimmune diabetes, but
most of all for early prediction of response to therapy, which might be very
useful for reducing the time and cost of clinical trials. "Because the
results in mice looked so good, and because our MGH colleagues have already
successfully used essentially the same drug on many patients with prostate cancer,"
said Dr. Benoist, "we have been able to move relatively quickly into clinical
trials." Dr. Turvey added: "We hope to know soon whether we can use
this drug and imaging technique to monitor pancreas inflammation in humans."
Joslin investigators are currently recruiting subjects for the Imaging in
Diabetes clinical trial
Journal of Clinical Investigation, Sept 1, 2005
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