PURPOSE:
Pharmacokinetic
analyses
estimate the mean concentration of drug within a given tissue
as a function of time, but do not give information about the spatial
distribution of drugs within that tissue. Here, we compare the
time-dependent spatial distribution of
three anticancer drugs within
tumors, heart, kidney, liver and brain.
METHODS:
Mice
bearing various xenografts were treated with
doxorubicin, mitoxantrone
or topotecan. At various times after injection, tumors and samples of
heart, kidney, liver and brain were excised.
RESULTS:
Within
solid tumors, the distribution of doxorubicin, mitoxantrone and
topotecan was limited to
perivascular regions at 10 min after
administration and the distance from blood vessels at which drug
intensity fell to half was ~25-75 μm. Although drug distribution
improved after 3 and 24 h, there remained a significant decrease in drug
fluorescence with increasing distance from tumor blood vessels. Drug
distribution was relatively uniform in the heart, kidney and liver with
substantially greater perivascular drug uptake than in tumors. There was
significantly higher total drug fluorescence in the liver than in
tumors after 10 min, 3 and 24 h. Little to no drug fluorescence was
observed in the
brain.
CONCLUSIONS:
There are marked
differences in the spatial distributions of three anticancer drugs
within tumor tissue and normal tissues over time, with greater exposure
to most normal tissues and limited drug distribution to many cells in
tumors. Studies of the spatial distribution of drugs are required to
complement pharmacokinetic data in order to better understand and
predict
drug effects and toxicities.
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