a, Box-whisker plot of natural log of lung emission counts by imaging day. Initially, more radiolabeled MSCs are present in the left lung (left) than the right lung (right) because of the injection being performed with the animal on the left side (ie, dependent lung uptake). The lung emission counts over time decay faster than predicted by radioactive decay alone (eg, linear decay shown as crosses), indicating either redistribution of MSCs to other organs or cell death and removal. b, Uptake of 111In oxine–labeled MSCs increased in the kidney, liver, spine, and spleen at 24 hours after injection (day 2). After day 3, the uptake decreased at a rate faster than the radioactive decay of 111In oxine, indicating cell loss or loss of tracer. c, Activity in the infarcted anterior apex of the heart (left) was relatively constant for the first 24 hours after injection, indicating redistribution of 111In oxine–labeled MSCs to the infarcted tissue, whereas a rapid decrease in activity in the noninfarcted myocardium (right) was observed in the first 24 hours after injection, indicating a combination of radioactive decay plus loss of MSCs in normal heart tissue. d, In 3 animals demonstrating a focal uptake of activity to the heart, the decay of the activity was ≈3 times faster than predicted for radioactive decay of 111In oxine.