Title :
Mechanisms of contrast agent destruction
Author :
Chomas, James E. ; Dayton, Paul ; Allen, John ; Morgan, Karcn ; Ferrara, Katherinc W.
Author_Institution :
Dept. of Biomed. Eng., California Univ., Davis, CA, USA
Abstract :
Various applications of contrast-assisted ultrasound, including blood vessel detection, perfusion estimation, and drug delivery, require controlled destruction of contrast agent microbubbles. The lifetime of a bubble depends on properties of the bubble shell, the gas core, and the acoustic waveform impinging on the bubble. Three mechanisms of microbubble destruction are considered: fragmentation, acoustically driven diffusion, and static diffusion. Fragmentation is responsible for rapid destruction of contrast agents on a time scale of microseconds. The primary characteristics of fragmentation are a very large expansion and subsequent contraction, resulting in instability of the bubble. Optical studies using a novel pulsed-laser optical system show the expansion and contraction of ultrasound contrast agent microbubbles with the ratio of maximum diameter to minimum diameter greater than 10. Fragmentation is dependent on the transmission pressure, occurring in over 55% of bubbles insonified with a peak negative transmission pressure of 2.4 MPa and in less than 10% of bubbles insonified with a peak negative transmission pressure of 0.8 MPa. The echo received from a bubble decorrelates significantly within two pulses when the bubble is fragmented, creating an opportunity for rapid detection of bubbles via a decorrelation-based analysis. Preliminary findings with a mouse tumor model verify the occurrence of fragmentation in vivo. A much slower mechanism of bubble destruction is diffusion, which is driven by both a concentration gradient between the concentration of gas in the bubble compared with the concentration of gas in the liquid, as well as convective effects of motion of the gas-liquid interface. The rate of diffusion increases during insonation, because of acoustically driven diffusion, producing changes in diameter on the time scale of the acoustic pulse length, thus, on the order of microseconds. Gas bubbles diffuse while they are not being insonified, termed s- - tatic diffusion.
Keywords :
biodiffusion; biomedical ultrasonics; bubbles; acoustic pulse length; acoustic waveform; acoustically driven diffusion; blood vessel detection; bubble shell; contrast agent destruction; contrast-assisted ultrasound; convective effects; decorrelation-based analysis; drug delivery; fragmentation; gas core; microbubbles; peak negative transmission pressure; perfusion estimation; primary characteristics; pulsed-laser optical system; static diffusion; transmission pressure; tumor model; Acoustic pulses; Acoustic signal detection; Acoustic waves; Blood vessels; Decorrelation; Drug delivery; Mice; Neoplasms; Optical pulses; Ultrasonic imaging; Animals; Blood Vessels; Contrast Media; Humans; Male; Mice; Mice, Nude; Phospholipids; Prostatic Neoplasms; Tumor Cells, Cultured; Ultrasonography; Xenograft Model Antitumor Assays;
Journal_Title :
Ultrasonics, Ferroelectrics, and Frequency Control, IEEE Transactions on
