Molecular imaging of thrombus with microbubbles targeted to alphavbeta3-integrin using an agarose flow chamber model.
- Author:
Guang-quan HU
1
;
Jian LIU
;
Li YANG
;
Yi YAN
;
Jue-fei WU
;
Jia-jia XIE
;
Jing-jing CAI
;
Li-jing JI
;
Jian-ping BIN
Author Information
- Publication Type:Journal Article
- MeSH: Antibodies, Monoclonal; chemistry; immunology; Contrast Media; chemistry; Humans; Integrin alphaVbeta3; immunology; metabolism; Microbubbles; Sepharose; Thrombosis; diagnostic imaging; Ultrasonography
- From: Journal of Southern Medical University 2010;30(3):478-481
- CountryChina
- Language:Chinese
-
Abstract:
OBJECTIVETo assess the binding ability of microbubbles targeted to alphavbeta3-integrin (MBp) for thrombus-targeted contrast-enhanced ultrasound.
METHODSTargeted microbubbles were prepared by conjugating the monoclonal antibody against alphavbeta3-integrin to lipid shell of the microbubble via the avidin-biotin bridges. Equivalent isotype control microbubbles (MB) or targeted ultrasound microbubbles (MBp) were randomly added into the flow chamber. After a 30-min incubation with the thrombus fixed in an agarose flow chamber model, the thrombus was washed with a continuous flow of PBS solution (15 cm/s) for 2, 4, 6, 8 and 10 min, followed by thrombus imaging using contrast-enhanced ultrasound and measurement of the video intensity (VI) values of the images.
RESULTSThe VI of the thrombus in MBp group was reduced by 28%-66%, while that in control MB group was decreased by 87%-94%, and the VI values of the thrombus group were significantly greater in former group at each of the time points (P<0.05).
CONCLUSIONMBP has good targeting ability to the thrombus with resistance to the shear stress after adhesion to the thrombus. In vitro evaluation of the thrombus-binding capability of the targeted microbubble (MBp) by simulating the shear stress in vivo can be helpful for predicting the in vivo effects of ultrasonic molecular imaging using MBp.
