In vivo imaging of sterile microglial activation in rat brain after disrupting the blood-brain barrier with pulsed focused ultrasound: [18F]DPA-714 PET study

被引:44
作者
Sinharay, Sanhita [1 ,6 ]
Tu, Tsang-Wei [2 ,3 ,7 ]
Kovacs, Zsofia, I [2 ,8 ]
Schreiber-Stainthorp, William [1 ]
Sundby, Maggie [2 ]
Zhang, Xiang [4 ]
Papadakis, Georgios Z. [1 ,9 ,10 ]
Reid, William C. [1 ]
Frank, Joseph A. [2 ,5 ]
Hammoud, Dima A. [1 ]
机构
[1] NIH, Hammoud Lab, Ctr Infect Dis Imaging, Clin Ctr, 10 Ctr Dr,Bldg 10,Room 1C-368, Bethesda, MD 20892 USA
[2] NIH, Frank Lab, Radiol & Imaging Sci, Clin Ctr, Bethesda, MD 20892 USA
[3] Uniformed Serv Univ Hlth Sci, Ctr Neurosci & Regenerat Med, Bethesda, MD 20814 USA
[4] NHLBI, Imaging Probe Dev Ctr, NIH, Rockville, MD USA
[5] Natl Inst Biomed Imaging & Bioengn, NIH, Bethesda, MD USA
[6] Univ Texas MD Anderson Canc Ctr, Houston, TX 77030 USA
[7] Howard Univ, Dept Radiol, Washington, DC 20059 USA
[8] Swiss Fed Inst Technol, Inst Biomed Engn, Zurich, Switzerland
[9] Univ Crete, Dept Radiol, Iraklion, Greece
[10] Heraklion Univ Hosp, Dept Med Imaging, Iraklion, Greece
关键词
Neuroinflammation; 18F]DPA-714 PET; Pulsed focused ultrasound; Magnetic resonance imaging; Translocator protein; CONTRAST AGENT; DRUG-DELIVERY; MOUSE MODEL; 18; KDA; INFLAMMATION; MICROBUBBLES; PERMEABILITY; PATHOLOGY; DISEASE; SYSTEM;
D O I
10.1186/s12974-019-1543-z
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
BackgroundMagnetic resonance imaging (MRI)-guided pulsed focused ultrasound combined with the infusion of microbubbles (pFUS+MB) induces transient blood-brain barrier opening (BBBO) in targeted regions. pFUS+MB, through the facilitation of neurotherapeutics' delivery, has been advocated as an adjuvant treatment for neurodegenerative diseases and malignancies. Sterile neuroinflammation has been recently described following pFUS+MB BBBO. In this study, we used PET imaging with [18F]-DPA714, a biomarker of translocator protein (TSPO), to assess for neuroinflammatory changes following single and multiple pFUS+MB sessions.MethodsThree groups of Sprague-Dawley female rats received MRI-guided pFUS+MB (Optison (TM); 5-8x10(7)MB/rat) treatments to the left frontal cortex and right hippocampus. Group A rats were sonicated once. Group B rats were sonicated twice and group C rats were sonicated six times on weekly basis. Passive cavitation detection feedback (PCD) controlled the peak negative pressure during sonication. We performed T1-weighted scans immediately after sonication to assess efficiency of BBBO and T2*-weighted scans to evaluate for hypointense voxels. [18F]DPA-714 PET/CT scans were acquired after the BBB had closed, 24h after sonication in group A and within an average of 10days from the last sonication in groups B and C. Ratios of T1 enhancement, T2* values, and [18F]DPA-714 percent injected dose/cc (%ID/cc) values in the targeted areas to the contralateral brain were calculated. Histological assessment for microglial activation/astrocytosis was performed.ResultsIn all groups, [18F]DPA-714 binding was increased at the sonicated compared to non-sonicated brain (%ID/cc ratios >1). Immunohistopathology showed increased staining for microglial and astrocytic markers in the sonicated frontal cortex compared to contralateral brain and to a lesser extent in the sonicated hippocampus. Using MRI, we documented BBB disruption immediately after sonication with resolution of BBBO 24h later. We found more T2* hypointense voxels with increasing number of sonications. In a longitudinal group of animals imaged after two and after six sonications, there was no cumulative increase of neuroinflammation on PET.ConclusionUsing [18F]DPA-714 PET, we documented in vivo neuroinflammatory changes in association with pFUS+MB. Our protocol (utilizing PCD feedback to minimize damage) resulted in neuroinflammation visualized 24h post one sonication. Our findings were supported by immunohistochemistry showing microglial activation and astrocytosis. Experimental sonication parameters intended for BBB disruption should be evaluated for neuroinflammatory sequelae prior to implementation in clinical trials.
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页数:11
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