Disrupting the blood-brain barrier by focused ultrasound induces sterile inflammation.
Authors: Kovacs ZI, Kim S, Jikaria N, Qureshi F, Milo B, Lewis BK, Bresler M, Burks SR, Frank JA
MRI-guided pulsed focused ultrasound (pFUS) combined with systemic infusion of ultrasound contrast agent microbubbles (MB) causes localized blood-brain barrier (BBB) disruption that is currently being advocated for increasing drug or gene delivery in neurological diseases. The mechanical acoustic cavitation effects of opening the BBB by low-intensity pFUS+MB, as evidenced by contrast-enhanced MRI, resulted in an immediate damage-associated molecular pattern (DAMP) response including elevations in heat-shock protein 70, IL-1, IL-18, and TNFα indicative of a sterile inflammatory response (SIR) in the parenchyma. Concurrent with DAMP presentation, significant elevations in proinflammatory, antiinflammatory, and trophic factors along with neurotrophic and neurogenesis factors were detected; these elevations lasted 24 h. Transcriptomic analysis of sonicated brain supported the proteomic findings and indicated that the SIR was facilitated through the induction of the NFκB pathway. Histological evaluation demonstrated increased albumin in the parenchyma that cleared by 24 h along with TUNEL<sup>+</sup> neurons, activated astrocytes, microglia, and increased cell adhesion molecules in the vasculature. Infusion of fluorescent beads 3 d before pFUS+MB revealed the infiltration of CD68<sup>+</sup> macrophages at 6 d postsonication, as is consistent with an innate immune response. pFUS+MB is being considered as part of a noninvasive adjuvant treatment for malignancy or neurodegenerative diseases. These results demonstrate that pFUS+MB induces an SIR compatible with ischemia or mild traumatic brain injury. Further investigation will be required before this approach can be widely implemented in clinical trials.
Introduction
Purpose
Drug delivery with BBB opening
Study Objective
To determine whether MRI-guided pulsed focused ultrasound combined with systemic microbubble infusion that opens the blood–brain barrier induces a sterile inflammatory response and to characterize its molecular, transcriptomic, and histological features.
Animal model / Human subject
rat, Sprague-Dawley, not reported, male
Disease model
healthy
MRI or image guidance method
MRI-guided
Targeted brain region(s)
Striatum
Cargo name and characteristics
Fluorescent beads — fluorescent tracer particles infused systemically 3 days before pFUS+MB to track infiltration; particle size/composition not specified
Outcomes and Safety
Summary of Outcomes
MRI-guided low-intensity pulsed focused ultrasound (pFUS) combined with systemic microbubble (MB) infusion transiently opens the blood–brain barrier but induces a sterile inflammatory response (elevated DAMPs HSP70, IL‑1, IL‑18, TNFα), activation of NFκB signaling, glial activation, TUNEL+ neuronal death, vascular albumin leakage that clears by 24 h, and macrophage infiltration by day 6. Successful parameter: low‑intensity MRI‑guided pFUS with systemic microbubble infusion.
Duration of biological effect
24 h
Safety-related matter
Induced transient DAMP elevations, glial activation, and TUNEL+ neuronal death, resolving within days.
Brain Region
Ultrasound Parameters
Ultrasound instrument
single-element focused ultrasound transducer
FUS Frequency
1 MHz
FUS Intensity
not reported
FUS Pressure
0.5 MPa
FUS Mode
pulsed
Pulse duration
not reported
Duration of a single FUS session
120 s
Treatment frequency
single session
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