Next Article in Journal
Ultra-High-Frequency ECG in Cardiac Pacing and Cardiac Resynchronization Therapy: From Technical Concept to Clinical Application
Previous Article in Journal
Interventricular Septal Involvement Is Associated with More Impaired Ventricular Function and Mechanics in Apical Hypertrophic Cardiomyopathy
 
 
Search for Articles:
Title / Keyword
Author / Affiliation / Email
Journal
Article Type
 
 
Advanced Search
 
Section
Special Issue
Volume
Issue
Number
Page
 
Journals
JCDD
Volume 11
Issue 3
10.3390/jcdd11030075
jcdd-logo
Submit to this Journal Review for this Journal Propose a Special Issue
Article Menu

Article Menu

share Share announcement Help format_quote Cite question_answer Discuss in SciProfiles thumb_up
...
Endorse textsms
...
Comment
first_page
settings
Order Article Reprints
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Review

Sonothrombolysis for Ischemic Stroke

by
Narayanaswamy Venketasubramanian
1,*,
Leonard L. L. Yeo
2,
Benjamin Tan
2 and
Bernard P. L. Chan
2
1
Raffles Neuroscience Centre, Raffles Hospital Singapore, Singapore 188770, Singapore
2
Division of Neurology, National University Hospital, Singapore and Yong Loo Lin School of Medicine, National University of Singapore, Singapore 119074, Singapore
*
Author to whom correspondence should be addressed.
J. Cardiovasc. Dev. Dis. 2024, 11(3), 75; https://doi.org/10.3390/jcdd11030075
Submission received: 22 November 2023 / Revised: 14 February 2024 / Accepted: 17 February 2024 / Published: 22 February 2024
(This article belongs to the Section Stroke and Cerebrovascular Disease)
Versions Notes

Abstract

:
Stroke is a major cause of death and disability globally, with ischemic stroke being the predominant mechanism. While spontaneous recanalization may occur, significant neuronal injury would have occurred in the interim. Intravenous thrombolysis administered within the first 4.5 h after stroke onset and endovascular thrombectomy within 24 h in patients with a salvageable penumbra improves functional independence. Ultrasound has been shown in both in vivo and in vitro models to enhance clot lysis, even more-so in the presence of thrombolytic agents. The use of transcranial Doppler and transcranial color-coded Doppler ultrasound in acute IS has been reported in case series, case-controlled studies, and clinical trials. While ultrasound at a frequency of 300 kHz increases the risk of intracranial hemorrhage, the 2 MHz range ultrasound aids thrombolysis and improves recanalization without significantly increasing the risk of symptomatic intracranial hemorrhage. Despite this, functional independence was not increased in clinical trials, nor was a benefit shown with the adjunctive use of microbubbles or microspheres. Nonetheless, newer technologies such as endovascular ultrasound, endovascular delivery of microbubbles, and thrombolytic-filled microbubbles await clinical trials. More evidence is needed before sonothrombolysis can be routinely used in the hyperacute management of ischemic stroke.

1. Introduction

Stroke is a major cause of health burden globally. Based on the Global Burden of Disease Study, in 2019, stroke incidence was 12.2 million cases (95% UI 11.0–13.6), with a prevalence of 101 million cases (95% UI 93.2–111) and a mortality of 6.55 million cases (95% UI 6.00–7.02), with 143 million (95% UI 133–153) disability-adjusted life years (DALYs) lost due to stroke [1]. Among incident cases, the most common cause of stroke was arterial occlusion causing ischemic stroke (IS) at 62.4% (7.63 million [95% UI 6.57–8.96]), with 27.9% (3.41 million [95% UI 2.97–3.91]) due to intracerebral hemorrhage (ICH), and 9.7% (1.18 million [95% UI 1.01–1.39]) due to subarachnoid hemorrhage (SAH).
It is estimated that in patients with IS, due to acute large arterial occlusion, in each hour, 120 million neurons, 830 billion synapses, and 714 km of myelinated fibers are lost; in each minute, the respective numbers are 1.9 million, 14 billion, and 12 km [2]. This has bolstered the concept that ‘time is brain’ and the need to begin treatment as soon as possible. Thus, among the key approaches in the management of acute IS is emergent and rapid revascularization of the occluded artery to re-establish adequate perfusion to ischemic tissue so as to rescue as much brain tissue as possible and limit further damage caused by ongoing ischemia [3].

2. Recanalization after Ischemic Stroke

In a systemic review of 10 angiographic studies among patients with IS (n = 1130), the authors found that spontaneous recanalization (SR) occurred in approximately 17% of patients in the first 6 to 8 h after stroke onset, with a lack of occlusion seen in 28% to 50% of patients by four days [4]. This shows that some SR occurs naturally after large vessel occlusion, but the proportion is small in the early hours after IS onset, and still poor even after four days, which, in the absence of adequate collateral flow, can lead to brain tissue continuing to be damaged from inadequate perfusion and ongoing ischemia. It would be difficult to obtain similar data on small vessel occlusion due to their tiny size and difficulty in their visualization on cerebral angiography, but as these are usually end-arteries with little collateral flow, the ischemic injury, although to a smaller volume of brain tissue, is likely to be more severe within that territory.
As a corollary, in a study of adults, 38 with IS compared to 17 healthy controls, central motor conduction times (CMCTs) at day 14 post-stroke were improved if spontaneous recanalization occurred within 24 hours compared to after 24 h (87% vs. 62% of patients, p = 0.005); CMCT improved in only 17% of those with no recanalization [5]. Thus, early recanalization is crucial. Delayed recanalization, even if it occurs, may not only be unhelpful in aiding stroke recovery due to irrecoverable tissue damage from prolonged inadequate perfusion, but it also carries the serious risk of reperfusion vasogenic oedema and hemorrhagic transformation, which may be deleterious to the already fragile ischemic tissue [6,7].
The process of SR involves the natural lysis of the fibrin network that holds the clot together, allowing blood to flow past the site of occlusion [8]. SR is achieved by plasmin-dependent and plasmin-independent pathways. Of the plasmin-dependent pathways, vascular endothelial cells produce activators of fibrinolysis, such as the tissue-type plasminogen activator (tPA) and the urokinase-type plasminogen activator (uPA). These activators convert circulating plasminogen to plasmin, which then breaks down fibrin and lyses the clot. Plasmin-independent pathways involve the accumulation of polymorphonuclear leucocytes at the site of the clot that then activate plasmin-dependent pathways as well as release serine proteases, including proteinase 3, cathepsin G, and elastase, that break up the clot. Monocytes infiltrating into the clot also release plasminogen activators that then cause clot lysis.
Various thrombolytic agents have been developed that are able to enhance the intrinsic clot lysis by their ability to convert circulating plasminogen to plasmin, which then lyses the clot [9]. Such agents include alteplase, duteplase, desmoteplase, reteplase, staphylokinase, streptokinase, pro-urokinase, urokinase, tenecteplase, and anistreplase (APSAC), to name a few. In a meta-analysis of 27 randomized trials (n = 10,187), thrombolytic therapy, mostly given up to six hours after the onset of IS, significantly reduced the odds of death or dependency (modified Rankin Score mRS 3–6) at three to six months after a stroke (odds ratio (OR) 0.85, 95%CI 0.78–0.93) [10]). When administered within three hours of the onset of IS (11 trials, n = 2187), death or dependency was even more significantly reduced (OR 0.66, 95% CI 0.56–0.79) without increasing mortality. The early administration of intravenous thrombolysis (IVT) within 4.5 h of acute IS onset among patients without contraindications is now the standard of care [3]. Patients treated with IVT from 4.5 to 9 h after stroke onset, or wake-up stroke, would also benefit if they had imaging evidence of a perfusion mismatch [11].
Mechanical (also called endovascular) thrombectomy (EVT) involves the physical removal of clots in large intracranial arteries using a device passed intra-arterially to the level of the clot in a technique that uses cerebral angiography to visualize the vasculature. A meta-analysis of five large landmark trials of acute IS patients with occlusion of the proximal anterior circulation artery treated by EVT within 12 h of onset (n = 1287) showed that EVT significantly reduced disability as measured by the mRS at 90 days compared with a control (adjusted cOR 2.49, 95% CI 1.76–3.53) [12]. In a meta-analysis of nine randomized controlled trials combining IVT with EVT (n = 3740) versus EVT alone, the combination group was superior in functional independence (mRS 0–2) (OR 1.27, 95% CI 1.11–1.46) [13]. In a systematic review and meta-analysis of 16 studies (n = 7572) where intra-arterial thrombolysis was added to EVT, functional independence (mRS 0–2) at 90 days was non-significantly different (OR 1.14, 95%CI: 0.95–1.37) [14]. Thrombectomy within 24 h of onset among stroke patients with proximal large artery occlusion and a salvageable penumbra, with bridging IVT if it can be initiated within 4.5 h, is now the standard of care [3]. EVT has shown a functional benefit even among those with significant brain damage, as evidenced by an Alberta Stroke Program Early Computed Tomography Score of 3–5 or a calculated infarct volume of >50 mL [15].

3. Ultrasound

Sound is a form of mechanical energy [16]. Sound occurs when its source vibrates and produces cyclical oscillations of longitudinal waves that then allow the propagation of the energy. There are two phases in a sound wave—compression, which is the high-pressure phase of a sound wave, and rarefaction, which is the low-pressure phase. Sound needs a medium for it to travel—it is unable to travel in a vacuum. The frequency of an ultrasound is the number of wave cycles per second produced by the source—it is expressed in hertz (Hz). Sound waves conducted at a frequency above the upper limit of human hearing of 20 kHz (i.e., above 20,000 Hz) are called ultrasound. Ultrasound frequencies for clinical use range from 1 MHz to 20 MHz (i.e., 1 million to 20 million Hz).
When ultrasound enters tissue, a small amount is reflected by highly reflective objects back to the source/transducer, which forms the basis of diagnostic ultrasound imaging [16]. The sound waves may also be refracted if they pass through a different medium and thus shift direction. They may be scattered in multiple directions, or they may be absorbed, which forms the basis of therapeutic ultrasound. The absorbed energy causes vibration, heating, and the occurrence of vapor- or gas-filled cavitations/bubbles, as well as circulation of the liquid and the appearance of oxidation products [17].
Cavitation occurs when ultrasound passing through a liquid medium interacts with gaseous inclusions in that medium, e.g., microbubbles (MBs) [18]. Cavitation is broadly divided into stable cavitation (also called gas body activation (formerly identified as stable cavitation)), and inertial cavitation (also called transient cavitation). In stable cavitation, a relatively low level of ultrasound intensity activates a pre-existing gas body that resonates and undergoes periodic and regular volume changes in response to the applied acoustic pressure. Inertial cavitation requires a relatively higher ultrasound intensity that makes the MBs also undergo periodic volume changes in sync with the applied acoustic pressure, but the rapid increases in size lead to the bubble becoming unstable and then violently imploding.

4. In Vitro and In Vivo Effects of Ultrasound on Clots

The effect of ultrasound on blood clots has long been studied, with laboratory evidence in the 1950s showing that it is able to compress and retract clots [19,20]. While high-intensity ultrasound is able to mechanically fragment clots [21], low-intensity ultrasound is able to augment enzymatic fibrinolysis through non-thermal mechanisms by improving entry of fibrinolysis activators into the clot [22], reversibly altering fibrin structure and increasing tPA binding to fibrin [23]. The main mechanisms for clot lysis by ultrasound include acoustic stable cavitation and radiation force [24]. The use of ultrasound to cause or enhance clot lysis is called ‘sonothrombolysis’.
Among the earliest studies of therapeutic ultrasound for clot lysis, Sobbe et al. [25], building on earlier work by Ehringer et al. [26], showed that ultrasound was able to recanalize thrombosed femoral arteries in dogs without complications. Transcutaneous ultrasound applied in vivo combined with streptokinase was able to significantly augment the lysis of thrombi in the iliofemoral arteries of rabbits [27].
High-intensity focused ultrasound (1.5 MHz) initiated thrombolysis effectively and safely in a rabbit model of embolic stroke [28]. Ultrasound combined with a recombinant tissue plasminogen activator (rTPA) was more effective than rTPA treatment alone in reducing infarct volume in an embolic rat stroke model [29].
The value of magnetic resonance imaging (MRI)-guided focused ultrasound (MRgFUS) has been investigated. In a study using MRgFUS and monitoring using an MR angiogram (MRA) performed at 1-minute intervals, a 1 MHz ultrasound combined with rTPA was better able than rTPA alone to dissolve clots in the carotid artery of New Zealand rabbits [30].
Studies also evaluated the MRgFUS system through a plastic phantom skull. When combined with thrombolytic drugs and using transducers at either 0.5 or 1 MHz, clots could be destroyed in this in-vitro model [31].
In a study using a human temporal bone, a 1.8-MHz pulsed-wave (PW) ultrasound was passed through a human temporal bone onto whole blood clots. While clot weight was reduced using ultrasound alone compared to controls, an even greater reduction was achieved when ultrasound was combined with rTPA compared with rTPA alone [32].
To explore the impact of the human calvarium, artificial thrombi were placed inside the skull and located at the transducer focus point. Clot lysis increased with increasing acoustic output powers [33]. In another study, longer duty cycles combined with longer pulse widths had the highest potential to lyse clots [34].
Lower-frequency ultrasound in the kHz range, compared to the MHz range, is less attenuated by bone and is thus able to pass through the skull more easily [35]. Embolic rat models have shown that low-frequency ultrasound is able to significantly reduce infarct volume compared to pure TPA treatment. Animal studies did not show an increased rate of bleeding or harm to the blood–brain barrier.
There are reasonable concerns as to the formation of clot fragments when the clot is broken down by ultrasound, leading to the risk of distal embolization of these fragments and subsequent vascular occlusion. Rosenschein et al. showed in an animal model that 93% of clot fragments from sonothrombolysis were sub-capillary in size (<8 microns) [36] and thus unlikely to cause significant distal vascular occlusion. Other researchers have also reported very small fragments, 96% being <5 microns [37] or all being <11 microns [38]. It can be expected that the body’s endogenous fibrinolytic system would dissolve fragments, a process further enhanced by the co-administration of thrombolytic agents.

5. Microbubbles

Further progress came with the increased understanding of MBs. Under conditions of inertial cavitation, due to Bjerknes acoustic radiation forces and large-amplitude oscillations of MBs, there is a mechanical effect causing thrombus pitting and deformation [39]. The expansion and collapse of bubbles are able to stretch individual fibers within clots, while the dissipation of acoustic energy is able to break individual fibers in the clot—if the bubble located outside the clot collapses asymmetrically, an impinging jet is created that aids in clot destruction [40].
MB-mediated sonothrombolysis is a complex process involving the clot, ultrasound, thrombolytic drug, and MBs. Clot lysis is best achieved by combining ultrasound at a high acoustic pressure with TPA and MB, compared to a single agent or in any other combination [41]. A similar result was seen an in vitro circulating flow model evaluating the role of tenecteplase (TNK-tPA)-mediated thrombolysis of fully retracted porcine blood clots where higher FUS frequencies (1 MHz) are associated with better thrombolysis compared to lower FUS frequencies (0.6 MHz), and an even better thrombolytic efficacy of the combination of 1-MHz FUS pulses with TNK-tPA and MBs [42]. In a thromboembolic stroke model of middle cerebral artery occlusion (MCAO) in rats, MB-mediated sonothrombolysis led to a similar reduction in infarct volume compared to rTPA [43]. A systematic review of 16 pre-clinical studies found heterogeneity in ultrasound parameters and types of MBs used, but four studies showed the superiority of sonothrombolysis over rTPA based on clinical criteria; however, safety data was limited [44].
Contrast agents are MBs that are given intravenously, are sufficiently small and stable enough to survive the cardiopulmonary circulation, and remain in the circulation to then enter other vascular beds, e.g., the cerebral circulation [45]. These MBs increase the Doppler signal by 10 dB to 30 dB, allowing the detection of flow in locations for which attenuation may make successful insonation impossible, e.g., the transcranial examination of intracranial vessels, especially through unfavorable bone windows. They can increase the success rate of the examination, reduce the time required for the examination, and facilitate the detection of a greater number of vessels.
Contrast agents and MB formulations used in animal models include Sonovue, Definity, perflutren lipoid, albumin, and BR38 [46,47,48,49,50]. Magnetic targeting of MBs using a single magnet allows for increased lysis rates [51].
New research has shown that different shapes showed different cavitation reactivity, e.g., of two different gold nanoparticles in shape functionalized with the rtPA, rtPA-functionalized asymmetric gold nanostars (NSt) were superior to gold nanospheres (NPt) in causing cavitation [52]. As clots fragmented by sonothrombolysis may result in debris that then migrates distally and causes further occlusions, phase-change nanodroplets can reduce the overall clot debris size and may allow for safer sonothrombolysis [53].
More recent techniques involve the intraluminal visualization of clots and the delivery of ultrasound intravascularly [54]. Intra-arterial B-mode ultrasound imaging was able to verify intra-clot delivery and clot penetration of the concurrently administered ultrasound contrast agents Optison and SonoVue with rTPA [55]. MBs may also be delivered intra-arterially while the ultrasound is applied from an extracranial source [56]. A dual-mode ultrasound catheter that combined a 16-MHz high-frequency element (imaging transducer) and a 220-kHz low-frequency element (treatment transducer) showed successful in-vitro sonothrombolysis [57].
Hollow nanogels loaded with thrombolytic agents, e.g., urokinase-type plasminogen activator (uPA), octafluoropropane, and rTPA-loaded echogenic liposomes (OFP t-ELIP), when sonolysed at the site of the clot, allow the delivery of thrombolytic agents at the site of the thrombus [58].
In parallel, there has been a greater understanding of how the characteristics of a clot may affect its susceptibility to sonothrombolysis. Sonothrombolysis is more successful on fresh thrombi and those with high cholesterol levels within it [59]. Platelet-rich clots are resistant to thrombolysis, which may explain some of the failures in recanalization [60]. Higher acoustic pressure is needed to lyse arterial thrombi compared to venous thrombi [61].

6. Transcranial Ultrasound Imaging

The intracranial structures can be imaged in various ways, including by computed tomography (CT) and MRI [62]. The vasculature can be studied by CT angiography (CTA), where intravenous contrast is injected and high-resolution small-thickness slice images are rapidly taken of the brain and blood flow through the vessels and usually reconstructed into easily interpretable images—while a rapid technique and widely available, it does carry a radiation risk and needs a contrast injection which can be an issue in those with renal dysfunction or a contrast allergy. MR angiography (MRA) is another method where the signals generated by flowing blood in a magnetic field are used to again reconstruct easily interpretable images of blood flowing through the vessels—while it carries no radiation risk and does not usually require contrast injection, it may not be easily available especially after office hours if at all, takes much longer than CTA, and may be a challenge in claustrophobic or clinically unstable patients, or those with pacemakers.
Ultrasound imaging has the advantages of being safe, portable, and rapid, and is usually widely available—transcranial Doppler (TCD) is routinely performed on stroke centers to evaluate blood flow in the basal cerebral arteries in acute stroke [63]. Transcranial color-coded duplex (TCCD) imaging marries the blind TCD technique with B-mode imaging and color coding of Doppler signals generated by flowing to allow a more accurate ultrasound visualization of the intracranial vessels and is also used in stroke centers as a complementary technique to study blood flow [64]. Both TCD and TCCD involve passing low-frequency ultrasound waves in the 2 MHz range through the intact skull to visualize flowing blood and can diagnose arterial stenosis, vasospasm, occlusion, compensatory flow, and embolization, to name a few [65].

7. Clinical Case Series

There have been a few publications reporting the clinical experience with sonothrombolysis for acute ischemic stroke (Table 1).
Among the earliest case series was by Alexandrov et al. in 2000, where 40 patients with acute IS of a moderate severity were monitored using a 2 MHz TCD while they were receiving rTPA [66]. They found recanalization in 70% of patients, with dramatic recovery during rTPA infusion in 20%, all of whom had full recanalization. At 24 h, 40% had significantly improved or recovered fully; despite a small risk of hemorrhage. The authors felt that ultrasound may result in the exposure of a greater amount of the clot surface and thus assist in thrombolysis.
Another publication in 2002 by Cintas et al. using TCCD in six severe IS patients with MCA occlusion but no thrombolytic agent showed at least partial recanalization in 83%, with a reduction in the neurological deficit over the first 24 h; they did not find any hemorrhage [67].
Alexandrov et al. built on their previous work by performing a combined lysis of thrombus in brain ischemia using transcranial ultrasound and systemic TPA (CLOTBUST) trial [68]. Their Phase 1 data on 55 moderately severe IS patients with arterial occlusion receiving rTPA and TCD, again documented complete recanalization in 36% by 2 h and dramatic or at least significant improvement at 24 h in 49%, but a small risk of hemorrhage.
Brunser et al. treated 61 moderately severe acute IS patients, most with MCA occlusion, attending their clinic with thrombolysis and TCD [69]. Complete recanalization occurred in 44.3%; at three months, 60% attained a modified Rankin score (mRS) of 0–2, with a 10% case fatality. Gu et al. reported their experience with 20 IS patients treated with thrombolysis and TCD, which resulted in full or partial recanalization in 36%, with 76% being ADL-independent at three months [70]. Aaron et al. reported on their 18 IS patients receiving thrombolysis and TCD, with immediate dramatic improvement in 30%, which reached 50% in the next 24 h [71]. Despite the small hemorrhagic risk and 11% mortality at six months, 63% attained an mRS ≤ 2.

8. Case-Controlled Studies and Non-Randomized Clinical Trials

While case series are able to provide useful initial information, comparing with suitable controls would allow a more accurate understanding of outcomes (Table 2).
Encouraged by animal data on the safety and efficacy of low-frequency ultrasound [35], Daffertshofer et al. performed a non-randomized transcranial low-frequency ultrasound-mediated thrombolysis in brain ischemia (TRUMBI) clinical trial using 300 kHz ultrasound among moderately severe acute IS patients with documented vascular occlusion already receiving rTPA [72]. The study was stopped prematurely due to significantly higher bleeding rates in those receiving ultrasound. Subsequent simulations showed that low-frequency ultrasound led to large standing waves and peak rarefactional pressure that was higher than the inertial acoustic cavitation threshold in large areas of the brain, even away from the targeted clot, leading to hemorrhage [73].
Table 2. Case-controlled studies and non-randomized trials of sonothrombolysis for acute ischemic stroke.
Table 2. Case-controlled studies and non-randomized trials of sonothrombolysis for acute ischemic stroke.
AuthorDaffertshofer M, et al. [72]Perren F, et al. [74]Rubiera M, et al.
[75]		Dinia L, et al.
[76]		Bardon P, et al.
[77]		Dwedar AZ, et al.
[78]		Reinhard M, et al.
[79]
Year of publication2005200820082009201220142015
Number of patients26
(14 vs. 12)		26
(11 vs. 15)		138
(91 vs. 47)		236
(138 vs. 98 historic controls)		49
(12 bilateral TCD vs. 37 unilateral TCD)		42
(21 vs. 21)		132
(73 EVT vs. 59 ST)
Age (yr)70.4 ± 9.761 ± 27 Average 64.1 ± 9.4
Range 47–78
vs.
Average 62.2 ± 12.1
Range 32–78		Mean
59.2 ± 10.6
vs.
59.2 ± 9.3
Range 40–70 		Median
71 (IQR 60–78)
vs.
75 (IQR 61–82)
Time windowMean 2.42 ± 0.50 h
(range 0.50–4.35 h)		≤3 h178 min (mean)≤3 hMean 133.8 ± 58.4 min
vs.
142.3 ± 56.6 min		Mean 5.02 ± 1.2 h
vs.
8.0 ± 2.2 h		Median 117 min
(IQR 95–116)
vs.
105 (IQR 83–148) and 234 (IQR 187–325) til DSA
Stroke type‘Vascular obstruction’ MCA occlusion MCA occlusionMCA occlusionM1 or carotid T occlusion
TechniqueTCDTCCDTCDTCDTCDTCDTCD
Frequency 300 kHz2 MHz2 MHz2 MHz2 MHz2 MHz1.6 MHz
Concomitant thrombolysisYesYes, plus Sonovue contrast agent perfusionYes, plus Levovist (galactose-based air-filled MB)Yes, plus 3 doses of 2.5 g of MB after tPA bolusNo vs. yesNoYes
ComparatorNo USGNo SonovueSonovue (sulfur hexafluoride-filled MB) instead of LevovistHistoric controls60-min bilateral 2-MHz pulsed-wave
Doppler monitoring of the area of occlusion
vs.
standard sonothrombolysis		Patients who did not receive 1 h continuous TCDThrombectomy
OutcomePartial or complete recanalization—28.6 vs. 50% (p = 0.2629)Recanalization 64% vs. 53%
Patients who received ECA improved their NIHSS significantly more than
those who were only TCCD monitored (Mann–Whitney U = 48.0; p = 0.050), and their
flow signal improved more (Mann–Whitney U = 40.0; p < 0.03).		Recanalization rates after 1 h (32.2% vs. 35.6%), 2 h (50.0% vs. 46.7%) and 6 h (63.8% vs. 54.5%) (p > 0.3).
Clinical improvement (NIHSS decrease ≥ 4 points) at 24 h (54.9% vs. 51.1%), (p = 0.400)
mRS ≤ 2 at 3 mo—44% vs. 48.5%		Recanalization rates higher in the MB compared with the control
group at 1, 2, 6, and 12 h (p < 0.05).
MB administration associated with higher degree of clinical improvement at 24 h (54.9% vs. 31.1%, p = 0.004)		Complete recanalization found in 30.0% of Group 1 and
32.4% of Group 2
Independent at 90 days—58.3% in Group 1 vs. 59.5% in Group 2		Mean flow velocity (MFV) in MCA one after the initial study, at 20 and 60 min—change in MFV after insonation for Group 1 in comparison to Group 2 at 3 time points was significantly high (p < 0.001).Functional independence (mRS 0–2) higher for
EVT (adjusted OR 3.89 (95% CI 1.36–12.58))
Ordinal mRS analysis favored EVT (adjusted common OR 1.70
(95% CI 0.88–3.31)).
Adverse eventsBleeding in MRI—92.9% vs. 33.3% (p < 0.01) Symptomatic intracranial hemorrhage 9% vs. 7% Symptomatic intracranial hemorrhage rate (3.3% vs. 2.1%, p = 0.580) MB administration associated with
an increased risk of hemorrhagic infarction (HI1-HI2 (21% vs. 12%, p = 0.026)
Parenchymal hematoma (PH1-PH2 and symptomatic intracranial hemorrhage)—similar in both groups		Symptomatic intracranial hemorrhage—2.7% of the Group 2NilSymptomatic intracerebral hemorrhage—4.1%
In EVT group
In a non-randomized clinical trial using TCCD, Perren et al. investigated the added value of adding the contrast agent Sonuvue to thrombolysis and ultrasound in 11 patients versus 15 controls. Those receiving contrast had improved flow signals and NIHSS scores [74].
Rubiera et al. compared the effects of two different MBs—galactose-based air-filled MBs (Levovist) (n = 91) and sulfur hexafluoride-filled MBs (Sonovue) (n = 47)—on recanalization and clinical outcomes among patients already receiving thrombolysis [75]. Recanalization rates, clinical improvement functional outcome, and symptomatic intracranial hemorrhage (ICH) rates were similar between the two groups.
Dinia et al. studied the risk of hemorrhagic transformation of administering MBs after thrombolysis and TCD for 138 IS patients, compared to 98 historical controls [76]. While the MB group had better recanalization and clinical improvement, there was also an increased risk of hemorrhagic transformation, but not symptomatic intracranial hemorrhage.
Bardon et al. conducted a pilot study comparing bilateral TCD monitoring among 12 IS patients contraindicated for thrombolysis, compared with 37 patients receiving thrombolysis and unilateral TCD—they found no difference in recanalization rates or 90-day functional outcomes [77].
In a study by Dwedar of moderately severe IS patients with MCA occlusion not receiving thrombolysis in 21 cases receiving TCD and 21 not receiving TCD, there were significantly better blood flow velocities among the cases with no bleeding events [78].
In this era of MT, Reinhard et al. compared EVT (n = 73) versus sonothrombolysis (n = 59) in acute IS patients with proximal MCA or carotid-T occlusion [79]. While they found that EVT led to better functional independence at the end of neurorehabilitation, this may apply more to the carotid-T occlusion group. EVT did carry a small bleeding risk.

9. Randomized Controlled Trials

Adequately powered randomized controlled trials (RCTs) are considered the gold standard to assess the efficacy and safety of medical interventions. There have been a number of RCTs of sonothrombolysis for acute stroke published since 2003 [80,81,82,83,84,85,86,87,88] (Table 3).
Eggers et al. were among the first to report a controlled trial involving patients with acute MCA occlusion who were receiving rTPA, with 11 undergoing continuous TCCD and the 14 controls not undergoing TCCD [75]. While there was a higher hemorrhagic rate among the cases, they also had a higher recanalization rate and a better functional outcome. The authors had similar findings in a similar trial conducted five years later [85].
The CLOTBUST trial by Alexandrov et al. built on their earlier work [66,68] by equally randomizing 126 patients with acute ischemic stroke from MCA occlusion receiving intravenous t-PA within three hours after the onset of symptoms to either receive continuous 2-MHz transcranial Doppler ultrasonography or a placebo [81]. The primary combined end point of complete recanalization as assessed by transcranial Doppler ultrasonography or dramatic clinical recovery at 24 h was seen significantly more in the intervention arm, but dramatic clinical recovery at 24 h and good functional outcome (mRS 0–1) at three months was not different.
As a corollary to their earlier trial [80], Eggers et al. studied the effect of TCCD on 15 patients with acute MCA occlusion who were contraindicated for thrombolysis [82]. By day four, recanalization and neurologic improvement were more frequent in the intervention group. There was no increase in hemorrhage. Ultrasound may have a role in clot lysis for patients contraindicated for thrombolytic therapy.
Molina et al. continued their work on MBs [83] by performing a three-arm trial comparing rTPA alone (n = 36), rTPA plus TCD (n = 37), and both with three doses of MBs (n = 38) among 111 patients with MCA occlusion [78]. Triple therapy led to the best recanalization and neurological outcome, with an increase in the risk of hemorrhage.
Alexandrov et al. performed a pilot safety trial of adding perflutren-lipid microspheres to TCD with thrombolysis in four cases: one control ratio in 15 patients with MCA occlusion [84]. There was no increase in hemorrhagic risk. Recanalization was better with the microspheres group than in the control arm of CLOTBUST [81].
MRX-801 microspheres were investigated by Molina et al. in the TUSCON trial of low vs. high vs. no microspheres among 36 patients with proximal intracranial occlusion receiving rTPA and TCD [86]. While recanalization was better among those receiving microspheres, the higher dose was associated with increased hemorrhage.
The NOR-SAS clinical trial by Nacu et al. involved administering the ultrasound contrast agent Sonuvue to 183 acute ischemic stroke patients also receiving TCD and rTPA [87]. There was no impact on neurological or functional outcome, or hemorrhage.
The most recent trial was CLOTBUST-ER by Alexandrov et al., delivering ultrasound using an operator-independent device to 676 patients with acute ischemic stroke receiving rTPA [88]. While safe, there was no improvement in functional outcome.
Most trials had small numbers except the one by Alexandrov et al. in 2019 [88]; most had time windows < 3 h; most used TCD, although Eggers et al. used TCCD in all their trials [80,82,85]; the ultrasound frequency was 1.8 to 2 MHz; almost all had concomitant rTPA except for the one by Eggers in 2005 [82]; and two by Molina et al. [83,86] and one by Alexandrov et al. [84] also tested the addition of MBs or microspheres [84,88].
Chen et al. performed a meta-analysis of seven RCTs (n = 549) of sonothrombolysis versus non-sonothrombolysis for acute IS [89]. Compared to no sonothrombolysis, sonothrombolysis improved complete recanalization (RR 2.16, 95% CI 1.51 to 3.08, p < 0.001), complete or partial recanalization (RR 1.90, 95% CI 1.26 to 2.88, p = 0.002), with a tendency to improvement of ≥4 points in NIHSS score (RR 1.43, 95% CI 0.99 to 2.07, p = 0.057). However, there were no significant differences in neurological recovery and adverse events. In a subgroup analysis, factors that may improve efficacy outcomes included concomitant use of t-PA, severe stroke (NIHSS > 15), treatment time ≤ 150 min, and a relatively younger age (≤65 years).
However, this meta-analysis did not include the largest trial by Alexandrov et al. [88]. A subsequent individual patient data meta-analysis of patients with proven large vessel occlusion did include this trial [90]. Among the seven randomized controlled clinical trials (n = 1102), 138 were randomized to treatment and 134 to control. Patients receiving sonothrombolysis were more likely to achieve complete recanalization compared with those receiving IVT only (40.3% vs. 22.4%; OR 2.17 [95% CI, 1.03–4.54]; adjusted OR, 2.33 [95% CI, 1.02–5.34]). There was no significantly increased risk of symptomatic intracranial hemorrhage (7.3% versus 3.7%; OR, 2.03 [95% CI, 0.68–6.11]; adjusted OR, 2.55 [95% CI, 0.76–8.52]). The likelihood of asymptomatic intracranial hemorrhage and functional independence at three months was similar.
A recent analysis [91] of studies using MBs and ultrasound in peripheral arterial thrombosis reviewed eight clinical stroke studies, including two case series [92,93]. There was high heterogeneity among the studies, which made it impossible to perform a meta-analysis. Still, overall, recanalization rates were higher in the groups that underwent contrast-enhanced sonothombolysis.

10. Progress in Ultrasound Delivery to Patients

The traditional ultrasound beam at a frequency of 2 MHz allows for the insonation of deeper structures but suffers from severe attenuation by the skull and the highly demanding skill needed to focus the beam at the site of occlusion [63]. The initial promise of an easy-to-use device using a low frequency of 300 kHz that would transgress the skull easily and not need precise targeting of the occlusion [33] was broken when the TRUMBI trial showed an unacceptable risk of ICH [72]. Progress was made when a hands-free, operator-independent device was developed and shown to be safe before being tested in the CLOTBUST-ER clinical trial [88].
Delivery of ultrasound intra-arterially was tested using the EkoSonic Endovascular System in a prospective study of 14 patients, mean age 65.1 ± 11.2 years, with moderate acute IS and occluded middle cerebral artery (n = 7) or basilar artery (n = 7), compared with historical controls [94]. Endovascular sonolysis was started within 8 h of stroke onset. Arterial recanalization was achieved in 85.7% of patients with MCA occlusion and 100% with BA occlusion. There were no symptomatic intracerebral hemorrhage nor periprocedural complications. The median mRS at 90 days was one (IQR 1–3.5) in MCA occlusion and three (IQR 2–4.5) in BA occlusion, compared to five (IQR 305) and six (IQG4.5–6), respectively, among the controls.

11. Stroke Prevention

In view of the risk of new brain ischemic lesions that may occur in up to two-thirds of patients undergoing coronary artery bypass grafting or cardiac valve surgery, Skoloudik et al. found in the randomized controlled SONORESCUE trial (n = 60 vs. 60, mean age 65.3 yr) that intra-operative sonolysis would reduce the risk of new lesions > 0.5 mL as well as the median volume of new ischemic lesions on diffusion-weighted imaging (DWI) MRI in this group of patients [95]. Clinical stroke or transient ischemic attack (TIA) occurred in 0% of treated vs. 3.3% of untreated patients (p = 0.496). The subsequent SONOREDUCE randomized controlled trial involving 144 patients undergoing coronary stenting only was neutral [96].
As silent brain infarctions may occur in up to one-third of patients undergoing carotid endarterectomy and two-thirds of those undergoing carotid angioplasty and/or stenting, Skoloudik et al. investigated in the randomized controlled SONOBUSTER trial the use of intraoperative sonolysis in these patients [97]. They found that new lesions on an MRI were again less frequent among the 121 patients (mean age, 66.65 ± 7.17 years) compared to 121 controls (75; 66.02 ± 8.11 years). Clinical stroke or TIA occurred in 0.8% vs. 2.5% respectively (p > 0.3).
In the randomized controlled SONOBIRDIE trial of sonolysis of patients while they were undergoing carotid endarterectomy, (n = 1004, mean age 68 ± 7.8 years), the primary composite outcome of ischemic stroke, TIA, or death within 30 days occurred in 2.2% vs. 7.6% in controls (risk difference 5.5%; 95% CI 2.8–8.3%; p < 0.001)—stroke/TIA occurred in 1.8% vs. 7.5% (p < 0.001) while a new ischemic lesion on an MRI was seen in 8.6% vs. 17.4% of patients (p < 0.01) [98].

12. Conclusions

Emergent recanalization of occluded arteries remains the holy grail of hyperacute therapy in ischemic stroke. IVT and, more recently, EVT for carefully selected patients are now the standard of care. Transcranial ultrasound either as TCD or TCCD, alone or in addition to IVT, for occluded arteries, in the 2 MHz range, has been shown in vitro and in vivo, both in animal models and humans, to aid thrombolysis and improve recanalization without significantly increasing the risk of symptomatic intracranial hemorrhage. The use of 300 kHz ultrasound is unsafe. The adjunctive use of MBs or microspheres has not shown a benefit in randomized controlled trials. Further evidence is needed on the clinical value of endovascular ultrasound. Other techniques explored in animal models, including the endovascular delivery of MBs, the use of IVTMBs filled with thrombolytics, and differentially shaped nanoparticles, await clinical trials. While much has been done, much more lies ahead as evidence is generated for the clinical role of sonothrombolysis in the management of acute ischemic stroke.

Author Contributions

Conceptualization, N.V., L.L.L.Y., B.T. and B.P.L.C.; methodology, N.V., L.L.L.Y., B.T. and B.P.L.C.; data curation, N.V.; writing—original draft preparation, N.V.; writing—review and editing, L.L.L.Y., B.T. and B.P.L.C.; visualization, N.V. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

This study did not require ethical approval.

Informed Consent Statement

Not applicable.

Data Availability Statement

No new data were created or analyzed in this study.

Conflicts of Interest

The authors declare no conflict of interest.

References

  1. GBD 2019 Stroke Collaborators. Global, regional, and national burden of stroke and its risk factors, 1990–2019: A systematic analysis for the Global Burden of Disease Study 2019. Lancet Neurol. 2021, 20, 795–820. [Google Scholar] [CrossRef] [PubMed]
  2. Saver, J.L. Time is brain—Quantified. Stroke 2006, 37, 263–266. [Google Scholar] [CrossRef] [PubMed]
  3. Powers, W.J.; Rabinstein, A.A.; Ackerson, T.; Adeoye, O.M.; Bambakidis, N.C.; Becker, K.; Biller, J.; Brown, M.; Demaerschalk, B.M.; Hoh, B.; et al. Guidelines for the Early Management of Patients with Acute Ischemic Stroke: 2019 Update to the 2018 Guidelines for the Early Management of Acute Ischemic Stroke: A Guideline for Healthcare Professionals from the American Heart Association/American Stroke Association. Stroke 2019, 50, e344–e418. [Google Scholar] [CrossRef] [PubMed]
  4. Kassem-Moussa, H.; Graffagnino, C. Nonocclusion and spontaneous recanalization rates in acute ischemic stroke: A review of cerebral angiography studies. Arch. Neurol. 2002, 59, 1870–1873. [Google Scholar] [CrossRef] [PubMed]
  5. Vang, C.; Dunbabin, D.; Kilpatrick, D. Effects of spontaneous recanalization on functional and electrophysiological recovery in acute ischemic stroke. Stroke 1999, 30, 2119–2125. [Google Scholar] [CrossRef] [PubMed]
  6. Camara, R.; Matei, N.; Zhang, J.H. Evolution of the stroke paradigm: A review of delayed recanalization. J. Cereb. Blood Flow Metab. 2021, 41, 945–957. [Google Scholar] [CrossRef] [PubMed]
  7. Gourdin, M.J.; Bree, B.; De Kock, M. The impact of ischaemia-reperfusion on the blood vessel. Eur. J. Anaesthesiol. 2009, 26, 537–547. [Google Scholar] [CrossRef]
  8. Kovacs, I.B.; Yamamoto, J. Spontaneous thrombolysis: A forgotten determinant of life or death. Clin. Appl. Thromb. Hemost. 2006, 12, 358–363. [Google Scholar] [CrossRef]
  9. Mican, J.; Toul, M.; Bednar, D.; Damborsky, J. Structural Biology and Protein Engineering of Thrombolytics. Comput. Struct. Biotechnol. J. 2019, 17, 917–938. [Google Scholar] [CrossRef]
  10. Wardlaw, J.M.; Murray, V.; Berge, E.; del Zoppo, G.J. Thrombolysis for acute ischaemic stroke. Cochrane Database Syst. Rev. 2014, 2014, CD000213. [Google Scholar] [CrossRef]
  11. Berge, E.; Whiteley, W.; Audebert, H.; De Marchis, G.M.; Fonseca, A.C.; Padiglioni, C.; de la Ossa, N.P.; Strbian, D.; Tsivgoulis, G.; Turc, G. European Stroke Organisation (ESO) guidelines on intravenous thrombolysis for acute ischaemic stroke. Eur. Stroke J. 2021, 6, I–LXII. [Google Scholar] [CrossRef]
  12. Goyal, M.; Menon, B.K.; van Zwam, W.H.; Dippel, D.W.; Mitchell, P.J.; Demchuk, A.M.; Dávalos, A.; Majoie, C.B.; van der Lugt, A.; de Miquel, M.A.; et al. Endovascular thrombectomy after large-vessel ischaemic stroke: A meta-analysis of individual patient data from five randomised trials. Lancet 2016, 387, 1723–1731. [Google Scholar] [CrossRef]
  13. Zheng, M.; Li, L.; Chen, L.; Li, B.; Feng, C. Mechanical thrombectomy combined with intravenous thrombolysis for acute ischemic stroke: A systematic review and meta-analyses. Sci. Rep. 2023, 13, 8597. [Google Scholar] [CrossRef]
  14. Qureshi, A.I.; Lodhi, A.; Akhtar, I.N.; Ma, X.; Kherani, D.; Kwok, C.S.; Ford, D.E.; Hanley, D.F.; Hassan, A.E.; Nguyen, T.N.; et al. Mechanical thrombectomy with intra-arterial thrombolysis versus mechanical thrombectomy alone in patients with acute ischemic stroke: A systematic review and meta-analysis. Int. J. Stroke 2024, 19, 16–28. [Google Scholar] [CrossRef]
  15. Atchley, T.J.; Estevez-Ordonez, D.; Laskay, N.M.B.; Tabibian, B.E.; Harrigan, M.R. Endovascular Thrombectomy for the Treatment of Large Ischemic Stroke: A Systematic Review and Meta-Analysis of Randomized Control Trials. Neurosurgery 2024, 94, 29–37. [Google Scholar] [CrossRef]
  16. Grogan, S.P.; Mount, C.A. Ultrasound Physics and Instrumentation. [Updated 27 March 2023]. In StatPearls [Internet]; StatPearls Publishing: Treasure Island, FL, USA, 2023. Available online: https://www.ncbi.nlm.nih.gov/books/NBK570593/ (accessed on 13 February 2024).
  17. Goldman, D.E.; Lepeschkin, W.W. Injury to living cells in standing sound waves. J. Cell Comp. Physiol. 1952, 40, 255–268. [Google Scholar] [CrossRef] [PubMed]
  18. Miller, M.W.; Miller, D.L.; Brayman, A.A. A review of in vitro bioeffects of inertial ultrasonic cavitation from a mechanistic perspective. Ultrasound Med. Biol. 1996, 22, 1131–1154. [Google Scholar] [CrossRef] [PubMed]
  19. Burstein, M.; Lewi, S. Action des ultrasons sur le caillot plasmatique [Effect of ultrasonics on plasma clot]. C. R. Seances Soc. Biol. Fil. 1951, 145, 1599–1600. [Google Scholar]
  20. Burstein, M.; Lewi, S. Sur les propriétés physiques du caillot plasmatique; compressibilité et rétraction par ultrasons [The physical properties of the plasma clot; compressibility and retraction by ultrasonics]. C. R. Seances Soc. Biol. Fil. 1952, 146, 1544–1546. [Google Scholar] [PubMed]
  21. Howkins, S.D.; Weinstock, A. The effect of focused ultrasound on human blood. Ultrasonics 1970, 8, 174–176. [Google Scholar] [CrossRef]
  22. Francis, C.W.; Suchkova, V.N. Ultrasound and thrombolysis. Vasc. Med. 2001, 6, 181–187. [Google Scholar] [CrossRef]
  23. Francis, C.W. Ultrasound-enhanced thrombolysis. Echocardiography 2001, 18, 239–246. [Google Scholar] [CrossRef] [PubMed]
  24. Bader, K.B.; Gruber, M.J.; Holland, C.K. Shaken and stirred: Mechanisms of ultrasound-enhanced thrombolysis. Ultrasound Med. Biol. 2015, 41, 187–196. [Google Scholar] [CrossRef] [PubMed]
  25. Sobbe, A.; Stumpff, U.; Trübestein, G.; Figge, H.; Kozuschek, W. Die Ultraschall Auflösung von Thromben [Thrombolysis by ultrasound (author’s transl)]. Klin. Wochenschr. 1974, 52, 1117–1121. [Google Scholar] [CrossRef] [PubMed]
  26. Ehringer, H.; Fischer, M. Erfolgreiche thrombolytische Therapie bei subakuten arteriellen Thrombosen. Vorläufiger Bericht. [Successful thrombolytic therapy in subacute arterial thrombosis. Preliminary report]. Med. Welt. 1968, 32, 1726–1728. [Google Scholar] [PubMed]
  27. Luo, H.; Nishioka, T.; Fishbein, M.C.; Cercek, B.; Forrester, J.S.; Kim, C.J.; Berglund, H.; Siegel, R.J. Transcutaneous ultrasound augments lysis of arterial thrombi in vivo. Circulation 1996, 94, 775–778. [Google Scholar] [CrossRef] [PubMed]
  28. Burgess, A.; Huang, Y.; Waspe, A.C.; Ganguly, M.; Goertz, D.E.; Hynynen, K. High-intensity focused ultrasound (HIFU) for dissolution of clots in a rabbit model of embolic stroke. PLoS ONE 2012, 7, e42311. [Google Scholar] [CrossRef] [PubMed]
  29. Daffertshofer, M.; Huang, Z.; Fatar, M.; Popolo, M.; Schroeck, H.; Kuschinsky, W.; Moskowitz, M.A.; Hennerici, M.G. Efficacy of sonothrombolysis in a rat model of embolic ischemic stroke. Neurosci. Lett. 2004, 361, 115–119. [Google Scholar] [CrossRef]
  30. Damianou, C.; Hadjisavvas, V.; Mylonas, N.; Couppis, A.; Ioannides, K. MRI-guided sonothrombolysis of rabbit carotid artery. J. Stroke Cerebrovasc. Dis. 2014, 23, e113–e121. [Google Scholar] [CrossRef]
  31. Damianou, C.; Hadjisavvas, V.; Ioannides, K. In Vitro and In Vivo evaluation of a magnetic resonance imaging-guided focused ultrasound system for dissolving clots in combination with thrombolytic drugs. J. Stroke Cerebrovasc. Dis. 2014, 23, 1956–1964. [Google Scholar] [CrossRef]
  32. Eggers, J.; Ossadnik, S.; Seidel, G. Enhanced clot dissolution in vitro by 1.8-MHz pulsed ultrasound. Ultrasound Med. Biol. 2009, 35, 523–526. [Google Scholar] [CrossRef] [PubMed]
  33. Wright, C.C.; Hynynen, K.; Goertz, D.E. Pulsed focused ultrasound-induced displacements in confined in vitro blood clots. IEEE Trans. Biomed. Eng. 2012, 59, 842–851. [Google Scholar] [CrossRef] [PubMed]
  34. Hölscher, T.; Raman, R.; Fisher, D.J.; Ahadi, G.; Zadicario, E.; Voie, A. Effects of varying duty cycle and pulse width on high-intensity focused ultrasound (HIFU)-induced transcranial thrombolysis. J. Ther. Ultrasound 2013, 1, 18. [Google Scholar] [CrossRef] [PubMed]
  35. Daffertshofer, M.; Hennerici, M.G. Sonothrombolysis: Experimental evidence. Front. Neurol. Neurosci. 2006, 21, 140–149. [Google Scholar] [CrossRef]
  36. Rosenschein, U.; Furman, V.; Kerner, E.; Fabian, I.; Bernheim, J.; Eshel, Y. Ultrasound imaging-guided noninvasive ultrasound thrombolysis: Preclinical results. Circulation 2000, 102, 238–245. [Google Scholar] [CrossRef]
  37. Maxwell, A.D.; Cain, C.A.; Duryea, A.P.; Yuan, L.; Gurm, H.S.; Xu, Z. Noninvasive thrombolysis using pulsed ultrasound cavitation therapy—Histotripsy. Ultrasound Med. Biol. 2009, 35, 1982–1994. [Google Scholar] [CrossRef]
  38. Ahadi, G.; Welch, C.S.; Grimm, M.J.; Fisher, D.J.; Zadicario, E.; Ernström, K.; Voie, A.H.; Hölscher, T. Transcranial sonothrombolysis using high-intensity focused ultrasound: Impact of increasing output power on clot fragmentation. J. Ther. Ultrasound 2013, 1, 22. [Google Scholar] [CrossRef]
  39. Chen, X.; Leeman, J.E.; Wang, J.; Pacella, J.J.; Villanueva, F.S. New insights into mechanisms of sonothrombolysis using ultra-high-speed imaging. Ultrasound Med. Biol. 2014, 40, 258–262. [Google Scholar] [CrossRef]
  40. Weiss, H.L.; Selvaraj, P.; Okita, K.; Matsumoto, Y.; Voie, A.; Hoelscher, T.; Szeri, A.J. Mechanical clot damage from cavitation during sonothrombolysis. J. Acoust. Soc. Am. 2013, 133, 3159–3175. [Google Scholar] [CrossRef]
  41. Petit, B.; Bohren, Y.; Gaud, E.; Bussat, P.; Arditi, M.; Yan, F.; Tranquart, F.; Allémann, E. Sonothrombolysis: The contribution of stable and inertial cavitation to clot lysis. Ultrasound Med. Biol. 2015, 41, 1402–1410. [Google Scholar] [CrossRef] [PubMed]
  42. Papadopoulos, N.; Yiallouras, C.; Damianou, C. The Enhancing Effect of Focused Ultrasound on TNK-Tissue Plasminogen Activator-Induced Thrombolysis Using an In Vitro Circulating Flow Model. J. Stroke Cerebrovasc. Dis. 2016, 25, 2891–2899. [Google Scholar] [CrossRef]
  43. Braun, T.; Sünner, L.; Hachenberger, M.; Müller, C.; Wietelmann, A.; Juenemann, M.; Pons-Kühnemann, J.; Kaps, M.; Gerriets, T.; Tschernatsch, M.; et al. Microbubble-mediated sonothrombolysis with BR38 of a venous full blood thrombus in a rat embolic stroke model. Ann. Transl. Med. 2021, 9, 1061. [Google Scholar] [CrossRef]
  44. Auboire, L.; Sennoga, C.A.; Hyvelin, J.M.; Ossant, F.; Escoffre, J.M.; Tranquart, F.; Bouakaz, A. Microbubbles combined with ultrasound therapy in ischemic stroke: A systematic review of in-vivo preclinical studies. PLoS ONE 2018, 13, e0191788. [Google Scholar] [CrossRef] [PubMed]
  45. Burns, P.N. Overview of echo-enhanced vascular ultrasound imaging for clinical diagnosis in neurosonology. J. Neuroimaging 1997, 7 (Suppl. 1), S2–S14. [Google Scholar] [PubMed]
  46. Nedelmann, M.; Ritschel, N.; Doenges, S.; Langheinrich, A.C.; Acker, T.; Reuter, P.; Yeniguen, M.; Pukropski, J.; Kaps, M.; Mueller, C.; et al. Combined contrast-enhanced ultrasound and rt-PA treatment is safe and improves impaired microcirculation after reperfusion of middle cerebral artery occlusion. J. Cereb. Blood Flow Metab. 2010, 30, 1712–1720. [Google Scholar] [CrossRef] [PubMed]
  47. Brown, A.T.; Flores, R.; Hamilton, E.; Roberson, P.K.; Borrelli, M.J.; Culp, W.C. Microbubbles improve sonothrombolysis in vitro and decrease hemorrhage in vivo in a rabbit stroke model. Investig. Radiol. 2011, 46, 202–207. [Google Scholar] [CrossRef]
  48. Pajek, D.; Burgess, A.; Huang, Y.; Hynynen, K. High-intensity focused ultrasound sonothrombolysis: The use of perfluorocarbon droplets to achieve clot lysis at reduced acoustic power. Ultrasound Med. Biol. 2014, 40, 2151–2161. [Google Scholar] [CrossRef] [PubMed]
  49. Culp, W.C.; Flores, R.; Brown, A.T.; Lowery, J.D.; Roberson, P.K.; Hennings, L.J.; Woods, S.D.; Hatton, J.H.; Culp, B.C.; Skinner, R.D.; et al. Successful microbubble sonothrombolysis without tissue-type plasminogen activator in a rabbit model of acute ischemic stroke. Stroke 2011, 42, 2280–2285. [Google Scholar] [CrossRef] [PubMed]
  50. Schleicher, N.; Tomkins, A.J.; Kampschulte, M.; Hyvelin, J.M.; Botteron, C.; Juenemann, M.; Yeniguen, M.; Krombach, G.A.; Kaps, M.; Spratt, N.J.; et al. Sonothrombolysis with BR38 Microbubbles Improves Microvascular Patency in a Rat Model of Stroke. PLoS ONE 2016, 11, e0152898. [Google Scholar] [CrossRef] [PubMed]
  51. de Saint Victor, M.; Barnsley, L.C.; Carugo, D.; Owen, J.; Coussios, C.C.; Stride, E. Sonothrombolysis with Magnetically Targeted Microbubbles. Ultrasound Med. Biol. 2019, 45, 1151–1163. [Google Scholar] [CrossRef] [PubMed]
  52. Choi, W.; Key, J.; Youn, I.; Lee, H.; Han, S. Cavitation-assisted sonothrombolysis by asymmetrical nanostars for accelerated thrombolysis. J. Control Release 2022, 350, 870–885. [Google Scholar] [CrossRef]
  53. Guo, S.; Guo, X.; Wang, X.; Zhou, D.; Du, X.; Han, M.; Zong, Y.; Wan, M. Reduced clot debris size in sonothrombolysis assisted with phase-change nanodroplets. Ultrason. Sonochem. 2019, 54, 183–191. [Google Scholar] [CrossRef]
  54. Wu, H.; Tang, Y.; Zhang, B.; Klippel, P.; Jing, Y.; Yao, J.; Jiang, X. Miniaturized Stacked Transducer for Intravascular Sonothrombolysis with Internal-Illumination Photoacoustic Imaging Guidance and Clot Characterization. IEEE Trans. Biomed. Eng. 2023, 70, 2279–2288. [Google Scholar] [CrossRef]
  55. Soltani, A.; Singhal, R.; Obtera, M.; Roy, R.A.; Clark, W.M.; Hansmann, D.R. Potentiating intra-arterial sonothrombolysis for acute ischemic stroke by the addition of the ultrasound contrast agents (Optison™ & SonoVue(®)). J. Thromb. Thrombolysis 2011, 31, 71–84. [Google Scholar] [CrossRef] [PubMed]
  56. Dixon, A.J.; Li, J.; Rickel, J.R.; Klibanov, A.L.; Zuo, Z.; Hossack, J.A. Efficacy of Sonothrombolysis Using Microbubbles Produced by a Catheter-Based Microfluidic Device in a Rat Model of Ischemic Stroke. Ann. Biomed. Eng. 2019, 47, 1012–1022. [Google Scholar] [CrossRef] [PubMed]
  57. Wu, H.; Zhang, B.; Huang, C.C.; Peng, C.; Zhou, Q.; Jiang, X. Ultrasound-Guided Intravascular Sonothrombolysis with a Dual Mode Ultrasound Catheter: In Vitro Study. IEEE Trans. Ultrason. Ferroelectr. Freq. Control. 2022, 69, 1917–1925. [Google Scholar] [CrossRef] [PubMed]
  58. Shekhar, H.; Kleven, R.T.; Peng, T.; Palaniappan, A.; Karani, K.B.; Huang, S.; McPherson, D.D.; Holland, C.K. In vitro characterization of sonothrombolysis and echocontrast agents to treat ischemic stroke. Sci. Rep. 2019, 9, 9902. [Google Scholar] [CrossRef] [PubMed]
  59. Zhou, Y.; Murugappan, S.K.; Sharma, V.K. Effect of clot aging and cholesterol content on ultrasound-assisted thrombolysis. Transl. Stroke Res. 2014, 5, 627–634. [Google Scholar] [CrossRef]
  60. Tomkins, A.J.; Schleicher, N.; Murtha, L.; Kaps, M.; Levi, C.R.; Nedelmann, M.; Spratt, N.J. Platelet rich clots are resistant to lysis by thrombolytic therapy in a rat model of embolic stroke. Exp. Transl. Stroke Med. 2015, 7, 2. [Google Scholar] [CrossRef]
  61. Black, J.J.; Yu, F.T.; Schnatz, R.G.; Chen, X.; Villanueva, F.S.; Pacella, J.J. Effect of Thrombus Composition and Viscosity on Sonoreperfusion Efficacy in a Model of Micro-Vascular Obstruction. Ultrasound Med. Biol. 2016, 42, 2220–2231. [Google Scholar] [CrossRef]
  62. Regenhardt, R.W.; Potter, C.A.; Huang, S.S.; Lev, M.H. Advanced Imaging for Acute Stroke Treatment Selection: CT, CTA, CT Perfusion, and MR Imaging. Radiol. Clin. N. Am. 2023, 61, 445–456. [Google Scholar] [CrossRef] [PubMed]
  63. Wan, Y.; Teng, X.; Li, S.; Yang, Y. Application of transcranial Doppler in cerebrovascular diseases. Front. Aging Neurosci. 2022, 14, 1035086. [Google Scholar] [CrossRef] [PubMed]
  64. Baumgartner, R.W.; Mattle, H.P.; Aaslid, R. Transcranial color-coded duplex sonography, magnetic resonance angiography, and computed tomography angiography: Methods, applications, advantages, and limitations. J. Clin. Ultrasound 1995, 23, 89–111. [Google Scholar] [CrossRef] [PubMed]
  65. Sloan, M.A.; Alexandrov, A.V.; Tegeler, C.H.; Spencer, M.P.; Caplan, L.R.; Feldmann, E.; Wechsler, L.R.; Newell, D.W.; Gomez, C.R.; Babikian, V.L.; et al. Assessment: Transcranial Doppler ultrasonography: Report of the Therapeutics and Technology Assessment Subcommittee of the American Academy of Neurology. Neurology 2004, 62, 1468–1481. [Google Scholar] [CrossRef] [PubMed]
  66. Alexandrov, A.V.; Demchuk, A.M.; Felberg, R.A.; Christou, I.; Barber, P.A.; Burgin, W.S.; Malkoff, M.; Wojner, A.W.; Grotta, J.C. High rate of complete recanalization and dramatic clinical recovery during tPA infusion when continuously monitored with 2-MHz transcranial doppler monitoring. Stroke 2000, 31, 610–614. [Google Scholar] [CrossRef] [PubMed]
  67. Cintas, P.; Le Traon, A.P.; Larrue, V. High rate of recanalization of middle cerebral artery occlusion during 2-MHz transcranial color-coded Doppler continuous monitoring without thrombolytic drug. Stroke 2002, 33, 626–628. [Google Scholar] [CrossRef] [PubMed]
  68. Alexandrov, A.V.; Demchuk, A.M.; Burgin, W.S.; Robinson, D.J.; Grotta, J.C.; CLOTBUST Investigators. Ultrasound-enhanced thrombolysis for acute ischemic stroke: Phase I. Findings of the CLOTBUST trial. J. Neuroimaging 2004, 14, 113–117. [Google Scholar]
  69. Brunser, A.; Hoppe, A.; Muñoz, P.; Cárcamo, D.; Lavados, P.M.; Gaete, J.; Roldán, A.; Rivas, R. Sonotrombolisis en el ataque cerebrovascular isquémico: Once años de experiencia en Clínica Alemana de Santiago [Sonothrombolysis for acute ischemic stroke]. Rev. Med. Chil. 2014, 142, 1238–1244. [Google Scholar] [CrossRef]
  70. Gu, T.; Wester, P.; Johansson, E. Ny lovande behandling vid akut ischemisk stroke--Sonotrombolys kan förstärka effekten av intravenös trombolys [Promising new treatment for acute ischemic stroke--Sonothrombolysis can enhance the effect of intravenous thrombolysis]. Lakartidningen 2015, 112, C9LF. [Google Scholar]
  71. Aaron, S.; Mani, S.; Prabhakar, A.T.; Babu, P.S.; Kumar, S.; Benjamin, R.N.; Sivadasan, A.; Muthusamy, K.; Patil, A.K.; Mathew, V.; et al. Sonothrombolysis for acute ischemic stroke—Break on through to the other side. Neurol. India 2017, 65, 52–57. [Google Scholar] [CrossRef]
  72. Daffertshofer, M.; Gass, A.; Ringleb, P.; Sitzer, M.; Sliwka, U.; Els, T.; Sedlaczek, O.; Koroshetz, W.J.; Hennerici, M.G. Transcranial low-frequency ultrasound-mediated thrombolysis in brain ischemia: Increased risk of hemorrhage with combined ultrasound and tissue plasminogen activator: Results of a phase II clinical trial. Stroke 2005, 36, 1441–1446. [Google Scholar] [CrossRef]
  73. Baron, C.; Aubry, J.F.; Tanter, M.; Meairs, S.; Fink, M. Simulation of intracranial acoustic fields in clinical trials of sonothrombolysis. Ultrasound Med. Biol. 2009, 35, 1148–1158. [Google Scholar] [CrossRef]
  74. Perren, F.; Loulidi, J.; Poglia, D.; Landis, T.; Sztajzel, R. Microbubble potentiated transcranial duplex ultrasound enhances IV thrombolysis in acute stroke. J. Thromb. Thrombolysis 2008, 25, 219–223. [Google Scholar] [CrossRef]
  75. Rubiera, M.; Ribo, M.; Delgado-Mederos, R.; Santamarina, E.; Maisterra, O.; Delgado, P.; Montaner, J.; Alvarez-Sabín, J.; Molina, C.A. Do bubble characteristics affect recanalization in stroke patients treated with microbubble-enhanced sonothrombolysis? Ultrasound Med. Biol. 2008, 34, 1573–1577. [Google Scholar] [CrossRef]
  76. Dinia, L.; Rubiera, M.; Ribo, M.; Maisterra, O.; Ortega, G.; del Sette, M.; Alvarez-Sabin, J.; Molina, C.A. Reperfusion after stroke sonothrombolysis with microbubbles may predict intracranial bleeding. Neurology 2009, 73, 775–780. [Google Scholar] [CrossRef]
  77. Bardon, P.; Kuliha, M.; Herzig, R.; Kanovsky, P.; Skoloudik, D. Safety and efficacy of sonothrombolysis using bilateral TCD monitoring by diagnostic 2 MHz probes—A pilot study. Biomed. Pap. Med. Fac. Univ. Palacky Olomouc. Czech Repub. 2014, 158, 233–237. [Google Scholar] [CrossRef] [PubMed]
  78. Dwedar, A.Z.; Ashour, S.; Haroun, M.; El Nasser, A.A.; Moustafa, R.R.; Ibrahim, M.H.; Elsadek, A. Sonothrombolysis in acute middle cerebral artery stroke. Neurol. India 2014, 62, 62–65. [Google Scholar] [CrossRef] [PubMed]
  79. Reinhard, M.; Taschner, C.A.; Hörsch, N.; Allignol, A.; Maurer, C.J.; Niesen, W.D.; Lambeck, J.; Wallesch, C.W.; Urbach, H.; Weiller, C.; et al. Endovascular Treatment versus Sonothrombolysis for Acute Ischemic Stroke. Cerebrovasc. Dis. 2015, 40, 205–214. [Google Scholar] [CrossRef] [PubMed]
  80. Eggers, J.; Koch, B.; Meyer, K.; König, I.; Seidel, G. Effect of ultrasound on thrombolysis of middle cerebral artery occlusion. Ann. Neurol. 2003, 53, 797–800. [Google Scholar] [CrossRef]
  81. Alexandrov, A.V.; Molina, C.A.; Grotta, J.C.; Garami, Z.; Ford, S.R.; Alvarez-Sabin, J.; Montaner, J.; Saqqur, M.; Demchuk, A.M.; Moyé, L.A.; et al. Ultrasound-enhanced systemic thrombolysis for acute ischemic stroke. N. Engl. J. Med. 2004, 351, 2170–2178. [Google Scholar] [CrossRef]
  82. Eggers, J.; Seidel, G.; Koch, B.; König, I.R. Sonothrombolysis in acute ischemic stroke for patients ineligible for rt-PA. Neurology 2005, 64, 1052–1054. [Google Scholar] [CrossRef] [PubMed]
  83. Molina, C.A.; Ribo, M.; Rubiera, M.; Montaner, J.; Santamarina, E.; Delgado-Mederos, R.; Arenillas, J.F.; Huertas, R.; Purroy, F.; Delgado, P.; et al. Microbubble administration accelerates clot lysis during continuous 2-MHz ultrasound monitoring in stroke patients treated with intravenous tissue plasminogen activator. Stroke 2006, 37, 425–429. [Google Scholar] [CrossRef]
  84. Alexandrov, A.V.; Mikulik, R.; Ribo, M.; Sharma, V.K.; Lao, A.Y.; Tsivgoulis, G.; Sugg, R.M.; Barreto, A.; Sierzenski, P.; Malkoff, M.D.; et al. A pilot randomized clinical safety study of sonothrombolysis augmentation with ultrasound-activated perflutren-lipid microspheres for acute ischemic stroke. Stroke 2008, 39, 1464–1469. [Google Scholar] [CrossRef]
  85. Eggers, J.; König, I.R.; Koch, B.; Händler, G.; Seidel, G. Sonothrombolysis with transcranial color-coded sonography and recombinant tissue-type plasminogen activator in acute middle cerebral artery main stem occlusion: Results from a randomized study. Stroke 2008, 39, 1470–1475. [Google Scholar] [CrossRef] [PubMed]
  86. Molina, C.A.; Barreto, A.D.; Tsivgoulis, G.; Sierzenski, P.; Malkoff, M.D.; Rubiera, M.; Gonzales, N.; Mikulik, R.; Pate, G.; Ostrem, J.; et al. Transcranial ultrasound in clinical sonothrombolysis (TUCSON) trial. Ann. Neurol. 2009, 66, 28–38. [Google Scholar] [CrossRef]
  87. Nacu, A.; Kvistad, C.E.; Naess, H.; Øygarden, H.; Logallo, N.; Assmus, J.; Waje-Andreassen, U.; Kurz, K.D.; Neckelmann, G.; Thomassen, L. NOR-SASS (Norwegian Sonothrombolysis in Acute Stroke Study): Randomized Controlled Contrast-Enhanced Sonothrombolysis in an Unselected Acute Ischemic Stroke Population. Stroke 2017, 48, 335–341. [Google Scholar] [CrossRef]
  88. Alexandrov, A.V.; Köhrmann, M.; Soinne, L.; Tsivgoulis, G.; Barreto, A.D.; Demchuk, A.M.; Sharma, V.K.; Mikulik, R.; Muir, K.W.; Brandt, G.; et al. Safety and efficacy of sonothrombolysis for acute ischaemic stroke: A multicentre, double-blind, phase 3, randomised controlled trial. Lancet Neurol. 2019, 18, 338–347. [Google Scholar] [CrossRef]
  89. Chen, Z.; Xue, T.; Huang, H.; Xu, J.; Shankar, S.; Yu, H.; Wang, Z. Efficacy and safety of sonothombolysis versus non-sonothombolysis in patients with acute ischemic stroke: A meta-analysis of randomized controlled trials. PLoS ONE 2019, 14, e0210516. [Google Scholar] [CrossRef]
  90. Tsivgoulis, G.; Katsanos, A.H.; Eggers, J.; Larrue, V.; Thomassen, L.; Grotta, J.C.; Seitidis, G.; Schellinger, P.D.; Mavridis, D.; Demchuk, A.; et al. Sonothrombolysis in Patients with Acute Ischemic Stroke with Large Vessel Occlusion: An Individual Patient Data Meta-Analysis. Stroke 2021, 52, 3786–3795. [Google Scholar] [CrossRef]
  91. Nederhoed, J.H.; Tjaberinga, M.; Otten, R.H.J.; Evers, J.M.; Musters, R.J.P.; Wisselink, W.; Yeung, K.K. Therapeutic Use of Microbubbles and Ultrasound in Acute Peripheral Arterial Thrombosis: A Systematic Review. Ultrasound Med. Biol. 2021, 47, 2821–2838. [Google Scholar] [CrossRef]
  92. Pagola, J.; Ribo, M.; Alvarez-Sabín, J.; Lange, M.; Rubiera, M.; Molina, C.A. Timing of recanalization after microbubble-enhanced intravenous thrombolysis in basilar artery occlusion. Stroke 2007, 38, 2931–2934. [Google Scholar] [CrossRef]
  93. Ribo, M.; Molina, C.A.; Alvarez, B.; Rubiera, M.; Alvarez-Sabin, J.; Matas, M. Intra- arterial administration of microbubbles and continuous 2-MHz ultrasound insonation to enhance intra-arterial thrombolysis. J. Neuroimaging 2010, 20, 224–227. [Google Scholar] [CrossRef]
  94. Kuliha, M.; Roubec, M.; Jonszta, T.; Krajca, J.; Czerny, D.; Krajina, A.; Langová, K.; Herzig, R.; Procházka, V.; Školoudík, D. Safety and efficacy of endovascular sonolysis using the EkoSonic endovascular system in patients with acute stroke. AJNR Am. J. Neuroradiol. 2013, 34, 1401–1406. [Google Scholar] [CrossRef] [PubMed]
  95. Školoudík, D.; Hurtíková, E.; Brát, R.; Herzig, R.; SONORESCUE Trial Group. Sonolysis in Prevention of Brain Infarction During Cardiac Surgery (SONORESCUE): Randomized, Controlled Trial. Medicine 2016, 95, e3615. [Google Scholar] [CrossRef] [PubMed]
  96. Viszlayová, D.; Brozman, M.; Langová, K.; Herzig, R.; Školoudík, D.; a SONOREDUCE Trial Group. Sonolysis in risk reduction of symptomatic and silent brain infarctions during coronary stenting (SONOREDUCE): Randomized, controlled trial. Int. J. Cardiol. 2018, 267, 62–67. [Google Scholar] [CrossRef]
  97. Školoudík, D.; Kuliha, M.; Hrbáč, T.; Jonszta, T.; Herzig, R.; SONOBUSTER Trial Group. Sonolysis in Prevention of Brain Infarction During Carotid Endarterectomy and Stenting (SONOBUSTER): A randomized, controlled trial. Eur. Heart J. 2016, 37, 3096–3102. [Google Scholar] [CrossRef] [PubMed]
  98. Skoloudik, D.; Hrbáč, T.; Herzig, R.; Fiedler, J.; Beneš, V.; Kesnerova, P.; Kovar, M.; Vosko, M.; Nosal, V.; Beneš, V.; et al. Sonolysis in prevention of brain infarctions during internal carotid endarterectomy (SONOBIRDIE): The results of randomized controlled trial. Eur. Stroke J. 2023, 8, 680. [Google Scholar]
Table 1. Case series of sonothrombolysis for acute ischemic stroke.
Table 1. Case series of sonothrombolysis for acute ischemic stroke.
AuthorAlexandrov AV, et al. [66]Cintas, et al.
[67]		Alexandrov AV, et al.
[68]		Brunser A, et al.
[69]		Gu T, et al.
[70]		Aaron S, et al.
[71]
Year of publication200020022004201420152017
Number of patients40655612014
Age (yr)Mean 70 ± 16 Mean 54.3 ± 14.7 Mean 69 ± 15 Mean 66 ± 18Median 71
(IQR 63–82)		Mean 55
(range 32–76)
Time window (min)Mean 125 ± 52Mean 210 ± 86Mean 125 ± 36Mean 127 Median 98
(IQR 67–131)		Mean 138
(Range 65–256)
Stroke type‘Occluded vessels’
(MCA. ICA, BA)		MCA occlusion‘Proximal arterial occlusion’MCA occlusion ‘Flow obstruction’LA-AIS
TechniqueTCDTCCDTCDTCDTCDTCD
Frequency (MHz)222222
Concomitant thrombolysisYesNoYesYesYesYes
ComparatorNilNilNilNilNilNil
OutcomeRecanalization found at 45 ± 20 min—complete in 30%, partial in 40%.
Dramatic recovery (total NIHSS score < 3)—20%)—all had complete recanalization. Improvement by ≥10 NIHSS points or complete recovery—30% at the end of tPA infusion, 40% at 24 h
Improvement by ≥4 NIHSS points—62.5% at 24 h
3-month mortality—20%		Partial recanalization (blunted waveforms)—83%.
Mean time to beginning of recanalization
17.2 ± 9.6 min. Complete recanalization at 24 h—16.6%
Mean NIHSS score in patients who recanalized during monitoring—21.2 ± 4.1 at baseline, 19.2 ± 5 at 2 h, and 15.6 ± 3.4 at 24 h 		Complete recanalization within 2 h 36%. Dramatic recovery (NIHSS score ≤ 3)—20% at 2 h, 24% at 24 h.
Improvement by ≥4 NIHSS points—49% at 24 h		Complete recanalization—44.3%.
Modified Rankin Scale of 0–2 at 3 months—60%
Case fatality—9.8%		Full recanalization—29%
Full or partial recanalization—36%
3-month follow-up—76% ADL independent		TIBI residual flow grade of ≥2—83%. Immediate dramatic improvement (NIHSS score ≤ 3
points or improvement by ≥10 points)—30%;
within the next 24 h—50%.
At 6 months—mortality 11%,
mRS ≤ 2 63%
Adverse eventsSymptomatic intracerebral hemorrhage—7.5%No hemorrhageSymptomatic hemorrhage—5.5%Asymptomatic intracranial hemorrhage—9.8%No symptomatic intracranial bleedingSymptomatic hemorrhage—5.5%
Table 3. Randomized controlled trials of sonothrombolysis for acute ischemic stroke.
Table 3. Randomized controlled trials of sonothrombolysis for acute ischemic stroke.
AuthorEggers J, et al. [80]Alexandrov AV, et al. [81]Eggers J., et al.
[82]		Molina CA, et al. [83]Alexandrov AV, et al. [84]Eggers J, et al.
[85]		Molina CA, et al.
[86]		Nacu A, et al.
[87]		Alexandrov AV, et al. [88]
Year of publication200320042005200620082008200920172019
Number of patients11 vs. 14 controls63 vs. 63 controls8 vs. 738 vs. 37 vs. 3612 vs. 319 vs. 1812 vs. 11 vs. 1293 vs. 90335 vs. 341
Age (yr)61 ± 967 ± 12
70 ± 13		58.968 ± 12 vs. 70 ± 9 vs. 68 ± 1175 ± 13 vs. 58 ± 3361 ± 10 68.8 ± 16.270
Time window144.2 min150 vs. 130 min213.4 min158 ± 35 vs. 161 ± 38 vs. 152 ± 33<3 h143.2<3 h170 ± 69121.5
Stroke typeMCA occlusionMCA occlusionMCA occlusionMCA occlusionMCA occlusionMCA occlusion‘Proximal intracranial occlusion’Acute ISAcute IS
TechniqueTCCDTCDTCCDTCDTCDTCCDTCDTCDTCD
Frequency2 MHz2 MHz2 MHz2 MHz2 MHz1.8 MHz2 Mz2 MHz2 MHz
Concomitant thrombolysisYesYesNoYes, plus TCD plus 3 doses of 2.5 g of MB after tPA bolusYes, plus 2.8 mL microS (perflutren-lipid microspheres)YesYes, plus microS (MRX-801) infusion 1.4 mL or 2.8 mLYes, plus TCD plus contrastYes
ComparatorNo ultrasonographyNo TCDNo USGrTPA plus TCD
vs.
rTPA only		No microS No USGNo microS (MRX-801)No contrastNo USG
OutcomeRecanalization 27.3 vs. 21.4%
3-month favorable functional outcome
54.5% vs. 36.3%		Complete recanalization or dramatic clinical
recovery within two hours after the administration of a t-PA bolus—49% vs. 30% p = 0.03).
At 24 h, dramatic clinical recovery—44% vs. 40% (p = 0.7).
At three
months, mRS 0–1
42 % vs. 29%
(p = 0.20).		Recanalization 62.5% vs. 0%
3-month favorable functional outcome 25% vs. 0%		Two-hour recanalization was seen in 71% vs. 68% vs. 39%
>4 point improvement of NIHSS score at 24 h—55% vs. 41% vs. 31%		At 2 h, sustained complete recanalization—42% in treatment arm
NIHSS scores 0 to 3—17% in treatment arm		Recanalization
(complete or partial) after 1 h 57.9% vs. 22.2% (p = 0.045)
US group
showed greater improvement in National Institutes of Health Stroke Scale values
at days 1 and 4
After 90 days,
modified Rankin Score ≤1—21.1% vs. 0% (p = 0.106)
Barthel Index ≥ 95—42.1% vs. 0% (p = 0.003)		Sustained complete
67% vs. 46% vs. 33% (p = 0.255)
3-month clinical recovery rates
75% vs. 50% vs. 36% (p = 0.167).		Neurological improvement at 24 h—51% vs. 46%
90 days mRS 0–1—48% vs. 51%
Death 6% vs. 9%		Improvement in modified Rankin Scale score at 90 days—31.3% vs. 32.0% (p = 0.74).
Mortality 16% vs. 13% (p = 0.37)
Adverse eventsSymptomatic intracranial hemorrhage 18.2% vs. 0%Symptomatic
intracerebral hemorrhage 4.8% in both groups		Symptomatic intracranial hemorrhage 0% vs. 14.3%Symptomatic intracranial hemorrhage 2.6% vs. 2.7% vs. 5.5%Symptomatic intracranial hemorrhage 0%
Asymptomatic intracranial hemorrhage
25% vs. 33.3%		Symptomatic intracranial
hemorrhage 15.8% vs. 5.6%		Symptomatic intracranial hemorrhage 0% vs. 25% vs. 0%Symptomatic intracerebral hemorrhage 2% vs. 4%Symptomatic intracranial hemorrhage 2.5% vs. 1.5%
Disclaimer/Publisher’s Note: The statements, opinions and data contained in all publications are solely those of the individual author(s) and contributor(s) and not of MDPI and/or the editor(s). MDPI and/or the editor(s) disclaim responsibility for any injury to people or property resulting from any ideas, methods, instructions or products referred to in the content.

Share and Cite

MDPI and ACS Style

Venketasubramanian, N.; Yeo, L.L.L.; Tan, B.; Chan, B.P.L. Sonothrombolysis for Ischemic Stroke. J. Cardiovasc. Dev. Dis. 2024, 11, 75. https://doi.org/10.3390/jcdd11030075

AMA Style

Venketasubramanian N, Yeo LLL, Tan B, Chan BPL. Sonothrombolysis for Ischemic Stroke. Journal of Cardiovascular Development and Disease. 2024; 11(3):75. https://doi.org/10.3390/jcdd11030075

Chicago/Turabian Style

Venketasubramanian, Narayanaswamy, Leonard L. L. Yeo, Benjamin Tan, and Bernard P. L. Chan. 2024. "Sonothrombolysis for Ischemic Stroke" Journal of Cardiovascular Development and Disease 11, no. 3: 75. https://doi.org/10.3390/jcdd11030075

Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.

Article Metrics

Back to TopTop