Focused ultrasound–mediated blood-brain barrier opening in Alzheimer’s disease: long-term safety, imaging, and cognitive outcomes

Rezai, Ali R.; Ranjan, Manish; Haut, Marc W.; Carpenter, Jeffrey; D’Haese, Pierre-François; Mehta, Rashi I.; Najib, Umer; Wang, Peng; Claassen, Daniel O.; Chazen, J. Levi; Krishna, Vibhor; Deib, Gerard; Zibly, Zion; Hodder, Sally; Wilhelmsen, Kirk C.; Finomore, Victor; Konrad, Peter; Kaplitt, Michael G.

doi:10.3171/2022.9.jns221565

Cited by 31 publications

(39 citation statements)

References 48 publications

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“…With BBB limiting an estimated 99.8 % of peripherally administered large molecule drugs such as therapeutics antibodies (95), we next tested the possibility of enhancing the permeabilisation of ALS BBB to large molecules with FUS +MB . As a proof-of-concept, we trialled the delivery of anti-TDP-43 antibody, considering promising preclinical development of TDP-43 targeted immunotherapies (96)(97)(98)(99) as well as the recent clinical success of therapeutic antibodies in the treatment of other neurodegenerative disorders (100)(101)(102)(103)(104). Although the utilised anti-TDP-43 antibody has not yet proved therapeutically beneficial, we were previously successful in delivering Aducanumab (Aduhelm TM ) and anti-tau therapeutic antibodies with FUS +MB in human Alzheimer's disease in vitro models (37,41); and a recent clinical study demonstrated beneficial effects of Aducanumab combined with FUS +MB in Alzheimer's disease patients, as compared to Aducanumab alone (104).…”

Section: Discussionmentioning

confidence: 99%

“…As a proof-of-concept, we trialled the delivery of anti-TDP-43 antibody, considering promising preclinical development of TDP-43 targeted immunotherapies (96)(97)(98)(99) as well as the recent clinical success of therapeutic antibodies in the treatment of other neurodegenerative disorders (100)(101)(102)(103)(104). Although the utilised anti-TDP-43 antibody has not yet proved therapeutically beneficial, we were previously successful in delivering Aducanumab (Aduhelm TM ) and anti-tau therapeutic antibodies with FUS +MB in human Alzheimer's disease in vitro models (37,41); and a recent clinical study demonstrated beneficial effects of Aducanumab combined with FUS +MB in Alzheimer's disease patients, as compared to Aducanumab alone (104). Hence, we hypothesised that analogously, achieving increased permeability of this model anti-TDP-43 antibody in our cell platform could be representative of future clinically approved ALS immunotherapeutics.…”

Section: Discussionmentioning

confidence: 99%

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A patient-derived amyotrophic lateral sclerosis blood-brain barrier cell model reveals focused ultrasound-mediated anti-TDP-43 antibody delivery

Wasielewska,

Castro Cabral-da-Silva,

Pecoraro

et al. 2024

Preprint

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BackgroundAmyotrophic lateral sclerosis (ALS) is a rapidly progressing neurodegenerative disorder with minimally effective treatment options. An important hurdle in ALS drug development is the non-invasive therapeutic access to the motor cortex currently limited by the presence of the blood-brain barrier (BBB). Focused ultrasound and microbubble (FUS+MB) treatment is an emerging technology that was successfully used in ALS patients to temporarily open the cortical BBB. However, FUS+MB-mediated drug delivery across ALS patients’ BBB has not yet been reported. Similarly, the effects of FUS+MBon human ALS BBB cells remain unexplored.MethodsHere we established the first FUS+MB-compatible, fully-human ALS patient-cell-derived BBB model based on induced brain endothelial-like cells (iBECs) to study anti-TDP-43 antibody delivery and FUS+MBbioeffectsin vitro.ResultsGenerated ALS iBECs recapitulated disease-specific hallmarks of BBB pathology, including changes to BBB integrity, permeability and TDP-43 proteinopathy. Our results also identified differences between sporadic ALS and familial (C9orf72expansion carrying) ALS iBECs reflecting patient heterogeneity associated with disease subgroups. Studies in these models revealed successful ALS iBEC monolayer openingin vitrowith a lack of adverse cellular effects of FUS+MB. This was accompanied by the molecular bioeffects of FUS+MBin ALS iBECs including changes in expression of tight and adherens junction markers, and drug transporter and inflammatory mediators, with sporadic and C9orf72 ALS iBECs generating transient specific responses. Additionally, we demonstrated an effective increase in the delivery of anti-TDP-43 antibody with FUS+MBin C9orf72 (2.7-fold) and sporadic (1.9-fold) ALS iBECs providing the first proof-of-concept evidence that FUS+MBcan be used to enhance the permeability of large molecule therapeutics across the BBB in a human ALSin vitromodel.ConclusionsTogether, our study describes the first characterisation of cellular and molecular responses of ALS iBECs to FUS+MBand provides a fully-human platform for FUS+MB-mediated drug delivery screening on an ALS BBBin vitromodel.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

A patient-derived amyotrophic lateral sclerosis blood-brain barrier cell model reveals focused ultrasound-mediated anti-TDP-43 antibody delivery

Wasielewska,

Castro Cabral-da-Silva,

Pecoraro

et al. 2024

Preprint

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“…While it has been suggested that, in some instances, the BBB integrity could already be compromised by the occurring disease [48], thus facilitating the trafficking of antibodies to the brain, the improvement of antibody delivery in the CNS is an area of active research. Recently, Alzheimer's disease researchers used focused ultrasound to disrupt specific sections of the BBB, leading to an improved penetration of antibeta-amyloid antibodies into the brain, focally enhancing the removal of amyloid plaques [49 ▪ ]. Increased transport through the BBB could also be achieved by creating antibodies with improved binding to Fc Receptor [50 ▪ ] or with bifunctional properties [51].…”

Section: Broadly Neutralizing Antibodiesmentioning

confidence: 99%

Strategies to target the central nervous system HIV reservoir

Mastrangelo,

Gama,

Cinque

2024

Current Opinion in HIV and AIDS

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Purpose of the review The central nervous system (CNS) is an hotspot for HIV persistence and may be a major obstacle to overcome for curative strategies. The peculiar anatomical, tissular and cellular characteristics of the HIV reservoir in the CNS may need to be specifically addressed to achieve a long-term HIV control without ART. In this review, we will discuss the critical challenges that currently explored curative strategies may face in crossing the blood–brain barrier (BBB), targeting latent HIV in brain-resident myeloid reservoirs, and eliminating the virus without eliciting dangerous neurological adverse events. Recent findings Latency reversing agents (LRA), broadly neutralizing monoclonal antibodies (bNabs), chimeric antigen receptor (CAR) T-cells, and adeno-associated virus 9-vectored gene-therapies cross the BBB with varying efficiency. Although brain penetration is poor for bNAbs, viral vectors for in vivo gene-editing, certain LRAs, and CAR T-cells may reach the cerebral compartment more efficiently. All these approaches, however, may encounter difficulties in eliminating HIV-infected perivascular macrophages and microglia. Safety, including local neurological adverse effects, may also be a concern, especially if high doses are required to achieve optimal brain penetration and efficient brain cell targeting. Summary Targeting the CNS remains a potential problem for the currently investigated HIV curing strategies. In vivo evidence on CNS effectiveness is limited for most of the investigated strategies, and additional studies should be focused on evaluating the interplay between the cerebral HIV reservoir and treatment aiming to achieve an ART-free cure.

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“…The primary objective of the study is to assess the safety and feasibility of FUS-induced BBBO in Alzheimer's disease patients, using a portable, noninvasive FUS system. Secondary objectives includes testing the feasibility of cavitation mapping and observing changes in 18 F-Florbetapir PET and in blood biomarkers. Six Alzheimer's disease patients (2M/4F, age = 69.7±7.2 yr) were enrolled in a phase 1 trial under FDA and Columbia University IRB approval (NCT04118764) (Table 1).…”

Section: Study Overviewmentioning

confidence: 99%

“…Figure 7 shows the percent changes in standard uptake value ratio (SUVR) or asymmetry SUVR of 18 F-Florbetapir compared to the baseline. Subject 3 was excluded due to the absence of BBBO.…”

Section: A Modest Decrease In Asymmetry Suvr Correlated With the Size...mentioning

confidence: 99%

Transcranial Blood–Brain Barrier Opening in Alzheimer’s Disease Patients Using a Portable Focused Ultrasound System with Real-Time 2-D Cavitation Mapping

Bae,

Liu,

Pouliopoulos

et al. 2023

Preprint

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Focused ultrasound (FUS) has recently shown great promise in facilitating blood-brain barrier opening (BBBO) for drug delivery and immunotherapy in Alzheimer’s disease. However, FUS-mediated BBBO treatment is currently limited to systems integrated with the MRI or post-surgical implants, thus restricting its widespread clinical adoption. In this pilot study, we present the outcomes of a phase 1 clinical study with mild to moderate Alzheimer’s disease patients (N=6) using a portable neuronavigated FUS system that did not require surgery or an online MRI during treatment. BBBO occurred in 5 out of 6 subjects with the volume of 983±626 mm3following a single session of FUS at the right frontal lobe. The outpatient treatment was completed within 34.8±10.7 min. Real-time cavitation monitoring was used to ensure the efficacy and safety of the BBBO procedure. Cavitation doses significantly correlated with the BBBO volume (R2>0.9, p<0.05), demonstrating the portable FUS system’s capability of predicting opening volumes. Larger BBBO volumes correlated with increased levels of Alzheimer’s disease biomarkers assayed in serum-derived extracellular vesicles, including Aβ42/Aβ40 (R2=0.74, p=0.1), Tau (R2=0.95, p=0.02), and P-Tau181 (R2=0.86, p=0.02), indicating the release of the two hallmark proteins into the bloodstream. Subjects showed a reduced Aβ accumulation rate in the treated frontal lobe region compared to the contralateral, as indicated by18F-Florbetapir PET scans. Clinical changes in mini-mental state examination over 6 months were within the expected range of decline. In conclusion, we have shown the safety and feasibility of this low-cost and portable FUS for BBBO in Alzheimer’s patients, providing a new avenue for FUS treatment in Alzheimer’s disease, with or without drug delivery.

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Focused ultrasound–mediated blood-brain barrier opening in Alzheimer’s disease: long-term safety, imaging, and cognitive outcomes

Cited by 31 publications

References 48 publications

A patient-derived amyotrophic lateral sclerosis blood-brain barrier cell model reveals focused ultrasound-mediated anti-TDP-43 antibody delivery

A patient-derived amyotrophic lateral sclerosis blood-brain barrier cell model reveals focused ultrasound-mediated anti-TDP-43 antibody delivery

Strategies to target the central nervous system HIV reservoir

Transcranial Blood–Brain Barrier Opening in Alzheimer’s Disease Patients Using a Portable Focused Ultrasound System with Real-Time 2-D Cavitation Mapping

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