Low intensity focused ultrasound stimulation in stroke: A phase I safety & feasibility trial
Ziping Huang, Charalambos C. Charalambous, Mengyue Chen, Taewon Kim, Estate M. Sokhadze, Allen W. Song, Sin-Ho Jung, Shashank Shekhar, Jody Feld, Xiaoning Jiang, Wuwei Feng
Abstract
Objective We aimed to determine the maximum safe spatial-peak pulse-average intensity (I SPPA ) of low-intensity focused ultrasound stimulation (LIFUS) in stroke patients and explore its effect on motor learning and corticospinal excitability. Methods We adopted the classic 3 + 3 design to escalate I SPPA (estimated in-vivo transcranial value) from 0, 1, 2, 4, 6, to 8 W/cm 2 . Stopping rules were pre-defined: 2 nd -degree scalp burn, clinical seizure, new lesion on diffusion-weighted imaging or major reduction in apparent diffusion coefficient, and participant discontinuation due to any reason. We applied 12-min LIFUS over the ipsilesional motor cortex while participants were concurrently practicing 3 blocks of a motor sequence learning (MSL) task using the affected hand. We measured MSL (response time) and corticospinal excitability (motor evoked potential) pre- and post-stimulation and compared MSL and corticospinal excitability between the LOW (0, 1, and 2 W/cm 2 ) and HIGH (4, 6, and 8 W/cm 2 ) groups. Results I SPPA was escalated to 8 W/cm 2 with 18 stroke participants without meeting the stopping rules. Compared to the LOW, more participants in the HIGH performed better on MSL (6/9 vs. 0/9, p = 0.009) and showed a sign of greater corticospinal excitability (7/9 vs. 5/9, p = 0.62). Interpretation Our phase-I safety study suggests that one session of LIFUS up to 8 W/cm 2 I SPPA is safe and feasible in stroke patients, and LIFUS at high intensity induces positive changes in both MSL and corticospinal excitability. The next logical step is to conduct a phase-II trial testing the efficacy of LIFUS and continuously monitoring its safety profiles.