Patent Application
20220395685
The present disclosure relates to botulinum toxin injections, more specifically, to devices, systems, and methods of mapping neuromuscular junctions for botulinum toxin injections.
Botulinum toxin (BoNT) injection for treatment of facial wrinkles is the most frequently performed cosmetic procedure in the United States, and it is one of the most common entry procedures for clinicians seeking to incorporate aesthetic treatments into their practice. Wrinkles are formed by dermal atrophy and repetitive contraction of underlying facial musculature. BoNT is a potent neurotoxin that inhibits release of acetylcholine at the neuromuscular junction (NMJ). Injection of appropriate quantities of NMJs into specific overactive muscles causes localized muscle relaxation that smooths the overlying skin and reduces wrinkles. BoNT effects take about two weeks to fully develop and last three to four months. Treatment of frown lines and crow's feet, which are the cosmetic indications approved by the U.S. Food and Drug Administration (FDA). It has become a common treatment for wrinkles occurring in the upper one-third of the face (i.e., frown lines, horizontal forehead lines, and crow's feet).
BoNT injection has been applied to facial muscles for noncosmetic uses including treatment of spastic facial dystonias, temporary treatment of idiopathic or thyroid dysfunction-induced upper eyelid retraction, suppression of undesired hyperlacrimation, induction of temporary ptosis by chemodenervation in facial paralysis, and correction of lower eyelid spastic entropion. Additional periocular uses include control of synchronic eyelid and extraocular muscle movements after aberrant regeneration of cranial nerve palsies.
Provided in accordance with aspects of the present disclosure is a system for mapping neuromuscular junctions for botulinum neurotoxin (BoNT) injections including a stimulation electrode configured to stimulate at least one nerve innervated with a facial muscle group in a body of a person. A stimulation electrode controller is in electrical communication with the stimulation electrode. An electromyography (EMG) sensor array includes a plurality of EMG sensors configured to be arranged about the person's face. Each EMG sensor detects muscle activity of at least one muscle of the facial muscle group. An EMG amplifier is in electrical communication with the stimulation electrode, the stimulation electrode controller and the EMG sensor array. The EMG amplifier includes a plurality of input channels. Each input channel receives data of facial muscle activity in the facial muscle group of the body of the person from the EMG sensor array. A computer is in communication with the EMG amplifier. The computer includes a processor and a memory. The processor identifies a plurality of neuromuscular junctions (NMJs) of the facial muscle group of the body of the person based on the data of facial muscle activity received from the EMG sensor array. The plurality of NMJs are mapped with respect to the at least one facial muscle group of the body of the person. At least one NMJ site for BoNT injection is recommended by the computer.
In an aspect of the present disclosure, the EMG sensors of the EMG sensor array are arranged on a flexible substrate configured to conform to contours of the person's face. The flexible substrate is formed of silicone.
In an aspect of the present disclosure, each EMG sensor array is a flexible surface EMG sensor array.
In an aspect of the present disclosure, the data of facial muscle activity includes data of at least one overactive facial muscle. The data of facial muscle activity includes a quantitative assessment of severity of overactivity in the at least one overactive facial muscle.
In an aspect of the present disclosure, the recommendation of at least one NMJ site for BoNT injection includes a recommendation of a particular BoNT dose.
In an aspect of the present disclosure, the recommendation of at least one NMJ site for BoNT injection includes a recommendation of a dosing schedule for BoNT.
In an aspect of the present disclosure, the EMG sensor array is configured to detect passive muscle activity and identify an occurrence of at least one spontaneous facial muscle spasm of a facial muscle group of the body of the person.
In an aspect of the present disclosure, the computer is wirelessly or cable connected with the EMG amplifier.
In an aspect of the present disclosure, the computer is included in a smartphone or tablet computer.
Provided in accordance with aspects of the present disclosure is a method for mapping neuromuscular junctions for BoNT injections including stimulating at least one nerve innervated with at least one facial muscle group in a body of a person. The method includes detecting muscle activity of at least one muscle of the at least one facial muscle group. The method includes receiving facial muscle activity in the at least one facial muscle group. The method includes mapping NMJs of the at least one facial muscle group of the body of the person based on the data of facial muscle activity received from the EMG sensor array. The method includes recommending at least one NMJ site for BoNT injection.
In an aspect of the present disclosure, the method includes recommending BoNT dosage for each BoNT injection.
Various aspects and features of the present disclosure are described hereinbelow with reference to the drawings wherein:
Descriptions of technical features or aspects of an exemplary configuration of the disclosure should typically be considered as available and applicable to other similar features or aspects in another exemplary configuration of the disclosure. Accordingly, technical features described herein according to one exemplary configuration of the disclosure may be applicable to other exemplary configurations of the disclosure, and thus duplicative descriptions may be omitted herein.
Exemplary configurations of the disclosure will be described more fully below (e.g., with reference to the accompanying drawings). Like reference numerals may refer to like elements throughout the specification and drawings.
The effectiveness of botulinum neurotoxin (BoNT) injections is a at least partially dependent on delivery of an appropriate dose to an appropriate injection site. Accurate localization of a BoNT injection to a desired neuromuscular junction (NMJ), for example, can minimize an effective dose and reduce or eliminate any known clinical side effects of BoNT injections. BoNT treatment has had problems with variable clinical effectiveness and high treatment cost. As BoNT acts at NMJs, injection directed to the proximity of NMJs will retain and potentiate the treatment efficacy while reducing dosage and consequently minimizing adverse effects and treatment cost. Injecting BoNT to non-NMJ locations requires larger injecting dosage compared to NMJ-target injection, as the injection needs to defuse to NMJs to be effective. Studies have demonstrated that increasing the injection distance by as little as 1 cm from the NMJ reduced the effect of BoNT by 46%.
Efforts have been taken to localize NMJ locations, however, there is no technology currently available for accurately localizing NMJ by eliminating the blurring effect caused by low-conductive fat and skin tissues, and the interfering effects (cross talk) caused by neighboring muscles. Furthermore, there is no technology currently available for correlating the severity assessment for specific overactive muscles with their NMJ locations to guide personalized precision BoNT injection.
The minimal amplitude channel and/or the channel with phase reversal in the single differential signal may be utilized to identify the surface NMJ locations. The NMJs can be localized over the skin surface through visual inspections or automatic algorithms such as bi-dimensional cross correlation, template matching or optical flow. Those surface innervation zone (IZ) mapping techniques can also be used to localize IZs over the skin surface to improve the BoNT injection outcome, but the application of those surface localization methods can be limited by the blurring effects caused by low-conductive fat and skin tissues, and the interfering effect (cross talk) caused by neighboring muscles. Clinically, the motor point (MP) is used as the injection site of BoNT since it is homologous to the IZ. However, a significant difference between the MP and IZ locations has been observed. There is an unmet need in both technical (the need for a precision and clinically friendly NMJ mapping and overactive muscle severity assessment technique) and clinical terms (the need for NMJ distribution patterns in facial muscles for precision BoNT injection with personalized injection sites and optimized injection dosage).
Aspects of the present disclosure provide a novel transcutaneous NMJ mapping technique to accurately localize NMJ locations from multi-channel surface EMG signals recorded during spontaneous activity or under nerve stimulation.
Aspects of the present disclosure provide a novel muscle overactivity severity assessment technique to quantitatively assess the severity of overactive muscles. By employing guided precision BoNT injections to facial muscles for both cosmetic and non-cosmetic indications, and by personalizing BoNT injection sites using NMJ mapping results and personalizing BoNT injection dosage using muscle overactivity severity assessment results, improved BoNT injection treatment outcomes with reduced treatment cost and minimized side effects are achieved.
The devices, systems and methods described herein fulfill the current clinical and research needs for precision injection of BoNT into the proximity of NMJs of overactive facial muscles for the best treatment outcome with minimized dosage and side effects. The devices, systems and methods described herein employ a flexible surface EMG array in a variety of configurations with different number of electrode number and shapes to meet the needs of recording muscle activity for different facial muscle groups, and an electrical simulator which will be used to deliver electrical stimulations to at least one facial nerve.
The flexible surface array detects complete and detailed neuromuscular information of any specific facial muscle groups of interest with the appropriate choice of the configuration. The flexible surface arrays may be customized for each specific facial muscle of interest, and may be customized to meet individual facial contours. Surface EMG signals can be collected at rest and/or during voluntary contraction for muscle overactivity severity assessment, and during facial nerve stimulation for NMJ mapping. Surface EMG signals may be amplified and digitized by an amplifier and analog to digital (A/D) converter for online and offline single processing via a processing computer. Multi-channel surface EMG may be used for multiple neuromuscular function evaluation techniques with monopolar or differential setups such as myoelectric source imaging, NMJ identification, surface EMG decomposition and motor unit number estimation. For example, minimal or no response to facial nerve stimulation reveal innervation deficit; large variability of firing rate of motor units during voluntary may suggest compromised central regulation of muscle functions; loss of motor unit number may indicate neural degeneration or axonal injury.
The devices, systems and methods described herein can be employed to guide precision BoNT injections to facial muscles for both cosmetic and non-cosmetic indications, by personalizing BoNT injection sites using NMJ mapping results and personalizing BoNT injection dosage using muscle overactivity severity assessment results, to maximize and stabilize the BoNT injection treatment outcome with reduced treatment cost and minimized side effects.
The devices, systems and methods described herein can be employed to personalize BoNT injection for both cosmetic purpose (reducing the appearance of facial wrinkles) and non-cosmetic purpose (treating Blepharospasm, Strabismus, spastic facial dystonias and other facial muscle spasms).
The devices, systems and methods described herein can be employed to quantitatively assess nerve innervation for pre-surgery planning, pre/post-surgery evaluation, surgery monitoring, and other neuromuscular function and innervation assessment associated with disease diagnosis, disease progress and treatment outcome evaluation. The devices, systems and methods described herein can also be employed for developing treatment regimens of BoNT injections and monitoring the progress of such treatment regimens in terms of desired clinical outcomes.
Referring to
According to an aspect of the present disclosure, the stimulation electrode 102 may execute a pre-programmed stimulation program including a series of intermittent electrical pulses controlled by the computer 107 described herein and delivered to at least one nerve innervated with at least one facial muscle group.
An electromyography (EMG) sensor array 103 includes a plurality of EMG sensors 104 configured to be arranged about the person's face. Each EMG sensor 104 detects muscle activity of at least one muscle of the facial muscle group. For example, each EMG sensor 104 is a subcutaneous EMG sensor for measuring muscle activity through a person's skin when the EMG sensor array is arranged about a person's face.
The EMG sensors 104 of the EMG sensor array 103 are arranged on a flexible substrate 108 configured to conform to contours of the person's face. The flexible substrate 108 may be formed of or may include silicone. The flexible substrate 108 may include an adhesive side that faces a person's face and is used to secure the flexible substrate to the person's face.
The EMG sensors 104 of the EMG sensor array 103 can detect an initial action potential elicited in a particular region of a facial muscle and can detect a propagation of actional potentials across the facial muscle in a particular direction. Data of the direction of action potential propagation can be utilized to identify a particular muscle by cross-referencing the direction of action potential propagation with a known arrangement of facial muscles. As an example, the computer 107 may store a reference database of known facial muscles including data of a size and directional orientation of such facial muscles employable by the computer for cross-referencing to identify a facial muscle. A machine learning algorithm may be employed to identify a particular facial muscle based on a directional propagation profile of detected actional potentials.
An EMG amplifier 105 is in electrical communication with the stimulation electrode 101, the stimulation electrode controller 102 and the EMG sensor array 103. The EMG amplifier 105 includes a plurality of input channels 106. Each input channel 106 receives data of facial muscle activity in the facial muscle group of the body of the person from an EMG sensor 104 of the EMG sensor array 103.
A computer 107 (see, e.g.,
The data of facial muscle activity includes data of at least one overactive facial muscle. The data of facial muscle activity includes a quantitative assessment of severity of overactivity in the at least one overactive facial muscle. Thus, a corresponding NMJ site of the overactive facial muscle that is identified may be recommended as a desired NMJ injection site for BoNT. The recommendation of at least one NMJ site for BoNT injection may include a recommendation of a particular BoNT dose. Additionally, the recommendation of at least one NMJ site for BoNT injection may include a recommendation of a dosing schedule for BoNT.
In an aspect of the present disclosure, the EMG sensor array 103 is configured to detect passive muscle activity and identify an occurrence of at least one spontaneous facial muscle spasm of a facial muscle group of the body of the person. The EMG sensor array 103 may also detect voluntary facial muscle movements.
Referring to
In an aspect of the present disclosure, the method 400 described with reference to
Referring to
In some aspects of the disclosure, the memory 502 can be random access memory, read-only memory, magnetic disk memory, solid state memory, optical disc memory, and/or another type of memory. The memory 502 can communicate with the processor 501 through communication buses 510 of a circuit board and/or through communication cables such as serial ATA cables or other types of cables. The memory 502 includes computer-readable instructions that are executable by the processor 501 to operate a control unit embodying the computer 107. The computer may 107 include a network interface 504 (e.g., a wireless network interface) to communicate with other computers or a server. A storage device 505 may be used for storing data. The computer 107 may include one or more FPGAs 506. The FPGA 506 may be used for executing various machine learning algorithms.
In an aspect of the present disclosure, the computer 107 is wirelessly or cable connected with the EMG amplifier 105. Alternatively, the computer 107 may be connected with the EMG amplifier 105 via a wired connection (e.g., a USB connection). As an example, the computer 107 may be included in a smartphone or tablet computer. The computer may also be a laptop or desktop computer in communication with the EMG amplifier 105.
It will be understood that various modifications may be made to the aspects and features disclosed herein. Therefore, the above description should not be construed as limiting, but merely as exemplifications of various aspects and features. Those skilled in the art will envision other modifications within the scope and spirit of the claims appended thereto.
This U.S. Non-Provisional Patent application claims priority to U.S. Provisional Patent Application No. 63/209,626, filed on Jun. 11, 2021, the entire contents of which are incorporated by reference herein.
| Number | Date | Country | |
|---|---|---|---|
| 63209626 | Jun 2021 | US |
