Coverage Guideline

This document addresses a type of tremor analysis device that includes an accelerometer and a gyroscope. These devices are proposed for use in diagnosing tremor, in the management of individuals with implanted deep brain stimulation devices to guide adjustments to the neurostimulator settings, and other indications.

For information on additional testing, see:

• CG-ANC-08 Mobile Device-Based Health Management Applications
• CG-MED-24 Electromyography and Nerve Conduction Studies
• MED.00092 Automated Nerve Conduction Testing

Note: For a high-level overview of this document, please see “Summary for Members and Families” below.

Investigational and Not Medically Necessary:

The use of accelerometer/motion analysis testing devices is considered investigational and not medically necessary for all applications, including, but not limited to, the evaluation of tremors.

This document describes clinical studies and expert recommendations, and explains whether use of tremor analysis devices that include accelerometers and gyroscopes are appropriate. The following summary does not replace the medical necessity criteria or other information in this document. The summary may not contain all of the relevant criteria or information. This summary is not medical advice. Please check with your healthcare provider for any advice about your health.

Key Information

Motion analysis devices that use accelerometers and gyroscopes are being studied to help diagnose tremors or adjust treatments for conditions like Parkinson’s disease. These devices can be worn on the body or used through smartphones or smartwatches. They measure body movement and may help track symptoms like shaking, trouble walking, or sleep problems. Several devices have been approved by the U.S. Food and Drug Administration (FDA) for specific purposes. However, research shows mixed results on whether these devices actually help doctors make better decisions or improve people’s health. Because of this, these tests are not recommended for use in diagnosis or treatment decisions at this time.

What the Studies Show

Some small studies have explored using smartphones, smartwatches, or wearable sensors to measure tremors or other symptoms of movement disorders like Parkinson’s disease. These studies found that the devices could measure movement and sometimes match up with standard clinical tests. However, these studies had problems such as small numbers of participants, missing data, and different methods that make it hard to compare results. One larger study used smartphone tests and found they could tell the difference between people with Parkinson’s and those without, but missing information from the devices and about the participants’ other health conditions make the results unreliable.

A recent review looked at five wearable devices. One device, the PKG, showed good ability to track tremor and stiffness and sometimes led doctors to change treatments. But improvements in health scores were not clearly proven. Other devices like the STAT-ON^™ and Kinesia 360^™ showed they could detect movement problems, but there wasn’t enough evidence to show they helped people feel better or function better in daily life. Many of the studies focused only on people taking common medications, so it’s unclear if these tools help people using other types of treatment. More research is needed to know which tools work best, how long benefits last, and who would benefit most.

Is this clinically appropriate?

The use of Motion analysis devices that use accelerometers and gyroscopes is not appropriate because they have not been proven to improve health. While some studies suggest accelerometer and motion analysis devices can track tremors or movement symptoms, the results are inconsistent and mostly come from small or poorly designed studies. Better studies are needed to know if these tests lead to better decisions or outcomes. Unnecessary or unproven tests can lead to confusion or treatment that does not help.

(Return to Description/Scope)

Summary:

This document evaluates devices that record tremor using accelerometers and gyroscopes, including wearable sensors, smartphone- or smartwatch-based systems, and other motion-analysis platforms. It reviews their proposed use for diagnosis of tremor, monitoring movement disorders such as Parkinson’s disease, and guiding adjustments to deep brain stimulation settings, as well as other potential clinical applications.

Clinical evidence consists largely of small, heterogeneous, or methodologically limited studies assessing tremor quantification or remote symptom monitoring. While many studies show that accelerometer- or gyroscope-based devices can measure tremor characteristics or differentiate some patient groups from controls, the evidence demonstrates:

• Inconsistent results across studies, with frequent limitations such as small sample sizes, missing data, lack of controls, and variable test methods.
• Insufficient demonstration of clinical utility, meaning it is unclear whether use of these devices leads to improved clinical decision-making or better health outcomes.
• Remote monitoring systems (e.g., PKG, Kinesia 360, STAT-ON) show some ability to detect motor symptoms, but evidence that their use improves patient outcomes is limited or inconclusive.
• Current research does not establish which populations would benefit most or whether these tools outperform established clinical assessments.

Overall, the existing evidence does not demonstrate that accelerometer- or gyroscope-based tremor recording improves health outcomes or clinical management.

The document references the American Academy of Neurology (AAN) Evidence-based guideline update: Treatment Of Essential Tremor (Zesiewicz, 2011), which does not provide recommendations supporting the clinical use of accelerometric tremor analysis for diagnosis or management.

Discussion:

A few small studies have investigated the clinical utility of accelerometric measurements for evaluation of tremor and functional ability in dyskinetic conditions, such as Parkinson’s disease and stroke. The results, to date, have demonstrated inconsistent conclusions, and the authors acknowledge the need for further study to elucidate the clinical utility of these test devices and which population groups would potentially benefit from their use (Boroojerdi, 2019; Cheung, 2011; Gebruers, 2010; Perez Lloret, 2010).

Several studies have investigated the use of smartphone-based remote monitoring technology with the use of accelerometer and gyroscope data to assess tremors.

In 2017, Zheng published a study with the aim to use a smartwatch with a triaxial accelerometer, a smartphone, and a remote server to quantify tremor objectively during daily activities. The study enrolled 9 participants, but 1 participant’s data was lost. The remaining 8 participants each had an average effective data collection time of 26 hours. Despite scattered data points, the authors calculated significant correlation between the participants’ Fahn-Tolosa-Marin Tremor Rating Scale (FTMTRS) self-assessment scores and the device (r=0.84, p<0.001); the device’s qualitative measurements and the participants’ self-assessment scores (r=0.97, p=0.032); the device’s qualitative measurements and the neurologists’ standardized assessment scores (r=0.80, p=0.005); and the neurologists FTMTRS and participants’ FTMTRS mean auto-assessment scores (r=0.84, p=0.009). While this study had significant results, there were several limitations including small sample size, lack of control group or blinding, and incomplete data collection.

Lipsmeier reported on the data of two independent smartphone-based remote monitoring studies (2018). One study was a 6-month phase 1b clinical drug trial with 44 individuals with Parkinson’s disease. The other was a 6-week observational study of 35 age- and sex-matched healthy controls. Individuals received a smartphone with a mobile application pre-installed and a belt with a pouch in which to carry the smartphone. After training on the use of the smartphone and mobile application, individuals were instructed to complete six daily active tests (sustained phonation, rest tremor, postural tremor, finger-tapping, balance, and gait), then carry the smartphone throughout the remainder of the day for passive monitoring of daily activities, and lastly, charge the smartphone overnight. Once quality control was performed on the data collected, 15% of sustained phonation data (phonation not sustained for an adequate period) and 3% of all other active test data (for example, no walking during balance test) were removed. The data showed the individuals with Parkinson’s disease completed 5135 active tests, which resulted in an average daily test completion of 3.5 out of 7 days per week and 61% of all possible test sessions. Active test features demonstrated moderate-to-excellent test-retest reliability (average intraclass correlation coefficient=0.84). A significant difference was found by all active tests and passive monitoring features in differentiating individuals with Parkinson’s disease from healthy controls (p<0.005). Except for sustained phonation, all active tests were significantly related to the corresponding International Parkinson and Movement Disorder Society-Sponsored UPDRS clinical severity ratings (rest tremor, postural tremor, finger tapping, gait task: p<0.05; balance task: p<0.01). The authors stated, “On passive monitoring, time spent walking had a significant (p=0.005) relationship with average postural instability and gait disturbance scores.” This study had several significant findings; however, there were also several limitations. First, intraclass correlation coefficients were calculated with mean data rather than individual data, which may have led to falsely higher values. And second, the data used was extracted from two separate studies with different study designs.

In 2018, Mehrang released the results of a retrospective data analysis of age- and gender-matched individuals with Parkinson’s disease (n=616) and controls (n=621). These individuals were part of the first phase of the larger mPower study conducted in 2015. All individuals were recruited remotely through their smartphones and inclusion criteria was very broad including being at least 18 years of age or older, in the United States, and proficient at reading and writing on the smartphone in English. The mPower study required individuals to participate in four different tests aimed to assess physical and mental abilities. One of the tests was a gait assessment test in which individuals had to walk 20 steps in a straight line while carrying their smartphone in their pocket or bag. Those individuals who completed at least one walking test and answered whether or not they had Parkinson’s disease were age- and gender-matched using background data provided through the mPower study. The investigators found the accuracy, sensitivity, and specificity were all equal 0.7, which showed that individuals with Parkinson’s disease could be differentiated from those without Parkinson’s disease through the 20-step walking test. A major limitation to this study due to the retrospective design was the lack of data collected. Additionally, there was no information on the medications the individuals were taking, other diseases that could have impacted gait, or disease severity of Parkinson’s disease.

Cox (2024) conducted a systematic review on five wearable remote devices used to continuously monitor motor symptoms, tremors, and sleep disturbances in individuals with Parkinson's disease. These devices, which require minimal user input, include the Personal KinetiGraph^™ (PKG) Movement Recording System, Kinesia 360 and KinesiaU^™ motor assessment systems, PDMonitor^®, and STAT-ON. The review analyzed 77 studies, focusing on the diagnostic accuracy, impact on clinical decision-making, clinical outcomes, and the opinions of both participants and clinicians regarding these technologies.

In the review, 57 studies were analyzed to assess the effectiveness of the PKG in monitoring symptoms of Parkinson's disease. The PKG demonstrated good diagnostic accuracy for bradykinesia, dyskinesia, and tremor, but less so for sleep disturbances. It was found to influence changes in clinical management plans in 31.8-79% of cases, often resulting in increased treatment doses. A non-randomized trial with 162 participants indicated that PKG use might improve Unified Parkinson’s Disease Rating Scale (UPDRS) scores, although the reductions in bradykinesia, dyskinesia, and tremor were not statistically significant. PKG was notably beneficial for individuals whose symptoms were not adequately controlled. While participant feedback on PKG was positive, particularly as a medication reminder, clinician opinions were mixed, with only 33-47% expressing support. No p-values were reported in the study.

The review by Cox (2024) included 15 studies of the STAT-ON device used in monitoring Parkinson's disease symptoms. The findings revealed that STAT-ON demonstrated high diagnostic accuracy for detecting treatment "on-off" times and bradykinesia, along with high sensitivity but lower specificity for identifying freezing of gait. However, no studies provided evidence on the intermediate or clinical impact of the STAT-ON device.

Three studies addressed the Kinesia 360 device, which demonstrated moderate-to-good diagnostic accuracy for detecting bradykinesia, dyskinesia, and tremor. However, two small randomized controlled trials (RCTs) involving 64 participants provided inconclusive evidence regarding the device's effectiveness in improving UPDRS and Parkinson’s Disease Quality of Life (PDQOL) scores compared to standard management. Additionally, one small cohort study with 16 participants was deemed too small to draw meaningful conclusions.

The authors concluded that the PKG demonstrates accurate measurement of bradykinesia and dyskinesia, potentially leading to treatment modifications and improved clinical outcomes when evaluated with the UPDRS. While there is some promising evidence for the STAT-ON and Kinesia 360 devices, the data is insufficient to confirm clinical benefits. There was also insufficient evidence to assess the clinical value of the KinesiaU and PDMonitor devices. Most existing studies focus on individuals undergoing pharmacological therapy, primarily levodopa, and it remains unclear if PKG or other remote monitoring technologies offer benefits for those receiving advanced therapies. Additionally, the extent and longevity of treatment effects are uncertain.

Additional studies have investigated the clinical validity of accelerometric measurements to evaluate physical activity and gait variables in the elderly and in those with hip osteoarthritis using differing devices and methods of data analysis and reporting. The authors acknowledged the need for further research to standardize testing methods and data reporting that compare devices in clinical practice (Bento, 2012; Item-Glatthorn, 2012). There is a lack of published evidence evaluating the clinical utility of accelerometers as compared to conventional testing modalities.

There are multiple types of motion analysis accelerometers on the market for various applications including evaluation of physical exercise, weight reduction progress, and motion disorders, associated with certain conditions, such as Parkinson’s disease. These devices attach to the individual's arm and other body parts to measure body motion. Once attached, the person is then asked to do several tasks, such as resting with their hands in their lap for several seconds, holding their arms straight out in front of them for several seconds, or extending their arm and touching their nose. Some models of these devices also include an electromyography (EMG) testing component.

Several devices are available in the US, including the Kinesia (Great Lakes NeuroTechnologies, Cleveland, OH) which obtained clearance from the U.S. Food and Drug Administration (FDA) on April 6, 2007 through the 510(k) approval process. The Kinesia device is indicated to:

• monitor physical motion and muscle activity to quantify the kinematics of movement disorder symptoms, such as tremor; and
• assess activity in any instance where quantifiable analysis of motion and muscle activity is desired (FDA, 2007).

The Personal KinetiGraph (PKG) Movement Recording System (GKC Manufacturing Pty Ltd., Rockville, MD) received FDA clearance on July 24, 2014, with the indication to quantify kinematics of movement disorder symptoms in conditions such as Parkinson's disease, including tremor, bradykinesia and dyskinesia.

The NeuroRPM^™ (New Touch Digital Inc., Washington, DC) received FDA clearance on February 15, 2023, to quantify movement disorder symptoms during wake periods in adult patients 46 to 85 years of age with Parkinson's disease.

The Kneu Platform (Kneuhealth Digital, Ltd. London, United Kingdom) received FDA clearance on April 25, 2025, with the indication to quantify the kinematics of movement disorder symptoms, including tremor in adults (45 years and older) with mild to moderate Parkinson's disease.

Several other devices have been investigated and developed for similar indications, but have not received approval or clearance by the FDA for marketing in the U.S. This includes the PDMonitor (PD Neurotechnology, London, UK) and the STAT-ON (SENSE4CARE SL, Barcelona, Spain).

As technology has evolved, accelerometers and gyroscopes have been incorporated into smartphones and smartwatches, which allows analysis of motion through mobile applications. Performance of various tests, such as sitting to assess tremors and walking to assess balance and gait, while wearing such devices has been proposed as a method of testing for and managing tremor-related conditions.

Accelerometer: A device that measures change in position by detecting variations in motion or acceleration.

Clinical utility: An assessment of the risks and benefits resulting from using a particular test and the likelihood that the test will lead to an improved overall outcome.

Clinical validity: The accuracy with which a test identifies or predicts an individual’s clinical status.

Gyroscope: A device composed of a spinning disc or light mechanism in a static frame. This type of device uses the principle of conservation of angular momentum to measure or detect changes in orientation and angular velocity.

Kinematics: A branch of physics that deals with aspects of motion apart from considerations of mass and force.

The following codes for treatments and procedures applicable to this document are included below for informational purposes. Inclusion or exclusion of a procedure, diagnosis or device code(s) does not constitute or imply member coverage or provider reimbursement policy. Please refer to the member's contract benefits in effect at the time of service to determine coverage or non-coverage of these services as it applies to an individual member.

When services are Investigational and Not Medically Necessary:

Peer Reviewed Publications:

1. Bento T, Cortinhas A, Leitão JC, Mota MP. Use of accelerometry to measure physical activity in adults and the elderly. Rev Saude Publica. 2012; 46(3):561-570.
2. Boroojerdi B, Ghaffari R, Mahadevan N, et al. Clinical feasibility of a wearable, conformable sensor patch to monitor motor symptoms in Parkinson's disease. Parkinsonism Relat Disord. 2019; 61:70-76.
3. Cheung VH, Gray L, Karunanithi M. Review of accelerometry for determining daily activity among elderly patients. Arch Phys Med Rehabil. 2011; 92(6):998-1014.
4. Cox E, Wade R, Hodgson R, et al. Devices for remote continuous monitoring of people with Parkinson's disease: a systematic review and cost-effectiveness analysis. Health Technol Assess. 2024; 28(30):1-187.
5. Elble RJ. Gravitational artifact in accelerometric measurements of tremor. Clin Neurophysiol. 2005; 116(7):1638-1643.
6. Gebruers N, Vanroy C, Truijen S, et al. Monitoring of physical activity after stroke: a systematic review of accelerometry-based measures. Arch Phys Med Rehabil. 2010; 91(2):288-297.
7. Giuffrida JP, Riley DE, Maddux BN, Heldman DA. Clinically deployable Kinesia technology for automated tremor assessment. Mov Disord. 2009; 24(5):723-730.
8. Godfrey A, Conway R, Meagher D, OLaighin G. Direct measurement of human movement by accelerometry. Med Eng Phys. 2008; 30(10):1364-1386.
9. Hoff JI, van der Meer V, van Hilten JJ. Accuracy of objective ambulatory accelerometry in detecting motor complications in patients with Parkinson disease. Clin Neuropharmacol. 2004; 27(2):53-57.
10. Item-Glatthorn JF, Casartelli NC, Petrich-Munzinger J, et al. Validity of the IDEEA accelerometry system for quantitative gait analysis in patients with hip osteoarthritis. Arch Phys Med Rehabil. 2012; 93(11):2090-2093.
11. Kavanagh JJ, Menz HB. Accelerometry: a technique for quantifying movement patterns during walking. Gait Posture. 2008; 28(1):1-15.
12. Keijsers NL, Horstink MW, Gielen SC. Automatic assessment of levodopa-induced dyskinesias in daily life by neural networks. Mov Disord. 2003; 18(1):70-80.
13. Lipsmeier F, Taylor KI, Kilchenmann T, et al. Evaluation of smartphone-based testing to generate exploratory outcome measures in a phase 1 Parkinson's disease clinical trial. Mov Disord. 2018; 33(8):1287-1297.
14. Machowska-Majchrzak A, Pierzchała K, Pietraszek S. Analysis of selected parameters of tremor recorded by a biaxial accelerometer in patients with parkinsonian tremor, essential tremor and cerebellar tremor. Neurol Neurochir Pol. 2007; 41(3):241-250.
15. Mansur PH, Cury LK, Andrade AO, et al. A review on techniques for tremor recording and quantification. Crit Rev Biomed Eng. 2007; 35(5):343-362.
16. Mathie MJ, Coster AC, Lovell NH, et al. A pilot study of long-term monitoring of human movements in the home using accelerometry. J Telemed Telecare. 2004; 10(3):144-151.
17. Mehrang S, Jauhiainen M, Pietil J, et al. Identification of Parkinson's disease utilizing a single self-recorded 20-step walking test acquired by smartphone's inertial measurement unit. Conf Proc IEEE Eng Med Biol Soc. 2018; 2018:2913-2916.
18. Milosevic M, Van de Vel A, Cuppens K, et al. Feature selection methods for accelerometry-based seizure detection in children. Med Biol Eng Comput. 2017; 55(1):151-165.
19. Perez Lloret S, Rossi M, Cardinali DP, Merello M. Actigraphic evaluation of motor fluctuations in patients with Parkinson's disease. Int J Neurosci. 2010; 120(2):137-143.
20. Thielgen T, Foerster F, Fuchs G, et al. Tremor in Parkinson's disease: 24-hr monitoring with calibrated accelerometry. Electromyogr Clin Neurophysiol. 2004; 44(3):137-146.
21. Verceles AC, Hager ER. Use of accelerometry to monitor physical activity in critically ill subjects: a systematic review. Respir Care. 2015; 60(9):1330-1336.
22. Zheng X, Campos AV, Ordieres-Meré J, et al. Continuous monitoring of essential tremor using a portable system based on smartwatch. Front Neurol. 2017; 8:96.

Government Agency, Medical Society, and other Authoritative Publications:

1. U.S. Food and Drug Administration (FDA). Center for Devices and Radiologic Health (CDRH). Kinesia^™ (Cleveland Medical Devices, Inc., Cleveland, OH). K063872. April 6, 2007. Available at: http://www.accessdata.fda.gov/cdrh_docs/pdf6/K063872.pdf. Accessed on December 17, 2025.
2. U.S. Food and Drug Administration (FDA). Center for Devices and Radiologic Health (CDRH). Kneu Platform^™ (Kneuhealth Digital Ltd. London, United Kingdom) K250153. April 25, 2025. Available at: https://www.accessdata.fda.gov/cdrh_docs/pdf25/K250153.pdf. Accessed on December 14, 2025.
3. U.S. Food and Drug Administration (FDA). Center for Devices and Radiologic Health (CDRH). NeuroRPM^™ (New Touch Digital Inc., Washington, DC). K221772. April 6, 2007. Available at: https://www.accessdata.fda.gov/cdrh_docs/pdf22/K221772.pdf. Accessed on December 17, 2025.
4. U.S. Food and Drug Administration (FDA). Center for Devices and Radiologic Health (CDRH). Personal Kinetigraph (PKG) System^™ (GKC Manufacturing Pty Ltd., Rockville, MD). K140086. July 24, 2014. Available at: https://www.accessdata.fda.gov/cdrh_docs/pdf14/K140086.pdf. Accessed on December 17, 2025.
5. U.S. Food and Drug Administration (FDA). Center for Devices and Radiologic Health (CDRH). Tremorometer^® (FlexAble Systems, Inc. Fountain Hills, AZ). K010270. July 25, 2001. Available at: https://www.accessdata.fda.gov/cdrh_docs/pdf/K010270.pdf. Accessed on December 17, 2025.
6. Zesiewicz TA, Elble R, Louis ED, et al. Evidence-based guideline update: treatment of essential tremor. Report of the Quality Standards Subcommittee of the American Academy of Neurology. Neurology. 2011; 77(19):1752-1755.

1. National Institute of Neurological Disorders and Stroke. Tremor. Last reviewed on March 25, 2025. Available at: https://www.ninds.nih.gov/health-information/disorders/tremor. . Accessed on December 17, 2025.

Accelerometer
Dyskinesia
Gyroscope
Kinesia
Kneu PlatformMotus Portable System
Movement Analysis
Tremor Analysis
Tremorometer

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Federal and State law, as well as contract language, including definitions and specific contract provisions/exclusions, take precedence over Coverage Guidelines and must be considered first in determining eligibility for coverage. The member’s contract benefits in effect on the date that services are rendered must be used. Coverage Guidelines, which addresses medical efficacy, should be considered before utilizing medical opinion in adjudication. Medical technology is constantly evolving, and we reserve the right to review and update Coverage Guidelines periodically.

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