Minimal detectable difference of the finger and wrist range of motion: comparison of goniometry and 3D motion analysis

The measurement of finger and wrist postures is one of the important parameters for the clinicians when assessing the outcomes of therapeutic interventions and compare them. Joint angular measurements are also essential for hand therapists to record the progress of rehabilitation. It is therefore important for clinicians and researchers to have complete and relevant information on the accuracy, repeatability, and reliability of these measurements. While the manual goniometer is commonly used in clinical practice as a tool to measure joint angles, 3D motion capture systems are increasingly applied in research to measure hand motion [1‐5]. Moreover, 3D motion capture systems allow the dynamic evaluation of all hand joints simultaneously [6‐8]. They determine the position of skin markers highly accurate. The main advantages of the manual goniometry are that it is cheap, fast, and does not require data post-processing or joint angle calculations, and the main drawback is that it relies on rater’s performance for the quality of measurements. For evaluative instruments that are used to measure changes in the same subject over time, the ability to detect minimal clinically important differences is essential. Hence, it is fundamental to know the size of the measurement error is required not only for the selection of the appropriate measurement tool, but also for the interpretation of the data and the comparison between different studies.

Trained therapists generally have adequate intrarater reliability for the measurement of wrist and finger postures; however, some joints are easier to assess [9‐12]. When standard goniometry is used, variability between 2 and 7° occurs in joint angle measurements of the hand [13‐15]. The validation of goniometer measurement was done in splinted positions, which means that the force applied on the joint by the examiner was neutralized. This is not the case in real life where joints are examined looking for the actual angles and not a predefined one [16, 17]. Moreover, there are few studies comparing manual goniometer measurement and 3D motion capture, but none of them taking into account all the joints of the hand [16].

Sample size calculation (power) is a standard requirement for high-quality studies. Minimal detectable difference (MDD) and standard error of measurement (SEM) are among the most important parameters for its calculation. If we can reduce them, this will result in a smaller sample size.

Therefore, the aim of this study was to assess the repeatability of ROM of the hand joints with manual goniometer and 3D motion capture system and to calculate the minimal detectable difference and the standard error of measurement for both methods.

Two-tailed t tests (p ≤ 0.05) were performed to compare motion analysis and goniometry regarding the mean test-retest difference (meanD_V vs. meanD_G) as well as the average ROM (Mean_romV vs. Mean_romG). For a healthy population, we assumed ROM to be constant over time. Therefore, DIFF_G and DIFF_V are considered as an estimation of measurement error, and a limit of 5° was set based upon the accuracy of the manual goniometer shown to be around 5° in literature [28]. The null hypotheses were that:

(H₀₁) Within the same method, meanD equals zero, (H₀₂) DIFF lies within 5°, and (H₀₃) the ROM is equivalent when measured with the goniometer or the motion capture system.

H₀₁ was rejected, if the absolute value of the ratio of meanD and standard deviation of difference (SDD) exceeds the 5% level of agreement (|T| > 1.96; p ≤ 0.05). H₀₂ was rejected, if the estimated precision represented by the SEM was > 5°.

For the 3D motion capture system, no valid joint angle could be calculated for four subjects at the radioulnar joint and for one subject at the MCP5 joint due to issues with visibility of markers or a lost marker at the elbow. Furthermore, one subject had a misplaced marker on the thumb, affecting MCP1 calculations, and one subject had a shifted marker affecting MCP4 and MCP5 angle calculations. Therefore, these values had to be excluded from further data analysis after visual inspection of the recorded data. The available data are reported in the second column of Table 2.

There was a wide range of maximum ROM among the healthy subjects (SD_romV 9°, SD_romG 10°) (Tables 3 and 4). The two-tailed t test revealed significant (p < 0.05) differences of the Mean_rom derived from the different methods only for the pronation-supination movement of the radioulnar joint. For this joint, Mean_romG and Mean_romV differ by almost 57°, with the lower values measured with the 3D motion capture system.

The results of the test-retest parameters are presented in Table 2. No statistically significant difference (H₀₁) of the ROM (p level ≤ 0.05) was found between the first and second measurement for both methods in all joints.

For the 3D motion capture method, MDD_V lay between 5 and 12° except for the MCP1, IP, and MCP5. For the goniometric measurements, MDD_G was between 12 and 30°.

The observed precision of the measurement represented by the SEM is displayed in Fig. 3 and Table 2. SEM_V lied below the limit of 5° for all joints except for the MCP5 (SEM_V 5.7°), IP (SEM_V 5.0°), and MCP1 (SEM_V 5.0°). For the goniometric measurements, SEM_G exceeds the limit of 5° (SEM_G 5.0–11.0°) in all joints, except for PIP2-4 and DIP5 (SEM_G 4.2–4.9°).

ICC ranged from 0.35 to 0.87 (ICC_G) and 0.66 to 0.97 (ICC_V) for the goniometric and 3D motion capture measurements, respectively (Table 2). Six out of 17 joints (radioulnar, MCP3, PIP2-5) did not achieve the reliability criterion with the manual goniometer. In comparison, the ICC_V value for the 3D motion capture system was higher for all degrees of freedom, and the ROM measurements with the motion capture system met the reliability criterion for all joints except for the PIP3.

Overall, 43% and 67% of the goniometric measurements had a test-retest difference below 5° (PD_G < 5°) and 10° (PD_G < 10°), respectively (Table 2). The corresponding percentages for the 3D motion capture system were 67% (PD_V < 5°) and 92% (PD_V < 10°), respectively. The DIP5 was the only joint for which slightly more volunteers had an angular difference of less than 5° for the goniometric measurements compared to the 3D motion capture system. For all other joints, the 3D motion capture system had a higher percentage of individuals with small (< 5°) inter-session differences.

In this study, we assessed the repeatability of ROM measurements of the hand joints with 3D motion capture system, compared them with manual goniometry, and calculated the MDD for both methods. We measured all joints of the fingers and the wrist.

We observed method differences from − 57 to + 11°, where negative values indicate higher ROM when examined with the goniometer (Mean_romG > Mean_romV).

Since the true value of the joint angle is unknown, the comparison between the two methods serves as the first step in the validation of the new motion analysis protocol. Skin movement relative to the bone is the biggest source of error in motion analysis with skin markers [29, 30]. Longitudinal rotations are more affected from skin movement artifacts, therefore leading to an under-/overestimation of the joint angle in motion analysis [30, 31]. In agreement, we found the highest method disagreement (57°) and the only significant difference for the pronation-supination movement. Difficulties to measure the radioulnar joint with a goniometer (ICC 0.35_G, SEM_G 6.8°) might have further contributed to the large difference between the methods.

Armstrong et al. suggest that the lack of precision in goniometric measurement could be technique related, as the current method of measuring true forearm rotation involves placing a flat goniometer along the curved surface of the flexion/extension crease of the wrist [32]. The observed significant difference between the methods for measuring forearm rotation indicates that adjustments to the methodology are necessary. Schmidt et al. propose a procedure to reduce the influence of skin movement artifacts by looking at the hand rotation during pronation-supination instead of the rotation of the forearm itself [33]. Implementation of such simple corrections might further improve the presented measurement method.

A comparison with a gold standard, such as an imaging technique, would be a possibility to estimate the accuracy of the measurements. However, the validity of the data is beyond the scope of this article. Still, our results reveal that the measurement system used to obtain the ROM has to be considered for clinical data interpretation. Therefore, a specific norm database for every method is highly recommended.

n a clinical setting, methods are often used to evaluate the effects of interventions or monitor changes over time within the same subject. Therefore, a focus on agreement parameters is recommended by de Vet et al. [26]. The SEM and MDD express measurement error in the same unit as the original value, which facilitates clinical interpretation. In contrast to ICC, SEM and MDD are not influenced by variability among the sample [34]. Hence, their values can be transferred to various groups of patients.

Averaged over all analyzed joints, the MDD_V was 10°, compared to 18° MDD_G. Therefore, measurements by means of a motion capture system allow us to recognize smaller changes in joint mobility than with goniometer. This means that we have to be very careful in the clinical setting to interpret a change in the ROM as a true change, or just as a measurement error. For the wrist joint flexion/extension and radial/ulnar deviation, MDD_G was 18°. Macedo and Magee examined the passive ROM of the wrist with a universal goniometer in 12 healthy adults. They found a MDD_G for the wrist flexion of 11° and for the wrist extension of 8°, which is lower than our MDD_G, but higher than our MDD_V [35].

The MDD_G for the finger joint lied between 12° and 24°. Ellis and Bruton examined the finger joints with a goniometer, but in a splinted position, so they had MDD (reported as 95% confidence interval of difference) of between 4° and 5° [1].

Overall, the calculated precision of the ROM measurements was SEM_V 3.6° and SEM_G 6.4° for the 3D motion capture system and goniometer, respectively. The mean values of all repeatability parameters indicate higher test-retest agreement for the 3D motion capture method. For the wrist joint, the SEM_G with the goniometer was 6.4° (F/E) and 6.5° (R/U). LaStayo and Wheeler assessed the passive ROM of the wrist with a universal goniometer in 120 patients with wrist conditions. They reported SEM between 5.6° and 8.1°, like Macedo and Magee with SEM between 2.9° and 7.4°, compare to Horger who calculated a SEM between 2.6° and 4.5° [12, 35, 36]. Our results consider the ROM of the movement, so both measurement points (e.g., maximum flexion and extension position) are affected from independent error associated with the placement of the goniometer, whereas the other studies showed the results of each direction separately.

For the finger joints, SEM_G was between 4.2° and 8.8°. Stam et al. evaluated 20 healthy subjects with a goniometer while holding cylinders with different diameter and had a SEM between 4° and 6°, similar to our results [37].

In comparison with previous repeatability goniometry studies, the intrarater reliability for the active ROM of the middle finger found in our study lies within the range of the intra- and interrater reliability (ICC 0.43 to 0.99) determined by Lewis et al. [2]. Solgaard et al. assessed intraobserver SDD for the goniometry of the wrist of 5.2–8° [38]. Compared to these findings, our results for wrist goniometry are slightly higher. In contrast, the 3D motion capture of the wrist ROM had better repeatability than the goniometry results in both studies.

Compared to previous measurements by 3D motion capture, we found excellent test-retest reliability on the wrist (ICC 0.90–0.97). The corresponding values in Levanon et al. were only good (ICC 0.77–0.83) [39]. In contrast, the root-mean-square error in our study was 5.3°, whereas Sancho-Bru et al. found smaller errors in repeatability (3.4°) [8]. In that study, a different marker set was used and the repeatability was assessed for grasping different objects while we analyzed the maximum ROM. It is possible that variability of the ROM movement is bigger than in specific grasping tasks, but to quantify the source of error, a validation would be needed.

In conclusion, the MDD of the 3D motion capture system is smaller than of the goniometer measurement. This is particularly important in an experimental setup where a higher degree of precision is requested. In the clinical research, better MDD permits relevant reduction of the sample size.