Artifact characterization of Nitinol needles in magnetic resonance imaging-guided musculoskeletal interventions at 3.0 tesla: a phantom study
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Interventional Radiology - Original Article
P: 719-732
September 2023

Artifact characterization of Nitinol needles in magnetic resonance imaging-guided musculoskeletal interventions at 3.0 tesla: a phantom study

Diagn Interv Radiol 2023;29(5):719-732
1. Department of Radiology, University Hospital, LMU Munich, Munich, Germany
No information available.
No information available
Received Date: 19.04.2023
Accepted Date: 11.06.2023
Publish Date: 05.09.2023
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ABSTRACT

PURPOSE

To characterize the artifacts of an 18-gauge coaxial nickel-titanium needle using a balanced steady-state free precession sequence in magnetic resonance imaging-guided interventions at 3.0 tesla.

CONCLUSION

To minimize needle artifacts, it is recommended to use FAs of 40°–60°, a ST of >7 mm, and, if possible, an IA of 45°–60°. The visibility of the target lesion and the needle’s artifact behavior must be weighed up against each other when choosing the ST, while higher FAs (40°–60°) and matrices (224 × 224/256 × 256) are associated with low artifacts and sufficient lesion visibility.

RESULTS

The artifact diameters decreased with an increase in FA for all IAs (P < 0.001) and with an increase in ST for IAs of 45°–90° (all P < 0.05). Tip artifacts occurred at low IAs (0°–45°) and gradually increased in size with a decrease in IA (P = 0.022). The interrater reliability was high (ICC: 0.994–0.999). The contrast-enhanced target lesion to non-enhanced muscle tissue contrast ratio presented positive correlations with increasing FAs and matrices (P < 0.001; P = 0.003) and a negative correlation with increasing STs (P = 0.007).

METHODS

The influence of flip angle (FA), bandwidth, matrix, slice thickness (ST), and read-out direction on needle artifact behavior was investigated for different intervention angles (IA). Artifact diameters were rated at predefined positions. Subgroup differences were assessed using Bonferroni-corrected non-parametric tests and correlations between continuous variables were expressed using the Bravais–Pearson coefficient. Interrater reliability was quantified using intraclass correlation coefficients (ICCs), and a contrast-enhanced target lesion to non-enhanced muscle tissue contrast ratio was quantified.

Main points

• The use of a flip angle (FA) of 40°–60° and a slice thickness (ST) of 10–17 mm minimized the needle artifacts while maintaining the best possible visualization of the coaxial intervention needle in this musculoskeletal phantom study at 3.0 tesla. To find a compromise, since the ST should not be set too thick to ensure accurate needle placement during the procedure, we ultimately recommend an ST of >7 mm in clinical practice.

• In addition, if possible, the intervention angles should be 45°–60° to specifically avoid tip artifacts.

• The visibility of the target lesion and the artifact behavior of the intervention needle must be weighed up against each other when choosing the ST, while higher FAs (40°–60°) and matrices (224 × 224/256 × 256) were associated with both low needle artifacts and sufficient target lesion visibility.

Magnetic resonance imaging (MRI) encompasses excellent characteristics for the image guidance of interstitial interventional procedures, including a lack of ionizing radiation, high soft tissue contrast, and multiplanar needle guidance with quasi-simultaneous acquisition of two or three orthogonal, oblique slices in near real-time.1,2,3,4,5,6,7,8 In practice, MRI-guided interventions are performed in clinical routines involving a wide range of body regions with a primary focus on the tissues of organs for which MRI is superior to other imaging modalities, such as the liver, prostate, breast, or spine.6,8,9,10,11,12,13,14 However, interventions of peripheral joints for, for example, the purpose of biopsy extraction, are still most likely to be ultrasound-guided, with MRI-guidance of musculoskeletal interventions beyond the spine rarely performed. Nevertheless, there exist a number of approaches that have trialed real-time dynamic MRI in the field of musculoskeletal imaging. For example, Bayer et al.15 demonstrated that dynamic visualization of the finger anatomy during a full range of motion can be obtained by using a balanced steady-state free precession (bSSFP) sequence.

To be MR-compatible and to ensure a safe procedure for the patient and the performing interventionalist, biopsy needles are made of alloys that cause minimal interference with the outer magnetic field, such as nickel-titanium (Nickel Titanium Naval Ordnance Laboratory; Nitinol), titanium, glass fiber, or steel.16 However, needle artifacts, which mostly present as low intensity signals in the region around the needle’s shaft or tip, cannot be completely excluded and can impair accurate visualization of both the needle and the needle-to-target distance. To successfully perform MRI-guided interventions with reliable target localization for musculoskeletal issues at 3.0 tesla (T) units, a thorough understanding of needle artifact behavior is crucial, regardless of the intended biopsy site. The artifact size is influenced by different parameters, which are either related to the individual composition of the needle, such as the alloy, the diameter, and the length, or, to different MRI-related parameters, such as the orientation of the intervention angle (IA) in relation to the static magnetic field (B0), the strength of the B0 field, or the pulse sequence type.5,10,17,18,19,20,21,22 Therefore, it is important to reassess the technical and methodological fundamentals of musculoskeletal MRI-guided interventions at 3.0 T. This is, on the one hand, because 3.0 T interventional MRI is more demanding in terms of safety and artifact behavior than interventions at lower fields (e.g., at 1.5 T) and on the other hand, because it can provide rewarding superior image quality when considering important aspects in acquisition parameter selections.

This paper presents a systematic investigation of the artifact behavior of an 18-gauge (G) commercially coaxial Nitinol needle as a function of the IA and sequence parameter variations using a bSSFP sequence in a muscle phantom model at 3.0 T. The study aims to characterize artifact formation during clinical MRI-guided high-field interstitial interventions, providing valuable guidance for musculoskeletal tissue biopsies.

Methods

Image acquisition

The MRI process was performed using a closed-bore 3.0 T unit (MAGNETOM Vida, Siemens Healthineers, Erlangen, Germany) with a system length (cover-to-cover) of 186 cm and a bore diameter of 70 cm. The gradient system had a maximum gradient strength of 60 mT/m and a slew rate of 200 T/m/s. The MRI protocol was based on an interventional real-time fluoroscopic bSSFP pulse sequence with true fast imaging with steady-state free precession (TrueFISP) contrast (“Needle Intervention Add-in” package, Siemens Healthineers, Erlangen, Germany). This pulse sequence allows for visual real-time updates and interactive graphical modification of the slice geometry during imaging. A four-channel flex coil (Siemens Healthineers, Erlangen, Germany) with a weight of 550 g (516 × 224 mm) was used as the receive coil.

Ethics committee approval was waived for this study due to the exclusively experimental study design without any animals or patients being involved.

Bovine muscle phantom model

A bovine muscle phantom model with a weight of 5.925 kg, a length of 33 cm, a width of 24 cm, a height of 13 cm, and a maximum transverse diameter of 53 cm was used. As expected, the bovine muscle phantom model had an MRI signal intensity comparable to that of human skeletal muscle. The complete scan series could be performed using the same model, ensuring comparability of the results. Before placing the needles, 0.5 mL of 1.0 mmol/mL gadolinium (Gadovist®, Bayer AG, Leverkusen, Germany) diluted at 1:1000 in 0.9% sodium-chloride (B. Braun, Melsungen, Germany) was applied in a 1.0-mL syringe (B. Braun, Melsungen, Germany) centrally into the muscle phantom by using a 20-G Nitinol needle (ITP, Innovative Tomography Products GmbH, Bochum, Germany) to simulate a contrast-enhanced target lesion at the center of the muscle tissue specimen. Thereafter, a total of seven MR-compatible coaxial Nitinol needles (as described below) were positioned at 0°, 15°, 30°, 45°, 60°, 70°, and 90° relative to the B0 field using the “entry and target points function” within the real-time fluoroscopic MRI software to guarantee an exact and parallel position of the needles in the B0 field (2° accepted deviation). The experimental setup is shown in Figure 1.

Figure 1

Magnetic resonance-compatible intervention needle

A commercially available MR-compatible coaxial Nitinol needle (ITP, Innovative Tomography Products GmbH, Bochum, Germany) with a size of 18G (outer diameter: 1.25 mm, length: 150 mm, standardized facet cut) was investigated.

Scan series

The phantom was positioned in the isocenter of the XZ plane using the light visor of the MR tomograph. The influence of the following five parameters was investigated as a function of the IA on artifact formation: flip angle (FA), receiver bandwidth (BW), matrix, slice thickness (ST), and read-out direction. The IA (the needle angle relative to the B0 field) varied from 0°–90° (0°, 15°, 30°, 45°, 60°, 75°, and 90°). As one parameter was modified, the others remained constant with the following predefined settings. The matrix was fixed to 128 × 128 voxels, which was a compromise between acquisition time and spatial resolution. Echo time (TE) and repetition time (TR), which yield an influence on acquisition time, were set to a minimum (TE: 1.71 ms, TR: 3.42 ms) as fixed parameters, resulting in an acquisition time of 461 ms per plane. The field of view was uniformly set to 300 × 300 mm2. The predefined setting was 50° for the FA, 930 Hz/pixel for the BW, and 10 mm for the ST. The fixed read-out direction was right to left. An overview of the default settings is provided in Supplementary Table 1. Starting with these default settings, each of the parameters mentioned above was modified, as described in detail in Supplementary Table 2, resulting in acquisition times of 346–1.148 ms per plane. For each parameter modification, the TrueFISP sequence was performed in the same manner. Prior to the start of the fluoroscopic TrueFISP sequence, the correct angles (accepted deviation of 2°) between the needles and the B0 field and the position in the isocenter of the MR scanner were verified using test sequences.

Table 1
Table 2

Artifact diameter measurement

For image acquisition and evaluation of the artifact diameter, Visage Imaging software (Visage Imaging GmbH, Berlin, Germany) was used. The artifact diameters were measured in a standardized plane at two predefined positions (50% and 25% of the inserted needle length measured from the tip of the needle) for every modification of the scan series to ensure comparability. If there was a ball-like tip artifact (IA: 0°, 15°, 30°, and 45°), the maximum diameter of this artifact was determined in the same standardized plane regardless of its two-dimensional direction of largest extension (Figure 2). The needle artifacts were measured by two independent and blinded readers (V.F.S. and S.S.G.) with three and four years of diagnostic MRI experience, respectively, for each modification of the evaluated parameters.

Figure 2

Contrast-enhanced target lesion to non-enhanced muscle tissue ratio

For the evaluation of the contrast ratio of the contrast-enhanced target lesion to the non-enhanced muscle tissue, regions of interests (ROIs) with a diameter of at least 5 mm2 were used to quantitatively assess corresponding signal intensities (SI). The primary ROI was placed inside the contrast-enhanced target lesion and the second ROI within the adjacent non-enhanced muscle tissue at a distance of 20 mm while sparing visible muscle inhomogeneities. In addition, the latter ROI placement was defined at an identical anatomical depth to the target lesion to avoid any potential influence from surface coil sensitivity profiles. The position, size, and shape of the ROIs were kept almost identical for all measurements. The contrast-enhanced target lesion to non-enhanced muscle tissue contrast ratio (R) was defined in terms of the following formula based on the mean SIs in the ROIs:

R=SIcontrast-enhanced target lesion/SInon-enhanced muscle tissue

Statistical analysis

Statistical analysis was performed using dedicated statistics software (SPSS version 26, SPSS Inc., Chicago, IL, USA). For the descriptive statistics, the numerical values were presented as means ± standard deviation at 95% confidence intervals. To evaluate the differences between the modified sequence parameters in the related samples, the Wilcoxon signed-rank test (in the case of two values of the modified parameter) and the Friedman test (in the case of more than two values) including post-hoc testing and Bonferroni multiple testing correction were used. Furthermore, possible positive or negative correlations between the values of the modified parameters and the size of the artifact diameter, as well as the contrast-enhanced target lesion to non-enhanced muscle tissue contrast ratio were evaluated. For this purpose, the Bravais–Pearson correlation coefficient was calculated and tested for significance on both sides. To assess the significance of the results, the effect strength, r, of the Bravais–Pearson correlation coefficient was additionally presented using Cohen’s classification (r = 0.10: weak effect, r = 0.30: medium effect, r = 0.50: strong effect). To determine the differences between the IAs of the MR-compatible needles as unrelated samples, the Kruskal–Wallis test was used. To measure the interrater reliability between the two blinded readers, the intraclass correlation coefficient (ICC) was calculated. A P value of 0.05 was set as the limit of statistical significance.

Results

Intervention angle

The seven IAs (0°–90°) exhibited significant differences (P < 0.001) in artifact diameters (Figures 3, 4, 5), with the artifacts increasing considerably with higher IAs, which also proved to be significant for multiple pairwise comparisons (14 pairs) (Supplementary Table 3). Here, only seven pairwise comparisons of stepwise increased IAs did not show any significant differences (Supplementary Table 3).

Figure 3
Figure 4
Figure 5
Table 3

Artifact diameters at 50% and 25% of the inserted 18G coaxial Nitinol needle length at various sequence parameters as a function of the intervention angle

The mean values and standard deviations of needle shaft artifact diameters as a function of the IA in relation to the B0 field of both readers are presented in Table 1.

Table 1

Flip angle

The artifact size decreased gradually with an increase in FA for each IA (IA0: 1.40–7.05 mm, IA15: 5.05–7.40 mm, IA30: 7.15–12.35 mm, IA45: 9.85–15.45 mm, IA60: 11.30–16.25 mm, IA75: 14.55–19.45 mm, IA90: 18.90–24.85 mm; P < 0.001) (Supplementary Figure 1). The pairwise comparison did not reveal any significant differences among the stepwise increased parameters. However, the multiple testing revealed significant differences among four pairs of FAs (Supplementary Table 4). For all seven IAs, significant and strong positive correlations between the FAs and the artifact diameters were observed (r = −0.973, P = 0.001; r = −0.910, P = 0.012; r = −0.981, P < 0.001; r = −0.970, P = 0.001; r = −0.973, P = 0.001; r = −0.978, P < 0.001; r = −0.919, P = 0.010) (Figure 3). In addition to the central hypointense needle artifact, a hyperintense peripheral rim was observed at FAs of 10° and 20°, which was included in the artifact diameter measurements.

Figure 1
Figure 3

Bandwidth

On modifying the receiver BW, no significant difference in artifact diameter was found for any of the different IAs (IA0: 3.45–3.90 mm, IA15: 6.15–6.25 mm, IA30: 8.00–8.55 mm, IA45: 11.40–11.75 mm, IA60: 11.90–12.85 mm, IA75: 15.75–15.90 mm, IA90: 18.90–20.25 mm; P = 0.594) and neither was there a significant correlation between the artifact diameter and the BW (r = −0.576, P = 0.424; r = −0.575, P = 0.425; r = −0.680, P = 0.320; r = 0.746, P = 0.254; r = 0.573, P = 0.427; r = −0.817, P = 0.188).

Matrix

The Friedman test revealed no significant differences between the artifact diameters when comparing six matrix sizes for each IA (IA0: 3.25–3.95 mm, IA15: 4.70–6.85 mm, IA30: 8.60–9.65 mm, IA45: 10.30–11.95 mm, IA60: 12.25–14.10 mm, IA75: 17.20–18.10 mm, IA90: 19.70–26.40 mm; P = 0.335). In addition, the pairwise comparisons did not indicate any significant differences (P = 1.000) (Supplementary Table 4). However, significant positive correlations were found between the mean artifact diameters of both readers and the matrix for the IAs of 75° and 90° (r = 0.873, P = 0.023; r = 0.969, P = 0.001, respectively) (Figure 4). For the other IAs, there was no significant correlation between the artifact diameter and the matrix. In addition, an increased differentiation between the display of the actual needle and the surrounding needle artifact was observed with larger matrices.

Figure 4

Slice thickness

On modifying the ST, significant differences in artifact diameter were found for each IA (IA0: 3.20–6.40 mm, IA15: 4.90–7.85 mm, IA30: 7.25–9.25 mm, IA45: 10.10–12.65 mm, IA60: 11.40–15.65 mm, IA75: 15.65–19.75 mm, IA90: 18.10–26.25 mm; P < 0.001) (Supplementary Figure 2). The multiple testing revealed significant differences between the STs of 3 and 17 mm (P < 0.001) (Supplementary Table 4). A significant correlation between the artifact diameters and ST was found for IAs of 45°, 60°, 75°, and 90° (r = −0.943, P = 0.016; r = −0.933, P = 0.020; r = −0.880, P = 0.049, r = −0.955, P = 0.011) (Figure 5).

Figure 2
Figure 5

Read-out direction

For the two different read-out directions (right >> left, anterior >> posterior), no significant differences in artifact diameters were found during the Wilcoxon signed-rank test (P = 0.785), with generally similar artifact diameters for both read-out directions.

Artifact diameters at the tip of the 18G coaxial Nitinol needle at various sequence parameters as a function of the intervention angle

The mean values and standard deviations of the artifact diameters at the needle tip as a function of the IA in relation to the B0 field of both readers are presented in Table 2. A ball-like tip artifact occurred using low IAs of 0°–45°. The maximum diameter of this artifact increased gradually with a decrease in IA (P = 0.022) (Figure 6). The pairwise comparisons revealed significant differences between 0° and 30° (P = 0.041), as well as between 0° and 45° (P = 0.047) (Supplementary Table 5). The modification of the sequence parameters, BW, matrix, ST, read-out direction, had no significant influence on this artifact (P = 0.082, P = 0.614, P = 0.163, P = 0.465), while that of the FA did (P = 0.003).

Table 2
Figure 6

Interrater reliability

For the various IAs (0° 15°, 30°, 45°, 60°, 75°, 90°), the ICCs were 0.998, 0.994, 0.995, 0.999, 0.997, 0.998, and 0.998, respectively (P < 0.001), indicating excellent interrater reliability (Table 3).

Table 3

Contrast-enhanced target lesion to non-enhanced muscle tissue contrast ratio

The lesion-to-muscle-contrast ratio, R, presented significant positive correlations with an increase in FA and matrices (P < 0.001; P = 0.003), as well as a significant negative correlation with an increase in ST (P = 0.007). No significant correlations were found for the modified BWs (P = 0.171). The corresponding data are presented as supplemental information (Supplementary Table 6).

Discussion

In this 3.0 T musculoskeletal phantom study, the influence of different sequence parameters of an interventional real-time fluoroscopic pulse sequence with TrueFISP contrast on the artifact behavior of a commercially available MR-compatible coaxial 18G Nitinol needle was investigated as a function of the IA.

Needle artifacts pose a major limitation to high-field MRI-guided interventions in particular, regardless of the intended target, and are caused by several different physical processes, of which inhomogeneities of the B0 field experienced by the nuclei are the most important. This needle-induced B0 inhomogeneity is caused by the geometric characteristics and the individual magnetic susceptibility of the imaged object. Distortions of the spatial geometry, as well as intra-voxel dephasing are caused by these static field errors.17,23 Among other artifacts, needle artifacts can be caused by radiofrequency effects such as B1 enhancement.24 With this background, the present study aimed to analyze artifact formation with a focus on its relevance for MRI-guided high-field musculoskeletal interventional procedures through modifying different sequence parameters (FA, BW, matrix, ST, and read-out-direction) as a function of the IA. Completely erased or too-small artifacts are not always desirable in MR-guided intervention since the needle is visualized by the artifact itself and minimizing artifacts can mean the needle is difficult to recognize.

In general, the technological advances in magnet, coil, protocol, biopsy needle, and probe design have made MRI-guidance a clinically valuable imaging technique for minimally invasive procedures. Due to the continuing innovations in augmented reality, targeting software, and compatible devices, it is crucial to reassess methodological and technical fundamentals, such as needle artifacts. This is especially the case for MRI-guided procedures for musculoskeletal interventions, which is an extremely new field, and specific adaptations need to be made. As such, a phantom that has been adapted to the target tissue in musculoskeletal interventions (muscle phantom) was selected, in contrast to previous studies, which generally employed a 3 T MRI scanner.25,26 Singh et al.25 evaluated needle artifact diameters using an acrylic phantom modifying only two parameters: IA and read-out direction. Furthermore, in the present study, contrast medium application was also performed for experimental evaluation of the visibility of the target lesion and to emulate as far as possible the clinical routine, exemplarily imitating contrast-enhanced MR-guided punctures of joint structures in the case of capsulitis.

It is well known that the IA is closely associated with the artifact size.17,22,27 In line with this, the seven IAs (0°–90°) analyzed in this study exhibited significant differences in artifact diameters, with the artifacts increasing considerably with higher IAs, which also proved to be significant for most of the multiple pairwise comparisons. Elsewhere, Schmidt et al.20 demonstrated a positive correlation between artifact size and increasing IAs in their 1.5 T-liver phantom study. At this point, it should be noted that it is advantageous to use low susceptibility materials since these can be used at higher IAs. In addition, Frahm et al.28 analyzed the relationship between the magnetic field strength and the IA. The authors found that the needle artifact growth with an increase in IA was lower with a 0.2-T field strength than with a 1.5-T strength and that at high-field strengths, the artifact size correlated closely with an increase in IA relative to the B0 field.28

In the present study, decreasing artifact diameters were observed with an increase in FA for each IA. At FAs of 10° and 20°, an additional hyperintense peripheral rim artifact was observed around the otherwise hypointense artifact along the shaft of the needle, which was included in the measurements. This artifact consecutively extends the area of potential misinterpretation of the actual needle position and needs to be considered when choosing a FA of 10° or 20° for the TrueFISP sequence. Interestingly, in a previous liver phantom study by Schmidt et al.20 that analyzed a T1-weighted gradient echo (GRE) sequence at 1.5 T, this hyperintense peripheral rim artifact was observed at high FAs of >45°. Another previous investigation of needle artifacts by Bauch29, who also modified the FA in a T1-weighted GRE sequence, revealed no relevant changes to the artifact diameter in a stepwise comparison for FAs of <45°, which is in line with both the results of the present study and those obtained by Schmidt et al.20 However, a T1-weighted GRE sequence was analyzed in these studies and therefore these results cannot be expected to be directly transferrable to ours. This notwithstanding, the multiple testing revealed significant differences between four pairs of FAs, and significant and strong positive correlations between FA and artifact diameter were observed in the present study for all seven IAs. While the previous investigations demonstrated optimal artifact behavior with FAs of <45° for T1-weighted GRE sequences,20,29 in contrast, the present study found the smallest artifact sizes with higher FAs (>40°).

No significant correlation was found between artifact diameter and modifications of the BW, although varying the BW is reported in the literature to be a crucial parameter for the minimization of needle artifacts.30 The physical context is that the Larmor frequencies of the hydrogen protons are altered to a certain amount by a metallic object of a given size and susceptibility. Thus, reducing the BW increases the number of pixels that are visibly affected by the variance in frequencies and consecutively increases the size of the susceptibility artifact.31 However, this finding using a TrueFISP sequence is consistent with Schmidt et al.’s20 results when analyzing the BW as a potential influencing parameter on artifact diameters for a T1-weighted GRE sequence, who also did not find any significant differences between different BWs and artifact behavior in a liver phantom. The fact that the BW variations did not significantly influence the needle artifact size may have been because the artifact was too small, meaning potentially significant differences could have remained hidden. However, the BW range in the present study was chosen according to the standard BWs used in clinical practice.

No significant differences in artifact diameter were found when comparing various matrix sizes for each IA, which was also the case with the pairwise comparisons. However, significant positive correlations were found between artifact diameter and matrix for IAs of 75° and 90°. In addition, an increased differentiation between the display of the actual needle and the surrounding needle artifact with larger matrices was observed, which is also in line with Schmidt et al.’s20 results, who observed smaller artifact diameters at higher matrix sizes in their liver phantom study (not statistically significant). Generally, a higher matrix size reduces the artifact diameters and optimizes the image quality due to decreased voxel volume. In determining the spatial resolution, the matrix is a quality feature of the acquired image data,28 meaning higher matrices may improve the differentiation of the actual intervention needle and therefore allow for more exact lesion targeting. Nonetheless, the increase in acquisition time is the major reason why matrix sizes cannot be set as high as possible in clinical practice.29

The voxel size is not only determined by the matrix, but also by the ST. A decrease in ST is equivalent to a reduction in voxel size and leads to a decreased field inhomogeneity within each individual voxel and subsequently results in lower artifact dependence and the generation of smaller needle artifacts.28,32 In the present study, significant differences in artifact diameters were observed for each IA when modifying the ST. In addition, the multiple testing revealed significant differences between STs of 3 and 16 mm, and a significant correlation between the artifact diameters and the ST was found for IAs of 45°, 60°, 75°, and 90°. However, in our study setting, smaller artifact sizes were found for higher STs. In this context, it must be noted that the artifact size in the ST-modified scan series appears to be highly influenced by different IAs and that the differentiation of the actual needle shaft and tip is much better with higher STs (>10 mm) when looking at higher IAs. However, it should also be remembered that the ST should not be set too high during the procedure to allow for accurate needle placement. Thus, a potential compromise is selecting a ST of >7 mm. No significant differences in needle artifact sizes were observed for the two different read-out directions (RL or AP) in this study. This is consistent with previous studies on T1-weighted GRE sequences,18,20,28 but not with a previous study on spin-echo and turbo spin-echo sequences, in which the artifacts were more pronounced when the read-out direction was perpendicular to the needle shafts.18

Ball-like tip artifacts were observed with low IAs of 0°–45° and these increased in size with a decrease in IA. Interestingly, this artifact was not significantly influenced by any sequence parameter other than the FA. This artifact at the needle tip particularly impairs the visibility of the tip, which makes precise needle guidance difficult and can be expected to affect the targeting accuracy. Moreover, it is problematic that this tip artifact extends in all directions such that it often resembles a ball; hence the “ball-like” description.29,33 In line with our results, this tip artifact occurred with low IAs of 0°–10° in a previous study by Schmidt et al.20 As previously described by Liu et al.34, the B0 field is most strongly influenced in the area around the needle tip, which is particularly noticeable in materials with lower magnetic susceptibility, such as carbon fiber or titanium, when compared with other materials (e.g., chromium, cobalt, or nickel).

Regarding clinical routine high-field musculoskeletal interventional procedures, we recommend using a FA of 40°–60° to minimize hypointense artifact formation around the needle shaft and to avoid the occurrence of additional hyperintense artifact formation, which only occurred at low FAs of 10° and 20° in the present scan series. In addition, an ST of 10–16 mm returned the best image quality. To specifically avoid ball-like tip artifacts, IAs of 45°–60° should be selected.

Furthermore, it is important to not only minimize needle artifacts but also to guarantee sufficient visibility of the target lesion. Therefore, the contrast ratio of a gadolinium-enhanced target lesion placed centrally into the muscle phantom and that of the adjacent non-enhanced muscle tissue were evaluated by quantitatively analyzing the corresponding SIs. The contrast-enhanced target lesion was best visualized at higher FAs (40°–60°) and matrices (224 × 224/256 × 256), while a negative correlation between the visibility of the target lesion with increasing STs was observed, which can be explained by the increasing partial-volume effects at higher STs. For small lesions (relative to the ST), this might lead to a potential conflict since higher STs of 10–16 mm minimized the needle artifacts while maintaining the best possible visualization of the coaxial intervention needle. To the best of the authors’ best knowledge, there are no comparable previous studies that investigated the visibility of a contrast-enhanced lesion in a similar setting.

However, this study involves a number of potential limitations. First, a fixed phantom was used, which provided an optimal background signal intensity and therefore an optimized depiction of signal voids. In an in vivo setting, it must be assumed that both the image quality and the artifact contrast will be worse due to, for example, motion artifacts. Second, this phantom study was performed at a single field strength (3.0 T), and lower field strengths (e.g., 1.5 T) will need to be investigated with this TrueFISP sequence in view of scenarios such as when the patient is not suitable for a high-field intervention due to only 1.5 T-conditional external materials. Nevertheless, 3.0 T is the preferable field strength in the majority of musculoskeletal investigations. Third, only a single alloy (Nitinol) and a single needle size (18G) were investigated. As both alloy and needle size have an impact on artifact behavior,29,33 further studies are needed to examine these effects. Fourth, the artifact diameters were determined by manual measurements and automatized artifact measurements would minimize any potential reader bias. However, high inter-reader agreement was observed in our study. Furthermore, the artifact diameters were measured in two-dimensional terms and it must be acknowledged that needle artifacts occur three-dimensionally and that the needle artifact volume might be a relevant parameter for exact needle guidance. Nonetheless, depending on the sequence acquisitions, it might not be adequately feasible to conduct such measurements with the available fluoroscopic MRI hardware and software. Fifth, only one single sequence parameter was modified in our scan series to avoid any additional confounding variable; however, the BW was not modified separately but only coupled to the TR since the minimum TR had been systematically chosen in our experimental setting. Furthermore, while the image quality will not be affected by increasing motion artifacts with longer scan times (with an increase in TR) in a phantom model, it may be in real-world settings. Sixth, minimized artifact diameters do not necessarily imply that the “true” position of the needle within the tissue is better known, as it is inherently difficult to be certain about the exact needle position from real-time fluoroscopic MRI visualization. Therefore, further studies with coordinate registration are needed to ensure more accurate verification of the exact needle position and, in particular, the position of the needle tip. In a previous study, Yamada et al.35 applied real-time ultrasound imaging fused with reformatted static MR images and coordinate registration for needle guidance during MR-guided percutaneous tumor ablations and revealed targeting errors of 1.6 ± 0.6 mm. Last, the investigated sequence parameter settings need to be analyzed and adapted to clinical use cases.

In conclusion, to minimize needle artifacts, it is recommended to use FAs of 40°–60°, a ST of >7 mm, and, if possible, an IA of 45°–60°. The visibility of the target lesion and the needle’s artifact behavior must be weighed up against each other when choosing the ST, while higher FAs (40°–60°) and matrices (224 × 224/256 × 256) are associated with low artifacts and sufficient lesion visibility.

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