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Occult Lumbosacral Dysraphism in Children and Young Adults: Diagnostic Performance of Fast Screening and Conventional MR Imaging¹

¹ From the Department of Radiology, Health Services and Policy Section, Children's Hospital Medical Center, 3333 Burnet Ave, Cincinnati, OH 45236 (L.S.M.), and the Department of Radiology, Harvard Medical School, Children's Hospital, Boston, Mass (M.A.O., D.Z., T.Y.P., J.D., P.D.B.). Received January 27, 1998; revision requested April 7; revision received September 11; accepted November 9. Address reprint requests to L.S.M.

	Abstract

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PURPOSE: To compare fast screening and conventional magnetic resonance (MR) imaging for the detection of occult dysraphic myelodysplasias in children and young adults.

MATERIALS AND METHODS: A retrospective case-control study included 101 patients (mean age, 4.9 years; range, 1 day to 26 years) suspected of having occult lumbosacral dysraphism. Sixty case patients had myelodysplastic lesions (19 filar lipoma, 14 syringomyelia, 10 intradural lipoma, eight dermal sinus, five diastematomyelia, five lipomyelomeningocele, two caudal regression syndrome); 41 control patients had no dysraphic lesions; 17 patients had associated renal anomalies. Two neuroradiologists reviewed MR images from conventional and fast screening protocols. Diagnostic performance parameters included sensitivity, specificity, and area under the receiver operating characteristic curve (A_z value).

RESULTS: The sensitivity of conventional and fast screening MR studies was 97.1% and 98.5%, respectively; the specificity was 90.9% and 84.8%, respectively. The A_z value was 0.973 for the fast screening and 0.976 for the conventional MR studies (P = .83). Interobserver agreement was very good for fast screening images ( = 0.68) and excellent for conventional images ( = 0.75). For renal anomalies, the A_z value was 0.786 and 0.853 for fast screening and conventional MR imaging, respectively (P = .28).

CONCLUSION: Conventional three-plane lumbosacral MR imaging in children and young adults suspected of having occult dysraphism provides better diagnostic information than does fast screening two-plane MR imaging because of its higher specificity and interobserver agreement.

Index terms: Magnetic resonance (MR), in infants and children • Spinal cord, developmental defect, 33.145, 33.148, 33.361 • Spinal cord, MR, 33.121411 • Spinal cord, neoplasms, 33.361, 33.368, 33.369

	Introduction

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Occult spinal dysraphism is one of the most common indications for spinal magnetic resonance (MR) imaging in children and young adults. The clinical findings range from skin stigmata such as a dimple, hair patch, or hemangioma to dysfunctions of gait, bladder, or bowel (1–3). In addition, occult dysraphism commonly is associated with genitourinary tract anomalies (4). Spinal MR imaging, therefore, has the important role of helping determine the presence of a dysraphic myelodysplasia and associated urinary tract anomalies so that appropriate surgical and medical treatment can be instituted.

The authors of several descriptive studies (1–3,5–7) have illustrated the importance of spinal MR imaging for the characterization of a variety of occult dysraphic lesions, including filar lipoma, intradural lipoma, dermal sinus, lipomeningocele, and diastematomyelia. However, these studies have had two limitations. First, varying imaging protocols were used in these studies. Hence, the number of MR imaging sequences used per protocol ranged from two to six, depending on the institutional preference. Second, most of these studies lacked an adequate control group. Therefore, the diagnostic performance (ie, sensitivity, specificity, and receiver operating characteristic [ROC] curve) for the different lumbosacral MR protocols is not known. To our knowledge, no large analytic study has been performed to determine the diagnostic performance of different MR protocols in children and young adults suspected of having occult dysraphism. The determination of optimal MR imaging standards that are based on diagnostic performance is of prime importance to patient care, because of the ongoing restructuring of the field of health care.

We hypothesized that a fast screening MR imaging protocol that includes acquisition of only axial and sagittal T1-weighted images would have the same diagnostic performance as a conventional MR imaging examination and could be used as a screening examination for lumbosacral dysraphism. To test this hypothesis, a case-control study was conducted with children and young adults suspected of having lumbosacral occult dysraphism. A blinded comparative analysis of the results of a fast screening MR imaging protocol versus those of a conventional MR imaging protocol was performed to determine the diagnostic performance of both protocols in relation to the outcomes of dysraphism and associated renal anomalies.

	MATERIALS AND METHODS

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Study Design
All patients in the study were referred for lumbosacral spinal MR imaging for evaluation of possible occult dysraphic myelodysplasia. The specific clinical findings are shown in Table 1. Patients with a history of nonoccult dysraphism (ie, spina bifida aperta or myelomeningocele), intracranial abnormalities, or central nervous system surgery were excluded from the study.

All patients underwent MR imaging with a 1.5-T system (Signa; GE Medical Systems, Milwaukee, Wis) equipped with a surface spine coil. A complete conventional lumbosacral MR imaging study was obtained in all patients. The MR imaging studies were subsequently classified in two protocol sets: conventional studies and fast screening studies (Table 4). The conventional four-sequence MR imaging protocol included the following pulse sequences: a thick-section sagittal spin-echo T1-weighted localizer sequence followed by thin-section sagittal, axial, and coronal spin-echo T1-weighted sequences. The fast screening two-sequence protocol included thin-section sagittal and axial spin-echo T1-weighted sequences.

Study Analysis and Statistical Tests
The fast screening and conventional MR images were read independently by two experienced pediatric neuroradiologists (T.Y.P., P.D.B.), who had pediatric spinal MR imaging experience of 7 (T.Y.P.) and 13 years (P.D.B.). Both reviewers were blinded to the study population case mix, clinical data, and results of other imaging studies. All patient-identifying marks, including age, sex, and history, were covered with a black mask. In all cases, the fast screening MR study was read first, followed by the conventional MR study. The cases were read in random order with at least 4 weeks between readings of the two sets of studies. This was done to prevent test-interpretation and memory-recollection biases (9).

For occult dysraphic myelodysplasias and renal abnormalities, rating scores for each reader were dichotomized as positive or negative and were compared with the final diagnosis to determine the sensitivity and specificity. The 95% CIs were derived by using the Pratt approximation (10).

ROC curve analyses were performed because these analyses provide a description of disease detectability independent of the effects of disease prevalence and decision threshold (11). ROC curves were obtained by using a questionnaire with a five-point confidence-rating scale: score of 1, definitely not present; score of 2, probably not present; score of 3, indeterminate; score of 4, probably present; and score of 5, definitely present. ROC curve analyses were performed by using the ROC ANALYZER program for Windows (Centor RM, University of Alabama, Birmingham). The area under the curve (A_z) and the standard error of A_z were calculated by using the nonparametric trapezoidal rule (12). The A_z values for the screening and conventional MR imaging studies were compared for each reader by using the Wilcoxon statistic (13). The questionnaire also included information about imaging findings, differential diagnosis, number of kidneys, specific renal abnormalities, and the technical quality of the imaging study.

Results of the independent readings were analyzed with the statistic to measure the degree of interobserver agreement (14). Two-tailed P values were calculated, and a value of less than .05 was considered to indicate a statistically significant difference.

	RESULTS

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Characteristics of the Study Population
The study included 101 patients suspected of having occult dysraphism. The mean age (±SD) was 4.9 years ± 5.2, and the age range was 1 day to 26 years. Forty-six (46%) patients were aged younger than two years. There were 36 male (36%) and 65 female (64%) patients.

The case group included 60 (59%) patients with a broad spectrum of occult myelodysplastic lesions (Table 2), and the control group included 41 (40%) patients with no dysraphic disorders (Table 3). The 60 patients in the case group had a total of 68 lesions, because eight patients had two abnormalities each (Table 2). Seventeen patients had renal abnormalities, 15 (88%) of whom also had a dysraphic lesion (Table 2).

Protocol Analysis
Occult dysraphic myelodysplasias.—Table 5 shows the sensitivity and the specificity associated with the MR imaging protocols and the readers. The sensitivity of fast screening MR imaging for occult myelodysplasias was 98.5% (95% CI = 92.1%, 99.9%) for both readers. The sensitivity of conventional MR imaging was 97.1% (95% CI = 89.8%, 99.7%) for reader 1 (T.Y.P.) and 95.6% (95% CI = 87.6%, 99.1%) for reader 2 (P.D.B.). The specificity of fast screening MR imaging was 84.8% (95% CI = 68.1%, 94.9%) for reader 1 and 75.8% (95% CI = 57.7%, 88.9%) for reader 2. The specificity of conventional MR imaging was 90.9% (95% CI = 75.7%, 98.1%) for both readers.

With regard to interobserver agreement for occult myelodysplasias, values of 0.68 for fast screening MR images and 0.75 for conventional MR images were obtained.

Figures 1 and 2 show the ROC curves for the readers and MR imaging protocols. Table 6 shows that the A_z values for both readers were greater than 0.9 for both MR imaging protocols. Comparison of A_z values revealed no significant differences (reader 1, P = .83; reader 2, P = .24).

View larger version (13K): [in this window] [in a new window]   Figure 1. ROC curve for detection by reader 1 of occult dysraphism on conventional and fast screening MR images.

View larger version (14K): [in this window] [in a new window]   Figure 2. ROC curve for detection by reader 2 of occult dysraphism on conventional and fast screening MR images.

The ROC curve analysis demonstrated A_z values of 0.786–0.874 for both protocols and readers (Table 6). There were no significant differences between the ROC curves (reader 1, P = .28; reader 2, P = .29).

Time Analysis
The acquisition time for the conventional MR imaging protocol ranged from 15 minutes 27 seconds to 16 minutes 44 seconds (Table 4), and the total examination time (including patient positioning, study localization, and study acquisition) was 25–30 minutes. The acquisition time for the fast screening MR imaging protocol ranged from 8 minutes 11 seconds to 9 minutes 28 seconds (Table 4), and the total examination time was 18–20 minutes.

	DISCUSSION

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The conditions in the 101 patients included in this study represented a wide spectrum of occult dysraphic myelodysplasias and associated renal anomalies (Table 2). For the outcome of dysraphic myelodysplasia, the sensitivity of fast screening MR imaging (98.5%) was similar to that of conventional MR imaging (95.6%–97.1%). The specificity of conventional MR imaging (90.9%) was greater than that of fast screening MR imaging (75.8%–84.8%). However, the ROC curve analysis demonstrated excellent diagnostic performance with both protocols, with A_z values greater than 0.9 and no significant differences (P .24). None of the patients with false-positive or false-negative results obtained with either imaging protocol had a tethering lesion that necessitated surgery. Interobserver agreement was very good for the fast screening MR images ( = 0.68) and excellent for the conventional MR images ( = 0.75) (15).

For the outcome of renal abnormalities, the sensitivity of fast screening MR imaging (61.5%–76.9%) was less than that of conventional MR imaging (70.6%–81.3%). The specificities of conventional and fast screening MR imaging were the same (90.9%). Diagnostic performance, determined on the basis of ROC curve analyses, showed A_z values of 0.786–0.874 for both imaging protocols. No significant differences were noted when the A_z values were compared (P .28). However, 12 fast screening and four conventional MR imaging studies were read as indeterminate for renal abnormalities because of incomplete imaging.

The diagnostic performance of fast screening MR imaging for the detection of occult myelodysplasia may allow its use as a screening examination. The 5-mm sagittal spin-echo T1-weighted localizer images and the 3-mm coronal spin-echo T1-weighted images from the conventional protocol did not help improve the sensitivity of MR imaging for the detection of occult dysraphic myelodysplasias. However, the availability of these two additional sequences as part of the conventional MR imaging protocol resulted in an increase in the specificity of MR imaging and a decrease in the number of indeterminate renal evaluations.

For both protocols, the diagnostic performance (ie, A_z value) for renal abnormalities was less than that for the dysraphic lesions. This result suggests that additional renal MR imaging sequences (ie, axial and coronal fast spin-echo T2-weighted imaging) should be performed in patients with occult dysraphism if commonly associated renal anomalies are to be adequately assessed. The additional MR imaging sequences may be more time efficient and cost-effective than a separate renal US examination. This consideration may be of particular importance in markets where capitation plays a major role.

In the event that an occult dysraphic lesion is identified on either the fast screening or the conventional lumbosacral MR images, neither study may provide all the pertinent information needed to fully characterize dysraphic myelodysplasia. Lumbosacral MR imaging studies in children should be monitored regardless of the protocol, so that preoperative sequences such as T2-weighted and fat-suppressed contrast material–enhanced T1-weighted MR imaging in patients with diastematomyelia and dermal sinus can be ordered appropriately. This is especially true in the child who is sedated. MR imaging of the entire spine may be necessary in patients with clinical findings above the lumbosacral level or with symptoms and signs that may be due to conditions other than dysraphic myelodysplasia despite a negative lumbosacral fast screening MR study.

By design, this case-control study involved a population with a high prevalence of occult dysraphism. Because sensitivity and specificity are characteristics of a test, they are independent of the prevalence of disease (11,16). This, therefore, allowed us to determine the sensitivity and specificity of spinal MR imaging protocols by using a broad case mix of occult dysraphic myelodysplasias.

Additional analytic studies are needed to confirm the findings we have described. Multicenter prospective randomized trials could be performed to compare different imaging modalities and to determine the best approach for the outcomes of occult dysraphic myelodysplasias and associated renal anomalies. These studies could include newer MR imaging techniques such as spinal cord motion sequences, the clinical effectiveness of which has not yet been fully determined (17). In addition, decision-analysis and cost-effectiveness studies are necessary to determine optimal imaging strategies in children and young adults suspected of having occult dysraphism.

In conclusion, recent changes in the field of health care have emphasized the importance of determining the exact diagnostic performance of different MR imaging protocols to ensure optimal patient care. Our results suggest that conventional three-plane lumbosacral MR imaging in children and young adults suspected of having occult dysraphism provides better information than fast screening two-plane MR imaging because of the higher specificity and interobserver agreement of the former.

	Footnotes

 
Abbreviation: ROC = receiver operating characteristic

Author contributions: Guarantors of integrity of entire study, L.S.M., P.D.B.; study concepts, L.S.M., M.A.O., D.Z.; study design, L.S.M., M.A.O.; definition of intellectual content, L.S.M.; literature research, L.S.M., M.A.O.; clinical studies, L.S.M., M.A.O., T.Y.P., P.D.B.; data acquisition, T.Y.P., P.D.B.; data analysis, L.S.M., M.A.O., D.Z., J.D.; statistical analysis, L.S.M., D.Z., J.D.; manuscript preparation, L.S.M., M.A.O., D.Z.; manuscript editing, L.S.M., D.Z., T.Y.P., P.D.B.; manuscript review, L.S.M.

	References

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