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AJR 2000; 175:407-411
© American Roentgen Ray Society


Original Report

Clinical Value of Thin Collimation in the Diagnostic Workup of Pulmonary Embolism

Martine Remy-Jardin1, Jacques Remy, Froohar Baghaie, Marc Fribourg, Dominique Artaud and Alain Duhamel

1 All authors: Department of Thoracic Imaging, Hospital Calmette, Blvd. Jules Leclerc, 59037, Lille Cedex, France.

Received July 29, 1999; accepted after revision January 26, 2000.

 
Address correspondence to M. Remy-Jardin.


Abstract
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Abstract
Introduction
Subjects and Methods
Results
Discussion
References
 
OBJECTIVE. We report our experience with thin-collimation helical CT in a population of patients suspected of having pulmonary embolism.

CONCLUSION. Thin-collimation helical CT provided technically acceptable examinations for pulmonary embolism in 360 patients (97%). In this population, CT revealed pulmonary embolism in 104 patients (29%), negative findings in 217 patients (59%), indeterminate findings in 39 patients (10%), and alternative diagnoses in 65% of patients with negative or inconclusive findings. Ventilation-perfusion scanning and Doppler sonography of the lower extremities were performed in 158 (44%) and 133 patients (37%), respectively, whereas pulmonary angiography was performed in 27 patients (7.5%). The estimated false-negative rate of helical CT was 5%.


Introduction
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Abstract
Introduction
Subjects and Methods
Results
Discussion
References
 
To date, most investigations that have evaluated helical CT in the diagnostic workup of pulmonary embolism have stressed its excellent sensitivity and specificity but have limited the accuracy of CT to the segmental pulmonary artery bed. The recent introduction of subsecond scanning times has enabled the scanning of patients with thin collimation, improving spatial resolution without requiring a longer breath-hold period or sacrificing anatomic coverage. We describe our experience with thin-collimation helical CT in a population of patients suspected of having pulmonary embolism.


Subjects and Methods
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Abstract
Introduction
Subjects and Methods
Results
Discussion
References
 
Between August 1996 and December 1997, 370 patients (261 men and 109 women; age range, 15-90 years; mean age, 58.6 years) were examined with thin-collimation helical CT angiography after helical CT. Helical CT scans were analyzed during the course of clinical workup by one of four subspecialty-trained chest radiologists experienced in evaluating helical CT studies for acute pulmonary embolism. A retrospective interpretation was organized at the end of the inclusion period that involved an experienced chest radiologist and a junior radiologist to calculate interobserver variation.

The presence of endoluminal clots on CT scans was considered diagnostic of embolism; central emboli included thrombi in main arteries, lobar arteries, or both; peripheral thrombi consisted of endoluminal clots in segmental and/or subsegmental branches. Isolated subsegmental embolism was assessed on concordant imaging studies (CT and pulmonary angiography) with positive findings or on CT with positive findings and rapid clinical improvement after the initiation of anticoagulation therapy. When helical CT did not depict thrombus down to the subsegmental level, the examination had negative findings; according to the degree of their clinical suspicion, the clinicians were responsible for referring this group of patients to undergo pulmonary angiography. When helical CT revealed negative findings without further pulmonary angiographic evaluation, the patients were followed up for at least 3 months to detect any clinical events that could be related to pulmonary embolism. If pulmonary embolism was diagnosed on pulmonary angiography or during follow-up, then the helical CT study was labelled false-negative. When the confident exclusion of pulmonary embolism on helical CT scans was limited to central pulmonary arteries, helical CT was interpreted as inconclusive; these cases consisted of technically limited CT scans that could not allow the assessment or exclusion of peripheral emboli.

All followed patients were clinically reexamined after a mean period of 3.2 months (range, 2.7-4 months). Patients were asked to return to the hospital if they experienced symptoms or signs that suggested pulmonary embolism. If the follow-up examination could not be performed at our institution, we contacted the patients' family physicians by telephone and asked about the occurrence of any clinical events that could be related to pulmonary embolism. These patients did not undergo further investigation. If the patient had died, the cause of death was determined by means of discussion with the physician in charge at the time of death. Ventilation-perfusion scanning and lower extremity Doppler sonography were not systematically included in the initial imaging techniques because of the specificities of the population studied (i.e., high proportion of patients with a history of cardiopulmonary disease or cardiac dysfunction and local equipment constraints).

Helical CT angiograms of the pulmonary arteries were obtained with a Somatom Plus A4 scanner (Siemens Medical Systems, Erlangen, Germany) with a 0.75 sec per revolution scanning time. According to the patient's breath-hold capabilities, two acquisition protocols were considered. When patients were able to hold their breath for a 20-sec period, they were scanned with a 2-mm collimation and a table feed of 4 mm per revolution (pitch of 2). When patients were only able to hold their breath for a shorter period of time (e.g., 12 sec), a 3-mm collimation and a table feed of 5 mm per revolution (pitch of 1.7) were selected. When patients were unable to maintain strict apnea, they were scanned while gently breathing with a 2-mm collimation and a table feed of 4 mm per revolution (pitch of 2). According to the acquisition parameters, the study group was divided into two groups of patients: those scanned with a 2-mm collimation and a pitch of 2 (n = 284) and those scanned with a 3-mm collimation and a pitch of 1.7 (n = 86). The patients received an injection of 120-140 mL of 24% (n = 143) or 30% (n = 227) iodinated contrast material at a rate of 4 mL/sec (n = 284) or 5 mL/sec (n = 86), respectively.

Interobserver agreement was expressed as a percentage of agreement and as a kappa coefficient, the latter accounting for the chance agreement between two observers. Kappa values were interpreted as follows: less than 0.20, poor; 0.21-0.40, fair; 0.41-0.60, moderate; 0.61-0.80, good; 0.81-1.0, very good.


Results
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Abstract
Introduction
Subjects and Methods
Results
Discussion
References
 
In 10 patients (3%; group 1), helical CT scans were technical failures because of severe dyspnea (n = 6), poor signal-to-noise ratio (n = 5), and/or suboptimal enhancement of the pulmonary vasculature (n = 4), thus precluding any detection of pulmonary embolism. In 39 patients (10%; group 2), helical CT scans had technical limitations, enabling an accurate evaluation of central arteries but preventing the detection of peripheral thrombi; therefore, these examinations were considered inconclusive. Helical CT scans revealed positive findings for pulmonary embolism in 104 patients (28%; group 3) and negative findings down to the segmental level in 217 patients (59%; group 4). The presence of thrombi in a main or lobar pulmonary artery, whatever the presence of more peripheral clots, defined central pulmonary embolism; it was identified in 75 patients. Thrombi exclusively located within subsegmental and/or segmental arteries defined instances of peripheral pulmonary embolism, which was identified in 29 patients. Among these 29 patients, isolated subsegmental thrombi were depicted in six (two with angiographic confirmation and four assessed on CT with positive results and a rapid clinical improvement after the initiation of anticoagulation therapy) (Figs. 1A,1B,1C and 2A,2B,2C,2D,2E,2F).



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Fig. 1A. —42-year-old woman with symptoms suggestive of acute pulmonary embolism. Helical CT scans (2-mm collimation; pitch, 2; 24% nonionic contrast material; flow rate, 4 mL/sec) obtained at level of lower lobes at mediastinal (window width, 350 H; window level, 30 H) and lung (window width, 1600 H; window level, -600 H) settings show filling defect (arrows) at level of enlarged subsegmental branch of anterior segmental artery of left lower lobe. Note large area of peripheral consolidation suggestive of lung infarction.

 


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Fig. 1B. —42-year-old woman with symptoms suggestive of acute pulmonary embolism. Helical CT scans (2-mm collimation; pitch, 2; 24% nonionic contrast material; flow rate, 4 mL/sec) obtained at level of lower lobes at mediastinal (window width, 350 H; window level, 30 H) and lung (window width, 1600 H; window level, -600 H) settings show filling defect (arrows) at level of enlarged subsegmental branch of anterior segmental artery of left lower lobe. Note large area of peripheral consolidation suggestive of lung infarction.

 


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Fig. 1C. —42-year-old woman with symptoms suggestive of acute pulmonary embolism. Selective left pulmonary angiogram (left posterior oblique view) obtained 24 hr after A and B shows vascular cutoff (arrow) of subsegmental branch of anterior segmental artery of left lower lobe, confirming diagnosis of peripheral pulmonary embolism.

 


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Fig. 2A. —70-year-old man with chronic obstructive pulmonary disease and acute worsening of dyspnea. CT was performed with 2-mm collimation; pitch, 2; 24% nonionic contrast material; flow rate, 4 mL/sec., Helical CT scans at mediastinal window settings (window width, 350 H; window level, 30 H) show filling defects at level of bifurcation of anterior segmental artery of right lower lobe (arrow, A and B) and one of its subsegmental branches (arrow, C).

 


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Fig. 2B. —70-year-old man with chronic obstructive pulmonary disease and acute worsening of dyspnea. CT was performed with 2-mm collimation; pitch, 2; 24% nonionic contrast material; flow rate, 4 mL/sec., Helical CT scans at mediastinal window settings (window width, 350 H; window level, 30 H) show filling defects at level of bifurcation of anterior segmental artery of right lower lobe (arrow, A and B) and one of its subsegmental branches (arrow, C).

 


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Fig. 2C. —70-year-old man with chronic obstructive pulmonary disease and acute worsening of dyspnea. CT was performed with 2-mm collimation; pitch, 2; 24% nonionic contrast material; flow rate, 4 mL/sec., Helical CT scans at mediastinal window settings (window width, 350 H; window level, 30 H) show filling defects at level of bifurcation of anterior segmental artery of right lower lobe (arrow, A and B) and one of its subsegmental branches (arrow, C).

 


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Fig. 2D. —70-year-old man with chronic obstructive pulmonary disease and acute worsening of dyspnea. CT was performed with 2-mm collimation; pitch, 2; 24% nonionic contrast material; flow rate, 4 mL/sec. Corresponding CT scans of lung (window width, 1660 H; window level, -600 H) show segmental (arrow, D and E) and subsegmental (arrow, F) pulmonary artery branches.

 


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Fig. 2E. —70-year-old man with chronic obstructive pulmonary disease and acute worsening of dyspnea. CT was performed with 2-mm collimation; pitch, 2; 24% nonionic contrast material; flow rate, 4 mL/sec., Corresponding CT scans of lung (window width, 1660 H; window level, -600 H) show segmental (arrow, D and E) and subsegmental (arrow, F) pulmonary artery branches.

 


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Fig. 2F. —70-year-old man with chronic obstructive pulmonary disease and acute worsening of dyspnea. CT was performed with 2-mm collimation; pitch, 2; 24% nonionic contrast material; flow rate, 4 mL/sec., Corresponding CT scans of lung (window width, 1660 H; window level, -600 H) show segmental (arrow, D and E) and subsegmental (arrow, F) pulmonary artery branches.

 

Agreement between the two interpreters for the diagnosis of pulmonary embolism on a per patient basis occurred in 364 patients (98%; {kappa}=0.97). When only the main and lobar arteries were considered, the interobserver agreement was 99%, with a kappa value of 0.99. When only the segmental arteries were considered, the interobserver agreement was 99%, with a kappa value of 0.98. When only the subsegmental arteries were considered, the interobserver agreement was 98%, with a kappa value of 0.97. No significant difference was found between the kappa values on 2-mm and 3-mm collimation scans for central and segmental arteries. At the subsegmental level, the kappa value was significantly better on 2-mm ({kappa} = 0.98) than on 3-mm ({kappa} = 0.94) collimation scans (p < 0.05). Overall, discord was most frequent for the subsegmental arteries of the right and left upper lobes.

Pulmonary angiography was performed in 27 (7.5%) of 360 patients with a technically adequate helical CT scan (group 2, n = 5; group 3, n = 2; group 4, n = 20). In group 2, pulmonary angiography revealed negative findings in four patients and depicted an isolated segmental thrombus in the right lower lobe of one patient. In group 3, pulmonary angiographic findings confirmed the CT findings of two patients in whom CT had revealed an isolated subsegmental thrombus. In group 4, pulmonary angiography revealed positive findings in one patient and showed an isolated subsegmental thrombus in the apical segment of the right upper lobe that was not visible in retrospect on helical CT because of the focal suboptimal enhancement of the first centimeter of the z-axis coverage (Fig. 3A,3B). Overall, acute pulmonary embolism was diagnosed in 106 (29%) of 370 patients at the time of the initial evaluation.



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Fig. 3A. —35-year-old woman who was examined for pulmonary embolism after surgery. Helical CT scan obtained at level of upper lobes (2-mm collimation; pitch, 2; 30% nonionic contrast material; flow rate, 4 mL/sec) reveals poor opacification of pulmonary arteries in first centimeter of volume scanned in caudocranial direction, despite 18-sec scanning delay.

 


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Fig. 3B. —35-year-old woman who was examined for pulmonary embolism after surgery. Selective right pulmonary angiogram (right posterior oblique view) shows partial filling defect at level of segmental (long arrow) and subsegmental (short arrow) branches of apical segmental artery of right upper lobe.

 

In 165 patients (22/39 in group 2 and 143/217 in group 4), alternative diagnoses were considered that could explain the clinical presentation but were unrelated to pulmonary embolism (Fig. 4) (Table 1). These diagnoses were made by clinicians at the time of the initial evaluation and recorded in the medical charts. Pneumonia (n = 64) was proven by bacterial culture; acute respiratory failure caused by bronchial infection (n = 58), by resolution of clinical symptoms after treatment with specific medication; malignancy (n = 18), by histologic or cytologic findings; chronic obstructive pulmonary disease (n = 16) and lung fibrosis (n = 4), by functional and imaging techniques; postoperative bronchopleural fistula (n = 4), by fiberoptic endoscopy; and pneumomediastinum (n = 1), by imaging. Apart from the 58 patients diagnosed with acute respiratory failure caused by bronchial infection, helical CT provided diagnostic information in the remaining 107 patients (29% of the study group; 41.8% of patients with negative or inconclusive findings on CT).



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Fig. 4. —47-year-old man with severe lung fibrosis caused by sarcoidosis. Patient was referred for acute chest pain. High-resolution CT scan obtained at level of right bronchus intermedius reveals pneumomediastinum, unsuspected on chest radiograph (not shown) because of superimposition of extensive honeycombing, which explains clinical presentation.

 

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TABLE 1 Alternative Diagnoses Made During Initial Examination

 

Ventilation—perfusion scans were obtained in 158 (44%) of 360 patients with technically adequate helical CT scans (group 2, n = 12; group 3, n = 39; group 4, n = 107). In 12 patients in group 2, ventilation—perfusion scanning revealed high probability in two patients and an intermediate probability in 10. In 39 patients in group 3, ventilation—perfusion scanning revealed high probability in 22 patients and low probability in 17. In 107 patients in group 4, ventilation—perfusion scanning revealed high probability in 25 patients, intermediate probability in 76, and normal findings in six. A combined interpretation of ventilation—perfusion scans and helical CT scans in the 25 patients with ventilation—perfusion scans with a high probability and helical CT scans with normal results led to the identification of focal lung and/or bronchial abnormalities on CT scans in 21 of 25 patients. The following changes were depicted: lung consolidation (n = 9), focal bronchiectasis (n = 6), diffuse emphysema with more severe lesions in the areas of scintigraphic high probability (n = 4), and bronchopulmonary carcinoma (n = 2). Among the 25 patients with discordant CT and ventilation—perfusion scan results, eight underwent pulmonary angiography, which revealed negative findings in every patient. The remaining patients underwent clinical follow-up, which did not reveal recurrent pulmonary embolism. Doppler sonography of the lower extremities was performed in 133 (37%) of 360 patients with a technically adequate helical CT scan (group 2, n = 13; group 3, n = 65; group 4, n = 55). Positive findings were revealed in four patients in group 2, 42 patients in group 3, and 14 patients in group 4. Therefore, a total of 18 patients from groups 2 and 4 received anticoagulants because of deep vein thrombosis in the absence of CT findings of pulmonary embolism.

Seventy-one patients (group 2, n = 12; group 4, n = 59) with unresolved suspicion of pulmonary embolism did not receive anticoagulant drugs and were followed up. All five patients who fulfilled the following criteria were gathered under the label of unresolved suspicion of pulmonary embolism: absence of pulmonary embolism on helical CT or pulmonary angiography, no alternative diagnosis at the time of the initial evaluation, and no anticoagulation therapy for deep vein thrombosis. Three patients from group 2 died within 3 days of the initial helical CT examination. Autopsy was not performed in these patients. The cause of death was related to myocardial infarction in one patient and to end-stage cancer in the remaining two. Sixty-eight patients were alive at the time of follow-up. Among the nine patients from group 2 alive at the time of follow-up, pulmonary embolism was diagnosed in two on helical CT scans at the 1- and 2-month follow-up examinations. None of the 59 patients in group 4 experienced clinical symptoms suggestive of deep vein thrombosis and/or acute respiratory symptoms.

In summary, thin-section helical CT depicted acute pulmonary embolism in 104 patients (29%), including six with isolated subsegmental pulmonary embolism (2%). Initial helical CT results were false-negative in four (two pulmonary embolisms were angiographically revealed at the time of the initial evaluation and two recurrences of pulmonary embolism were diagnosed during the 3-month follow-up examination) of 256 patients without pulmonary embolism on the initial helical CT.


Discussion
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Abstract
Introduction
Subjects and Methods
Results
Discussion
References
 
The prevalence of pulmonary embolism in our study was 29% (104 pulmonary embolisms diagnosed on helical CT scans; four false-negative helical CT scans), which is in the range of that previously described in the literature. Among the 104 patients with positive findings on helical CT, 75 had central thrombi. In 29 patients, helical CT depicted endoluminal clots located in subsegmental and/or segmental pulmonary arteries. Six of these 29 patients (2% of the study group) had isolated subsegmental clots, mainly observed in the lower lung zones. This diagnosis was angiographically confirmed in two patients and clinically confirmed in four in whom a rapid clinical improvement after the initiation of anticoagulation therapy was observed.

Helical CT revealed negative findings down to the subsegmental level in 217 patients and inconclusive findings in 39. In the latter group, CT scans were of technically limited quality, enabling the interpreters to exclude central pulmonary embolism but not peripheral thrombi. Ten examinations (3%) were technical failures, precluding any confident depiction of acute pulmonary embolism even at the level of the central pulmonary arteries. This proportion of technical failures is similar to that (2-4%) previously reported in the literature. The failures were variably related to suboptimal enhancement, poor signal-to-noise ratios, and/or marked motion artifacts [1,2,3]. Among patients with inconclusive or negative findings on helical CT, alternative diagnoses were made by the clinicians in 165 patients on the basis of specific diagnostic clues and/or the resolution of clinical symptoms after treatment with specific medication. Among these patients, helical CT provided diagnostic information that helped explain the clinical presentation in 107 cases: namely, 30% of the study group and 65% of the patients with negative of inconclusive findings on CT. Our results are in agreement with those of three studies that have investigated the role of CT as a provider of alternative diagnoses [3,4,5]. In our study, the results of these patients' clinical follow-up examinations would have helped us classify their helical CT scans as those with true-negative findings.

This study reflects our experience with helical CT for the diagnosis of pulmonary embolism. The study has one major limitation: the absence of a systematic comparison with another imaging technique. The high percentage of patients with poor respiratory reserve explains why this investigation was not included as a first-line diagnostic test.

The second limitation of our study was the absence of a systematic search for deep vein thrombosis because of local equipment limitations at the time of the initiation of this study, a situation that underlines the influence of local equipment availability on the treatment of pulmonary embolism. Moreover, pulmonary angiography was indicated by the clinicians in only 27 (7.5%) of 360 patients examined with helical CT. This low rate confirms the well-known reluctance of clinicians to use the gold standard of acute pulmonary embolism. In the absence of systematic pulmonary angiographic confirmation, analysis of the outcome was of crucial importance in patients with negative or inconclusive findings on helical CT. Among these patients, the absence of anticoagulant treatment was associated with a low incidence of later pulmonary embolism (2/71; 2.8%) diagnosed during the 3-month follow-up studies that involved patients clinically suspected of having acute pulmonary embolism but without thrombi on pulmonary angiography [6,7,8,9,10,11]. In the final analysis of the false-negative rate of helical CT, deep vein thrombosis was found in 14 of 217 patients in whom helical CT scans revealed negative findings and in four of 39 patients with inconclusive findings on CT. Considering that asymptomatic pulmonary embolism may be present in up to 50% of patients with deep vein thrombosis [12], one may theoretically hypothesize that nine of these 18 patients had pulmonary embolisms overlooked on helical CT scans that were fortuitously detected via lower extremity Doppler sonography. Therefore, this interpretation would increase the possible false-negative rate of helical CT in our study from four (1.6%) of 256 patients to 13 (5%) of 256 patients. Despite different levels of expertise between the two interpreters, an excellent interobserver agreement was observed in the retrospective interpretation of the cases (98%), suggesting a direct influence of a thin collimation in the analysis of the pulmonary artery bed.

Our study illustrates our experience with thin-collimation helical CT in the diagnostic workup of patients with pulmonary embolism. Thin-collimation helical CT images the population suspected of pulmonary embolism with better spatial resolution, subsequently rendering the peripheral pulmonary artery bed accessible to evaluation with helical CT angiography.


References
Top
Abstract
Introduction
Subjects and Methods
Results
Discussion
References
 

  1. Remy-Jardin M, Remy J, Deschildre F, et al. Diagnosis of acute pulmonary embolism with helical CT: comparison with pulmonary angiography and scintigraphy. Radiology 1996;200:699 -706[Abstract/Free Full Text]
  2. Mayo JR, Remy-Jardin M, Muller NL, et al. Pulmonary embolism: prospective comparison of helical CT and ventilation-perfusion scintigraphy. Radiology 1997;205:447 -452[Abstract/Free Full Text]
  3. van Rossum AB, Pattynama, PMT, Mallens WMC, Hermans J, Heijerman HGM. Can helical CT replace scintigraphy in the diagnostic process in suspected pulmonary embolism? A retrolective-prolective cohort study focusing on total diagnostic yield. Eur Radiol 1998;8:90 -96[Medline]
  4. Ferretti GR, Bosson JL, Buffaz PD, et al. Acute pulmonary embolism: role of helical CT in 164 patients with intermediate probability at ventilation-perfusion scintigraphy and normal results at duplex US of the legs. Radiology 1997;205:453 -458[Abstract/Free Full Text]
  5. Kim KI, Muller NL, Mayo JR. Clinically suspected pulmonary embolism: utility of helical CT. Radiology 1999;210:693 -697[Abstract/Free Full Text]
  6. Hull RD, Raskob GE, Ginsberg JS, et al. A noninvasive strategy for the treatment of patients with suspected pulmonary embolism. Arch Intern Med 1994;154:289 -297[Abstract]
  7. Stein PD, Athanasoulis C, Alavi A, et al. Complications and validity of pulmonary angiography in acute pulmonary embolism. Circulation 1992;85:462 -468[Abstract/Free Full Text]
  8. Henry JW, Relyea B, Stein PD. Continuing risk of thromboemboli among patients with normal pulmonary angiograms. Chest 1995;107:1375 -1378[Abstract/Free Full Text]
  9. Hull RD, Hirsch J, Carter CT, et al. Pulmonary angiography, ventilation lung scanning, and venography for clinically suspected pulmonary embolism with abnormal perfusion lung scan. Ann Intern Med 1983;98:891 -899
  10. Novelline RA, Baltarowich OH, Athanasoulis CA, Waltman AC, Greenfield AJ, McKusick KA. The clinical course of patients with suspected pulmonary embolism and a negative pulmonary arteriogram. Radiology 1978;126:561 -567[Abstract]
  11. Cheely R, McCartney WH, Perry JR, et al. The role of noninvasive tests versus pulmonary angiography in the diagnosis of pulmonary embolism. Am J Med 1981;70:17 -22[Medline]
  12. Browse NL, Thomas ML. Source of non-lethal pulmonary emboli. Lancet 1974;1:258 -259[Medline]

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M. J.L. van Strijen, W. de Monye, J. Schiereck, G. J. Kieft, M. H. Prins, M. V. Huisman, P. M.T. Pattynama, and for the Advances in New Technologies Evaluating th
Single-Detector Helical Computed Tomography as the Primary Diagnostic Test in Suspected Pulmonary Embolism: A Multicenter Clinical Management Study of 510 Patients
Ann Intern Med, February 18, 2003; 138(4): 307 - 314.
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RadiologyHome page
I. Tillie-Leblond, I. Mastora, F. Radenne, S. Paillard, A.-B. Tonnel, J. Remy, and M. Remy-Jardin
Risk of Pulmonary Embolism after a Negative Spiral CT Angiogram in Patients with Pulmonary Disease: 1-year Clinical Follow-up Study
Radiology, May 1, 2002; 223(2): 461 - 467.
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Arch SurgHome page
G. C. Velmahos, P. Vassiliu, A. Wilcox, S. E. Hanks, A. Salim, D. Harrel, S. Palmer, and D. Demetriades
Spiral Computed Tomography for the Diagnosis of Pulmonary Embolism in Critically Ill Surgical Patients: A Comparison With Pulmonary Angiography
Arch Surg, May 1, 2001; 136(5): 505 - 510.
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RadiologyHome page
V. Raptopoulos and P. M. Boiselle
Multi-Detector Row Spiral CT Pulmonary Angiography: Comparison with Single-Detector Row Spiral CT
Radiology, December 1, 2001; 221(3): 606 - 613.
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