| Literature DB >> 27757521 |
S A Taylor1, F Avni2, C G Cronin3, C Hoeffel4, S H Kim5, A Laghi6, M Napolitano7, P Petit8, J Rimola9, D J Tolan10, M R Torkzad11, M Zappa12, G Bhatnagar11, C A J Puylaert13, J Stoker13.
Abstract
OBJECTIVES: To develop guidelines describing a standardised approach to patient preparation and acquisition protocols for magnetic resonance imaging (MRI), computed tomography (CT) and ultrasound (US) of the small bowel and colon, with an emphasis on imaging inflammatory bowel disease.Entities:
Keywords: Computed tomography; Crohn disease; Magnetic resonance imaging; Small bowel; Ultrasound
Mesh:
Year: 2016 PMID: 27757521 PMCID: PMC5408044 DOI: 10.1007/s00330-016-4615-9
Source DB: PubMed Journal: Eur Radiol ISSN: 0938-7994 Impact factor: 5.315
Fig. 1Summary of consensus process
Literature search strategy (from Puylaert et al. [4])
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| Time period: January 1983–December 2015 |
|---|---|
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| 1 | Crohn’s disease |
| 2 | Crohn [tiab] |
| 3 | Inflammatory bowel disease |
| 4 | 1 OR 2 OR 3 |
| 5 | Computed tomography |
| 6 | CT [tiab] |
| 7 | MRI |
| 8 | “Magnetic resonance” [All fields] OR (“magnetic” [All fields] AND “resonance” [All fields]) |
| 9 | Ultrasound |
| 10 | 5 OR 6 OR 7 OR 8 OR 9 |
| 11 | 4 AND 10 |
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| |
| 1 | Crohn’s disease.ab,ti,sh,kw |
| 2 | Inflammatory bowel disease.ab,ti,sh,kw |
| 3 | 1 OR 2 |
| 4 | Computer Assisted Tomography.ab,ti,sh,kw |
| 5 | Exp Computer Assisted Tomography/ |
| 6 | Nuclear magnetic resonance imaging.ab,ti,sh,kw |
| 7 | Exp Nuclear magnetic resonance imaging/ |
| 8 | Echography.ab,ti,sh,kw |
| 9 | Exp echography/ |
| 10 | 4 OR 5 OR 6 OR 7 OR 8 OR 9 |
| 11 | 3 AND 10 |
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| |
| 1 | Crohn disease [Mesh] |
| 2 | Inflammatory bowel disease [Mesh] |
| 3 | 1 OR 2 |
| 4 | Diagnostic techniques and procedures [Mesh] |
| 5 | 3 AND 4 |
Current clinical practice of expert committee members (n = 13)
| Panel members performing routinely | Mean annual case load | |
|---|---|---|
| MRE | 13 | 313 |
| MR enteroclysis | 4 | 14 |
| CTE | 8 | 70 |
| CT enteroclysis | 4 | 23 |
| US | 5 | 110 |
MRE MR enterography, CTE CT enterography, US enteric ultrasound
Statements for which consensus could not be reached after attempted modification
| Statement |
| • It is recommended that the minimal volume of oral contrast for dedicated MRE/MR enteroclysis or CTE/CT enteroclysis is 500 ml ( |
| • Splitting the oral contrast into two loads and scanning after ingestion of each to improve small bowel distension is not recommended |
| • The optimal field strength for MRE/MR enteroclysis is 1.5 T |
| • It is recommended to split-the dose of spasmolytics before T2W sequences and before contrast-enhanced T1W sequences |
| • It is recommended to routinely use small bowel motility sequences during MRE |
| • It is recommended to routinely use an axial diffusion-weighted sequence during MRE/MR enteroclysis |
| • It is recommended that if a spasmolytic is used, and hyoscine butylbromide is unavailable/ contraindicated, a second-line agent is employed during CTE/CT enteroclysis |
| • It is recommended to administer a spasmolytic before MRE in the paediatric population |
| • It is recommended that if CT scanning is used in the paediatric population, no specific preparation is usually required although administration of positive oral contrast could be considered; for example, prior to percutaneous drainage of abscesses |
Evidence strength (Oxford Centre for Evidence Based Medicine) shown in parentheses
Final list of consensus statements (achieving agreement score 4 or 5 by at least 80 % of committee members) a
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| • It is recommended that routine medications should not be stopped |
| • It is recommended that patients should not eat any solid food for 4-6 h |
| • It is recommended that patients should not drink any fluid for 4-6 h, although non-sparkling water is permissible |
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| • There is no single preferred contrast agent for MRE or CTE. Recommended agents include mannitol (with or without locust bean gum), PEG, sorbitol and lactulose amongst others |
| • The optimal volume of oral contrast is 1,000-1,500 ml |
| • It is recommended that ingestion time of oral contrast without previous major small bowel resection should be 46-60 min |
| • It is recommended that when scanning patients with a stoma, the stoma should be plugged before oral contrast ingestion |
| • It is not recommended that laxative bowel preparation is administered |
| • It is not recommended that a rectal water enema is administered before a routine examination |
| • It is recommended to administer a liquid enema or prolonged oral contrast preparation without laxative for dedicated colonic evaluation during CTE or MRE |
| • It is recommended to use water as the distension agent if a liquid rectal enema is used for dedicated colonic evaluation |
| • It is recommended that the volume of a water rectal enema is based on patient tolerance if used for dedicated colonic evaluation |
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| • There is no single preferred contrast agent for MR enteroclysis. Recommended agents include mannitol (with or without locust bean gum), PEG, sorbitol and lactulose amongst others |
| • There is no single preferred contrast agent for CT enteroclysis. Recommended agents include mannitol (with or without locust bean gum), PEG, sorbitol, lactulose and water amongst others |
| • Fluoroscopic guidance for NJ tube insertion prior to MR enteroclysis/ CT enteroclysis is mandatory |
| • It is recommended that the NJ tube for MR enteroclysis and CT enteroclysis should be 8-10 F |
| • It is recommended that contrast infusion before MR enteroclysis or CT enteroclysis should be via an automated pump |
| • It is recommended that the rate of contrast infusion before MR enteroclysis or CT enteroclysis should be between 80 and 120 ml/min |
| • MRI fluoroscopic monitoring of small bowel filling during MR enteroclysis is mandatory |
| • It is recommended that enteric contrast progression should be monitored on the MRI table during MR enteroclysis |
| • It is recommended that enteric contrast progression should be monitored on the CT table during CT enteroclysis |
| • The optimal volume of enteric contrast for MR enteroclysis or CT enteroclysis should be based on monitoring using MRI/CT |
| • It is recommended that patients can be scanned prone or supine during MRE, CTE, MR enteroclysis or CT enteroclysis |
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| • Both 1.5 and 3 T are adequate field strengths |
| • The use of phased-array coils is mandatory |
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| • It is recommended that spasmolytic agents are administered during MRE and MR enteroclysis |
| • The timing of spasmolytic agent administration should take into account the susceptibility of the applied MRI sequences to motion artefact |
| • The recommended first line spasmolytic agent is i.v. hyoscine butylbromide |
| • The recommended dose of i.v. hyoscine butylbromide is 20 mg |
| • It is recommended to use a second line spasmolytic agent if the first line agent cannot be given |
| • The recommended second line agent is i.v. glucagon |
| • The recommended dose of i.v. glucagon is 1 mg |
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| • It is recommend to use the following sequences |
| b) Axial and coronal steady state free precession gradient echo (SSFP GE) sequences without fat saturation |
| c) An axial or coronal FSE T2W sequence with fat saturation |
| d) Non-enhanced coronal T1W sequence with fat saturation followed by contrast-enhanced coronal and axial T1W sequences with fat saturation |
| e) In patients with known or suspected inflammatory bowel disease, contrast-enhanced sequences should be in the enteric (45 s) or portal venous phase (70 s) |
| f) In patients with suspected chronic GI bleeding contrast-enhanced sequences is should be in the arterial (30 s), enteric (45 s) or portal venous phase (70 s) phase |
| • It is recommended that i.v. gadolinium is pump-injected with an infusion rate of 2 ml/s and a dosage of 0.1–0.2 mmol/kg |
| • It is recommended that the maximal slice thickness for FSE T2W and SSFP GE sequences should be 5 mm |
| • It is recommend that FSE T2W sequences may be performed in either 2D or 3D, although 2D is preferred. |
| • It is recommended that the maximal slice thickness for axial and coronal T1W sequences, should be 3 mm |
| • It is recommended that T1W sequences should be performed in 3D |
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| • Optional additional sequences include an additional FSE T2W sequence with fat saturation, axial and coronal SSFP GE sequences with fat saturation, cine motility and diffusion weighted imaging |
| • It is recommended that a free breathing technique is used if diffusion-weighted sequences are performed |
| • It is recommended that diffusion-weighted sequences should include lower |
| • It is recommended that the maximal slice thickness for a diffusion-weighted sequence should be 5 mm |
| • Coronal diffusion-weighted sequences are not recommended |
| • Dynamic contrast-enhanced sequences are not mandatory, but may provide additional information in the form of quantitative measurements of contrast enhancement |
| • Magnetization transfer sequences are not recommended |
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| • It is recommended that scan coverage should include at least the small bowel and colon extended to include the perineum |
| • It is recommended that in general the total acquisition time for should be equal to or less than 30 min |
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| • MDCT with at least 64 slices is optimal |
| • MDCT with 16 slices or more is considered adequate |
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| • The use of a spasmolytic agent during CTE/CT enteroclysis is optional |
| • It is recommended that if a spasmolytic is used the first line agent is i.v. hyoscine butylbromide |
| • The recommended dose of i.v. hyoscine butylbromide is 20 mg |
| • The recommended second line agent is i.v. glucagon |
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| • It is recommended that a variable tube current is used, according to the tube voltage used and patient body habitus, but should be kept as low as possible |
| • It is recommended to use automatic exposure control |
| • It is recommended that scan coverage should include the whole abdomen and pelvis including the liver |
| • It is recommended that image-based or raw data-based iterative reconstruction is used if available |
| • The use of multiplanar reformats is mandatory |
| • It is recommended that the maximal slice thickness for displaying axial, coronal and sagittal reconstructed images should be 3 mm |
| • It is recommended that CT acquisition should be cranio-caudal |
| • It is recommended that an upper dose exposure limit is defined |
| • It is recommended that the cumulative value of radiation dose should be recorded, especially in patients affected by chronic conditions resulting in repeat CT imaging |
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| • It is recommended that either an enteric phase or portal venous phase acquisition is performed |
| • Additional acquisitions including pre-contrast, arterial, and delayed phase (6-7 min) are not recommended |
| • It is recommended that i.v. iodinated contrast should be pump injected at rate of 3-5 ml/s |
| • It is recommended that i.v. iodinated contrast iodine content is within a range of 300-370 mg/ml |
| • It is recommended that the i.v. iodinated contrast iodine dose should be varied according to the patients’ weight at 1.5 ml/kg |
| • It is recommended that the tube voltage should be within a range of 80-120 according to the patient body habitus |
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| • Arterial and portal phases acquisitions are mandatory |
| • It is recommended that i.v. iodinated contrast should be pump injected at rate of 3-5 ml/s |
| • It is recommended that the i.v. iodinated contrast iodine dose should be varied according to the patients’ weight |
| • It is recommended that the tube voltage should be within a range of 80-140 according to the patient body habitus |
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| • It is recommended that patients should be nil by mouth for solids for 4-6 h |
| • It is recommended patients should not drink any fluid for 4-6 h prior to the procedure, although water is permissible. If examination of the extra enteric organs is performed, patients should be nil by mouth as per standard protocols |
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| • It is recommended that evaluation with both low and high frequency probes is performed |
| • The optimal probe frequency for high resolution bowel imaging is 8-10 MHz |
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| • It is not recommended that laxative bowel preparation is administered |
| • It is not recommended that a rectal water enema is administered before a routine examination |
| • Use of an spasmolytic agent is not recommended |
| • It is recommended that for dedicated colonic evaluation, a standard protocol without specific modification is used |
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| • It is not recommended that laxative bowel preparation is administered |
| • The use of a spasmolytic agent is not recommended |
| • There is no single preferred contrast agent for hydosonography. Recommended agents include mannitol (with or without locust bean gum), PEG, sorbitol and lactulose amongst others |
| • It is recommended that the optimal volume of oral contrast for should exceed 500 ml |
| • It is recommended that ingestion time of oral contrast should be 45 min |
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| • It is recommended to routinely use colour Doppler |
| • The optimal Doppler flow setting is between 1 and 8 cm/s |
| • Routine use of i.v. US contrast agent is not recommended |
| • If i.v. contrast agent is given, the optimal dose of sulphur hexafluoride is 2.4-4.8 ml |
| • If i.v. contrast agent is given, the standard number of boluses of sulphur hexafluoride is 1 |
| • If i.v. contrast agent is given, the maximum dose of sulphur hexafluoride is 4.8 ml |
| • Scanning between 10 and 40 s after administration of sulphur hexafluoride i.v. contrast is mandatory |
| • Perfusion or time-intensity curves (e.g. ratio max enhancement/baseline) are not recommended |
| • It is recommended that peak enhancement after contrast injection is measured |
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| • It is recommended that formal reporting of enteric US should state whether the extra enteric organs were examined or not |
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| • It is recommended that children aged 6-9 should not eat any solid food for 2-4 h |
| • It is recommended that children aged 6-9 should not undergo fluid restriction |
| • It is recommended that children aged over 9 years should not eat any solid food for 4-6 h |
| • It is recommended that children aged over 9 years should not undergo fluid restriction |
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| • It is recommended that the optimal volume of oral contrast for MRE or CTE is 20 ml/kg with a maximum up to 25 ml/kg |
| • It is recommended that the use of a spasmolytic agent is optional |
| • The recommended first line spasmolytic agent is i.v. hyoscine butylbromide, if a spasmolytic is used |
| • The recommended dose of hyoscine butylbromide is 0.5 mg/kg i.v. |
| • The recommended second line agent is i.v. glucagon, if a spasmolytic agent is used |
| • The recommended dose of glucagon in the paediatric population is 0.5 mg (<24.9 kg) and 1 mg (>24.9 kg), given as a slow infusion with i.v. saline at an infusion rate at 1 ml/s |
| • The recommended dose of i.v. gadolinium is 0.1 mmol/kg |
| • It is recommended that the total scan duration should equal to or be less than 45 min |
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| • Use of CT scanning in children should be limited to exceptional circumstances, when US and/or MRE cannot address the clinical question |
| • It is recommended that if CT scanning is used, only a portal phase from the diaphragm to the pubic symphysis is acquired |
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| • It is recommended that children aged 1-9 should not eat any solid food for 2-4 h |
| • It is recommended that children aged 1-9 years should be nil by mouth for carbonated and milk beverages for 2-4 h. Ingestion of still water or non-carbonated fruit juice is recommended |
| • It is recommended that children aged over 9 years should not eat any solid food for 4-6 h |
| • It is recommended that children aged over 9 years should be nil by mouth for carbonated and milk beverages for 4-6 h. Ingestion of still water or non-carbonated fruit juice is recommended |
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| • Use of laxative bowel preparation is not recommended |
| • Additional colonic distension with a rectal water enema is not recommended |
| • It is recommended that for dedicated colonic evaluation, a standard protocol without specific modification is used |
| • Use of a spasmolytic agent is not recommended |
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| • The use of i.v. US contrast is not recommended |
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| • It is recommended that scan coverage should include an abdominal and pelvic examination, including the liver |
Evidence strength (Oxford Centre for Evidence Based Medicine) shown in parentheses
MRE MR enterography, CTE CT enterography, T1W T1-weighted, T2W T2-weighted
a4 = somewhat agree, 5 = strongly agree