Veilig gebruik van contrastmiddelen

Initiatief: NVvR Aantal modules: 54

Preventie van contrastmiddel-geïnduceerde encefalopathie (CIE)

Uitgangsvraag

Wat zijn strategieën om contrastmiddel-geïnduceerde encefalopathie (CIE) te voorkomen?

Aanbeveling

Zorgmedewerkers zouden alert moeten zijn op het voorkomen van contrastmiddel-geïnduceerde encefalopathie (CIE) na toediening van een jodiumhoudend contrastmiddel (CM).

 

Adequate preventiestrategieën zijn niet in detail onderzocht. Het algemene advies voor de klinische praktijk:

  1. Minimaliseer de hoeveelheid toegediend jodiumhoudend CM zoveel mogelijk tijdens endovasculaire interventies
  2. Overweeg om patiënten met een ernstige verminderde nierfunctie (eGFR <30 ml/min/1.73m2) te hydrateren voordat jodiumhoudend CM wordt toegediend (zie protocol in Hoofdstuk 2. PC-AKI).
  3. Monitor patiënten de eerste 6 uur na endovasculaire interventies voor neurologische symptomen en consulteer laagdrempelig een neuroloog bij ontstaan van neurologische symptomen.
  4. Behandel, afhankelijk van de klinische symptomen van CIE, met anti-epileptische medicatie, corticosteroïden, intraveneuze hydratatie en/of mannitol.

Overwegingen

Contrast-induced encephalopathy is a complication of iodine-based contrast media (ICM) affecting the central nervous system. Usually, CIE is associated with intra-arterial administration of ICM during cardiac catheterization (Spina, 2017) or neuro-interventional procedures (Quintas-Neves, 2020), however, it can also occur after intravenous administration (Hinsenveld, 2017; Law, 2012). It can be challenging to distinguish CIE from thromboembolic stroke after endovascular procedures, of which the latter is a far more common complication. Patients may therefore be misdiagnosed and not adequately treated.

 

Symptoms arise within 24h after administration of ICM and include an altered mental status, focal neurological deficits, seizures, aphasia, and transient cortical blindness (Allison, 2021; Chu, 2020; Dunkley, 2021). It has been hypothesized that ICM disrupts the blood-brain barrier due to its hyperosmolarity, resulting in oedema and neurologic dysfunction (Chu, 2020; Dunkley, 2021; Matsubara, 2017; Kariyanna, 2020). Diagnosis is often a combination of both clinical and radiologic findings. Imaging typically shows cortical and subcortical contrast enhancement on CT and vasogenic oedema on MRI. Dual Energy CT can differentiate haemorrhage from contrast staining (Chu, 2020).

 

Risk factors include haemodialysis, hypertension, previous stroke, diabetes mellites, kidney disease, large volumes of ICM and previous adverse reactions (Allison, 2021; Matsubara, 2017). Renal dysfunction impairs clearance of contrast medium, and may result in more severe CIE, while previous stroke may already have disrupted blood-brain barriers (Chu, 2020; Matsubara, 2017; Zhang, 2020).

 

In most cases of CIE, spontaneously resolution of symptoms has been reported in several days with supportive care, although patients with permanent symptoms have also been described (Leong, 2012; Niimi, 2008; Shinoda, 2004; Zhao, 2019). Median time to recovery was reported to be around 30 hours (Kocabay, 2014).

 

The systematic research did not identify any comparative studies, but some potential preventative strategies have been proposed in the literature. Some advice to use low- osmolar ICM instead of iso- or high osmolar ICM, but in the recent years CIE has still been observed with low osmolar ICM and no comparative case-control studies have been performed (Kariyanna, 2020; Quintas-Neves, 2020, Spina, 2020). It has been reported that in most patients with CIE more than 100 ml ICM was administered. Limiting the amount of ICM administration or diluting ICM could be beneficial (Kariyanna, 2020).

 

One of the risk factors for developing CIE is renal dysfunction (Chu, 2020; Matsubara, 2017). It has been advocated that haemodialysis in patients with renal dysfunction might be beneficial in case of CIE, but no comparative studies have been performed (Matsubara, 2017). In the general population good hydration is generally advised around ICM administration (see protocol in Chapter 2. PC-AKI), although it is uncertain if this can avoid CIE. Another risk factor is hypertension. Hypertension itself can also induce a hypertensive encephalopathy. Whether lowering blood pressure before ICM administration decreases the risk of CIE is unknown.

 

In case of CIE, corticosteroid treatment has been advocated (Allison, 2021). Corticosteroid treatment may be used as preventative treatment in patients who previously have developed CIE or as a treatment to resolve the neurological symptoms during CIE. Animal studies showed that premedication with low molecular weight dextran and corticosteroids reduced the neurotoxic effects of contrast media, due to prevention of blood cell aggregation and decreased osmotic permeability of the blood brain barrier (Kariyanna, 2020). However, no studies in humans exist to date to support these findings.

 

A general recommendation is to closely observe patients directly after endovascular interventions, as most cases of CIE occur within the first few hours after intervention (Kocabay, 2014).

 

Recommendations

 

No comparative studies were identified to provide evidence-based strategies to avoid CIE. The recommendations below are based on expert opinions.

Health care providers should be aware of the existence of Contrast-Induced Encephalopathy (CIE) following iodine-based contrast media administration.

 

Adequate prevention strategies have not been investigated in detail. General advice for clinical practice:

  1. Minimize the amount of iodine-based contrast media as much as possible during endovascular interventions.
  2. Consider to hydrate patients with severe renal dysfunction (eGFR <30 ml/min/1.73m2) receiving iodine-based contrast media (see protocol in Chapter 2. PC-AKI).
  3. Closely monitor patients the first six hours after endovascular interventions for neurological symptoms and consult a neurologist immediately in case of neurological symptoms.
  4. Depending on the clinical symptoms of contrast-induced encephalopathy, treatment with antiepileptic drugs, corticosteroids, intravenous hydration, and/or mannitol may be recommended.

Onderbouwing

Contrast-induced encephalopathy (CIE) is a rare complication of the use of iodine-based contrast media (ICM), affecting the central nervous system. It has been associated with the administration of large volumes of ICM during endovascular interventions. This module aims to report on the optimal management of this complication as well as on strategies to prevent CIE.

No studies were included in the analysis of the literature. Therefore, no systematic literature analysis could be performed.

A systematic review of the literature was performed to answer the following question: Which strategies are effective for prevention of Contrast-Induced Encephalopathy (CIE)?

 

P (Patients): Adult (>18 years) patients, with an indication for examination with intravenous or ICM administration.

I (Intervention): Prevention strategy - ICM administration with one type or volume of contrast medium.

C (Comparison): No prevention strategy (care as usual) - ICM administration with another type or volume of ICM.

O (Outcome): Contrast-induced encephalopathy, severity of CIE, neurotoxicity.

 

Relevant outcome measures

The guideline development group considered contrast-induced encephalopathy as a critical outcome measure for decision making; and severity of CIE, neurotoxicity as important outcome measures for decision making.

 

The working group defined the outcome measure contrast induced encephalopathy as follows: a complication of intravenous or intra-arterial contrast administration resulting in a clinical deterioration, not caused by stroke, seizures, and other metabolic abnormalities, with oedematous changes on brain imaging, usually accompanied with contrast staining (Chu, 2020; Quintas-Neves, 2020).

 

Search and select (Methods)

The databases Medline (via OVID) and Embase (via Embase.com) were searched with relevant search terms until July 20th, 2021. The detailed search strategy is depicted under the tab Methods. The systematic literature search resulted in 419 hits. Studies were selected based on the following criteria: the description of contrast induced encephalopathy or neurotoxicity after administration of contrast media and the comparison of one preventive strategy to another strategy. Nineteen studies were initially selected based on title and abstract screening. After reading the full text, no studies were included.

 

Results

No studies were included in the analysis of the literature. Therefore, no systematic literature analysis could be performed.

  1. Allison C, Sharma V, Park J, Schirmer CM, Zand R. Contrast-Induced Encephalopathy after Cerebral Angiogram: A Case Series and Review of Literature. Case Rep Neurol. 2021; 13(2): 405-413.
  2. Chu YT, Lee KP, Chen CH, Sung PS, Lin YH, Lee CW, Tsai LK, Tang SC, Jeng JS. Contrast-induced encephalopathy after endovascular thrombectomy for acute ischemic stroke. Stroke. 2020; 51(12): 3756-3759.
  3. Dunkley JC, Patel KH, Doodnauth AV, Kariyanna PT, Valery E, McFarlane SI. Contrast-induced encephalopathy post cardiac catheterization, a rare mimicry of acute stroke - case presentation and review of the literature. Am J Med Case Rep. 2021; 9(5): 291-294.
  4. Hinsenveld WH, Vos EM, Blom RJ, Langezaal LCM, Schonewille WJ. Uw diagnose. TNN Neuro- imaging. 2017; 118. 118-121.
  5. Kariyanna PT, Aurora L, Jayarangaiah A, Das S, Gonzalez JC, Hegde S, McFarlane IM. Neurotoxicity associated with radiological contrast agents used during coronary angiography: a systematic review. Am J Med Case Rep. 2020; 8(2): 60-66.
  6. Kocabay G, Karabay CY, Kalayci A, Akgun T, Guler A, Oduncu V, Tanboga IH, Izgi A, Kirma C. Contrast-induced neurotoxicity after coronary angiography. Herz. 2014; 39(4): 522-
    527.
  7. Law S, Panichpisal K, Demede M, et al. Contrast-induced neurotoxicity following cardiac catheterization. Case Rep Med. 2012; 2012: 267860.
  8. Leong S, Fanning NF. Persistent neurological deficit from iodinated contrast encephalopathy following intracranial aneurysm coiling. A case report and review of the literature.
    Interv Neuroradiol. 2012; 18(1): 33-41.
  9. Matsubara N, Izumi T, Miyachi S, Ota K, Wakabayashi T. Contrast-induced encephalopathy following embolization of intracranial aneurysms in hemodialysis patients. Neurol Med Chir (Tokyo). 2017; 57(12): 641-648.
  10. Niimi Y, Kupersmith MJ, Ahmad S, Song J, Berenstein A. Cortical blindness, transient and otherwise, associated with detachable coil embolization of intracranial aneurysms. AJNR Am J Neuroradiol. 2008; 29(3): 603-607.
  11. Quintas-Neves M, Araújo JM, Xavier SA, Amorim JM, Cruz E Silva V, Pinho J. Contrast-induced neurotoxicity related to neurological endovascular procedures: a systematic review.
    Acta Neurol Belg. 2020; 120(6): 1419-1424.
  12. Shinoda J, Ajimi Y, Yamada M, Onozuka S. Cortical blindness during coil embolization of an unruptured intracranial aneurysm--case report. Neurol Med Chir (Tokyo). 2004; 44(8): 416-419.
  13. Spina R, Simon N, Markus R, Muller DW, Kathir K. Contrast-induced encephalopathy following cardiac catheterization. Catheter Cardiovasc Interv. 2017; 90(2): 257-268.
  14. Zhang G, Wang H, Zhao L, Li T, Sun M, Zhang Y, Hu H, Teng G, Chen J, Jian Y, Liu J. Contrast- induced encephalopathy resulting from use of ioversol and iopromide. Clin Neuropharmacol. 2020; 43(1): 15-19.
  15. Zhao, W., Zhang, J., Song, Y. et al. Irreversible fatal contrast-induced encephalopathy: a case report. BMC Neurol. 2019; 19: 46.

Autorisatiedatum en geldigheid

Laatst beoordeeld  : 28-11-2022

Laatst geautoriseerd  : 28-11-2022

Geplande herbeoordeling  : 01-12-2023

Validity

The Radiological Society of the Netherlands (NVvR) will determine around 2027 if this guideline (per module) is still valid and applicable. If necessary, the scientific societies will form a new guideline group to revise the guideline. The validity of a guideline can be shorter than 5 years, if new scientific or healthcare structure developments arise, that could be a reason to commence revisions. The Radiological Society of the Netherlands is the owner of this guideline and thus primarily responsible for the actuality of the guideline. Other scientific societies that have participated in the guideline development share the responsibility to inform the primarily responsible scientific society about relevant developments in their field.

Initiatief en autorisatie

Initiatief:
  • Nederlandse Vereniging voor Radiologie
Geautoriseerd door:
  • Nederlandse Internisten Vereniging
  • Nederlandse Vereniging van Maag-Darm-Leverartsen
  • Nederlandse Vereniging voor Cardiologie
  • Nederlandse Vereniging voor Heelkunde
  • Nederlandse Vereniging voor Neurologie
  • Nederlandse Vereniging voor Obstetrie en Gynaecologie
  • Nederlandse Vereniging voor Radiologie
  • Nederlandse Vereniging voor Klinische Chemie en Laboratoriumgeneeskunde
  • Patiëntenfederatie Nederland
  • Nederlandse Vereniging voor Allergologie en Klinische Immunologie
  • Nederlandse Vereniging voor Endocrinologie
  • Nederlandse Vereniging voor Vaatchirurgie

Algemene gegevens

General Information

The Kennisinstituut van de Federatie Medisch Specialisten (www.kennisinstituut.nl) assisted the guideline development group. The guideline was financed by Stichting Kwaliteitsgelden Medisch Specialisten (SKMS) which is a quality fund for medical specialists in The Netherlands.

Samenstelling werkgroep

Guideline development group (GDG)

A multidisciplinary guideline development group (GDG) was formed for the development of the guideline in 2020. The GDG consisted of representatives from all relevant medical specialization fields which were using intravascular contrast administration in their field.

 

All GDG members have been officially delegated for participation in the GDG by their scientific societies. The GDG has developed a guideline in the period from June 2020 until November 2022. The GDG is responsible for the complete text of this guideline.

 

Guideline development group

  • Dekkers I.A. (Ilona), clinical epidemiologist and radiologist, Leiden University Medical Center, Leiden
  • Geenen R.W.F. (Remy), radiologist, Noordwest Ziekenhuisgroep, Alkmaar
  • Kerstens M.N. (Michiel), internist-endocrinologist, University Medical Centre Groningen
  • Krabbe J.G. (Hans), clinical chemist-endocrinologist, Medisch Spectrum Twente, Enschede
  • Rossius M.J.P. (Mariska), radiologist, Erasmus Medical Centre, Rotterdam
  • Uyttenboogaart M. (Maarten), neurologist and neuro-interventionalist, University Medical Centre Groningen
  • van de Luijtgaarden K.M. (Koen), vascular surgeon, Maasstad Ziekenhuis, Rotterdam
  • van der Molen A.J. (Aart), chair guideline development group, radiologist, Leiden University Medical Center, Leiden
  • van der Wolk S.L. (Sabine), gynaecologist-obstetrician, Haga Ziekenhuis, Den Haag
  • van de Ven A.A.J.M. (Annick), internist-allergologist-immunologist, University Medical Centre Groningen (until 1.7.2022)
  • van der Houwen, T.B. (Tim), internist-allergologist-immunologist, Amsterdam University Medical Center (from 1.7.2022)

Invited experts

  • van Maaren M.S. (Maurits), internist-allergologist-immunologist, Erasmus MC, Rotterdam

Belangenverklaringen

Conflicts of interest

The GDG members have provided written statements about (financially supported) relations with commercial companies, organisations or institutions that were related to the subject matter of the guideline. Furthermore, inquiries have been made regarding personal financial interests, interests due to personal relationships, interests related to reputation management, interest related to externally financed research and interests related to knowledge valorisation. The statements on conflict of interest can be requested from the administrative office of Kennisinstituut van de Federatie Medisch Specialisten (secretariaat@kennisinstituut.nl) and were summarised below.

 

Last name

Function

Other positions

Personal financial

interests

Personal relations

Reputation management

Externally financed

research

Knowledge valorisation

Other interests

Signed

Actions

Dekkers IA

Radiologist, LUMC

Clinical Epidemiologist

 

Member of contrast media safety committee, European Society of Urogenital Radiology (no payment)

 

Member, Gadolinium Research and Education Committee, European Society of Magnetic Resonance in Medicine, and Biology (no

payment)

No

No

No

No

No

Received consultancy fees from Guerbet, 2019-

2022

July 24th, 2020, Reaffirmed October 12th, 2022

No restrictions: received in part 3 of the guideline speaker fees, but this guideline does not mention specific medication, not of working mechanism, nor of side effects.

Geenen RWF

Radiologist, Noordwest ziekenhuisgroep

/Medisch specialisten

Noordwest

Member of contrast media safety

committee, European

Society of Urogenital

Radiology (no payment)

No

No

No

No

No

No

April 11th, 2020, Reaffirmed October 12th,

2022

No restrictions

Houwen T, van der

Internist - Immunologist - Allergologist, Amsterdam UMC, also seconded allergologist in Huid Medisch

Centrum

None

None

None

None

None

None

None

July 11th, 2022 Reaffirmed October 12th, 2022

No restrictions

Kerstens MN

Internist- endocrinologist, UMCG

Chairman Bijniernet (no payment)

No

No

No

No

No

No

July 1st, 2020, reaffirmed October 25th,

2022

No restrictions

Krabbe JG

Clinical chemist, Medisch Spectrum Twente

No

No

No

No

No

No

No

September 1st, 2020,

Reaffirmed October 13th, 2022

No restrictions

Luijtgaarden KM, van de

Vascular surgeon, Maasland Ziekenhuis

No

No

No

No

No

No

No

August 1st, 2020,

reaffirmed October 26th, 2022

No restrictions

Molen AJ, van der

Radiologist LUMC

Member of contrast media safety committee, European Society of Urogenital Radiology (no

payment)

 

Member, Gadolinium Research and Education Committee, European Society of Magnetic Resonance in Medicine, and Biology (no

payment)

No

No

No

No

No

Received consultancy fees from Guerbet, 2019-

2022

July, 24th, 2020 Reaffirmed October 12th, 2022

No restrictions: received in part 3 of the guideline speaker fees, but this guideline does not mention

Specific medication, not

of working mechanism, nor of side effects.

Rossius MJP

Radiologist Erasmus Medical Centre

Medical coordinator (no payment)

No

No

No

No

No

No

April 7th, 2020, Reaffirmed October 13th,

2022

No restrictions

Uyttenboogaart M

Neurologist and neuro- interventionalist UMCG

Advisor International Federation of Orthopaedic Manipulative Physical Therapist / Nederlandse Vereniging Manuele Therapie

No

No

Subsidy Hart Stichting for CONTRAST

(Consortium of New Treatments in Acute Stroke): WP8 Stroke logistics and Epidemiology: financing of 2 PhD students by the Hart Stichting / PPS

Allowance

Work package leader CONTRAST

(Consortium of New Treatments in Acute Stroke): WP8 Stroke logistics and Epidemiology

No

No

June 30th, 2020, reaffirmed October 26th, 2022

No restrictions: the CONTRAST

consortium wp8 is only about organisation and treatment of stroke.

Stroke is not in this guideline.

Ven AAJM, van de

Internist- allergologist- immunologist, UMCG

Education and research related to work as internist-

allergist

No

No

No

No

No

No

April 7th, 2020, Reaffirmed October 19th, 2022

No restrictions

Wolk S, van der

Gynaecologist- obstetrician, Haga Ziekenhuis

No

No

No

No

No

No

No

June 30th, 2021, reaffirmed October 25th,

2022

No restrictions

Inbreng patiëntenperspectief

Input of patient’s perspective

The guideline does not address a specific adult patient group, but a diverse set of diagnoses. Therefore, it was decided to invite a broad spectrum of patient organisations for the stakeholder consultation. The stakeholder consultation was performed at the beginning of the process for feedbacking on the framework of subjects and clinical questions addressed in the guideline, and during the commentary phase to provide feedback on the concept guideline. The list of organisations which were invited for the stakeholder consultation can be requested from the Kennisinstituut van de Federatie Medisch Specialisten (secretariaat@kennisinstituut.nl). In addition, patient information on safe use of contrast media in pregnancy and lactation was developed for Thuisarts.nl, a platform to inform patients about health and disease.

Implementatie

Implementation

During different phases of guideline development, implementation and practical enforceability of the guideline were considered. The factors that could facilitate or hinder the introduction of the guideline in clinical practice have been explicitly considered. The implementation plan can be found in the ‘Appendices to modules’. Furthermore, quality indicators were developed to enhance the implementation of the guideline. The indicators can also be found in the ‘Appendices to modules’.

Werkwijze

Methodology

AGREE

This guideline has been developed conforming to the requirements of the report of Guidelines for Medical Specialists 2.0 by the advisory committee of the Quality Counsel (www.kwaliteitskoepel.nl). This report is based on the AGREE II instrument (Appraisal of Guidelines for Research & Evaluation II) (www.agreetrust.org), a broadly accepted instrument in the international community and based on the national quality standards for guidelines: “Guidelines for guidelines” (www.zorginstituutnederland.nl).

 

Identification of subject matter

During the initial phase of the guideline development, the GDG identified the relevant subject matter for the guideline. The framework is consisted of both new matters, which were not yet addressed in part 1 and 2 of the guideline, and an update of matters that were subject to modification (for example in case of new published literature). Furthermore, a stakeholder consultation was performed, where input on the framework was requested.

 

Clinical questions and outcomes

The outcome of the stakeholder consultation was discussed with the GDG, after which definitive clinical questions were formulated. Subsequently, the GDG formulated relevant outcome measures (both beneficial and harmful effects). The GDG rated the outcome measures as critical, important and of limited importance (GRADE method). Furthermore, where applicable, the GDG defined relevant clinical differences.

 

Search and select

For clinical questions, specific search strategies were formulated, and scientific articles published in several electronic databases were searched. First, the studies that potentially had the highest quality of research were reviewed. The GDG selected literature in pairs (independently of each other) based on the title and abstract. A second selection was performed by the methodological advisor based on full text. The databases used, selection criteria and number of included articles can be found in the modules, the search strategy in the appendix.

 

Quality assessment of individual studies

Individual studies were systematically assessed, based on methodological quality criteria that were determined prior to the search. For systematic reviews, a combination of the AMSTAR checklist and PRISMA checklist was used. For RCTs the Cochrane risk of bias tool and suggestions by the CLARITY Group at McMaster University were used, and for cohort studies/observational studies the risk of bias tool by the CLARITY Group at McMaster University was used. The risk of bias tables can be found in the separate document Appendices to modules.

 

Summary of literature

The relevant research findings of all selected articles were shown in evidence tables. The evidence tables can be found in the separate document Appendices to modules. The most important findings in literature were described in literature summaries. When there were enough similarities between studies, the study data were pooled.

 

Grading quality of evidence and strength of recommendations

The strength of the conclusions of the included studies was determined using the GRADE- method. GRADE stands for Grading Recommendations Assessment, Development and Evaluation (see http://www.gradeworkinggroup.org) (Atkins, 2004). GRADE defines four levels for the quality of scientific evidence: high, moderate, low, or very low. These levels provide information about the certainty level of the literature conclusions (http://www.guidelinedevelopment.org/handbook).

 

The evidence was summarized in the literature analysis, followed by one or more conclusions, drawn from the body of evidence. The level of evidence for the conclusions can be found above the conclusions. Aspects such as expertise of GDG members, local expertise, patient preferences, costs, availability of facilities and organisation of healthcare aspects are important to consider when formulating a recommendation. These aspects are discussed in the paragraph justifications. The recommendations provide an answer to the clinical question or help to increase awareness and were based on the available scientific evidence and the most relevant justifications.

 

Appendices

Internal (meant for use by scientific society or its members) quality indicators were developed with the guideline and can be found in the separate document Appendices to modules. In most cases, indicators were not applicable. For most questions, additional scientific research on the subject is warranted. Therefore, the GDG formulated knowledge gaps to aid in future research, which can be found in the separate document Appendices to modules.

 

Commentary and authorisation phase

The concept guideline was subjected to commentaries by the involved scientific societies. The list of parties that participated in the commentary phase can be requested from the Kennisinstituut van de Federatie Medisch Specialisten (secretariaat@kennisinstituut.nl). The commentaries were collected and discussed with the GDG. The feedback was used to improve the guideline; afterwards the GDG made the guideline definitive. The final version of the guideline was offered to the involved scientific societies for authorization and was authorized.

 

Literature

Brouwers MC, Kho ME, Browman GP, et al. AGREE Next Steps Consortium. AGREE II: advancing guideline development, reporting and evaluation in health care. CMAJ. 2010; 182(18): E839-E842.

Medisch Specialistische Richtlijnen 2.0. Adviescommissie Richtlijnen van de Raad Kwaliteit, 2012. Available at: [URL].

Schünemann H, Brożek J, Guyatt G, et al. GRADE handbook for grading quality of evidence and strength of recommendations. Updated October 2013. The GRADE Working Group, 2013. Available at: [URL].

Schünemann HJ, Oxman AD, Brozek J, et al. Grading quality of evidence and strength of recommendations for diagnostic tests and strategies. BMJ. 2008;336(7653):1106- 1110. Erratum published in: BMJ 2008;336(7654).

Ontwikkeling van Medisch Specialistische Richtlijnen: stappenplan. Kennisinstituut van Medisch Specialisten, 2020.

Volgende:
Preventie van jodium-geïnduceerde hyperthyroïdie (IIHT) na het gebruik van jodiumhoudend contrastmiddel