Behandeling van acute hypersensitiviteitsreacties na CM
Uitgangsvraag
Wat is de optimale behandeling van acute hypersensitiviteitsreacties na contrastmiddel (CM)-toediening?
Aanbeveling
Voorbereiding:
- Zorg ervoor dat de medicatie (als minimum vereiste: adrenaline, salbutamol, H1-antihistaminicum (clemastine) IV en corticosteroid IV (bijvoorbeeld prednisolon)), uitrusting en protocol voor de behandeling van een acute hypersensitiviteitsreactie gereed liggen in elke kamer waar CM worden toegediend.
- Houd je aan lokale protocollen voor bereikbaarheid van een reanimatie en een spoed interventie team (SIT).
- Houd elke patiënt met een acute hypersensitiviteitsreactie na toediening van CM in een medische omgeving gedurende minstens 30 minuten na injectie van CM. Matige en ernstige reacties behoeven een langere observatietijd.
Acute behandeling, algemene principes:
- Check en stabiliseer de patiënt volgens de ABCDE-methode.
- Stop met toediening van CM en vervang infuus door een kristalloïd.
- Dyspneu of stridor: laat patiënt rechtop zitten.
- Hypotensie: houd patiënt in liggende positie, leg de benen hoger.
- Overweeg het bepalen van serum tryptase (zie aanbevelingen in module 3.5.1 In vitro testen bij patiënten met hypersensitiviteitsreacties na CM).
- Vermeld acute hypersensitiviteitsreacties in de allergieregistratie van het Elektronisch Patiënten Dossier (zie hoofdstuk Organisatie van zorg Hypersensitiviteitsreacties).
N.B: Na toediening van clemastine kan het reactievermogen van de patiënt sterk verminderd zijn. Patiënt wordt afgeraden gedurende die tijd een voertuig te besturen of een machine te bedienen. Patiënt is strafbaar en vaak niet verzekerd bij eventueel ongeluk/schade.
Ernstige reacties:
Cardiaal of respiratoir arrest:
- Start cardiopulmonale reanimatie.
- Bel het reanimatie team.
Anafylactische reactie of stridor:
- Bel het Spoed Interventie Team (SIT-team).
- Geef zuurstof 10 tot 15L/min via een non-rebreathing masker.
- Geef 0.5mg adrenaline IM in laterale bovenste deel van het dijbeen.
- Geef bolus van een kristalloïd 500ml IV in 10 minuten, herhaal indien nodig.
- Overweeg verneveling met salbutamol 5mg of budesonide 2mg voor stridor.
- Geef clemastine 2mg IV, herhaal indien nodig.
- Overweeg toevoegen corticosteroid (b.v. prednisolon 50mg IV*)
* Of equivalente dosis van een ander corticosteroïd
50 mg prednisolon is equivalent aan:
- 40 mg methylprednisolone.
- 8mg dexamethasone.
- 200mg hydrocortisone.
* Overweeg toevoegen van corticosteroïden voor preventie van geprotraheerde of bifasische anafylactische reacties als de initiële symptomen ernstig zijn.
Matig-ernstige reacties:
Overweeg om patiënt te verplaatsen naar een afdeling met faciliteiten voor het monitoren van vitale functies.
Geïsoleerd bronchospasme:
- Salbutamol 2.5 tot 5mg verneveling in zuurstof door middel van een gezichtsmasker 10 tot 15 L/min (verneveling is makkelijker om toe te dienen en meer effectief dan dosis aerosol).
- Bij milde reacties mogen astmapatiënten de eigen salbutamoldosis aerosol gebruiken.
- Indien klachten toenemen geef adrenaline 0.5mg IM en neem contact op met het spoed-interventie-team.
Geïsoleerd gezichtsoedeem zonder stridor:
- Geef zuurstof 10 tot 15L/min via een non-rebreathing masker.
- Geef clemastine 2mg IV.
- Indien oedeem ernstig is of dichtbij luchtwegen is gelokaliseerd of indien er stridor ontstaat: behandel als anafylaxie.
Geïsoleerde urticaria/diffuse erytheem:
- Geef clemastine 2mg IV.
- Indien vergezeld van hypotensie: behandel als anafylaxie.
Geïsoleerde hypotensie:
- Geef bolus van kristalloïd 500ml IV, herhaal indien nodig.
- Indien vergezeld van bradycardie, overweeg atropine 0.5mg IV.
- Indien vergezeld door andere symptomen behandel als anafylaxie.
Milde reacties
Algemeen:
- Milde reacties behoeven soms enkel geruststelling.
- Observeer vitale functies totdat symptomen voorbij zijn.
- Verwijder iv toegang niet tijdens observatie.
Overweeg:
- Voorschrijven van een niet-sederend H1-antihistaminicum, bijvoorbeeld desloratidine 5mg PO (eenmaal daags) voor milde hypersensitiviteitsreacties.
- Ondansetron 4mg iv voor persistent overgeven.
Overwegingen
As there are no comparative studies investigating the research question, the recommendations in this national guideline are based mainly on results of observational studies and reviews (for example Cohan, 1996; Bang, 2013; Morzycki, 2017; Boyd, 2017) and of the recommendations of the American College of Radiology 2018 (Manual on Contrast Media v10.3) (ACR, 2018), the European Society of Urogenital Radiology 2018 (electronic v10) (ESUR, 2018), the International Consensus On Drug Allergy 2014 (Demoly, 2014), the World Allergy Organisation (WAO) Anaphylaxis Guidelines 2011, update 2015 (Simons, 2015), the European Association for Allergy and Clinical Immunology (EAACI) Guidelines 2014 (Moraro, 2014), and adapted to the Dutch situation (Het Acute Boekje, NIV 2017).
Because of the diminished frequency of acute adverse reactions to contrast media, there are now fewer opportunities for physicians to recognize and appropriately treat such adverse reactions. Reactions vary from very mild itching to anaphylactic shock. These reactions are often unpredictable; they can happen to people who have not been exposed to contrast media in the past. A mild reaction may be self-limited but can also develop quickly into a severe reaction. When a hypersensitivity reaction to a contrast medium occurs, there may be insufficient time or opportunity to study the treatment protocols and medication doses. It is therefore important for personnel to be prepared for any adverse reaction, to have clear treatment guidelines, and to have access to a rapid response team in case of an emergency. (Segal, 2011).
Because of this diminished frequency and lack of experience in treatment, major guidelines recommend to restricting adrenaline injection in the hands of non-experienced users to intramuscular administration route only.
Risk factors
Patients with a history of previous moderate or severe acute hypersensitivity reaction to an iodine-based contrast medium or gadolinium-based or ultrasound contrast agent, asthma requiring medical treatment and atopy requiring medical treatment are at increased risk (ESUR 2018; ACR 2018).
Prevention
Use a low-osmolar or iso-osmolar non-ionic iodine-based contrast medium. In patients at risk consider an alternative test not requiring a contrast agent of similar class.
For previous contrast agent reactors: use a different contrast medium/agent, preferably after consultation with a specialist in drug allergy
The radiology department should be prepared for an acute reaction. This requires regular and optimized training of personnel. See Chapter: Organisation of healthcare.
Note:
Instead of adrenaline 1:1,000 ampules for IM administration each department may also opt for selecting the (more expensive) adrenaline 1:1,000 auto-injectors, for example EpiPen (Asch 2017).
Onderbouwing
Achtergrond
Acute hypersensitivity reactions often create stress and confusion and appropriate training and clear protocols are advisable. In addition, depending on the location where a patient suffers an acute hypersensitivity reaction to contrast media, the available expertise of the personnel that cares for such a patient may differ. Similarly, the availability of equipment and drugs to treat a (possible serious) hypersensitivity (or anaphylactic) reaction will be different. In a radiology or cardiology department the possibilities are different (and usually more limited) than in a department of emergency medicine or on a hospital ward. In addition, different treatments will have variable modes of action. What is the most appropriate management of a patient with an acute hypersensitivity reaction to contrast media?
Samenvatting literatuur
Not applicable. There were no studies investigating the research question. The non-comparative studies are briefly described in the evidence table below.
Zoeken en selecteren
To answer the clinical question a systematic literature analysis was performed.
P (Patient) Patients with acute hypersensitivity reaction after contrast media administration.
I (Intervention) Treatment, antihistamines, corticosteroids, epinephrine, adrenalin, dopamine, norepinephrine, noradrenalin, histamine H1 antagonists, histamine H2 antagonists, H1 antihistamines, H2 antihistamines, adrenergic beta-2 receptor agonists, glucocorticoids, management/treatment of hypersensitivity reactions/allergic reactions after contrast media, antihistamines, volume resuscitation, bronchodilators.
C (Comparison) Conservative treatment or comparison of interventions mentioned above.
O (Outcomes) Duration of acute reaction, severity of complaints, morbidity, mortality, costs, hospitalization in an IC-unit, length of stay.
Relevant outcome measures
The working group considered morbidity, mortality, and hospitalization in an IC-unit, critical outcome measures for the decision-making process, and duration of acute reaction, length of stay and costs important outcomes for the decision-making process.
Methods
The databases Medline (OVID) and Embase were searched from 1s of January 1985 to 28th of December 2017 using relevant search terms for systematic reviews (SRs), randomized controlled trials (RCTs) and observational studies (OBS).
Search terms are shown under the Tab “Literature Search”. The literature search procured 328 hits: 20 SR, 64 RCTs and 224 OBS. Based on title and abstract a total of 47 studies were selected. After examination of full text all studies were excluded, and no studies definitely included in the literature summary.
4 studies describing treatment effects of acute adverse reactions were found. Although these studies did not fulfil the search criteria, a short description is included in the literature summary, due to lack of other evidence. Since no control groups were available, no evidence tables or risk of bias tables or conclusions of these studies are included.
Referenties
- Acute boekje 2017. Een initiatief van de Nederlandse Internisten Vereniging. Available at: https://www.hetacuteboekje.nl/hoofdstuk/anafylaxie/anafylaxie.html. Accessed: 11 March 2019
- American College of Radiology. ACR Manual on contrast media. V.10.3. Available at: https://www.acr.org/Clinical-Resources/Contrast-Manual. Accessed: 11 March 2019.
- Asch D, Pfeifer KE, Arango J, Staib L, Cavallo J, Kirsch JD, Arici M, Pahade J. Benefit of epinephrine autoinjector for treatment of contrast reactions: comparison of errors, administration times, and provider preferences. AJR Am J Roentgenol 2017; 209: W363-W369.
- Bang TJ, Suby-Long T, Borgstede JP, et al. University of Colorado radiologist adult contrast reaction smartcard. J Am Coll Radiol 2013; 10: 467-469.
- Boyd B, Leder RA, Castillo M. Managing adverse reactions to contrast agents. Magn Reson Imaging Clin North Am 2017; 25: 737-742.
- Cohan RL, Leder RA, Ellis JH. Treatment of adverse reactions to radiographic contrast media in adults. Radiol Clin North Am 1996; 34: 1055-1076.
- Collins MS, Hunt CH, Hartman RP. Use of IV epinephrine for treatment of patients with contrast reactions: lessons learned from a 5-year experience. AJR Am J Roentgenol 2009; 192: 455-461.
- Demoly P, Adkinson NF, Brockow K, et al. International Consensus on drug allergy. Allergy 2014; 69: 420-437.
- ESUR Contrast Media Safety Committee. ESUR Guidelines on contrast safety, v10. Available at: www.esur-cm.org. Accessed: 17 February 2019.
- Muraro A, Roberts G, Worm M, et al. Anaphylaxis: guidelines of the European Association of Allergy and Clinical Immunology. Allergy 2014; 69: 1026-1045.
- Morzycki A, Bhatia A, Murphy KJ. Adverse reactions to contrast material: A Canadian update. Can Assoc Rad J 2017; 68: 167-193.
- Piscaglia F, Bolondi L; Italian Society for Ultrasound in Medicine and Biology (SIUMB) Study Group on Ultrasound Contrast Agents. The safety of Sonovue in abdominal applications: retrospective analysis of 23,188 examinations. Ultrasound Med Biol 2006; 32: 1369-1275
- Power S, Talbot N, Kucharczyk W, Mandell DM. Allergic-like Reactions to the MR Imaging Contrast Agent Gadobutrol: A Prospective Study of 32 991 Consecutive Injections. Radiology 2016; 281: 72-77.
- Segal AJ, Bush Jr. WH. Avoidable errors in dealing with anaphylactoid reactions to contrast media. Invest Radiol 2011, 46: 147-151.
- Simons FER, Ebisawa M, Sanchez-Borges M, et al. 2015 update of the evidence base: World Allergy Organization anaphylaxis guidelines. World Allergy Organization Journal 2015; 8:32.
- Wang CL, Cohan RL, Ellis JH, Caoli EM, Wang G, Francis IR. Frequency, outcome and appropriateness of treatment of nonionic iodinated contrast media reactions. AJR Am J Roentgenol 2008; 191: 409-415.
Evidence tabellen
Exclusion Table After full text review
Author and year |
Reasons for exclusion |
Boyd, 2017 |
Narrative review. No control arm |
Brockow, 2011 20 |
Narrative review. No control arm |
Bush, 1991 |
Patient group not treated with CM. Does not cover treatment |
Cochran, 2005 |
Expert opinion |
Cohan, 1996 |
Narrative review. |
Collins, 2009 |
Narrative review. No control arm. |
Coors, 2006 |
Narrative review. No control arm. |
Davis, 2015 |
Narrative review. No control arm |
Dawson, 2002 |
Narrative review. No control arm. Does not cover treatment |
Drain, 2001 |
Narrative review. No control arm. |
Hash, 1999 |
Narrative review. No control arm |
Hollingswerth, 1991 |
Patient group not treated with CM |
Iyer, 2013 |
Narrative review. No control arm. |
Kounis, 2015 |
Narrative review. No control arm |
Liebhart, 2007 |
Narrative review. No control arm. Patient group not treated with CM |
Marycz, 2014 |
Narrative review. No control arm |
Masch, 2016 |
Narrative review. No control arm |
Meth, 2006 |
Narrative review. No control arm. |
Morcos, 2001 |
Narrative review. No control arm. |
Morcos, 2005 |
Expert opinion |
Morcos, 2005 |
Narrative review. No control arm. |
Morcos, 2006 |
Narrative review. No control arm. |
Morzycki, 2017 |
Narrative review. No control arm |
Namasivayam, 2006a |
Narrative review. No control arm. Patient group not treated with CM |
Namasivayam, 2006b |
Narrative review. No control arm. |
Nandwana, 2015 |
Narrative review. No control arm. Patient group not treated with CM |
Nayak, 2009 |
Narrative review. No control arm. |
Newmark, 2012 |
Narrative review. No control arm |
Petscavage, 2012 |
Patient group not treated with CM |
Pumphrey, 2004 |
Narrative review. No control arm. |
Ring, 2010 |
Narrative review. Patient group not treated with CM |
Rose, 2015 |
Narrative review |
Sadler, 1994 |
Patient group not treated with CM |
Seikh, 2013 |
Expert opinion. Patient group not treated with CM |
Shellock, 1993 |
Patient group not treated with CM |
Skowronski, 1987 |
Patient group not treated with CM |
Szebeni, 2004 |
Narrative review. No control arm. |
Thompsen 1998b |
Narrative review. No control arm. |
Thompsen, 1998a |
Narrative review. No control arm. |
Thompsen, 2004 |
More recent guideline available |
Thompsen, 2016 |
Narrative review. No control arm |
Toncic, 2009 |
Narrative review. No control arm. Patient group not treated with CM |
Toogood, 1987 |
Patient group not treated with CM |
Wang, 2008 |
Narrative review. No control arm. |
Wang, 2014 |
No comparison between effectivity of several treatments |
Winbery, 2002 |
Narrative review. No control arm. |
Wolkenstein, 1995 |
Narrative review. No control arm. Patient group not treated with CM |
Table 1 Treatment effects of acute adverse reaction
Abbreviations: CM contrast media; CPR Cardio-Pulmonary Resuscitation; IV intravenous;
Reference |
Total n |
CM type |
Acute reaction(s) |
Treatment |
Outcome |
Remarks |
Collins, 2009 |
9 (3) |
LOCM or Gadolinium |
Ranged from laryngeal oedema, hypotension, tachycardia, dyspnoea to hypoxia |
All patients received epinephrine; seven 0.1 mg (recommended initial dose) and two 0.3mg.
Oxygen, diphenhydramine, steroids |
7/9 discharged in good condition on same day of CM administration 1/9 Intubation during transport to emergency department, admitted to ICU, discharged 5 days later in good condition
1/9 Full cardiac arrest; autopsy showed retroperitoneal haemorrhage as cause of death |
4/9 patients had some form of cardiovascular side effects attributed to epinephrine (such as “chest tightness”) |
Wang, 2008 |
11 (3) |
Non-ionic iodinated contrast media |
Ranged from erythema, hypotension, tachycardia, unresponsiveness, arrhythmia, cardiopulmonary arrest, nausea, diaphoresis, rash, hypotension, semi-responsiveness, dizziness, gagging and difficulty speaking, bronchospasm, chest pain, generalized seizure to facial oedema |
Ranged from CPR, 1 mg of epinephrine IV, 1 mg of atropine IV, 50 mEq of sodium bicarbonate, 1 g 10% calcium chloride, 10 L of O2 by face mask, normal saline, 50% dextrose, 50 mg of diphenhydramine IV, 100 mg of diphenhydramine to 120 mg of methylprednisolone |
2/10 returned to their normal baseline conditions within 1 hour. 6/10 manifestations resolved completely within 24 hours, despite their severe symptoms and often extensive treatment. 1 unknown outcome |
Allergic-type reactions occurred in 545/84,928 (0.6%) of IV injections of nonionic iodinated contrast media in adults. 221 received treatment. |
Power, 2016 |
85 (sex unknown) |
Gadobutrol |
81 mild allergic-like reactions: urticaria, rash, pruritus, limited erythema, Localized facial oedema, itchy eyes, scratchy throat, sneezing, coughing
3 moderate reactions: erythema over the anterior chest with dyspnoea, rash and soft palate swelling, pruritic rash and throat tightness
1 severe: breathing and swallowing |
Half of the patient with mild reaction received treatment with oral diphenhydramine
All patients with moderate reactions received treatment with diphenhydramine.
50-minute resuscitation effort |
All patients were discharged |
|
Piscaglia, 2006 |
29 (sex unknown) |
SonoVue |
Ranged from dyspnoea, bronchospasm, slight hypotension and bradycardia, clouding of consciousness, lumbar pain, severe hypotension, cutaneous rash to paraesthesia at the upper limbs |
IV corticosteroids, antihistamines, 1 g of hydrocortisone, lying down with both legs raised, lying down. |
All patients recovered |
|
Verantwoording
Autorisatiedatum en geldigheid
Laatst beoordeeld : 24-06-2020
Laatst geautoriseerd : 24-06-2020
Geplande herbeoordeling : 01-01-2025
Validity
The board of the Radiological Society of the Netherlands will determine at the latest in 2024 if this guideline (per module) is still valid and applicable. If necessary, a new working group will be formed 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 seen as a reason to commence revisions. The Radiological Society of the Netherlands is considered the keeper of this guideline and thus primarily responsible for the actuality of the guideline. The 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.
Initiative
Radiological Society of the Netherlands
Authorization
The guideline is submitted for authorization to:
- Association of Surgeons of the Netherlands
- Dutch Association of Hospital Pharmacists
- Dutch Federation of Nephrology
- Dutch Society for Allergology and Clinical Immunology
- Dutch Society for Dermatology and Venereology
- Dutch Society of Intensive Care
- Netherlands Association of Internal Medicine
- Netherlands Society of Cardiology
- Netherlands Society of Emergency Physicians
- Netherlands Society of Intensive Care
- Radiological Society of the Netherlands
Algemene gegevens
General Information
The guideline development was assisted by the Knowledge Institute of the Federation Medical Specialists (www.kennisinstituut.nl) and was financed by the Quality Funds for Medical Specialists (Stichting Kwaliteitsgelden Medisch Specialisten: SKMS).
Doel en doelgroep
Goal
The aim of the Part 2 of Safe Use of Contrast Media guidelines is to critically review the present recent evidence with the above trend in mind and tries to formulate new practical guidelines for all hospital physicians to provide the safe use of contrast media in diagnostic and interventional studies. The ultimate goal of this guideline is to increase the quality of care, by providing efficient and expedient healthcare to the specific patient populations that may benefit from this healthcare and simultaneously guard patients from ineffective care. Furthermore, such a guideline should ideally be able to save money and reduce day-hospital waiting lists.
Users
This guideline is intended for all hospital physicians that request or perform diagnostic or interventional radiologic or cardiologic studies for their patients in which CM are involved.
Samenstelling werkgroep
Working group members
A multidisciplinary working group was formed for the development of the guideline in 2016. The working group consisted of representatives from all relevant medical specialization fields that are involved with intravascular contrast administration.
All working group members have been officially delegated for participation in the working group by their scientific societies. The working group has developed a guideline in the period from May 2016 until July 2019.
The working group is responsible for the complete text of this guideline.
Working group
Brummer I., emergency physician, Treant Healthcare Group, Emmen
de Geus H.R.H., internist-intensivist, Erasmus Medical Centre, Rotterdam
de Monchy J.G.R., allergologist, DC-Klinieken, Amsterdam
Dekker H.M., radiologist, Radboud University Medical Centre, Nijmegen
Dekkers I.A., clinical epidemiologist and radiologist in training, Leiden University Medical Centre, Leiden
Geenen R.W.F., radiologist, Noordwest Ziekenhuisgroep (NWZ), Alkmaar
Gotte M., cardiologist, Free University Medical Centre, Amsterdam (from July 2018)
Kardaun S.H., dermatologist, University Medical Centre Groningen, Groningen (until March, 2018)
Leiner T., radiologist, University Medical Centre Utrecht, Utrecht (until November 2018)
van der Molen A.J., radiologist, Leiden University Medical Centre, Leiden (chairman)
van der Putten K., nephrologist, Tergooi, Hilversum
van der Vlugt M., cardiologist, Radboud University Medical Centre, Nijmegen (until April 2018)
Wikkeling O.R.M., vascular surgeon, Heelkunde Friesland Groep, location: Nij Smellinghe Hospital, Drachten
Zielhuis S.W., hospital pharmacist, Medical Centre Leeuwarden, Leeuwarden
Methodological support
Buddeke J., advisor, Knowledge Institute of the Federation Medical Specialists (from April 2018)
Harmsen W., advisor, Knowledge Institute of the Federation Medical Specialists (from April 2018)
Mostovaya I.M., senior advisor, Knowledge Institute of the Federation Medical Specialists
Belangenverklaringen
Conflicts of interest
The working group members have provided written statements about (financially supported) relations with commercial companies, organisations or institutions that are 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 at the administrative office of the Knowledge Institute of Medical Specialists and are summarised below.
Last name |
Function |
Other positions |
Personal financial interests |
Personal relations |
Reputation management |
Externally financed research |
Knowledge valorisation |
Other interests |
Signed |
Brummer |
Emergency physician |
None |
None |
None |
None |
None |
None |
None |
February 23rd, 2018 |
De Geus |
Internist-Intensivist Erasmus MC Rotterdam |
None |
None |
None |
None |
None |
None |
None |
March 31st, 2016 |
Dekker |
Radiologist |
None |
Not applicable |
Not applicable |
Not applicable |
Not applicable |
Not applicable |
Not applicable |
July 10th, 2016 |
Dekkers |
Radiologist in training and PhD-candidate |
None |
None |
Not applicable |
Not applicable |
Not applicable |
Not applicable |
Not applicable |
July 8th, 2016 |
Geenen |
Radiologist |
Member of commission prevention of PC-AKI |
None |
None |
None |
None |
None |
Has held several presentation about contrast media on invitation (GE, BAYER) |
March 25th, 2016 |
Kardaun |
Dermatologist – researcher Universitair Medisch Centrum Groningen: unpaid |
Replacing dermatologist in clinical practice - unpaid |
None |
None |
None |
None |
None |
None |
February 24th, 2016 |
Roodheuvel |
Emergency physician |
Instructor OSG/VvAA for courses on echography – paid position Member of department for burn treatment – unpaid. |
None |
None |
None |
None |
None |
None |
December 21st, 2015 |
Van der Molen |
Chairman |
None |
None |
None |
None |
None |
Not applicable |
One-off royalties Springer Verlag (2014) Incidental payments for presentations or being day chairman at contrast safety congress (2016 Netherlands + Europe |
September 6th, 2016 |
Van der Putten |
Internist nephrologist |
None |
None |
None |
None |
None |
None |
None |
October 14th, 2015 |
Van der Vlugt |
Cardiologist |
None |
None |
None |
Chairman of the working group Cardiac MRI & CT and Nuclear imaging of the Netherlands Society of Cardiology |
None |
None |
None |
March 1st, 2016 |
Wikkeling |
Vascular surgeon |
None |
None |
None |
None |
None |
None |
Not applicable |
July 19th, 2016 |
Zielhuis |
Hospital pharmacist |
None |
In the past (2013-2015) has participated in an advisory panel on expensive medication for the companies AbbVie and Novartis. Has received an expense allowance for this. Both forms do not produce contrast media that this guideline is about. Currently not active in an advisory panel. |
None |
None |
None |
None |
None |
January 8th, 2016 |
Inbreng patiëntenperspectief
Input of patient’s perspective
It was challenging to find representation for the patient’s perspective, since the guideline does not discuss a specific group of patients with a disease. The Dutch Kidney Patients Association was invited to participate in an advisory board to the working group, but declined since this subject was not specific enough for them to give adequate input; The Dutch Kidney Patients Association did provide written feedback for specific modules during the commentary phase. The Dutch Kidney Patients Association and the Patient Federation of the Netherlands was invited to participate in the invitational conference in which the framework of the guideline was discussed. Furthermore, the concept guideline has been submitted for feedback during the comment process to the Patient Federation of the Netherlands and the Dutch Kidney Patient Association.
Methode ontwikkeling
Evidence based
Implementatie
Implementation
In the different phases of guideline development, the implementation of the guideline, and the practical enforceability of the guideline were taken into account. 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 with the Related Products. Furthermore, quality indicators were developed to enhance the implementation of the guideline. The indicators can also be found with the Related Products.
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 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 chairman, working group and the advisor inventory the relevant subject matter for the guideline. Furthermore, an Invitational Conference was organized, where additional relevant subjects were discussed. A report of this meeting can be found in Related Products.
Clinical questions and outcomes
During the initial phase of guideline development, the chairman, working group and advisor identified relevant subject matter for the guideline. Furthermore, input was acquired for the outline of the guideline during an Invitational Conference. The working group then formulated definitive clinical questions and defined relevant outcome measures (both beneficial land harmful effects). The working group rated the outcome measures as critical, important and not important. Furthermore, where applicable, the working group defined relevant clinical differences.
Strategy for search and selection of literature
For the separate clinical questions, specific search terms were formulated and published scientific articles were sought after in (several) electronic databases. Furthermore, studies were scrutinized by cross-referencing for other included studies. The studies with potentially the highest quality of research were looked for first. The working group members selected literature in pairs (independently of each other) based on title and abstract. A second selection was performed based on full text. The databases, search terms and selection criteria are described in the modules containing the clinical questions.
Quality assessment of individual studies
Individual studies were systematically assessed, based on methodological quality criteria that were determined prior to the search, so that risk of bias could be estimated. This is described in the “risk of bias” tables.
Summary of literature
The relevant research findings of all selected articles are shown in evidence tables. The most important findings in literature are 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 scientific publications 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 gradations for the quality of scientific evidence: high, moderate, low or very low. These gradations provide information about the amount of certainty about the literature conclusions. (http://www.guidelinedevelopment.org/handbook/).
Formulating conclusions
For diagnostic, etiological, prognostic or adverse effect questions, the evidence was summarized in one or more conclusions, and the level of the most relevant evidence was reported. For intervention questions, the conclusion was drawn based on the body of evidence (not one or several articles). The working groups weighed the beneficial and harmful effects of the intervention.
Considerations
Aspects such as expertise of working group members, patient preferences, costs, availability of facilities and organisation of healthcare aspects are important to consider when formulating a recommendation. These aspects were discussed in the paragraph Considerations.
Formulating recommendations
The recommendation answers the clinical question and was based on the available scientific evidence and the most relevant considerations.
Constraints (Organisation of healthcare)
During the development of the outline of the guideline and the rest of the guideline development process, the Organisation of healthcare was explicitly taken into account. Constraints that were relevant for certain clinical questions were discussed in the Consideration paragraphs of those clinical questions. The comprehensive and additional aspects of the Organisation of healthcare were discussed in a separate chapter.
Development of quality indicators
Internal (meant for use by scientific society or its members) quality indicators are developed simultaneously with the guideline. Furthermore, existing indicators on this subject were critically appraised; and the working group produces an advice about such indicators. Additional information on the development of quality indicators is available by contacting the Knowledge Institute for the Federation Medical Specialists. (secretariaat@kennisinstituut.nl).
Knowledge Gaps
During the development of the guideline, a systematic literature search was performed the results of which help to answer the clinical questions. For each clinical question the working group determined if additional scientific research on this subject was desirable. An overview of recommendations for further research is available in the appendix Knowledge Gaps.
Comment- and authorisation phase
The concept guideline was subjected to commentaries by the involved scientific societies. The commentaries were collected and discussed with the working group. The feedback was used to improve the guideline; afterwards the working group made the guideline definitive. The final version of the guideline was offered for authorization to the involved scientific societies and was authorized.
References
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 Kwalitieit, 2012. Available at: http://richtlijnendatabase.nl/over_deze_site/over_richtlijnontwikkeling.html.
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: http://gdt.guidelinedevelopment.org/central_prod/_design/client/handbook/handbook.html.
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):1106-10. Erratum published in: BMJ 2008;336(7654).
Ontwikkeling van Medisch Specialistische Richtlijnen: stappenplan. Kennisinstituut van Medisch Specialisten.
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