Drug Safety in Translational Paediatric Research: Practical Points to Consider for Paediatric Safety Profiling and Protocol Development: A Scoping Review
Abstract
:1. Introduction
2. Methods
3. Results
4. Discussion
5. Conclusions
Author Contributions
Funding
Acknowledgments
Conflicts of Interest
Appendix A
Database; Date of Last Search | Keyword/Mesh Terms/Website |
---|---|
Pubmed 3 February 2021 | ((“clinical trials as topic”[MeSH Terms] OR (“clinical”[All Fields] AND “trials”[All Fields] AND “topic”[All Fields]) OR “clinical trials as topic”[All Fields]) AND (“pharmacovigilance”[MeSH Terms] OR “pharmacovigilance”[All Fields])) NOT (“vaccines”[MeSH Terms] OR “vaccines”[All Fields] OR “vaccine”[All Fields]) AND (“humans”[MeSH Terms] AND English[lang] AND (“infant”[MeSH Terms] OR “child”[MeSH Terms] OR “adolescent”[MeSH Terms] AND 2020/07/01:2020/12/31[Date - Publication])) |
((protocol[All Fields] AND design[All Fields]) AND (“pharmacovigilance”[MeSH Terms] OR “pharmacovigilance”[All Fields])) NOT (“vaccines”[MeSH Terms] OR “vaccines”[All Fields] OR “vaccine”[All Fields]) AND (“humans”[MeSH Terms] AND English[lang] AND (“infant”[MeSH Terms] OR “child”[MeSH Terms] OR “adolescent”[)MeSH Terms] AND 2020/07/01:2020/12/31[Date-Publication])) | |
((protocol[All Fields] AND (“growth and development”[Subheading] OR (“growth”[All Fields] AND “development”[All Fields]) OR “growth and development”[All Fields] OR “development”[All Fields])) AND (“pharmacovigilance”[MeSH Terms] OR “pharmacovigilance”[All Fields])) NOT (“vaccines”[MeSH Terms] OR “vaccines”[All Fields] OR “vaccine”[All Fields]) AND (“humans”[MeSH Terms] AND English[lang] AND (“infant”[MeSH Terms] OR “child”[MeSH Terms] OR “adolescent”[MeSH Terms] AND 2020/07/01:2020/12/31[Date-Publication])) | |
((“clinical trial protocol”[Publication Type] OR “clinical trial protocols as topic”[MeSH Terms] OR “clinical trial protocol”[All Fields]) AND (“pharmacovigilance”[MeSH Terms] OR “pharmacovigilance”[All Fields])) NOT (“vaccines”[MeSH Terms] OR “vaccines”[All Fields] OR “vaccine”[All Fields]) AND (“humans”[MeSH Terms] AND English[lang] AND (“infant”[MeSH Terms] OR “child”[MeSH Terms] OR “adolescent”[MeSH Terms] AND 2020/07/01:2020/12/31[Date-Publication])) | |
Embase 3 February 2021 | (‘clinical trial protocol’/exp OR ‘clinical trial protocol’) AND (‘pharmacovigilance’/exp OR pharmacovigilance) NOT (‘vaccine’/exp OR vaccine) AND ([newborn]/lim OR [infant]/lim OR [child]/lim OR [preschool]/lim OR [school]/lim OR [adolescent]/lim) AND [humans]/lim AND [english]/lim AND [<1966–2020]/py |
(‘clinical trial’/exp OR ‘clinical trial’) AND (‘pharmacovigilance’/exp OR pharmacovigilance) AND ([newborn]/lim OR [infant]/lim OR [child]/lim OR [preschool]/lim OR [school]/lim OR [adolescent]/lim) AND [humans]/lim AND [english]/lim AND [<1966–2020]/py NOT vaccine | |
Web of science 5 February 2021 | TOPIC: (clinical trial protocol) AND TOPIC: (pharmacovigilance) AND TOPIC: (paediatric) NOT TOPIC: (vaccine)Timespan: 1956-2020. Indexes: SCI-EXPANDED, SSCI, A&HCI, CPCI-S, CPCI-SSH, BKCI-S, BKCI-SSH, ESCI, CCR-EXPANDED, IC. FILTER: English |
TOPIC: (clinical trial) AND TOPIC: (pharmacovigilance) AND TOPIC: (paediatric) NOT TOPIC: (vaccine)Timespan: 1956-2020. Indexes: SCI-EXPANDED, SSCI, A&HCI, CPCI-S, CPCI-SSH, BKCI-S, BKCI-SSH, ESCI, CCR-EXPANDED, IC. FILTER: English | |
EMA 8 February 2021 | https://ec.europa.eu/health/documents/eudralex/vol-10_en - Chapter II Safety reporting - Chapter V Additional documents |
https://www.ema.europa.eu/en/human-regulatory/research-development/scientific-guidelines/clinical-efficacy-safety/clinical-efficacy-safety-general | |
https://www.ema.europa.eu/en/human-regulatory/research-development/scientific-guidelines/clinical-efficacy-safety-clinical-pharmacology-pharmacokinetics | |
https://www.ema.europa.eu/en/human-regulatory/research-development/scientific-guidelines/ich/ich-safety | |
https://www.ema.europa.eu/en/human-regulatory/research-development/paediatric-medicines/scientific-guidelines-paediatrics | |
https://www.ema.europa.eu/en/human-regulatory/post-authorisation/pharmacovigilance/good-pharmacovigilance-practices | |
FDA 8 February 2021 | https://www.fda.gov/science-research/science-and-research-special-topics/pediatrics |
https://www.fda.gov/drugs/development-resources/division-pediatric-and-maternal-health-pediatric-guidances | |
CIOMS 3 February 2021 | https://cioms.ch/pharmacovigilance/ Filters: English, not vaccine |
WHO 3 February 2021 | https://www.who.int/childmedicines/publications/en/ |
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Points to Consider for the Development of a Paediatric Safety Specification | Data Available for * | ||||
---|---|---|---|---|---|
Adults | Children But Not Age Group of Study Population | Age Group of Paediatric Study Population | No Data | ||
Is there safety data on the study drug?† | |||||
Nonclinical safety | Consider assessment of developmental toxicity [20,21] | ||||
Pharmaco- kinetics (PK) | If there is insufficient paediatric data, consider doing a PK study prior to an efficacy/safety study [22,23,29] | ||||
Pharmaco- dynamics (PD) | Consider the feasibility of a paediatric PD study (on & off- target) prior to an efficacy/safety study and/or include PD into the study protocol [22,24,29] | ||||
Pharmaco- genetics | Consider potential effect of age group specific pharmaco-genetics [25] | ||||
Formulation | Ensure the formulation is adapted to the paediatric study population [24,26] | ||||
Excipients | Consider formulation without excipients; assess potential excipient toxicity and total daily excipient dose (study drug(s) and comedications [24,26,30] | ||||
Medication errors | Consider assessing risk for medication errors (study drug(s) and comedications) [5] | ||||
Clinical trial safety data | Assess cumulative clinical trial safety data for all age groups and stratified by age group [4,5,6,10,12,27] | ||||
Spontaneous reports | Summarise cumulative spontaneous reports for all age groups and stratified by age group [4,5,6,10,12,27] | ||||
Pharmaco- epidemiolo-gical data | Explore whether paediatric drug utilisation and safety data are available for the study drug. Be aware of the specific challenges for paediatric pharmacoepidemiological data [31,32,33,34,35,36,37,38,39] | ||||
Class effects | Review class effects in overall population and stratified by age group [4,5,6,10,12,27] | ||||
Literature search | Search for safety concerns (i.e., signals) for the study drug/drug class for all age groups and children; review health authority websites [4,5,6,10] | ||||
Is there data on the paediatric study population?‡ | |||||
Age corrected reference values | Be aware of the age group specific references values for laboratory data, vital signs and developmental assessment and how these change in the developing child [40,41,42,43,44,45,46] | NA | |||
Specifics of ADRs in children | Understand how adverse drug reactions (ADRs) present in children and how they differ from other paediatric age groups and adults [4] | NA | |||
Paediatric comorbidities | Describe common paediatric comorbidities for the study population (e.g., epilepsy and developmental delay) [12] | NA | |||
Comedication | Different compared to adults; increased risk of medication errors from comedication; risk of additive effect of excipients (total daily dose); consider the paediatric safety specification of comedications [12,24,26] | NA | |||
Overall outcome | Normal or disease specific development (e.g., Downs) [12,27,45] | NA | |||
Limited biosampling | Consider scavenged and opportunistic sampling; different recommendations on allowed blood volume by age & region [12,47] | NA | |||
Limitations for study procedures | Example: Blood pressure (BP) measurements in premature babies can be very disruptive. Small children will not sit still; consider taking BP during sleep [12,27] | NA |
EMA ICH E 6 Protocol Guidance [11] | Points to Consider for the Development of Safety Sections in a Paediatric Protocol | Practical Examples in the Literature | |
---|---|---|---|
Protocol Sections Concerning Drug Safety | ICH Guidance | ||
Background information | Summary of nonclinical studies that potentially have clinical significance and from clinical trials relevant to the trial | Including nonclinical safety data on excipients and missing, non-clinical information (e.g., juvenile animal studies) [4,5,20,21,30,48] | [48,49] |
Summary of the known and potential risks and benefits | Including risks of excipients and missing safety data (incl. medication errors) [4,5,22,24,26,30,48] | [50,51,52] | |
Description and justification for route of administration, dosage, dosage regimen, and treatment period(s) | Age group specific PK/PD data for study drug and excipient; formulation adapted to paediatric target population [12,22,23,24,26,27,30,48,53] | [48,54,55] | |
Description of the population to be studied | Describing how ADRs present in children (including risk factors and confounders), comedications (including excipients and medication errors) and paediatric reference ranges (laboratory tests, vital signs, development) [4,5,6,7,28] | [54,55,56,57,58,59] | |
Literature and data relevant to the trial providing background for the trial | Including class effects in children [4,5,6,7] | [50,58,60,61] | |
Objectives and purpose | A detailed description of the objectives and the purpose of the trial | Safety should be a study objective (paediatric safety data is often lacking and reporting SAEs is mandatory) [4,5,6,7,19,28] | [49,54,55] |
Trial design | A description of the stopping rules or discontinuation criteria for individual subjects, parts of trial and entire trial | [56,62] | |
Selection and withdrawal of subjects | Subject exclusion criteria | [51,55,57,58,60] | |
Withdrawal criteria and procedures specifying when and how to withdraw subjects, type and timing of data collection and FU | [55,56,60] | ||
Treatment of subjects | FU period(s) for subjects | Safety FU: based on paediatric safety specification [4,7,10,11] | [60] |
Treatment(s) not permitted for safety reasons before/during the trial | Based on paediatric safety specification [4,7,10,11] | [54] | |
Assessment of safety | Specification of safety parameters | [55,59,60] | |
The methods and timing for assessing, recording, and analysing safety parameters | [50,56,58,59,61] | ||
Procedures for eliciting reports and for recording and reporting AEs | How do AEs/ADRs present in children, comorbidities [4,7,10,12] | [54] | |
Type and duration of FU after AEs | Based on paediatric safety specification, including missing information [4,5,7,10,11] | [60] | |
Statistics | Statistical methods (including timing of interim analyses) | Based on paediatric safety specification, including missing safety information [4,5,7,10,11] | [55,56,64] |
Safety criteria for trial termination | Based on paediatric safety specification [4,7,10,11] | [55,56] |
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Aurich, B.; Jacqz-Aigrain, E. Drug Safety in Translational Paediatric Research: Practical Points to Consider for Paediatric Safety Profiling and Protocol Development: A Scoping Review. Pharmaceutics 2021, 13, 695. https://doi.org/10.3390/pharmaceutics13050695
Aurich B, Jacqz-Aigrain E. Drug Safety in Translational Paediatric Research: Practical Points to Consider for Paediatric Safety Profiling and Protocol Development: A Scoping Review. Pharmaceutics. 2021; 13(5):695. https://doi.org/10.3390/pharmaceutics13050695
Chicago/Turabian StyleAurich, Beate, and Evelyne Jacqz-Aigrain. 2021. "Drug Safety in Translational Paediatric Research: Practical Points to Consider for Paediatric Safety Profiling and Protocol Development: A Scoping Review" Pharmaceutics 13, no. 5: 695. https://doi.org/10.3390/pharmaceutics13050695
APA StyleAurich, B., & Jacqz-Aigrain, E. (2021). Drug Safety in Translational Paediatric Research: Practical Points to Consider for Paediatric Safety Profiling and Protocol Development: A Scoping Review. Pharmaceutics, 13(5), 695. https://doi.org/10.3390/pharmaceutics13050695