Tuesday, November 15, 2022

Treatment Emergent AEs (TEAEs), On-Study AEs, On-Treatment AEs, Non-TEAEs

During the clinical trial, the adverse events (AEs) are collected from the signing of the informed consent to the last dose of the study drug plus some follow-time. For statistical analyses of adverse event data, the treatment-emergent AEs (TEAEs) are usually defined. AEs with an onset date at or after the first dose of the study drug will be defined as TEAEs. AEs with an onset date prior to the first dose of the study drug will then be defined as Non-TEAEs. 

For example, the TEAE can be defined as:

"TEAEs are defined as events that start within the day of the first dose of trial treatment until 28 days after the last dose of treatment" in an SAP for an EMD Serono study.

"Treatment-emergent AEs (TEAEs) are defined as AEs that are not present at baseline or represent an exacerbation of a preexisting condition during the treatment period. Therefore, referencing the protocol, TEAEs will be defined programmatically as any AE record with a start date/time on or after the first study treatment administration (greater than or equal to study day 1), inclusive to the end of the study (specifically the EOS visit or ET visit)." in an SAP for a Regeneron's study

The TEAEs can be further defined based on the comparison of the AE onset date with a cut-off date where the cut-off date may be the last dose date or 28 days after the last dose date. 

In FDA's clinical review document for AstraZeneca's asthma drug, the on-study AE and on-treatment AE were defined:

  • On-study AE: events with onset between the first-day dosing and the scheduled follow-up visit. 
  • On-treatment AE: events with onset between the first day of treatment and the scheduled end of treatment (EOT) or investigational product discontinuation (IPD) visit. 
  • Post-treatment AE: events with onset after the on-treatment period defined above

 On-study AEs include all TEAEs - all AEs recorded on or after the first dose date. 

On-treatment AEs are a subset of all TEAEs or on-study AEs. The AEs with an onset date after the cut-off date will be excluded from on-treatment AEs. 

There are some clinical trials with on-treatment AEs defined as the same as traditional TEAEs (i.e., any AEs with an onset date on or after the first dose of the study drug regardless of the cut-off date).

In a recent workshop "Advancing Premarket Safety Analysis" organized by FDA and Duke Margolis Center for Health Policy, the on-study and on-treatment AEs were specifically discussed. Here are the presentation slides for this topic:







The concept of on-treatment AEs has already been implemented in some clinical trials. For example, in a GSK-sponsored trial "A Phase 3a, Repeat Dose, Open-label, Long-term Safety Study of Mepolizumab in Asthmatic Subjects", the primary outcome measure is "Number of Participants With Any On-treatment Adverse Event (AE) or On-treatment Serious AE (SAE)" where On-treatment AEs and on-treatment SAEs are the events occurring on/after the first dose of open-label mepolizumab date and before/on last dose+28 days.

In a BMS trial "A randomized, open-label, phase 3 study of  BMS-936558 vs. Everolimus in Subjects with advanced or metastatic clear-cell renal cell carcinoma who have received prior anti-angiogenic therapy", the on-treatment AEs were defined as the following with a cut-off date of 100 days of the last dose of study treatment.
"On-treatment AEs will be defined as AEs with an onset date-time on or after the DateTime of the first dose of study treatment (or with an onset date on or after the day of first dose of study treatment if time is not collected or is missing). For subjects who are off study treatment, AEs will be counted as on-treatment if event occurred within 100 days of the last dose of study treatment. No “subtracting rule” will be applied when an AE occurs both pre-treatment and post-treatment with the same preferred term and grade."
Defining on-treatment AEs will require specifying a cut-off date and the cut-off date may be different depending on the potential impact of the study drug after the drug discontinuation and the half-life of the investigational products. 

Defining on-treatment AEs may be necessary for studies with the treatment policy estimand where the efficacy data and AE/SAEs are continued to be collected after the study participants have discontinued the study treatment. 

Previous discussions: 

No comments: