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Related Concept Videos

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Constraints and Statical Determinacy

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Related Experiment Video

Updated: Jul 4, 2026

A Method for Studying the Temperature Dependence of Dynamic Fracture and Fragmentation
09:12

A Method for Studying the Temperature Dependence of Dynamic Fracture and Fragmentation

Published on: June 28, 2015

A Δ‑Based Framework For Internal Release Limits In Plateau Stability Systems.

Thanh N Tran1

  • 1CMC Statistics and Chemometrics Innovation (CMEI), The Netherlands; Analytical Chemistry & Chemometrics, Institute for Molecules and Materials, Radboud University Nijmegen, The Netherlands; Data Science, Institute for Computing and Information Sciences (iCIS), Radboud University Nijmegen, The Netherlands; Principal Scientist, MS&T, Abbott, Weesp, The Netherlands.

European Journal of Pharmaceutical Sciences : Official Journal of the European Federation for Pharmaceutical Sciences
|July 2, 2026
PubMed
Summary
This summary is machine-generated.

This study introduces a new Δ-based framework for setting pharmaceutical Internal Release Limits (IRLs). This model-independent approach accurately estimates future batch compliance without relying on potentially unsupported kinetic extrapolation, especially for plateauing stability data.

Keywords:
Internal release limits (IRLs)Pharmaceutical quality controlPharmaceutical stabilityStability PlateauTolerance intervals

Related Experiment Videos

Last Updated: Jul 4, 2026

A Method for Studying the Temperature Dependence of Dynamic Fracture and Fragmentation
09:12

A Method for Studying the Temperature Dependence of Dynamic Fracture and Fragmentation

Published on: June 28, 2015

Area of Science:

  • Pharmaceutical Manufacturing
  • Analytical Chemistry
  • Statistics

Background:

  • Internal Release Limits (IRLs) are typically set using statistical methods like time-series regression for shelf-life assignment.
  • These methods assume identifiable degradation slopes and require prediction beyond observed timepoints, which may not hold true for sparse or plateauing stability data.
  • Regression-based inference can be statistically unsupported in practical IRL scenarios.

Purpose of the Study:

  • To introduce a Δ-based framework for Internal Release Limit (IRL) determination that is model-independent and data-appropriate.
  • To formalize identifiability conditions, certify plateau behavior, and partition variance in stability datasets.
  • To provide explicit future-batch population coverage using one-sided tolerance intervals.

Main Methods:

  • Development of a Δ-based framework for IRL determination.
  • Formalization of identifiability conditions and plateau certification.
  • Application of one-sided tolerance intervals for future-batch coverage.
  • Validation through simulation studies and analysis of a monoclonal antibody dataset.

Main Results:

  • The Δ-based framework provides direct and accurate estimates of future-batch-protective release limits, outperforming model-based approaches in plateauing systems.
  • Application to a monoclonal antibody dataset demonstrates transformation of sparse stability data into a regulatorily actionable strategy.
  • The framework recovers IRL decisions consistent with time-dependent modeling under weaker assumptions when plateau behavior is verified.

Conclusions:

  • The Δ-based IRL determination is the identifiable limiting case for stability systems with time-invariant late-age behavior and unreliably estimable kinetic parameters.
  • This approach offers greater uncertainty transparency and aligns with analytical lifecycle management expectations.
  • It provides a robust and regulatorily actionable strategy for IRLs, particularly for biologics with plateauing stability profiles.