Cleaning Validation
The Industries First Choice for Automated Cleaning Validation & Risk Management
Benefits that save you time & money
- Fast ROI providing significant time savings over manual processes
- Data Security with 21 cfr 11 Part 11 compliance
- Reduced Error with a totally paperless system
- Efficiency through electronic management and approval of master data.
- System Defined Protocols with sampling plans that are automatically generated for validation groups
- Comprehensive Reporting enables users to quickly retrieve in-depth standard reports and statistical analysis
How can you calculate so many risk factors manually?
A holistic & process-specific risk mitigation system
Nova-Cleaning Validation software significantly enhances product integrity by managing changes and assessing the risks associated with cross-contamination and product impurities within a dynamic production environment. All changes to methods, APIs, products, equipment, and family groups are automatically evaluated to ensure product integrity and regulatory compliance. Nova-Cleaning Validation complies with 21 CFR Part 11 and EU Annex 11. The system uses a risk-based approach and is designed based on PDA Technical Reports 29 and 49, ISPE MaPP, 21 CFR Part 211.67.
Unique & innovative features
Computerized worst case evaluation. Risk factors including dosage, toxicity, cleanability, solubility and more can be defined together or separately, allowing the user to have complete control over the evaluation settings. The worst case is determined and displayed for all validation groups, enabling users to focus on the biggest risk to product quality. The worst case assessment is automatically triggered when any validation group property is changed. Fully automated
MAC calculations. Carryover limits are calculated for all sample points for APIs, cleaning agents, and microbial testing. Hundreds of MAC formulas are executed in seconds, rather than hours. The calculations take into account all possible product A and product B combinations for the affected equipment trains and validation groups, and the lowest MAC values are highlighted, making user review of the calculated values quick and easy.
The process dedicated change evaluation feature consolidates the impact of multiple changes in one snapshot of the risks and consequences of potential changes to any factor that may affect the validated state of the cleaning process. These factors include changing equipment, introducing new products, modifying batch sizes, and anything else that relates to both the product and equipment families that are part of equipment trains and validation groups
AUTOMATE
RISK-BASED
EVALUATIONS &
MAC CALCULATIONS
IDENTIFY
THE RISK OF
CHANGES
IN REAL-TIME
ACHIEVE
COMPLETE COMPLIANCE
& CONTAMINATION
CONTROL
Frequently Asked Questions
There are a few different methods which have been used to calculate the maximum allowable carry over (MACO). If we look at the changes in the approach to calculating limits over time, we see the evolution of the MACO calculations from arbitrary limits to Science, health-based and risk-based limits.
Initially an arbitrary MACO calculation method was Part Per Million (PPM). Then dose-based criteria, using limited data like LD50 values was applied to derive allowable carry over into the next product. At present, the current regulatory thinking for MACO limits include the health-based limit calculations (HBELs) using acceptable or permitted daily exposure (ADE/ PDE). ADE and PDE values are calculated based on scientifically sound toxicological data and incorporate a risk-based approach to derive their values.
One should perform MACO for Active Pharmaceutical Ingredients, microbial residue, cleaning agent residue and disinfectants where applicable.
Using spreadsheets are ubiquitous around the world and its intended use for businesses is to manage financial data and perform financial analysis.
Spreadsheet software was never intended to be used for cleaning validation data and advanced MACO calculations. These spreadsheets and spreadsheet tools have no built in compliancy, data integrity features, or formula validation features, and although some companies have used such spreadsheets for calculating cleaning validation limits, it is really a work around and can never replace a software system dedicated to the cleaning validation process.
It is better to use a dedicated cleaning validation software product that not only adheres to Data Integrity and 21 CFR Part 11 regulations but is flexible enough to calculate hundreds of risk factors simultaneously and provide the worst-case scenarios. Novatek Europe provides a pharmaceutical cleaning validation software.
The worst-case product is determined using the properties of both the product and the API in the product. The first measure of worst case is the toxicity based on daily exposure, the lower the PDE the more toxic the product is. Worst case also considers physical properties like solubility in water, solubility in other solvents, or the cleanability.
It is possible to use a simple calculation to obtain a risk score by assigning the toxicological data into ranges, the solubility, and other physical properties into risk ratings, and then assigning a weighting to each criterion.
Risk based worst case analysis takes into consideration the risk associate with every factor and choose the worst case among several options. Sometimes hard to reach equipment, hard to clean surface or a non-soluble API maybe worse than toxicity, so one needs to evaluate all types of risks and scientifically choose the worst-case scenario. Finally, the worst-case method should also consider the potent and non-potent products when determine the marker compound.
There are different approaches for calculating the MACO values on the batch level. These are equations used to calculate MACO. The last equation is the one which uses the toxicological data to calculate the MACO value. The industry is transitioning from MACO to MSC which represents the maximum safe carry over.
In the PIC/S PI 006-01 Guidelines, the following statements are made regarding the definition of limits.
Carry-over of product residues should meet defined criteria, for example the most stringent of the following three criteria:
a) No more than 0.1% (1/1000th) of the normal therapeutic dose of any product will appear in the maximum daily dose of the following product.
b) No more than 10 ppm of any product will appear in another product.
c) No quantity of residue should be visible on the equipment after cleaning procedures are performed.
In the last 10 years the dose-based calculation (e.g., 1/1000th dose) has prevailed in the manufacture of pharmaceutical products. Where dose data are not available, an absolute value (e.g., 10 ppm) is prescribed.
For residues where dose data are not available but toxicological data are (e.g. tensides), it is normal to perform the calculation based on the NOEL/ADI (no effect level/acceptable daily intake) value along with a safety factor (SF).
Cleaning limits are calculated on the batch level, but they also need to be calculated at the sample point level so the results for samples collected for cleaning validation and interim monitoring events after cleaning operations can be compared to these limits to confirm that the cleaning process is effective. These equations use the shared and are and the sample point area, as well as the recovery factor of the sampling method to calculate the MAC limits per sample point.
MAC means the Maximum Allowable Carryover, and MACO means virtually the same thing, the difference being that the MACO acronym splits the C into two words which result in maximum Safe Carry Over. No matter which acronym, the meaning is the maximum allowable carry over of contamination of a previous product, cleaning agent, or any residue, into the next product being manufactured on the same equipment.
Over time, as the industry has evolved, subject matter experts have asked… Who is allowing this allowable carry over? Instead of what is allowed shouldn’t we use science to determine what is the Maximum Safe Carryover (MSC) level? The new science and risk-based approach to cleaning validation uses Health-Based Exposure Limits (HBELs), and the latest techniques, to provide companies with the means to effectively clean, to confirm the Maximum Safe Carryover is not exceeded, an to ensure product quality and patient safety.
Achieve complete contamination control with the combination of NOVA-CLEANING VALIDATION. Achieve complete contamination control with NOVATEK’S CLEANING VALIDATION & ENVIRONMENTAL MONITORING SOFTWARE
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