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Clinical drug concepts in the international edition are authored either using presentation strength (for discrete dose forms) or using concentration strength (for liquid dose forms and patches, etc.) as appropriate for different types of product (see Appendix A of the international International Medicinal Product Model specification). Concentration strength in SNOMED CT is where the description of the strength of a clinical drug has been normalised such that the denominator value is "one" and the denominator unit is a unit of mass (e.g., grams) or volume (e.g., milllilitres). Presentation strength is strength is a description of the strength of the clinical drug as it is present in its unit of presentation (vial, ampoule, sachet). In national extensions, the concentration strength clinical drug may be sufficient, or there may be a requirement to represent some, usually liquid dose form product clinical product clinical drugs, using both concentration and presentation strength either for the abstract clinical drug, or for the real clinical drug, or for both. This is shown in the diagram below:
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Even within a single jurisdiction, authorisations are not always consistent in dealing with presentation and concentration strength. Some regulatory agencies have or are moving to licensing all parenteral liquid products using presentation strength (with the exception of some products such as insulins and large volume parenteral fluid parenteral fluid replacement products and bulk use vials, etc.); other agencies have been or are using this pattern for some products (e.g., pre-filled syringes) and may change for others as IDMP takes effect. Some national terminologies are working to normalise the patterns of strength representation particularly for safety considerations; others are dealing with the mixed economy that exists "as is". This international specification provides support for the different patterns for both clinical drugs and real clinical drugs whilst maintaining the requirement that concepts will classify correctly within the system.
This modelling modeling pattern is advised for use with usually liquid products that are placed inside a unit of presentation such as an ampoule, vial, cartridge or pre-filled syringe, which itself is then put inside a package, usually but not always with other identical units, for placement into the supply chain. For these products, the presentation strength is itself often clinically relevant, and therefore, although the fully specified name pattern (as currently described) uses the concentration strength, a synonym (which could be the preferred term for a national extension) could use the presentation strength description; for example: "enoxaparin sodium 120 milligram/0.8 millilitre conventional release solution for injection in pre-filled syringe".
As the unit of presentation is the "countable entity" of the clinical drug, this modelling modeling pattern is not advised for continuous semi-solids (creams, ointments, etc.) or continuous liquids (oral solutions, suspensions) where there is no "countable entity". The unit of presentation should not be confused with the package for continuous semi-solids and liquids that is placed into the supply chain (tubes, bottles, etc.). The package should be described using the (R)PCD structure which describes the package size , but not currently the package type. For example: chloramphenicol 5 chloramphenicol 5 milligram/1 milliliter conventional release eye drops are supplied in a 10mL bottle; the clinically relevant information is the "10mL" volume, which is the package size.
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This is the pattern for a national extension to author a presentation strength representation of a clinical drug that is described using concentration strength in the international edition. This can be used for:
- liquid parenteral products presented in units of presentation, such as ampoules, vials, pre-filled syringes, cartridges, or bags/bottles
- liquid oral products presented in a sachet or other unit dose unit of presentation
- liquid pulmonary products presented in a unit dose presentation unit of presentation
In addition to the usual attributes for a concentration strength clinical drug, the unit of presentation size and unit of presentation unit attributes are used. The concept will then classify correctly as a child of the existing concentration strength clinical drug. This does mean that the exact presentation strength must be authored manually as an additional description and that the exact presentation strength is not provided in the logical definition (other than via calculation), but this pattern has been found to be the most efficient method for authoring such concepts, especially when there are multiple active ingredient substances. The alternative was to author both concentration strength and presentation strength in two role groups, which, whilst it does also give the correct classification, is very labour intensive.
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| Semantic tag | (clinical drug) | |||||
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| Definition status |
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Cardinality
Notes
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Cardinality
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Cardinality
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Range
Cardinality (within role group)
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Attribute Attribute
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Cardinality (within role group)
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Role Group One role group is required for each precise active ingredient | Attribute
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Cardinality (within role group)
Notes
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Attribute
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Cardinality (within role group)
Notes
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Attribute
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Cardinality (within role group)
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Attribute
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Cardinality (within role group)
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Attribute
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Cardinality (within role group)
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Attribute
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Cardinality (within role group)
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Also note that the unit of presentation, the unit of presentation size quantity, and the unit of presentation size unit are not role grouped together, as there should only ever be 0..1 of each present for any one clinical drug concept.
For clinical drugs that have two or more active ingredient substances that are modifications of the same base substance, and where MP precisely concepts are required in the national extension, and for single ingredient product concepts where the active substance is an ingredient in these multiple modification multi-ingredient products, the following extra ingredient count attribute will be required in order to support correct relationships generated by the MRCM:
Attribute
| Range
Cardinality
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For concepts that have two or more active ingredient substances that are modifications of the same the same base active ingredient substance (i.e., parent ingredient substance) and where one is a further modification of the other (for example, a multi-ingredient product containing both dexamethasone phosphate and dexamethasone sodium phosphate, where the dexamethasone phosphate is a modification of dexamethasone (base) and dexamethasone sodium phosphate is a further modification of the dexamethasone phosphate) and where MP precisely concepts are required in the national extension, and for single ingredient product concepts where the active substance is an ingredient in these multiple modification multi-ingredient products, the following extra ingredient count attribute will be required in order to support correct relationships generated by the MRCM:
Attribute
| Range
Cardinality
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Example Diagrams
Some examples of clinical drug concepts, with concentration strength and presentation strength in a national drug extension, are shown below.
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