Hubbry Logo
Anatomical Therapeutic Chemical Classification SystemAnatomical Therapeutic Chemical Classification SystemMain
Open search
Anatomical Therapeutic Chemical Classification System
Community hub
Anatomical Therapeutic Chemical Classification System
logo
7 pages, 0 posts
0 subscribers
Be the first to start a discussion here.
Be the first to start a discussion here.
Anatomical Therapeutic Chemical Classification System
Anatomical Therapeutic Chemical Classification System
Anatomical Therapeutic Chemical Classification System
View on Wikipedia
from Wikipedia

The Anatomical Therapeutic Chemical (ATC) Classification System is a drug classification system that classifies the active ingredients of drugs according to the organ or system on which they act and their therapeutic, pharmacological and chemical properties. Its purpose is an aid to monitor drug use and for research to improve quality medication use. It does not imply drug recommendation or efficacy.[1] It is controlled by the World Health Organization Collaborating Centre for Drug Statistics Methodology (WHOCC), and was first published in 1976.[2][3][4]

Coding system

[edit]

This pharmaceutical coding system divides drugs into different groups according to the organ or system on which they act, their therapeutic intent or nature, and the drug's chemical characteristics. Different brands share the same code if they have the same active substance and indications. Each bottom-level ATC code stands for a pharmaceutically used substance, or a combination of substances, in a single indication (or use). This means that one drug can have more than one code, for example acetylsalicylic acid (aspirin) has A01AD05 (WHO) as a drug for local oral treatment, B01AC06 (WHO) as a platelet inhibitor, and N02BA01 (WHO) as an analgesic and antipyretic; as well as one code can represent more than one active ingredient, for example C09BB04 (WHO) is the combination of perindopril with amlodipine, two active ingredients that have their own codes (C09AA04 (WHO) and C08CA01 (WHO) respectively) when prescribed alone.

The ATC classification system is a strict hierarchy,[5] meaning that each code necessarily has one and only one parent code, except for the 14 codes at the topmost level which have no parents. The codes are semantic identifiers,[5] meaning they depict information by themselves beyond serving as identifiers (namely, the codes depict themselves the complete lineage of parenthood). As of 7 May 2020, there are 6,331 codes in ATC; the table below gives the count per level.[6]

ATC level Codes Different names/pharmaceuticals
Level 1 14 14
Level 2 94 94
Level 3 267 262
Level 4 889 819
Level 5 5067 4363

History

[edit]

The ATC system is based on the earlier Anatomical Classification System, which is intended as a tool for the pharmaceutical industry to classify pharmaceutical products (as opposed to their active ingredients).[7] This system, confusingly also called ATC, was initiated in 1971 by the European Pharmaceutical Market Research Association (EphMRA) and is being maintained by the EphMRA and Intellus. Its codes are organised into four levels.[8] The WHO's system, having five levels, is an extension and modification of the EphMRA's. It was first published in 1976.[2]

Classification

[edit]

In this system, drugs are classified into groups at five different levels:[9]

First level

[edit]

The first level of the code indicates the anatomical main group and consists of one letter. There are 14 main groups:[10]

Code Contents
A Alimentary tract and metabolism
B Blood and blood forming organs
C Cardiovascular system
D Dermatologicals
G Genito-urinary system and sex hormones
H Systemic hormonal preparations, excluding sex hormones and insulins
J Antiinfectives for systemic use
L Antineoplastic and immunomodulating agents
M Musculo-skeletal system
N Nervous system
P Antiparasitic products, insecticides and repellents
R Respiratory system
S Sensory organs
V Various

Example: C Cardiovascular system

Second level

[edit]

The second level of the code indicates the therapeutic subgroup and consists of two digits.[11]

Example: C03 Diuretics

Third level

[edit]

The third level of the code indicates the therapeutic/pharmacological subgroup and consists of one letter.

Example: C03C High-ceiling diuretics

Fourth level

[edit]

The fourth level of the code indicates the chemical/therapeutic/pharmacological subgroup and consists of one letter.

Example: C03CA Sulfonamides

Fifth level

[edit]

The fifth level of the code indicates the chemical substance and consists of two digits.

Example: C03CA01 furosemide

Other ATC classification systems

[edit]

ATCvet

[edit]

The Anatomical Therapeutic Chemical Classification System for veterinary medicinal products (ATCvet) is used to classify veterinary drugs. ATCvet codes can be created by placing the letter Q in front of the ATC code of most human medications. For example, furosemide for veterinary use has the code QC03CA01.

Some codes are used exclusively for veterinary drugs, such as QI Immunologicals, QJ51 Antibacterials for intramammary use or QN05AX90 amperozide.[12]

Herbal ATC (HATC)

[edit]

The Herbal ATC system (HATC) is an ATC classification of herbal substances; it differs from the regular ATC system by using 4 digits instead of 2 at the 5th level group.[13]

The herbal classification is not adopted by WHO. The Uppsala Monitoring Centre is responsible for the Herbal ATC classification, and it is part of the WHODrug Global portfolio available by subscription.[14]

Defined daily dose

[edit]
Main article: Defined daily dose

The ATC system also includes defined daily doses (DDDs) for many drugs. This is a measurement of drug consumption based on the usual daily dose for a given drug. According to the definition, "[t]he DDD is the assumed average maintenance dose per day for a drug used for its main indication in adults."[15]

Adaptations and updates

[edit]

National issues of the ATC classification, such as the German Anatomisch-therapeutisch-chemische Klassifikation mit Tagesdosen, may include additional codes and DDDs not present in the WHO version.[16]

ATC follows guidelines[17] in creating new codes for newly approved drugs. An application is submitted to WHO for ATC classification and DDD assignment. A preliminary or temporary code is assigned and published on the website and in the WHO Drug Information for comment or objection. New ATC/DDD codes are discussed at the semi-annual Working Group meeting. If accepted it becomes a final decision and published semi-annually on the website and WHO Drug Information and implemented in the annual print/on-line ACT/DDD Index on January 1.[18]

Changes to existing ATC/DDD follow a similar process to become temporary codes and if accepted become a final decision as ATC/DDD alterations. ATC and DDD alterations are only valid and implemented in the coming annual updates; the original codes must continue until the end of the year.[19][20] An updated version of the complete on-line/print ATC index with DDDs is published annually on January 1.[21]

See also

[edit]

References

[edit]
[edit]
Revisions and contributorsEdit on WikipediaRead on Wikipedia

Anatomical Therapeutic Chemical Classification System

View on Grokipedia
from Grokipedia
The Anatomical Therapeutic Chemical (ATC) Classification System is a hierarchical method for organizing based on their anatomical site of action, therapeutic use, and , serving as the for utilization and statistics. Developed by the (WHO) and its Collaborating Centre for Drug Statistics Methodology in , , the system classifies active substances using International Nonproprietary Names () and assigns unique seven-character codes to facilitate the comparison of drug consumption data across countries. The ATC structure consists of five levels: the first level divides drugs into 14 main anatomical or pharmacological groups (e.g., A for alimentary tract and metabolism, N for nervous system); the second and third levels specify therapeutic, pharmacological, or chemical subgroups; the fourth level denotes chemical, pharmacological, or therapeutic subgroups; and the fifth level identifies the specific chemical substance. This classification emphasizes the primary therapeutic or pharmacological action of the drug, with separate codes often assigned for different routes of administration or combination products to reflect distinct uses. Established in its current form since 1975 for statistical purposes and first published as guidelines in 1990, the system is updated annually by the WHO International Working Group for Drug Statistics Methodology, which meets biannually to review and assign new codes based on requests from regulators, manufacturers, and researchers, ensuring stability for longitudinal trend analysis. Complementing the ATC is the Defined Daily Dose (DDD), a fixed unit representing the assumed average maintenance dose per day for a drug's main indication in adults, which enables standardized measurement of drug consumption volume rather than cost or value. While primarily a research tool to improve the quality of drug use and support pharmacoepidemiological studies, the ATC/DDD system is not intended for decisions on reimbursement, pricing, or therapeutic substitution, as it does not reflect clinical efficacy or safety profiles. Adopted globally by organizations such as the (EMA) and national health authorities, it underpins initiatives like the WHO's drug consumption monitoring and has been integral to international pharmacovigilance since its globalization in 1996.

Overview

Purpose and Scope

The Anatomical Therapeutic Chemical (ATC) Classification System is a hierarchical framework for organizing the active ingredients of medicines based on their primary anatomical site of action, therapeutic indications, pharmacological properties, and chemical characteristics. This structure enables standardized categorization that supports consistent identification and analysis of pharmaceuticals across diverse contexts. The primary purposes of the ATC system include serving as an essential tool for drug utilization research to enhance the quality of prescribing and consumption, advancing pharmacoepidemiological studies, informing reimbursement policies in healthcare systems, and enabling international comparisons of consumption patterns. By providing a uniform method to quantify and compare use, it helps identify trends in use, evaluate utilization patterns, and promote rational use globally. In terms of scope, the ATC system primarily encompasses human medicines, assigning approximately 6,900 unique codes to active substances as of 2025, while excluding medical devices, veterinary products, and classifications based on brand names or proprietary formulations. It focuses exclusively on the therapeutic roles of active ingredients, ensuring applicability to a wide array of pharmaceuticals without regard to or commercial identifiers. Key applications of the ATC system extend to its adoption by the (WHO) for compiling global drug consumption statistics, by national health agencies for constructing formularies and regulatory monitoring, and by researchers for analyzing drug utilization patterns to inform public health policies. This broad utility underscores its role in fostering evidence-based improvements in healthcare delivery worldwide.

Development and Maintenance

The Anatomical Therapeutic Chemical (ATC) Classification System, developed in , was established as an by the (WHO) for drug utilization research and has overseen its evolution since its initial publication in 1976. The system was developed in during the early 1970s, building on earlier classification efforts like the European Pharmaceutical Market Research Association (EphMRA) system, to address the growing need for standardized drug monitoring following increased attention to drug utilization research in the . WHO's endorsement in 1981 by its Regional Office for marked formal recognition for international use, with global standardization recommended in 1996. Primary maintenance of the ATC system is handled by the WHO Collaborating Centre for Drug Statistics Methodology, established in 1982 at the Norwegian Institute of Public Health in , . This centre coordinates ongoing development, including the classification of new active substances, assignment of Defined Daily Doses (DDDs), and revisions to existing codes to reflect advances in and therapeutic practices. Maintenance processes feature annual reviews, typically through expert meetings held in spring and autumn, where proposed changes are evaluated and implemented to ensure the system's relevance and accuracy. Collaboration with international is facilitated via the WHO International Working Group for Statistics , comprising 12 members selected from WHO's Expert Advisory Panels on and on Policies and Management (including aspects related to the International Pharmacopoeia and Pharmaceutical Preparations). This group provides technical advice on classifications, approves new ATC codes, and promotes the system's application in drug utilization studies worldwide. The centre also responds to inquiries from national drug regulatory authorities and researchers to maintain consistency across global datasets. Funding for the Collaborating Centre's operations is provided by the WHO and the Norwegian government, enabling its role as a non-profit entity dedicated to . The ATC index, guidelines, and related resources are freely accessible through an online database hosted by the centre, supporting open use for research, policy-making, and without licensing fees.

History

Origins and Early Development

The conceptual roots of the Anatomical Therapeutic Chemical (ATC) classification system lie in mid-20th-century European efforts to standardize categorization for and statistical purposes. In the , organizations like the European Pharmaceutical Market Research Association (EPhMRA), founded in 1953, developed the Anatomical Classification of Pharmaceutical Products, which grouped drugs primarily by their therapeutic indications and anatomical targets to support sales data analysis across . This system emphasized a hierarchical structure based on organ systems and uses, influencing later therapeutic classifications. Scandinavian models contributed significantly to the ATC's evolution, particularly through Norwegian initiatives in the and early . Amid rising interest in utilization research (DUR), Norway's Norwegian Medical Depot (NMD) adapted and expanded the EPhMRA framework into the ATC system around 1970–1972, adding therapeutic, pharmacological, and chemical subgroups for more precise statistical tracking. This development was spurred by a 1969 WHO symposium in Oslo, which identified the need for an international standard to compare consumption patterns amid growing concerns over rational use. The (WHO) initiated formal involvement in 1970 to address the demand for standardized drug statistics, leading to the establishment of the Drug Utilization Research Group (DURG) and the creation of an initial ATC prototype that integrated anatomical, therapeutic, and chemical elements. This prototype built directly on the Norwegian modifications to EPhMRA, aiming to enable comparable international data for policy. The first complete ATC index was published in 1975 by the newly formed on Medicines (NLN), providing a comprehensive list of substances classified under the system for use in Nordic drug consumption statistics. This publication represented the culmination of early prototyping efforts and marked the system's readiness for broader application in utilization studies.

Adoption and Evolution

The Anatomical Therapeutic Chemical (ATC) classification system, initially developed in in the mid-1970s based on earlier systems, was first utilized for Nordic drug statistics around 1975–1976. In 1981, the (WHO) Regional Office for formally recognized the combined ATC/ (DDD) system for drug utilization studies and recommended its application across European countries to enable comparable consumption statistics. This marked the initial endorsement for international use in monitoring drug consumption patterns. By 1982, the system was integrated into a formalized framework through the establishment of the WHO Collaborating Centre for Drug Statistics Methodology in , which coordinated its further refinement and application for global drug utilization research. Key evolutionary milestones shaped the system's robustness and applicability. During the 1980s, the ATC structure expanded with additional subgroups to accommodate emerging pharmaceuticals, increasing the total number of classified substances from around 1,000 in the early years to over 3,000 by the decade's end, reflecting growing pharmaceutical diversity. The first formal ATC/DDD guidelines were published in , standardizing the for international use. In 1996, WHO elevated the ATC/DDD to an , prompting the launch of digital tools and databases that facilitated easier access and data sharing for utilization studies worldwide. The saw further adaptations to include biologics and vaccines, with dedicated subgroups such as J07 for vaccines and expansions in L (antineoplastic and immunomodulating agents) for biologics like monoclonal antibodies, ensuring the system addressed advances in . By 2025, the ATC system had achieved widespread global adoption, utilized in drug utilization and efforts across more than 100 countries, enabling standardized comparisons of consumption at national and international levels. In the , it is mandated under regulations for reporting, with the assigning ATC codes to all authorized medicines to track adverse events and market trends. In the United States, adaptations of the ATC have been incorporated into Medicare analyses for evaluating drug utilization patterns, complementing national coding systems like the National Drug Code. Evolutionary challenges, such as harmonizing ATC with the (ICD), have been addressed through mapping initiatives that link drug classes to disease codes, supporting integrated epidemiological .

Classification Structure

First Level: Anatomical Main Groups

The first level of the Anatomical Therapeutic Chemical (ATC) Classification System provides a broad categorization of medicinal substances into 14 main groups, designated by the letters A through N, with an additional group V. This level organizes drugs primarily according to the anatomical region or on which they primarily act, offering an initial therapeutic-independent grouping that facilitates international drug utilization studies and pharmacoepidemiological . By focusing on anatomical main groups, the ATC system enables a standardized framework for classifying active ingredients based on their site of action, such as the digestive tract or cardiovascular system, without delving into specific pharmacological mechanisms or chemical properties at this stage. This approach supports the comparison of consumption patterns across populations and healthcare systems globally. The 14 main groups are as follows:
CodeMain GroupBrief Description
AAlimentary Tract and Drugs primarily affecting the digestive system and metabolic processes.
BBlood and Blood Forming OrgansAgents targeting blood components and hematopoiesis.
CCardiovascular SystemMedications acting on the heart and vascular system.
DDermatologicalsPreparations for skin conditions and topical applications.
GGenito and HormonesSubstances influencing the urinary tract, reproductive organs, and related hormones.
HSystemic Hormonal Preparations, excl. Hormones and InsulinsSystemic hormones excluding those for reproduction or .
JAntiinfectives for Systemic UseSystemic agents combating infections.
LAntineoplastic and Immunomodulating AgentsDrugs for and modulation.
MMusculo-skeletal SystemTreatments for muscles, bones, and joints.
NAgents affecting the central and peripheral nervous systems, including analgesics and psychotropics.
PAntiparasitic Products, Insecticides and RepellentsProducts against parasites and for .
RMedications for the airways and lungs.
SSensory OrgansPreparations for eyes, ears, and other sensory structures.
VVariousMiscellaneous substances not fitting other anatomical groups, such as diagnostic agents and allergens.
These anatomical main groups serve as the foundational tier, upon which subsequent levels build more detailed therapeutic and chemical classifications. The system continues to evolve, with new subgroups and codes added annually for innovative therapies, such as gene and cell therapies (as of 2025).

Second Level: Therapeutic Subgroups

The second level of the Anatomical Therapeutic Chemical (ATC) classification system delineates therapeutic subgroups that subdivide anatomical main groups from the first level, organizing drugs according to their primary therapeutic applications within specific organ systems or physiological processes. This level employs a two-digit numerical code appended to the single-letter code of the first level, resulting in a three-character identifier that refines the anatomical categorization by emphasizing the intended clinical use of the drugs. For instance, the code A10 designates "Drugs used in " under the alimentary tract and main group (A), grouping medications primarily aimed at managing blood glucose levels. Therapeutic subgroups at this level focus on clustering drugs by their main therapeutic purpose, such as alleviating symptoms, treating underlying diseases, or supporting physiological functions relevant to the anatomical group. This approach balances the broad anatomical foundation of the first level—such as targeting the cardiovascular system—with more precise therapeutic orientations, enabling researchers and regulators to analyze drug utilization patterns by clinical indication rather than solely by site of action. Another example is C09, which covers "Agents acting on the renin-angiotensin system" within the cardiovascular main group (C), encompassing therapies directed at regulation and . By prioritizing therapeutic utility, this level facilitates comparisons across drugs with overlapping indications while maintaining hierarchical consistency in the overall ATC framework. As of 2025, there are approximately 100 therapeutic subgroups at the second level, distributed variably among the 14 main groups, with most main groups containing around 5 to 10 subgroups to reflect the diversity of therapeutic needs within each anatomical domain. This finite number ensures a manageable yet comprehensive structure for international drug statistics, supporting applications in pharmacoepidemiology, reimbursement policies, and lists. The assignment of drugs to these subgroups is determined by their predominant therapeutic role, as evaluated by the WHO Collaborating Centre for Drug Statistics Methodology, which maintains the system to promote standardized global reporting.

Third Level: Pharmacological Subgroups

The third level of the Anatomical Therapeutic Chemical (ATC) classification system subdivides the therapeutic subgroups established at the second level into more specific pharmacological subgroups, denoted by the third character of the ATC code, which is a letter. This level focuses on grouping drugs based on their pharmacological properties, such as mechanisms of action or drug classes, rather than solely on therapeutic indications. For instance, within the therapeutic subgroup of analgesics (N02), the third level distinguishes N02A for , which act primarily on opioid receptors to provide central analgesia, from N02B for other analgesics and antipyretics, such as non-steroidal anti-inflammatory drugs that inhibit enzymes peripherally. This pharmacological subclassification enables a nuanced categorization that reflects how drugs exert their effects, facilitating comparisons across agents with similar modes of action. Examples include C07A for beta blocking agents, which antagonize beta-adrenergic receptors to reduce and in cardiovascular therapy, and N06A for antidepressants, encompassing classes like selective serotonin reuptake inhibitors that modulate levels in the . By prioritizing pharmacological distinctions, the third level accommodates drugs with multiple therapeutic applications without assigning them to a single primary use, thus supporting flexible yet precise classification. The rationale for this level lies in its ability to aggregate drugs with comparable pharmacological profiles, which is essential for on , , and utilization patterns. It allows investigators to analyze outcomes like rates or therapeutic responses within homogeneous groups, such as comparing beta-blockers for their cardioselectivity or opioids for their mu-receptor affinity, without delving into chemical structures. This approach enhances the ATC system's utility in pharmacoepidemiology and development by providing a standardized framework for grouping that balances specificity and practicality.

Fourth Level: Chemical Subgroups

The fourth level in the Anatomical Therapeutic Chemical (ATC) Classification System delineates chemical, pharmacological, or therapeutic s within the broader pharmacological categories defined at level, providing a finer based primarily on molecular or structural characteristics. This level is represented by a single letter as the fourth character in the ATC code, which groups drugs sharing similar chemical properties or mechanisms that distinguish them from other subgroups at the same hierarchical tier. For instance, within antidiabetic agents, the subgroup for biguanides is designated to cluster compounds with a common chemical backbone, facilitating distinctions from other oral blood glucose-lowering agents. A key aspect of the fourth level is its emphasis on structural similarities to enable precise categorization, particularly when pharmacological actions alone are insufficient for differentiation. In antibacterial classifications, for example, sulfonamides form one chemical subgroup, while penicillins constitute another, highlighting differences in molecular frameworks such as the sulfa moiety versus the beta-lactam ring. Similarly, beta-lactam antibiotics are grouped to reflect their shared cyclic amide structure, and HMG CoA reductase inhibitors are unified under a subgroup based on their chemical class, which targets synthesis pathways. This approach prioritizes chemical homogeneity where possible, though pharmacological criteria may supersede when they better serve analytical needs, ensuring the system remains adaptable to evolving pharmaceutical knowledge. The utility of the fourth level lies in its role in supporting advanced pharmacoepidemiological analyses, regulatory oversight, and toxicity assessments by identifying clusters of chemically related compounds for targeted studies. By aggregating data on structurally akin drugs, it aids in monitoring utilization patterns, evaluating safety profiles across similar molecules, and informing policy decisions without delving into individual substances. This level's design promotes consistency in international drug statistics, allowing researchers to compare therapeutic equivalence or substitution potential within defined chemical boundaries, thereby enhancing the overall robustness of drug classification frameworks.

Fifth Level: Individual Substances

The fifth level of the Anatomical Therapeutic Chemical (ATC) classification system provides the most detailed categorization by assigning unique codes to individual active pharmaceutical ingredients or chemical substances, denoted by the final two digits of the seven-character ATC code, which follow a sequential numbering system. This level ensures precise identification of specific drugs within their pharmacological subgroups, using International Nonproprietary Names (INN) where available, or Adopted Names (USAN) or British Approved Names (BAN) otherwise. The system covers thousands of such substances, focusing on those with established therapeutic uses, and is not exhaustive but inclusion-based upon requests from regulatory authorities or pharmaceutical companies. Codes at this level are assigned according to the substance's primary therapeutic indication and typical , with generally one code per substance to maintain consistency in drug utilization studies. However, exceptions occur when a substance has multiple distinct indications or formulations, allowing for separate codes; for example, receives A10BA52 for low-dose use in alopecia and G04CB01 for higher doses in . Fixed-ratio combinations of substances are treated as distinct entities and receive their own fifth-level codes, often in dedicated subgroups ending in "51" or similar (e.g., M01AE51 for + , or C10BX04 for simvastatin + acetylsalicylic acid + ), provided they are marketed for a specific therapeutic purpose. Examples illustrate this granularity: metformin, an oral antidiabetic, is coded A10BA02 under blood glucose-lowering drugs excluding insulins; , a long-acting insulin analogue, is A10AE04; and prednisolone may have multiple codes depending on formulation and use, such as A01AC01 for dental preparations or S01BA04 for ophthalmic applications. New substances, including innovative therapies, are incorporated as they are approved; for instance, RNA-based vaccines for and prevention were assigned J07BB55 in 2024. Initially, novel drugs without a permanent place may be temporarily classified in miscellaneous "X" groups until further evaluation.

Coding System

Code Format and Composition

The Anatomical Therapeutic Chemical (ATC) classification system employs a standardized seven-character alphanumeric to uniquely identify each active substance and its position within the hierarchical structure. This format consists of one uppercase letter followed by six characters comprising digits and letters, ensuring a systematic and searchable representation of drugs. For instance, the N02BE01 designates (also known as acetaminophen), where the structure delineates the substance's therapeutic category and specificity. The composition of the ATC code is divided across its five levels as follows: the first character is a single letter (A to Z) representing the anatomical main group, such as 'N' for the ; positions two and three are two digits (00 to 99) indicating the therapeutic subgroup, like '02' for analgesics; position four is a single letter (A to Z) for the pharmacological subgroup, exemplified by 'B' for other analgesics and antipyretics; position five is another letter (A to Z) denoting the chemical subgroup, such as 'E' for Anilides; and positions six and seven are two digits (01 to 99) specifying the individual chemical substance, with '01' assigned to . This breakdown allows for a hierarchical progression from broad anatomical categories to precise substance identification, facilitating international comparability in drug statistics. Special notations within the coding system accommodate variations and miscellaneous entries. The digit '9' is conventionally used to signify "other" or miscellaneous subgroups, particularly at the second level (e.g., A09 for other products) or in the final digits for undefined or residual categories, ensuring comprehensive coverage without disrupting the . Fixed-dose combinations of substances are handled by assigning dedicated codes, often in the 50-series (e.g., N02BE51 for combinations of with other drugs) or, in specific cases like psycholeptics, the 70-series, where the code reflects the primary ingredient while indicating the combination nature; a plus sign (+) may be appended in textual descriptions for clarity but is not part of the core . ATC codes are designed to be unique and non-overlapping, with each active substance normally receiving a single code based on its main therapeutic use, with the same code generally used for different formulations and routes of administration unless distinct therapeutic indications require separate codes, to prevent unnecessary duplication and maintain consistency. This uniqueness is enforced through the maintenance of the official ATC Index by the WHO Collaborating Centre for Drug Statistics Methodology, making codes verifiable and searchable via the publicly available WHO ATC/DDD database, which supports global drug utilization research and regulatory applications.

Assignment and Validation Rules

The assignment of Anatomical Therapeutic Chemical (ATC) codes to medicinal substances is primarily determined by their main therapeutic use, which encompasses the primary indication for which the is licensed or most commonly prescribed. This criterion takes precedence, ensuring alignment with the anatomical main group and therapeutic subgroups that best reflect the drug's intended anatomical or physiological target. Additional factors, such as the 's and , guide placement within pharmacological and chemical subgroups, particularly when multiple therapeutic uses exist. For instance, a substance like is classified under N06AX (other s) based on its primary indication, despite potential off-label uses. The process for assigning ATC codes begins with submissions to the WHO Collaborating Centre for Drug Statistics Methodology, typically required by January 15 or August 15 annually to align with the International Working Group's review meetings in or October. Submitters, often pharmaceutical companies or regulatory authorities, must provide detailed documentation including the chemical structure, pharmacological profile, and evidence of marketing authorization or clinical use. The , comprising international experts, conducts a thorough to resolve any conflicts or ambiguities, such as overlapping therapeutic indications, and proposes classifications that are then open for public comment. Provisional codes may be issued for investigational drugs or substances with incomplete data, allowing temporary inclusion in the system pending further evidence; these are finalized without objection after the comment period and implemented in the subsequent January update. Validation of assigned ATC codes involves rigorous cross-checks against established pharmacopoeias, approved dosage recommendations from national drug catalogues, and peer-reviewed journals to confirm therapeutic relevance and consistency. The International periodically reviews classifications, particularly after three years for new entries, incorporating prescribed daily dose data to verify ongoing fit. Reclassification occurs when emerging evidence, such as shifts in clinical practice or new approvals, alters the primary indication—for example, is classified in both G02AD06 (oxytocics for low-dose induction of labour) and A02BB01 (prostaglandins for peptic treatment at standard doses), reflecting its multiple indications. Such changes are proposed during meetings and implemented only after expert consensus and absence of objections, ensuring stability while adapting to real-world utilization patterns. Challenges in assignment and validation arise particularly with complex substances like biologics and enantiomers, which require nuanced evaluation to maintain the system's hierarchical integrity. Biologics, such as type A (M03AX01 for migraine prophylaxis), are classified based on their therapeutic action rather than alone, often necessitating new subgroups if no suitable fit exists. Enantiomers, like the R- and S-isomers of certain beta-blockers, receive separate ATC codes and defined daily doses only if their potencies or indications differ significantly, as seen with (N07BC05) versus racemic (N07BC02). These cases highlight the need for detailed pharmacological data to avoid misclassification, with provisional assignments serving as a bridge until full validation through clinical evidence.

Veterinary Applications (ATCvet)

The ATCvet system represents an adaptation of the Anatomical Therapeutic Chemical (ATC) classification specifically for veterinary medicinal products, maintaining the core principles of the human ATC while incorporating modifications to address animal-specific therapeutic needs. Established in 1990 by the on Medicines and transferred to the WHO Collaborating Centre for Drug Statistics in 2001, it enables the standardized international, national, and local comparison of veterinary drug utilization data. A defining feature of ATCvet is the addition of a "Q" prefix to existing ATC codes, distinguishing veterinary applications without altering the underlying classification for substances used in both human and animal medicine; for instance, the alimentary tract and metabolism group shifts from A in human ATC to QA in ATCvet. This prefix-based approach minimizes redundancy while allowing for veterinary-exclusive codes where necessary, such as those for species-specific indications like intramammary antibacterials (QJ51) or certain antiparasitics (QP). The system also uniquely includes coverage for , immunologicals, and feed additives, which are prominent in animal health but less so in human therapeutics. At its core, ATCvet preserves the five-level hierarchical structure of the ATC system—anatomical main groups, therapeutic subgroups, pharmacological subgroups, chemical subgroups, and individual substances—with the "Q" prefix integrated at the first level and additional veterinary-oriented subgroups at subsequent levels. A notable structural difference is the introduction of as the first-level group for immunologicals, encompassing species-specific products such as avian infectious bronchitis vaccines or bovine clostridial vaccines, which require tailored classifications not found in the human ATC. The complete ATCvet Index, listing all established codes, is updated annually by the WHO Collaborating Centre, with the 2025 edition reflecting ongoing adaptations to emerging veterinary needs; in the European context, the (EMA) collaborates on its maintenance and application. In practice, ATCvet supports regulatory oversight in the , particularly through the EMA's European Surveillance of Veterinary Antimicrobial Consumption (ESVAC) program, which relies on ATCvet codes to monitor sales and usage patterns of across member states. This classification aids in identifying trends in drug consumption, evaluating risks, and informing policy on prudent use. Furthermore, it contributes to residue control efforts by standardizing the categorization of pharmacologically active substances evaluated for maximum residue limits (MRLs), ensuring alignment with regulations under EU law.

Herbal and Traditional Medicines (HATC)

The Herbal Anatomical Therapeutic Chemical (HATC) classification system was developed in the late 1990s and early 2000s by the Monitoring Centre (UMC), a (WHO) collaborating centre, as an extension to the standard ATC framework specifically for herbal and traditional medicines. Proposed initially by pharmacologist Peter A.G.M. De Smet in 1998 to ensure compatibility with the ATC system, HATC was refined and integrated into the WHO Drug Global Dictionary (WHODrug) by 2004, with revisions continuing through subsequent years, including a notable update in 2005. Although not formally adopted by WHO for the main ATC index, HATC serves as a specialized tool managed by UMC to address the growing global use of herbal remedies outside conventional pharmaceutical classifications, and has been fully integrated into WHODrug Global to support in databases like VigiBase. The structure of HATC mirrors the five-level hierarchy of the ATC system—anatomical main group, therapeutic subgroup, pharmacological subgroup, chemical subgroup, and individual substance—but adapts it to emphasize botanical and traditional origins rather than synthetic chemistry. The first level comprises 14 anatomical groups labeled A through V, identical to ATC (e.g., A for alimentary tract and metabolism, D for dermatologicals). Subsequent levels use alphanumeric codes, with the fifth level employing four digits (e.g., 5001) to denote specific herbal ingredients, distinguishing them from the two-letter codes for chemical substances in standard ATC. For instance, the code A06AB5001 classifies the dry leaf juice of Mill. as a contact under alimentary tract therapies, highlighting its botanical source and therapeutic application. Some herbal products with established medical uses are integrated directly into the main ATC system based on their primary indication (e.g., root in antacids under A02AA), while purer traditional formulations rely on HATC for precise grouping. This dual approach allows flexibility, with HATC codes often marked by prefixes like 'h' for officially recognized herbals in WHODrug databases. HATC covers a range of herbal and traditional preparations, including single-plant extracts, multi-herb combinations, and less-defined remedies derived from botanicals, excluding fully synthetic or homeopathic products that fall under separate guidelines. These codes facilitate in and clinical studies, particularly for monitoring adverse events in global databases. The primary purpose of HATC is to support the safe integration of traditional and herbal medicines into modern healthcare systems, promoting harmonized nomenclature for , research, and regulatory oversight worldwide. This is especially relevant in regions like and , where traditional medicines serve up to 80% of the population for primary healthcare needs, aiding in the standardization of utilization data and without implying proven or for each classified item.

Defined Daily Dose

Definition and Methodology

The Defined Daily Dose (DDD) is defined as the assumed average maintenance dose per day for a drug used for its main indication in adults. This metric serves as a standardized unit within the Anatomical Therapeutic Chemical (ATC) classification system to enable international comparisons of consumption patterns. Only one DDD is assigned per ATC code and specific , reflecting the primary therapeutic use rather than all possible doses or off-label applications. The DDD is determined by the WHO Collaborating Centre for Drug Statistics , in consultation with the WHO International Working Group on Drug Statistics, which comprises 12 international experts meeting biannually. This process relies on clinical guidelines, pharmacokinetic and pharmacodynamic data, dosing recommendations from drug regulatory authorities, and expert consensus to establish the value. DDD values are expressed in mass units, such as grams or milligrams, for most substances; for example, the DDD for (ATC code N02BE01) is 3 g for oral administration. Key factors considered include the (e.g., oral, parenteral) and the target patient population, primarily adults, though adjustments may account for specific therapeutic contexts. No DDD is assigned to topical preparations, diagnostic agents, or substances where dosing varies widely due to non-standardized use. Conceptually, the DDD facilitates utilization by providing a benchmark for estimating treatment days from consumption data, where the number of DDDs consumed = total consumption (in mass units) / DDD value. This metric can approximate the number of patients treated, assuming one DDD per patient per day, ensuring the metric remains fixed and assumption-based, independent of actual market consumption patterns.

Applications in Drug Utilization

The (DDD), integrated with the Anatomical Therapeutic Chemical (ATC) classification system, is primarily applied to quantify consumption as DDD per 1,000 inhabitants per day, providing a standardized metric for cross-national comparisons of drug utilization patterns. This approach enables the aggregation and analysis of sales or prescription data across diverse healthcare systems, highlighting variations in prescribing practices and access to medicines. In practice, DDD-based metrics support targeted monitoring of specific therapeutic areas; for instance, trends in the ATC group J01 (antibacterials for systemic use) are used to track overall consumption, informing strategies to combat by identifying high-use regions or periods. Similarly, assessments of analgesics in ATC group N02A through DDD calculations help evaluate consumption levels, revealing patterns of use that may indicate risks of dependency or inadequate . The synergy between DDD and ATC facilitates the generation of internationally comparable statistics for drug utilization research, allowing for decisions on and . However, limitations arise in contexts such as , where DDD values—based on adult maintenance doses—may overestimate or underestimate actual use, and in off-label applications, where prescribed amounts deviate from the defined standard. On a global scale, the ATC/DDD methodology underpins World Health Organization (WHO) reports evaluating medicine access and promoting rational drug use, with ongoing applications in 2025 to address inequities in low- and middle-income countries through data-driven interventions.

Updates and Adaptations

Revision Process

The revision process for the Anatomical Therapeutic Chemical (ATC) Classification System is managed by the WHO Collaborating Centre for Drug Statistics Methodology in Oslo, Norway, ensuring annual updates to reflect evolving pharmacological knowledge and therapeutic practices. Proposals for new ATC codes, changes to existing classifications, or Defined Daily Dose (DDD) assignments are accepted year-round from manufacturers, regulatory authorities, and other users through an online application form submitted to the Centre. Upon receipt, the Centre confirms the proposal and, for straightforward cases, issues a preliminary ATC code within 6-8 weeks based on initial assessment of the drug's main therapeutic indication and pharmacological properties. More complex proposals undergo evaluation by the WHO International Working Group (IWG) for ATC Classification and DDD Assignment, which convenes twice annually in and to review evidence such as clinical data, , and therapeutic guidelines. Decisions from these meetings are published on the Centre's website and in WHO Drug Information, followed by a period for public comments and objections, typically 60 days, to allow stakeholder input on major changes. If no substantive objections arise, the approved alterations are implemented in the subsequent annual ATC/DDD Index, typically released in late December for use from January, with full integration occurring 6-12 months after approval to accommodate national adaptations. Changes to the ATC system are governed by strict criteria to maintain stability and therapeutic , prioritizing the drug's primary indication over secondary uses or commercial factors. Additions occur for newly approved substances with distinct therapeutic profiles; mergers or splits of subgroups happen when new evidence reveals overlaps or improved specificity in anatomical or pharmacological grouping; and deletions apply to obsolete drugs no longer in clinical use. For instance, the system emphasizes consistency in assigning codes based on the main and target organ, avoiding frequent reclassifications unless supported by robust . As of the 2025 ATC/DDD Index, recent revisions include expansions in various therapeutic areas such as antivirals and , reflecting emerging evidence. These updates, totaling approximately 200-300 new codes and alterations in 2025, as is typical annually, underscore the system's responsiveness to emerging therapeutic areas while adhering to evidence-based criteria. As of November 2025, ongoing WHO initiatives continue to emphasize global harmonization, with the next review cycle planned for 2026.

National and International Variations

While the Anatomical Therapeutic Chemical (ATC) classification system is maintained internationally by the (WHO) Collaborating Centre for Drug Statistics Methodology, many countries implement national extensions or adaptations to accommodate local regulatory needs, traditional medicines, and data integration requirements. These variations ensure the system aligns with domestic healthcare policies, , and reimbursement frameworks, often involving additional codes or mappings without altering the core ATC structure. In , the ATC system has been extended to include medicines, traditional formulations integral to the national healthcare system. A provisional ATC (HATC) coding system assigns codes to over 200 preparations, allowing their integration into drug utilization studies and reimbursement processes while preserving the standard ATC hierarchy for Western pharmaceuticals. This adaptation supports the widespread prescription of by physicians, with formulations like kakkonto classified under relevant therapeutic groups such as those for respiratory or gastrointestinal conditions. The , where the (FDA) primarily relies on the National Drug Code (NDC) system for product identification, employs unofficial mappings to link NDC codes to ATC classifications. These mappings, facilitated through the National Library of Medicine's RxNorm database, enable researchers and regulators to analyze drug utilization patterns comparably with international data, though the FDA does not mandate ATC use for approvals or surveillance. For instance, NDC-to-ATC conversions decompose into steps linking NDC products to RxNorm ingredients and then to ATC codes, supporting pharmacoepidemiological studies without official endorsement. In the , ATC codes are required for medicinal products seeking centralized marketing authorization through the (EMA), facilitating harmonized and statistical reporting across member states. Applicants must provide or request an ATC code from the WHO index during the submission process, ensuring consistency in the European database of medicinal products. Similarly, in , the () integrates ATC codes with PBS item numbers to classify subsidized medicines, incorporating cost and utilization data for policy decisions and epidemiological analysis. This linkage allows grouping of drugs by therapeutic action, with ATC stability aiding long-term trend monitoring despite occasional PBS code changes. Challenges in these adaptations include discrepancies in Defined Daily Doses (DDD) due to regional differences in dosing practices or population demographics, which can complicate cross-national comparisons. For example, when prescribed daily doses (PDD) substantially deviate from international DDD values, adjustments are needed for accurate utilization metrics. The WHO addresses these through its International Working Group on Drug Statistics , which reviews proposals for new codes, DDD alterations, and to promote global consistency, though national priorities sometimes lead to persistent variations. As of 2025, the ATC system and its variants are adopted in over 100 countries worldwide, with ongoing WHO initiatives emphasizing convergence to enhance international drug monitoring and research.

References

  1. https://www.who.int/teams/health-product-and-policy-standards/inn/atc-ddd
  2. https://atcddd.fhi.no/atc/structure_and_principles/
  3. https://www.who.int/standards/classifications/other-classifications/the-anatomical-therapeutic-chemical-classification-system-with-defined-daily-doses
  4. https://www.ema.europa.eu/en/glossary-terms/atc-code
  5. https://www.who.int/tools/atc-ddd-toolkit/atc-classification
  6. https://www.who.int/tools/atc-ddd-toolkit/applications-methodology
  7. https://build.fhir.org/ig/HL7NZ/nzf/ValueSet-atc-code.html
  8. https://www.who.int/tools/atc-ddd-toolkit/history
  9. https://atcddd.fhi.no/atc_ddd_methodology/history/
  10. https://www.who.int/tools/atc-ddd-toolkit/methodology
  11. https://atcddd.fhi.no/
  12. https://atcddd.fhi.no/atc_ddd_methodology/who_international_working_group/
  13. https://atcddd.fhi.no/atc_ddd_methodology/who_collaborating_centre/
  14. https://www.ephmra.org/anatomical-classification
  15. https://atcddd.fhi.no/atc_ddd_methodology/the_ephmra_classification_system/
  16. https://atcddd.fhi.no/atc_ddd_methodology/history/history
  17. https://www.ntnu.no/ojs/index.php/norepid/article/view/532/500
  18. https://atcddd.fhi.no/filearchive/publications/2024_guidelines__final_web.pdf
  19. https://onlinelibrary.wiley.com/doi/full/10.1111/1468-0009.12565
  20. https://ijpds.org/article/view/1314
  21. https://www.drugsandalcohol.ie/29364/1/WHO%2520Collaborating%2520Centre%2520for%2520Drug%2520Statistics%2520Methodology.pdf
  22. https://www.canada.ca/en/health-canada/services/drugs-health-products/drug-products/drug-product-database/terminology.html
  23. https://atcddd.fhi.no/atc_ddd_index/?code=A10BA02
  24. https://atcddd.fhi.no/atc_ddd_index/?code=A10AE04
  25. https://atcddd.fhi.no/lists_of__temporary_atc_ddds_and_alterations/new_atc_5th_levels/
  26. https://www.whocc.no/atc/structure_and_principles/
  27. https://atcddd.fhi.no/filearchive/publications/2025_guidelines__final_web.pdf
  28. https://www.fhi.no/en/fi/who-collaborating-centre-for-drug-statistics-methodology/atcddd-handbook/general/atcvet-methodology/
  29. https://atcddd.fhi.no/atcvet/atcvet_methodology/history/
  30. https://www.fhi.no/en/fi/who-collaborating-centre-for-drug-statistics-methodology/atcddd-handbook/atcvet/relationship-between-atcvet-and-atc/
  31. https://atcddd.fhi.no/atcvet/atcvet/general_principles/
  32. https://atcddd.fhi.no/atcvet/atcvet_index_and_guidelines/atcvet_index/
  33. https://www.ema.europa.eu/en/documents/report/european-sales-use-antimicrobials-veterinary-medicine-annual-surveillance-report-2023_en.pdf
  34. https://www.ema.europa.eu/en/veterinary-regulatory-overview/research-development-veterinary-medicines/maximum-residue-limits-mrl
  35. https://who-umc.org/whodrug/whodrug-global/herbal-atc/
  36. https://pmc.ncbi.nlm.nih.gov/articles/PMC7419327/
  37. https://www.iomcworld.com/open-access/innovative-approach-for-classification-of-traditional-system-of-medicine-43409.html
  38. http://www.pharmadhoc.com/uploads/3/2/7/4/3274790/who_drug_herbal.pdf
  39. https://www.famhp.be/en/human_use/medicines/herbal_medicinal_products/marketing_authorisation_procedures/herbal-atc-codes
  40. https://www.researchgate.net/publication/283623354_Innovative_Approach_for_Classification_of_Traditional_System_of_Medicine
  41. https://www.who.int/tools/atc-ddd-toolkit/about-ddd
  42. https://atcddd.fhi.no/ddd/definition_and_general_considera/
  43. https://atcddd.fhi.no/atc_ddd_index/?code=N02BE01
  44. https://www.who.int/data/gho/indicator-metadata-registry/imr-details/5766
  45. https://pmc.ncbi.nlm.nih.gov/articles/PMC6716286/
  46. https://www.fhi.no/en/fi/who-collaborating-centre-for-drug-statistics-methodology/atcddd-handbook/atc/application/
  47. https://atcddd.fhi.no/atc/application_form/
  48. https://atcddd.fhi.no/atc_ddd_index/
  49. https://atcddd.fhi.no/atc_ddd_index/updates_included_in_the_atc_ddd_index/
  50. https://atcddd.fhi.no/atc_ddd_alterations__cumulative/atc_alterations/
  51. https://www.researchgate.net/publication/51396713_Regulatory_sciences_in_herbal_medicines_and_dietary_supplements
  52. https://data.lhncbc.nlm.nih.gov/public/mor/pubs/pdf/2017-amia-fk-poster.pdf
  53. https://www.ema.europa.eu/en/documents/other/chapter-3ii-xevprm-detailed-user-guidance-electronic-submission-information-medicinal-products-human-use-marketing-authorisation-holders-ema_en.pdf
  54. https://www.saxinstitute.org.au/wp-content/uploads/PBS-Data-Dictionary-October-2020.pdf
  55. https://cdn.who.int/media/docs/default-source/international-nonproprietary-names-%28inn%29/atc-ddd/57th_atc-ddd_executive_summary.pdf?sfvrsn=c147156e_5
Add your contribution
Related Hubs
User Avatar
No comments yet.