The ACTTION-American Pain Society-American Academy of Pain Medicine Pain Taxonomy (AAAPT): A Multidimensional Approach to Classifying Acute Pain Conditions

Michael Kent; Patrick Tighe; Inna Belfer; Timothy J Brennan; Stephen Bruehl; Chad Brummett; Chester Buckenmaier, III; Asokumar Buvanendran; Robert I Cohen; Paul Desjardins; David Edwards; Roger Fillingim; Jennifer Gewandter; Debra Gordon; Robert Hurley; Henrik Kehlet; John Loeser; Sean Mackey; Samuel McLean; Rosemary Polomano; Siamak Rahman; Srinivasa Raja; Michael Rowbotham; Santhanam Suresh; Bernard Schachtel; Kristin Schreiber; Mark Schumacher; Brett Stacey; Steven Stanos; Knox Todd; Dennis Turk; Steven Weisman; Christopher Wu; Daniel Carr; Robert Dworkin; Gregory Terman

doi:10.1016/j.jpain.2017.02.421

. Author manuscript; available in PMC: 2020 Jun 29.

Published in final edited form as: J Pain. 2017 May;18(5):479–489. doi: 10.1016/j.jpain.2017.02.421

The ACTTION-American Pain Society-American Academy of Pain Medicine Pain Taxonomy (AAAPT): A Multidimensional Approach to Classifying Acute Pain Conditions.

Michael Kent ¹, Patrick Tighe ², Inna Belfer ³, Timothy J Brennan ⁴, Stephen Bruehl ⁵, Chad Brummett ⁶, Chester Buckenmaier III ⁷, Asokumar Buvanendran ⁸, Robert I Cohen ⁹, Paul Desjardins ¹⁰, David Edwards ¹¹, Roger Fillingim ¹², Jennifer Gewandter ¹³, Debra Gordon ¹⁴, Robert Hurley ¹⁵, Henrik Kehlet ¹⁶, John Loeser ¹⁷, Sean Mackey ¹⁸, Samuel McLean ¹⁹, Rosemary Polomano ²⁰, Siamak Rahman ²¹, Srinivasa Raja ²², Michael Rowbotham ²³, Santhanam Suresh ²⁴, Bernard Schachtel ²⁵, Kristin Schreiber ²⁶, Mark Schumacher ²⁷, Brett Stacey ²⁸, Steven Stanos ²⁹, Knox Todd ³⁰, Dennis Turk ³¹, Steven Weisman ³², Christopher Wu ³³, Daniel Carr ³⁴, Robert Dworkin ³⁵, Gregory Terman ³⁶

¹Department of Anesthesiology, Walter Reed National Military Medical Center

²Department of Anesthesiology, University of Florida, Gainesville

³Center for Drug Evaluation and Research, Food and Drug Administration

⁴Department of Anesthesiology, University of Iowa

⁵Department of Anesthesiology, Vanderbilt University

⁶Department of Anesthesiology, University of Michigan Health System

⁷Defense and Veteran’s Center for Integrative Pain Management, Uniformed Services University

⁸Department of Anesthesiology, Rush University Medical Center

⁹Department of Anesthesiology, Beth Israel Deaconess Medical Center

¹⁰Desjardins Associates LLC

¹¹Department of Anesthesiology, Vanderbilt University

¹²Department of Community Dentistry and Behavioral Science, University of Florida, Gainesvile

¹³Department of Anesthesiology, University of Rochester Medical Center, School of Medicine and Dentistry

¹⁴Department of Anesthesiology and Pain Medicine, University of Washington

¹⁵Department of Anesthesiology, Medical College of Wisconsin

¹⁶University of Copenhagen

¹⁷Department of Neurological Surgery, Department of Anesthesiology and Pain Medicine

¹⁸Department of Anesthesiology, Perioperative and Pain Medicine, Stanford University

¹⁹Department of Emergency Medicine, University of North Carolina, Chapel Hill

²⁰Department of Biobehavioral Sciences, University of Pennsylvania School of Nursing

²¹Department of Anesthesiology, University of California, Los Angeles

²²Department of Anesthesiology and Critical Care Medicine, Johns Hopkins University

²³Department of Anesthesiology, University of California, San Francisco

²⁴Department of Anesthesiology, Northwestern University Feinberg School of Medicine

²⁵Schachtel Associates, Inc.

²⁶Department of Anesthesiology and Pain Management, Brigham and Women’s Hospital

²⁷Department of Anesthesiology, University of California, San Francisco

²⁸Center for Pain Relief, University of Washington Medical Center

²⁹Swedish Medical Group

³⁰EMLine

³¹Department of Anesthesiology and Pain Medicine, University of Washington

³²Children’s Hospital of Wisconsin

³³Department of Anesthesiology, Johns Hopkins University

³⁴Department of Anesthesiology, Tufts University School of Medicine

³⁵University of Rochester Medical Center, School of Medicine and Dentistry

³⁶Department of Anesthesiology and Pain Medicine, University of Washington

^✉

Corresponding Author: Michael Kent MD, CDR MC USN, 11300 Rockville Pike Suite 709, Rockville, MD 20852, Phone: (310) 922-5333, Fax: (301) 816-4705, Kentml@gmail.com

PMCID: PMC7323793 NIHMSID: NIHMS1586094 PMID: 28495013

Abstract

With the increasing societal awareness of the prevalence and impact of acute pain, there is a need to develop an acute pain classification system that both reflects contemporary mechanistic insights and helps guide future research and treatment. Existing classifications of acute pain conditions are limiting, with a predominant focus on the sensory experience (e.g. pain intensity) and pharmacologic consumption. Consequently, there is a need to more broadly characterize and classify the multidimensional experience of acute pain.

As a complement to a taxonomy recently developed for chronic pain, the Analgesic, Anesthetic, and Addiction Clinical Trial Translations, Innovations, Opportunities, and Networks (ACTTION) public-private partnership with the U.S. Food and Drug Administration, the American Pain Society (APS), and the American Academy of Pain Medicine (AAPM) convened a consensus meeting of experts to develop an acute pain taxonomy using prevailing evidence. Key issues pertaining to the distinct nature of acute pain are presented followed by the agreed upon taxonomy. The ACTTION-APS-AAPM Acute Pain Taxonomy will include the following dimensions: 1) Core Criteria 2) Common Features 3) Modulating Factors 4) Impact/Functional Consequences 5) Putative Pathophysiologic Pain Mechanisms. Future efforts will consist of working groups utilizing this taxonomy to develop diagnostic criteria for a comprehensive set of acute pain conditions.

Introduction

In contrast with the pathophysiologic state of chronic pain, acute pain exists as one of life’s core experiences, inevitably experienced by nearly all, and evolutionarily preserved to serve a critical role in protecting the host against a myriad of threats. Despite this critical role in protecting the host, acute pain can be associated with suffering and a reduction in physical function and productivity – thereby causing a significant burden on the person, their family and society as a whole. It is now appreciated that acute pain represents a major public health problem.

One of the challenges to both researchers and clinicians is in understanding the distinction between acute and chronic pain. This distinction is important as a better understanding of acute pain may help us to devise therapies to prevent the development of chronic pain. Furthermore, better classification of these pain conditions will help promote more safe, effective and targeted treatments for individuals suffering from acute pain (i.e. Precision Medicine). Unfortunately, we currently lack precision when discussing the measurement, treatment, research, or even public policy related to acute pain. We therefore need an organized taxonomy of acute pain that establishes a set of common concepts, diagnostic criteria, features and mechanisms that defines and categorizes the multidimensional aspects of acute pain. This classification will then promote future research into mechanisms, prevention and treatments for acute pain.

In 2012, an effort to enhance the precision of dialog about chronic pain was initiated by the Analgesic, Anesthetic, and Addiction Clinical Trial Translations, Innovations, Opportunities, and Networks (ACTTION) and the American Pain Society (APS). This initiative subsequently developed the ACTTION-APS Pain Taxonomy (AAPT) with the objective of creating an “evidence-based chronic pain taxonomy based on a consistently-applied multidimensional framework”(1). Taxonomy in this sense refers to an organization of concepts arranged using hierarchal relationships. The AAPT sought to develop a hierarchical arrangement of characteristics of chronic pain conditions to address the research, clinical, and regulatory limitations of the International Association for the Study of Pain (IASP) taxonomy of pain. AAPT performed this by providing a “standardized, systematic, and evidence-based approach to pain classification that incorporates information regarding biopsychosocial mechanisms and that can be applied to all common chronic pain conditions.(2)”

AAPT developed an approach that included 5 dimensions that incorporated emerging evidence, while retaining some conceptual features of existing chronic pain classifications. (Table 1). Further, AAPT proposed specific categories of chronic pain conditions (i.e. peripheral and central nervous system; musculoskeletal; orofacial and cranial; visceral, pelvic and urogenital pain; and disease-associated pains not otherwise specified) that would each be characterized along the 5 AAPT dimensions by separate working groups.

Table 1.

The ACTTION-APS Chronic Pain Taxonomy (AAPT) Multidimensional Framework. Table reused with permission from Dworkin et al. Multidimensional Diagnostic Criteria for Chronic Pain: Introduction to the ACTTION–American Pain Society Pain Taxonomy (AAPT). The Journal of Pain, Vol 17, No 9 (September), Suppl. 2, 2016: pp T1-T9

Dimension	Description
1: Core diagnostic criteria	Symptoms, signs, and diagnostic test findings required for the diagnosis of the chronic pain condition. Includes differential diagnosis considerations.(60)
2: Common features	Additional information regarding the disorder, including common pain characteristics (eg, location, temporal qualities, descriptors), nonpain features (numbness, fatigue), the epidemiology of the condition, and life span considerations, including those specific to pediatric and geriatric populations. These features are important in describing the disorder but are not components of the core diagnostic criteria.(60,61)
3. Common medical and psychiatric comorbidities	Medical and psychiatric disorders that commonly occur with the chronic pain condition. For example, major depression is comorbid with many chronic pain conditions. Also includes chronic overlapping pain conditions, that is, those chronic pain conditions that are comorbid with each other.(62)
4. Neurobiological, psychosocial, and functional consequences	Neurobiological, psychosocial, and functional consequences of chronic pain. Examples include sleep and mood disorders and pain-related interference with daily activities.(63,64)
5: Putative neurobiological and psychosocial mechanisms, risk factors, and protective factors	Putative neurobiological and psychosocial mechanisms contributing to the development and maintenance of the chronic pain condition, including risk and protective factors. Examples include central sensitization, decreased descending inhibition, and somatosensory amplification.(65)

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In 2014, discussions began amongst APS, ACTTION and the AAPM about the value of developing a taxonomy of acute pain. Such discussions were spurred by a resurgent interest in acute pain, including increased recognition of the societal burden of the transition from acute to chronic pain. While a prior working definition of acute pain was formulated by the AAPM Acute Pain Medicine Special Interest Group in 2015 (Table 2), it was apparent that work was needed to further characterize the complex nature of acute pain. A preliminary step in conducting this work was a state-of-the-science expert report that summarized existing literature to inform practice education, research and health policy(3). The report included an important observation that organization and integration of acute pain science has been hampered by the lack of a taxonomic structure necessary to promote widespread utilization and acceptance(3). Given the AAPT’s previous success in defining a taxonomy of chronic pain, a similar methodology was proposed for the creation of a taxonomy of acute pain: the ACTTION-APS-AAPM Pain Taxonomy (AAAPT) for Acute Pain. The principal objective of the first AAAPT meeting was to review the AAPT taxonomy for chronic pain and determine its appropriateness, applicability, and adaptability if extended to acute pain.

Table 2:

AAPM Acute Pain SIG Working Definition of Acute Pain

AAPM APMSIG Working Definition: Acute Pain
Acute pain is the physiologic response to and experience of noxious stimuli that can become pathologic, is normally sudden in onset, time limited, and motivates behaviors to avoid potential or actual tissue injury.

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Importance of an Acute Pain Ontology/Taxonomy

Prevalence of Acute Pain

Despite advances in multimodal analgesia, acute pain remains a pervasive source of suffering. Work by Apfelbaum et al. in 2003 demonstrated that 80% of patients suffered acute pain after surgery, and that 86% of these patients reported moderate, severe or extreme pain(4). Moreover, the majority of these patients experienced worse pain following discharge from the hospital. More recent work by Buvanendran in 2015 demonstrated that 66% of patients reported moderate, severe or extreme pain after surgery, and 59% of patients reported moderate, severe or extreme pain during the first 2 weeks following hospital discharge (5). Within emergency departments, acute pain accounts for up to 78% of ED visits with a reported median pain intensity of 8/10 on an 11-point numeric rating scale (NRS) (6–9). Finally, primary care physicians commonly encounter challenging acute pain scenarios (e.g. subacute post-surgical pain, acute exacerbations of chronic back pain). In a prospective survey of general practitioners providing acute pain management of ambulatory post-surgical patients, Robaux et al. demonstrated a significant need for education and guidelines addressing the diagnosis, optimal treatment, and expected time course for acute pain conditions presenting to the primary care setting(10).

Societal and Clinical Impact

The Institutes of Medicine’s (IOM) report Relieving Pain in America: A Blueprint for Transforming Prevention, Care, Education, and Research drew attention to pain as a major health problem and placed it on the national agenda(11). This report called for work to promote tangible objectives to advance pain treatment, education and research, and acknowledged that not all acute pain is being effectively managed. Such efforts are necessary because those with acute pain are currently not offered comprehensive, integrated, evidence-based assessment and treatments.

Acute pain has broader societal impact beyond the initial suffering imparted by the originating insult. Inadequately managed acute pain can lead to patient dissatisfaction, pathophysiologic sequelae, and maladaptive behaviors(12). With musculoskeletal conditions alone, one in four patients progress from acute to chronic pain contributing to serious long term pain and pain related physical disability (13). The U.S. Department of Health and Human Services National Pain Strategy and the Centers for Disease Control and Prevention (CDC) guidelines on opioid prescriptions for chronic noncancer pain, both recently released, emphasize that chronic pain begins with acute pain (14,15). However, the transition from acute to chronic pain remains difficult to predict and little is known about how to prevent its development(16).

Conversely, unintended consequences of the treatment of acute pain can directly threaten patient safety. For example, there exists a wealth of data on the cardiovascular, renal and gastrointestinal adverse events associated with non-steroidal anti-inflammatory drugs (NSAIDS), and the risk of hepatic toxicity from over-the-counter analgesics containing acetaminophen remain a substantial public health problem (17–20). Public policy debates on acute pain in the United States have recently centered on opioid analgesics and their effects both on near-term patient safety (e.g. respiratory depression, cognitive dysfunction) as well as longer-term issues of opioid use disorders. It is well known that patients who develop opioid use disorders often have their first exposure to opioids during an acute pain episode(21,22). With increasing numbers of surgeries and the push to better control pain, there are concerning trends about increases in both number and dosage of opioid prescriptions following surgery and their contribution to the US opioid epidemic(23). Researchers have recently identified certain surgeries and patient vulnerabilities that are associated with increased likelihood of being on persistent opioids after surgery(24–27). However, much research is needed to determine if preventive strategies can reduce the development of opioid use disorders. An acute pain taxonomy would be an important part of that effort.

Do any Acute Pain Taxonomies exist?

The literature on acute pain assessment and treatment largely focuses on acute pain intensity (e.g. as assessed by Numerical Rating Scales, Verbal Rating Scales, Visual Analog Scales, various facial scales, or observational pain scales) reflecting a one-dimensional approach to acute pain(28). Such approaches are in keeping with the recommendations of multiple organizations in the 1990s advocating for clinically feasible, standardized approaches to pain assessment, further promulgated by core measures utilized in single dose analgesic trials(29). Recent studies have expanded such assessments, classifying the acute ‘pain experience’ through a variety of approaches such as multidimensional pain related patient-reported outcomes and trajectories(30). However, no comprehensive frameworks exist that incorporate mechanistic information in conjunction with pain experience, functional consequences, and psychologic/social impact (i.e. biopsychosocial experience) indexed to a standardized array of acute pain conditions. Further, while numerous sources (e.g., textbooks, conference proceedings) have provided groupings of acute pain conditions (i.e., postsurgical pain, ischemic pain, musculoskeletal pain), such groupings are not unified within a taxonomy.

Impact on research and education initiatives

Not only would the creation of an acute pain taxonomy provide much needed standardization of clinical diagnostic criteria, it also would benefit research and education. Numerous documents describe optimization of acute pain trial designs and call attention to gaps in both the assessment and treatment of acute pain (31,32). For example, Gordon et al. described a need for future randomized-controlled trials (RCTs) and observational studies to include patients with defined phenotypes(31). At present, the majority of acute pain studies lack the foundation of a comprehensive acute pain taxonomy to codify inclusion and exclusion criteria, and generally do not capture the biopsychosocial outcomes (e.g. pain behavior, pain interference, physical function, sleep disturbance, self-efficacy, social satisfaction, etc.) related to acute pain(33). For example, a recent meta-analysis of 15 RCTs addressing acute post-mastectomy pain shows a predominant focus on pain intensity with little mention of functional or biopsychosocial measures(34). However, a growing number of investigations are utilizing multidimensional measures to predict post-operative outcomes and embrace such measures to determine analgesic efficacy(35–38). Thus, beyond establishing a framework for inclusion and exclusion criteria, an evidence-based acute pain taxonomy offers the potential to illuminate the complex biopsychosocial experience of acute pain and encourage research to move beyond unidimensional measures of pain intensity.

Importantly, a multidimensional approach to an acute pain taxonomy would also provide an essential foundation for training acute pain medicine physicians. In 2014 the Accreditation Council for Graduate Medical Education (ACGME) Board of Directors voted to accept Regional Anesthesia and Acute Pain Medicine as an accredited fellowship, a move that was later approved in October 2016. Since that time, significant effort has led to the creation of a set of competencies embracing the comprehensive practice of acute pain medicine. An evidence-based acute pain taxonomy will advance the structure and content of this curriculum. Moreover, this structure will support ongoing efforts to bolster pain education across medical specialties and ancillary services.

Acute Pain Taxonomy Considerations: Differentiating Acute from Chronic?

The AAAPT Steering Committee convened a meeting of experts in April of 2016 with the goal of addressing the need for a comprehensive acute pain taxonomy. This two-day conference began with discussions on (1) the need for formal taxonomies for pain, and (2) whether initial efforts in developing a taxonomy for chronic pain by the AAPT could serve as a basis for developing an acute pain taxonomy. Presentations on the historical contexts of acute pain through both ancient and modern history segued into a review of known biological mechanisms of acute pain (Table 3). Discussions then turned to principles of taxonomic organization and the validity and reliability of diagnostic criteria as a means of informing further development. Follow on discussions focused on specific types of acute pain including postoperative pain, acute pain related to trauma and burn, visceral pain, acute cancer pain, acute neuropathic pain, acute musculoskeletal pain, acute orofacial pain, and acute pain in special populations such as pediatrics. These discussions culminated in a group discussion on developing a multidimensional structure for the acute pain taxonomy based upon the AAPT chronic pain initiative.

Table 3:

Presentation topics during AAAPT taxonomy development meeting.

Presented Topics
AAPT Chronic Pain Effort (RF/RD)
Distinctions among acute, subacute, and chronic pain (DC)
Pathophysiologic mechanisms and acute pain conditions (TB)
Taxonomy of acute pain conditions (PT)
Acute surgical/procedural pain (CW)
Acute trauma pain (CB)
Acute musculoskeletal pain (SS)
Acute visceral pain (MK)
Cancer/immune mediated acute pain (KT)
Acute neuropathic pain (SR)
Acute orofacial pain (PD)
Acute pain in pediatric, geriatric, and special populations (SW)
Approached to providing an evidence base for acute pain diagnostic criteria (SB)

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Time-based criteria

In the AAAPT discussions, differentiation of acute pain from chronic pain quickly emerged as a principal topic, with an emphasis on timing as a key differentiator. Historically, the Food & Drug Administration has suggested that pain occurring within 30 days of an insult or injury is considered acute pain, and that after 90 days post-injury/insult such pain is referred to as chronic pain(33,39). Recent CDC guidelines pertaining to opioid prescriptions posit a 72-hour period for acute pain treatment of non-traumatic and non-surgical origins(14). Other experts have variously characterized durations of acute pain ranging from 7 to 14 days, with numerous examples throughout the perioperative, emergency department, and primary care settings. The heterogeneity of definitions of acute pain with respect to delineations of time intervals, as well as clinical contexts and excluded patient populations, highlights the gaps and opportunities raised with most of the a priori time thresholds.

In the search for a definitive cut-point between acute and chronic pain, it is important to consider the perspective that acute and chronic pain are not entirely ‘separate’ entities, but rather different aspects along a continuum of pain(40). Given that perspective, clear separation of acute from chronic pain may be impossible, and a focus on ‘at what time’ acute pain becomes chronic may be misguided or misleading and unnecessary. Our evolutionary approach thus follows that of the AAPT effort on chronic pain; we simply do not have sufficient mechanistic data at this time to render a ‘revolutionary’ consideration of the acute to chronic transition. Given numerous examples of prolonged and/or repetitive nociception/pain events that do not progress into chronic pain, future iterations of the AAAPT taxonomy may be able to better focus on the ‘why’ and ‘how’ for the transition between acute and chronic pain rather than solely its temporal parameters.

Despite concerns regarding a formal cut-off point for acute pain, AAAPT adopted the following time-based definition of acute pain for pragmatic and heuristic purposes at this time:

Acute pain is considered to last up to 7 days, with the following qualifications:

Its duration reflects the mechanism and severity of the underlying inciting event.
Prolongations to 7–30 days are common.
Prolongations beyond the duration of acute pain but not extending past 90 days post onset/injury are common. This refers to the ill-defined but important period of “subacute” pain that warrants further specification and consideration in future taxonomic, research, and regulatory efforts.
Our understanding of pain mechanisms is currently insufficient to link these durations to specific physiologic mechanisms.

Unique Attributes of Acute Pain

Apart from the temporal differentiation separating acute and chronic pain, there are other characteristics which differentiate the two conditions. One of the foremost differences between acute and chronic pain remains the ambiguity of its contextual meaning. Acute pain has often been considered a protective mechanism against further injury that may facilitate recovery from injury. Those aspects of acute pain that are normative, protective and helpful deserve special attention as they contrast starkly with chronic pain, which is invariably considered pathologic with no direct benefit to the patient. Such contrasts are not unique to acute and chronic pain. For instance, immune function and inflammation are generally considered normative, protective responses against insults yet can generate pathologic states that are life-threatening (e.g. sepsis, autoimmune disease)(41,42). Notably, as with allergy, inflammation, anaphylaxis and sepsis, the transition points seem key, yet the nature of the points of inflection remain enigmatic.

Mechanism-based

Similar to the AAPT chronic pain experience, it was hoped that the AAAPT could inform its dimensional constructs by mapping onto underlying pain mechanisms. As with chronic pain, it was agreed that the current understanding of acute pain mechanisms poorly differentiates between acute and chronic pain and is often insufficient to distinguish amongst many types of acute pain conditions. One of the foremost examples of such a failure is the intertwined nature of the pathophysiologic mechanisms (e.g. nociceptive, neuropathic, inflammatory, musculoskeletal) contributing to acute pain. Since each of these components is present in nearly all acute pain conditions, distinguishing amongst acute pain conditions according to their nociceptive, neuropathic or inflammatory components is presently infeasible. A similar issue arises in considering biochemical mediators, since current evidence suggests that acute and chronic disease states often display similar profiles of peripheral mediators.

Another approach to differentiate between acute and chronic pain, or among acute pain types, is to consider whether the mechanism of sensitization is peripheral or central. Although acute pain may initially involve prominent peripheral sensitization, it may also occur during chronic pain and therefore discourages reliance upon criterion of peripheral sensitization as a key differentiator between acute and chronic pain. On the other hand, central sensitization seems to play a larger role (and has been characterized more extensively) in chronic pain conditions but yet is evident in acute pain as well. Future research will be needed to better characterize the relative contributions of peripheral and central sensitization to the overall acute pain process – and its transition to chronic pain.

The presence and nature of tissue injury probably differentiates best between acute and chronic pain, as well as amongst different types of acute pain conditions. At the level of tissue injury, distinct profiles of injured structures, tissue-specific mediators, receptors, and responses may help differentiate acute pain conditions. For instance, the high affinity receptor (trkA) for the nociceptive mediator nerve growth factor (NGF) is expressed in notably higher levels in visceral bladder afferent versus cutaneous sensory afferents(43). Further, acute pain stemming from periosteal injury has distinct mechanisms, mediators, and transmission compared with acute pain stemming from cutaneous injury. While many examples of acute tissue injury involve damage to an array of tissues (post-traumatic or post-surgical models), other etiologies that are more tissue specific. For example, acute neuropathic pain may be in part initiated by infectious and inflammatory injury more specifically to neural structures, such as dorsal root ganglion neurons. Similarly, certain types of acute pain are strongly associated with a particular anatomic location, e.g. fracture or burn pain.

Dimensional Considerations

Given the usefulness of the AAPT multidimensional framework, the AAAPT undertook a similar approach to organizing various acute pain conditions. In the consensus approach that emerged from the AAAPT discussions, acute pain and chronic pain are considered subclasses of pain. Acute pain conditions are broadly characterized according to the 5 dimensions that are described below. Specific categories of prototypical acute pain conditions would be differentiated according to these 5 dimensions. Notably in this construct, each dimension can be further organized as needed during future iterations. A strategic decision was made to defer discussions on acute pain assessment and treatment for a future effort.

DIMENSIONS

Discussion on how to categorize acute pain conditions began with the 5 dimensions used for the AAPT. These were extended to consider 10–12 dimensions, before then collapsing back to a final 5 dimensions aligned with, but differing from, the AAPT chronic pain dimensional framework. The rationale for this approach included recognition of the close link between acute and chronic pain, and the potential benefits of aligning their dimensional structures for research and practice updates. The AAAPT specified that no one dimension be considered to be more important than or superior to the others. The 5 dimensions for the AAAPT were finalized as (1) core criteria, (2) common features, (3) modulating factors, (4) impact/functional consequences, and (5) putative pathophysiologic pain mechanisms. (Table 4)

Table 4:

AAAPT Acute Pain Dimensions

Dimension 1: Core Criteria	Specifies the inciting event, timing from the event, and tissue involved. Inciting events descriptions include ICD10x diagnostic and/or procedure codes where possible.
Dimension 2: Common Features	Characterizes the acute pain condition through common pain variables (symptoms, signs, quality). Emphasizes temporal trajectory, physical spatial distribution, and recovery expectations.
Dimension 3: Modulating factors	Includes comorbidities (i.e. opioid tolerance) as well as sociodemographic, biopsychosocial, and surgical factors that may modulate the acute pain experience. Biopsychosocial risk factors (e.g., catastrophizing) for significant acute pain are considered here.
Dimension 4: Impact/Functional Consequences	Describes the recovery trajectory including the interrelations of physical, social, psychologic, and vocational consequences resulting from the acute pain condition.
Dimension 5: Putative Mechanisms	Includes the neurobiological mechanisms related to the acute pain condition. Considers all phases of the acute pain experience and identifies risk factors for development of significant acute pain. Addresses genetic and mechanism based processes to guide treatment.

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Dimension 1: Core Criteria

Core Criteria represent the key features of a given acute pain condition that permit it to be diagnosed and distinguished from other acute pain conditions. Unlike the AAPT Dimension 1 for chronic pain which emphasizes the clinical features of the pain condition itself, the Core Criteria here put greater emphasis on the nature of the inciting event. This is because in many cases, distinct acute pain conditions may not differ so much in their characteristic signs and symptoms, but rather, in their inciting event, a feature not always identifiable in chronic pain. Moreover, the inciting event would often be associated with a specific International Classification of Disease Version 10 (ICD10x) diagnostic or procedure code that in turn would link the acute pain taxonomy to established diagnostic and procedural ontologies. The international standardization of the ICD system links this Dimension to a broader array of efforts to codify various classification systems used throughout healthcare. This feature also permits the AAAPT taxonomy to align with existing clinical entities. Further, this approach enables a mechanism to remap the existing dimensional framework to future disease classification schemas according to the prescribed approaches normally specified during such ICD transitions.

Another key aspect of Dimension 1 is the time elapsed from the inciting event to the observation of the patient, which is critical for defining the condition as ‘acute’. If not specified, the time from the inciting event within this framework is presumed to follow the proposed time-based criteria for acute pain described above.

Core Criteria are intended to be the defining aspects of each condition. They differ from Dimension 2: Common Features, in that the latter is intended to be a more comprehensive and descriptive collection of characteristics of each acute pain condition that are not necessary for a diagnosis.

Dimension 2: Common Features

Attributes of this dimension include common pain-related signs, symptoms, and qualities of each acute pain condition. Special emphasis was placed on three additional attributes in this category: temporal trajectory, spatial and anatomical distribution, and anticipated recovery. Current and anticipated temporal trajectories (i.e. characteristic changes in a given pain measure over time in the acute phase) are key elements given their impact on both treatment as well as the acute to chronic transition. Likewise, spatial and anatomical distribution is intended to reflect not only radiation but also peripheral, and potentially central, sensitization. Anticipated recovery refers to the expected duration of recovery, but could also be considered a binary response. For example, patients suffering from an uncomplicated ankle sprain will substantially recover pre-injury function, while patients suffering from hemipelvectomy for sarcoma will likely suffer from persistent pain and loss of functioning stemming in part from this pain. Although it is a specific attribute distinct from other features, anticipated recovery is frequently impacted by Core Criteria (Dimension 1), Modulating Factors (Dimension 3), Impact/Functional Consequences (Dimension 4), and Putative Pain Pathophysiologic Mechanisms (Dimension 5).

Dimension 3: Modulating Factors

Modulating factors include not only comorbid medical conditions, but also sociodemographic, biological, clinical, behavioral and affective conditions likely to modulate the acute pain experience (e.g., pain catastrophizing, state anxiety, opioid tolerance, evidence of central sensitization, adverse childhood experiences) (36,37,44–46). These factors may include factors pertaining to spatiotemporal summation and diffuse noxious inhibitory control, which more recently has been termed conditioned pain modulation to specify ‘psychosocial paradigms in which a conditioning stimulus is used to affect a test stimulus”(47–50). Dimension 3 strongly considers the context of the inciting event. This context includes not just the events surrounding the inciting event of Dimension 1, but also the social setting in which the patient lives and works. Such environmental factors may extend to the treatment environment and clinicians, that may influence which diagnostic and therapeutic interventions are offered. For example, following a significant acute pain event, availability of analgesic modalities/techniques is highly dependent on the environment of care (clinic, rural hospital, large tertiary care center). Previous pain experiences may be included here. Finally, a variety of neurobiological mechanisms may also modulate the acute pain experience. While far from condition specific, such mechanisms may serve as risk factors for significant acute pain by either impacting pain sensitivity (e.g. genetic variants of COMT, TRPA1), or influencing treatment options such as in drug metabolism/receptor interaction (e.g. genetic variants of CYP2D6, OPRM1) (51–55).

Dimension 4: Impact/Functional Consequences

The fourth dimension describes the recovery trajectory including the interrelations of physical, social, psychologic, and vocational consequences resulting from the acute pain condition. This dimension highlights that in acute pain syndromes, the acute pain itself may not be the principal factor requiring attention, but rather an important hurdle to recovery from the principal diagnosis/procedure. For example, patients undergoing total hip arthroplasty reporting severe pain also report significant disturbances in social relations and mood(56). Operationally, The National Pain Strategy has taken the step of defining “high-impact chronic pain” as “being associated with substantial restriction of participation in work, social, and self-care activities for six months or more.” Similar definitions could also be applied to “high-impact acute pain”.

Dimension 5: Putative Pain Pathophysiologic Mechanisms

When possible, this dimension characterizes pain-relevant neurobiologic pathways prior to, during, and after the inciting event. This dimension delineates the step-by-step natural history of nociceptive, neuropathic, and inflammatory processes that occur at the site of injury extending through cerebral processing. One example would be activation of visceral nociceptive afferents (e.g. TRPV1 activation in urothelial cells) that transmit noxious stimuli via autonomic ganglia through a variety of spinal pathways (e.g. spinohypothalamic) ultimately processed in cerebral locations such as the anterior cingulate gyrus(57–59). While we lack the knowledge to classify acute pain conditions on a purely mechanistic basis and many overlapping mediators exist, such condition-specific descriptions provide a platform for future research and clarification. Further, while the exact processes underlying the transition from acute to chronic pain remain nebulous, initial iterations of this taxonomy will consider descriptions of such postulated mechanisms (e.g. peripheral/central sensitization) for at risk acute pain conditions (e.g. amputation, thoracotomy, polytrauma).

Acute Pain Categories

Organization of specific prototypical acute pain conditions diverged from the AAPT model in allowing two broad categories, within which particular conditions would be placed (Table 5). The first category specifically considers acute pain related to surgery, including procedural pain. Within this category fall acute pain conditions related to different types of surgery, such that acute pain from appendectomy could be differentiated from acute pain from thoracotomy, knee replacement, or Caesarean delivery. For current purposes, we use the term ‘procedural pain’ to refer to acute pain that exists during the time of a procedure itself, implying the expectation of minimal to no post-procedural discomfort. Examples of this might include percutaneous insertion of an intravenous catheter, endoscopy, cardiac catheterization, or extracorporeal shock wave lithotripsy.

Table 5:

Acute pain categories to be defined under dimensional structure in future working groups.

Acute Pain Categories
Surgical/Procedural	Non Surgical
Cardiovascular Surgery	Acute Neuropathic
Dental Surgery	Acute Ischemic
General Surgery	Musculoskeletal
Neurosurgery	Trauma (Including burns)
Obstetric Surgery	Orofacial
Ophthalmic Surgery	Visceral
Orthopedic Surgery	Special Populations
Otolaryngology	Adolescent
Out of Operating Room Procedures	Cancer
Pediatric Surgery	Elderly
Plastic and Reconstructive Surgery	Labor
Thoracic Surgery	Pediatric/Neonatal/Fetal
Urology	Sickle Cell Other

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One critical rationale for this differentiation between surgical and non-surgical categories of acute pain pertains to the timing, anticipation and possible preventive aspects of scheduled tissue injury. Importantly, this scheduling permits the opportunity to intervene prior to the onset of, and during tissue injury, and to prospectively plan for analgesia and functional recovery in the time immediately following injury. From a mechanistic standpoint, intervention to decrease acute pain in the perioperative/periprocedural period may be key in the effort to block the transition to chronic pain. However, further specification will be necessary to address the role of tissue injury and pain which predates the surgery itself.

The second category comprises acute pain related to non-surgical etiologies. This is a large category, and thus subcategories of nonsurgical pain include trauma (including burn), visceral, orofacial, acute neuropathic, and musculoskeletal, as manifested in the population at large or in special populations (labor, sickle cell, pediatrics, ischemic pain, etc.). Similar to the aforementioned chronic pain taxonomy, this approach is admittedly imperfect, as many of the above acute pain conditions share overlapping characteristics with surgical acute pain (i.e. traumatic laceration versus surgical incision). Indeed, the context, environment, and psychosocial modulating factors may account for greater individual variability of the pain experience than currently available mechanistic characterization of such overlapping conditions.

Further development of the description and taxonomy of each specific acute pain sub-categories will be carried out by several ongoing AAAPT workgroups. Each acute pain condition will be described according to the five AAAPT dimensions, with additional characterization as needed.

Conclusion

This multidimensional framework proposed by the AAAPT provides a taxonomy of acute pain which will allow the various acute pain conditions to be characterized in a uniform fashion. This acute pain taxonomy is intended to be a dynamic framework that may continually evolve alongside ever-emerging evidence on the nature and impact of acute pain. While separate from the AAPT taxonomy of chronic pain conditions, the long-term vision is to establish sufficient understanding of pain such that a standard, unifying model can evolve, linking the proposed dimensions of both the acute and chronic pain taxonomies.

Contributor Information

Michael Kent, Department of Anesthesiology, Walter Reed National Military Medical Center.

Patrick Tighe, Department of Anesthesiology, University of Florida, Gainesville.

Inna Belfer, Center for Drug Evaluation and Research, Food and Drug Administration.

Timothy J Brennan, Department of Anesthesiology, University of Iowa.

Stephen Bruehl, Department of Anesthesiology, Vanderbilt University.

Chad Brummett, Department of Anesthesiology, University of Michigan Health System.

Chester Buckenmaier, III, Defense and Veteran’s Center for Integrative Pain Management, Uniformed Services University.

Asokumar Buvanendran, Department of Anesthesiology, Rush University Medical Center.

Robert I. Cohen, Department of Anesthesiology, Beth Israel Deaconess Medical Center.

Paul Desjardins, Desjardins Associates LLC.

David Edwards, Department of Anesthesiology, Vanderbilt University.

Roger Fillingim, Department of Community Dentistry and Behavioral Science, University of Florida, Gainesvile.

Jennifer Gewandter, Department of Anesthesiology, University of Rochester Medical Center, School of Medicine and Dentistry.

Debra Gordon, Department of Anesthesiology and Pain Medicine, University of Washington.

Robert Hurley, Department of Anesthesiology, Medical College of Wisconsin.

Henrik Kehlet, University of Copenhagen.

John Loeser, Department of Neurological Surgery, Department of Anesthesiology and Pain Medicine.

Sean Mackey, Department of Anesthesiology, Perioperative and Pain Medicine, Stanford University.

Samuel McLean, Department of Emergency Medicine, University of North Carolina, Chapel Hill.

Rosemary Polomano, Department of Biobehavioral Sciences, University of Pennsylvania School of Nursing.

Siamak Rahman, Department of Anesthesiology, University of California, Los Angeles.

Srinivasa Raja, Department of Anesthesiology and Critical Care Medicine, Johns Hopkins University.

Michael Rowbotham, Department of Anesthesiology, University of California, San Francisco.

Santhanam Suresh, Department of Anesthesiology, Northwestern University Feinberg School of Medicine.

Bernard Schachtel, Schachtel Associates, Inc..

Kristin Schreiber, Department of Anesthesiology and Pain Management, Brigham and Women’s Hospital.

Mark Schumacher, Department of Anesthesiology, University of California, San Francisco.

Brett Stacey, Center for Pain Relief, University of Washington Medical Center.

Steven Stanos, Swedish Medical Group.

Knox Todd, EMLine.

Dennis Turk, Department of Anesthesiology and Pain Medicine, University of Washington.

Steven Weisman, Children’s Hospital of Wisconsin.

Christopher Wu, Department of Anesthesiology, Johns Hopkins University.

Daniel Carr, Department of Anesthesiology, Tufts University School of Medicine.

Robert Dworkin, University of Rochester Medical Center, School of Medicine and Dentistry.

Gregory Terman, Department of Anesthesiology and Pain Medicine, University of Washington.

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[R1] 1.Fillingim RB, Bruehl S, Dworkin RH, Dworkin SF, Loeser JD, Turk DC, et al. The ACTTION-American Pain Society Pain Taxonomy (AAPT): An Evidence-Based and Multidimensional Approach to Classifying Chronic Pain Conditions. The Journal of Pain. Elsevier; 2014. March 1;15(3):241–9. [DOI] [PMC free article] [PubMed] [Google Scholar]

[R2] 2.Merskey H, Bogduk N. Classification of Chronic Pain. International Assn for the Study of Pain; 1994. 1 p. [Google Scholar]

[R3] 3.Tighe P, Buckenmaier CC, Boezaart AP, Carr DB, Clark LL, Herring AA, et al. Acute Pain Medicine in the United States: A Status Report. Pain Medicine. 2015. September 1;16(9):1806–26. [DOI] [PMC free article] [PubMed] [Google Scholar]

[R4] 4.Apfelbaum JL, Chen C, Mehta SS, Gan TJ. Postoperative Pain Experience: Results from a National Survey Suggest Postoperative Pain Continues to Be Undermanaged. Anesthesia & Analgesia. 2003. August 1;97(2):534–40. [DOI] [PubMed] [Google Scholar]

[R5] 5.Buvanendran A, Fiala J, Patel KA, Golden AD, Moric M, Kroin JS. The Incidence and Severity of Postoperative Pain following Inpatient Surgery. Pain Medicine. The Oxford University Press; 2015. December;16(12):2277–83. [DOI] [PubMed] [Google Scholar]

[R6] 6.Tanabe P, Buschmann M. A prospective study of ED pain management practices and the patient’s perspective. J Emerg Nurs. 1999. June;25(3):171–7. [DOI] [PubMed] [Google Scholar]

[R7] 7.Johnston CC, Gagnon AJ, Fullerton L, Common C, Ladores M, Forlini S. One-week survey of pain intensity on admission to and discharge from the emergency department: a pilot study. J Emerg Med. 1998. May;16(3):377–82. [DOI] [PubMed] [Google Scholar]

[R8] 8.Todd KH, Ducharme J, Choinière M, Crandall CS, Fosnocht DE, Homel P, et al. Pain in the Emergency Department: Results of the Pain and Emergency Medicine Initiative (PEMI) Multicenter Study. The Journal of Pain. 2007. June;8(6):460–6. [DOI] [PubMed] [Google Scholar]

[R9] 9.Cordell WH, Keene KK, Giles BK, Jones JB, Jones JH, Brizendine EJ. The high prevalence of pain in emergency medical care. The American Journal of Emergency Medicine. 2002. May;20(3):165–9. [DOI] [PubMed] [Google Scholar]

[R10] 10.Robaux S, Bouaziz H, Cornet C, Boivin JM, Lefèvre N, Laxenaire MC. Acute postoperative pain management at home after ambulatory surgery: a French pilot survey of general practitioners’ views. Anesthesia & Analgesia. 2002. November;95(5):1258–62. [DOI] [PubMed] [Google Scholar]

[R11] 11.Institute of Medicine (US) Committee on Advancing Pain Research, Care, and Education. Relieving Pain in America: A Blueprint for Transforming Prevention, Care, Education, and Research. Washington (DC): National Academies Press (US); 2011. [PubMed] [Google Scholar]

[R12] 12.Sinatra R. Causes and Consequences of Inadequate Management of Acute Pain. Pain Medicine. Blackwell Publishing Inc; 2010. December 1;11(12):1859–71. [DOI] [PubMed] [Google Scholar]

[R13] 13.Walsh NE, Brooks P, Hazes JM, Walsh RM, Dreinhöfer K, Woolf AD, et al. Standards of care for acute and chronic musculoskeletal pain: the Bone and Joint Decade (2000–2010). Arch Phys Med Rehabil. 2008. September;89(9):1830–45. [DOI] [PubMed] [Google Scholar]

[R14] 14.Dowell D, Haegerich TM, Chou R. CDC Guideline for Prescribing Opioids for Chronic Pain - United States, 2016. MMWR Recomm Rep. 2016;65(1):1–49. [DOI] [PubMed] [Google Scholar]

[R15] 15.Interagency Pain Research Coordinating Committee National Pain Strategy. April 2015.

[R16] 16.Katz J, Seltzer Z. Transition from acute to chronic postsurgical pain: risk factors and protective factors. Expert Rev Neurother. Informa HealthcareLondon; 2009. May;9(5):723–44. [DOI] [PubMed] [Google Scholar]

[R17] 17.Salvo F, Fourrier-Réglat A, Bazin F, Robinson P, Riera-Guardia N, Haag M, et al. Cardiovascular and gastrointestinal safety of NSAIDs: a systematic review of meta-analyses of randomized clinical trials. Clin Pharmacol Ther. 2011. June;89(6):855–66. [DOI] [PubMed] [Google Scholar]

[R18] 18.Scheiman JM. NSAID-induced Gastrointestinal Injury: A Focused Update for Clinicians. Journal of clinical gastroenterology. 2016. January;50(1):5–10. [DOI] [PubMed] [Google Scholar]

[R19] 19.Ng SC, Chan FKL. NSAID-induced gastrointestinal and cardiovascular injury. Current opinion in gastroenterology. 2010. November;26(6):611–7. [DOI] [PubMed] [Google Scholar]

[R20] 20.Mathiesen O, Wetterslev J, Kontinen VK, Pommegraard HC, Nikolajsen L, Rosenberg J, et al. Adverse effects of perioperative paracetamol, NSAIDs, glucocorticoids, gabapentinoids and their combinations: a topical review. Acta Anaesthesiol Scand. 2014. November 1;58(10):1182–98. [DOI] [PubMed] [Google Scholar]

[R21] 21.Calcaterra SL, Yamashita TE, Min S-J, Keniston A, Frank JW, Binswanger IA. Opioid Prescribing at Hospital Discharge Contributes to Chronic Opioid Use. J Gen Intern Med. Springer US; 2016. May;31(5):478–85. [DOI] [PMC free article] [PubMed] [Google Scholar]

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PERMALINK

The ACTTION-American Pain Society-American Academy of Pain Medicine Pain Taxonomy (AAAPT): A Multidimensional Approach to Classifying Acute Pain Conditions.

Michael Kent, MD

Patrick Tighe, MD

Inna Belfer, MD, PhD

Timothy J Brennan, MD, PhD

Stephen Bruehl, PhD

Chad Brummett, MD

Chester Buckenmaier III, MD

Asokumar Buvanendran, MD

Robert I Cohen, MD

Paul Desjardins, DMD, PhD

David Edwards, MD, PhD

Roger Fillingim, PhD

Jennifer Gewandter, PhD

Debra Gordon, RN, DNP

Robert Hurley, MD, PhD

Henrik Kehlet, MD, PhD

John Loeser, MD

Sean Mackey, MD, PhD

Samuel McLean, MD, MPH

Rosemary Polomano, PhD, RN

Siamak Rahman, MD

Srinivasa Raja, MD

Michael Rowbotham, MD

Santhanam Suresh, MD

Bernard Schachtel, MD, PhD

Kristin Schreiber, MD, PhD

Mark Schumacher, MD, PhD

Brett Stacey, MD

Steven Stanos, DO

Knox Todd, MD, MPH

Dennis Turk, PhD

Steven Weisman, MD

Christopher Wu, MD

Daniel Carr, MD

Robert Dworkin, PhD

Gregory Terman, MD, PhD

Abstract

Introduction

Table 1.

Table 2:

Importance of an Acute Pain Ontology/Taxonomy

Prevalence of Acute Pain

Societal and Clinical Impact

Do any Acute Pain Taxonomies exist?

Impact on research and education initiatives

Acute Pain Taxonomy Considerations: Differentiating Acute from Chronic?

Table 3:

Time-based criteria

Unique Attributes of Acute Pain

Mechanism-based

Dimensional Considerations

DIMENSIONS

Table 4:

Dimension 1: Core Criteria

Dimension 2: Common Features

Dimension 3: Modulating Factors

Dimension 4: Impact/Functional Consequences

Dimension 5: Putative Pain Pathophysiologic Mechanisms

Acute Pain Categories

Table 5:

Conclusion

Contributor Information

References

ACTIONS

PERMALINK

RESOURCES

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