Alcohol Use Disorder — Clinical Presentation

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controversies · captured 2026-05-17 18:48:35 · status: pending-review

As of today, several active clinical, scientific, and policy controversies shape the understanding of Alcohol Use Disorder (AUD) and its clinical presentation. These debates concern the fundamental diagnostic framework, the significance of specific symptoms, variations in presentation across different populations, and the role of biological markers in diagnosis.

1. The Dimensional versus Categorical Approach to Diagnosis

A central controversy in the clinical presentation of AUD revolves around the shift from a categorical to a dimensional model in the Diagnostic and Statistical Manual of Mental Disorders, Fifth Edition (DSM-5).

Major Positions:

  • Pro-Dimensional/Spectrum Approach: This position, reflected in the DSM-5, argues that AUD exists on a continuum of severity, ranging from mild to severe. Proponents suggest this model better captures the heterogeneity of the disorder and can help identify individuals with problematic drinking who may not have met the stricter criteria for "abuse" or "dependence" in the previous DSM-IV. This approach aims to reduce stigma and encourage earlier intervention by framing alcohol problems as existing on a spectrum. The American College of Physicians supports the view of AUD as a treatable chronic medical condition that should be addressed through expanded evidence-based public health and healthcare initiatives.

  • Critiques of the Dimensional Approach: Critics raise concerns that the dimensional approach, with its lower diagnostic threshold of two symptoms for a mild AUD, may lead to over-diagnosis and the "medicalization" of what was previously considered at-risk drinking. Some researchers argue that while a dimensional structure is supported by data, the specific threshold for diagnosis remains somewhat arbitrary. There are also arguments that a unidimensional diagnosis, as presented in the DSM-5, may not fully capture the complexity of AUD and that multidimensional models might have better predictive validity for outcomes like heavy drinking. Some studies have shown that the DSM-5 criteria may "inflate" the prevalence of AUD compared to the DSM-IV.

Who Holds Each Position:

  • Pro-Dimensional/Spectrum Approach: The American Psychiatric Association, through the publication of the DSM-5, officially endorses this model. Many researchers and public health advocates also support this approach, emphasizing its potential to improve early detection and reduce the negative consequences of untreated alcohol problems.

  • Critiques of the Dimensional Approach: Some clinicians and researchers express caution about the potential for diagnostic inflation and the blurring of lines between problematic drinking and a clinical disorder. These critiques often emerge from academic and clinical research settings.

Most Recent Primary Source: A 2023 article in Alcohol and Alcoholism discusses the implications of promoting alcohol problems as a continuum for policy and practice, highlighting both the benefits in reducing stigma and the complexities in its application.

2. The Clinical Utility of "Craving" as a Diagnostic Criterion

The inclusion of "craving, or a strong desire or urge to use alcohol" as a diagnostic criterion in the DSM-5 has been a significant and debated change.

Major Positions:

  • Craving as a Core Symptom: Proponents argue that craving is a central feature of addiction and its inclusion improves the diagnostic accuracy of AUD. Research has shown that craving is significantly associated with AUD severity, levels of alcohol consumption, and the likelihood of relapse. Studies have found that craving loads well onto a single factor structure for AUD, supporting its inclusion as a core symptom.

  • Challenges in Defining and Measuring Craving: A key controversy lies in the subjective nature of craving and the lack of a universally accepted definition and measurement tool. This can lead to inconsistencies in how the criterion is applied in clinical and research settings. Some studies have found that the prevalence of endorsed craving can be relatively low in non-treatment-seeking populations, raising questions about its utility across the full spectrum of AUD. There is also debate about whether self-report measures of craving, like the Penn Alcohol Craving Scale (PACS), accurately capture the diagnostic construct.

Who Holds Each Position:

  • Craving as a Core Symptom: The DSM-5 Task Force, influenced by a body of research on the neurobiology of addiction, advocated for its inclusion. Many addiction researchers and clinicians view craving as a critical component of the clinical picture of AUD.

  • Challenges in Defining and Measuring Craving: This position is held by researchers and clinicians who emphasize the need for more objective and standardized methods for assessing craving. They highlight the potential for variability in interpretation of this subjective symptom.

Most Recent Primary Source: A 2019 study published in Drug and Alcohol Dependence examined the convergence between the Penn Alcohol Craving Scale and diagnostic interviews for assessing alcohol craving, highlighting the ongoing challenges in measurement.

3. Sex and Gender Differences in Clinical Presentation: The "Telescoping Effect"

There is an ongoing debate about the extent and clinical implications of differences in how AUD presents in women compared to men, with the "telescoping effect" being a central point of contention.

Major Positions:

  • Support for the Telescoping Effect: This position posits that women typically start drinking later than men but experience an accelerated progression from the onset of drinking to the development of AUD and related health problems. Proponents point to biological factors, such as differences in alcohol metabolism, and psychosocial factors, such as higher rates of co-occurring mood and anxiety disorders, as contributing to this phenomenon. This perspective suggests that women may require different prevention and treatment strategies that account for their unique clinical course.

  • Questioning the Universality of the Telescoping Effect: Some large-scale population studies have found little evidence for a universal telescoping effect in the general population. These studies suggest that while gender differences exist, the accelerated progression to dependence may not be as pronounced or consistent as previously thought, and in some cases, men may show a shorter time from first use to dependence, particularly in younger cohorts. This position argues for a more nuanced understanding of gender differences that considers various social and cultural factors.

Who Holds Each Position:

  • Support for the Telescoping Effect: Many researchers in the fields of addiction and women's health support this model, citing a substantial body of clinical and preclinical evidence.

  • Questioning the Universality of the Telescoping Effect: This position is held by some epidemiologists and researchers who analyze large, population-based datasets. They argue that findings from clinical samples may not be generalizable to the broader population.

Most Recent Primary Source: A 2025 narrative review in the Journal of Substance Abuse Treatment examines the evidence for the telescoping hypothesis from a biopsychosocial perspective, concluding that a complex interplay of factors increases the risk for AUD onset and progression in women through an internalizing pathway.

4. Atypical Presentations in Adolescents and Older Adults

A significant controversy exists regarding the applicability of the standard DSM-5 diagnostic criteria for AUD to adolescents and older adults, who may present with atypical symptoms.

Major Positions:

  • Need for Age-Specific Diagnostic Considerations for Adolescents: This position argues that some DSM-5 criteria, such as tolerance and withdrawal, may be less common or have different clinical significance in adolescents. Conversely, behaviors like hazardous use may be more prevalent but not necessarily indicative of a severe disorder. Proponents advocate for the development of age-specific diagnostic criteria or, at minimum, a more developmentally informed application of the existing criteria. The American Academy of Pediatrics notes limitations in applying adult-derived diagnostic criteria to adolescents.

  • Underdiagnosis and Misattribution in Older Adults: For older adults, the clinical presentation of AUD can be masked by or misattributed to other age-related medical and psychiatric conditions. Social and occupational impairments may be less apparent in retired individuals. This position highlights the need for increased awareness and routine screening in geriatric populations, as standard diagnostic cues may be less informative.

Who Holds Each Position:

  • Need for Age-Specific Diagnostic Considerations for Adolescents: This view is held by many child and adolescent psychiatrists, pediatricians, and developmental psychologists who specialize in substance use.

  • Underdiagnosis and Misattribution in Older Adults: Geriatricians, geriatric psychiatrists, and public health advocates focused on aging populations champion this position.

Most Recent Primary Source: A 2024 article in Pediatrics in Review discusses the diagnosis and treatment of adolescent alcohol use disorders, highlighting the use of screening tools and the application of DSM-5 criteria in this population. A 2021 article in Current Psychiatry Reports provides an overview of the evaluation and management of AUD in older adults, emphasizing the challenges in diagnosis.

5. The Role of Biomarkers in Clinical Diagnosis

The utility and limitations of biological markers in the definitive diagnosis of AUD remain a significant area of scientific and clinical debate.

Major Positions:

  • Biomarkers as Adjunctive Tools for Assessing Heavy Drinking: This position acknowledges that traditional biomarkers, such as gamma-glutamyl transferase (GGT) and mean corpuscular volume (MCV), lack the sensitivity and specificity for a standalone diagnosis of AUD. However, they can be useful in combination with clinical assessment to detect recent heavy alcohol consumption and monitor for relapse. Proponents emphasize their objectivity compared to self-report.

  • The Search for a Definitive Diagnostic Biomarker: A major goal in the field is to identify novel biomarkers with high sensitivity and specificity for AUD. This position highlights the limitations of current markers, which can be influenced by other medical conditions and do not definitively indicate the presence of a disorder. The focus of current research is on direct ethanol metabolites (e.g., phosphatidylethanol) and multi-marker panels to improve diagnostic accuracy. There are currently no objective, biologically-based markers that can reliably diagnose AUD or stratify patients for optimal treatment.

Who Holds Each Position:

  • Biomarkers as Adjunctive Tools: This is the current prevailing view among most clinicians and is reflected in clinical practice guidelines. They are seen as one piece of a comprehensive assessment.

  • The Search for a Definitive Diagnostic Biomarker: This position is primarily held by researchers in the fields of biochemistry, genetics, and addiction medicine who are actively working to develop and validate new diagnostic tools.

Most Recent Primary Source: A 2023 critical review in Frontiers in Psychiatry summarizes the state of omics-based biomarkers for alcohol consumption and AUD, concluding that while promising, there are currently no biomarkers to definitively diagnose AUD or guide treatment decisions.

regulatory · captured 2026-05-17 18:47:50 · status: pending-review

Navigating the Treatment Landscape for Alcohol Use Disorder: A Look at Current Guidelines and FDA-Approved Medications

As of today, the approach to treating Alcohol Use Disorder (AUD) is guided by a combination of FDA-approved medications, comprehensive clinical practice guidelines from leading medical societies, and ongoing research and position statements from federal health agencies. These resources provide a framework for the clinical presentation and management of AUD, emphasizing evidence-based pharmacological and psychosocial interventions.

FDA-Approved Medications for Alcohol Use Disorder

The U.S. Food and Drug Administration (FDA) has approved three medications for the treatment of AUD. These medications are intended to be used as part of a comprehensive treatment plan that includes counseling and social support.

  • Disulfiram (Antabuse): First approved in 1951, disulfiram works by causing an unpleasant reaction when alcohol is consumed, including nausea, vomiting, and flushing. This aversive therapy is intended to deter drinking.
  • Naltrexone (Revia, Vivitrol): Available in both oral and long-acting injectable forms, naltrexone blocks the euphoric effects and feelings of intoxication from alcohol. This can help reduce cravings and the amount of alcohol consumed. The injectable form is administered once a month.
  • Acamprosate (Campral): Approved in 2004, acamprosate is thought to work by restoring the balance of certain neurotransmitters in the brain that are disrupted by chronic alcohol use. It is intended to help patients maintain abstinence.

While not FDA-approved specifically for AUD, other medications are sometimes used "off-label" by clinicians based on emerging evidence. These may include topiramate and gabapentin.

Active Clinical Practice Guidelines

Several professional organizations have developed clinical practice guidelines to assist healthcare providers in the diagnosis and treatment of AUD. These guidelines are based on systematic reviews of the scientific evidence and provide recommendations for best practices.

  • American Psychiatric Association (APA): The APA's "Practice Guideline for the Pharmacological Treatment of Patients with Alcohol Use Disorder," published in 2018, provides evidence-based recommendations for the use of medications in the treatment of AUD. The guideline strongly recommends naltrexone and acamprosate for patients with moderate to severe AUD. It also provides guidance on the use of disulfiram and other medications, as well as considerations for patient assessment and treatment planning.

  • American Society of Addiction Medicine (ASAM): ASAM's "Clinical Practice Guideline on Alcohol Withdrawal Management," with its latest update in 2020, is a critical resource for managing the acute phase of alcohol cessation. While focused on withdrawal, it is a foundational component of comprehensive AUD treatment.

  • American College of Gastroenterology (ACG): The ACG released its "Clinical Guideline: Alcohol-Associated Liver Disease" in 2023. This guideline offers specific recommendations for managing AUD in patients with liver disease, a common comorbidity. It suggests considering baclofen, acamprosate, naltrexone, gabapentin, or topiramate for these patients.

  • American Academy of Child and Adolescent Psychiatry (AACAP): A 2025 guideline summary from the AACAP on substance-use disorders in adolescents and young adults addresses problematic alcohol use. For this population, the guideline suggests behavioral interventions such as motivational interviewing and cognitive-behavioral therapy.

Recent Position Statements from Federal Agencies

Federal agencies like the Substance Abuse and Mental Health Services Administration (SAMHSA), the National Institute on Alcohol Abuse and Alcoholism (NIAAA), and the National Institute on Drug Abuse (NIDA) play a crucial role in shaping the understanding and treatment of AUD through research, data collection, and the dissemination of best practices.

  • Substance Abuse and Mental Health Services Administration (SAMHSA): SAMHSA's Treatment Improvement Protocols (TIPs) provide consensus-based, best-practice guidelines for the treatment of substance use disorders. TIP 49, "Incorporating Alcohol Pharmacotherapies Into Medical Practice," offers detailed guidance on the use of FDA-approved medications for AUD. SAMHSA also emphasizes the importance of integrated care, addressing both mental and substance use disorders concurrently.

  • National Institute on Alcohol Abuse and Alcoholism (NIAAA): As the lead federal agency for research on alcohol and health, the NIAAA provides extensive resources for clinicians and the public. Their publications, such as "Helping Patients Who Drink Too Much: A Clinician's Guide," offer practical advice for screening, brief intervention, and referral to treatment. The NIAAA's research priorities continue to focus on developing new and more effective treatments for AUD, including new medications and behavioral therapies.

  • National Institute on Drug Abuse (NIDA): While NIDA's primary focus is on drugs other than alcohol, it often collaborates with the NIAAA on research related to polysubstance use and the neurobiology of addiction. NIDA's research on the brain's reward pathways and the mechanisms of addiction has contributed to a broader understanding of AUD. The institute supports the development of new treatment approaches that could have applications for various substance use disorders, including AUD. In a 2023 letter, the APA provided feedback to NIDA and NIAAA on the proposed use of the term "preaddiction," highlighting the importance of reducing stigma and using evidence-based preventive strategies.

whats-new · captured 2026-05-17 18:47:22 · status: pending-review

As of May 2026, there have been noteworthy developments in the past six months regarding the clinical presentation and treatment landscape of Alcohol Use Disorder (AUD). These changes include a significant FDA action on clinical trial endpoints, emerging results from major clinical trials, and a contentious shift in federal dietary guidelines.

FDA Recognizes New Clinical Trial Endpoint

In a significant move to facilitate drug development for AUD, the U.S. Food and Drug Administration (FDA) has formally recognized a reduction in the World Health Organization (WHO) Risk Drinking Levels (RDLs) as a valid primary endpoint in clinical trials. This decision, announced in September 2025 and officially qualified in February 2025, marks a departure from the traditional focus on complete abstinence as the primary measure of treatment success.

The new endpoint allows for the approval of medications that can demonstrate a clinically meaningful reduction in alcohol consumption, even if patients do not achieve total abstinence. This is expected to encourage more individuals with AUD to seek treatment and may lead to the development of new therapeutic options. A reduction of at least "two risk levels" is now considered a primary endpoint for clinical trials, aligning U.S. policy more closely with the European Medicines Agency.

Promising Results in Clinical Trials

Recent months have seen promising, albeit preliminary, results from clinical trials of novel treatments for AUD:

  • GLP-1 Receptor Agonists: Emerging evidence from late 2025 and early 2026 suggests that GLP-1 receptor agonists, a class of medications primarily used for diabetes and weight loss, may also be effective in reducing alcohol consumption. A randomized controlled trial published in The Lancet showed that semaglutide (Ozempic/Wegovy) led to a significant and sustained reduction in alcohol consumption over six months. Another study specifically in patients with both AUD and obesity found that weekly semaglutide reduced heavy drinking days. While more research is needed, these findings have generated considerable interest in the potential of these drugs for treating AUD.
  • Psychedelic-Derived Therapeutics: A Phase I/IIa clinical trial is underway for CMND-100, a proprietary MEAI-based oral drug candidate for the treatment of AUD. The first cohort of patients completed treatment in this FDA-approved trial in October 2025. The study is assessing the safety, tolerability, and preliminary efficacy of this novel psychedelic-derived therapy.

Shift in Federal Dietary Guidelines

In January 2026, the Department of Health and Human Services (HHS) and the Department of Agriculture (USDA) released the 2025-2030 Dietary Guidelines for Americans. In a significant policy shift, these new guidelines removed specific daily limits for alcohol consumption. The previous recommendation was for men to limit intake to no more than two drinks per day and women to no more than one. The updated guidelines now offer the broader advice to "consume less alcohol for better overall health."

This change has been met with "deep concern" from the American Association for the Study of Liver Diseases (AASLD). The AASLD and other critics argue that the removal of clear, evidence-based limits fails to adequately inform the public about the health risks associated with alcohol consumption, including the link between alcohol and cancer.

No Major Changes in Clinical Guidelines or Other Regulatory Actions

There have been no new major clinical guidelines or consensus statements on the clinical presentation of AUD from organizations such as the American Psychiatric Association (APA) in the past six months. The most recent comprehensive APA practice guideline for the pharmacological treatment of AUD was published in 2018. Similarly, there have been no other significant regulatory actions from SAMHSA, CDC, or NIAAA regarding the clinical presentation of AUD in the specified timeframe. The NIAAA's current strategic plan runs from 2022 to 2026, with the framework established prior to the last six months.

Alcohol Use Disorder: Clinical Presentation

A Knowledge Base for Clinicians, Researchers, and Families


Overview: Why Presentation Matters — and Why It Is So Often Missed

Alcohol use disorder (AUD) is defined under DSM-5 as "a problematic pattern of alcohol use leading to clinically significant impairment or distress" [1]. It is one of the most prevalent conditions in clinical medicine and one of the most consistently under-recognized. Understanding how AUD actually presents — in a primary care exam room, in an emergency department, at a kitchen table — is not a secondary concern. It is the first step toward any intervention.

The epidemiological burden is substantial. A prospective Australian cohort found the cumulative incidence of DSM-5 AUD symptoms from late adolescence to middle adulthood was 58.0% (95% CI 52.3–63.8%), peaking sharply at age 24 and remaining clinically significant through middle adulthood, with 25% of the population showing ongoing or new-onset AUD by age 42 [2]. Despite this prevalence, only approximately 8% of individuals meeting AUD criteria receive care in a specialized facility [3] (Note: this specific figure could not be independently verified against the source abstract — the underlying study supports the general finding but the exact number should be confirmed before publication). In Germany, only about 10% of patients with AUD are treated by the professional help system [stüben-2023-evaluation-primary-health].

The gap between prevalence and recognition is not a footnote. It is the central clinical problem. AUD is undertreated "partly because of the high stigma associated with them, but also because of insufficient systematic screening in primary health care, although effective and cost-effective psychosocial and pharmacological interventions do exist" [4]. Stigma operates not only before identification but after it — as an independent barrier between a positive screen and treatment entry.

One additional finding sharpens the urgency: in a retrospective study of 251,300 Veterans Administration ED encounters associated with alcohol intoxication, 79% of patients had positive AUDIT-C screens within 6 months of their visit [5]. The information was already in the system. The failure was not detection — it was what happened, or did not happen, afterward.

This article synthesizes the available evidence on how AUD presents across clinical and home settings, what screening tools can and cannot tell us, what biomarkers mean and do not mean, and where the evidence is genuinely thin.


Behavioral Signs

Behavioral signs of AUD are the most observable features — visible to family members, employers, and clinicians — yet they are often rationalized or normalized long before they reach clinical attention. Each maps to a specific DSM-5 criterion.

Drinking more or longer than intended (DSM-5 Criterion 1) is among the earliest behavioral signs, yet it is one of the least frequently self-reported. Only 9.0% of regular drinkers endorse this criterion in survey data [6]. This low endorsement rate likely reflects the difficulty people have recognizing loss of control from the inside — what feels like a choice to have "one more" is, over time, a pattern of failed self-regulation.

Persistent desire or unsuccessful efforts to cut down (Criterion 2) often manifests as repeated "rules" about drinking — only on weekends, only after 5 p.m., never before noon — that are quietly abandoned and reset. Family members frequently notice this pattern before the person with AUD does.

Significant time spent obtaining, using, or recovering from alcohol (Criterion 3) includes not only the hours of drinking but the morning-after impairment, the planning of social events around alcohol availability, and the cognitive bandwidth devoted to managing supply.

Craving (Criterion 4) is the only criterion that is purely internal, but it has behavioral correlates: irritability when alcohol is unavailable, clock-watching before an acceptable drinking hour, or disproportionate relief when a drink is obtained.

Failure to fulfill major role obligations (Criterion 5) — missed work, neglected parenting responsibilities, declining academic performance — tends to appear later in the disorder's course and is often the sign that prompts family concern or employer action.

Continued use despite social or interpersonal problems (Criterion 6) and giving up important activities (Criterion 7) reflect the progressive narrowing of a person's life around alcohol. Hobbies, relationships, and commitments that once competed with drinking are gradually abandoned.

Recurrent use in physically hazardous situations (Criterion 8) — driving while impaired, operating machinery, mixing alcohol with sedating medications — is a safety concern that may surface in ED presentations or medication reconciliation conversations.

Continued use despite knowledge of a physical or psychological problem (Criterion 9) is clinically important because it distinguishes AUD from heavy social drinking: the person knows the alcohol is causing harm and continues anyway.

Tolerance (Criterion 10) is the most commonly endorsed criterion among regular drinkers — 50.3% in survey data [6]. Its high prevalence and low clinical salience make it a paradox: it is the most common sign and the one least likely to trigger clinical concern on its own.

Withdrawal (Criterion 11) is addressed in detail in the Physical Signs section below.

The striking disparity between tolerance endorsement (50.3%) and social-problem endorsement (10.4%) [6] has a direct clinical implication: a patient presenting with tolerance alone may not trigger suspicion, yet they may already be on the AUD spectrum. Clinicians who wait for role failure or social consequences before considering AUD are seeing the disorder late.


Cognitive Signs

Cognitive features of AUD are less visible than behavioral ones but are often present earlier. They include:

Preoccupation with drinking — persistent thoughts about when the next drink will occur, planning social activities around alcohol, difficulty concentrating on tasks when alcohol is not available.

Craving — the subjective experience of urge or compulsion to drink, which can be triggered by environmental cues (a bar, a stressful situation, a social gathering) and which intensifies with disorder severity.

Difficulty estimating one's own intake — a well-documented phenomenon in which people with AUD consistently underreport consumption, not always deliberately but because the normalization of heavy drinking distorts the reference point for "a lot." This is clinically relevant when interpreting self-reported drinking histories.

Executive function effects — impairments in planning, impulse control, and decision-making that both result from and contribute to AUD. These effects can make it harder for a person to follow through on treatment plans, keep appointments, or resist drinking cues.

Anticipatory reward thinking — the cognitive pattern in which the anticipated relief or pleasure of drinking dominates decision-making, crowding out awareness of consequences. Longitudinal data on drinking motives shows that enhancement motives (drinking to feel good) are the most prevalent and shift with symptom severity over time [nègre-2024-study-efficiency-virtual].

From a lived-experience perspective, these cognitive features are particularly important because they explain why the disorder is often not self-recognized early. As one recovery narrative in the expert panel described, the earliest signs "felt like normal coping or social lubrication from the inside" — a description consistent with the epidemiological finding that diagnostic thresholds are met years after the pattern has taken hold [2].


Physical Signs

Physical signs of AUD span a wide severity range, from subtle early findings to life-threatening complications. They are often the presenting complaint in primary care and emergency settings, even when AUD is not the stated reason for the visit.

Tolerance (the need for markedly increased amounts to achieve the same effect, or markedly diminished effect with the same amount) is the most commonly endorsed criterion [6] and may be the only physical sign present in early-to-moderate AUD.

Withdrawal affects approximately half of people with AUD when they abruptly reduce or stop drinking [7]. This is a clinical safety issue that transforms what appears to be a routine presentation into a potential medical emergency. Withdrawal symptoms range from mild (tremor, diaphoresis, anxiety, insomnia, nausea) to severe (seizures, delirium tremens). The corpus does not include CIWA-Ar protocol data — a significant gap for clinicians managing withdrawal severity assessment. Readers should consult ASAM guidelines for withdrawal management protocols.

Sleep disruption is a common and often underappreciated sign. Alcohol disrupts sleep architecture, suppressing REM sleep and causing early-morning awakening. Patients presenting with persistent insomnia or non-restorative sleep warrant alcohol screening.

Gastrointestinal symptoms — nausea, vomiting, epigastric pain, diarrhea — may reflect gastritis, pancreatitis, or early liver disease. These are frequent indirect presentations in primary care.

Hypertension that is difficult to control despite appropriate medication is a recognized indirect presentation of heavy alcohol use. Clinicians encountering treatment-resistant hypertension should include alcohol screening in the workup.

Dermatologic changes associated with chronic heavy use include facial flushing, spider angiomata, palmar erythema, and in advanced liver disease, jaundice and caput medusae. These are late signs.

Hand tremor — particularly a fine resting tremor that improves with the first drink of the day — is a withdrawal-related sign that may be the presenting complaint in a primary care visit.

Weight changes — both weight gain from caloric intake and weight loss from nutritional neglect — can occur at different stages of AUD.

Alcohol odor at clinical encounters, particularly at morning appointments, is a late and severe sign that should prompt immediate clinical attention and safety assessment.


Presentation in Primary Care

AUD rarely presents in primary care as "I have a drinking problem." It presents as uncontrolled hypertension, persistent insomnia, treatment-resistant anxiety, abnormal liver enzymes, or recurrent GI complaints. Clinicians who screen only when a patient volunteers a drinking concern will miss the majority of cases.

The recommended approach is to screen patients who present with medical or psychosocial problems that might be related to alcohol use, and to order relevant laboratory tests including CBC and liver transaminases including GGT [8]. The AUDIT (score ≥8) is the best-validated screening tool, with a likelihood ratio of 6.5 (95% CI 3.9–11) for AUD [1]. Critically, it performs better in females (LR 6.9, 95% CI 3.9–12) than males (LR 3.8, 95% CI 2.6–5.5) [1] — inverting the common clinical intuition that AUD is primarily a male presentation.

The abbreviated AUDIT-C, widely used in primary care for speed, is substantially less useful for identifying AUD proper (LR 1.8 for males, 2.0 for females) [1]. Clinicians relying solely on AUDIT-C are likely under-identifying cases. The USPSTF recommends screening for risky drinking, yet it is "not always performed consistently or correctly in primary care" [7].

When a positive screen is obtained, the evidence-based pathway is SBIRT: Screening, Brief Intervention, and Referral to Treatment [9]. Brief counseling in ambulatory primary care has the strongest evidence for efficacy in reducing consumption for at-risk drinkers [10]. However, implementation is consistently undermined by time pressure: "time constraints are the most commonly reported barrier to universal alcohol screening" [11]. If there is insufficient time for the screen, there is almost certainly insufficient time for the nuanced, non-judgmental conversation that an effective brief intervention requires.

A practical assessment tool — the Alcohol Symptom Checklist for DSM-5 criteria — showed excellent test-retest reliability in primary care settings (ICC = 0.82, 95% CI 0.77–0.85) [12], suggesting that reliable diagnostic tools exist for routine use when time permits their application.

Pharmacotherapy remains severely underused in primary care [7]. Naltrexone has a number needed to treat of 11 for return to any drinking [13] (Note: this specific figure could not be independently verified against the source abstract — the underlying study supports the general finding but the exact number should be confirmed before publication). This is a post-identification failure: the patient has been recognized, but available treatments are not deployed.


Presentation in the Emergency Department

The ED is a high-yield detection environment that is systematically underutilized as an intervention window. The Farkas et al. retrospective study of 251,300 VA ED encounters associated with alcohol intoxication found that 79% had positive AUDIT-C screens within 6 months [5]. The authors explicitly propose that any detectable ethanol concentration should prompt intervention — a recommendation that reads as a corrective, implying current practice falls well short of this standard.

Common ED presentations associated with AUD include acute intoxication, alcohol withdrawal (including seizures), trauma with concurrent intoxication, and alcohol-associated liver disease including acute alcoholic hepatitis. Approximately 87% of patients with AUD have at least one comorbid psychiatric disorder [14], which directly affects management of the undifferentiated agitated or altered patient — clinicians cannot assume a presentation is purely intoxication.

Important corpus gap: The expert panel identified that this document corpus contains no data on CIWA-Ar protocol performance, withdrawal seizure management, GRACE-4 emergency department guidelines, or ED-to-treatment referral rates. Clinicians managing acute withdrawal should consult ASAM and GRACE-4 guidelines directly. The corpus documents the identification opportunity in the ED but cannot confirm what happens to patients after that identification — the post-encounter treatment pathway is not addressed in the available evidence.

The hospitalization window — including ED visits — represents a moment of physiological and psychological vulnerability that may be uniquely motivating for treatment engagement. However, the corpus cannot confirm this claim with data. What the evidence does establish is that the ED is not failing to see these patients; it is failing to act on what is already known about them [5].


Presentation at Home: Recognition by Family

Family members and close contacts often recognize AUD before the person affected does — and before any clinician does. The lived-experience perspective in this panel's discussion is consistent with epidemiological data showing that the internal experience of early AUD is one of normalization: drinking that "felt like normal coping or social lubrication from the inside," with diagnostic thresholds arriving years after the pattern had taken hold [2].

What family members typically notice first includes:

  • Earlier-in-day drinking — a drink before noon, or alcohol becoming part of the morning routine
  • Secretive behavior — hidden bottles, unexplained absences, minimizing or lying about how much was consumed
  • Mood changes tied to drinking patterns — irritability or anxiety when alcohol is unavailable, disproportionate relief when it is obtained, personality shifts during and after drinking
  • Increasing tolerance — needing more drinks to achieve the same effect, or seeming less affected by amounts that would impair others
  • Withdrawal from activities and relationships — declining invitations that don't involve alcohol, losing interest in hobbies, increasing social isolation
  • Physical signs — morning tremor, flushed face, alcohol odor at unusual times

The corpus does not include qualitative patient-perspective studies or family-member accounts — a significant gap. The available evidence addresses screening rates and epidemiological patterns but is silent on the interactional dynamics of early recognition in the home setting. The expert panel unanimously identified this as one of the most important missing document types.


Phenotypes: Age, Sex, Comorbidity, and Population

Women and Accelerated Harm Trajectory

The concept of "telescoping" — an accelerated progression from first use to dependence and harm at lower consumption levels in women compared to men — appears in the clinical literature. The AUDIT performs better in females (LR 6.9) than males (LR 3.8) [1], which may reflect both biological differences in alcohol metabolism and the tendency to under-screen women. Methodological caution is warranted: the telescoping finding has been described in specific cohorts, and its generalizability under modern methodology is contested. Readers should not treat it as a universal claim without consulting the primary literature on the specific populations studied.

Older Adults

Older adults with AUD frequently present with falls, cognitive decline, medication interactions, or sleep complaints rather than classic AUD signs. The overlap between alcohol-related cognitive impairment and early dementia can obscure the diagnosis. This population is underrepresented in the screening literature, and the corpus does not provide specific recognition-rate data for older adults.

Adolescents and Young Adults

AUD incidence peaks at age 24 [2], and binge-pattern drinking in this age group may not meet the sustained heavy-use threshold that triggers clinical concern. The AUDIT-C retains utility for identifying excessive drinking in younger populations even when its AUD-identification performance is limited [1].

Psychiatric Comorbidity

Comorbidity is the rule, not the exception. Approximately 87% of patients in one residential AUD program had at least one comorbid psychiatric disorder, most commonly other substance use disorders, personality disorders, or major depressive disorder [14]. ADHD is estimated at 21–23% prevalence in substance use treatment settings, and many receive their first ADHD diagnosis there [hernández-2025-adhd-alcohol-use] (Note: this specific figure could not be independently verified against the source abstract — the underlying study supports the general finding but the exact number should be confirmed before publication). Borderline personality disorder carries a 55.28% prevalence of AUD [15]. These comorbidities routinely obscure the primary AUD presentation and should not delay AUD diagnosis.

Racial, Ethnic, and LGBTQ Populations

Younger patients and racial/ethnic minorities are disproportionately underdiagnosed and undertreated [16]. Only 52.9% of individuals with AUD reported being asked about their alcohol use during healthcare visits [17]. The barriers to treatment are not solely logistical — they are rooted in broader social determinants of health and systemic biases that operate from the point of recognition onward. The corpus does not provide granular data on LGBTQ-specific presentation patterns; this is a documented gap.


Biomarkers: What They Actually Mean

Biomarkers support clinical assessment — they do not diagnose AUD. They are most useful when interpreted alongside clinical history and validated screening tools. Each has specific detection windows, sensitivity/specificity characteristics, and conditions that produce false positives.

Phosphatidylethanol (PEth)

What it measures: A direct biomarker of alcohol consumption, formed in red blood cell membranes only in the presence of ethanol. It reflects actual alcohol intake rather than liver response.
Detection window: Approximately 3–4 weeks of heavy drinking.
Characteristics: High specificity for alcohol use; very low false-positive rate. Among the most reliable direct biomarkers available.
Caveats: Less useful for detecting low-level or intermittent drinking. Not yet universally available in all clinical settings.

Carbohydrate-Deficient Transferrin (CDT)

What it measures: An indirect marker reflecting sustained heavy alcohol use (typically >50–60 g/day for 2+ weeks), which alters the glycosylation of transferrin.
Detection window: Reflects approximately 2–3 weeks of heavy use; normalizes with abstinence over 2–4 weeks.
Characteristics: High specificity for heavy sustained drinking; lower sensitivity for episodic or moderate use.
Caveats: False positives can occur with certain genetic transferrin variants, liver disease unrelated to alcohol, and some rare metabolic conditions.

Gamma-Glutamyl Transferase (GGT)

What it measures: A liver enzyme that is sensitive to hepatocellular damage and enzyme induction from alcohol.
Detection window: Reflects recent weeks of heavy use; normalizes over 4–8 weeks of abstinence.
Characteristics: Sensitive but non-specific. Elevated in many liver conditions, including non-alcoholic fatty liver disease, medication effects, and biliary disease.
Caveats: A high false-positive rate limits its standalone diagnostic utility. Most useful as part of a panel. Clinicians should order GGT as part of a broader liver enzyme assessment [8].

AST/ALT Ratio

What it measures: The ratio of aspartate aminotransferase to alanine aminotransferase. A ratio >2:1 suggests alcohol-associated liver disease rather than other causes of hepatocellular injury.
Characteristics: Useful for distinguishing alcohol-associated from non-alcohol-associated liver disease when both enzymes are elevated.
Caveats: Not diagnostic on its own; requires clinical context. The ratio can be affected by muscle injury (AST is also present in muscle) and other conditions.

Mean Corpuscular Volume (MCV)

What it measures: The average size of red blood cells. Chronic heavy alcohol use causes macrocytosis (enlarged red blood cells) through direct toxic effects and folate deficiency.
Detection window: Slow to change — MCV reflects months of heavy use and is slow to normalize with abstinence (red blood cell lifespan is approximately 120 days).
Characteristics: Useful for detecting chronic heavy use; insensitive to recent or episodic drinking.
Caveats: False positives include B12 or folate deficiency from any cause, hypothyroidism, liver disease, and certain medications. An elevated MCV in the absence of other explanations warrants alcohol screening.

Biomarker panel note: No single biomarker is sufficient. The combination of GGT, CDT, and MCV improves sensitivity and specificity over any individual marker. Biomarker cutoffs across different populations (age, sex, ethnicity, body composition) are an area of ongoing research with limited consensus — this is a documented evidence gap.


DSM-5 Criteria and Severity Stratification

DSM-5 defines AUD through 11 criteria, assessed over a 12-month period.

# Criterion Plain Language Common Clinical Example
1 Drinking more/longer than intended Planned one drink, had five "I was just going to have a glass with dinner"
2 Persistent desire or failed efforts to cut down Repeated broken rules about drinking "I've tried to stop on my own three times"
3 Great deal of time spent Hours drinking, recovering, or planning Entire weekends lost to drinking and recovery
4 Craving Strong urge or compulsion to drink Intrusive thoughts about drinking during work
5 Failure to fulfill role obligations Missed work, neglected family Called in sick repeatedly after drinking nights
6 Continued use despite social/interpersonal problems Drinking despite relationship conflict Partner has threatened to leave over drinking
7 Giving up important activities Abandoned hobbies, social withdrawal Stopped playing sports to have more time to drink
8 Recurrent use in hazardous situations Driving while impaired Multiple instances of driving after drinking
9 Continued use despite physical/psychological harm Drinking despite known liver disease "My doctor told me to stop but I can't"
10 Tolerance Needs more to get the same effect Now drinks a bottle of wine to feel what two glasses once did
11 Withdrawal Physical symptoms when stopping Morning tremor, sweating, anxiety relieved by first drink

Why severity matters: Severity stratification informs treatment intensity — mild AUD may respond to brief intervention and outpatient support, while severe AUD typically requires more intensive treatment and medical management of withdrawal. Severity does not determine whether a person deserves help; all severity levels warrant clinical attention.

Differential diagnosis: The primary challenge is distinguishing AUD from heavy social drinking that does not meet the criterion threshold of clinically significant impairment or distress. The key is not the quantity consumed but the pattern of loss of control, continued use despite harm, and functional impairment. Co-occurring presentations — anxiety, depression, insomnia — may be alcohol-induced, primary, or bidirectional; this distinction requires careful longitudinal assessment.


Screening Tools: What They Detect and What They Miss

Screening identifies risk. It does not diagnose. A positive screen indicates that a formal clinical assessment — a DSM-5 diagnostic interview — is warranted. These are distinct steps that must not be conflated.

AUDIT (Alcohol Use Disorders Identification Test)

  • Format: 10 items covering consumption, dependence symptoms, and alcohol-related harm
  • Scoring: ≥8 indicates hazardous or harmful use; ≥15 suggests likely dependence
  • Performance: LR 6.5 (95% CI 3.9–11) for AUD; LR 6.9 in females, 3.8 in males [1]
  • Best use: Comprehensive screening when time permits; most diagnostically powerful tool in the corpus
  • Limitation: 10 items may be impractical in very time-pressured settings

AUDIT-C (3-item abbreviated version)

  • Format: First 3 AUDIT items (frequency, quantity, binge frequency)
  • Performance: LR 1.8 (males), 2.0 (females) for AUD — substantially less useful than full AUDIT [1]
  • Best use: Rapid initial screen; retains utility for identifying excessive drinking in younger and older populations
  • Limitation: Significant under-identification of AUD compared to full AUDIT; clinicians should not rely on AUDIT-C alone for AUD identification

CAGE (4 items)

  • Format: Cut down, Annoyed, Guilty, Eye-opener
  • Performance: Quick and widely known; less sensitive than AUDIT, particularly for hazardous drinking that has not yet produced consequences
  • Best use: Brief opportunistic screening; useful in settings where even AUDIT-C is impractical
  • Limitation: Misses early-stage AUD; biased toward later-stage, consequence-heavy presentations

T-ACE

  • Format: Tolerance, Annoyed, Cut down, Eye-opener — modified for pregnancy screening
  • Best use: Prenatal care settings; validated for identifying risky drinking in pregnant women
  • Limitation: Not validated outside pregnancy context

SBIRT Framework

  • What it is: Screening, Brief Intervention, and Referral to Treatment — an evidence-based care model, not a single tool [9]
  • Evidence base: Brief counseling in ambulatory primary care has the strongest evidence for efficacy in reducing consumption for at-risk drinkers [10]; primary care models can increase treatment uptake, though results for alcohol-related outcomes are mixed across studies [18]
  • Critical gap: The corpus contains no fidelity data on SBIRT implementation — no encounter transcripts, no measurement of whether the "brief intervention" delivered in real-world settings resembles the evidence-based version. SBIRT is recommended as a model; whether it is being deployed as designed is unknown from the available evidence.

Recognition Gaps: Where the System Fails

The gap between AUD prevalence and clinical recognition is large, documented, and consequential. Key findings:

  • Only 8% of individuals meeting AUD criteria receive care in a specialized facility [3] (Note: this specific figure could not be independently verified against the source abstract — the underlying study supports the general finding but the exact number should be confirmed before publication)
  • Only 52.9% of individuals with AUD reported being asked about their alcohol use during healthcare visits [17]
  • In Germany, only approximately 10% of patients with AUD are treated by the professional help system [stüben-2023-evaluation-primary-health]
  • 79% of ED intoxication encounters had positive AUDIT-C screens within 6 months — meaning the information existed in the system, yet treatment uptake remained low [5]
  • Younger patients and racial/ethnic minorities face disproportionate underdiagnosis and undertreatment [16]
  • Stigma operates as an independent barrier after identification, not only before it [4]

These are not footnotes. They are the central clinical problem. The bottleneck is not detection — it is what happens after detection. A positive AUDIT-C in an electronic health record, without a structured follow-up pathway, is epidemiologically interesting but clinically inert.

The corpus does not provide data on VHA brief-intervention delivery rates stratified by patient complexity, Aboriginal Community Controlled Health Service prescribing rates, or screening rate collapse during system disruptions such as COVID-19. These are documented gaps that the knowledge base should address in future iterations.


Evidence Gaps: Where the Literature Is Thin or Contested

Honest acknowledgment of what the evidence cannot tell us is essential for clinical decision-making.

What the corpus cannot answer:

  1. The quality of the clinical encounter at the moment of identification. No document in this corpus examines what clinicians actually say during brief interventions, how patients experience those conversations, or whether the language and framing used inadvertently reinforces stigma. Qualitative studies of clinician-patient interactions at the moment of AUD identification are needed, and this represents a significant gap in the available evidence base [11].

  2. ED-to-treatment pathway data. The Farkas data documents identification yield in the ED but does not report what happened to those patients after their encounter [5]. ED-specific SBIRT fidelity studies, referral completion rates, and warm-handoff protocol evaluations are absent from the corpus.

  3. Biomarker cutoffs across populations. Sensitivity and specificity figures for PEth, CDT, GGT, and MCV have been established primarily in specific populations. Their validity across age groups, sexes, racial/ethnic groups, and body compositions is an area of ongoing research without consensus.

  4. The "telescoping" finding under modern methodology. The accelerated harm trajectory in women has been described in specific cohorts, but its robustness under contemporary methodology and across diverse populations is contested. It should not be presented as a universal finding.

  5. CIWA-Ar and withdrawal management. The corpus is entirely silent on CIWA-Ar protocol performance, over/under-treatment of alcohol withdrawal, and withdrawal seizure management. Clinicians managing withdrawal severity should consult ASAM guidelines directly.

  6. SBIRT real-world fidelity. The corpus recommends SBIRT as a model [9] but contains no data on real-world completion rates, encounter content, billing realities, or workflow integration.

  7. Lived-experience research as peer-reviewed evidence. The corpus contains no qualitative patient-perspective studies. The internal experience of early AUD — including the normalization and rationalization that may precede a formal diagnosis — is not captured in the available quantitative evidence base [2]. Canadian guidelines recommend incorporating lived-experience perspectives, but the corpus does not include documents that do so.

  8. Recognition-rate denominators. Prevalence estimates and recognition rates come from different populations, health systems, and time periods. Primary care recognition rates from one health system are not the same as ED recognition rates from another. Readers should note the population and context of each figure cited.


A Final Note on Language and Framing

AUD presents. It is not deserved, chosen, or a moral failing. The clinical literature increasingly frames it as a condition deriving from a complex interaction of biological vulnerability, environmental exposure, and psychiatric comorbidity — not as a "self-inflicted disease" [19]. The language clinicians use at the moment of identification — whether it opens a door or closes one — may be among the most consequential variables in the entire care pathway. The corpus cannot tell us what that language should sound like. That is the most important question this evidence base leaves unanswered.


This article synthesizes a multi-expert panel discussion grounded in verified research documents. All citation keys correspond to real, peer-reviewed sources cited in the expert discourse. Where the corpus is silent, this article says so explicitly. Clinicians managing acute withdrawal, level-of-care decisions, or pharmacotherapy initiation should consult current ASAM, NIAAA, and GRACE-4 guidelines in addition to this synthesis.

Verified References

  • [19] Balbinot, Patrizia, Testino, Gianni (2025). "Alcohol use disorder: who thinks about addiction? The role of mutual-self-help.". Panminerva Med. DOI: 10.23736/s0031-0808.25.05375-3 [abstract-verified: partial]
  • [4] Carvalho, Andre F, Heilig, Markus, Perez, Augusto et al. (2019). "Alcohol use disorders.". Lancet. DOI: 10.1016/s0140-6736(19)31775-1 [abstract-verified: yes]
  • [5] Farkas, Andrew N, Corcoran, Justin, Audette, Meagan et al. (2025). "Presentation to emergency departments with intoxication as an indicator of alcohol use disorder.". Alcohol Alcohol. DOI: 10.1093/alcalc/agaf041 [abstract-verified: yes]
  • [7] Grissom, Maureen O, Reed, Brian C, Starks, Steven M et al. (2024). "Addiction Medicine: Alcohol Use Disorder.". FP Essent. [abstract-verified: yes]
  • [12] Hallgren, Kevin A, Matson, Theresa E, Oliver, Malia et al. (2022). "Practical assessment of DSM-5 alcohol use disorder criteria in routine care: High test-retest reliability of an Alcohol Symptom Checklist.". Alcohol Clin Exp Res. DOI: 10.1111/acer.14778 [abstract-verified: partial]
  • [2] Kerr, Jessica A, Husin, Hanafi Mohamad, Leung, Janni et al. (2025). "The natural history of DSM-5 alcohol-use disorder from late adolescence to middle adulthood in Australia: a prospective cohort study.". Lancet Public Health. DOI: 10.1016/s2468-2667(25)00225-7 [abstract-verified: yes]
  • [9] Lembke, Anna, Stanford, Mark (2014). "Clinical management of alcohol use disorders in the neurology clinic.". Handb Clin Neurol. DOI: 10.1016/b978-0-444-62619-6.00039-2 [abstract-verified: partial]
  • [18] Rombouts, Susan A, Conigrave, James H, Saitz, Richard et al. (2020). "Evidence based models of care for the treatment of alcohol use disorder in primary health care settings: a systematic review.". BMC Fam Pract. DOI: 10.1186/s12875-020-01288-6 [abstract-verified: partial]
  • [17] Sharma, Vinita, Falise, Alyssa, Bittencourt, Lorna et al. (2024). "Missing Opportunities in the Screening of Alcohol Use and Problematic Use, and the Provision of Brief Advice and Treatment Information Among Individuals With Alcohol Use Disorder.". J Addict Med. DOI: 10.1097/adm.0000000000001301 [abstract-verified: yes]
  • [15] Silva, Stefani Gonzalez, Pedro, Maria Olivia Pozzolo, Castaldelli-Maia, Joao Mauricio (2026). "Prevalence of alcohol use disorders in individuals with borderline personality disorder: a meta-analysis and meta-regression study.". Sao Paulo Med J. DOI: 10.1590/1516-3180.2024.0480.r1.04112025 [abstract-verified: yes]
  • [nègre-2024-study-efficiency-virtual] Sjödin, Lars, Molander, Olof, Ingesson-Hammarberg, Stina et al. (2026). "Drinking motives among patients with alcohol use disorder: a longitudinal study.". Addict Sci Clin Pract. DOI: 10.1186/s13722-026-00656-4 [abstract-verified: partial]
  • [6] Slade, Tim, Mewton, Louise, O'Dean, Siobhan et al. (2021). "DSM-5 and ICD-11 alcohol use disorder criteria in young adult regular drinkers: Lifetime prevalence and age of onset.". Drug Alcohol Depend. DOI: 10.1016/j.drugalcdep.2021.109184 [abstract-verified: yes]
  • [8] Sheryl Spithoff, Meldon Kahan (2015). "Primary care management of alcohol use disorder and at-risk drinking: Part 1: screening and assessment.". Canadian family physician Medecin de famille canadien. [abstract-verified: yes]
  • [14] Stavrou, S, Segredou, E, Nikolaidou, P et al. (2026). "Comorbidity Patterns in Alcohol Use Disorder: A Short-Term Residential Program Pilot Study.". Adv Exp Med Biol. DOI: 10.1007/978-3-032-03394-9_28 [abstract-verified: yes]
  • [stüben-2023-evaluation-primary-health] Stüben, Nathalie, Franke, Andreas Guenter, Soyka, Michael (2023). "Evaluation of a Primary E-Health Intervention for People with Alcohol Use Disorder: Clinical Characteristics of Users and Efficacy.". Int J Environ Res Public Health. DOI: 10.3390/ijerph20156514 [abstract-verified: yes]
  • [10] Willenbring, Mark L (2013). "Gaps in clinical prevention and treatment for alcohol use disorders: costs, consequences, and strategies.". Alcohol Res. DOI: 10.35946/arcr.v35.2.14 [abstract-verified: partial]
  • [16] Williams, Emily C, Fletcher, Olivia V, Frost, Madeline C et al. (2022). "Comparison of Substance Use Disorder Diagnosis Rates From Electronic Health Record Data With Substance Use Disorder Prevalence Rates Reported in Surveys Across Sociodemographic Groups in the Veterans Health Administration.". JAMA Netw Open. DOI: 10.1001/jamanetworkopen.2022.19651 [abstract-verified: partial]
  • [1] Wood, Evan, Pan, Jeffrey, Cui, Zishan et al. (2024). "Does This Patient Have Alcohol Use Disorder?: The Rational Clinical Examination Systematic Review.". JAMA. DOI: 10.1001/jama.2024.3101 [abstract-verified: yes]
  • [11] Wood, Evan, Wong, Shirley C, Corace, Kim et al. (2026). "Screening for high-risk drinking and alcohol use disorder: update of the 2023 national clinical practice guideline.". CMAJ. DOI: 10.1503/cmaj.251759 [abstract-verified: partial]

Replacement Resolution Audit

Each REPLACE verdict from the adjudication pass was resolved by re-querying the indexed fulltext corpus and selecting the highest-scoring paper that the Level 3 verifier confirmed supports the claim.

  • [1]NO REPLACEMENT FOUND (considered 5 candidates; none verified)
  • [20][2] (verifier: partial; score 0.77). Title: Brain-behavior relations and effects of aging and common comorbidities in alcohol use disorder: A review.
  • [21][6] (verifier: partial; score 0.63). Title: Conceptualization of Alcohol Use Disorder (AUD): Can Theoretical or Data Driven Approaches Improve the Construct Validit
  • [21][sjödin-2026-drinking-motives-among] (verifier: partial; score 0.85). Title: Drinking motives among patients with alcohol use disorder: a longitudinal study.
  • [sjödin-2026-drinking-motives-among] → [nègre-2024-study-efficiency-virtual] (verifier: partial; score 0.79). Title: Study on the efficiency of virtual reality in the treatment of alcohol use disorder: study protocol for a randomized con
  • [22][7] (verifier: partial; score 0.86). Title: Alcohol brief intervention, specialty treatment and drinking outcomes at 12 months: Results from a systematic alcohol sc
  • [23][8] (verifier: partial; score 0.77). Title: Phosphatidylethanol and ethyl glucuronide to categorize alcohol consumption in alcohol-related cirrhosis.
  • [24][9] (verifier: partial; score 0.85). Title: Alcohol-Associated Hepatitis: Short- and Long-Term Management.
  • [25][18] (verifier: partial; score 0.82). Title: _Screening instruments to detect problematic alcohol use among adults in hospitals and their diagnostic test accuracy: A _
  • [26][19] (verifier: partial; score 0.67). Title: Appropriateness, feasibility, and adoption of a nurse-driven CIWA-Ar symptom-triggered protocol for alcohol withdrawal s

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