Introduction
People who inject drugs (PWID) experience disproportionate morbidity and mortality related to their drug use [
1,
2]. Opioid overdose, in particular, is a leading cause of mortality amongst PWID [
1]. Non-fatal opioid overdose is common amongst PWID [
3‐
6] and associated with an increased risk of subsequent fatal overdose [
7,
8]. Monitoring overdose occurrence therefore presents a key surveillance target and a potential opportunity to inform interventions to reduce opioid related deaths.
Internationally, there is growing interest in utilising ‘syndromic surveillance’, like that used for infectious disease outbreaks, for drug related harms [
9,
10]. The ongoing, systematic gathering of clinical and non-clinical data could provide timely, actionable information on new or emerging drug trends and help facilitate prompt intervention and responses [
9,
10]. PWID frequently attend hospital emergency departments (EDs) [
11], including for overdose-related presentations [
12], and so ED data offer potential utility for surveillance and a rich source of information on drug-related morbidity.
Challenges arise, however, when using health data to study non-fatal opioid overdose due to lack of consensus regarding a case definition of opioid overdose in the literature and a lack of sensitivity and specificity of hospital diagnostic coding practices in detecting these cases [
13‐
18]. The World Health Organization (WHO) International classification of diseases (ICD) is the most commonly employed diagnostic coding method used in health-related administrative data, currently at its tenth revision (ICD-10). The clinical syndrome of any ‘drug overdose’ is typically represented by two broad ranges of codes within the ICD-10; “T36 to T50 Poisoning by drugs, medicaments and biological substances” (‘T-codes’) and “F10 to F19 Mental and behavioural disorders due to psychoactive substance use” (‘F-codes’). Consensus statements released by the WHO Substance Abuse Department recommend that ICD-10 F-codes specifying ‘acute intoxication’ should be used to classify drug overdoses in people with known substance use disorders, reserving the T-codes for poisonings in non-substance dependent people [
13,
14]. In practice, however, both T-codes and F-codes are used variably in the clinical setting [
15,
16]. These non-standardised coding practices limit the validity and utility of ICD-10 codes in drug overdose surveillance [
17,
18]. A thorough understanding of real world ICD-10 coding practices is essential to optimising surveillance efforts.
In this paper we examine F-codes and T-codes in ED attendances among a cohort of known PWID, whose drug use trends [
5,
19], rates of ED attendance and reasons for presentation [
11,
20] have been characterised previously. Here, we focus specifically on the extent to which different ICD-10 codes are used in coding overdose attendances and consider the implications of this coding for understanding patterns and trends in the presentations of PWID in the ED.
Results
There was a total of 3459 ED presentations for the cohort during the five and half year study period. Diagnostic data were missing in 436 records (13%) due to patients leaving after clinical advice about treatment options (without being seen by a definitive service provider) (n = 31) or leaving at risk without treatment (n = 405) and therefore did not require a diagnostic code to be recorded in VEMD. Ninety-three percent of the remaining 3023 records had only a primary diagnosis recorded, with 7% having a secondary diagnosis and less than 1% having a tertiary diagnosis.
There were 232 T-code mentions across all diagnostic fields in the study period and, when accounting for records with multiple T-codes within the same encounter (
n = 4), this represented 228 unique presentations (7%) for ‘poisonings’. There were 232 F-code mentions across all diagnostic fields in the study period and, after accounting for cases with multiple F-codes in the same encounter (
n = 5), this represented 227 (7%) unique presentations for ‘mental and behavioural disorders due to psychoactive substances’. Only six cases had both F and T codes recorded within the same encounter, resulting in a total of 449 unique presentations containing F or T codes, contributed by 168 individuals. One third of all F and T code encounters (
n = 138, 31%) were due to five individuals with repeat presentations. Demographic details for the 168 individuals at their first F or T code diagnosis in the study period are presented in Table
1.
Table 1
Demographic characteristics of 168 participants at their first F or T code diagnosis in ED during the study period
Mean Age | 28.1 years (SD 4.3) | – | – |
Proportion by age group (years) | 15–19 | 6 |
4
|
20–24 | 40 |
24
|
25–29 | 66 |
39
|
30–34 | 52 |
31
|
35–39 | 3 |
2
|
40–44 | 1 |
1
|
Sex | Male | 104 |
62
|
Female | 64 |
38
|
Preferred Language | English | 167 |
99
|
Vietnamese | 1 |
1
|
Country of birth | Australia | 137 |
82
|
Vietnam | 8 |
5
|
England | 3 |
2
|
New Zealand | 3 |
2
|
Other | 14 |
8
|
Missing | 3 |
2
|
Marital status | Never married | 70 |
42
|
De Facto | 5 |
3
|
Married | 2 |
1
|
Not stated/missing | 91 |
54
|
Usual Accommodation | Private residence (with others) | 115 |
68
|
Private residence (alone) | 14 |
8
|
Supported Residential Service (community based) | 4 |
2
|
Boarding house/Hostel | 3 |
2
|
Homeless | 3 |
2
|
Homeless shelter / Other refuge | 2 |
2
|
Other | 2 |
2
|
Not stated/missing | 25 |
15
|
Tables
2 and
3 list T and F codes separately, in order of frequency. There were 16 different T-codes and 18 different F-codes representing seven different broad drug classes. Table
2 shows that, among the 228 encounters with poison codes in this PWID cohort, the most frequently recorded T-code was T50.9, a non-specific drug/medication category (
n = 77, 34%). Table
3 shows there were 139 (61%) ‘acute intoxication’ codes recorded across a range of drug classes, with nearly half of these pertaining to acute alcohol intoxication (
n = 62, 45%). ‘F19.-: mental and behavioural disorders due to multiple drugs and psychoactive substances’ was the most common diagnostic category amongst the F-codes (
n = 83, 37%) and included diagnoses pertaining to withdrawal. Examining Tables
2 and
3 together, which represented 449 unique presentations (six presentations involved both T and F codes), T-codes for ‘poisonings’ were more frequent overall compared to F-codes for ‘acute intoxication’ in this cohort of known PWID (51% versus 31% across all F or T code encounters). F-codes were more commonly used to reflect adverse effects of alcohol or polysubstance use, while T-codes were generally used to reflect poisonings due to specific illicit drug classes. Over one third of the F and T codes assigned did not identify a specific drug class (
n = 160, 36%) and 10% (
n = 46) had an unspecified clinical presentation which could not distinguish between presentations related to overdose or withdrawal. There were 37 (8%) F-codes which specified withdrawal from substances as opposed to overdose. Therefore, the highest ranked F or T code per encounter could be used to reasonably infer an illicit drug overdose (ie. specifying both an illicit drug class (excludes alcohol) AND a clinical reaction of ‘poisoning’ or ‘acute intoxication’) less than half the time (
n = 188, 42%).
Table 2
Distribution of the 228 T-codes assigned during study period, in order of frequency (highest ranked onlya)
T50.9 | Other and unspecified drugs, medicaments and biological substancesb | 77 | 33.8 | 17.1 |
T40.1 | Heroin | 37 | 16.2 | 8.2 |
T42.4 | Benzodiazepines | 33 | 14.5 | 7.3 |
T40.6 | Other and unspecified narcotics | 16 | 7.0 | 3.6 |
T39.1 | 4-Aminophenol derivatives | 11 | 4.8 | 2.4 |
T43.9 | Psychotropic drug, unspecified | 11 | 4.8 | 2.4 |
T42.7 | Antiepileptic and sedative-hypnotic drugs, unspecified | 10 | 4.4 | 2.2 |
T40.2 | Other opioids | 9 | 4.0 | 2.0 |
T40.3 | Methadone | 6 | 2.6 | 1.3 |
T43.6 | Psychostimulants with abuse potential | 4 | 1.8 | 0.9 |
T40.0 | Opium | 3 | 1.3 | 0.7 |
T40.7 | Cannabis (derivatives) | 3 | 1.3 | 0.7 |
T41.2 | Other and unspecified general anaesthetics | 3 | 1.3 | 0.7 |
T40.4 | Other synthetic narcotics | 2 | 0.9 | 0.4 |
T43.0 | Tricyclic and tetracyclic antidepressants | 2 | 0.9 | 0.4 |
T40.9 | Other and unspecified psychodysleptics [hallucinogens] | 1 | 0.4 | 0.2 |
Table 3
Distribution of the 227 F-codes assigned during study period, in order of frequency (highest ranked onlya)
F10.0-F19.9, Mental and behavioural disorders due to use of: | n | N = 227 | N = 449 |
F10.0 | Alcohol: Acute intoxication | 62 | 27.3 | 13.8 |
F19.0 | Multiple drugs and use of other psychoactive substances: Acute intoxicationb | 40 | 17.6 | 8.9 |
F19.3 | Multiple drugs and use of other psychoactive substances: Withdrawal statebd | 32 | 14.1 | 7.1 |
F11.0 | Opioids: Acute intoxication | 21 | 9.3 | 4.7 |
F10.9 | Alcohol: Unspecified mental and behavioural disorderc | 16 | 7.1 | 3.6 |
F19.9 | Multiple drugs and use of other psychoactive substances: Unspecified mental and behavioural disorderbc | 11 | 4.9 | 2.4 |
F13.0 | Sedatives or hypnotics: Acute intoxication | 10 | 4.4 | 2.2 |
F11.9 | Opioids: Unspecified mental and behavioural disorderc | 9 | 4.0 | 2.0 |
F12.9 | Cannabinoids: Unspecified mental and behavioural disorderc | 5 | 2.2 | 1.1 |
F15.1 | Other stimulants, including caffeine: Harmful use | 5 | 2.2 | 1.1 |
F10.3 | Alcohol: Withdrawal stated | 4 | 1.8 | 0.9 |
F15.0 | Other stimulants, including caffeine: Acute intoxication | 4 | 1.8 | 0.9 |
F13.9 | Sedatives or hypnotics: Unspecified mental and behavioural disorderc | 3 | 1.3 | 0.7 |
F10.4 | Alcohol: Withdrawal state with deliriumd | 1 | 0.4 | 0.2 |
F12.0 | Cannabinoids: Acute intoxication | 1 | 0.4 | 0.2 |
F16.9 | Hallucinogens: Unspecified mental and behavioural disorderc | 1 | 0.4 | 0.2 |
F18.0 | Volatile solvents: Acute intoxication | 1 | 0.4 | 0.2 |
F18.9 | Volatile solvents: Unspecified mental and behavioural disorderc | 1 | 0.4 | 0.2 |
Table
4 excludes codes representing withdrawal states to look more closely at potential overdose related presentations and depicts the diagnostic level (primary, secondary or tertiary) that overdose related codes occur, along with T or F-code co-mentions within a given encounter. A subset of specific ICD-10 code categories were chosen, representing opioid poisonings, mental and behavioural disturbances related to opioids, the highest occurring T and F categories (T50.- and F19.-), as well as all poisonings and all mental and behavioural disturbances due to psychoactive substances. The table shows that when present, F or T codes were frequently primary diagnoses and there was very little overlap, both within or between categories as most overdose-related F or T code presentations received only a primary diagnosis for the encounter (
n = 346, 83%). Opioid poisonings were more commonly diagnosed than mental and behavioural disturbances due to opioids. Opioid poisoning represented one third of all T-code poisonings (
n = 74, 32%) and mental and behavioural disorders due to opioids represented 13% (
n = 30) of F-code diagnoses.
Table 4
Number of ED presentations with diagnoses in selected ICD-10 categories, and hierarchical position of the diagnosis within each presentation
T40.0-T40.4 & T40.6 | Opioid poisonings | 74 | 2 | 72 | 2 | 0 | 2 | 0 |
F11.0-F11.9a | Mental and behavioural disorders due to opioids | 30 | 1 | 30 | 0 | 0 | 0 | 1 |
T50.9 | Poisoning: Other and unspecified drugs, medicaments and biological substances | 79 | 2 | 73 | 6 | 0 | 2 | 3 |
F19.0-F19.9b | Mental and behavioural disorders due to multiple drugs and psychoactive substances | 52 | 2 | 47 | 4 | 1 | 1 | 1 |
T36.0-T50.9 | ALL: Poisoning by drugs, medicaments and biological substances | 228 | 7 | 220 | 12d | 0 | – | 6 |
F10.0-F19.9c | ALL: Mental and behavioural disorders due to psychoactive substances | 190 | 6 | 174 | 19e | 1 | 6 | – |
Discussion
We examined how a selection of F and T codes were assigned within ED data for a cohort of 688 known PWID between January 2008 and June 2013. Our findings suggest that ED diagnostic codes used in isolation are not suitable for surveillance of specific drug overdoses in Victoria. There were 449 unique presentations with F and T codes mentioned during the study period. Nearly half of the F and T codes utilised in the cohort were non-specific and either did not identify the drug class involved (36%) or the exact nature of the clinical effect of the drug (overdose versus withdrawal, 10%). As such, only 188 (42%) of F or T codes could be used to reasonably infer an illicit drug overdose event, with the ICD-10 code referencing both an illicit drug class and a clinical reaction of ‘poisoning’ or ‘acute intoxication’. Despite the WHO recommendation to utilise F-codes of ‘acute intoxication’ to characterise overdose in substance dependent persons [
14], T-codes for poisonings were more commonly ascribed in this cohort of known PWID, most of whom would be considered clinically substance dependent. A large proportion of ‘acute intoxication’ codes related to alcohol toxicity (45%) rather than illicit substances.
There was a wide dispersion of F and T codes within the cohort, implicating up to seven different drug classes and 18 different substances as primary causes of overdose. Within our cohort, whose patterns of drug use have been well characterised and predominantly involve the use of heroin, other opioids and stimulants [
5], this suggests a high degree of misclassification of overdoses and poisonings within the ED. It is well recognised that ED clinicians face numerous diagnostic challenges in classifying drug overdoses. A prospective observational study in a large, tertiary ED in Melbourne, Australia showed that clinicians’ impressions of the substances involved in suspected recreational drug overdose matched laboratory blood tests in 78% of cases, however this figure dropped to 46% when exploring opioids specifically [
24]. In a culture where co-ingestion is increasingly common, and pre-hospital naloxone administration (an opioid antagonist) is widely available, the classic opioid poisoning toxidrome of pupillary meiosis, respiratory depression and stupor may not manifest [
25]. Toxicological assays are not yet rapid or reliable enough to be clinically useful in acute overdose [
26] and precise identification of the causative agent may be clinically irrelevant in the ED context with critically unwell, obtunded or agitated patients who require immediate, symptom directed, supportive care regardless of aetiology [
25]. Many overdoses are managed by ambulance services in the community itself without requiring subsequent hospitalisation [
27‐
29], however Victorian ambulance clinical practice guidelines recommend that patients who have not responded within ten minutes to naloxone treatment in the community or have other complicating features should be brought to hospital [
30]. This increases the complexity of the ED casemix, further challenging clinicians’ abilities to accurately identify the substances involved in overdoses or poisonings. An additional effect of this on ICD-10 coding may be that, even if an opioid overdose is the underpinning primary event, the clinical diagnosis chosen in ED may pertain to the complicating features necessitating transportation to ED, rather than the overdose itself. For example, a clinician may enter a diagnosis reflecting ‘polysubstance overdose’ because the patient failed to respond to community administered naloxone or record only the medical complications of overdose such as aspiration pneumonia. These coding practices limit the sensitivity and specificity of ICD-10 codes in detecting overdose presentations.
The most common single overdose-related code used was “T50.9: Other and unspecified drugs, medicaments and biological substances”. The official WHO definition states the ‘T50.9’ code is applicable when substances are ‘not elsewhere classified’, listing examples of “acidifying agents, alkalizing agents, immunoglobulin, immunologicals, lipotropic drugs and parathyroid hormones and derivatives” [
31]. These substances are highly unlikely to be the most common primary cause of drug overdose in our cohort of PWID with a known predilection for the use of heroin, other opioids and stimulants. Our findings therefore suggest that, in clinical practice, it appears ‘T50.9’ is being adopted as a means to classify encounters where ‘unknown’ or ‘unspecified’ substance(s) are involved. The ‘F19.-’ category, encompassing codes F19.0-F19.9, was the most common diagnostic category seen in the cohort, representing “mental and behavioural disorders due to multiple drugs and psychoactive substances”. Once again, this category is non-specific, referring to ‘multiple drugs’ but not implicating any specific agent or drug class. WHO recommends ‘F19.-’ codes are used in cases when “two or more psychoactive substances are known to be involved but it is impossible to assess which substance contributed most” or “when the exact identity of some or all the psychoactive substances being used is uncertain or unknown” [
31]. It is plausible that, despite clinicians’ intensive efforts in ED, the specific substances involved in a drug overdose cannot be identified. However, the high frequency use of this code within a cohort of known PWID with relatively stable drug usage patterns [
19] suggests that other contextual factors, such as a lack of understanding of the importance of detailed clinical documentation for surveillance efforts, insensitive data collection tools and competing priorities in a busy ED, may be influencing non-specific coding practices as well. Studies have shown insufficient awareness about ICD-10 coding practices amongst both clinicians and trained coders [
16,
22] and there has been criticism that the significantly abridged ICD-10 codes do not adequately capture all substances, particularly new and emerging drugs, forcing clinicians’ diagnoses to be mapped back to inappropriate codes [
15]. It is unclear, however, whether increasing the number and specificity of codes available will yield more accurate data. Our study revealed that majority (83%) of overdose encounters with F or T code diagnoses had only a primary diagnosis recorded, despite the option for clinicians to record up to three. In the context of general medical or surgical presentations, a single diagnosis may be appropriate and reflect single organ system dysfunction, however in the context of drug poisoning or overdose, co-ingestion is increasingly common and warrants numerous diagnostic entries to reflect each involved substance. In the busy ED setting, broad non-specific headings such as ‘other and unspecified drugs’ or ‘multiple drugs and psychoactive substances’ may appear convenient and all-encompassing default options to indicate polysubstance overdose, rather than individually entering multiple different agents.
While broad coding practices may be efficient and sufficient for clinical practice, they significantly hamper individual drug overdose surveillance efforts, as non-specific codes are frequently excluded when establishing case definitions. Given then frequent non-specific coding seen within our cohort of primarily opioid users, it is likely that the use of ED data collated on the basis of ICD diagnosis alone would considerably underestimate the incidence of opioid overdose. One way to improve surveillance may be to integrate information from free-text coding available in the VEMD, but this information is not always available (including for this study) and is of unknown reliability or validity [
17,
18]. Nevertheless, the question remains as to whether to include non-specific codes within surveillance case definitions, and studies have shown that their inclusion increases sensitivity but reduces specificity of case detection [
17,
32]. Potential measures to reduce the utilisation of non-specific codes within the ED could include educating clinicians in data collection processes and implications for surveillance, collaborative review regarding the ICD-10 tool and its appropriateness for drug overdose diagnosis in ED and consideration of the involvement of trained, dedicated coders within EDs (similar to clinical coding used for inpatient records [
33]) to relieve the data collection burden from busy clinical staff and potentially improve data quality and consistency.
Acknowledgements
This study was made possible by the contribution of many people, including the original MIX investigators; the team who recruited the participants and the participants themselves; the Centre for Victorian Data Linkage for their cooperation and expertise in assisting with access to departmental databases; and colleagues at Burnet Institute for their guidance and technical assistance.