Frailty and Co-Prescribing of Potentially Interacting Drugs in New Users of Warfarin.

BACKGROUND: Warfarin is underutilised in frail older people because of the fear of bleeding complications. Drug interactions are an independent bleeding risk factor. However, the extent to which potential drug interactions are taken into account at warfarin therapy initiation in frail patients is not known.
OBJECTIVE: The objective of this study was to investigate the use of potentially interacting drugs increasing the bleeding risk before and after warfarin initiation in frail and non-frail patients.
METHODS: We conducted an observational study including inpatients aged ≥ 60 years initiated on warfarin in a tertiary hospital in Adelaide, South Australia. Frailty status was assessed with the Reported Edmonton Frail Scale. Medication charts were reviewed before and after warfarin initiation.
RESULTS: In total, 151 patients (102 non-frail and 49 frail) were included. Before warfarin initiation, the use of clopidogrel and acetaminophen was more common in frail patients compared with non-frail patients (25.5% vs 10.2%, p = 0.0135, 63.8% vs 35.7% p = 0.0014, respectively). The use of non-steroidal anti-inflammatory drugs, 9.2% in non-frail patients and 6.4% in frail patients before warfarin initiation, was completely stopped after warfarin initiation in both groups. The use of antiplatelet drugs decreased from 56.1% in non-frail patients and 66.0 % in frail patients to 12.2% and 14.9%, respectively. Instead, the use of drugs affecting the metabolism of warfarin or vitamin K increased in both groups. No statistically significant difference was seen in the exposure to interacting drugs between study groups after warfarin initiation. Acetaminophen, senna glycosides and cytochrome P450 2C9 inhibiting drugs were the most common interacting drugs at discharge used in 49.0%, 18.4% and 20.4% of non-frail patients and 53.2%, 29.8% and 19.1% of frail patients, respectively.
CONCLUSIONS: The overall frequency of potential drug interactions was moderate and frail patients were not exposed to warfarin drug interactions more often than non-frail patients. Further studies in larger study populations are required to verify these results.

Key Points

Introduction

Bleeding is a common and potentially serious complication of warfarin therapy. The risk is increased with advanced age [1, 2] and drug interactions [3, 4]. The fear of serious bleeding complications is the key reason for the underutilisation of warfarin, especially in frail older people, as shown by previous studies [5, 6]. Considering the high prevalence of comorbidities and polypharmacy in frail patients [7], the risk of drug interactions is high in this population.

Frail patients are more vulnerable to adverse drug reactions [8], and thus the bleeding risk caused by drug interactions may be even higher than reported in non-frail patients. More importantly, the excess risk caused by drug interactions is predictable and often avoidable by choosing alternative medications. Despite this, previous studies show that up to 60–80% of warfarin users, the majority of whom are older people, are exposed to potential drug interactions [9-12]. However, to our knowledge, there is no existing research on the frequency of warfarin drug interactions in frail patients compared to non-frail patients. Our aim was to examine the exposure to drug interactions increasing the bleeding risk and the number of all regular medications before and after warfarin initiation with a special focus on frailty status at the early phase of warfarin therapy.

Methods

Study Design, Setting and Subjects

This observational study was performed at the Royal Adelaide Hospital, in Adelaide, South Australia between October 2012 and May 2013. The study was approved by the institutional human research ethics committee (Royal Adelaide Hospital Protocol No. 120911).

We included previously warfarin-naïve inpatients, aged ≥ 60 years, in whom warfarin was initiated within 2 weeks for any indication. Eligible patients were identified either by ward pharmacists or from daily International Normalized Ratio (INR) measurement reports provided by the hospital laboratory. Patients were recruited from all units of the hospital. The majority of the patients included in the study were treated in the units of general medicine, cardiothoracic surgery, cardiology and neurology. All participants provided written informed consent to participate. For patients with cognitive impairment, a third-party consent was obtained from patients’ next of kin, carer or significant other. We excluded patients with previous warfarin use or severe hearing impairment.

Data Collection

We collected data on patients’ clinical characteristics (age, sex, comorbidities, standard haematological, hepatic and renal laboratory parameters, indication for warfarin therapy and reason for hospitalisation) and medication by reviewing patient files and medication charts and by interviewing patients.

Frailty Assessment

Frailty status was assessed at the time of the recruitment by performing the reported version of the Edmonton Frail Scale as modified by Hilmer et al. [13] and utilised in several previous studies [5, 14, 15]. The Edmonton Frail Scale assesses cognition, general health status, functional independence, social support, medication use, nutrition, mood, continence and functional performance [16]. It has been validated for the assessment of frailty by non-medically trained researchers [16]. In the reported version, the observed ‘get up and go’ is substituted with a self-report of function 2 weeks prior to admission to avoid confounding by the effects of acute illness [13]. The reported Edmonton Frail Scale scores defines patients’ frailty status as follows: 0–5 not frail, 6–7 apparently vulnerable, 8–9 mild frailty, 10–11 moderately frail and 12–18 severe frailty. In the analysis, the frailty scale was collapsed into two categories because of the low number of patients in the categories of the highest frailty. Patients with score of ≥ 8 were considered frail. Similar merging of categories has been reported in previous studies [5, 13–15].

Medication Data

We collected information on medications used as outpatients prior to the current admission (home medication) and at discharge. Home medication data were obtained by the ward pharmacist as the best available medication history by interviewing the patient, as well as the general practitioner and community pharmacist, where necessary. In the case where a patient had been admitted earlier than 1 week prior to the day of warfarin initiation, home medication was recorded as the medication on the ward 7 days prior to the day of warfarin initiation. Discharge medication data were obtained from discharge summaries in the medical records, also reconciled by the hospital pharmacist.

We collected information on the use of all regular, systemically administered medications. We excluded medication formulations for topical treatment (e.g. topical creams, oral gels, intravaginal preparations) because the extent of systemic absorption is either minimal or uncertain.

Interacting Drugs

We utilised the INXBASE® (previously SFINX®) drug–drug interaction database [17] in defining warfarin interaction drugs. Based on the INXBASE® search, we chose to study drugs classified as ‘to be avoided’ and ‘special consideration required’ with warfarin. We reviewed the use of interacting drugs prior to warfarin initiation and at discharge. The list of these interacting drugs is provided in File 1 of the Electronic Supplementary Material.

Risk Scores

We calculated bleeding and stroke risk scores and the comorbidity index [18] for each patient (Table 1). The HAS-BLED score was calculated without scoring ‘Labile INR values’ and HEMORR2HAGES without information on the cytochrome P450 (CYP) 2C9 genotype as reported by previous articles [6, 19].

Table 1

Bleeding and stroke risk scores and comorbidity score calculated for each patient

Risk score and scoring components	Score
Outpatient Bleeding Risk Index (OBRI) [20]
Age ≥ 65 years	1
History of stroke	1
History of gastrointestinal bleeding	1
Recent myocardial infarction, haematocrit < 30 %, creatinine > 1.5 mg/dL or diabetes mellitus	1
Low risk 0, intermediate risk 1–2, high risk 3–4	Maximum 4
Anticoagulation and risk factors (ATRIA) [21]
Anaemia	3
Renal disease	3
Age ≥ 75 years	2
Prior bleeding	1
Hypertension	1
Low risk 0–3, intermediate risk 4, high risk 5–10	Maximum 10
HEMORR2HAGES [22]
Hepatic or renal disease	1
Ethanol abuse	1
Malignancy	1
Older age (age > 75 years)	1
Reduced platelet count or function	1
Hypertension (uncontrolled)	1
Anaemia	1
Genetic factors	1
Excessive falls risk	1
Stroke	1
Prior bleed	2
Low risk 0–3, intermediate risk 4, high risk 5–10	Maximum 11
HAS-BLED [23, 24]
Hypertension	1
Abnormal renal function	1
Abnormal liver function	1
Stroke	1
Bleeding history or predisposition	1
Labile INR	1
Elderly	1
Drugs concomitantly	1
Alcohol concomitantly	1
Low risk 0–1, intermediate risk 2–3, high risk ≥4	Maximum 9
CHADS2 [25]
Congestive heart failure	1
Hypertension	1
Age ≥75 years	1
Diabetes mellitus	1
Stroke	2
Low risk 0, intermediate risk 1–2, high risk ≥3	Maximum 6
CHA2DS2-Vasc [26]
Congestive heart failure	1
Hypertension	1
Age ≥ 65 years	1
Age ≥ 75 years	2
Diabetes mellitus	1
Stroke	2
Vascular disease	1
Female	1
Low risk 0, intermediate risk 1, high risk ≥ 2	Maximum 9
Charlson Comorbidity Index [18]
Myocardial infarct	1
Congestive heart failure	1
Peripheral vascular disease	1
Cerebrovascular disease	1
Dementia	1
Chronic pulmonary disease	1
Connective tissue disease	1
Ulcer disease	1
Mild liver disease	1
Diabetes mellitus	1
Hemiplegia	2
Moderate or severe renal disease	2
Diabetes mellitus with end organ damage	2
Any tumour	2
Leukaemia	2
Lymphoma	2
Moderate or severe liver disease	3
Metastatic solid tumour	6
AIDS	6

AIDS Acquired Immune Deficiency Syndrome, INR International Normalized Ratio

Statistical Analysis

Relationships between dependent and independent variables were studied with descriptive statistics, McNemar test, Fisher’s exact test and analysis of variance models. Continuous variables were characterised using means and standard errors for normally distributed variables and median and interquartile range of values for variables that were not normally distributed. The normality of variables was evaluated visually and tested with the Shapiro–Wilk test. Square root transformation was used when necessary to make variables more normally distributed. The main statistical analyses for risk scores were performed using analysis of variance. Sex, age group, atrial fibrillation and frailty were included in all models.

The number of drugs used was primarily examined using repeated analysis of variance. Measurements from different time points for the same person were considered repeated measurements. Sex, age group, atrial fibrillation and frailty were included in all models. Furthermore, multiple interaction terms were included to compare subgroups sufficiently within the model.

The McNemar test was used to test statistical significance of the differences in the use of individual drugs between time points, and the Fisher’s exact test was used to test statistical significance of the differences between frailty groups. More complicated models were not fitted to data on individual drugs because of the small sample size.

The statistical significance level was set at 0.05 in all tests (two-tailed). Analyses were performed using the SAS system, version 9.4 for Windows (SAS Institute Inc., Cary, NC, USA).

Results

We recruited 151 inpatients (94 were male and 57 were female), of whom 102 were non-frail and 49 frail. The characteristics, age distribution and risk scores are presented in Table 2. There was a slight preponderance of male individuals and patients in the younger age categories in the non-frail group compared with the frail group (p = 0.11 and p = 0.14, respectively). The majority of calculated risk scores for bleeding and stroke were slightly higher in frail patients; yet a statistically significant difference was observed only for the Outpatient Bleeding Risk Index score (1.7 vs 1.9 for non-frail and frail patients, respectively, p = 0.0446) and the CHA2DS2-VASc score (2.0 vs 2.5 for non-frail and frail patients, respectively, p = 0.0164). Instead, the Charlson Comorbidity Index was significantly higher for frail patients (4.0) compared with non-frail patients (2.0, p < 0.0001). No statistically significant differences were observed in the measured laboratory parameters (data not shown).

Table 2

Characteristics of frail and non-frail patients

	Non-frailn = 102	Frailn = 49
Women, % (n)	33 (34)	47 (23)
Age (median, range), years	71 (60–93)	74 (61–96)
60–69, % (n)	45.1 (46)	30.6 (15)
70–79, % (n)	36.3 (37)	38.8 (19)
≥80, % (n)	18.6 (19)	30.6 (15)
Operated during the admission, % (n)	44.1 (45)	28.6 (14)
Charlson Comorbidity Index, estimated mean (SE)	2.0 (0.1)	4.0 (0.1)**
Risk scores, estimated mean (SE)
Outpatient Bleeding Risk Index (OBRI)	1.7 (0.1)	1.9 (0.1)*
Anticoagulation and risk factors (ATRIA)	7.0 (0.2)	7.0 (0.3)
HEMORR2HAGES	3.2 (0.1)	3.5 (0.2)
HAS-BLED	3.0 (0.1)	3.4 (0.2)
CHADS2	1.1 (0.1)	1.3 (0.1)
CHA2DS2-VASc	2.0 (0.1)	2.5 (0.2)*

An analysis of variance model including sex, age group, atrial fibrillation and frailty was utilised for comparing the difference between frailty groups

SE standard error, * p < 0.05; ** p < 0.001 compared to non-frail category

Medication and Frailty

Medication data before and after warfarin initiation were available for 98 non-frail and 47 frail patients. Frail patients were using on average 10.7 regular medications before warfarin initiation and 9.8 at discharge; in non-frail patients, the corresponding numbers were 7.1 and 7.6 (p < 0.0001 and p = 0.0228 between frail and non-frail groups, respectively) (Table 3). A sex-specific effect was observed when the number of regular medications before and after warfarin initiation were compared. Frail male patients had a higher number of regular medications than their non-frail counterparts before warfarin initiation (p < 0.001), whereas in non-frail male patients, the number of medications increased significantly after warfarin initiation (p = 0.0010). In the non-frail group, female patients had more medications before warfarin initiation than male patients (8.6 vs. 5.7, respectively, p = 0.068). When both sexes were considered together, the within-group change was not significant in frail and non-frail patients.

Table 3

Mean number of drugs in use before (home) and after (discharge) warfarin initiation stratified by frailty, sex and presence of atrial fibrillation (AF)

	Home mean (SE)	Discharge mean (SE)
Non-frail, n = 98	7.1 (0.44)	7.6 (0.44)
AF	8.4 (0.59)	8.6 (0.59)
Non-AF	5.8 (0.67)	6.7 (0.68)
Male	5.7 (0.55)	7.5 (0.55)***
Female	8.6 (0.72)†	7.8 (0.73)
Frail, n = 47	10.7 (0.60)**	9.8 (0.60)*
AF	12.4 (0.81)*	11.3 (0.81)
Non-AF	8.9 (0.88)	8.3 (0.89)
Male	11.6 (0.82)**	10.2 (0.81)
Female	9.7 (0.87)	9.4 (0.89)

A repeated analysis of variance model was utilised for comparing the difference between frailty groups

SE standard error, *p < 0.05 compared to corresponding group of non-frail patients; **p < 0.001 compared to corresponding group of non-frail patients; ***p < 0.05 compared to number of drugs used prior to warfarin initiation (home) within the subgroup; †p < 0.05 compared to number of drugs used prior to warfarin initiation (home) in non-frail male patients

Cardiovascular drugs was the most commonly used drug class both in non-frail and frail patients, used by over 80% of the patients (Table 4). The use of beta-blockers, particularly, showed a tendency for increased use in both patient groups after warfarin initiation. Systemic antimicrobials, including antibiotics and antifungals, were used especially by frail patients before warfarin initiation (14.9% vs. 5.1% in non-frail patients), but their use increased in both patient categories during the hospital stay so that almost 25% of patients were taking an anti-infective medication at discharge.

Table 4

Drug use before (home) and after (discharge) warfarin initiation in frailty categories expressed as the proportions (%) and number of users (in brackets)

	Non-frail, n = 98		Frail, n = 47
	Home	Discharge	Home	Discharge
GI drugs	37.8 (37)	57.1 (56)	74.5 (35)	78.7 (37)
DM drugs	21.4 (21)	20.4 (20)	36.2 (17)	34.0 (16)
Insulins	5.1 (5)	7.1 (7)	21.3 (10)	19.1 (9)
Oral DM drugs	19.4 (19)	16.3 (16)	27.7 (13)	25.5 (12)
Vitamins and minerals	29.6 (29)	35.7 (35)	31.9 (15)	36.2 (17)
Antithrombotics	57.1 (56)	27.6 (27)	68.1 (32)	27.7 (13)
Heparins	3.1 (3)	16.3 (16)	4.3 (2)	19.1 (9)
Antiplatelets	56.1 (55)	12.2 (12)	66.0 (31)	14.9 (7)
Acetylsalicylic acid	50.0 (49)	11.2 (11)	48.9 (23)	8.5 (4)
Antianemic preparations	6.1 (6)	8.2 (8)	19.1 (9)	14.9 (7)
Cardiovascular drugs	78.6 (77)	88.8 (84)	91.5 (43)	93.6 (44)
Diuretics	37.8 (37)	37.8 (37)	46.8 (22)	46.8 (22)
Beta blockers	31.6 (31)	51.0 (50)	40.4 (19)	55.3 (26)
Calcium blockers	30.6 (30)	22.4 (22)	36.2 (17)	23.4 (11)
RA system drugs	62.2 (61)	58.2 (57)	66.0 (31)	55.3 (26)
Statins	54.1 (53)	60.2 (59)	55.3 (26)	48.9 (23)
Urological drugs and sex hormones	10.2 (10)	6.1 (6)	4.3 (2)	2.1 (1)
Hormonal preparations	17.3 (17)	15.3 (15)	19.1 (9)	21.3 (10)
Corticosteroids	7.1 (7)	7.1 (7)	8.5 (4)	10.6 (5)
Systemic antimicrobials	5.1 (5)	24.5 (24)	14.9 (7)	25.5 (12)
Antineoplastics and immunomodulators	4.1 (4)	4.1 (4)	10.6 (5)	10.6 (5)
Musculoskeletal system drugs	24.5 (24)	12.2 (12)	21.3 (10)	10.6 (5)
NSAIDa	9.2 (9)	0 (0)	6.4 (3)	0 (0)
Antigout drugs	8.2 (8)	9.2 (9)	6.4 (3)	6.4 (3)
Bisphosphonates	0 (0)	1.0 (1)	6.4 (3)	4.3 (2)
Nervous system	52.0 (51)	64.3 (63)	80.9 (38)	70.2 (33)
Acetaminophen	35.7 (35)	49.0 (48)	63.8 (30)	53.2 (25)
Opioids	8.2 (8)	26.5 (26)	34.0 (16)	25.5 (12)
Antiepileptics	6.1 (6)	7.1 (7)	6.4 (3)	8.5 (4)
Antipsychotics	4.1 (4)	2.0 (2)	10.6 (5)	10.6 (5)
Antidepressants	14.3 (14)	18.4 (18)	25.5 (12)	21.3 (10)
Non-selective MAO reuptake inhibitors	3.1 (3)	3.1 (3)	8.5 (4)	4.3 (2)
SSRI	5.1 (5)	8.2 (8)	2.1 (1)	2.1 (1)
MAO-A inhibitors	0 (0)	0 (0)	4.3 (2)	2.1 (1)
Other antidepressants	6.1 (6)	8.2 (8)	10.6 (5)	12.8 (6)
COPD and asthma drugs	23.5 (23)	16.3 (16)	27.7 (13)	31.9 (15)
Ophthalmic drugs	7.1 (7)	7.1 (7)	6.4 (3)	6.4 (3)

COPD chronic obstructive pulmonary disease, DM diabetes mellitus, GI gastrointestinal, MAO monoamine oxidase, MAO-A monoamine oxidase-A, NSAID non-steroidal anti-inflammatory drug, RA system, renin-angiotensin system, SSRI selective serotonin reuptake inhibitor

aExcluding glucosamine

The use of drugs potentially interacting with warfarin was analysed by individual medication, medication class and by interaction mechanism (Table 5). Antithrombotics and analgesics were the most commonly used interacting medications both in non-frail and frail patients before warfarin initiation. Acetylsalicylic acid was used by half of all patients, whereas the use of clopidogrel was more common in frail patients (27.1%) compared with non-frail patients (9.9%, p = 0.0135). An anticipated and statistically significant decrease was seen in the use of both clopidogrel and acetylsalicylic acid after warfarin initiation; approximately 10% of patients in both patient groups were using acetylsalicylic acid and only a few patients were taking clopidogrel at discharge. On the contrary, the use of enoxaparin significantly increased during hospital stay in both frailty categories (p = 0.0029 and p = 0.0196, for non-frail and frail groups, respectively). The use of acetaminophen was nearly two-fold in frail patients compared with non-frail patients before warfarin initiation (63.8% vs. 35.7%, respectively, p = 0.0014). After warfarin initiation, the use of acetaminophen increased in non-frail patients and decreased in frail patients, with the change being statistically significant in the former group. At discharge, about half of the patients in both groups were using acetaminophen. Less than 10% of patients in both groups were using non-steroidal anti-inflammatory drugs (NSAIDs) before warfarin initiation and no users was detected thereafter. An opposite trend was observed for tramadol, the use of which increased from 0.0% before warfarin initiation to 7.1% thereafter for non-frail patients and from 4.2% to 8.3% in frail patients, respectively.

Table 5

Proportions of potentially interacting drug users prior (home) and after (discharge) warfarin initiation (home) by frailty

% (n)	Non-frail, n = 98		Frail, n = 47
	Home	Discharge	Home	Discharge
Enoxaparin	3.1 (3)	15.3 (16)**	4.3 (2)	19.1 (9)*
Clopidogrel	10.2 (10)	2.0 (2)**	27.7 (13)***	6.4 (3)**
Acetylsalisylic acid	50.0 (49)	11.2 (11)**	48.9 (23)	8.5 (4)**
NSAIDsa	9.2 (9)	0.0 (0)**	6.4 (3)	0.0 (0)
Acetaminophen	35.7 (35)	49.0 (48)*	63.8 (30)***	53.2 (25)
Tramadol	0.0 (0)	7.1 (7)**	4.3 (2)	8.5 (4)
Senna glycosides	5.1 (5)	18.4 (18)**	12.8 (6)	29.8 (14)**
Simvastatin	11.2 (11)	9.2 (9)	12.8 (6)	12.8 (6)
Rosuvastatin	15.3 (15)	17.3 (17)	14.9 (7)	10.6 (5)
SSRIsb	5.1 (5)	8.2 (8)	2.1 (1)	2.1 (1)
SNRIsc	4.1 (4)	4.1 (4)	6.4 (3)	8.5 (4)
Oral anti-infectivesd	0.0 (0)	5.1 (5)*	2.1 (1)	6.4 (3)
CYP2C9 inhibitorse	3.1 (3)	20.4 (20)**	10.6 (5)	19.1 (9)*
Amiodarone	0.0 (0)	16.3 (16)**	2.1 (1)	6.4 (3)
Fibrates	3.1 (3)	2.0 (2)	6.4 (3)	6.4 (3)
CYP3A4 inhibitors	12.2 (12)	11.2 (11)	10.6 (5)	6.4 (3)
Corticosteroidsf	6.1 (6)	7.1 (7)	8.5 (4)	8.5 (4)
Levothyroxine sodium	10.2 (10)	10.2 (10)	10.6 (5)	10.6 (5)
Othersg	4.1 (4)	3.1 (3)	6.4 (3)	6.4 (3)

CYP cytochrome P450, NSAID non-steroidal anti-inflammatory drug, SNRI serotonin-norepinephrine reuptake inhibitor, SSRI selective serotonin reuptake inhibitor, *p < 0.05 compared to the proportion of users at home within the frailty category; **p < 0.01 compared to the proportion of users at home within the frailty category; ***p < 0.05 compared to the proportion of users at home in non-frail category

McNemar test was used for comparing the differences in the use of individual drugs between time points, and Fisher’s exact test was for comparing the differences between frailty groups

No statistically significant differences were observed in the proportions of users between frailty categories at discharge

aNSAIDs include indomethacin, meloxicam and ibuprofen (combination products)

bSSRIs include fluoxetine, citalopram, paroxetine, sertraline and escitalopram

cSNRIs include venlafaxine and duloxetine

dOral anti-infectives include dicloxacillin, sulfamethoxazole and trimethoprim, moxifloxacin and metronidazole

eCYP2C9 inhibitors include amiodarone, fenofibrate, gemfibrozil, sulfamethoxazole-trimethoprim and metronidazole

fCorticosteroids include dexamethasone, prednisolone, hydrocortisone and cortisone

gOthers include mesalazine, dipyridamole, carbimazole, mercaptopurine, azathioprine and phenytoin

The use of senna glycosides increased in both frail and non-frail patients during hospitalisation, being more common in frail patients (Table 5). The use of statins and fibrates was of a similar magnitude and remained as such in non-frail and frail patients over the hospital stay. The use of antidepressants remained low in both frailty groups.

The use of CYP2C9 inhibitors increased statistically significantly in both frailty groups. The increase was seen especially in non-frail patients and was mainly due to amiodarone; its contribution in the frail patients was smaller. No concomitant use of fluconazole (a CYP2C9 inhibitor) or CYP2C9 inducing drugs was observed; metronidazole was used at discharge by a single patient only in each group (data not shown). We also examined the use of known CYP3A4 inhibitors, which inhibit the metabolism of R-warfarin (Table 5). Fluoxetine was the only drug initiated over the admission, whereas the use of verapamil and diltiazem decreased over the admissions. No concomitant use was detected for other studied CYP3A4 inhibitors. When the proportions of interacting drug users at discharge were compared between frailty categories, no statistically significant differences were observed (Table 5).

Discussion

In this observational study, we examined the association between frailty and the exposure to potential interactions with warfarin in a real-care setting. We observed similar changes in the use of interacting drugs in both frail and non-frail groups between admission and discharge except for acetaminophen and amiodarone. After warfarin initiation, we found no significant differences in warfarin drug interaction frequencies between frail and non-frail patients. Overall, the exposure to interacting drugs was modest in both groups and potentially serious drug interactions were few. A slight decrease in the total number of medications was observed between admission and discharge in frail patients, whereas the opposite was seen in non-frail patients.

The results of this study are encouraging as they suggest that concomitant medication as a risk factor for bleeding is taken into account when warfarin is initiated regardless of patients’ frailty status. The study was conducted in a tertiary hospital and the patients included were predominantly treated in general medicine, cardiothoracic surgery, cardiology, and neurology units where warfarin is commonly prescribed and clinicians are likely to be well aware of warfarin drug interactions. The hospital setting may also have enabled the rationalising of medication in frail patients resulting in the decrease in the total number of drugs. On the contrary, the minor increase in total drug number seen in non-frail patients may be explained by better health status prior to admission, as indicated by the lower Charlson Comorbidity Index, and by the initiation of drug therapy to treat the cause of hospitalisation.

Of interacting drugs, the most notable changes were observed for antithrombotic medications. The significantly increased use of enoxaparin in both frailty groups may be explained by bridging the subtherapeutic period of warfarin therapy shortly after its initiation. The opposite was observed for antiplatelet drugs: in both groups, only approximately every tenth patient continued on acetylsalicylic acid and few patients had clopidogrel in use at discharge. We presume that these patients who continued on antiplatelet drugs had an indication for dual antithrombotic medication as the indication for medications other than warfarin was not documented in the case notes. The more frequent use of clopidogrel prior to warfarin initiation in frail patients may be attributable to more common cardiovascular morbidity compared with non-frail patients. Furthermore, the vast decrease in the use of antiplatelet drugs may also result from the switch to warfarin because of clinical reasoning rather than avoiding the interaction.

The use of NSAIDs was modest before warfarin initiation in all patients and no use was detected in either of the frailty groups after warfarin initiation. In earlier studies, NSAIDs have been among the most common interacting drugs in inpatients and outpatients taking warfarin [3, 4, 9, 27]. This trend seems to have changed and similar results to ours have been recently published in large register-based studies [11, 28, 29]. These findings may indicate increased awareness of clinicians of the increased bleeding risk associated with concomitant use of NSAIDs with warfarin. In our study population, the avoidance of prescribing NSAIDs may have contributed to the increased use of tramadol and acetaminophen in non-frail patients. Moreover, operations were more common in non-frail compared with frail patients (44.1% vs 28.5%, p = 0.06) and the analgesic effect of NSAIDs may have been considered inadequate for postoperative pain treatment. However, neither tramadol nor acetaminophen are trouble-free in patients taking warfarin. Tramadol impairs platelet function by inhibiting serotonin reuptake to platelets [30] and its concomitant use with warfarin is also associated with excess anticoagulation [31-34]. A metabolite of acetaminophen, N-acetyl-p-benzoquinone, interferes with vitamin K metabolism and the synthesis of coagulation factors [35] thereby potentiating the warfarin response [36-38]. Moreover, acetaminophen may also have antiaggregatory effects [39]. Parallel results of increased use of tramadol and avoidance of NSAIDs were also reported by a Swedish register-based study, indicating that the warfarin-tramadol interaction may be poorly known among clinicians [28]. Altogether, pain management in patients receiving warfarin is a clinical challenge because of various types of drug interactions between commonly used analgesics and warfarin.

Another noteworthy finding in our study was the increase in the use of CYP2C9 inhibiting drugs in both groups. In non-frail patients, amiodarone constituted 80% of the CYP2C9 inhibitor use at discharge whereas in frail patients amiodarone, fibrates and oral anti-infectives each comprised one third of these interactions. The common use of amiodarone in our study population is most likely explained by cardiac surgery procedures, e.g. heart valve replacement and cardiac bypass surgery, performed in tertiary hospitals, and these would have been more likely in non-frail patients. Although the warfarin-amiodarone interaction is of clinical significance and leads to an increased anticoagulant effect by inhibiting warfarin metabolism [40], long-term use and stable dosing of amiodarone enables the control of the effect of interaction by adjusting warfarin dose according to INR values. The same principle applies also to CYP2C9 inhibiting fibrates whereas oral anti-infectives are more challenging: not only do they inhibit the metabolism of warfarin but they also affect the gut microbiota disturbing the vitamin K production. Therefore, the effects of anti-infectives on warfarin response are difficult to predict and control even after the course. Nevertheless, the number of interactions caused by oral anti-infectives was few and by CYP2C9 inhibitors modest in total, mainly comprising amiodarone, the effect of which (as discussed) is possible to compensate by warfarin dosing.

We also detected a significant increase in senna use in both non-frail and frail patients after warfarin initiation. Constipation is a common problem in hospitalised elderly patients [41]. Senna increases bowel motility thereby potentially decreasing the absorption of vitamin K and resulting in elevated INR values [42]. In patients newly started on warfarin, senna use may lead to exaggerated anticoagulation and early bleeding complications despite close INR monitoring during the hospital admission. The use of simvastatin and rosuvastatin remained at a similar order of magnitude in both frailty groups before and after warfarin initiation. The clinical significance of the warfarin–statin interaction has been a matter of discrepancy in previous literature [43, 44]. A recent nationwide database study found no association between the concomitant use of statins and an increased rate of bleeding in new warfarin users [45]. We suspect that the inconsistency in the literature about the significance of the warfarin–statin interaction as well as the clinical experience of prescribing physicians on the concomitant use may explain the stable use of statins in our study.

This study has some important strengths and limitations. The main strength of our study is the comprehensive and detailed data describing real-world drug use and capturing an incident cohort of warfarin users without previous oral anticoagulation use. As drugs were administered during the inpatient care, the actual exposure to interacting medication is highly likely. The most significant limitation of this study is the small sample size. The insignificant differences in the interaction drug use between frailty classes may be due to the small number of observations. This study was performed at a single hospital and the results may be influenced by local practices, which may hinder the generalisation of our results.

Conclusions

Our study showed that frailty status is not associated with exposure to drug interactions increasing the bleeding risk in new warfarin users. Acetaminophen, CYP2C9 inhibitors and senna were the most common interacting drugs in all patients. Overall, the initiation of warfarin therapy appeared to be well considered in relation to other medications independent of a patient’s frailty status. However, future studies including larger study populations and longer follow-up are required to confirm our findings and to study the sustainability of medication changes.

Below is the link to the electronic supplementary material.

Supplementary material 1 (PDF 106 kb)

The frequency of warfarin drug interactions was moderate and did not differ in frail and non-frail patients after warfarin initiation.

The use of non-steroidal anti-inflammatory drugs and antiplatelets decreased following warfarin initiation in both frail and non-frail patients. Acetaminophen, cytochrome P450 2C9 inhibiting drugs and senna glycosides were the most common interacting drugs in both groups.

Overall, potential drug interactions appeared to be taken into account at warfarin initiation independent of a patient’s frailty status.