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DOI: 10.1055/s-0044-1785524
Disease Burden, Clinical Outcomes, and Quality of Life in People with Hemophilia A without Inhibitors in Europe: Analyses from CHESS II/CHESS PAEDs
Abstract
Introduction Limited data relating to treatment burden, quality of life, and mental health burden of hemophilia A (HA) are currently available.
Aim To provide a comprehensive overview of unmet needs in people with HA (PwHA) using data generated from the Cost of Haemophilia in Europe: a Socioeconomic Survey-II (CHESS II) and CHESS in the pediatric population (CHESS PAEDs) studies.
Methods CHESS II and CHESS PAEDs are cross-sectional surveys of European males with HA or hemophilia B (HB) aged ≥18 and ≤17 years, respectively. Participants with FVIII inhibitors, mild HA, or HB were excluded from this analysis, plus those aged 18 to 19 years. Annualized bleeding rates (ABRs), target joints, and other patient-reported outcomes were evaluated.
Results Overall, 468 and 691 PwHA with available data for the outcomes of interest were stratified by hemophilia severity and treatment regimen in CHESS II and CHESS PAEDs, respectively. In these studies, 173 (37.0%) and 468 (67.7%) participants received FVIII prophylaxis, respectively; no participants received the FVIII mimetic emicizumab or gene therapy. ABRs of 2.38 to 4.88 were reported across disease severity and treatment subgroups in both studies. Target joints were present in 35.7 and 16.6% of participants in CHESS II and CHESS PAEDS; 43.8 and 23.0% had problem joints. Chronic pain was reported by a large proportion of PwHA (73.9% in CHESS II; 58.8% in CHESS PAEDs). Participants also reported low EQ-5D scores (compared with people without HA), anxiety, depression, and negative impacts on their lifestyles due to HA.
Conclusions These analyses suggest significant physical, social, and mental burdens of HA, irrespective of disease severity. Optimization of prophylactic treatment could help reduce the burden of HA on patients.
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Introduction
Despite hemophilia A (HA) severity being classified by level of factor (F)VIII activity, the heterogeneity in bleeding phenotypes requires an individualized approach to treatment and prevention of bleeds for the best outcomes in individual patients.[1] Joint bleeding and resultant hemophilic arthropathy are common among people with HA (PwHA) of all ages and disease severities, despite the aim of prophylactic treatment to prevent recurring joint bleeds, demonstrating the necessity for improvement in the management of HA.[2] [3] [4] [5] In the absence of prophylaxis, PwHA can experience frequent spontaneous bleeding and long-term health consequences, including premature mortality.[1]
In previous analyses from the Cost of Haemophilia in Europe: a Socioeconomic Survey (CHESS) study, target joints were associated with, and a significant driver of, chronic pain, decreased health-related quality-of-life (HRQoL) scores, and increased direct costs in PwHA.[6] [7]
Treatment practice varies throughout Europe, with both prophylactic and on-demand treatment used in PwHA with moderate and severe disease.[8] Current treatment programs require optimization, as PwHA still present with high numbers of bleeds and target joints regardless of treatment approach.[8] In a separate analysis of people with moderate (n = 864) and severe HA (n = 1810), both groups showed similar annualized bleeding rates (ABRs) and hemophilia joint health scores, suggesting PwHA, particularly those with moderate HA, are not receiving optimal treatment.[9]
Limited data relating to treatment burden via patient-reported outcomes in PwHA are available.[10] [11] [12] [13] However, treatment burden, including time for preparation and administration of treatment, and infusion frequency, may impact treatment adherence.[14] In addition, many PwHA perceive multiple barriers to initiation of prophylaxis, resulting in reduced control of their hemophilia and thus limiting their daily activities.[11] [13] [15]
Reports of the mental health burden of HA and its treatment are scarce, potentially underrepresenting the impact of HA in this population.[12] Previously published data highlight the impact of HA on quality of life (QoL) for both adults and children: PwHA experience anxiety and depression more often than the general population, which often goes undiagnosed and is associated with lower treatment adherence.[6] [16] [17] QoL data for the nonsevere population are also based on small datasets.
Further analysis of PwHA is required to accurately determine their unmet needs. This analysis provides a comprehensive overview of real-world outcomes in PwHA receiving replacement FVIII across Europe using data generated from the CHESS II and CHESS in the pediatric population (CHESS PAEDs) studies.
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Methods
Study Design
We conducted retrospective analyses of the interim CHESS II and final CHESS PAEDs study populations, the methodologies of which have been reported previously.[3] [18]
CHESS II was a cross-sectional survey of adult men (aged ≥ 18 years) with HA or hemophilia B (HB) of any severity, with or without FVIII inhibitors, across eight European countries (Germany, Spain, France, Italy, Romania, the Netherlands, Denmark, and the United Kingdom), performed between 2019 and 2020. Participants voluntarily self-reported HRQoL and nondirect medical and indirect costs (relating to work productivity outcomes [patient/caregiver presenteeism/absenteeism or patient early retirement] and caregiver burden [hours of care per week]) via a paper-based questionnaire. Not all participants for whom clinical data are available completed a questionnaire, which explains variable participant numbers for some HRQoL endpoints. Health care providers completed online forms with clinical information from the participants' medical records and health care resource utilization, from which direct medical costs were derived.
CHESS PAEDs used a similar design with male children and adolescents (aged ≥1 years to ≤17 years of age with ≥12 months of data available) with moderate (FVIII levels 1–5%) or severe (FVIII level <1%) HA or HB, with or without inhibitors. Participants were sampled from five European countries (France, Germany, Italy, Spain, and the United Kingdom) between 2017 and 2018. Information on hemophilia-related costs and HRQoL was provided by either the participant or the caregiver (dependent on age and questionnaire).
For this analysis, data from all CHESS participants with inhibitors to FVIII, mild HA, or HB of any severity were excluded. CHESS PAEDs and CHESS II were conducted as separate studies, with a 2-year gap between data collection for the two studies. As a result of this, overlap in populations may be possible (i.e., patients who were 16–17 years old during CHESS PAEDs may have been 18–19 during data collection for CHESS II and therefore captured in both studies). Therefore, to avoid duplication, CHESS II participants aged 18 to 19 years were also excluded from this analysis. Participant treatment regimen was categorized as prophylaxis or “other” (on-demand or no treatment in the preceding 12 months). Only participants for whom data were available for the outcomes of interest are included in this analysis; no imputation was performed.
Physicians reported presence and frequency of recurrent bleeding into a joint (“target joints”) and joints with chronic pain and/or a limited range of movement (“problem joints”). Chronic pain was physician reported on a 4-level scale that included no chronic pain, and mild, moderate, or severe chronic pain; definitions are included in [Supplementary Material S1] (available in the online version). Anxiety and depression were reported as comorbidities by the physicians, who abstracted the data from medical records. For participants in CHESS PAEDs, the age range for those with available anxiety and depression information was 4 to 17 years.
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Patient-Reported Health-Related Quality of Life
Patient-reported HRQoL was assessed using the EuroQol EQ-5D-5L questionnaire in CHESS II and the pediatric version of the EQ-5Q-3L (EQ-5D-Y) in CHESS PAEDs. The EQ-5D-5L comprises five domains (mobility, self-care, performance of usual activities, pain/discomfort, and anxiety/depression) with five levels. The EQ-5D-Y comprises the aforementioned five domains, with three levels.[19] CHESS PAEDs participants aged 8 to 17 completed the EQ-5D-Y themselves. CHESS II EQ-5D-5L index scores were derived via the United Kingdom value set for the EQ-5D-3L and cross-walk function.[20] EQ-5D-Y index scores were valued using the Spanish EQ-5D-Y value set.[21] Health state index utility scores were used to measure general health status and HRQoL, and were derived via algorithm from responses across all five domains; scores ranged from 0 (equivalent to “dead”) to 1 (“perfect health”). Derived scores of <0 (“worse than dead”) were possible.[22] Both CHESS study questionnaires used a 5-point Likert scale to evaluate hemophilia-related limitations related to reduction of social activities, exercise/physical activity, general opportunities, and frustration with the influence of hemophilia on their daily lives. Lower age limits were applied, when relevant, in QoL measures.
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Costs
Direct (associated with the health care system), indirect (not associated with the health care system), and total costs were estimated at the patient level for a 12-month retrospective period in accordance with the respective country-level unit cost databases.
Both the CHESS II and CHESS PAEDs studies received institutional review board approval, and informed consent, or assent where appropriate, was obtained.
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Results
Study Population
The CHESS II analysis included 468 PwHA with a mean age of 38.7 years ([Tables 1] and [2]). Of the 190/468 (40.6%) participants with moderate HA, 16 (8.4%) received primary FVIII prophylaxis (prophylaxis before the second joint bleed and aged <3 years); the majority (174 [91.6%]) received other treatment. Of the 278/468 (59.4%) participants with severe HA, 157 (56.5%) received FVIII prophylaxis (n = 33 [11.9%] primary; n = 124 [44.6%] secondary [prophylaxis initiated after two or more joint bleeds, usually at age ≥3 years]) and 121 (43.5%) received other treatment. No participant received emicizumab or gene therapy.
|
Characteristic |
(N = 468) |
|---|---|
|
Age, y |
|
|
Mean (SD) |
38.71 (13.95) |
|
Median (IQR) |
37.50 (22) |
|
Age category, y, n (%) |
|
|
18–35 |
210 (44.9) |
|
36–59 |
217 (46.4) |
|
60+ |
41 (8.8) |
|
Treatment approach, n (%) |
|
|
Prophylaxis |
173 (37.0) |
|
EHL FVIII |
25 (14.5) |
|
SHL or plasma-derived FVIII |
131 (75.7) |
|
Unknown |
17 (9.8) |
|
Other |
295 (63.0) |
|
EHL FVIII |
27 (9.2) |
|
SHL or plasma-derived FVIII |
152 (51.5) |
|
No FVIII administered in prior 12 mo[a] |
115 (39.0) |
|
Unknown |
1 (0.3) |
|
Severity, n (%) |
|
|
Moderate |
190 (40.6) |
|
Severe |
278 (59.4) |
|
Years since first diagnosis |
|
|
Mean (SD) |
24.31 (15.24) |
|
Median (IQR) |
23 (20) |
|
Years since first diagnosis category, n (%) |
|
|
< 5 |
66 (14.1) |
|
5–10 |
30 (6.4) |
|
> 10 |
372 (79.5) |
|
Country, n (%) |
|
|
Germany |
37 (7.9) |
|
Spain |
149 (31.8) |
|
France |
42 (9.0) |
|
Italy |
188 (40.2) |
|
Romania |
3 (0.6) |
|
Holland |
1 (0.2) |
|
UK |
48 (10.3) |
Abbreviations: EHL, extended half-life; IQR, interquartile range; SD, standard deviation; SHL, standard half-life.
a All participants who had not received FVIII in the prior 12 months had moderate hemophilia A.
|
Severity |
Total (N = 468) |
||||
|---|---|---|---|---|---|
|
Moderate (n = 190) |
Severe (n = 278) |
||||
|
Prophylaxis (n = 16) |
Other (n = 174) |
Prophylaxis (n = 157) |
Other (n = 121) |
||
|
Age |
|||||
|
Mean (SD) |
42.4 (16.9) |
39.6 (14.6) |
38.7 (14.0) |
37.0 (12.4) |
38.7 (13.9) |
|
Median (IQR) |
45.5 (29.5) |
38 (21) |
38 (22) |
36 (17) |
37.5 (22) |
|
Age category, n (%) |
|||||
|
18–35 |
7 (43.8) |
77 (44.3) |
67 (42.7) |
59 (48.8) |
210 (44.9) |
|
36–59 |
7 (43.8) |
77 (44.3) |
78 (49.7) |
55 (45.5) |
217 (46.4) |
|
60+ |
2 (12.5) |
20 (11.5) |
12 (7.6) |
7 (5.8) |
41 (8.8) |
|
Total |
16 (100) |
174 (100) |
157 (100) |
121 (100) |
468 (100) |
|
Treatment type, n (%) |
|||||
|
EHL FVIII |
1 (6.3) |
9 (5.2) |
24 (15.3) |
18 (14.9) |
52 (11.1) |
|
SHL or plasma-derived FVIII |
2 (12.5) |
50 (28.7) |
129 (82.2) |
102 (84.3) |
283 (60.5) |
|
No FVIII administered in prior 12 mo[a] |
0 (0) |
115 (66.1) |
0 (0) |
0 (0) |
115 (24.6) |
|
Unknown |
13 (81.3) |
0 (0) |
4 (2.5) |
1 (0.8) |
18 (3.8) |
|
Country |
|||||
|
Germany |
0 (0.0) |
16 (9.2) |
14 (8.9) |
7 (5.8) |
37 (7.9) |
|
Spain |
11 (68.8) |
53 (30.5) |
47 (29.9) |
38 (31.4) |
149 (31.8) |
|
France |
0 (0.0) |
16 (9.2) |
13 (8.3) |
13 (10.7) |
42 (9.0) |
|
Italy |
5 (31.3) |
68 (39.1) |
67 (42.7) |
48 (39.7) |
188 (40.2) |
|
Romania |
0 (0.0) |
2 (1.2) |
0 (0.0) |
1 (0.8) |
3 (0.6) |
|
Holland |
0 (0.0) |
1 (0.6) |
0 (0.0) |
0 (0.0) |
1 (0.2) |
|
UK |
0 (0.0) |
18 (10.3) |
16 (10.2) |
14 (11.6) |
48 (10.3) |
Abbreviations: EHL, extended half-life; IQR, interquartile range; SD, standard deviation; SHL, standard half-life.
a All participants who had not received FVIII in the prior 12 months had moderate hemophilia A.
The CHESS PAEDs analysis included 691 children and adolescents with HA, with a mean age of 10.3 years, of whom 53.8% (n = 372) were aged <12 years ([Tables 3] and [4]). Of 282/691 (40.8%) participants with moderate HA, 136 (48.2%) received FVIII prophylaxis and 146 (51.8%) received other treatment. Of 409/691 (59.2%) with severe HA, 332 (81.2%) received FVIII prophylaxis and 77 (18.8%) received other treatment. No participant received emicizumab or gene therapy.
|
Characteristic |
N = 691 |
|---|---|
|
Age, y, mean (SD) |
10.33 (4.70) |
|
Age category, y, n (%) |
|
|
< 2 |
20 (2.9) |
|
2–11 |
352 (50.9) |
|
12–17 |
319 (46.2) |
|
Treatment approach, n (%) |
|
|
Prophylaxis |
468 (67.7) |
|
EHL FVIII |
81 (17.3) |
|
SHL or plasma-derived FVIII |
383 (81.8) |
|
Unknown |
4 (0.9) |
|
Other |
223 (32.3) |
|
EHL FVIII |
27 (12.1) |
|
SHL or plasma-derived FVIII |
109 (48.9) |
|
No FVIII administered in prior 12 mo[a] |
83 (37.2) |
|
Unknown |
4 (1.8) |
|
Severity, n (%) |
|
|
Moderate |
287 (40.8) |
|
Severe |
416 (59.2) |
|
Country, n (%) |
|
|
France |
148 (21.1) |
|
Germany |
112 (15.9) |
|
Italy |
167 (23.8) |
|
Spain |
168 (23.9) |
|
UK |
108 (15.4) |
Abbreviations: EHL, extended half-life; SD, standard deviation; SHL, standard half-life.
a All participants who had not received FVIII in the prior 12 months had moderate hemophilia A.
|
Severity |
Total (N = 691) |
||||
|---|---|---|---|---|---|
|
Moderate (n = 282) |
Severe (n = 409) |
||||
|
Prophylaxis (n = 136) |
Other (n = 146) |
Prophylaxis (n = 332) |
Other (n = 77) |
||
|
Age |
|||||
|
Mean (SD) |
10.4 (4.6) |
11.0 (4.7) |
10.3 (4.7) |
9.1 (4.6) |
10.3 (4.7) |
|
Median (IQR) |
10 (7) |
12 (8) |
11 (8) |
10 (8) |
10 (8) |
|
Age category, n (%) |
|||||
|
< 2 |
5 (3.7) |
5 (3.4) |
8 (2.4) |
2 (2.6) |
20 (2.9) |
|
2–11 |
67 (49.3) |
67 (45.9) |
169 (50.9) |
49 (63.6) |
352 (50.9) |
|
12–17 |
64 (47.1) |
74 (50.7) |
155 (46.7) |
26 (33.8) |
319 (46.2) |
|
Treatment type, n (%) |
|||||
|
EHL FVIII |
21 (15.4) |
9 (6.2) |
60 (18.1) |
18 (23.4) |
108 (15.6) |
|
SHL or plasma-derived FVIII |
113 (83.1)0 (0) |
54 (37.0) |
270 (81.3) |
55 (71.4) |
492 (71.2) |
|
No FVIII administered in prior 12 mo[a] |
2 (1.5) |
82 (56.2) |
0 (0) |
1 (0.1) |
83 (12.0) |
|
Unknown |
0 (0) |
1 (0.6) |
2 (0.6) |
3 (3.9) |
8 (1.2) |
|
Country, n (%) |
|||||
|
France |
16 (11.8) |
6 (4.1) |
108 (32.5) |
17 (22.0) |
147 (21.3) |
|
Germany |
30 (22.1) |
14 (9.6) |
50 (15.1) |
18 (23.4) |
112 (16.2) |
|
Italy |
18 (13.2) |
63 (43.2) |
72 (21.7) |
13 (16.9) |
166 (24.0) |
|
Spain |
56 (41.2) |
45 (30.8) |
55 (16.6) |
5 (6.5) |
161 (23.3) |
|
UK |
16 (11.8) |
18 (12.3) |
47 (14.2) |
24 (31.2) |
105 (15.2) |
Abbreviations: EHL, extended half-life; IQR, interquartile range; SD, standard deviation; SHL, standard half-life.
a All participants who had not received FVIII in the prior 12 months had moderate hemophilia A.
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Annualized Bleeding Rate
The mean ABR was 3.36 for the overall population of CHESS II ([Table 5]) and 3.62 for the 691 PwHA with recorded ABRs in CHESS PAEDs ([Table 6]).
Abbreviations: ABR, annualized bleeding rate; IQR, interquartile range; SD, standard deviation.
Abbreviations: ABR, annualized bleeding rate; IQR, interquartile range; SD, standard deviation.
Mean ABRs were similar between treatment regimens in the moderate population: 2.38 in those on prophylaxis (n = 16) and 2.54 in participants on other treatment (n = 174) in CHESS II. In CHESS PAEDs, the mean ABR was 4.01 in participants on prophylaxis (n = 136) and 4.32 in those on other treatment (n = 146). For participants with severe HA, mean ABRs in CHESS II were 3.84 in those receiving prophylaxis (n = 157) and 4.02 in those receiving other treatment (n = 121). In CHESS PAEDs, the mean ABR was 2.86 on prophylaxis (n = 332) and 4.88 on other treatment (n = 77).
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Target Joints
In CHESS II, 167 participants (35.7%) had ≥1 target joint ([Table 5]); in CHESS PAEDs, 115 participants had ≥1 target joint (16.6%; [Table 6]).
The proportion of participants with target joints was numerically similar across disease severities and treatment regimens in both studies. In the moderate population of CHESS II, 37.5 and 22.4% of participants receiving prophylaxis and other treatment, respectively, had target joints; in the severe population, these percentages were 42.7 and 45.5%. In CHESS PAEDs, target joints were present in 17.6% of participants with moderate HA receiving prophylaxis and 4.8% receiving other treatment, and in 21.7% of participants with severe HA receiving prophylaxis and 15.6% receiving other treatment.
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Problem Joints
In CHESS II, 205 participants (43.8%) had ≥1 problem joint ([Table 5]); in CHESS PAEDs, 159 participants had ≥1 problem joint (23.0%; [Table 6]).
In CHESS II, more participants with severe disease reported ≥1 problem joint (47.1%) compared with the moderate population (38.9%). Between disease severity populations, similar proportions of participants reported 1 problem joint; however, a greater proportion in the severe population reported ≥2 problem joints. In CHESS PAEDs, reports of problem joints were similar across disease severity and treatment regimen subgroups, although they were reported less frequently in participants receiving other treatment for moderate HA, compared with prophylaxis. Problem joints were reported in participants aged 1 to 17 years, although 77% of reports were from participants aged > 8 years.
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Chronic Pain
In CHESS II, 346 participants (73.9%) had chronic pain ([Table 5]). In CHESS PAEDs, 406 participants (58.8%; aged 1–17) had chronic pain ([Table 6]).
Across disease severities in CHESS II, a greater proportion of those with severe disease had moderate or severe pain compared with those who had moderate HA (31.3 vs. 20.5% for moderate pain; 10.1 vs. 1.6% for severe pain). However, similar proportions of participants had mild or no pain across disease severities and treatment regimens, with the exception of PwHA receiving other treatment for moderate disease, where a larger proportion reported no pain.
In CHESS PAEDs, similar proportions of participants reported mild or no pain irrespective of disease severity or treatment regimen. A greater proportion of the moderate population reported no pain than the severe population (46.8 vs. 37.4%). Only two participants, receiving prophylaxis for severe disease, reported severe pain.
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Anxiety and Depression
In CHESS II and CHESS PAEDS, 86 (18.4%) and 56 (8.1%; aged 3–17 years) participants, respectively, had feelings of anxiety ([Tables 5] and [6]). Reports of anxiety in CHESS II were greater in those receiving prophylaxis across both disease severities: 50.0% of participants receiving prophylaxis versus 16.1% receiving other treatment in the moderate population and 21.7 versus 13.2% in the severe population.
Depression was reported in 49 (10.5%) participants in CHESS II ([Table 5]), and 13 (1.9%; aged 6–17 years) participants in CHESS PAEDs ([Table 6]). The proportions of participants with depression were consistent across disease severity and treatment regimen subgroups in both studies. Reports of depression were lower in all subgroups for the pediatric population compared with adults.
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Quality of Life
In CHESS II, the mean EQ-5D score was 0.71 for the overall population and was similar across disease severity and treatment regimen subgroups (0.66–0.76; [Table 7]).
Abbreviations: IQR, interquartile range; SD, standard deviation.
In CHESS PAEDs, the mean EQ-5D-Y score was 0.65 for the overall population (age range: 8–17 years) and ranged between 0.65 and 0.70 for those with moderate HA receiving prophylaxis or any treatment for severe disease ([Table 8]). However, participants with moderate HA receiving other treatment reported a lower score of 0.50.
Abbreviations: IQR, interquartile range; SD, standard deviation.
In both CHESS II and CHESS PAEDs, participants reported they had to reduce or give up social activities or exercise, missed out on opportunities, and felt frustrated by the influence of HA on their lifestyle ([Tables 7] and [8]).
ABR, target and problem joints, chronic pain, anxiety and depression, and QoL outcomes split by country of origin for CHESS II and CHESS PAEDs are presented in [Supplementary Tables S1] and [S2] (available in the online version), respectively.
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Costs
Direct, indirect, and total costs are summarized in [Table 9] for CHESS II and [Table 10] for CHESS PAEDs. In both studies, direct medical costs and total costs were higher in participants with severe HA versus participants with moderate HA.
Abbreviations: EUR, Euros; IQR, interquartile range; PPIE, patient and public involvement and engagement; SD, standard deviation.
Abbreviations: EUR, Euros; IQR, interquartile range; PPIE, patient and public involvement and engagement; SD, standard deviation.
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Discussion
This retrospective analysis of the CHESS II and CHESS PAEDs population studies reveals high ABRs and prevalence of target joints across disease severities and treatment regimens in PwHA. Such characteristics may contribute to chronic pain and reduced QoL measures, leading to physical, mental, social, and economic impacts in adults, children, and their caregivers. These findings suggest potential suboptimal administration of HA treatment, including prophylaxis, in PwHA in Europe.
Despite the larger proportion of people with severe HA compared with moderate HA in this analysis, a smaller proportion of adults in CHESS II received FVIII prophylactic treatment than other treatment. This demonstrates a considerable gap between the current standards of care and the aspirations laid out in the recent World Federation of Hemophilia (WFH) guidelines.[1]
Surprisingly, in CHESS II, ABRs and numbers of target joints were similar regardless of treatment regimen, perhaps reflecting the implementation of prophylaxis in patients who are considered to have severe bleeding phenotype. In CHESS PAEDs, target joints were present in similar proportions across subgroups; however, ABR values were higher in participants receiving other treatment versus prophylaxis, especially in the severe population, in line with clinical experience. These results indicate suboptimal administration of prophylactic treatment across PwHA in Europe, as optimal treatment aims to decrease ABRs and reduce numbers of target joints.[1] The failure to achieve the latter goal particularly reflects the recurrence of joint bleeds and inadequate prophylaxis.
Suboptimal outcomes may also indicate barriers to prophylaxis uptake in children/adolescents, such as parental inability to administer treatment, fear of needles, considerable burden of frequent injections, or not wanting to stand out from their peers. Additionally, ABRs and target joint scores for moderate and severe populations were similar, suggesting that many people with moderate HA may have inadequate bleed control. This issue has also been identified previously.[17]
High ABRs and the presence of target joints in PwHA are associated with compromised joint integrity, such as chronic synovitis or hemophilic arthropathy, leading to the development of problem joints, generally characterized by chronic pain and/or a limited range of movement. In these analyses, problem joints were more common in the adult population compared with children and were more prevalent in the severe population compared with other participants in CHESS II, representing cumulative joint damage over the lifetime of the patient. A previous analysis of problem joints in CHESS II and CHESS PAEDs indicated an association between problem joints and worsening clinical and QoL outcomes across disease severities.[23] Indeed, higher levels of chronic pain were reported in CHESS II than CHESS PAEDs. However, participants in both analyses had similar prevalence of chronic pain, regardless of treatment, indicating a need for more effective pain management in PwHA.[7]
The prevalence of depression and anxiety were similar across disease severity groups in both adult and pediatric populations, although they were numerically higher in those with moderate versus severe disease, which may warrant further examination of the factors impacting mental health in these groups. Subgroup analyses demonstrated a higher prevalence of anxiety in adults receiving prophylaxis than in those receiving other treatment, perhaps reflecting the burden perceived by participants; however, this was in a comparatively smaller subgroup. Depression was reported least frequently in adults with severe HA receiving prophylaxis and most frequently in those receiving prophylaxis for moderate HA. This may be related to the delayed initiation of prophylaxis in those with moderate HA, as poor disease outcomes manifest later in the course of disease. Furthermore, a participant may be frustrated by the treatment burden of prophylaxis should they not see equivalent improvements in their disease burden. As a result, increased monitoring, the use of a validated self-assessment tool, and the implementation of a mental health professional in the multidisciplinary team would all be valuable steps toward tackling mental health challenges in people with hemophilia. Indeed, WFH guidelines recognize the importance of psychosocial care in the management of hemophilia; recommendations are provided on how the hemophilia treatment center social worker and/or other members of the care team can support people with hemophilia and their caregivers in challenges with mental health, such as anxiety or depression.[1]
The prevalence of anxiety observed in adults in this analysis was slightly lower than in previous studies of PwHA.[17] [24] In an analysis of adults with hemophilia, the presence of depression, anxiety, and pain were found to be interrelated.[7] It is therefore possible that reducing the depression and anxiety identified in these populations may be achieved via improvements to pain management.
EQ-5D scores reported in CHESS II were low compared with the norms for the general population published previously.[25] [26] [27] Similar scores were reported in CHESS PAEDs, indicating a similar deficiency in HRQoL, although general population norms are unavailable for comparison. Those receiving prophylaxis reported greater impact on their QoL compared with those receiving other treatment. However, the majority of those receiving prophylaxis are likely to have severe HA, per the treatment guidelines, and results may therefore be impacted primarily by disease severity, rather than treatment received.[1]
Across both study populations, both PwHA and caregivers reported impacts on their daily lives, including missed opportunities, reduced social activities, and frustration with the influence of hemophilia over their lives. Lack of social support from family and friends has previously been linked to the presence of depressive symptoms in PwHA, demonstrating the potential to improve mental welfare by improving symptoms that affect daily activities and hence allow PwHA to engage in social activities.[7] [28]
Such impacts on the lives of PwHA may be consequences of the disease burden of HA. Current disease characteristics of PwHA in Europe highlight a remaining unmet need for improvements in the standard of care, the achievement of which could reduce the burden of HA and therefore tackle subsequent impacts on QoL and daily activities. To this point, there is growing evidence suggesting subcutaneously administered emicizumab, which has been characterized as a less burdensome prophylaxis option than standard-of-care FVIII replacement, can provide improved HRQoL.[29] Future analyses including therapies such as emicizumab, gene therapy, and other novel treatment options could provide necessary insight into whether the changing treatment landscape translates into improvements in the suboptimal outcomes reported here in participants receiving FVIII replacement.
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Limitations
The results of these analyses should be interpreted in the context of limitations inherent to cross-sectional studies measuring outcomes from defined snapshots in time. A further limitation may be the sample size, specifically in the number of participants with moderate HA receiving prophylaxis; therefore, interpretation of the results should take this into consideration. Participation in the CHESS studies was entirely voluntary and contingent on patients visiting their physician, so selection bias cannot be excluded. Additionally, there may be a degree of recall bias in patient-reported outcomes surveys and possible medical chart data abstraction errors. Possible country-specific differences in care provision and health care systems should also be taken into consideration when interpreting these results.
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Conclusion
These analyses highlight the unmet physical, mental, social, and economic needs faced by PwHA in Europe. Almost half of all PwHA, regardless of age or disease severity, still experienced ABRs ≥2, and target joints and problem joints were prevalent across all subgroups. Such outcomes highlight the suboptimal administration of prophylactic treatment in PwHA in Europe. Disease burden was associated with chronic pain, anxiety and depression, and negative impacts on QoL regardless of disease severity. These observations may reflect the need for improved prophylactic treatment options and optimal administration of such treatments. Our findings may be useful for defining new treatment strategies that decrease not only the physical burden, but also the social and mental burden of hemophilia for people in Europe.
What is known about this topic?
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Despite the availability of improved treatment options for people with hemophilia A (HA) in Europe, joint bleeding and resultant hemophilic arthropathy are common among people with HA of all ages.
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As a result, there are unmet needs among adults and children with moderate or severe HA in Europe.
What does this paper add?
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This analysis highlights the suboptimal administration of prophylactic treatment in adults and children with moderate or severe HA in Europe.
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There also appears to be association of disease burden with subsequent impacts on key patient-reported outcomes, such as prevalence of chronic pain, depression, and anxiety, regardless of disease severity.
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Improved prophylactic treatment options and optimal administration of these treatments may facilitate new treatment strategies that decrease the burden of HA in Europe, and bring us closer to achieving the goals laid out in the latest WFH guidelines.
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Conflict of Interest
P.C. has served on advisory boards for Bayer, Boehringer Ingelheim, Apcintex, CSL Behring, Chugai, Freeline, Novo Nordisk, Pfizer, F. Hoffmann-La Roche Ltd, Sanofi, Spark, Sobi, and Takeda and has received research funding from Bayer, CSL Behring, Freeline, Novo Nordisk, Pfizer, Takeda and Sobi. R.O. is a previous employee of F. Hoffmann-La Roche Ltd and current employee of AstraZeneca Plc. F.N. reports employment for F. Hoffmann-La Roche Ltd and Kite Pharma. E.F.G. is an employee of HCD Economics and has served on a Haemophilia Patient Council organized by BMRN on behalf of an advocacy organization representative and participated in an advisory board organized by Roche as a patient representative. M.A. is an employee and shareholder of F. Hoffmann-La Roche Ltd. K.M. is an employee and shareholder of F. Hoffmann-La Roche Ltd. T.B. is an employee of HCD Economics. B.N. reports speaker's fees from Sobi and sponsor-led clinical trials for CSL Behring, Sobi, Biogen, Biomnis, Sanofi, Bayer, and Alnylam. J.O.H. is an employee of HCD Economics. K.K. is an employee and shareholder of Haemnet Ltd.
Data Availability Statement
The data that support the findings of this study can be requested via the corresponding author and may be granted upon reasonable request. The data are not publicly available due to privacy and/or ethical restrictions.
Author Contributions
E.F.G., F.N., T.B., J.O.H., K.M., M.A., R.O. made substantial contributions to the conception and design of the work. B.N., E.F.G., F.N., K.K., M.A., P.C., R.O., T.B. contributed to the analysis and interpretation of data for the work. All authors revised the manuscript critically and provided final approval of the version to be published. All authors agree to be accountable for all aspects of the work.
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References
- 1 Srivastava A, Santagostino E, Dougall A. et al. WFH guidelines for the management of haemophilia, 3rd ed. Haemophilia 2020; 26 (S6): 1-158
- 2 Nissen F, Burke T, Asghar S. et al. An insight into clinical outcomes in mild, moderate, and severe haemophilia A (HA): a preliminary analysis of the CHESS II study. Res Pract Thromb Haemost 2020;4(01):
- 3 Castro F, Silkey M, Khair K. et al. Joint bleeds in paediatric patients with haemophilia A: a CHESS study analysis. Res Pract Thromb Haemost 2019;3(Suppl 1).
- 4 Hanley J, McKernan A, Creagh MD. et al; Musculoskeletal Working Party of the UKHCDO. Guidelines for the management of acute joint bleeds and chronic synovitis in haemophilia: a United Kingdom Haemophilia Centre Doctors' Organisation (UKHCDO) guideline. Haemophilia 2017; 23 (04) 511-520
- 5 Tagliaferri A, Feola G, Molinari AC. et al; POTTER Study Group. Benefits of prophylaxis versus on-demand treatment in adolescents and adults with severe haemophilia A: the POTTER study. Thromb Haemost 2015; 114 (01) 35-45
- 6 O'Hara J, Walsh S, Camp C. et al. The impact of severe haemophilia and the presence of target joints on health-related quality-of-life. Health Qual Life Outcomes 2018; 16 (01) 84
- 7 O'Hara J, Walsh S, Camp C. et al. The relationship between target joints and direct resource use in severe haemophilia. Health Econ Rev 2018; 8 (01) 1
- 8 Berntorp E, Dolan G, Hay C. et al. European retrospective study of real-life haemophilia treatment. Haemophilia 2017; 23 (01) 105-114
- 9 Scott MJ, Xiang H, Hart DP. et al. Treatment regimens and outcomes in severe and moderate haemophilia A in the UK: the THUNDER study. Haemophilia 2019; 25 (02) 205-212
- 10 Batty P, Austin SK, Khair K. et al. Treatment burden, haemostatic strategies and real world inhibitor screening practice in non-severe haemophilia A. Br J Haematol 2017; 176 (05) 796-804
- 11 Kizilocak H, Young G. Diagnosis and treatment of hemophilia. Clin Adv Hematol Oncol 2019; 17 (06) 344-351
- 12 Peyvandi F, Tavakkoli F, Frame D. et al. Burden of mild haemophilia A: systematic literature review. Haemophilia 2019; 25 (05) 755-763
- 13 Miesbach W, Kittler S, Bauhofer A. et al. Long-term analysis of the benefit of prophylaxis for adult patients with severe or moderate haemophilia A. Haemophilia 2020; 26 (03) 467-477
- 14 Wells JR, Gater A, Marshall C, Tritton T, Vashi P, Kessabi S. Exploring the impact of infusion frequency in haemophilia A: exit interviews with patients participating in BAY 94–9027 extension studies (PROTECT VIII). Patient 2019; 12 (06) 611-619
- 15 Canaro M, Goranova-Marinova V, Berntorp E. The ageing patient with haemophilia. Eur J Haematol 2015; 94 (Suppl. 77) 17-22
- 16 Witkop M, Neff A, Buckner TW. et al. Self-reported prevalence, description and management of pain in adults with haemophilia: methods, demographics and results from the Pain, Functional Impairment, and Quality of life (P-FiQ) study. Haemophilia 2017; 23 (04) 556-565
- 17 Witkop ML, Lambing A, Nichols CD, Munn JE, Anderson TL, Tortella BJ. Interrelationship between depression, anxiety, pain, and treatment adherence in hemophilia: results from a US cross-sectional survey. Patient Prefer Adherence 2019; 13: 1577-1587
- 18 O'Hara J, Hughes D, Camp C, Burke T, Carroll L, Diego DG. The cost of severe haemophilia in Europe: the CHESS study. Orphanet J Rare Dis 2017; 12 (01) 106
- 19 EQ-5D-Y user guide: how to apply, score, and present results from the EQ-5D-Y. 2020 . Accessed October 31, 2023 at: https://euroqol.org/wp-content/uploads/2019/10/EQ-5D-Y-User-Guide.pdf
- 20 van Hout B, Janssen MF, Feng YS. et al. Interim scoring for the EQ-5D-5L: mapping the EQ-5D-5L to EQ-5D-3L value sets. Value Health 2012; 15 (05) 708-715
- 21 Ramos-Goñi JM, Oppe M, Estévez-Carrillo A, Rivero-Arias O. IMPACT HTA HRQoL Group. Accounting for unobservable preference heterogeneity and evaluating alternative anchoring approaches to estimate country-specific EQ-5D-Y value sets: a case study using Spanish preference data. Value Health 2022; 25 (05) 835-843
- 22 Rabin R, de Charro F. EQ-5D: a measure of health status from the EuroQol group. Ann Med 2001; 33 (05) 337-343
- 23 McLaughlin P, Hermans C, Sohaib A. et al. Problem joints and their clinical and humanistic burden in children and adults with moderate and severe haemophilia A: CHESS Paediatrics and CHESS II. Blood 2020; 136 (Suppl. 01) 33-34
- 24 Al-Huniti A, Reyes Hernandez M, Ten Eyck P, Staber JM. Mental health disorders in haemophilia: systematic literature review and meta-analysis. Haemophilia 2020; 26 (03) 431-442
- 25 Grochtdreis T, Dams J, König HH, Konnopka A. Health-related quality of life measured with the EQ-5D-5L: estimation of normative index values based on a representative German population sample and value set. Eur J Health Econ 2019; 20 (06) 933-944
- 26 Hernandez G, Garin O, Pardo Y. et al. Validity of the EQ-5D-5L and reference norms for the Spanish population. Qual Life Res 2018; 27 (09) 2337-2348
- 27 Jensen MB, Jensen CE, Gudex C, Pedersen KM, Sørensen SS, Ehlers LH. Danish population health measured by the EQ-5D-5L. Scand J Public Health 2023; 51 (02) 241-249
- 28 Iannone M, Pennick L, Tom A. et al. Prevalence of depression in adults with haemophilia. Haemophilia 2012; 18 (06) 868-874
- 29 Skinner MW, Négrier C, Paz-Priel I. et al. The effect of emicizumab prophylaxis on long-term, self-reported physical health in persons with haemophilia A without factor VIII inhibitors in the HAVEN 3 and HAVEN 4 studies. Haemophilia 2021; 27 (05) 854-865
Address for correspondence
Publication History
Received: 22 November 2023
Accepted: 04 March 2024
Article published online:
15 April 2024
© 2024. The Author(s). This is an open access article published by Thieme under the terms of the Creative Commons Attribution License, permitting unrestricted use, distribution, and reproduction so long as the original work is properly cited. (https://creativecommons.org/licenses/by/4.0/)
Georg Thieme Verlag KG
Rüdigerstraße 14, 70469 Stuttgart, Germany
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References
- 1 Srivastava A, Santagostino E, Dougall A. et al. WFH guidelines for the management of haemophilia, 3rd ed. Haemophilia 2020; 26 (S6): 1-158
- 2 Nissen F, Burke T, Asghar S. et al. An insight into clinical outcomes in mild, moderate, and severe haemophilia A (HA): a preliminary analysis of the CHESS II study. Res Pract Thromb Haemost 2020;4(01):
- 3 Castro F, Silkey M, Khair K. et al. Joint bleeds in paediatric patients with haemophilia A: a CHESS study analysis. Res Pract Thromb Haemost 2019;3(Suppl 1).
- 4 Hanley J, McKernan A, Creagh MD. et al; Musculoskeletal Working Party of the UKHCDO. Guidelines for the management of acute joint bleeds and chronic synovitis in haemophilia: a United Kingdom Haemophilia Centre Doctors' Organisation (UKHCDO) guideline. Haemophilia 2017; 23 (04) 511-520
- 5 Tagliaferri A, Feola G, Molinari AC. et al; POTTER Study Group. Benefits of prophylaxis versus on-demand treatment in adolescents and adults with severe haemophilia A: the POTTER study. Thromb Haemost 2015; 114 (01) 35-45
- 6 O'Hara J, Walsh S, Camp C. et al. The impact of severe haemophilia and the presence of target joints on health-related quality-of-life. Health Qual Life Outcomes 2018; 16 (01) 84
- 7 O'Hara J, Walsh S, Camp C. et al. The relationship between target joints and direct resource use in severe haemophilia. Health Econ Rev 2018; 8 (01) 1
- 8 Berntorp E, Dolan G, Hay C. et al. European retrospective study of real-life haemophilia treatment. Haemophilia 2017; 23 (01) 105-114
- 9 Scott MJ, Xiang H, Hart DP. et al. Treatment regimens and outcomes in severe and moderate haemophilia A in the UK: the THUNDER study. Haemophilia 2019; 25 (02) 205-212
- 10 Batty P, Austin SK, Khair K. et al. Treatment burden, haemostatic strategies and real world inhibitor screening practice in non-severe haemophilia A. Br J Haematol 2017; 176 (05) 796-804
- 11 Kizilocak H, Young G. Diagnosis and treatment of hemophilia. Clin Adv Hematol Oncol 2019; 17 (06) 344-351
- 12 Peyvandi F, Tavakkoli F, Frame D. et al. Burden of mild haemophilia A: systematic literature review. Haemophilia 2019; 25 (05) 755-763
- 13 Miesbach W, Kittler S, Bauhofer A. et al. Long-term analysis of the benefit of prophylaxis for adult patients with severe or moderate haemophilia A. Haemophilia 2020; 26 (03) 467-477
- 14 Wells JR, Gater A, Marshall C, Tritton T, Vashi P, Kessabi S. Exploring the impact of infusion frequency in haemophilia A: exit interviews with patients participating in BAY 94–9027 extension studies (PROTECT VIII). Patient 2019; 12 (06) 611-619
- 15 Canaro M, Goranova-Marinova V, Berntorp E. The ageing patient with haemophilia. Eur J Haematol 2015; 94 (Suppl. 77) 17-22
- 16 Witkop M, Neff A, Buckner TW. et al. Self-reported prevalence, description and management of pain in adults with haemophilia: methods, demographics and results from the Pain, Functional Impairment, and Quality of life (P-FiQ) study. Haemophilia 2017; 23 (04) 556-565
- 17 Witkop ML, Lambing A, Nichols CD, Munn JE, Anderson TL, Tortella BJ. Interrelationship between depression, anxiety, pain, and treatment adherence in hemophilia: results from a US cross-sectional survey. Patient Prefer Adherence 2019; 13: 1577-1587
- 18 O'Hara J, Hughes D, Camp C, Burke T, Carroll L, Diego DG. The cost of severe haemophilia in Europe: the CHESS study. Orphanet J Rare Dis 2017; 12 (01) 106
- 19 EQ-5D-Y user guide: how to apply, score, and present results from the EQ-5D-Y. 2020 . Accessed October 31, 2023 at: https://euroqol.org/wp-content/uploads/2019/10/EQ-5D-Y-User-Guide.pdf
- 20 van Hout B, Janssen MF, Feng YS. et al. Interim scoring for the EQ-5D-5L: mapping the EQ-5D-5L to EQ-5D-3L value sets. Value Health 2012; 15 (05) 708-715
- 21 Ramos-Goñi JM, Oppe M, Estévez-Carrillo A, Rivero-Arias O. IMPACT HTA HRQoL Group. Accounting for unobservable preference heterogeneity and evaluating alternative anchoring approaches to estimate country-specific EQ-5D-Y value sets: a case study using Spanish preference data. Value Health 2022; 25 (05) 835-843
- 22 Rabin R, de Charro F. EQ-5D: a measure of health status from the EuroQol group. Ann Med 2001; 33 (05) 337-343
- 23 McLaughlin P, Hermans C, Sohaib A. et al. Problem joints and their clinical and humanistic burden in children and adults with moderate and severe haemophilia A: CHESS Paediatrics and CHESS II. Blood 2020; 136 (Suppl. 01) 33-34
- 24 Al-Huniti A, Reyes Hernandez M, Ten Eyck P, Staber JM. Mental health disorders in haemophilia: systematic literature review and meta-analysis. Haemophilia 2020; 26 (03) 431-442
- 25 Grochtdreis T, Dams J, König HH, Konnopka A. Health-related quality of life measured with the EQ-5D-5L: estimation of normative index values based on a representative German population sample and value set. Eur J Health Econ 2019; 20 (06) 933-944
- 26 Hernandez G, Garin O, Pardo Y. et al. Validity of the EQ-5D-5L and reference norms for the Spanish population. Qual Life Res 2018; 27 (09) 2337-2348
- 27 Jensen MB, Jensen CE, Gudex C, Pedersen KM, Sørensen SS, Ehlers LH. Danish population health measured by the EQ-5D-5L. Scand J Public Health 2023; 51 (02) 241-249
- 28 Iannone M, Pennick L, Tom A. et al. Prevalence of depression in adults with haemophilia. Haemophilia 2012; 18 (06) 868-874
- 29 Skinner MW, Négrier C, Paz-Priel I. et al. The effect of emicizumab prophylaxis on long-term, self-reported physical health in persons with haemophilia A without factor VIII inhibitors in the HAVEN 3 and HAVEN 4 studies. Haemophilia 2021; 27 (05) 854-865