Background
Rheumatoid arthritis (RA) is a chronic systemic inflammatory disease, which primarily causes a symmetric polyarthritis, clinically manifested by joint pain, stiffness, and swelling [
1]. It is estimated to affect between 0.5 and 1.0% of the adult population in Western countries [
2]. Untreated, most patients have a progressive course, resulting in short- and long-term disability [
3]. Evidence shows that an early diagnosis and management of RA can improve disease outcome [
4‐
6]. The European League Against Rheumatism (EULAR) recommends that patients presenting with arthritis should be referred to and seen by a rheumatologist, ideally within six weeks after the onset of symptoms [
7]. However, several studies have shown a delayed access to the treatment by RA patients at different settings [
8‐
11].
The introduction of biologics in the late 1990s revolutionized the management of RA. Despite its widespread availability there are differences in the biologic drugs use across Europe. Based on IMS sales data and adjusted estimates of RA prevalence in Europe Kobelt et al. estimated a variation of biologics use ranging from 1% to 30% of the diagnosed adult patient population in 2008. In Portugal, the observed proportion was 5.5%, the second lowest among the smallest western markets in Europe. Different factors can explain these variations. The two most important are the macro-economic environment and the treatment guidelines. The limited use of biologics can be a consequence of low access to specialists and the cost of biologics, the later contributing to restrictive treatment guidelines and administrative constrains, most likely related to GDP in each country [
12]. These findings led Laires et al. to conduct a desk-based research to compare the proportion of RA patients treated with biologics across Europe and to investigate the factors that most influence its use, with focus on the Portuguese case. In 2010, less than 7% of the estimated RA patient population was using biologics in Portugal, which is noticeably lower than the average rate of selected European countries (19%). This investigation also suggested that countries with the highest levels of consumption of biologics showed superior methotrexate consumption, higher GDP per capita and biologics retail distribution [
13].
A desk research complemented by semi-structured interviews to senior physicians and patient representatives in France, Germany, Italy, Spain and UK, found that the number of barriers conditioning the access to treatment in RA varied considerably between those countries. The main limiting factors included primarily delays in the diagnosis of RA due to the lack of specialists available and limited RA expertise among general practitioners (GPs), resulting in slow referrals to the rheumatologists. In addition, a low RA awareness in the population, contributes to a late consultation with the GP, worsening the global scenario. The access to biologics by patients with a pre-existing RA diagnosis is limited by differences in the reimbursement and prescription process and variations in the strictness of the treatment guidelines across countries [
14].
It is therefore pertinent to explore the views and experiences of Portuguese stakeholders directly involved in the RA therapeutic circuit and to identify the main barriers to access treatment, and ultimately to biologics, in order to improve this situation. To our knowledge, no such research has been conducted in Portugal before. This article, draws out the perspectives of its participants, presents qualitative findings regarding the key factors conditioning RA patient’s access to specialized healthcare and appropriate treatment and identifies potential solutions (leverage points).
Methods
In order to better understand the main barriers and possible leverage points a qualitative research was performed using a semi-structured interview with key stakeholders in Portugal. The interviews were conducted by researchers qualified in qualitative research methods and independent reviewers analysed the data.
Selection of stakeholders
The stakeholders were purposely selected based on their involvement in the RA therapeutic circuit. Candidates from eight groups of stakeholders were invited to take part: GPs from urban and rural areas, rheumatologists, hospital pharmacy managers and purchasers; hospital managers; regional and national budget holders, representatives from the Portuguese Society of Rheumatology (SPR) and National RA Patient Association (ANDAR). Physicians and hospitals from the most relevant geographical areas were selected. There was no predefined number of interviews per stakeholder group. The interviews to each group of stakeholders continued until overall data saturation was achieved, i.e. when no new themes emerged and the same themes were reiterated.
Preliminary desk research
Preliminary desk research based on consultation of an expert panel and relevant literature review [
12] yielded valuable information on the RA framework. From this preliminary work an interview script was developed with five pre-determined major research topics and related questions: 1) Estimation of target RA patients; 2) Access to healthcare services; 3) Access to RA treatment; 4) Treatment with biologics; 5) Hospital financing/management. These topics allow the characterisation of the access to healthcare and treatment by RA patients. The complete list of questions is displayed in Additional file
1.
Open questions were formulated for each topic to explore the views of stakeholders on potential barriers, leverage points and specific initiatives.
Interviews to the stakeholders
Face to face interviews were carried out between May and June 2011. Upon the explanation of the research objectives by the interviewer a written informed consent for data collection and publication of anonymous data was obtained from all participants.
A trained and qualified interviewer followed a script tailored to the background of the stakeholders with questions covering the major research topics. Stakeholders were encouraged to openly express their points of view. Both the identified barriers, leverage points and set of initiatives that could contribute to overcome the barriers were debated between the interviewer and each stakeholder. Each initiative was graded according to the following criteria: attractiveness to stakeholders (not interesting, likely interesting and clearly interesting) and expected impact of the initiative in overcoming the identified barriers (low, medium and high).
Each interview lasted approximately 60 minutes and was audio taped and later transcribed. In addition, interviewer’s field notes documented the contextual details and the non-verbal expressions of the interviewees, which were useful in the data analysis and interpretation. The interviewees were blinded about the funding of this project.
Qualitative analysis
Conventional content analysis was used through immersion/crystallization cycles as well as grounded theory approaches. The interviews were transcribed verbatim and organised thematically by the interviewer. Two independent researchers were involved in all the analysis steps. First, the data was read to achieve a good knowledge of the content. Then, portions of data that were similar in concept or idea were coded. For example, the ideas related to the inefficient referral from primary healthcare services or the waiting times at the hospital were coded as “difficulties in accessing secondary healthcare services”. The concepts were compared between transcripts and documents and in case of inconsistencies data portions were re-coded. The codification and concepts were also discussed between the researchers in order to achieve consensus. Afterwards, the researchers categorised each barrier identified under one of the five major topics described (see Table
1). Each category was associated with specific leverage points and initiatives. Based on the content of the interviews the researchers graded (as low, medium or high) each key initiative regarding the investment and effort required. No qualitative analysis software was used to manage the data.
Table 1
Major research topics addressed by each group of stakeholders
Number of interviews
|
5
|
5
|
9
|
6
|
4
|
3
|
1
|
1
|
Major research topics
| Estimation of target RA patients | | | • | | | | • | • |
Access to healthcare services | • | • | • | | | | • | • |
Access to RA treatment | | | • | • | • | | • | • |
Treatment with biologics | | | • | • | • | | • | • |
Hospital financing/management | | | • | • | • | • | • | • |
In order to confer more robustness, the main conclusions from the interviews, including the classification attributed to each initiative, were consolidated in a moderated group discussion involving one interviewee from each group of stakeholders.
Qualitative research exploring the viewpoints and opinions of healthcare professionals does not require ethical approval in Portugal.
Discussion
By exploring the views of individuals who in Portugal represent the range of stakeholder groups involved in the RA therapeutic circuit in Portugal, this study identified the main factors limiting access to healthcare and treatment, and ultimately to biologics, and the key initiatives that may be undertaken to overcome these barriers. Qualitative research methods were useful for this purpose by collecting written descriptions of how individuals experience this research topic [
15].
The most predominant view among stakeholders is that relevant barriers in RA are upstream of the rheumatology practice and consequently work needs to be done at the primary care level.
The lower density of GPs in rural areas as well as the unawareness of RA by the general population limits the access to primary care services in this clinical context. Access to rheumatologists is affected first by the geographical area of the patient, mainly in rural areas where hospitals are located outside the residential areas; second, by difficulties in diagnosing RA (which is often mistaken with other rheumatic diseases) at primary care level. These factors result in a longer and ineffective referral process to the specialist, leading to the delay of RA diagnosis and the postponement of the treatment with disease-modifying antirheumatic drugs (DMARDs) [
11]. Many studies have shown that an early RA diagnosis and an aggressive management can limit the burden of the disease [
9‐
11]. Furthermore, there is evidence that induction of remission early in the disease process can impact on its progression [
7,
16,
17]. In Europe, efforts have been made to reduce time for RA diagnosis and treatment, by promoting early diagnosis [
14]. However, because of different levels of disease awareness and diverse healthcare systems organisation, the success of these initiatives differs between countries.
At the secondary care level the most relevant barrier found was related to the difficulties in the approval of biologics prescription. These difficulties can be mainly explained by the high cost of biologics and the hard budget constraints observed in the Portuguese public hospitals.
We cannot ignore the possible existence of other factors limiting access to biologics at the hospital level. For example, although the lack of compliance to treatment guidelines was proactively explored during the interviews none of the relevant stakeholders viewed this as a key barrier to access to biologics.
Furthermore, none of the stakeholders believed there was a barrier directly influencing first-line treatment with non-biologic DMARDs (e.g. methotrexate) at the specialist setting.
The leverage points most valued by the interviewees at the primary care setting were focused on raising awareness about the disease among patients and GPs. This can be achieved by periodic and close interaction between rheumatologists and GPs, through regular visits of these specialists to primary care centres, disease workshops, clinical discussions and e-training or other similar activities. The analysis of successfully treated patients in the context of the clinical discussion will motivate GPs to diagnose and refer the patients to the specialist earlier. Clear and lean referral recommendations could also help GPs to identify cases requiring a specialist consultation.
Valorisation of RA among citizens must be enhanced and patients should be more aware of the RA symptoms. This could be achieved by awareness campaigns with the involvement of the media and through dissemination of information on rheumatic symptoms in primary care facilities. This sort of initiatives would have a considerable impact on the promotion of the disease among the general public.
The optimisation of the available registry of RA patients (Reuma.pt) [
18] was a key initiative pointed out by the RA Patient's Association, GPs and rheumatologists, which aimed to improve knowledge about the disease pattern in Portugal. This online register has a national coverage, linking all public and private Rheumatology Departments. Since June 2008, rheumatologists have been collecting data on rheumatic patients receiving biologic therapies or synthetic DMARDs. However, interviewees noted that it is essential to professionalize this registry process to ensure the data is reliable and updated. This will certainly foster disease knowledge help monitor patient’s conditions in the secondary care setting. Currently nationwide epidemiological programs, EpiReumaPt [
19] and CoReumaPt [
20], are conducted to gather more epidemiologic data and to evaluate the burden of different rheumatic diseases in Portugal, including RA. The results of this program will increase the overall knowledge of RA and raise public awareness of the relevance of this condition and its impact on the Portuguese population. Ultimately, it is expected that all these activities increase patient’s access to treatment, which will contribute to a global improvement in RA healthcare.
At the specialist setting the leverage points most valued by the interviewed rheumatologists and HMA were focused on the promotion of the benefits of biologics and the fulfilment of specialists with treatment guidelines. The most attractive initiative for stakeholders relates with the implementation of hospital-based research to collect real-world data. It is widely accepted that well-designed observational studies can identify clinically important differences among therapeutic options and provide data on the long-term drug effectiveness and safety. This type of studies can complement findings from randomized controlled trials and therefore increase the clinician’s knowledge on the available treatments [
21]. The interviewees believe that hospital-based studies comparing cohorts of RA patients using biologics versus other treatments would provide a clearer picture about the biologics effectiveness, safety profile and would allow a broader characterisation of the treatment patterns in the daily practice. A large electronic database, such as Reuma.pt, can be an invaluable resource for this type of research. A preliminary report from this registry was published in January 2011 characterizing a pool of 2,162 RA patients of which 700 were treated with biologics and 1,462 with synthetic DMARDs. This report characterised the average values of disease activity, the duration of treatment with biologics and the reasons for its discontinuation [
18]. More recently, another study based on REUMA.pt made a comparative effectiveness analysis of predictors of response to tumour necrosis factor inhibitor therapies in RA [
22]. This type of reports will help to clarify the effectiveness of biologics in the Portuguese clinical practice and will contribute to compliance with treatment guidelines.
Interestingly, two rheumatologists were apprehensive regarding the long term safety profile of biologics, particularly the potential increased risk of infection. This could suggest that concerns about hypothetical long-term safety issues rose in the initial phase of the use of biologics in the late 90’s have not been completely overcome by rheumatologists. However, this aspect was not considered a main barrier since only a minority of the interviewees saw it as a key factor within RA treatment. As long-term safety data for biologics are becoming available from large observational cohorts, such as those from national registries or from open label long-term extension of trials, it is reassuring to note that adverse effects tend to be more frequent in the early phase of treatment [
23]. Infection risk remains the major concern, but it clearly peaks during the first months of use and decreases over time to relatively low levels. Malignancy was an initial concern, particularly for long-term therapy but in fact all available data is reassuring regarding this hypothetical issue [
24].
The presentation of successful clinical cases related to the use of biologics was seen by specialists as a key initiative to promote its benefits and to demystify apprehensions about the safety of these agents. This initiative would require low investment and effort, involving the cooperation between healthcare centres and rheumatologists.
Rheumatologists believe that the use of RA evaluation tools such as 28-joint count Disease Activity Score (DAS28) should be encouraged. However, they recognise that this initiative can demand a high amount of effort, as it involves changing the established routine practices of some rheumatologists who may not follow this practice in patients who are treated with conventional DMARDs. DAS28 is an instrument to measure RA activity with a composite score of several variables including tenderness and swelling of 28-joint counts, erythrocyte sedimentation rate (ESR) and patient’s global assessment through a visual analogue scale [
25]. DAS28 has been widely accepted as a valuable tool for measuring disease activity [
26] and worldwide guidelines on RA management consider this parameter primordial. As in other countries, in Portugal the guidelines for the use of biologics in RA define specific disease activity levels (measured by DAS28) [
27]. DAS28 would not only support rheumatologists in therapeutic decisions, but would also improve the fulfilment of specialists with the treatment guidelines. Therefore, from the specialist´s point of view, a wider use of DAS28 in clinical practice would contribute to a better management of the disease.
Methodology discussion
We believe that the range of stakeholders groups selected in our study represents the most relevant and influential professional areas involved in the therapeutic circuit of RA in Portugal. The number of interviews per stakeholder group was adequate since data overall saturation method was followed. In addition, our study was conducted within the most representative geographical areas. Still, the perspective of the patient was not explored in this research. Patients are important stakeholders in a therapeutic circuit and their involvement would certainly enlighten our findings [
28]. Nonetheless, the Portuguese RA patient’s association (ANDAR) has a large number of associates and systematically collects their views, attitudes towards different problems, including those linked to treatment. We believe that by exploring the views of a representative from this association we obtained a reliable overview of RA patients’ experiences under this framework.
Although qualified and trained researchers were involved, we cannot ignore the increased risk of interviewer bias inherent to semi-structured interviews (e.g. prescriptive or leading questions).
The use of data-triangulation allowed the validation of the findings presented and conclusions were consolidated by a final meeting with one representative of each stakeholder group.
None the stakeholders involved had any vested interest in the project, thus biased views can be excluded.
Competing interests
The authors declare that they have no competing interests.
Authors’ contributions
All authors critically revised the manuscript for important intellectual content and approved the final manuscript. PAL and RM: Made substantial contributions to the conception and design of this research, and were involved in the interpretation of data and drafting of the manuscript LV, AMP and RC: were involved in the interpretation of data, drafting and revision of the manuscript. JEF: Was involved in the interpretation of data, critical revision of the manuscript and oversight of the submission process.