One-Year, Efficacy and Safety Open Label Study, with a Single Injection of a New Hyaluronan for Knee OA: The SOYA Trial.

PURPOSE: To assess the efficacy and safety of a single injection of a new formulation of hyaluronic acid (MPS-HA2%) in patients with symptomatic knee osteoarthritis after 12 months' follow-up. PATIENTS AND METHODS: Prospective, single-arm, multicentre, open-label, 12-month follow-up study. Patients with Kellgren-Lawrence (KL) 2-3 and visual analogue scale (VAS) pain scores of ≥40-< 80 mm received a single injection of MPS-HA2%. The primary outcome was the reduction in VAS pain scores from baseline, and the secondary outcomes were the Western Ontario and McMaster (WOMAC) Universities Osteoarthritis Index, the minimum clinically important improvement (MCII), and patient and investigator global assessments (PGA, IGA) measured on 5-point Likert scale. Adverse events were recorded throughout the study for safety purposes.
RESULTS: A total of 101 patients (mean age: 68 years; 74% female; and 78% overweight) were included. The mean reduction in pain at 12 months was 37.7%; the total WOMAC score improved by 36.5% and the pain, stiffness and physical function subscores returned improvements of 32.1%, 34.1% and 32.7%, respectively (p=0.0001 with respect to baseline). At 12 months, a statistically significant 62.2% of patients obtained an improvement equal to or greater than the MCII. The mean PGA score at baseline was 2.44 and 1.46 at 12 months (p<0.05), and the mean IGA scores at equivalent timepoints were 2.29 and 1.48 (p<0.05). Fourteen patients received a second injection at the 6-month follow-up visit. Eight patients reported a total of 12 treatment-related adverse events that were local, non-serious and of mild-to-moderate intensity.
CONCLUSION: With just a single intra-articular injection, this not controlled trial suggests that MPS-HA2% is effective 12 months after the procedure in most cases. Patient tolerability and safety were both optimal (NCT03852914).

Introduction

Osteoarthritis (OA) of the knee is a common joint disorder in which progressive cartilage destruction, osteophyte formation, subchondral sclerosis and synovitis lead to articular degeneration.1–3 It is a multifactorial disease with genetic alterations, gender and ageing playing crucial roles in the processes associated with cartilage and joint degeneration and therefore in the development of OA.4,5 The main manifestations include pain, physical dysfunction and markedly reduced quality of life.6 It constitutes a high socioeconomic burden, with joint replacement responsible for most of the direct healthcare costs, besides the indirect costs arising from productivity losses, premature death and early retirement.7 Due to the multifactorial nature, the different treatment targets and high frequency of associated comorbidities, researchers are yet to identify the ideal therapy for OA. This has led to a long-term multimodal approach including different pharmacological and nonpharmacological therapeutic interventions depending on the stage of the disease and each patient’s characteristics.4,5,7–9

Hyaluronic acid (HA) is a naturally occurring polysaccharide found within synovial fluid and produced by type-B synoviocytes, fibroblasts and chondrocytes; it is widely distributed in connective tissues and a primary component of articular fluid. It provides nutrients for articular cartilage, lubricates articulation and absorbs strains. The molecular weight (MW) and rheological properties of the HA in the synovial cavity change as we age and in the case of joint disorders.10

Viscosupplementation of the synovial fluid with intra-articular HA injections was first included in the therapeutic arsenal at the end of the 20th century, with the intention being to restore the concentration and molecular weight distribution of HA in the synovial fluid. However, there is now evidence that the clinical benefit of HA in OA is not only due to its mechanical properties; several studies have found that it also exerts a chondroprotective effect, promotes proteoglycan and glycosaminoglycan synthesis, and has anti-inflammatory, mechanical, subchondral and analgesic properties.11 Despite some discrepancies between scientific societies regarding the widespread use of intra-articular HA to treat knee OA, several systematic reviews and meta-analyses published recently concluded that viscosupplementation is a viable treatment option that provides a clinically important reduction in pain and improvement in function.12–19 This is especially true when the treatment is adequately tailored according to patient characteristics,20,21 with effects lasting more than those of intra-articular corticosteroids22–26 and with a better safety profile than other treatments for OA.19,24,27–30

Treatment with HA has traditionally consisted of several intra-articular injections administered at weekly intervals. However, there is an ever-increasing demand for shorter treatments, resulting in less visits and costs for both patients and healthcare providers. Furthermore, the use of single-dose treatments would reduce the potential risk of local adverse events related to the administration procedure. Different approaches have been developed in order to obtain effects that are as durable as those of multiple-injection treatments, such as greater injection volumes, higher concentrations, changes in the molecular structure (crosslinking) or the inclusion of different additives, but there is still no clear consensus about the impact of these modifications on the clinical results.31

Most studies of knee OA involving single-injection products were designed to follow the patients for no more than 6 months;32 therefore, in most cases, the scarcity of results makes it hard to comment on the long-term duration of the effects.

The SOYA (Symptomatic Osteoarthritis one Year Assessment) study was designed to investigate the efficacy and safety of a new formulation of HA in the treatment of patients with symptomatic knee OA, focusing particularly on the effects 12 months after a single injection.

Patients and Methods

Ethics and Registration

The trial was conducted in accordance with Good Clinical Practices and in compliance with the principles of the Declaration of Helsinki. Approval was obtained from the Alcorcón Hospital Institutional Review Board (Alcorcón, Madrid, Spain) (approved on 6th of September 2018, minutes nº 10/18) and the Spanish Agency of Medicines and Medical Devices. All patients provided their written informed consent to participate in this trial. The study was registered at ClinicalTrials.gov with the identifier NCT03852914.

Design

The study followed a prospective, single-arm, open-label design with a 12-month follow-up. Patients deemed eligible at screening completed a 14-day washout period prior to administration. Each patient then received a single intra-articular injection of MPS-HA2%, a new product consisting of a 2% wt./vol solution of medium MW (1000 kDa)33 HA obtained by fermentation and without any chemical modification, dosed in pre-filled syringes containing 98 mg of HA. Patients were followed for 12 months, with a telephone contact at 3 months for safety purposes and follow-up visits at 6 and 12 months (Figure 1). At 6 months, patients were offered a second injection if and when they met all the criteria established for re-treatment: 1) a reduction in pain from baseline on VAS < MCII; 2) the patient’s overall opinion; and 3) no treatment-related adverse events after the first administration; and were followed until completion of the initial 12 month period. Only paracetamol (up to 3 g/day) was permitted as rescue medication for OA pain during the study and it had to be discontinued at least 24 h before visits.

Figure 1

Study schedule.

Study Population

Eligible patients were men and women aged ≥ 45 years who met the following inclusion criteria: diagnosis of primary OA of the knee in the medial/lateral tibiofemoral compartment according to ACR criteria;34 radiological grade 2–3 according to the Kellgren and Lawrence (KL) scale35 confirmed by an anteroposterior X-ray; and VAS pain scores ≥ 40 – < 80 mm in the target knee and ≤ 20 mm in the contralateral knee. Patients had to be able to understand and comply with the study procedures and give their written consent to participate before entering in the study.

Exclusion criteria comprised a body mass index (BMI) ≥ 30 kg/m2, a severe varus/valgus deformity (>15°) or patellofemoral pain/syndrome, previous surgery in the target knee including arthroscopy within the past year, severe inflammation of the target knee, an inflammatory joint disease, significant OA in other joints requiring pharmacological treatment, venous or lymphatic stasis in the relevant limb. Patients with the following treatments were also excluded: intra-articular HA (within the last year), intra-articular corticosteroids or joint lavage (last 3 months) and symptomatic slow-acting drugs for OA (SYSADOA). Finally, patients could not participate if they had known hypersensitivity to HA or paracetamol, were pregnant or breastfeeding, or if they were on a waiting list for surgery or awaiting a disability assessment.

Outcome Measures

We used patient-reported outcomes and derived measures to evaluate the efficacy of the treatment. The primary endpoint was a reduction in pain intensity measured on a 0–100 mm VAS, where 0 was the absence of pain and 100 was extreme pain. Secondary variables included the Western Ontario and McMaster (WOMAC) Universities Osteoarthritis Index total and subscale scores for pain (WOMAC A), stiffness (WOMAC B) and physical function (WOMAC C); all were measured on a VAS and normalized. Similarly, the percentage of patients who achieved the minimum clinically important improvement (MCII),36 defined as a relative improvement over baseline of ≥ 20% in VAS scores, was another secondary endpoint. The patient global assessment (PGA) and investigator global assessment (IGA) were measured on a 5-point Likert scale where 0 was the best condition and 4 the worst. Adverse events (AEs) were recorded from screening until the end of the study.

Statistics

A sample size of at least 93 patients was necessary to provide sufficient evidence that MPS-HA2% is effective in the treatment of knee OA with a 90% power and considering a dropout rate of 35% after 12 months’ follow-up.

The statistical and dataset analyses were defined in the Statistical Analysis Plan. We considered the results in terms of three populations. The modified intention-to-treat (mITT) population included all patients who received at least one dose of study treatment and completed at least one post-baseline efficacy assessment. The per-protocol (PP) population included all patients who completed the study without any major protocol deviations. Finally, the safety population comprised all patients who received at least one dose of the study treatment. The main study population for the analysis was the mITT, although the PP population was also analysed.

Quantitative variables were reported as mean, median, standard deviation, interquartile range, minimum, maximum and the total number of patients with available data. Qualitative variables were described through their distribution of absolute and relative frequencies. Student’s t-test or Wilcoxon nonparametric tests were used depending on the type and distribution of each dataset.

The statistical analysis was performed with SAS® v9.3 and significance was set at p<0.05.

Results

Patient Disposition

Seven Spanish hospitals participated in the study between January 2019 and May 2020 and preselected 104 patients of whom three were found to be ineligible. Finally, 101 patients were included and a total of 83 (82.2%) completed the 12-month follow-up. The mITT population comprised 98 patients that received the study treatment and completed at least one post-baseline assessment. At 12 months, the PP population consisted of 74 patients who had completed the 12-month follow-up without any major protocol deviations. Of the 101 eligible patients, 17 did not complete the study: 2 cases were due to AEs (neither were study related), 6 patients decided to dropout, and 9 were withdrawn because of protocol violations. One additional patient was lost to follow-up. The CONSORT flow diagram of the trial is shown in Figure 2.

Figure 2

Flow diagram of the study.

Demographic and Baseline Characteristics

The patients had a mean age of 68 years and 50% were between 63 and 74 years old. The female/male ratio was approximately 3/1 and 98% of the patients were Caucasian. With respect to occupations, 51.49% of the patients were retired, 25.74% were homemakers and 19.80% were employed in different professions (information on occupation was unavailable for 3 patients). The sample had a mean weight of 71.56 kg and a height of 1.62 m. The mean BMI was 27.05 kg/m2 and 78.22% of the patients were overweight. Nearly two-thirds (65.35%) of the sample had three or more comorbidities and only 4% reported having no concomitant diseases. The most common comorbidities at inclusion were either related to the cardiovascular system or metabolic diseases, with frequencies of 60.40% and 53.47%, respectively.

The mean time elapsed since the diagnosis of OA was 4.1 years (range: 1–28 years). Regarding the KL radiological grade, 57.4% of the subjects were grade 3. Knee OA was unilateral in 26.70% of cases. All patients had predominantly tibiofemoral OA, while 62.38% also had some degree of patellofemoral compromise. Almost one-fifth (18.81%) of patients had previously undergone surgery on the target knee (arthroscopy in 12 patients and meniscectomy in 7 others). The mean time since this surgery was 14.1 years.

Symptoms at baseline were moderate-to-severe, as determined through VAS pain scores, total WOMAC and WOMAC subscales A, B and C, as shown in Table 1.

Table 1

Demographic and Baseline Characteristics of Eligible Patients (n=101)

	Mean (SD)	n (%)
Women		75 (74.26%)
Age (years)	68.04 (9.05)
BMI (kg/m2)	27.05 (2.68)
Underweight		1 (0.99%)
Normal weight		20 (19.80%)
Overweight		79 (78.22%)
Obese		1 (0.99%)*
Comorbidities
Cardiovascular system		61 (60.40%)
Metabolic and nutrition disorders		54 (53.47%)
Musculoskeletal and connective tissue disorders		34 (33.66%)
Nervous system		32 (31.68%)
Time since OA diagnosis (years)	4.14 (5.09)
Target knee (right) n (%)		58 (57.43%)
Kellgren–Lawrence grade of target knee
Grade 2		43 (42.57%)
Grade 3		58 (57.43%)
VAS pain (mm)	63.86 (11.60)
WOMAC (mm)
Total	50.53 (16.70)
Pain (A)	49.81 (17.42)
Stiffness (B)	49.52 (21.60)
Function (C)	52.25 (17.75)

Note: *This patient was excluded after confirming their BMI.

Abbreviations: SD, standard deviation; BMI, body mass index; VAS, visual analogue scale; WOMAC, Western Ontario and McMaster Universities Osteoarthritis Index.

Patients received one intra-articular injection of MPS-HA2% via a superolateral (45.54%), lateral (41.58%) or medial (11.88%) approach.

Efficacy Results

For the mITT population, the mean overall pain score (primary outcome) was 63.57 mm at baseline. By 6 months pain scores had reduced to a mean of 37.59 mm, and this improvement was sustained over time with a mean score of 38.37 mm at 12 months. Very similar values were obtained among the PP population, with a mean pain scores of 63.82 mm at baseline and 36.97 mm and 36.61 mm at 6 and 12 months, respectively. These reductions were statistically significant (p<0.0001) and well above the 20% established as clinically relevant (Table 2).

Table 2

Efficacy Results at 6 and 12 Months

Outcome	6 Months		12 Months
	mITT (n=98)	PP (n=81)	mITT (n=98)	PP (n=74)
Pain (% change from baseline)
Mean (SD)	−39.74* (4.78)	−41.01* (4.87)	−37.67* (5.11)	−40.81* (5.38)
95% CI	(−49.23; −30.25)	(−50.68; −31.34)	(−47.82; −27.52)	(−51.54; −30.08)
WOMAC (% Change from baseline)
WOMAC total mean (SD)	−36.57* (4.63)	−37.53* (4.72)	−36.47* (4.91)	−40.69* (5.09)
95% CI	(−45.77; −27.37)	(−46.91; −28.14)	(−46.20; −26.73)	(−50.84; −30.54)
WOMAC pain mean (SD)	−32.92* (5.27)	−33.40* (5.44)	−32.07* (5.60)	−35.97* (6.00)
95% CI	(−43.37; −22.46)	(−44.22; −22.59)	(−43.19; −20.95)	(−47.93; −24.00)
WOMAC stiffness mean (SD)	−35.24& (9.05)	−33.60# (9.85)	−34.08* (7.67)	−34.93* (9.31)
95% CI	(−53.22; −17.23)	(−53.18; −14.01)	(−49.30; 18.86)	(−53.49; −16.37)
WOMAC function mean (SD)	−33.95* (4.81)	−33.33* (5.12)	−32.71* (5.08)	−39.18* (4.88)
95% CI	(−43.49; −24.40)	(−43.49; −23.16)	(−42.80; −22.62)	(−48.91; −29.44)
MCII n (%)	65 (66.33)	61 (68.54)	61 (62.24)	49 (66.22)
PGA (much better/better) n (%)	65 (66.33)	60 (67.42)	55 (56.12)	46 (62.16)
IGA (much better/better) n (%)	70 (71.42)	66 (74.16)	55 (56.13)	47 63.51)

Note: *p<0.0001; &p=0.0002; #p=0.0010.

Abbreviations: mITT, Modified Intention to Treat; PP, per protocol; SD, standard deviation; CI, confidence interval; WOMAC, Western Ontario and McMaster Universities Osteoarthritis Index; MCII, minimally clinical important improvement; PGA, patient global assessment; IGA, investigator global assessment.

Significant improvements were also observed in the total WOMAC score and the pain, stiffness and function subscales for both the mITT and PP populations; again, the improvement reported at 6 months was maintained at 12 months (Table 2).

The percentage of mITT patients who achieved MCII based on their VAS pain scores was 66.33% and 62.24% at 6 and 12 months, respectively. The equivalent figures in the PP population were 68.54% and 66.22%.

The mean PGA score in the mITT population was 2.44 at baseline, 1.35 at 6 months and 1.46 at 12 months (p<0.05). The scores were very similar for the PP population and the PGA improved significantly (p<0.05) at the end of the study. As for the IGA among the mITT population, the mean score was 2.29 at baseline, 1.06 at 6 months and 1.48 at 12 months (p<0.05). Staying with the mITT sample, the PGA was “better” or “much better” for 66.33% of patients after 6 months and 56.12% at 12 months. In the PP population the figures were very similar, with a result of better/much better reported by 67.42% of patients at 6 months and 62.16% at 12 months. Investigators rated the patients’ condition as better/much better for 71.42% of cases at 6 months and 56.13% after 12 months’ follow-up. The figures were very similar for the PP population where the IGA was better/much better for 74.16% of patients at 6 months and 63.51% at 12 months.

The additional analyses revealed that normal weight patients responded better to the treatment than overweight patients, although the differences did not reach statistical significance (p>0.05). On the other hand, a greater improvement was noted at 6 months in patients with KL grade 2 compared to grade 3; the differences within groups for most of the parameters studied reached statistical significance at 6 months but not at 12 months. We also examined if there were any differences in the responses that could be attributed to the approach used for the injection. A significant (p<0.05) and clinically relevant reduction compared to baseline was observed for each approach. Greater improvements were evidenced in patients administered the treatment via a medial route, although the low number of patients treated meant the differences between the three approaches were not statistically significant (p>0.05).

A total of 14 patients who met the protocol retreatment criteria received a second injection at the 6-month visit and were followed for another 6 months until the end of the study. Six months after the second injection the mean reduction of pain in this group was 24.02% (p<0.05) and 50% of the group achieved MCII.

Six patients discontinued the study prematurely of their own accord due to a lack of expected response, three from the mITT population and the other three only belonged to the safety population as they had not completed a post-baseline assessment. Using the median study duration until dropout as an estimator of treatment efficacy, in this group of patients the treatment was effective for just over 5 months (5.29 months).

At the 12-month visit, almost 47% of the patients reported having taken paracetamol as rescue medication at some point during the follow-up period.

Safety Results

A total of 12 treatment-related adverse events were reported involving eight patients (7.9%). These adverse events were all local, of mild-to-moderate intensity and classified as non-serious. No treatment-related adverse events were reported after the second injection. No serious treatment-related adverse events were reported throughout the overall study period.

Discussion

Viscosupplementation is a recognised treatment for OA in different joints. Several systematic reviews and meta-analyses advocate its use in terms of efficacy and safety11,13,16–19,21,24,27,29 and, unlike other treatments such as oral drugs, HA is free from drug–product interactions and problems associated with compliance or the risks of overuse.37 The most widespread use of HA is in knee OA, and although they were initially administered in cycles of 3–5 injections, HA products based on a single injection have been in demand for some time. Since the effects of HA were believed to last for 6 months,38,39 very few studies have been conducted with single-injection products and follow-up periods lasting more than 6 months. Considering this background, after confirming the biocompatibility of MPS-HA2%,40 our objective was to study its efficacy and safety in patients with symptomatic knee OA for 1 year after a single injection.

The results suggest that MPS-HA2% is effective in relieving pain and improving function. The reduction of VAS pain at 6 months was significant compared to baseline and lasted for the whole follow-up period with relative reductions ranging from 37.67% to 41.01%. Significant improvements were also observed in WOMAC scores (A, B, C and total) with improvements ranging from 32.07% to 40.69% for the 12-month follow-up period; these results are well above the 20% considered as clinically relevant.16 After 6 months, 66.33% of patients achieved MCII and by 12 months this value was 62.24%. The patient and investigator global assessments followed a similar pattern.

Patient retention is a point of concern in clinical trials, especially long-term studies.41 In our study, the required sample size was estimated considering an expected dropout rate of 35% throughout the entire study period; therefore, a discontinuation rate of 18% after 12 months’ follow-up can be considered a good result that was probably due to the efficacy and tolerability of the treatment.

One of the keys to viscosupplementation is the correct identification of the patient characteristics that may be associated with a better response. Obesity and a high radiographic grade have been identified as predictors of viscosupplementation failure.42–44 Consequently, HA administration to obese patients and those with more severe grades of knee OA has frequently been discouraged. However, more recent studies have concluded that while these patients may have a reduced possibility of a positive response to HA treatment, the benefits obtained in those who do respond are similar to those of normal weight subjects and with mild/moderate OA.45 Although our study did not include obese patients, about 80% of our sample were overweight and we did not find significant differences in the response rates between overweight and normal or underweight patients. On the other hand, when considering the grade of OA, we found differences in some of the response parameters at 6 months but not after 12 months. As such, given there are very few effective and well-tolerated treatment options for OA, we share the opinion of most recent publications in that HA should not be ruled out as a therapeutic option for these patients because a substantial number can benefit from it.

Intra-articular injections can be administered via several approaches, and different outcomes have been reported in terms of efficacy and local reactions.46–48 In the present study the protocol did not specify the approach to be used and each investigator administered the treatment according to their own judgement and experience. The superolateral and lateral approaches were used in a similar number of patients, whereas the medial route was much less frequent. Although greater improvements were observed for patients treated via the medial approach, the reduced number of subjects meant the differences between groups were not statistically significant and the results should be considered with caution.

Just 14% of the patients received a second, single injection at 6 months and were followed for another 6 months, going on to record a clinically important improvement in pain and function and confirm that clinical outcomes can be improved by repeating HA administration if the symptoms reappear.19,49–52

With respect to safety, a single injection of MPS-HA2% was well tolerated and only 8 patients reported local, treatment-related adverse events. These adverse events were consistent with those commonly described for this class of products and none were serious.

The limitations of this study include the open-label design without a direct comparator arm. With regard to the possibility of a head-to-head design, we could not find any controlled trials with single-injection HA products that would have demonstrated 12-month efficacy in a significant number of patients.

Another limitation is due to the fact that although all our patients had predominantly tibiofemoral compromise, a significative percentage presented some degree of patellofemoral affectation. This could be a source of bias as patellofemoral involvement could lead to worse efficacy results,14,53 so many studies exclude these patients. The inclusion of purely tibiofemoral patients may have resulted in even better results, although we consider that our patient sample is a better reflection of the real situation.

Conclusions

The results of this study suggest that a single injection of MPS-HA2% provides long lasting improvement in patients with mild to moderate knee OA but further controlled trials must be performed to confirm or infirm these promising data. Patient tolerability and safety were both optimal.