Efficacy and Safety of HLX03, an Adalimumab Biosimilar, in Patients with Moderate-to-Severe Plaque Psoriasis: A Randomized, Double-Blind, Phase III Study.

INTRODUCTION: Adalimumab has been used successfully in the treatment of psoriasis. The objective of the study is to compare the efficacy, safety, and immunogenicity between HLX03, an adalimumab biosimilar, and adalimumab in Chinese patients with moderate-to-severe plaque psoriasis.
METHODS: In this double-blind, active-controlled, parallel-group study, 262 patients with moderate-to-severe plaque psoriasis were randomized (1:1) to receive HLX03 or adalimumab (80 mg at week 1, 40 mg at week 2, and then 40 mg every 2 weeks) for 48 weeks. The primary endpoint was improvement in Psoriasis Area and Severity Index (PASI) score at week 16 comparing to baseline. Equivalence was demonstrated if 95% confidence interval (CI) of the between group difference fell within the equivalence margins of ± 15%. Other efficacy endpoints, safety and immunogenicity were also evaluated.
RESULTS: In the full analysis set, PASI improvements at week 16 was 83.5% (n = 131) in the HLX03 group and 82.0% (n = 130) in the adalimumab group, with a least-square-mean difference of 1.5% (95% CI - 3.9% to 6.8%). There were no significant between-group differences in all secondary efficacy analyses including proportion of patients achieving ≥ 75% improvement from baseline PASI (PASI 75), physician global assessment (PGA) 0/1 (clear or almost clear) and change in dermatology life quality index (DLQI) score. The incidences of adverse events and the proportion of patients with antidrug antibodies were also comparable between the two treatment groups.
CONCLUSION: HLX03 demonstrated equivalent efficacy, similar safety and immunogenicity to reference adalimumab, supporting its development as an alternative treatment for patients with plaque psoriasis in China. CLINICAL TRIAL REGISTRATION: Chinadrugtrials.org.cn, CTR20171123 (November 27, 2017); ClinicalTrials.gov, NCT03316781 (October 20, 2017).

Key Summary Points

Introduction

Psoriasis is a chronic, immune-mediated, inflammatory disease affecting the skin, nails, and joints and is associated with significant morbidity and reduced quality of life. In 2012, the reported prevalence of psoriasis in China was 0.47%, representing a four-fold increase over 25 years [1].

Adalimumab (Humira®, AbbVie, IL, USA) is a recombinant humanized monoclonal anti-tumor necrosis factor alpha (anti-TNFα) antibody which has been approved globally for various immune-mediated conditions [2, 3], and in China for the treatment of rheumatoid arthritis, ankylosing spondylitis, Crohn’s disease, and plaque psoriasis [4, 5]. However, there remains an unmet need for more cost-effective treatment options [6, 7].

Biosimilars are highly similar to the licensed biological products, but are less expensive and more accessible to patients [8]. Before a biosimilar can be authorized in any regulated country, similarity must be established between the biosimilar and its originator product in quality, biological activity, structure/physicochemical and functional attributes, efficacy, safety, and immunogenicity [9-13]. Several adalimumab biosimilars have been approved for the treatment of inflammatory diseases by the United States Food and Drug Administration and European Medicines Agency, and four adalimumab biosimilars (BAT1406, IBI303, HS016, and HLX03) have been approved by China National Medical Products Administration (NMPA) [14-18]. Among these biologics, the confirmatory phase III studies of BAT1406, IBI303, and HS016 were conducted in patients with ankylosing spondylitis. HLX03 (Shanghai Henlius Biotech, China) is the first NMPA-approved adalimumab biosimilar (December 2, 2020) [19] evaluated in patients with moderate-to-severe plaque psoriasis.

HLX03 possesses the same amino acid sequence, and has comparative structural, functional, and preclinical characteristics to adalimumab [20]. Moreover, in a phase I study among healthy adult Chinese males, similar pharmacokinetic (PK) and safety profiles were observed between HLX03 and adalimumab [21]. Here, we report the phase III study, which was designed to validate the efficacy and safety similarity between HLX03 and adalimumab in patients with moderate-to-severe plaque psoriasis in China.

Methods

Study Design

This was a randomized, double-blind, active-controlled, parallel-group study carried out between 24 October 2017 and 29 March 2019 at 21 centers in China [Electronic Supplementary Material (ESM) Table S1]. The primary objective was to compare the efficacy of HLX03 and adalimumab in Chinese patients with moderate-to-severe plaque psoriasis. Secondary objectives were to evaluate the safety, tolerability, and immunogenicity of HLX03 and adalimumab.

A central interactive web response system was used to assign patients 1:1 to receive HLX03 or adalimumab with stratification of prior biological use (yes/no) according to their unique randomization code. Patients received an initial loading dose of 80 mg study drug on day 1 of week 1, followed by 40 mg on day 1 of week 2 and 40 mg every other week thereafter until week 48. Patients were followed up for 4 weeks. An end-of-treatment efficacy visit was performed at week 50, and an end-of-treatment safety visit was performed at week 52. Patients, the investigators, and the study sponsor remained blinded to treatment allocations. Study drugs were administered via subcutaneous injection by an appointed ‘unblinded’ nurse.

The trial was designed according to the Guidelines for Development and Evaluation of Biosimilar Drugs issued by the NMPA and was performed in accordance with Good Clinical Practice and the Declaration of Helsinki. The study protocol and all amendments were reviewed by independent ethics committees at each center, and all patients provided written informed consent.

Study Population

Adults aged 18–75 years with moderate-to-severe plaque psoriasis were eligible if they had stable disease for ≥ 6 months; were able to receive systemic therapy but had shown inadequate response or treatment intolerance, contraindication, or failure; had ≥ 10% body surface area (BSA) affected by psoriasis, a Physician Global Assessment (PGA) score ≥ 3 and a Psoriasis Area and Severity Index (PASI) score ≥ 12. Patients were excluded if they had a history of tuberculosis or active tuberculosis, nonplaque or drug-induced psoriasis, or any other skin conditions or systemic inflammatory diseases that might interfere with the evaluation of treatment efficacy. Patients who had used etanercept (within 4 weeks) or other biological agents (within 12 weeks), or who received trial-related drugs within 3 months prior to screening were also excluded. Full inclusion/exclusion criteria are listed in ESM Appendix S1.

Assessments

The primary efficacy endpoint was the percentage improvement in PASI score at week 16 comparing to baseline. Secondary efficacy endpoints included the percentage of patients who achieved a 75% improvement in PASI score (PASI 75), the percentage of patients who achieved a PGA 0/1 (clear or almost clear), and the change in Dermatology Life Quality Index (DLQI) score relative to baseline at weeks 4, 8, 12, 16, 20, 32, and 50. A change in DLQI score of five points was considered significant, and a change of ≤ 1 point was considered as no or little effect.

Safety was assessed up to week 52 by monitoring treatment-emergent adverse events (TEAEs), serious adverse events (SAEs), laboratory tests, and vital signs. Adverse events of special interest (AESIs) including infections, malignancies, hepatobiliary abnormalities in laboratory tests, and injection site reactions which were previously reported in patients treated with adalimumab or other TNF blockers [2] were also described in this study.

Plasma samples for evaluating serum drug concentrations and immunogenicity were collected at baseline and at weeks 4, 16, 20, 32, and 52. A bridging electrochemiluminescence assay was used to detect the presence of antidrug antibodies (ADAs) and a validated method based on an L-929 cell proliferation endpoint was used to measure neutralizing ADAs (NADAs). Both tests were conducted at a central laboratory (United-Power Pharma Tech, Beijing, China). The assay sensitivities for ADAs and NADAs were approximately 5.2 ng/mL and 187.5 ng/mL, respectively.

Statistical Analysis

Following the methodology of a previous study [22] and technical guidance from the NMPA, a sample size of 108 patients per group was determined to give an 80% power to achieve a statistical significance of 0.05 using a two-sided test for comparison of HLX03 and adalimumab, with a dropout rate of 20% [4, 9].

Efficacy data were analyzed using the full analysis set (FAS; all randomized patients receiving ≥ 1 dose of study drug and ≥ 1 post-dose efficacy evaluation) and the per-protocol set (PPS; all FAS patients without major protocol violations).

The primary efficacy endpoint was analyzed using the analysis of covariance model (ANCOVA), with treatment group as a fixed effect and previous use of biological therapy (yes/no) and baseline PASI as covariates to calculate the adjusted means, standard errors, and between-treatment differences. Equivalence was determined if the 95% confidence interval (CI) of the between-group difference fell within the predefined range of ± 15%. Subgroup analyses of the primary endpoint were performed on the basis of following factors: age (< 65 years old, ≥ 65 years old); gender (male, female); duration of psoriasis (< median, ≥ median); and previous use of biological therapy (yes/no), nonbiological therapy (yes/no), or traditional disease-modifying antirheumatic drugs (yes/no).

Secondary efficacy endpoints were analyzed using a mixed-effects model (for repeated measures) and a covariance analysis model. For continuous variables (percentage improvement of PASI and change in DLQI), adjusted means and standard errors of the change (or percentage) relative to baseline and two-sided 95% CIs were calculated. For categorical variables (PASI 75 and PGA 0/1), response rates, standard errors, odds ratios, and two-sided 95% CIs were calculated.

Safety data were analyzed using the safety set (all patients receiving ≥ 1 dose of study drug who had post-dose safety data). Immunogenicity analysis included patients in the safety set who had at least one evaluable antibody test result. PK data were analyzed using the PK full analysis set, which included all randomized subjects with at least one PK parameter after receiving the study drugs.

All statistical analyses were performed using SAS v.9.4 software (SAS Institute, Cary, NC, USA).

Results

Patient Baseline Demographics and Characteristics

Of the 262 randomized patients, 261 received ≥ 1 dose of the study drug (HLX03, n = 131; adalimumab, n = 130) and 214 completed the study (HLX03, n = 108; adalimumab, n = 106) (Fig. 1). The most common reasons for early withdrawal were TEAE and withdrawal of informed consent.

Fig. 1

Patient disposition. *Time of primary efficacy endpoint: percentage improvement in PASI score from baseline to Week 16. †FAS includes all randomized patients who received at least one dose of the study drug and had baseline values and at least one post-dose efficacy evaluation. ‡PPS includes all patients in the FAS who had no major protocol violations. Ten treated patients were excluded from the PPS in the HLX03 group (seven patients with < 16 weeks of dosing, two patients for not receiving study treatment at some visits and one patient for use of prohibited drugs). Twelve treated patients were excluded from the PPS in the adalimumab group (eight patients with < 16 weeks of dosing, one patient for not receiving study treatment at some visits, two patients for use of prohibited drugs and one patient erroneously injected with the drug meant for other patients). §Safety population includes all patients who received at least one dose of the study drug and had post-dose safety evaluation data. FAS full analysis set, PASI Psoriasis Area and Severity Index, PPS per protocol set

Baseline characteristics were well balanced between the two groups (Table 1) with the exception of higher baseline median PASI scores and median BSA affected by psoriasis in the HLX03 group compared with those in the adalimumab group (24.3 vs. 20.4 and 40.0 vs. 35.3, respectively).

Table 1

Baseline demographics and characteristics (FAS)

Characteristic	HLX03n = 131	Adalimumabn = 130
Age, median (range), years	38.0 (18.0–74.0)	38.5 (19.0–71.0)
Male, n (%)	99 (75.6)	91 (70.0)
Han ethnicity, n (%)	130 (99.2)	126 (96.9)
Weight, median (range), kg	74.0 (47.0–112.0)	74.0 (44.0–167.0)
Duration of psoriasis, median years	12.7	13.4
PASI score, median (Q1, Q3)	24.3 (18.0–32.9)	20.4 (14.9–26.1)
BSA affected, median (Q1, Q3)	40.0 (29.0–59.0)	35.3 (22.4–49.0)
PGA, n (%)
Clear/almost clear	0	0
Moderate	69	94
Severe	62	36
DLQI score, median (Q1, Q3)	15.0 (8.0–21.0)	15.0 (10.0–22.0)
Previous psoriasis medication, n (%)	131 (100)	130 (100)
Biological therapy	11 (8.4)	9 (6.9)
Concomitant psoriasis medication, n (%)	72 (55.0)	73 (56.2)
Traditional/herbal medicine	51 (38.9)	52 (40.0)
Nonbiological anti-psoriatic drugs	33 (25.2)	37 (28.5)
Glucocorticoids	23 (17.6)	29 (22.3)

BSA body surface area, DLQI Dermatology Life Quality Index, FAS full analysis set, PASI Psoriasis Area and Severity Index, PGA Physician Global Assessment, Q quartile

Primary Efficacy Endpoint

In the FAS, the percentage improvements in PASI at week 16 were 83.5% and 82.0% in the HLX03 and adalimumab groups, respectively (Fig. 2). The least-square-mean difference was 1.5% with a 95% CI of − 3.9% to 6.8%, which fell within the predefined equivalence margins (± 15%). The primary endpoint was also equivalent in the PPS [85.1% vs. 84.5%, respectively, with a between-group difference of 0.6% (95% CI − 3.3% to 4.6%)].

Fig. 2

Percentage improvement in PASI over time through week 50 (FAS). FAS full analysis set, LS least square, PASI Psoriasis Area and Severity Index, SE standard error

Persistent improvements in PASI were observed at weeks 4, 8, 12, 20, 32, and 50, with no significant between-group differences for either the whole FAS (Fig. 2) or any subgroups (ESM Fig. S1).

Secondary Efficacy Endpoints

At week 16, PASI 75 response rates were 92.0% in the HLX03 group and 88.7% in the adalimumab group [relative risk (RR): 1.1 (95% CI 0.8 to 1.4)]. PASI 75 response rates were sustained in > 90% of patients until week 50, and there were no statistical differences between groups at any visit (Fig. 3a). The percentage of patients reaching PGA 0/1 improved persistently until week 50, with no significant differences between treatments except at week 8, when the percentage in the HLX03 group was lower [RR 0.5 (95% CI 0.3–0.9)] (Fig. 3b). From week 4, DLQI improved significantly at each time point in both groups, with no significant between-group differences (Fig. 4). Results of secondary efficacy endpoints in the PPS were consistent with those in the FAS (data not shown).

Fig. 3

Percentage of patients achieving a PASI 75 and b PGA 0/1 over time through week 50 (FAS). FAS full analysis set, PASI 75 an improvement in Psoriasis Area and Severity Index of at least 75% relative to baseline, PGA 0/1 Physician’s Global Assessment of clear or almost clear

Fig. 4

Change in DLQI over time through week 50 (FAS). DLQI Dermatology Life Quality Index, FAS full analysis set, LS least square, SE standard error

Safety

The overall safety profiles of HLX03 and adalimumab were similar. The incidence of TEAEs was 89.3% (117/131) in the HLX03 group and 94.6% (123/130) in the adalimumab group, with no significant differences between groups in the incidence of AESIs, SAEs, or TEAEs leading to drug discontinuation (Table 2). The most common TEAEs were upper respiratory tract infection, hyperuricemia, liver dysfunction and urinary tract infection (Table 2). Most TEAEs were mild in severity [85/117 (72.6%) for HLX03 and 86/123 (69.9%) for adalimumab]. Seven (5.3%) HLX03-treated patients experienced 15 SAEs and nine (6.9%) adalimumab-treated patients experienced 10 SAEs. The most common SAE in both groups was tuberculosis, with three active and two suspected cases in the HLX03 and adalimumab groups and adalimumab groups, respectively.

Table 2

Safety summary: TEAEs up to week 52 (safety set)

Number of patients (%)	HLX03n = 131	Adalimumabn = 130
TEAEs	117 (89.3)	123 (94.6)
SAEs	7 (5.3)	9 (6.9)
AESIsa	87 (66.4)	92 (70.8)
TEAEs leading to study discontinuation	9 (6.9)	7 (5.4)
Deaths	0	0
TEAEs with an incidence ≥ 10% in any group
Upper respiratory infection	37 (28.2)	34 (26.2)
Hyperuricaemia	24 (18.3)	18 (13.9)
Liver dysfunctionb	23 (17.6)	22 (16.9)
Urinary tract infection	16 (12.2)	12 (9.2)
Hyperlipidaemia	10 (7.6)	16 (12.3)
Nasopharyngitis	10 (7.6)	13 (10.0)
AESIs by system organ class with an incidence ≥ 3% in any groupa
Infections and infectious diseases	62 (47.3)	60 (46.2)
Upper respiratory infection	37 (28.2)	30 (23.1)
Urinary tract infection	10 (7.6)	10 (7.7)
Hepatobiliary disorders	26 (19.9)	27 (20.8)
Liver dysfunction	23 (17.6)	22 (16.9)

AESI adverse event of special interest, SAE serious adverse event, TEAE treatment-emergent adverse event

aAESIs in this study included: tolerability at injection site, hepatobiliary abnormalities in laboratory test, infections (including tuberculosis), new active tuberculosis and new malignancy

bOne patient in the adalimumab group withdrew from the study due to reported liver function abnormalities; the patient was hospitalized and the subsequent discharge diagnosis was updated to acute hepatitis B

The incidence of AESIs was similar between two groups: 87 patients (66.4%) in the HLX03 group developed 203 AESIs and 92 patients (70.8%) in the adalimumab group developed 253 AESIs. The most common AESIs were upper respiratory tract infection and liver dysfunction (Table 2). Most AESIs were mild [73/87 (83.9%) and 74/92 (80.4%) patients in the HLX03 and adalimumab groups, respectively], including one patient tested positive for hepatitis B core antibody in the adalimumab group. One patient in the adalimumab group experienced a severe AESI (iridocyclitis). No new malignancies or deaths occurred, and there were no clinically significant abnormalities in laboratory test results, vital signs, physical examinations, or electrocardiogram test results.

Immunogenicity

The proportion of patients with ADAs increased gradually with the administration of study drugs and did not differ significantly between treatment groups at any time (Table 3). The percentage of patients with at least one positive test for ADAs was 81.9% in the HLX03 group and 80.6% in the adalimumab group. The accumulated proportions of patients with ADAs at week 52 were 69.5% and 73.7%, respectively (Table 3).

Table 3

Immunogenicity following treatment of HLX03 and adalimumab

	ADAs		NADAs
	HLX03n/N (%)	Adalimumabn/N (%)	HLX03n/N (%)	Adalimumabn/N (%)
Baseline	4/130 (3.1)	2/129 (1.6)	1/4 (25.0)	1/2 (50.0)
Week 4	18/130 (13.9)	19/128 (14.8)	4/18 (22.2)	1/19 (5.3)
Week 16	77/125 (61.6)	70/119 (58.8)	8/77 (10.4)	11/70 (15.7)
Week 20	86/122 (70.5)	80/119 (67.2)	6/86 (7.0)	11/80 (13.8)
Week 32	86/115 (74.8)	82/111 (73.9)	7/86 (8.1)	11/82 (13.4)
Week 52	82/118 (69.5)	84/114 (73.7)	14/82 (17.1)	18/84 (21.4)

ADAs antidrug antibodies, NADAs neutralizing antidrug antibodies, n/N number of positive patients/number of patients tested at each time point

The proportion of patients with NADAs had no significant association with duration of drug administration. The accumulated proportions of patients with NADAs at week 52 were 17.1% (HLX03) and 21.4% (adalimumab) (Table 3).

Discussion

Prior to HLX03, phase III studies of all NMPA-approved adalimumab biosimilars were conducted in patients with ankylosing spondylitis [16-18]. Although indication extrapolation avoids unnecessary conduction of clinical trials, some societies are concerned, as limited clinical efficacy and safety data are available for the extrapolated indications, which potentially restrict therapeutic uptake [23]. The study reported here is the first phase III study of adalimumab biosimilars conducted in patients with plaque psoriasis in China. Psoriasis represents a more sensitive indication for tests of clinical similarity with a relatively pronounced effect size by monotherapy when compared to other inflammatory diseases [24, 25].

In this study, HLX03 demonstrated equivalent efficacy to adalimumab based on the primary endpoint of percentage improvement in PASI score at week 16, as well as in subgroup analyses stratified by age, sex, duration of psoriasis, and previously used therapy. Equivalence was also demonstrated in the analyses of secondary efficacy endpoints (PASI 75, PGA 0/1, and DLQI). As improved quality of life is an important goal of biological therapy, it is noteworthy that patients treated with HLX03 or adalimumab showed significant and persistent improvements in DLQI over 50 weeks, starting as early as week 4.

The primary endpoint was chosen because it is a continuous variable and may offer a better comparative analysis than a binary assessment of meeting a minimum response threshold [22]. It also reflects current treatment goals that emphasize improvements in the severity and extent of psoriasis [26]. The efficacy results were broadly comparable with those from earlier trials investigating adalimumab treatment in Chinese [27] European [28] North American [29], or Japanese [30] patients with plaque psoriasis.

HLX03 and adalimumab showed comparable safety profiles up to week 52: the incidence and type of TEAEs were generally consistent with the known safety profile of adalimumab in patients with plaque psoriasis [2, 27]. Similar to a recent trial assessing adalimumab in Chinese patients with plaque psoriasis, upper respiratory tract infection was the most common AESI [27]. In the current trial, most AESIs were mild with only one patient treated with adalimumab experienced a severe AESI of iridocyclitis. Three active (in the HLX03 group) and two suspected (in the adalimumab group) cases of tuberculosis were possibly related to the study drugs, but all recovered (or were recovering) by the end of the study. Importantly, given the potential association between TNFα inhibitors and an increased risk of serious infections and cancers [31, 32], no new safety signals, malignancies or death were observed in this study.

Immunogenicity was similar between HLX03 and adalimumab at all time points, and ADA positive rates increased gradually with drug administration. The trends are similar to other head-to-head trials of adalimumab biosimilars (vs. the reference compound) [33]. The high positive rates of ADA were similar to those reported in recent studies of adalimumab biosimilars, in which assays with higher sensitivity were used [17, 34, 35]. In addition to detection methods, previous medication history and ethnicity might also contribute to the high positive rates of ADA in this study [17, 36].

Like all randomized controlled trials, generalizability of the results may be limited by a patient population that is less heterogeneous than in real-world clinical practice. The absence of PASI 90 and PASI 100 evaluations are other potential limitations of this study. Furthermore, as plaque psoriasis is a chronic disease, the follow-up period of 4 weeks in this study is rather short, and thus long-term observation would be beneficial for monitoring the effectiveness and safety of HLX03.

Conclusions

This phase III study demonstrated that HLX03 was equivalent to adalimumab with regards to clinical efficacy, safety, and immunogenicity. These results add to the totality of evidence supporting HLX03 as an adalimumab biosimilar and confirm HLX03 as an effective and well-tolerated treatment option for patients with moderate-to-severe plaque psoriasis in China.

Below is the link to the electronic supplementary material.

Supplementary file1 (DOCX 4170 kb)

This phase III equivalence study aimed to evaluate the clinical equivalence between HLX03 (an adalimumab biosimilar) and the reference adalimumab in patients with moderate-to-severe plaque psoriasis.

HLX03 and adalimumab showed equivalence efficacy in moderate-to-severe plaque psoriasis patients.

Similar safety and immunogenicity profiles were observed between HLX03 and adalimumab.

As an approved biosimilar to adalimumab, HLX03 provides an alternative treatment option for patients with moderate-to-severe plaque psoriasis.