Serplulimab, a novel anti-PD-1 antibody, in patients with microsatellite instability-high solid tumours: an open-label, single-arm, multicentre, phase II trial

Background Microsatellite instability-high/mismatch repair-deficient (MSI-H/dMMR) tumours have a high response rate to immunotherapy. Antitumour activity and safety of serplulimab, a novel humanised anti-PD-1 monoclonal antibody, were evaluated in this phase II study. Methods In this ongoing, single-arm, open-label, phase II trial, patients with previously treated unresectable or metastatic MSI-H/dMMR solid tumours received intravenous serplulimab 3 mg/kg every 2 weeks for up to 52 cycles. The primary endpoint was objective response rate (ORR) assessed by an independent radiological review committee per Response Evaluation Criteria in Solid Tumors v1.1. Secondary endpoints included additional efficacy measures, safety, and tolerability. Results As of 9 January 2021, 108 patients were enrolled, and 68 patients with confirmed MSI-H solid tumours were included in the main efficacy analysis population (MEAP). The median follow-up duration in the MEAP was 7.7 months, with an ORR of 38.2% (95% confidence interval, 26.7–50.8). Of the 108 patients, grade ≥3 treatment-emergent adverse events were reported in 53 (49.1%) patients; immune-related adverse events occurred in 52 (48.1%) patients. Conclusions Serplulimab demonstrates a durable antitumour effect and a manageable safety profile in previously treated patients with MSI-H solid tumours. Serplulimab is a promising tissue-agnostic treatment for previously treated MSI-H solid tumours. Trial registration NCT03941574.

tumour response observed with pembrolizumab (objective response rate [ORR] of 39.6%) across MSI-H/dMMR tumours provides evidence for the clinical benefits of using immunotherapy [14]. Pembrolizumab received tissue-agnostic approvals for MSI-H/dMMR tumours, which marked an advancement in precision medicine [15,16]. Nivolumab also received an approval based on MSI-H/dMMR, but only in previously treated CRC [17]. Currently, patients with MSI-H/dMMR tumours have limited treatment options, and thus alternative therapeutic agents may be beneficial.
Serplulimab (HLX10) is a novel humanised monoclonal anti-PD-1 antibody. In a phase I study involving patients with previously treated advanced or metastatic solid tumours (NCT03468751), serplulimab up to 10 mg/kg was safe and well tolerated [18]. Here we present data from a phase II study evaluating the antitumour activity and safety of serplulimab 3 mg/kg in Chinese patients with unresectable or metastatic MSI-H/dMMR solid tumours in the subsequent line setting.

Study design
This ongoing, single-arm, open-label, phase II trial was conducted at 39 study sites in China (of which 33 enrolled patients). Patients received intravenous serplulimab 3 mg/kg every 2 weeks for up to 52 cycles or until loss of clinical benefit, unacceptable toxicity, death, or withdrawal of consent. Patients could continue serplulimab treatment after a first documented disease progression (PD) per Response Evaluation Criteria in Solid Tumors (RECIST) v1.1 [19] if it was neither symptomatic nor rapidly progressive requiring urgent intervention, and if their Eastern Cooperative Oncology Group performance status did not deteriorate. Subsequent treatment for patients with confirmed PD at the next assessment (≥4 weeks from the first documented PD) by response criteria for cancer immunotherapy trials (iRECIST) [20] was at the discretion of the investigator. The trial was registered with ClinicalTrials.gov (NCT03941574).

Patients
Eligible patients were 18-75 years of age, had histologically or cytologically confirmed unresectable or metastatic MSI-H/dMMR solid tumours as assessed at central laboratory or study sites, and had progressed on or were intolerant to at least one prior line of standard therapy. Previous systemic antitumour therapy must have been discontinued ≥2 weeks prior to study treatment, and adverse events (AEs) must have resolved to at least grade 1 (graded per National Cancer Institute Common Terminology Criteria for Adverse Events v5.0, with the exception of grade 2 alopecia). Patients must have at least one measurable lesion as per RECIST v1.1, an Eastern Cooperative Oncology Group performance status score of 0 or 1 within 7 days before initiating study treatment, adequate organ function, and life expectancy of ≥12 weeks. Details of the inclusion and exclusion criteria are provided in Supplementary Material.

Assessments and outcomes
MSI status, tumour mutational burden (TMB), and programmed deathligand 1 (PD-L1) expression were determined at the designated central laboratory; MSI status could also be analysed at study sites. Assessment of mismatch repair (MMR) was performed at study sites.
Tumour assessments were performed at baseline, every 6 weeks until week 48, and every 12 weeks thereafter. The primary endpoint was ORR assessed by independent radiological review committee (IRRC) per RECIST v1.1; confirmation of complete response and partial response was required after 28 days. Secondary efficacy endpoints included ORR assessed by IRRC (per iRECIST) and by investigators (per RECIST v1.1 and iRECIST), disease control rate (DCR; stable disease [SD] was determined ≥42 days from first study treatment), overall survival (OS), 6-and 12-month OS rate, progression-free survival (PFS), 6-and 12-month PFS rate, and duration of response (DOR). DCR, PFS, and DOR were assessed both by IRRC and by investigators per RECIST v1.1 and iRECIST.
Other secondary endpoints included safety, pharmacokinetics (PK), immunogenicity, and health-related quality of life (HRQoL). Safety was monitored throughout the trial and for 90 days after treatment discontinuation. AEs were coded according to Medical Dictionary for Regulatory Activities (MedDRA) v23.1 and graded per National Cancer Institute Common Terminology Criteria for Adverse Events v5.0. Adverse events of special interest included infusion-related reactions and immune-related adverse events (irAEs) [21]. Serplulimab serum concentrations were determined for PK assessment. Immunogenicity was assessed by antidrug antibodies (ADAs) and neutralising antibodies (NAbs) against serplulimab, and patients were considered ADA or NAb positive if they had at least one positive ADA or NAb result. HRQoL was evaluated by quality of life questionnaires. Additional assessment methods are provided in Supplementary Material.

Statistical analysis
Assuming an ORR of 30%, a sample size of 40 patients were required to demonstrate that the lower limit of the 95% confidence interval (95% CI) for ORR was no lower than 15% at a one-sided 2.5% α-level. To account for censoring, dropout, and false positivity in detecting MSI-H/dMMR, the plan was to enrol around 100 patients.
Primary and secondary efficacy endpoints were analysed primarily in the main efficacy analysis population (MEAP). Subgroup analyses were conducted to investigate the impacts of PD-L1 expression (positive or negative), TMB status (low or high), MSI status (MSS/MSI-L or MSI-H), and tumour types (CRC or non-CRC) on efficacy. The efficacy endpoints were also analysed in the special-interest efficacy analysis population (SIEAP) and the sensitivity analysis population (SAP), two subsets of MEAP. Point estimates and Clopper-Pearson 95% CIs were calculated for ORR and DCR. OS, PFS, and DOR were estimated using the Kaplan-Meier method. The threshold for statistical success was a lower limit of the 95% CI of the primary endpoint being ≥15% in both the MEAP and the SIEAP. Safety was assessed in the safety set (SS) and in the MEAP. PK was analysed in the pharmacokinetic set. Immunogenicity assessment was based on the SS. Safety, HRQoL, PK, and immunogenicity data were summarised by descriptive statistics. Detailed definitions of the analysis sets are provided in Supplementary Material.
Statistical analysis was conducted using the SAS software, v9.4 or above (SAS Institute, NC, USA).

Reporting summary
Further information on research design is available in the Nature Research Reporting Summary linked to this article.

Patient characteristics and disposition
Between 22 July 2019 and 9 January 2021, 208 patients were screened, and 108 patients were enrolled (Fig. 1). The main reason for exclusion was not meeting the eligibility criteria. A total of 108 patients received at least one dose of serplulimab and comprised the SS. Of these patients, 68 had MSI-H tumours and were included in the MEAP; 58 and 42 were included in the SAP and the SIEAP, respectively.
In the MEAP, CRC was the most common tumour type (53 [77.9%]). A total of 30 (44.1%) patients were PD-L1 positive, and 55 (80.9%) were TMB-high, with a median TMB of 33.0 (Table 1). Baseline characteristics of patients in the SIEAP and SS were largely similar to those in the MEAP, except for a higher proportion of patients with TMB-H tumours in the MEAP (80.9%) and SIEAP (71.4%) than the SS (52.8%).
As of data cutoff (9 January 2021), the median duration of follow-up in the MEAP was 7.7 months (range, 1. A consistently favourable antitumour activity for serplulimab was demonstrated by IRRC assessments per iRECIST and by investigator assessments per RECIST v1.1 or iRECIST (Supplementary Tables S1 and S2).
Twelve patients in the MEAP had died by data cutoff (Fig. 3 tary Tables S5 and S6).
The incidences and severity of TEAEs in the MEAP were largely consistent with those in the SS (Table 3).

Pharmacokinetics
The mean trough concentration of serplulimab increased as treatment cycle increased, indicating an accumulation of serplulimab ( Supplementary Fig. S1). There was a trend toward lower accumulation in terms of trough concentration in ADApositive, PD-L1-negative, TMB-low, and MSS/MSI-L subgroups (Supplementary Table S8).

DISCUSSION
Serplulimab treatment resulted in durable and clinically meaningful tumour responses in Chinese patients with previously treated unresectable or metastatic MSI-H solid tumours. This study met the prespecified primary endpoint. ORR (38.2% as assessed by IRRC per RECIST v1.1) was comparable with that observed with pembrolizumab in MSI-H/dMMR solid tumours (39.6% based on a pooled analysis of five trials [14]) and with that for nivolumab in MSI-H/dMMR CRC (31.1%) [22]. Most of the patients still had ongoing tumour response at the data cutoff, with an estimated 95.7% of patients having a DOR of ≥1 year. The safety profile of serplulimab was consistent with that for PD-1 inhibitors.
Serplulimab demonstrated a sustained effect on MSI-H solid tumours, and this benefit was observed irrespective of previous lines of therapy. Patients with CRC and those with non-CRC tumours seemed to have similar responses to serplulimab treatment based on the ORR, though further studies with large sample sizes are needed to confirm the result. Moreover, the durable response was coupled with maintenance or improvements of HRQoL in most patients. The mature data on PFS and OS Tumour mutational burden (TMB) high was defined as a score ≥10.
from this ongoing trial will provide further insight into the clinical efficacy. Tumour responses assessed by RECIST v1.1 and iRECIST in this study provided additional evidence for the antitumour activity of serplulimab. In this study, outcomes were mostly consistent when evaluated by RECIST and by iRECIST. However, median PFS was shorter in the SIEAP when assessed per RECIST v1.1 than according to iRECIST (4.2 vs NR by IRRC or by the investigators), which may be due to misclassification of pseudoprogression as PD by RECIST v1.1. Nevertheless, similar outcomes according to assessment by IRRC and by the investigators add to the robustness of the tumour response results.
Discordance between MMR protein testing and MSI DNA testing results have been reported by previous studies, ranging from 1 to 10% [23,24]. In our study, MSI-H and dMMR overlapped partially, as 68 patients were MSI-H out of 108 patients identified as MSI-H or dMMR. The discordance may be due to differences in the sensitivity and specificity of techniques used, misinterpretation of testing results, or possibly biological reasons, such as functional redundancy of proteins for DNA mismatch repair and MSI-H originating from other genetic defects [24][25][26][27]. Caution should be taken when using MMR immunohistochemistry testing as a screening tool given occasional equivocal staining patterns, sometimes inadequate sensitivity due to antibodies used, requirements of pathologist's experience, and other pitfalls [23][24][25][26]. To circumvent these pitfalls, we used MSI DNA testing to select target patient population for serplulimab; MSI-H as a predictor of tumour response to serplulimab was supported by a better response in MSI-H patients than MSS/MSI-L patients.
Understanding the response to immune checkpoint inhibitors in MSI-H tumours is of interest, with high TMB shown to be predictive of better clinical outcomes in MSI-H cancers treated  CI confidence interval, IRRC independent radiological review committee, NR not reached, RECIST Response Evaluation Criteria in Solid Tumors. a Three and two patients did not have tumour assessments in the main efficacy analysis population and the special-interest efficacy analysis population, respectively. One patient included in both populations had stable disease as the best response, but the time from first study treatment to tumour assessment date was 38 days, which was shorter than the protocol specified minimum time from baseline (≥42 days), and thus tumour response was downgraded to non-evaluable.
with immune checkpoint inhibitors [28,29]. In contrast, tumour response to PD-1 inhibitors was found to be consistent across PD-L1 positive and negative MSI-H/dMMR tumours in the KEYNOTE-016 and CheckMate 142 studies [22,30]. Although numerical differences were observed in terms of ORR or PFS in our subgroup analyses according to PD-L1 expression and TMB, results were inconclusive given the small differences between groups and the small sample size, especially in the TMB-low group.
The TEAEs reported in this study were in line with AE profiles for other immunotherapies [14,31]. The most frequent grade ≥3 events and irAEs are also commonly observed during treatment with pembrolizumab in solid tumour patients [32,33]. For the three patients with grade 5 ADRs as determined by investigators, the sponsor assessment suggested that these cases were possibly unrelated to serplulimab, but probably due to PD as well as peritoneal metastasis and adhesion (for the case with intestinal obstruction), and underlying diseases (for two cases with PD).
Limitations of this study included lack of a comparator, a small sample size, and overrepresentation of CRC patients. Moreover, the interpretation of subgroup analysis by TMB was limited by the small number of patients who were TMB-low. As RAS mutation was shown to be associated with a shorter PFS in MSI-H/dMMR CRC patients treated with pembrolizumab in first-line setting [34], subgroup analysis according to BRAF, KRAS, and NRAS mutation status is recommended in future studies.
In conclusion, serplulimab provided encouraging efficacy and manageable safety profile in Chinese patients with unresectable or metastatic MSI-H solid tumours who have progressed on or been intolerant to at least one prior line of standard therapy, regardless of tumour type. Based on these results, the China National Medical  Abnormal liver function 4 (3.7) 4 (5.9) ADR adverse drug reaction, irAE immune-related adverse event, MSI-H microsatellite instability-high, SS safety set, TEAE treatment-emergent adverse event.