Abstract
Background
Rituximab and tacrolimus are therapies reserved for patients with frequently relapsing or steroid-dependent nephrotic syndrome who have failed conventional steroid-sparing agents. Given their toxicities, demonstrating non-inferiority of rituximab to tacrolimus may enable choice between these medications.
Methods
This investigator-initiated, single-center, open-label, pilot randomized controlled trial examined the non-inferiority of two doses of intravenous (IV) rituximab given one-week apart to oral therapy with tacrolimus (1:1 allocation), in maintaining sustained remission over 12 months follow-up, in patients with difficult-to-treat steroid-sensitive nephrotic syndrome, defined as frequently relapsing or steroid-dependent disease that had failed ≥ 2 steroid-sparing strategies. Secondary outcomes included frequency of relapses, proportion with frequent relapses, time to relapse and frequent relapses, and adverse events (CTRI/2018/11/016342).
Results
Baseline characteristics were comparable for 41 patients randomized to receive rituximab (n = 21) or tacrolimus (n = 20). While 55% of patients in each limb were in sustained remission at 1 year, non-inferiority of rituximab to tacrolimus was not demonstrated (mean difference 0%; 95% CI – 30.8%, 30.8%; non-inferiority limit – 20%; P = 0.50). Frequent relapses were more common in patients administered rituximab compared to tacrolimus (risk difference 30%, 95% CI 7.0, 53.0, P = 0.023). Both groups showed similar reductions in relapse rates and prednisolone use. Common adverse events were infusion-related with rituximab and gastrointestinal symptoms with tacrolimus.
Conclusions
Therapy with rituximab was not shown to be non-inferior to 12-months treatment with tacrolimus in maintaining remission in patients with difficult-to-treat steroid-sensitive nephrotic syndrome. Frequent relapses were more common with rituximab. While effective, both agents require close monitoring for adverse events.
Graphical abstract
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Introduction
Approximately 40–50% of patients with steroid-sensitive nephrotic syndrome have frequently relapsing or steroid-dependent disease. These patients are considered for therapy with steroid-sparing agents because of the morbidities associated with relapses and the risk of corticosteroid toxicity [1]. While the recent Kidney Disease: Improving Global Outcomes (KDIGO) clinical practice guidelines suggest levamisole or cyclophosphamide as preferred agents in patients with frequent relapses, they advise that the choice of the glucocorticoid-sparing agent in steroid dependence should be guided by patient and physician preference, likely adherence to therapy, and adverse effects, costs and availability of the medication [2]. In many regions of the world, patients with frequent relapses or steroid dependence usually receive initial therapy with prednisone on alternate days, cyclophosphamide, levamisole, and/or mycophenolate mofetil (MMF), failing which they are considered difficult-to-treat, and managed with either calcineurin inhibitors (CNI) or intravenous (IV) rituximab [1].
Therapy with ciclosporin or tacrolimus sustains satisfactory remission in the majority, but is reserved for later considering the risks of nephrotoxicity and metabolic adverse events [3]. Likewise, while B-lymphocyte depletion enables significant steroid-sparing and sustained remission for 6–15 months, rituximab therapy is associated with the risk of infusion reactions and hypogammaglobulinemia, particularly in young children [3]. Given a choice, physicians and parents prefer rituximab to CNI in patients with difficult-to-treat disease because of its perceived safety and ease of adherence to therapy. Evidence to guide this decision for patients with steroid-sensitive disease is limited to one retrospective series [4] and a single-center randomized controlled trial (RCT) [5] on patients with mild disease, and show conflicting results, possibly related to differences in age at therapy and disease severity. Therefore, this pilot RCT was planned to examine the non-inferiority of two doses of IV rituximab to 12 months of therapy with oral tacrolimus in sustaining remission in patients with difficult-to-treat frequently relapsing or steroid-dependent nephrotic syndrome.
Methods
Trial design
This open-label parallel-group pilot non-inferiority RCT was conducted at one center between November 2018 and December 2020. Following approval from the Institute Ethics Committee (IECPG-390/30.08.2018, RT-4/27.09.2018), the trial was registered at the Clinical Trials Registry of India (CTRI/2018/11/016342) and conducted according to the original protocol. The investigators conceived and designed the study and vouch for the accuracy and completeness in collation and analysis of data. This report complies with the Consolidated Standards of Reporting Trials statements for pilot and non-inferiority RCTs (Online Resource 1) [6, 7].
Patients
Patients, 3–18 year old, with difficult-to-treat steroid-sensitive nephrotic syndrome were eligible if they were in steroid-induced remission following a recent (< 3 months) relapse. Difficult-to-treat disease was diagnosed if each of the following criteria was met: (i) frequent relapses (≥ 2 relapses in 6 months or ≥ 3 relapses per year) or steroid dependence [2, 4], (ii) failure of ≥ 2 strategies (alternate-day prednisolone, levamisole, cyclophosphamide, MMF), and (iii) corticosteroid toxicity (cataract, glaucoma, short stature with low growth velocity [8], or obesity [9]). Patients with known secondary cause, initial or late steroid resistance, prior therapy with rituximab or tacrolimus, estimated glomerular filtration rate (eGFR) < 60 mL/min/1.73 m2 [10], seizures, impaired glucose tolerance (fasting glucose > 100 mg/dL or glycosylated hemoglobin, HbA1c > 5.7%) [11], chronic infections (tuberculosis, HIV, hepatitis B or C), < 6 months follow-up at this center, and reluctance to follow for the subsequent 12 months, were excluded.
Randomization
Following informed written consent, eligible patients were randomly assigned in 1:1 ratio in permuted blocks of four, while stratifying for steroid-dependence and age (≤ / > 8 years), to receive either IV rituximab (Mabtas®, Intas Pharmaceuticals, Ahmedabad) at 375 mg/m2 twice, one week apart, or oral tacrolimus (Takfa®, Intas Pharmaceuticals) at 0.1–0.2 mg/kg daily in two divided doses for 1 year. Personnel not caring for these patients used computer-generated random number sequence to prepare strata-wise lists and concealed the allocation in sequentially numbered, opaque sealed envelopes that were opened at randomization. The investigators, patients, and outcome assessors were aware of the therapy being received.
For patients administered rituximab, CD19 + B cells were measured one week after the second dose by flow cytometry (FACS Canto II analyzer, Becton Dickinson, NJ). Patients lacking B cell depletion (CD19 + cells < 1% of CD45 + cells or absolute count < 5 cells/µL) received additional doses of rituximab to a maximum of total four doses. B cell count was repeated at 6 months or at relapse, whichever was earlier, and at 12 months in patients with persistent depletion. B cell repopulation was defined as absolute count > 10 cells/µL [12]; rituximab was not repeated at repopulation. Dosing for tacrolimus was titrated to a 12-h trough level of 4–7 ng/mL, using chemiluminescence microparticle immunoassay. Levels were estimated at 2 weeks after randomization, 6 and 12 months follow-up, at relapse, and 2 weeks after dose titration.
Follow-up
Parents examined the first morning urine using dipstick and recorded details of proteinuria, infections, adverse events, and medication doses in a diary, which was reviewed at each visit, scheduled at 2 weeks, 1, 3, 6, 9, and 12 months, at each relapse, and at diagnosis of treatment failure. Standard deviation scores (SDS) were computed for anthropometric parameters and blood pressure [8, 9, 13]. Compliance to tacrolimus was assessed using history and pill count at each visit. Investigations, at 3-monthly visits, included blood counts, creatinine, electrolytes, transaminases, lipid profile, fasting glucose, and HbA1c. Kidney biopsy was not performed to document tacrolimus-induced nephrotoxicity. During the SARS-CoV2 pandemic, visits were delayed by 2–8 weeks and/or substituted by video teleconsultations, including questions on COVID-19 symptoms, review of anthropometry and investigations done by local physician, and images of diary and pill strips. If required, tacrolimus was supplied at home to ensure adherence.
Co-interventions
Patients in both groups received prednisolone on alternate days (1.5 mg/kg for 4 weeks, tapered by 0.25 mg/kg every 2 weeks), and discontinued at 10–14 weeks. All patients received calcium carbonate (250–500 mg) and vitamin D3 (200–400 IU) daily during steroid therapy. Hypertension was managed with enalapril (0.2–0.5 mg/kg daily), with additional amlodipine as required [13]. Infections were managed as per unit protocols. Relapse (recurrence of 3 + /4 + proteinuria for ≥ 3 days) was treated with prednisolone, at a dose of 2 mg/kg (maximum 60 mg) daily until remission (trace/negative proteinuria for ≥ 3 days), followed by 1.5 mg/kg (maximum dose 40 mg) on alternate days for 4 weeks, before discontinuation.
Outcomes
Primary outcome was the proportion of patients with sustained remission at 1-year follow-up. Secondary outcomes, at 1 year, included the proportions of patients with frequent relapses and treatment failure, frequency of relapses, time to first relapse and to treatment failure, cumulative prednisolone received, frequency and type of adverse events, and change in anthropometric and blood pressure SDS. Adverse events, assessed based on clinical and laboratory evaluation at each visit, were reported using the Common Terminology Criteria for Adverse Events (CTCAE) version 5.0 [14]. All SAE (serious adverse events) were reported to the Ethics Committee within 48 h. Causality of adverse events was attributed according to the World Health Organization Uppsala Monitoring Center system [15]. Treatment failure was the occurrence of frequent relapses, late steroid resistance, CTCAE grade 4–5 adverse event related to intervention or corticosteroids, or ≥ 2 SAE related to disease or intervention. Study participation was terminated at treatment failure and the patients managed at physicians’ discretion. All other patients were followed in the study for 1 year.
Statistical analysis
Continuous data is presented as median (interquartile range, IQR) and compared between and within groups using rank sum or sign rank tests, respectively. Categorical data is presented as percentages or frequencies with estimates of 95% CI and analyzed by chi-square or Fisher exact test. Frequency of relapses is presented as incidence density per person-year with 95% CI. Kaplan–Meier curves with the logrank test were used to estimate and compare the time to events between groups. Exploratory post hoc subgroup analysis compared outcomes in patient categories based on stratifying variables and sex. Statistical significance for primary and secondary outcomes in this non-inferiority trial was set at P < 0.025 (one-sided) and < 0.05, respectively, except for subgroup analysis, where Bonferroni correction was applied. Data was analyzed using Stata 14.0 (2015; StataCorp, College Station, Texas). Fragility index was the number of individuals whose endpoint status required to change for the result to lose statistical significance [16]. Modified intention-to-treat analysis included all patients who received at least one dose of either intervention following randomization. In patients lost to follow-up, efficacy was estimated based on last available observation. Per-protocol analysis excluded patients who missed a dose of rituximab or did not comply with the advised dose of tacrolimus for a cumulative period of > 3 weeks.
Previous studies indicate sustained remission in 50–90% of patients with difficult-to-treat steroid-sensitive disease treated with CNI or two doses of rituximab [3,4,5]. Assuming that 60% of such patients will maintain remission over 1 year after either intervention, at 90% power, 5% alpha error, a non-inferiority margin of 20%, and assuming loss to follow-up of 10%, 114 patients were required per group to demonstrate non-inferiority of rituximab over tacrolimus. The feasibility of this sample size in a single-center study was limited while enrolling selected patients with difficult-to-treat steroid-sensitive disease. Hence, participant enrolment in this pilot study was limited to 20 patients per limb.
Results
Participants
We screened 108 patients with frequent relapses or steroid dependence who had failed two or more strategies, and showed corticosteroid toxicity. Of 41 patients with difficult-to-treat steroid-sensitive disease who were randomized (Fig. 1), 21 were allocated to receive IV rituximab and 20 to oral tacrolimus. Modified intention-to-treat population included 40 patients; one patient assigned to rituximab did not return after randomization. No other patient was lost to follow-up. Baseline characteristics were similar for patients in the two groups (Table 1). The median disease duration exceeded 5 years. The majority of patients had steroid-dependent disease. Approximately 80% of patients each had failed therapy with prednisolone on alternate days, levamisole and cyclophosphamide, and a quarter in each group had also failed MMF (Table 1).
Primary outcome
At 12 months follow-up, 11 (55%) patients in each group were in sustained remission. Non-inferiority of rituximab over tacrolimus was not demonstrated since the lower 95% CI of the risk difference (– 31%) was beyond the pre-specified margin of – 20% (Fig. 2, Table 2).
Secondary outcomes
The proportion of patients in sustained remission at 3–12 months follow-up was similar between the groups (logrank P = 0.99; Fig. 3a). Two patients administered rituximab had one relapse each, while seven experienced two relapses within 6 months (frequent relapses) at 4.5–12 months follow-up. Eight patients administered tacrolimus had one relapse each; one patient with frequent relapses also developed late steroid resistance following the second relapse. Frequent relapses were the only cause of treatment failure in either group, making treatment failure significantly more common in the former (risk ratio 7; 95% CI 0.95–51.80; P = 0.023). While treatment failure in the rituximab group occurred beyond 6 months follow-up, the patient receiving tacrolimus failed therapy at 5 months (logrank P = 0.026; Fig. 3b]. The median time to relapse and frequent relapses could not be estimated (Fig. 3).
The incidence density of relapses, based on 16 relapses over 18.8 patient-years in the rituximab group and 10 relapses over 19.4 patient-years in the tacrolimus group, was comparable at 0.85 versus 0.52 relapses per person-year, respectively (Table 2). Within groups, the incidence of relapses declined by mean (95% CI) 3.3 (2.3–4.3) and 4.2 (3.2–5.2) relapses per patient-year in patients receiving rituximab and tacrolimus, respectively (both P < 0.0001). The cumulative prednisolone received was similar between the groups (Table 2).
Although there were significant improvements from baseline in anthropometric and blood pressure SDS, there were no significant between-group differences at end of study (Online Resource 2). While eGFR was comparable between groups at the end of study, therapy with tacrolimus was associated with decline in eGFR by median 19 (IQR – 5, 39) mL/minute/1.73 m2.
Adverse events
Online Resource 3 depicts adverse events observed during the study. Minor infections, accounting for one-third of events, were comparable between the groups. No patients had symptoms of, or tested positive for, SARS-CoV2. Severe infections requiring admission were observed in one patient in each group. Other SAE included two episodes of hypovolemia with relapse, and an inguinal herniotomy in patients receiving tacrolimus (Online Resource 4).
Nine patients showed 12 infusion-related reactions during or after administration of rituximab. While tachycardia was common, one patient had throat discomfort requiring IV pheniramine, a CTCAE grade 3 reaction. No event was categorized as CTCAE grade 4–5. Most common events associated with tacrolimus use were diarrhea and/or gastritis (55 episodes in 15 patients). Four of five episodes of acute kidney injury were in patients administered tacrolimus, associated with hypovolemia in relapse or high tacrolimus levels.
Monitoring of therapy
B cells were depleted after two doses of rituximab in 18 (90%) patients and after 3 doses in one patient; one did not deplete B cells despite four doses. The patient who required three doses to deplete B-lymphocytes relapsed at 6 months, while the one given four doses sustained remission till 12 months. B-lymphocytes had repopulated at relapse in the nine patients who relapsed [median count 304 (IQR 217–537) cells/µL; 11.6 (9.8–14.3)%], and by end of study in all patients [count 242 (22–657) cells/µL; 7.6 (0.6–21.0)%] (Online Resource 5). Tacrolimus was administered at median (IQR) dose of 0.08 (0.06–0.09) mg/kg/day; compliance to doses was 98% (94.1–99.8%). Median tacrolimus trough level was within the target range at baseline, at 6 months, and at end of study, but low (3.8 ng/mL) at relapse (Online Resource 6).
Per-protocol analysis
Per-protocol population included 15 patients in the tacrolimus group and 20 in the rituximab group (Fig. 1). Baseline characteristics of these patients were similar between groups (Online Resource 7). The proportions of patients in sustained remission at 1 year were 55% in the rituximab group and 67% in the tacrolimus group (risk ratio 0.83; 95% CI 0.48–1.41; Online Resource 8). There was a trend towards treatment failure being more common following therapy with rituximab (35 vs. 7%; risk ratio 5.25; 95% CI 0.72–38.23). The groups did not differ significantly in the incidence of relapses (incidence rate ratio 2.04; 95% CI 0.82, 5.68) and cumulative prednisolone dose (mean difference 0.04 mg/kg/day; 95% CI – 0.05, 0.13 mg/kg/day).
Exploratory post hoc analysis
There were no significant between-group differences in the proportions of patients with sustained remission or treatment failure, in subgroups based on age and disease severity on modified intention-to-treat (Online Resource 9) and per-protocol populations. Fragility index for treatment failure was one, i.e., changing the status of one patient from non-event to event in the tacrolimus group caused the difference in rates of treatment failure to lose statistical significance.
Discussion
This open-label, single-center pilot RCT examined the non-inferiority of two doses of IV rituximab to 1-year treatment with oral tacrolimus, in sustaining remission in patients with difficult-to-treat steroid-sensitive nephrotic syndrome. Baseline characteristics show selection of patients with prolonged steroid-dependent or frequently relapsing disease that had failed previous therapies, with significant steroid toxicity. Therapy with both agents enabled significant reduction in relapses and corticosteroid requirement compared to baseline, and improved anthropometric scores and blood pressure. While the proportions of patients with sustained remission were similar, non-inferiority of rituximab was not demonstrated. Although no patient relapsed during rituximab-induced B cell depletion, relapses beyond 6 months of therapy led to treatment failure in one-third of these patients. Relapses in the tacrolimus group were associated with low median trough levels, indicating the need for more frequent monitoring of drug levels and medication adherence using compliance questionnaires. The impact of the study is limited by its small size which led to inability to demonstrate the non-inferiority of rituximab in sustaining remission or claim superiority of tacrolimus in preventing frequent relapses.
While the management of frequently relapsing nephrotic syndrome is challenging, most patients attain satisfactory remission following prolonged therapy with prednisone and/or corticosteroid-sparing medications such as levamisole, cyclophosphamide, or MMF [17]. Therapy with CNI and rituximab is usually reserved for patients who continue to relapse frequently despite use of these agents, and/or show corticosteroid adverse effects. The reluctance to use these therapies early in the disease course stems from the risk of adverse effects, comprising chiefly nephrotoxicity with use of CNI [18], and infusion-related reactions, serious infections, and hypogammaglobulinemia with rituximab [3, 19].
The efficacy of CNI in steroid-dependent nephrotic syndrome was shown in multiple observational studies [20], and RCTs indicate that the risk of relapse at 1 year of therapy with ciclosporin was lower than on prednisolone (RR 0.72; 95% CI 0.46–1.13), similar to MMF (RR 0.53; 0.18–1.52), and higher than with alkylating agents (RR 1.96; 1.35–2.86) [3, 21]. Despite limited evidence of efficacy in steroid-sensitive disease [22,23,24], tacrolimus is preferred to ciclosporin given its lack of cosmetic adverse effects [25]. Following case series [19], five RCTs have compared the efficacy of rituximab to controls in high-threshold steroid- and/or CNI-dependence [26,27,28], or to prednisolone [29] or placebo [30] in frequent relapses or mild steroid dependence to confirm that B cell depletion, with or without steroids and CNI, is associated with reduced risk of relapse as compared to CNI or no therapy (3 RCT on 198 children; RR 0.63; 95% CI 0.42–0.93) [3].
The term “difficult-to-treat” nephrotic syndrome, while not defined clearly in the literature, is reserved for patients with steroid-sensitive nephrotic syndrome who continue to show frequent disease relapses despite use of multiple therapeutic agents, and patients with CNI-dependent or CNI-refractory steroid-resistant nephrotic syndrome [1, 28]. Conforming to our previous definition, we included patients with frequent relapses or steroid dependence who did not show satisfactory response to at least two strategies [4, 31, 32]. This definition was also endorsed in the revised guidelines of the Indian Society of Pediatric Nephrology [1]. Thus, the study was limited to patients with difficult-to-treat nephrotic syndrome in whom therapy with rituximab or CNI had not been used, so as to objectively examine the safety and efficacy of these two medications. Both groups of patients had received two or more therapies for frequent relapses, chiefly levamisole and cyclophosphamide; the use of MMF was restricted to less than one-third of patients, likely due to out-of-pocket costs and uncertain efficacy in absence of access to therapeutic drug monitoring. All patients had significant corticosteroid toxicity, precluding use of milder therapies. Overall, inclusion was deliberately restricted to a uniformly difficult category of patients to avoid heterogeneity.
The results of this pilot RCT are similar to our findings in a retrospective uncontrolled comparison on 21 patients with steroid-dependent disease that was refractory to therapy with multiple agents. Favorable short-term outcomes were observed in similar proportions of patients administered 2–3 doses of IV rituximab or oral tacrolimus for 1 year [4]. A recent open-label RCT compared the efficacy of two doses of rituximab to 12 months therapy with oral tacrolimus in 120 patients with frequent relapses [5]. In contrast to the present study, patients lacked any exposure to corticosteroid-sparing agents and were enrolled early in disease course (median duration of disease 2.5 years). Rates of relapse-free survival were significantly higher in patients administered rituximab compared to tacrolimus (90 vs. 63%; OR 5.2; 95% CI 1.9–14.1). In contrast, in the present study, only 55% patients in either group sustained remission for 1 year, and therapy with rituximab was associated with treatment failure more often than tacrolimus. While patients receiving tacrolimus fared similarly in the two studies, the variable outcomes following therapy with rituximab may be explained by the difference in disease severity. The rates of rituximab-induced sustained remission at 1 year were 25–66% in studies enrolling steroid- and/or CNI-dependent patients [26,27,28, 30], and 87% in a study on patients with low-threshold steroid-dependence [29].
About 10–25% patients receiving therapy with CNI for 2–3 years develop irreversible histological nephrotoxicity [33, 34]. Similar to the present report, controlled studies on children with steroid-sensitive or resistant nephrotic syndrome have observed decline in eGFR by 9–20 mL/min/1.73 m2 and acute kidney injury after 1-year therapy with CNI [21, 25, 35]. Gastrointestinal adverse events associated with tacrolimus therapy were more frequent than reported previously in nephrotic syndrome [21, 25, 35] and other diseases [36, 37]. Infusion reactions were the most prominent adverse events following rituximab therapy in the present study, confirming findings of a meta-analysis that found fivefold risk compared to controls (4 studies in 252 children; RR 5.8, 95% CI 1.3–25.3) [3]. Therapy was not associated with risk of serious bacterial infections or COVID-19. Hypogammaglobulinemia, reported usually following sustained B-lymphocyte depletion with sequential dosing, particularly in young children [38, 39], was not looked for.
The chief limitations of the study include its open label design and small sample size. The SARS-CoV2 pandemic imposed additional challenges in monitoring and evaluation. B lymphocyte subsets, such as memory B cells, and IgG levels were not monitored during therapy with rituximab. While confounding was avoided by stratified randomization, findings on post hoc analysis are limited by the small study size. Despite these limitations, this pilot trial enrolled a homogeneous population with severe disease, with careful attention to aspects of efficacy as well as safety, and reports outcomes using both per-protocol and modified intention-to-treat analysis without any attrition. The comparative efficacy of the two agents requires closer re-evaluation in adequately powered multicenter studies on patients with difficult-to-treat steroid-dependent nephrotic syndrome. Since the efficacy of rituximab wanes following B cell repopulation, future studies might examine the non-inferiority or superiority of a protocol involving redosing with rituximab every 6–12 months to sustain B cell depletion. Assessment of the safety of therapy would require evaluations for nephrotoxicity and hypogammaglobulinemia during 18–24 months follow-up.
Data availability
The datasets generated and analyzed during the current study are available from the corresponding author on reasonable request.
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Acknowledgements
Support of the Department of Biotechnology, Government of India (BT/PR11030/MED/ 30/1644/2016) and Indian Council of Medical Research (5/7/1090/2013-RHN) is acknowledged.
Funding
Interventions administered in the study (rituximab and tacrolimus) were supplied by Intas Pharmaceuticals (Ahmedabad, India). The sponsors had no influence or access to the design, execution or analysis of the study. No financial incentives were provided, directly to any of the authors or the institution, over the 36 months prior to the submission or subsequently.
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GM made substantial contribution to the acquisition, analysis, and interpretation of data and drafted the manuscript. NG and AA helped in clinical and laboratory work, respectively, and NG supervised drug administration. AS, PH, PK, and AB made substantial contributions to the conception and design of the work and revised the work critically for important intellectual content. AS agrees to be accountable for all aspects of the work in ensuring that questions related to the accuracy and integrity of the work are appropriately investigated and resolved.
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Institutional ethics committee approval was obtained in September 2018 (IECPG-390/30.08.2018, RT-4/27.09.2018) and the trial was prospectively registered with the Clinical Trials Registry of India (CTRI/2018/11/016342) in November 2018 before commencing the study.
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Written informed consent was obtained from either of parents or legal guardian before enrollment in the study. Consent for publication was obtained from parents or legal guardian before enrolment into the study.
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Mathew, G., Sinha, A., Ahmed, A. et al. Efficacy of rituximab versus tacrolimus in difficult-to-treat steroid-sensitive nephrotic syndrome: an open-label pilot randomized controlled trial. Pediatr Nephrol 37, 3117–3126 (2022). https://doi.org/10.1007/s00467-022-05475-8
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DOI: https://doi.org/10.1007/s00467-022-05475-8