The FLUCOLITH trial is a prospective, interventional, national, randomized in parallel groups (1:1), placebo-controlled, double blind trial, as summarized in Figure 1.
The national French recruitment will be ensured through two national rare disease networks (OSCAR and ORKiD networks); the participation of 26 French University Hospitals is expected, with physicians from Nephrology and Endocrinology Departments, and from adult and pediatric units (cf. Annex 2 - List of study sites). The trial is supported by a grant from the French Ministry of Health (Programme Hospitalier de Recherche Clinique National 2019) and the study sponsor is the Hospices Civils de Lyon (Lyon, France).
Participants
Eligibility criteria
The inclusion criteria will be the following: patients who presented in their medical history nephrolithiasis and/or nephrocalcinosis; patients who had, at least 4 weeks (±2 weeks) before inclusion and at inclusion (V1), a local biological evaluation with 24-hour urine calcium above 0.1 mmol/kg/day, and 1,25(OH)2D levels above or equal to 150 pmol/L, and 25-OH-D levels above or equal to 20 nmol/L, and calcemia levels below or equal to 2.65 mmol/L; children from 10 years or adults until 60 years; women using effective methods of contraception during the study period, partners of male patients of child-bearing potential must use highly effective methods of contraception; patients insured or beneficiary of a health insurance plan; evidence of signed and dated informed consent document(s) indicating that the subject and/or his parents/legal guardian have/has been informed of all pertinent aspects of the trial.
The non-inclusion criteria will be the following: patient who already received fluconazole or ketoconazole during the last 6 months before inclusion; patients weight below than 28 kg; patient with BMI>35; patients who cannot stop hydrochlorothiazide or other diuretics during the screening and study period; patients who cannot stop vitamin D supplementation and/or calcium supplementation (drugs, enriched waters, etc.) during the study period; hypersensitivity to fluconazole and/or other derivative azoles and/or excipients;
due to the presence of lactose excipient, patients presenting rare hereditary abnormalities of galactose intolerance, of Lapp lactase deficit or of glucose-galactose malabsorption); patients who need co-administration with other drugs known to prolong the QT interval and metabolized by cytochrome P450 (CYP3A4) such as pimozide, quinidine and erythromycin; patients with iatrogenic hypercalciuria (vitamin D intoxication, immobilization); patients with risk of QT interval prolongation (congenital Long QT syndrome, familial history of sudden cardiac death before 50 years of age, cardiopathy: ischemia or myocardial infarction, congestive cardiac insufficiency, left ventricle hypertrophy, cardiomyopathy, conduction trouble within 6 months preceding the inclusion, arrhythmia history, electrolytic instabilities; bradycardia (< 50 beats per minute), acute neurological events within 6 months preceding the inclusion, adult patients with a QT interval/corrected QT interval > 470ms for women and > 450ms for men at the ECG performed at the inclusion visit (V1), or children from 10 years with a QT interval/corrected QT interval should be > 460ms for girls and > 450ms for boys); children with a history of cardiac pathology, patients with an estimatedglomerular filtration rate < 60 mL/min/1.73m²; patients with a liver disease or an abnormality in the initial liver lab test; patients with enuresis; patients with another cause of identified lithiasis; patients suffering from granulomatosis pathology such as sarcoidosis; patient with hyperparathyroidism; women who are pregnant or breast feeding, or who have a project of pregnancy before the end of the study; women menopaused; patients with a project of travelling in a sunny area during the study period; immunodeficient patients, patients with other diseases or disorders that could preclude assessment; patient who is participating in another research study that may interfere with the results or conclusions of this study; patients under judicial protection.
Intervention
Inclusions will be performed only from mid-September to the beginning of February so as to avoid bias due to sunlight-induced vitamin D synthesis.
Patients will receive fluconazole or placebo during 18 weeks.
A therapeutic adjustment will be done during the first 6 weeks of treatment (titration period) according to the 24h-calciuria results. Treatment will be modified if necessary by increasing the number of capsules. Treatment will start with 50 mg/day until maximum 200 mg/day. Patients allocated will receive between 1 and 4 capsules of fluconazole/placebo during the first 6 weeks of the trial.
The site personnel will directly enter Calciuria results onto the eCRF. During the titration period (Week 2 (V3), Week 4 (V4) and Week 6 (V5)), the posology to adopt will be automatically given by the eCRF, via an algorithm common to both treatment groups:
· if 24-hour calciuria is > 0.1mmol/kg/d, fluconazole/placebo dose will be increased to 50 mg per day until the next visit,
· if 24-hour calciuria is ≤ 0.1mmol/kg/d, fluconazole/placebo dose will remain stable until the next visit.
From Week 6 (V5) and until the end of the treatment period (Week 18, V9), the treatment dose will remain stable (stable period), as illustrated in Figure 1.
Temporary or permanent discontinuation of investigational medical product can occur due to biological lab abnormalities (calcemia levels > 2.65 mmol/L after two tests, hepatic toxicity, neutrophil counts < 1 000 cells/µL, platelet count < 150 000 cells/µL), all anaphylactic reaction, cardiac abnormalities observed on the ECG exam, renal insufficiency with creatinine clearance <50 mL/min, significant vitamin D level reduction (25-OH-D level <20nmol/L) or hypophosphatemia.
Blinding procedure will be systematic thanks to the indistinguishable nature of the active product and placebo and their packaging. Only the biostatistician in charge of the production of the randomization list, the Centre Anti-Poison of Lyon, and the main pharmacy (Pharmacy Department Groupement Hospitalier Centre – Edouard Herriot Hospital – Hospices Civils de Lyon (Lyon, France), responsible for packaging, labeling and dispatching of experimental drugs to the sites will have access to a decoded list. Unblinding will be possible 24h/7d simply by phone call to the Centre Anti Poison de Lyon (CAP - 04 72 11 69 11). The CAP physician will be able to proceed to the unblinding if required.
The examinations realized during the visits will be performed specifically for the study: urine, and blood analysis, electrocardiogram, Dual X-ray absorptiometry (DXA), renal ultrasounds, dietetic questionnaires, oral calcium load tests (12). Bone evaluation with DXA : femoral neck (FN), lumbar spine vertebra 2 to 4 (LS2-4) and total body (TB) areal bone mineral density (aBMD, g.cm-2). Z-scores for TB and LS2-4: aBMD will be calculated depending of age and gender. DXA will be performed locally and we will only keep the results as Z-scores from the different centers, provided that DXA scans are locally performed according to the ISCD (International Society of Clinical Densitometry) guidelines. All DXA images will be anonymized by the investigator sites and centralized on an internet platform. The investigators will only have an access to their patients. A central review of all DXA results will be done by an engineer from INSERM Unit 1033 “pathophysiology, diagnostis and treatment of musculoskeletal disorders” in Edouard Herriot Hospital in Lyon.
The investigational medicinal product (IMP) is fluconazole. For the study, the IMP and its placebo will be provided in 22 capsules numbered bottles. Fluconazole 50 mg and placebo capsules are provided, in the same appearance (color, size, and packaging) by the sponsor. The IMP and placebo are prepared, blinded, labelled, and delivered in every participating center by the Pharmacy of the Edouard Herriot Hospital (FRIPHARM, Hospices Civils Lyon, France), authorized for the compounding of experimental drugs. Preparation of the IMP is realized according to good preparation practices from tablets of Fluconazole ARROW® 50 mg, supplied by ARROW (France). The placebo capsules are composed of lactose lactose (excipients in the labelling and package leaflet of medicinal products for human use).
Co-administration with medicinal products known to prolong the QT interval and metabolized by cytochrome P450 (CYP) 3A4 is contraindicated in patients treated with fluconazole. The Halofantrine, Amiodarone and medications used to treat the pathology are not recommended too.
Objectives and endpoints
The primary objective is to demonstrate that fluconazole normalizes or decreases urinary calcium after 4 months of treatment in patients with hypercalciuria and increased 1,25(OH)2D levels. The primary endpoint will be the proportion of patients with normalization of 24-hour urinary calcium between baseline and 16 weeks (W16), or with a relative decrease of 30% of 24-hour urinary calcium in patients who still display hypercalciuria (> 0.1mmol/kg/j) at W16.
The secondary objectives are to evaluate the effects of fluconazole on the evolution of biomarkers of calcium/phosphate metabolism and renal function over time, to describe precisely the cohort at baseline and after 4 months of treatment, to assess safety of fluconazole, to identify the onset of potential mycological resistances, to assess compliance of treated patients , and to measure quality of life and treatment satisfaction. In order to answer to the secondary objectives, corresponding secondary end-points (as summarized in Table 1) will be collected.
Table 1: secondary objectives and end-points of the FLUCOLITH trial
PTH: parathyroid hormone
25-OH-D: 25 OH vitamin D
1,25(OH)2D: 1-25 di-hydroxy-vitamin D
24-25(OH)2D: 24-25 di-hydroxy-vitamin D
OCL: oral calcium load
TmP/GFR: Tubular maximum Phosphate Reabsorption per Glomerular Filtration Rate
eGFR: estimated Glomerular Filtration Rate
FGF23: Fibroblast Growth Factor 23
DXA: Dual X-ray absorptiometry
LDH: lactate dehydrogenase
Benefit/risk ratio
The benefit for the patients is a standardized and complete medical follow-up and monitoring during the study period. Moreover, if Fluconazole is effective, recovering normal urinary calcium levels will decrease the risk of further nephrolithiasis and/or nephrocalcinosis, CKD and bone complications. There is no major risk expected for the participants. The study includes non-invasive and low-radiation radiological examinations (DXA and renal ultrasounds).
The patients will undergo additional blood and urine analyses as compared to usual standard practice. The blood volume taken for the study will not exceed the threshold volume defined by the Blood Volume Guidelines. Fluconazole is supposed to decrease urinary calcium by decreasing 1,25(OH)2D concentrations; however, in this population with increased 1,25(OH)2D levels at baseline, the risk of 1,25(OH)2D deficiency induced by fluconazole treatment appears very low. To monitor the possible emergence of Candida resistance, urine and buccal samples will be collected before the treatment period (W0) and after 8 and 16 weeks of treatment. Thus, the benefit/risk ratio does not seem to be unfavorable.
Randomization
The randomization will be stratified on the age group (children [10;18[, adult [18;60]) Randomization will be performed centrally through the Ennov Clinical software. , The lists for randomization will be provided by the department of biostatistics of the Hospices Civils de Lyon and built using the permuted block randomization method. The data from the 5 first treated adults during a period of 10 weeks after titration period (visit V8) will be at first evaluated by the DSMB and reported to ANSM to decide inclusion of patients < 18 years old.
Sample size
A total of 60 patients (adults and children) will be included.
The sample size calculation was performed according to these hypotheses: 15% of normalization of calciuria (≤0.1 mmol/kg/d) or decrease of 30% of calciuria (as compared to baseline) is expected in the placebo group vs 60% in the fluconazole group. Under these hypotheses, 25 patients should be randomized per group to achieve 89% power to show a statistical difference between the two groups (two-sided 5% alpha level, Fisher-test).
Amoung the patients included at V1, only patients with 24-hour calciuria > 0.1 mmol/kg/day and serum 1,25(OH)2D levels ≥ 150 pmol/L and serum 25-OH-D levels > 20 nmol/L and calcemia levels ≤ 2.65 mmol/L will be randomized. Hence, it is planned to recruit at V1, 60 patients to be sure to have at least 50 patients randomized. Moreover, it will allow to take into account lost to follow-up in the study.
Data management
There is a priori no criterion for premature drop-out. The patients, regardless of the randomization group, will not be excluded from the study and will be followed up according to the protocol.
Outcomes related to 24-hour calciuria measurements will be collected and reported at baseline and before every study visits V3, V4, V5, V6, V8, by the investigator or the authorized persons in the medical field of participant, as per site practice using a standard of care software. If there is missing data due to a problem during the collection of urine a four-days margin is planned to be able to organize a new collection at the patient's home/center.
All study results collected in electronic or paper source documents will be entered in an electronic case report form by the investigator or an authorized person who will be appearing on the tasks delegation sheet, as soon as they are collected (during/after patients’ visits). Data will be coded with respect to data confidentiality. Each form will be dated and signed electronically by the investigator, signifying its agreement with the data entered in the eCRF. The Ennov Clinical system was selected. Control quality of the data is performed both centrally and on site by monitors. Presence, accuracy and conformity of the data is verified.
Surveillance and emergence of adverse and serious adverse event is performed. All adverse and serious adverse event will be reported in the eCRF.
Statistical analyses
The intent to treat (ITT) population is defined as all the randomized patients according to their arm randomly allocated, whatever their inclusion criteria, their actual arm, would they be evaluable or not for the primary endpoint. Description of patients at baseline (inclusion) will be done in intent to treat. Primary and secondary endpoints regarding the efficacy of fluconazole will be analyzed in intent to treat. Per-protocol (PP) population is defined as the ITT population without the patients with major protocol deviations. Major protocol deviations will be identified during the blind review, and will include, but are not limited to cases of premature withdrawals and absence of corresponding data, non-respect of eligibility and/or non-eligibility criteria, very poor adherence to study treatment/ study treatment not taken, a late inclusion date leading to the ending of the study during summer, etc. They will be identified during the blind review, and will be specified in the statistical analysis plan. Per protocol analyses will be performed as secondary analysis of the primary endpoint. The safety population is defined as the population of patients with at least one dose of study treatment, analyzed in the actual treatment arm. The safety endpoints will be analyzed on the safety population.
The quantitative variables will be described by the following parameters: number of patients, number of missing values, mean, standard deviation (SD), median, first and third quartiles (Q1 and Q3), minimum and maximum. The qualitative variables will be described by the following parameters: number of patients, number of missing values, frequency and percentage of each modality (missing values will not be included in the denominator used for frequency computation). A p-value less than 5% will be considered as statistically significant. Two-sided 95% confidence intervals will be provided for the analyses. The analyses will be performed using the R and SAS software.
For the primary outcome, the proportions of patients with normalization of calciuria or decrease of 30% of calciuria (as compared to Baseline, V1 from W16, V8) will be described in both groups. The effect of fluconazole on calciuria will be quantified and tested through the odds ratio (with its 95% confidence interval), adjusted on the age class (children/adult) and on the level of 1,25(OH)2D during the screening period (150-200 pmol/L or >200 pmol/L). A description of the proportions of success depending on the dose of fluconazole administered at the end of the titration period will be performed. An exploratory analysis of the fluconazole effect will be performed in the subgroups defined by the level of 1,25(OH)2D during the screening period (150-200 pmol/L or >200 pmol/L). Secondary endpoints related to evolution over time will be analyzed using mixed effect models.
Missing data will generally not be imputed. If there is missing data due to a problem during the collection of urine (carrier, broken tube...) a four-days margin is planned to be able to organize a new collection at the patient's home/center. For the primary endpoint, a patient without calciuria assessment at W16 will be considered as a patient without normalization of calciuria. Two sensitivity analyses will be performed. The first one will be performed by multiple imputations, the outcome of patients without 24-hour calciuria assessment at W16 will be sampled from a Bernoulli distribution with probability equals to the proportion of calciuria normalization in the same treatment, initial 1,25(OH)2D level category and age class groups. A second analysis will be performed by excluding all patients without calciuria assessment at W16.
A detailed statistical analysis plan will be written before the database is frozen. It will take into account all protocol modifications or all unexpected events occurring throughout the study and having an impact on the analyses presented here. The planned analyses may be completed in line with the study objectives. They will be carried on by the Biostatistic Department of the Hospices Civils de Lyon.
Data Safety Monitoring Board
An independent monitoring committee (DSMB) will be set up. The DSMB will authorize in association with the ANSM the enrollment of pediatric patients in the study (patients <18 years old), once inclusion of 5 adult patients treated during a minimum period of 10 weeks at stable dose (week 16), in accordance with safety data collected in the study. The DSMB will evaluate the onset of potential mycological resistance among the study and monitor the unexpected adverse events.
It will be made of two specialists of nephrolithiasis, a pharmacologist, and an infectious disease specialist.
Further details can be found in the DSMB Charter (Annex 3).
Ethics
The study protocol was first approved by the Ethic committee EC Nord Ouest I on December 14th 2020 (20.09.22.57341), and then on June 17th 2021 (20.00146.057341-MS01) after substantial modifications and by the French competent authority (Agence Nationale de Sécurité du Médicament et des produits de santé, ANSM) on November 24th, 2020 (MEDAECPP-2020-09-00014) and then on June 30th 2021 (MEDMSANAT-2021-06-0053_2020-003011-97).This approval applies for all participating centres. It is registered under EudraCT number 2020-003011-97. The study is compliant with the reference methodology of Commission Nationale de l’Informatique et des Libertés. The study is conducted in accordance with the French legislation, the Good Clinical Practice and the Declaration of Helsinki.Written consent will be obtained for all patients before inclusion, for their participation to the study research and for the constitution and the storage of a biocollection. For patients who have not yet had a genetic analysis, a specific genetic consent will be proposed, to perform genetic testing and to store corresponding samples, according to current practice.
For minor, consent of both parents (or legal guardian) is required.
The sponsor has subscribed to an insurance policy for the entire duration of the study, covering its own civil liability as well as that of all the doctors involved in the realization of the study. It will also insure the full compensation for harmful consequences of the research for the participating persons and their beneficiaries, except with evidence, at their responsibility, that the damage is not attributable to their mistake or to that of all consultants, without the possibility of being opposed to an act by a third party or the voluntary withdrawal of the person who had initially consented to participate in the research.
The insurance contract was signed before the start of the study with the Société Hospitalière d’Assurance Mutuelle, 18 rue Edouard Rochet, 69008 Lyon, under the number 159077.
During the research involving human individuals or at its end, the data collected on the persons participating and sent to the sponsor by the investigators (or any other specialists) will be made anonymous. The persons having direct access to the data will take all necessary precautions to ensure the confidentiality of the information related to the trials, to the persons participating and, in particular, with regards to their identity as well as the results obtained.
Dissemination of the results
The protocol of the study will be published during the trial. The results will be processed within 1-year of the last visit of last patient. The results will be published in a peer-reviewed journal, recorded in accordance with the Consolidated Standards of Reporting Trials (CONSORT) Statement. Patients will be informed of global and individual (treatment arm, biological data…) results of the study.