A randomized controlled trial on the use of pessary plus progesterone to prevent preterm birth in women with short cervical length (P5 trial)

The study will be overseen by a Steering Committee (SC-P5) and a Data Safety and Monitoring Board (DSMB-P5). The SC-P5 is composed of the principal investigators, researchers of recognized national and international competence, a representative of an NGO dealing with preterm birth patients and members of the funding agencies (Bill & Melinda Gates Foundation, National Council for Scientific and Technological Development (CNPq) Ministry of Health) to evaluate the progress of the study and suggest changes when necessary.

The DSMB-P5 is composed of researchers of recognized national and international competence without any participation in the study group with the support of a statistician. This committee has complete access to the database and will meet at prespecified moments.

The Brazilian National Review Board (CONEP) approved the study under the number 1.055.555. Each local Institutional Review Boards also approved the study protocol. Protocol modifications will be reported to each relevant part including national and local institutional review boards and will be available to trial participants through the project website, to the investigators by an internal bulletin, to the registries and journals by publications, and to regulators by the review board report. No funding agency had any influence on the design and decision regarding data collections, managements, analysis and writing.

A Standard Operation Procedure with video classes was developed, provided to all centers and available online, with information on how to collect and store data, how to proceed with randomization, follow-up, and outcomes. The number of subjects will be monitored weekly by the project coordinators, monitoring visits to the other participating centers twice a year. The reports from this monitoring process will be available to the monitoring committees and to the centers themselves to document the need for improvement.

The research assistant will collect informed consent before submitting the participant to the ultrasound scan, and in case of the short cervix, another consent will be applied before the randomization. Data will be kept confidential during the study. The name and the personal information will be stored in a database different from the main results and will be available only to each respective local coordinator during the follow-up. After the end of the study personal data will be split from the clinical results and will be available only to the principal investigator (PI).

The final dataset will be available to the PI and collaborating researchers. If necessary, participants will receive ancillary and post-trial care, as compensation if there is any harm secondary to the participation on the trial. The PIs do not have any competing interests for the trial. Trial results will be published as scientific articles, and authorship eligibility will be considered according to the International Committee of Medical Journal Editors recommendations. Participating centers are listed in Fig. 1.

We will study women with a singleton or twin pregnancy. Pregnant women, no maternal age restriction, at a gestational age between 18 ^0/7 and 22 ^6/7 weeks will be offered cervical length measurement by ultrasound (US). Women with a cervical length below or equal to 30 mm (but more than 5 mm) are eligible for the trial.

Exclusion criteria are painful contractions, vaginal bleeding, cerclage during current pregnancy before the screening, PPROM, severe liver disease, cholestasis during this pregnancy, previous or current thromboembolism, placenta previa, cervical dilation greater than 1 cm, monoamniotic twin pregnancy, higher order twin pregnancy (triplets or higher), major fetal malformation of at least one fetus and stillbirth.

All participating members of the research team are trained to perform the cervical measurement by ultrasound and to manage the pessary. All sonographers are trained in cervical measurement according to The Fetal Medicine Foundation training program [33] and are encouraged to follow its certification program. Additionally, an online training program (using Moodle platform) was created to certificate all sonographers involved in the P5 study in standardizing cervical measurements, and at this Moodle platform, all participants of the research had signed the disclosure of contractual agreements that limit such access for investigations. The ultrasound examination will be performed using a GE Logic C5® equipment.

A research assistant will invite women attending the ultrasound department of each institution or outpatient clinics involved in the study to participate in the screening strategy and, after being informed about the study, to sign a written Informed Consent Form. A transvaginal ultrasound scan to measure cervical length as described above will be performed.

Women with a short cervix and without any exclusion criteria will then be invited to participate in the randomized clinical trial. After being informed about the study verbally and with a written patient information leaflet, women will be asked to sign an Informed Consent Form. Only after written informed consent, the local investigator will randomly assign patients. In case of an eligible participant under 18 years old, a consent form will be signed for both the underaged participant and his/her legal guardian/parent before been admitted into the study.

After written informed consent, women will be randomized into two groups: the use of pessary plus progesterone or the use of progesterone alone. Randomization will be stratified by center, number of fetuses (one or two) and cervical length (< 25 mm or 25-30 mm) using a 1:1 ratio and variable block sizes. Randomization is performed electronically in an online database added as a specific form in the online data collection system, using computer-generated random numbers. The system can be accessed 24/7 and a phone number is available to help the inclusion and randomization process. Each local coordinator will be responsible for the randomization process including enrollment and assignment of women to interventions.

Since the use of the pessary cannot be blinded, this is an open-label RCT. The pessary used is an Arabin type pessary registered at the national health surveillance agency of Brazil (Pessário AM® by Ingamed) with the dimensions: inner circle 30 mm; outer circle 70 mm; height 25 mm.

A physician trained specifically for pessary placement will insert the pessary up to 72 h from the randomization. An ultrasound scan to re-assess cervical length and pessary placement will be performed after its insertion.

We will use 200 mg micronized progesterone capsules that will be self-administered digitally inserted into the vagina every night. Commercial Progesterone (Utrogestam®) pills will be purchased from Besins Healthcare Pharmaceutics. Both interventions will be maintained until 36 weeks gestation unless antenatal care providers consider the need to withdrawal earlier.

The intervention will be discontinued before 36 weeks only if the assistant medical doctor judges it is necessary due to clinical conditions, or in case of woman request. Every enrolled woman will receive access to a P5 phone number for her to call in case of doubts or need to report side events. A research assistant will be full time available for solving such questions.

Women with threatened preterm labor will be treated with tocolysis, corticosteroids and magnesium sulfate according to local protocols.

Prenatal care will continue in each reference facility considering local protocols. In each visit, the participant will be asked about the use of progesterone and pessary, symptoms, adverse events, and admission to hospital. She will receive enough progesterone until the next appointment when more capsules will be delivered. One research assistant per center will follow up all enrolled women avoiding double data collection. Adherence monitoring will be checked in all visits with the woman returning her drug table.

All enrolled women will be followed-up until 10 weeks after birth. To avoid a loss to follow-up, participants will be contacted by telephone if they miss an appointment. Compliance will be measured by the number of progesterone pills returned by the subject at each antenatal care visits.

Our primary outcome is a composite of neonatal adverse events: periventricular leukomalacia (focal periventricular necrotic and diffuse gliosis in the surrounding cerebral white matter that may have cystic lesions secondary to necrotic foci in the white matter) [34], severe respiratory distress syndrome (grunting, retractions, or other typical distress symptoms in a premature infant immediately after birth with a chest radiography showing homogenous opaque infiltrates and air bronchograms) [35], bronchopulmonary dysplasia (infant requiring treatment with > 21% oxygen for at least 28 days) [36], periventricular hemorrhage grade II (hemorrhage is present in a nondistended lateral ventricle) or higher [37], necrotizing enterocolitis (spectrum of intestinal conditions including feeding intolerance, mild abdominal distention, spontaneous intestinal perforations and intestinal necrosis) [38], proven sepsis before discharge (generalized bacterial infection occurring within the neonatal period up to 4 weeks beyond the expected date of delivery accompanied by a positive blood culture) [39], stillbirth, or neonatal death.

Secondary outcomes will be gestational age at birth, birth weight, adequacy of birth weight for gestational age, first and fifth minute Apgar score, neonatal gestational age, overall, spontaneous and medical induced PTB rate before 28, 32, 34 and 37 weeks of gestation, PPROM rate, neonatal intensive care unit (NICU) admission and length of stay, maternal morbidity and mortality, maternal length of stay in hospital, maternal ICU admission, cost-benefit analysis of the screening program, treatment cost, maternal inpatient treatment costs, neonatal inpatient treatment costs and pessary use unwanted effects [40, 41].

Information on readmissions of mother and/or newborn and primary and secondary outcome will be collected during hospitalization for birth and at 10 weeks after due date, by telephone contact and patient’s registries review.

Considering the reduction in the risk of preterm delivery by the pessary described by the PECEP clinical trial [27], and considering our own outcomes in women with a short cervix, we anticipate a composite poor neonatal outcome rate of 22%. We consider a reduction of 10% as clinically relevant. The reduction from 22 to 12% in the composite poor neonatal outcomes (2-sided alpha 0.05, 80% power) can be detected if 438 women are randomized (219 per group). To assure a subgroup analysis for cervical length less than or equal to 25 mm, considering a reduction of 50% in adverse neonatal outcomes (17.3 to 8.65% [15]), it will be necessary to increase a sample to 468 women (234 per subgroup). Thus, the final sample should be composed of 936 women (468 in each group, 234 per subgroup).

The data will be collected using an online database, which is a new generation of application systems that allow the collection and cleaning of clinical trial data using the Internet. This technology was developed specifically for the study using an existing certified platform for medical offices management. The online database has distinct permission levels and is encrypted and protected by a personal security password. Data will be stored in cloud network and a backup is being performed every day.

The forms and the randomization process are inserted in the platform and access is given to each facility coordinator and research assistant for local data management. Each local coordinator is responsible for data entry. Data will be collected in printed forms or directly in the online form, available in the same online database where the randomization takes place, by a trained research assistant. The local coordinator will verify these data in the printed and online system, to assure the information is correct.

Data analysis will be performed according to the intention-to-treat principle. A statistical analysis plan will be finalized prior to the data lock.

Categorical variables will be expressed by the relative frequency on the corresponding allocation arm. For continuous variables minimum, first quartile, median, third quartile, maximum, mean, and standard deviation will be presented. Missing values will be reported for all variables.

The primary outcome is a binomial random variable. For this outcome, we will estimate a risk ratio (RR) with 95% CI. We will also calculate rates in the two groups as well as the number needed to treat (NNT). The comparisons of treatments will be performed with a generalized linear model [42], with the log link function. The model will include treatment as main effect and a full factorial of study center, type of pregnancy (twin or singleton) and cervix length (two categories). The main analysis will be performed using stratums according the randomization process. All factors are fixed. The factors study center, type of pregnancy and cervix length figure as randomization block terms.

An additional model including cervical length as continuous covariate will also be analyzed. The model better adjusted will be used as final model. The Akaike Information Criterion (AIc) e Bayesian Information Criterion (BIC) will be used to decide among models. To evaluate the potential efficacy of the pessary, a per-protocol analysis will also be performed.

Secondary outcomes will be analyzed using generalized linear models with treatment as main effect and a full factorial of study center, type of pregnancy (twin or singleton) and cervix length (two categories). All factors are fixed. An appropriated link function will be chosen to each response variable.

An additional model including cervical length as continuous covariate will also be analyzed. The model better adjusted will be used as final model. The Akaike Information Criterion (AIc) e Bayesian Information Criterion (BIC) will be used to decide among models.

Survival analysis to assess time to delivery will also be performed using Kaplan Meier and Cox Proportional Hazard Model. Differences in treatments among subgroups will be assessed including in the statistical models already described above a subgroup variable and a interaction term subgroup-treatment. These are the subgroups to be analyzed:

The DSMB-P5 will meet at predetermined intervals (after half of the randomized cases and after 2/3 of the randomized cases) to analyze the results regarding the possible adverse effects of the interventions or regarding the achievement of statistical significance for the main outcome. Other interim analyses will be calculated according to DSMB-P5 request. The committee will have the power to recommend completion of the study or an early interruption based on the evaluation of the interim results and on some pre-specified stopping rules.

The study started woman enrolment in July 2015. Chronogram considers finishing enrolment in April 2019. Final reports and publication are expected by December 2019.