Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT05787054 |
| Other study ID # |
1909 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
January 1, 2021 |
| Est. completion date |
May 27, 2023 |
Study information
| Verified date |
May 2023 |
| Source |
Fondazione Policlinico Universitario Agostino Gemelli IRCCS |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
The aim of this trial is to assess the efficacy and efficiency of the national and the
research sonographic screening protocols for fetal growth disorders.
In particular, in Italy at the moment we have two different national screening protocols: the
traditional one providing an early third trimester scan at 28-32 weeks'gestation, and a more
recent one, according to the new LEA (livelli essenziali di assistenza), providing a growth
scan during the third trimester only if there is a clinical indication. Both these national
protocols will be compared to a research protocol providing a late third trimester scan
between 35 and 37 weeks'gestation in terms of sensibility and specificity.
Description:
3. PURPOSES AND OBJECTIVES OF THE CLINICAL TRIAL The aim of this trial is to assess the
efficacy and efficiency of the national and the research sonographic screening protocols for
fetal growth disorders.
In particular, in Italy at the moment we have two different national screening protocols: the
traditional one providing an early third trimester scan at 28-32 weeks'gestation, and a more
recent one, according to the new LEA (livelli essenziali di assistenza), providing a growth
scan during the third trimester only if there is a clinical indication. Both these national
protocols will be compared to a research protocol providing a late third trimester scan
between 35 and 37 weeks'gestation in terms of sensibility and specificity.
4. EXPERIMENTAL DESIGN
4.1 STUDY ENDPOINTS
This study is designed to generate level 1 evidence of diagnostic efficacy. MAIN OUTCOME: The
main outcome of the two protocols in screening true late preterm and term SGA fetuses is
measured based Italian newborn weight charts centiles 8mmol/L, admission at NICU)
- Composite severe adverse perinatal (stillbirth or term live birth associated with
neonatal death, hypoxic ischaemic encephalopathy, use of inotropes, need for mechanical
ventilation, or severe metabolic acidosis (defined as a cord blood pH <7•0 and base
deficit >12 mmol/L)
TERTIARY OUTCOME
- Number of ultrasound scans performed in outpatient clinics by medical indication
(SSR-prescription) beyond Early-TT and late-TT scheduled exams, and number of ultrasound
scans performed on indication in outpatient clinics minus the first one indicated.
- Number of ultrasound scans by patient choice
- Econometrics of the two protocols, and of the estimated sanitary costs of outcomes
4.2 EXPERIMENTAL PLAN
Women who agree to participate are randomized to the local regional Protocol vs Late-TT
protocols. Basing on the different Regions'protocols the third trimester screening is
performed either in the early third trimester at 28-32 weeks of gestation (Early Third
Trimester screening - Early-TT) or only on clinical indication (Third Trimester on Indication
- TT-indication). For this reason, this trial will be in fact split into two independents
parallel randomisation. In practical terms this mean that women who agree to take part into
the trial and sign an informed consent, will be randomized to the Early third trimester
Protocol (Early-TT), vs Late Third Trimester Protocol (Late-TT)(Trial n°1) or to Third
Trimester U/S on indication (TT-Indication) vs Late Third Trimester Protocol (Late-TT)(Trial
n°2).
5. STUDY POPULATION
5.1 SAMPLE SIZE Sample size was calculated based on results by Roma et al2 considering a
sensitivity of Early-TT in detecting SGA at birth (birth weight below 10th centile) of 22.5%
compared to 38.8% of Late-TT, and Sovio et al considering a sensitivity of 20% compared to
57%, a confidence level of 95% (1-alpha) and an 80% power (1-beta), and a one to one ratio
between the TT-Indication and the Late-TT arms.
According to Fleiss14 each arm should be 138, which implies 270 for two arms of the Early-TT
vs Late-TT, and 101 for the two arms TT-Indication vs Late-TT considering the 10% of the SGA
population. The sample size needed considering both AGA and SGA, will then be 270 x10=2700
and 101x10=1010 pregnant women for the two randomizations respectively. Considering 10% of
drop-out and incomplete data the final sample size should be increased of such percentage in
each branch of the study. It has to be acknowledged that in the Late-TT arm there will be an
additional split of the women after the randomization allocation based on the uterine artery
Doppler velocimetry result. However, when calculating the sample size we did not take into
account this secondary partition because we aim to consider the overall performance of
Late-TT in identifying late preterm and term SGA as a primary outcome.
5.2 PATIENT SELECTION 5.2.1 INCLUSION CRITERIA Eligible cases are nulliparous pregnant women,
with first trimester ultrasound assessment of gestational age, who conceived singleton
fetuses. If the crown-rump-length (CRL) differs of more than ± 3-5 days from the last
menstrual period, gestational age is calculated on the CRL.
5.2.2 EXCLUSION CRITERIA
- major medical disease
- high risk for preeclampsia on history or detected in those centres that perform
pre-eclampsia screening at first trimester
- women older than 40 years on ASA low dose prophylaxis
- known immune disorders or clinical thrombophilic conditions;
- twin pregnancies;
- ovodonations
- suspected fetal anomalies at any gestational age
- Papp-A at Combined-Test<0.2
5.3 WITHDRAWAL PROCEDURES If a patient, during the study protocol, wanted to withdrawal, this
will not modify the subsequent monitoring of her pregnancy following local protocols.
6. SUBJECT TREATMENT
• RANDOMIZATION : Patients who agree to participate and sign an informed consent, Women who
agree to participate are randomized to the local regional Protocol vs Late-TT protocols.
There will be two different arms in each clinic: The Early third trimester Protocol
(Early-TT) versus the Late Third Trimester Protocol
