Psychomotor Impairment Clinical Trial
Official title:
Correlation Between Neonatal Cerebral Oxygenation and Later Psychomotor Outcome in Very-low-birth-weight Preterm Infants.
The recent improvements in neonatal intensive care have led to a substantial increase in the
survival rate of preterm infants; nevertheless, this population is still at high risk for
long-term neurodevelopmental disabilities. Significant anatomical changes in brain
structures and abnormal patterns of neuronal myelination and brain connectivity have been
associated with preterm birth, with possible long-term effects on cognitive, motor and
social skills.
The validation of clinical tools able to predict neurodevelopmental outcomes in the preterm
population might help at identifying infants at greatest risk of impairment, who would
benefit most from early supportive interventions exploiting brain neuroplasticity.
Near infrared reflected spectroscopy (NIRS) provides a bedside, non-invasive, continuous
monitoring of cerebral oxygen saturation (CrSO2), which has been proposed as a predictive
marker for later neurodevelopment in neonates undergone cardiac surgery; to date, however,
evidence on the correlation between CrSO2 and later neurodevelopment in preterm infants is
almost lacking.
This study aims to evaluate whether CrSO2 monitoring, performed before NICU discharge in
clinically stable very low birth weight (VLBW) preterm infants, can predict psychomotor
outcomes during the first 24 months of corrected age (ca).
The improvements in neonatal intensive care occurred over the last decades have led to a
substantial increase in the survival rate of preterm infants, especially of extremely low
birth weight. Nevertheless, the delicate maturation of central nervous system (CNS) in the
extrauterine environment, together with the possible development of prematurity-related
clinical complications that could result in brain injury, place this population at high risk
for long-term neurodevelopmental disabilities.
Significant anatomical changes in brain structures have been associated with preterm birth;
among these, enlarged ventricles and subarachnoid spaces, reduced subcortical white matter
and decreased cortical and deep nuclear grey matter are the most common. Additionally, there
is increasing evidence of abnormal patterns of neuronal myelination and brain connectivity
in preterm infants, with possible concerning long-term effects on language, motor and social
skills. As for cognitive abilities, a direct correlation with gestational age (GA) has been
previously shown in a large cohort of preterm born children at school age.
In its early phases, the developmental of CNS is characterized by an intrinsic
neuroplasticity, according which repeated experiences could influence the arrangement of
synaptic connections and neural circuitries, thus resulting in structural and functional
changes. By exploiting this feature, an early establishment of supportive interventions¬
might aid to compensate the anatomical and functional constraints connected to preterm birth
and to improve preterm infants' neurodevelopment.
The validation of clinical tools able to predict neurodevelopmental outcomes in the preterm
population might help at identifying infants at greatest risk of impairment, who would
benefit most from early rehabilitative interventions. Near infrared reflected spectroscopy
(NIRS) provides a bedside, non-invasive, continuous monitoring of cerebral oxygen saturation
(CrSO2) and has been largely adopted to assess neonatal brain oxygenation and perfusion in
intensive care settings. Perioperative CrSO2 has been recently proposed as a possible
predictor of later neurodevelopmental outcomes in neonates undergone cardiac surgery; data
evaluating the correlation between CrSO2 and later neurodevelopment in preterm infants,
however, are very scarce and limited to the first days of life; at this time, CrSO2 can be
widely influenced by the occurrence of systemic haemodynamic instability and is blind to
several clinical complications, known as potential causes of brain damage, that can occur
later on during hospital stay and thus are not necessarily directly related to changes in
cerebral oxygenation within the first days of life (e.g. necrotizing enterocolitis [NEC],
late onset sepsis).
Hence, the aim of this study was to evaluate whether CrSO2 monitoring, performed before NICU
discharge in clinically stable very low birth weight (VLBW) preterm infants, can predict
psychomotor outcomes during the first 24 months of corrected age (ca).
Infants meeting eligibility criteria (for details see specific section) undergo a 3-hour
continuous monitoring of CrSO2 by means of the INVOS 5100 oximeter when satisfying the
following condition: stable clinical condition, no need for oxygen supplementation, full
enteral feeding (defined as 160 ml/kg/day) After discharge, the enrolled infants are
included in a long-term neurodevelopmental follow-up, which is part of the normal routine
care for preterm-born infants and aims at the early identification and treatment of
neurocognitive sequelae possibly related to preterm birth.
In this context, psychomotor outcome (PSO) is assessed at 6, 12, 18 and 24 months ca by
means of the Griffiths Mental Development Scales 0-2 years [26]. These scales investigate
five main areas (locomotor, personal and social skills, hearing and language, eye and hand
coordination, performance), providing a general developmental quotient (DQ) of infant's
abilities and five sub-scale quotients (SQ) for each of the developmental areas.
The Griffiths Scales are administered individually, over a 45-min period, by the same
professional trained psychologist for the whole study period and are implemented in the
presence of the infant's parent.
A correlation analysis between mean CrSO2 values and GQ/SQ scores at each follow-up
appointment will be performed. In order to evaluate the effect of possible confounding
variables on the observed results, a mixed model including a number of risk factors known to
affect preterm infants' neurodevelopment will be built for hierarchical multiple regression
analysis. Significance level will be set at p<0.05.
;
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Completed |
NCT03297944 -
Sedative-Anxiolytic Effects on Simulated Driving Performance
|
Phase 4 | |
| Completed |
NCT02710578 -
Alcohol Effects on Driving-related Skills of Young Drivers
|
N/A | |
| Completed |
NCT03106363 -
Combined Alcohol and Cannabis Effects on Skills of Young Drivers
|
Early Phase 1 | |
| Completed |
NCT01592409 -
Cannabis Effects on Driving-related Skills of Young Drivers
|
N/A | |
| Recruiting |
NCT04288531 -
Iodine Impact on Thyroid Function and Psychomotor Development, Observational Study in the Portuguese Minho Region
|