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NCT03651648 Clinical Trial

Apnea Treatment in Premature Infants Using an Automatic Vibro-tactile Stimulator Triggered by the Detection of Apnea-bradycardia.

Apnea of Prematurity Clinical Trial

SENSITACT

Official title:
Apnea Treatment in Premature Infants Using an Automatic Vibro-tactile Stimulator Triggered by the Detection of Apnea-bradycardia.

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT03651648
Other study ID # 35RC16_9894_SENSITACT
Secondary ID
Status Recruiting
Phase N/A
First received
Last updated
Start date October 18, 2019
Est. completion date July 2, 2024

Study information
Verified date November 2023
Source Rennes University Hospital
Contact Patrick PLADYS, Pr
Phone 06 34 19 11 30
Email patrick.pladys@chu-rennes.fr
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The goal of the SENSITACT system is to activate an adaptive kinesthetic stimulation to treat apnea-bradycardia events on preterm infants, while minimizing deleterious effects, in particular arousals that can be due either to respiratory efforts or to kinesthetic stimulation itself. This novel system will provide an alternative treatment to apnea-bradycardia, with improved patient comfort and autonomy. In particular, it may become a complementary solution for the current treatments (Manual stimulation by caregivers, continuous or intermittent nasal positive pressure ventilation and methylxanthine therapies) that do not appear to be optimal and usually only allow a partial reduction in the number and severity of apneas.

Description:

The main hypothesis behind the SENSITACT system is that kinesthetic stimulation can terminate apneas-bradycardias with minimal patient arousal. The aim is to stimulate mechanoreceptors through the skin by kinesthetic stimulation on the lower abdominal zone. This is a region of the body that is covered with Pacinian corpuscles, a very sensitive kind of mechanoreceptors, which respond to rapid vibrations on the skin (200-300 Hz). Vibro-tactile stimulation of these mechano-receptors will trigger a reaction typical of the startle reflex. This reflex causes 1) an immediate myotonic reaction and 2) a widespread autonomic response. The former should have a direct effect on obstructive respiratory disorders with an increase in chin muscle tones within 80 to 100 ms. The latter should act on central respiratory disorders, with activation of the sympathetic nervous system. Since both responses are mediated via sub-cortical nervous center, it is expected that patient arousal will be limited. Preliminary clinical studies on adult patients conducted by LTSI, Sorin CRM and CHU de Grenoble (Skin&SAS, HYPNOS, EKINOx), that have used the same PASITHEA stimulation device have confirmed activation of the sympathetic nervous system and a significant reduction in the duration of apnea or hypopnea events, while no differences were observed on patients' sleep architecture. The SENSITACT system is able to detect apneas-bradycardias in real-time, so that kinesthetic stimulation can be triggered to stop respiratory disorders very early during the event. Detection is performed within the SENSITACT controller station that receives data from all sensors connected to the Patient Monitor in real-time. As soon as the early signs of an apnea-bradycardia are detected, the SENSITACT controller sends a trigger signal to the PASITHEA stimulator that immediately activates kinesthetic stimulation. Kinesthetic stimulation is stopped when a normal condition (normal cardiac rhythm) is detected or when a maximum number of stimulation pulses have been reached.

Recruitment information / eligibility
Status Recruiting
Enrollment 24
Est. completion date July 2, 2024
Est. primary completion date January 2, 2024
Accepts healthy volunteers No
Gender All
Age group 34 Weeks to 36 Weeks
Eligibility Inclusion Criteria: - written informed consent, - Premature infants, - born to a term less than 34 weeks of amenorrhea (AS), - Age less than 36 weeks post-menstrual age, - With a postnatal age greater than 4 days, - caffeine treated, for at least 36 hours, - Presenting episodes of bradycardia apnea significant (>10 sec with bradycardia <100 bpm or SaO2<80%) with an interval of less than 6 hours between two episodes observed in the 24 hours preceding inclusion. Exclusion Criteria: - Major congenital neurological abnormalities, - Congenital abnormalities of the respiratory tracts, - HIV grade 3 or 4, - Periventricular leukomalacia, - Invasive ventilation and non-invasive ventilation in NAVA mode, - Cyanogenic malformative heart disease, - Sepsis diagnosed in the 4 days prior to registration (CRP> 10mg / L), - maternal addiction during pregnancy, - Father and / or mother legally protected (under judicial protection, guardianship or supervision).

Study Design

Related Conditions & MeSH terms

Intervention

Device:
SENSITACT System
the activated stimulation (ON period of 6 hours) will be hidden from the care team, who will continue the care according to the usual procedures (blind treatment).
SENSITACT System
the desactivated stimulation (OFF period of 6 hours) will be hidden from the care team, who will continue the care according to the usual procedures (blind treatment).

Locations
Country Name City State
France CHU de Rennes Rennes

Sponsors (1)
Lead Sponsor Collaborator
Rennes University Hospital

Country where clinical trial is conducted

France, 

Outcome
Type Measure Description Time frame Safety issue
Primary Cumulative duration of apnea-bradycardia Cumulative duration of apnea-bradycardia over a period of 6 hours with stimulation activated or not. 12 hours (H12)
Secondary Distribution of bradycardia durations A bradycardia is defined by an acute event lasting at least 5 seconds with a decrease in heart rate of more than 33% of the basal heart rate (median of heart measured on 5-min stationary periods during quiet sleep).
The distribution of the durations will be quantified in terms of median, IQR and distribution curve		 12 hours (H12)
Secondary Depth of bradycardia A bradycardia is defined by an acute event lasting at least 5 seconds with a decrease in heart rate of more than 33% of the basal heart rate (median of heart measured on 5-min stationary periods during quiet sleep).
The depth of bradycardia will be measured by the area under the curve with the upper limit of the curve defined by the value of "basal heart rate-33%" and expressed in beats/min*sec The distribution of the depth of bradycardias will be quantified in terms of median, IQR and distribution curve		 12 hours (H12)
Secondary Depth of desaturations The depth of desaturation will be measured by the area under the curve with the upper limit of the curve set at a Saturation of 80% The distribution of the depth of desaturations will be quantified in terms of median, IQR and distribution curve 12 hours (H12)
Secondary Caregiver interventions The number of caregiver interventions associated with a cardio-respiatory event will be quantified and expressed in number/hour 12 hours (H12)
Secondary Cardiorespiratory parameters in response to stimulation The delay between the initiation of stimulation and the first breath will be measured and expressed in median IQR The delay between the initiation of stimulation and the normalization of heart rate above the limit of "basal heart rate-33%" will be measured and expressed in median IQR The delay between the initiation of stimulation and the observation of a Saturation above 80% will be measured and expressed in median IQR 6 hours (H6)
Secondary Premature's sleep-wake cycles Duration of the stages identified 12 hours (H12)
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