MedPath

Newborn Genomics Programme

Recruiting
Conditions
Newborn Morbidity
Genetic Disease
Interventions
Other: Genetic testing
Registration Number
NCT06081075
Lead Sponsor
Liggins Institute
Brief Summary

Genomic methods can significantly contribute to all facets of precision medicine, from diagnosis to prevention, therapeutic intervention, and management of acute and chronic illnesses. DNA based methods are already having a considerable impact across healthcare in fields that include: public health, infectious disease monitoring, acute and chronic disease, pharmacogenomics, prenatal testing and diagnosis, and therapeutic development. In this proposal, investigators are focusing on the application of genomic methods in precision medicine - specifically on rapid whole-genome sequencing of parents and children (i.e. a trio) for the identification of diseases that have genetic components.

Goals Primary goal: is to provide safe rapid whole genome sequencing to Neonatal Intensive Care Unit/Pediatric Intensive Care Unit patients.

Secondary goals: 1) Although several groups globally are implementing rapid sequencing of rare disease, these are predominantly in the research space, with many unanswered questions regarding the best way to implement them into a national healthcare system. Each country and their healthcare systems are unique, and valuable knowledge will be gained by implementing this process within a New Zealand context. As part of this the study will measure the impact on the individuals and families.

2) to expand the research team's understanding of non-coding disease-causing variants and methylation changes that contribute to severe disease in early life.

Primary Aims

1. To incorporate long-read RNA sequencing data into the diagnostic rapid Whole Genome Sequencing pipeline to provide a direct measure of the functional outcome of the variants of clinical concern.

2. To measure the clinical utility of analysing non-coding variants in the diagnosis of critically ill children who do not have pathogenic, likely pathogenic, or variants of unknown significance for mendelian disorders.

3. To identify, in a real-world setting within the New Zealand health-care system, the clinical and economic effects of deploying rapid Whole Genome Sequencing-informed rapid precision medicine for critically ill children.

Detailed Description

Not available

Recruitment & Eligibility

Status
RECRUITING
Sex
All
Target Recruitment
500
Inclusion Criteria
  • Acutely ill inpatient
  • Admitted to NICU or PICU between April 2023 - March 2026
  • Within 1 week of hospitalization or within 1 week of development of abnormal response to standard therapy for an underlying condition
  • Suspected genetic condition, without a clear non-genetic aetiology
Exclusion Criteria
  • Patients whose clinical course is entirely explained by
  • Isolated prematurity
  • Isolated unconjugated hyperbilirubinemia
  • Infection or sepsis with expected response to therapy
  • A previously confirmed genetic diagnosis that explains the clinical condition -
  • Isolated transient neonatal tachypnoea
  • Meconium aspiration syndrome
  • Trauma
  • Inability to source blood and buccal samples for DNA extraction from at least the mother and child

Study & Design

Study Type
OBSERVATIONAL
Study Design
Not specified
Arm && Interventions
GroupInterventionDescription
Acutely ill neonates with suspected genetic condition, without a clear non-genetic aetiologyGenetic testing-
Primary Outcome Measures
NameTimeMethod
To incorporate long-read RNA sequencing data into the diagnostic rapid Whole Genome Sequencing pipeline to provide a direct measure of the functional outcome of the variants of clinical concernJune 2025
To measure the clinical utility of analysing non-coding variants in the diagnosis of critically ill children who do not have pathogenic, likely pathogenic, or variants of unknown significance for mendelian disorders.June 2025
To identify, in a real-world setting within the New Zealand health-care system, the clinical and economic effects of deploying rapid Whole Genome Sequencing-informed rapid precision medicine for critically ill children.June 2025
Secondary Outcome Measures
NameTimeMethod

Trial Locations

Locations (1)

Auckland City Hospital

🇳🇿

Auckland, New Zealand

Related Trials

Genomic Medicine for Ill Neonates and Infants (The GEMINI Study)

CompletedNot Applicable
Tufts Medical Center
Posted 3/26/2019
Updated 8/28/2023

PErsonalized Genomics for Prenatal Abnormalities Screening USing Maternal Blood

Active, Not RecruitingNot Applicable
CHU de Quebec-Universite Laval
Posted 2/5/2019
Updated 2/12/2025

Perinatal Precision Medicine

Active, Not RecruitingNot Applicable
Rady Pediatric Genomics & Systems Medicine Institute
Posted 7/7/2017
Updated 3/1/2024
© Copyright 2025. All Rights Reserved by MedPath
HomeTerms & ConditionsPrivacy Policy