Genetic Disease Clinical Trial
— PISCESOfficial title:
Genome Sequencing in the Intensive Care Unit Population
Verified date | November 2023 |
Source | University of Pittsburgh |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
The purpose of this study is to understand how the use of whole genome sequencing (WGS) may be able to increase the speed with which a diagnosis is made for patients in an intensive care unit population. This is not an assessment of a new device, test, or technology. This project is an investigation of the utility of this technology in clinical care when compared to standard of care testing. The study will look at the ability to more quickly diagnose a patient (time to diagnosis and efficacy of testing) as compared to standard of care testing. The study will also look at the impact of WGS on patient outcomes and cost of clinical care.
Status | Enrolling by invitation |
Enrollment | 400 |
Est. completion date | November 2024 |
Est. primary completion date | July 2024 |
Accepts healthy volunteers | No |
Gender | All |
Age group | N/A to 1 Year |
Eligibility | Inclusion Criteria: - Neonates: In order to be approached to participate, a neonate must meet all of the following criteria: 1. Greater than 24 weeks gestational age 2. Birth weight greater than 600 grams 3. Admitted to the intensive care unit at UPMC Children's Hospital (CHP) and/or Magee Women's Hospital 4. Possibility of a genetic disorder based on signs, symptoms, and laboratory values triggering a formal clinical medical genetics consult by the clinical care team. 5. Triaged by PI or attending co-investigators and prioritized to introduction of this research study based on patient-specific clinical concerns 6. Documented informed consent from parent/guardian - Parents: Parent of a neonate who meets the above inclusion criteria and who has been consented to participate in the study. - Siblings: Siblings of a neonate who meets the above inclusion criteria and who has been consented to participate in the study. Siblings will only be recruited if their participation has been determined to be essential to the accurate interpretation of the neonate's genetic studies. - Historical Controls: Individuals who have been evaluated by Medical Genetics within the last 24 months and who meet the criteria for matched controls as defined by propensity score matching. Exclusion Criteria: - Neonates: An individual who meets any of the following criteria will be excluded from participating in this study: 1. Has a known etiologic diagnosis (e.g. prenatal testing) 2. Has a major congenital anomaly (renal, cardiac, hepatic, neurological, or pulmonary malformations) associated with a chromosomal anomaly detected on prenatal testing (e.g. ultrasound, genetic testing) 3. Sequencing sent after birth for any other reason than the genetics consult that triggers the study 4. Presence of documented significant congenital infection (e.g. congenital cytomegalovirus) - Parents: 1. Is not the biological parent of the identified neonate 2. There is no exclusion for parent participation. If the parent is less than 18 years of age, however, these individuals will be asked to assent to the study and their parent(s) will be asked to provide permission/consent for the minor parent's participation 3. Having had previous genetic testing does not exclude the parent from participating in this study. - Siblings: 1. Is not a biological sibling of a neonate who meets the inclusion criteria 2. Is not require for accurate interpretation of neonate results 3. Having had previous genetic testing does not exclude the sibling from participating in this study. - Historical Control: Has not been seen within the past 24 months and/or does not meet the criteria for matched control as defined by propensity score matching. Part of this matching requires that the historical control be matched to a study participant based on age, thus they will be selected based on all matching criteria and will be excluded if they do not meet the criteria, including age. |
Country | Name | City | State |
---|---|---|---|
United States | UPMC Children's Hospital of Pittsburgh | Pittsburgh | Pennsylvania |
Lead Sponsor | Collaborator |
---|---|
Jerry Vockley, MD, PhD |
United States,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Confirmed Diagnosis | Categorical Y/N confirmed diagnosis in the neonate participant detected with WGS, compared to results from standard of care (SOC) or as seen in the historical control (HC) | Up to 4 years | |
Primary | Diagnostic Rate | Diagnostic rate with analysis via WGS, the 1722 neonatal specific gene filter, vs whole exome filter | Up to 4 years | |
Primary | Time to Diagnosis | Time to diagnosis in days with WGS as compared to SOC testing or HC | Up to 4 years | |
Primary | Clinical Utility of WGS | Clinical utility of WGS (e.g. changes in care management) compared to SOC or HC. Clinical utility is rated by a physician involved with case following the return of results using a Likert scale (1 - Not Useful at all, 2 - Not Very Useful, 3 - Neutral, 4 - Useful, 5 - Very Useful) | Up to 4 years | |
Primary | Care Cost Evaluation | Total care cost in dollars in those receiving WGS as compared to HC | Up to 4 years | |
Primary | Length of Stay | Total length of hospital stay in days in those receiving WGS as compared to HC | Up to 4 years | |
Primary | Need for Medical Utilization | Number of major medical procedures, imaging studies, or consulting services encounters in subjects receiving WGS compared to those in HC | Up to 4 years |
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