IN a landmark study conducted across six New York City hospitals, researchers have found that genomic sequencing can significantly enhance newborn screening by detecting additional actionable conditions beyond the current standard newborn screening program. Involving 4,000 newborns from racially and ethnically diverse families, the study showed that targeted genomic screening not only achieved a 99.6% completion rate but also demonstrated a 3.7% screen-positive rate, identifying treatable conditions that standard tests often miss.
The study, part of the larger Genomic Uniform-Screening Against Rare Disease in All Newborns (GUARDIAN) project, highlights the feasibility and acceptance of genome sequencing in routine newborn screening programs. Of 5,555 families approached, 72% consented to participate, with 90.6% opting to include all tested conditions, underscoring parental willingness for expanded health insights in newborns. The sequenced gene panel targeted 156 known early-onset conditions with effective treatments, with an additional optional screen for neurodevelopmental disorders linked to seizures.
The screened newborns represented a diverse demographic profile: 16.5% were Asian, 25.1% Black, 44.7% White, and 13% multiracial, with 44% identified as Hispanic. This diversity aligns with the study’s goal of ensuring genome screening inclusivity across different racial and ethnic groups, addressing a crucial gap in current healthcare practices.
The findings are significant for healthcare providers, illustrating that targeted genomic screening can identify actionable genetic conditions early on, potentially reducing the burden of undiagnosed or late-diagnosed diseases in newborns. Although further research is needed to confirm these findings across broader populations, the study points toward a future where genomic sequencing could augment traditional screening, helping clinicians to intervene sooner and improve patient outcomes.
Reference: Sternberg c et al. Cell-autonomous IL6ST activation suppresses prostate cancer development via STAT3/ARF/p53-driven senescence and confers an immune-active tumor microenvironment. JAMA. 2024.
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