Human neonatal CITE-seq atlas identifies an immune transition at 32 weeks’ gestation from CD15⁺ myeloid-dominated to interferon-primed immunity
The study used human neonatal CITE-seq single-cell profiling across a wide gestational age range, analyzing 82 samples from 25 neonates plus adult controls, and included both baseline and stimulated immune conditions to assess functional responsiveness. The authors identified a gestational-age–dependent immune transition centered around 32 weeks, which separated extremely and very preterm neonates (GA <32 weeks) from those at higher gestational ages (≥32 weeks). Extremely/very preterm infants showed predominance of CD15+ granulocytic myeloid–derived suppressor cell-like programs, whereas more mature neonates displayed interferon-primed transcriptional profiles with divergent myeloid-to-lymphocyte signaling and qualitatively distinct NK and T cell bystander responses upon activation. The main caveat is that the atlas focuses on immune states at the first days of life, so longer-term developmental effects are not addressed. The paper does not explicitly discuss endometriosis or adenomyosis; it was included in the corpus via a keyword match in the upstream search index.
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- last seen: 2026-05-20T01:45:00.602351+00:00
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