Monocyte Subsets in Neonates and Children

¹ Department of Pediatrics and the Department of Radiological Sciences, UCLA School of Medicine and the Physics Department, California State University, Los Angeles

Volumetrically distinct subpopulations of peripheral blood monocytes, termed M₁, M₂, and M₃, were identified in healthy normal adults and children. Because normal neonates have abnormal monocyte chemotaxis, it was determined whether monocyte subpopulations have different chemotactic capabilities and, if so, whether chemotactically active subpopulations were quantitatively deficient in neonates. Chemotaxis tests with zymosan-activated normal human serum as the chemoattractant and purified monocyte subpopulations revealed that large M₃ monocytes were capable of significantly more directed migration than were small M₁ and M₂ monocytes. Volumetric analysis of monocytes from normal newborns rather than demonstrating an absence of M₃ cells revealed that these cells were the predominant monocyte subpopulation. Therefore, we conclude that the impaired chemotactic ability of newborn monocytes is due to a functional rather than quantitative deficiency of M₃ cells.

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