Prenatal Development of NADPH-diaphorase-Reactive Neurons in Human Frontal Cortex

doi:10.1093/cercor/6.5.737

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Cerebral Cortex 1996; 6:737-745
© Oxford University Press 1996

research-article

Prenatal Development of NADPH-diaphorase-Reactive Neurons in Human Frontal Cortex

X. X. Yan¹^,2, L. J. Garey³^, and L. S. Jen³

¹Department of Anatomy and Neurobiology, Hunan Medical University Changsha, Hunan 410078, People's Republic of China, ²Present address: Department of Anatomy and Neurobiology, University of California Irvine, CA 92717-1275, USA, ³Department of Anatomy, Charing Cross and Westminster Medical School London W6 8RF, UK

Correspondence should be addressed to L. J. Garey, Department of Anatomy, Charing Cross and Westminster Medical School, London W6 8RF, UK

Nicotinamide adenine dinucleotide phosphate-diaphorase (NADPH-d)histochemistry was used to study the morphology and developmentof neurons that metabolize nitric oxide (NO) in the frontalcortex of human fetuses aged from 13 weeks of gestation (13W)to term, to investigate whether the two distinct types of NOneuron described in the adult develop differently. Large, heavilystained, sparsely spiny, non-pyramidal neurons (Type I) developby 15W mainly in the subplate (SP) of the cortical Anlage. Theyachieve an adult-like pattern by 32W, distributed thoughoutthe cortex and subcortical white matter, but with the highestconcentration in the white matter. Small, lightly stained cells(Type II) develop later (32W) thoughout the cortex, but especiallyin layers II-IV. and increase in number to term. NADPH-d-positivedendrites and axons appear in the cortex and white matter by15W. They include thick, radially oriented, dendritic processesfrom Type I neurons in SP and CP Their arbors expand and maturebetween 17 and 28W. Fine horizontal axons are visible in layerI by 17W. Others develop in layers II-IV from 28W, and havereached a high degree of development by term. NADPH-d-positiveaxons in the cortex seem to have both intrinsic and extrinsicorigins. Thus the two types of NADPH-d neurons found in adultprimate, including human, cortex are reflected by differentdevelopmental forms prenatally. It is concluded that NO-metabolizingneurons in the human cortex may be involved in various aspectsof development, including morphological and functional maturation,and that the late-developing Type II neurons may represent acell line specific to primates, perhaps related to the developmentof their higher cortical activity and of potential importancein the pathophysiology of diseases of cognitive function.

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