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发育中的视觉皮层中胼胝体投射与联合投射的互换

Interchange of callosal and association projections in the developing visual cortex.

作者信息

Innocenti G M, Clarke S, Kraftsik R

出版信息

J Neurosci. 1986 May;6(5):1384-409. doi: 10.1523/JNEUROSCI.06-05-01384.1986.

Abstract

Neurons projecting transitorily into the corpus callosum from area 17 of the cat were retrogradely labeled by the fluorescent tracer Fast Blue (FB) injected into contralateral areas 17 and 18 on postnatal days 1-5. During the second postnatal month these neurons were still labeled by the early injection, although they had eliminated their callosal axon. At this time, 15-20% of these neurons could be retrogradely relabeled by injections of Diamidino Yellow (DY) into ipsilateral areas 17 and 18, but few or none by similar injections in the other areas that receive from area 17 (19, 21a, PMLS, 20a, 20b, DLS). Similarly, area 17 neurons projecting transitorily to contralateral area PMLS during the first postnatal week could be relabeled by DY injections in ipsilateral areas 17 and 18 but not in PMLS. Already around birth, many transitorily callosal neurons in area 17 send bifurcating axons both to contralateral areas 17 and 18 and ipsilateral area 18. It is probable that during postnatal development some of these neurons selectively eliminate their callosal axon collaterals and maintain the projection to ipsilateral area 18. In fact, some transitorily callosal neurons in area 17 can be double-labeled by simultaneous perinatal injections of FB in contralateral areas 17 and 18 and of a new long-lasting retrograde tracer, rhodamine-conjugated latex microspheres, in ipsilateral area 18. The same neurons can then be relabeled by reinjecting ipsilateral area 18 with DY during the second postnatal month. This finding, however, does not exclude the possibility that some transitorily callosal neurons send an axon to ipsilateral area 18 after eliminating their callosal axon. In conclusion, area 17 neurons that project transitorily through the corpus callosum later participate, probably permanently, in ipsilateral corticocortical projections but selectively to areas 17-18. The mechanism responsible for this selectivity is unknown, but it may be related to the differential radial distribution (i.e., to birth date) of area 17 neurons engaged in the various corticocortical projections. The problems raised by the use of long-lasting retrograde fluorescent tracers in neurodevelopmental studies and by the quantification of results of double- and triple-labeling paradigms are also discussed.

摘要

在出生后第1至5天,将荧光示踪剂快蓝(FB)注入猫对侧的17区和18区,可对从17区短暂投射到胼胝体的神经元进行逆行标记。在出生后的第二个月,尽管这些神经元已经消除了它们的胼胝体轴突,但早期注射仍能使它们被标记。此时,将双脒基黄(DY)注入同侧的17区和18区,可使15%-20%的这些神经元被逆行重新标记,但将其注入从17区接收投射的其他区域(19区、21a区、内侧旁中央小叶、20a区、20b区、背外侧沟)进行类似注射时,很少或没有神经元被重新标记。同样,在出生后第一周短暂投射到对侧内侧旁中央小叶的17区神经元,可通过向同侧17区和18区注射DY而被重新标记,但向内侧旁中央小叶注射则不能。在出生前后,17区许多短暂的胼胝体神经元就已发出分支轴突,分别投射到对侧的17区和18区以及同侧的18区。在出生后的发育过程中,这些神经元中的一些可能会选择性地消除其胼胝体轴突分支,并维持对同侧18区的投射。事实上,在围产期同时将FB注入对侧的17区和18区,以及将一种新的长效逆行示踪剂罗丹明偶联乳胶微球注入同侧的18区,可使17区一些短暂的胼胝体神经元进行双重标记。在出生后的第二个月,通过再次向同侧18区注射DY,这些相同的神经元可被重新标记。然而,这一发现并不排除一些短暂的胼胝体神经元在消除其胼胝体轴突后向同侧18区发出轴突的可能性。总之,那些短暂通过胼胝体投射的17区神经元,后来可能会永久性地参与同侧皮质-皮质投射,但只是选择性地投射到17-18区。造成这种选择性的机制尚不清楚,但可能与参与各种皮质-皮质投射的17区神经元的不同径向分布(即出生日期)有关。本文还讨论了在神经发育研究中使用长效逆行荧光示踪剂以及对双重和三重标记范式结果进行定量分析时所引发的问题。

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