Tieman S B
Neurobiology Research Center, State University of New York, Albany 12222.
Ann N Y Acad Sci. 1991;627:212-30. doi: 10.1111/j.1749-6632.1991.tb25926.x.
To summarize (Fig. 10), the structural consequences of monocular deprivation include the following changes: the relay cells in the binocular segments of the deprived geniculate layers shrink and contain less of the possible neurotransmitter NAAG. These changes appear to be secondary to a loss of terminal synaptic arbor. Certainly, deprived geniculocortical cells project to smaller ocular dominance patches in layer IV of visual cortex, where they make fewer and abnormal synapses. As a result, they activate ocular activation columns that, in addition to being small, are faint and usually fail to extend into extragranular layers. This failure to extend to other layers probably results from a failure of the poorly activated deprived-eye cells in layer IV to compete successfully with neighboring experienced-eye cells in layer IV, resulting in a loss of connections from layer IV to other layers (Fig. 11). Thus, the primary effect of monocular deprivation is probably the disruption of the geniculocortical synapse, with the other changes, such as cell size, and possibly the change in neurotransmitter content, being secondary. The disrupted synapse would result in poorly driven cortical cells and faint ocular activation columns, which in turn would bias a secondary competition for access to cells in extragranular layers. There are certain general principles that unite the findings presented in this chapter with the others in this session. First, there are similarities in the types of morphological changes observed, for example, changes in the number and size of synaptic terminals, as well as mitochondrial changes. This implies that there are similar changes during development and adult plasticity and also similar changes in vertebrates and invertebrates. Second, it is not so much the amount of activity that determines these changes, but the pattern of activity. In my results, the relative imbalance in activity is important, but not the absolute amount (for example, the columns activated by the 8-hr eye of an AME 8/1 are different from those activated by the 8-hr eye of an AME 8/8). Similarly, the binocular segment, where there was an imbalance and competition could occur, was affected, whereas the monocular segment, where there was no imbalance and competition could not occur, was not. Finally, the recent results of Reiter and Stryker suggest that monocular deprivation produces changes only when the activity of the presynaptic cell and the postsynaptic cell are correlated.(ABSTRACT TRUNCATED AT 400 WORDS)
总结(图10),单眼剥夺的结构后果包括以下变化:被剥夺的膝状体层双眼段中的中继细胞萎缩,且所含的可能神经递质N-乙酰天门冬氨酸较少。这些变化似乎继发于终末突触树突的丧失。当然,被剥夺的膝状体皮质细胞投射到视皮层IV层中较小的眼优势区,在那里它们形成的突触数量减少且异常。结果,它们激活的眼激活柱除了较小之外,还很微弱,通常无法延伸到颗粒外皮层。这种无法延伸到其他层的情况可能是由于IV层中被剥夺眼的细胞激活不足,无法与IV层中相邻的经验眼细胞成功竞争,导致从IV层到其他层的连接丧失(图11)。因此,单眼剥夺的主要影响可能是膝状体皮质突触的破坏,而其他变化,如细胞大小,以及可能的神经递质含量变化,则是继发的。被破坏的突触会导致皮质细胞驱动不足和眼激活柱微弱,进而会使在颗粒外皮层中获取细胞的二次竞争产生偏差。有一些一般原则将本章中的发现与本部分的其他发现统一起来。首先,观察到的形态学变化类型存在相似性,例如突触终末数量和大小的变化,以及线粒体变化。这意味着在发育和成年可塑性过程中存在类似变化,在脊椎动物和无脊椎动物中也存在类似变化。其次,决定这些变化的并非活动量,而是活动模式。在我的结果中,活动的相对不平衡很重要,但不是绝对量(例如,AME 8/1的8小时眼激活的柱与AME 8/8的8小时眼激活的柱不同)。同样,存在不平衡且可能发生竞争的双眼段受到影响,而不存在不平衡且不可能发生竞争的单眼段则未受影响。最后,赖特和斯特赖克最近的结果表明,单眼剥夺仅在突触前细胞和突触后细胞的活动相关时才会产生变化。(摘要截断于400字)
