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Genesis and death of vocal control neurons during sexual differentiation in the zebra finch

机译:斑胸草雀的性别分化过程中发声控制神经元的发生与死亡

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摘要

Several song-related regions in the adult zebra finch brain have substantially more neurons in males than in females. Such differences appear to arise from sex differences in circulating steroids during early posthatch life. In the present study, developmental mechanisms involved in the production of sex differences are explored by examinations of the normal time course of posthatch neurogenesis and cell death in vocal control circuits. As a first step toward determining whether rates of neuron production may be different in males and females, tritiated thymidine, a marker of cell division, was administered to zebra finches at various times during the first month after hatching. Birds were sacrificed at 60 d. The number of cells formed after hatching and present at 60 d was then evaluated in 3 vocal control regions--HVc (hyperstriatum ventralis pars caudalis) and its 2 principal targets, RA (robust nucleus of the archistriatum) and Area X. Cell death was quantified by counts of normal and pyknotic, degenerating cells made in these nuclei in additional, untreated birds of both sexes at 5 d intervals from 5 to 45 d of age. The combined results of these experiments suggest that differential cell death is a major factor in the development of sex differences in the song control system and provide the first direct evidence for sex differences in cell death in the developing telencephalon. Although developmental time tables differ among the 3 brain areas examined, at specific ages significantly higher numbers of pyknotic cells were observed in HVc, RA, and presumptive Area X in females compared to males. Peak levels of cell death in RA occur 4–6 weeks after hatching. This is about 3 weeks after the onset of sex differences in steroid levels that, in turn, lead to differential organization of song system nuclei. This pattern of results suggests that designation for death and actual cell loss are temporally dissociated in this system. Neuron proliferation for HVc and Area X, but not RA, continues throughout the first 30 d after hatching, and a significant sex difference was found in the number of cells present in HVc at 60 d that were formed after hatching. Comparisons of the timing of cell death and cell incorporation suggest that this difference may be best accounted for by differential survival of neurons formed after hatching rather than differential rates of neuron production. Neither differential neurogenesis nor differential neuron death can fully account for the apparent extreme sexual dimorphism in the number of neurons in Area X.(ABSTRACT TRUNCATED AT 400 WORDS)
机译:在成年斑马雀科大脑中,与歌曲相关的几个区域中,男性的神经元明显多于女性。这种差异似乎是由于孵化后早期生命周期中类固醇的性别差异引起的。在本研究中,通过检查声带控制回路中孵化后神经发生和细胞死亡的正常时间进程,探索了引起性别差异的发育机制。作为确定男性和女性神经元产生速率是否可能不同的第一步,在孵化后的第一个月内,在不同时间对斑纹雀进行了tri化胸腺嘧啶核苷的标记。在第60天处死鸟类。孵化后形成并在60 d出现的细胞数量随后在3个声带控制区域-HVc(腹侧hypertritriatum pars caudalis)及其2个主要靶标RA(弓形虫的健壮核)和X区进行了评估。通过正常和隐秘的数量对这些细胞核中退化的细胞进行定量,这些细胞是在5到45 d年龄间隔的5 d间隔内未处理的其他两性鸟类中。这些实验的综合结果表明,差异性细胞死亡是歌曲控制系统中性别差异发展的主要因素,并且为发育中的端脑中细胞死亡的性别差异提供了第一个直接证据。尽管在三个大脑区域中发育时间表有所不同,但在特定年龄段,与男性相比,女性的HVc,RA和X推测区域X的泌尿生殖细胞数量明显增多。孵化后4-6周,RA中细胞死亡的峰值水平出现。这是类固醇水平发生性别差异后大约3周,进而导致歌曲系统核的差异组织。这种结果模式表明,死亡和实际细胞丢失的指定在该系统中暂时不相关。孵化后的前30 d,HVc和X区(而非RA)的神经元增殖持续,并且在孵化后60 d HVc中存在的细胞数量存在明显的性别差异。细胞死亡时间和细胞掺入时间的比较表明,这种差异可能是由孵化后形成的神经元的差异存活而不是神经元产生的差异速率来最好地解释的。差异性神经发生和差异性神经元死亡都不能完全解释X区神经元数量的明显极端性二态性(摘要截断为400字)

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