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19号染色体三体小鼠神经节苷脂的发育概况

Developmental profiles of gangliosides in trisomy 19 mice.

作者信息

Lorke D E, Sonnentag U, Rösner H

机构信息

Department of Neuroanatomy, University of Hamburg, Federal Republic of Germany.

出版信息

Dev Biol. 1990 Nov;142(1):194-202. doi: 10.1016/0012-1606(90)90163-d.

Abstract

The ganglioside composition of the cerebrum, cerebellum, brainstem, liver, heart, and spleen was analyzed quantitatively in trisomy 19 (Ts19) mice aged 4 to 12 days postpartum. The developmental profiles of cerebral gangliosides were similar in Ts19 mice and control littermates: Total ganglioside-sialic acid as well as the proportions of the individual gangliosides GD1a and GM1 increased with age, while the percentages of GQ1b and GT1b decreased during development. Both the accretion of the total ganglioside content and the development of the individual ganglioside fractions were delayed by 2-3 days in the Ts19 telencephalon. Likewise, the shift from the b- to the a-pathway of ganglioside synthesis was retarded. Ganglioside development was equally delayed in the cerebellum and the brainstem of Ts19 mice. Since in Ts19 mice, morphogenesis of several brain regions is similarly delayed by 2 days, these results confirm the usefulness of gangliosides as biochemical markers for brain maturation. In contrast to brain gangliosides, the ganglioside composition of the Ts19 livers was clearly distinguished from that of control livers. Total ganglioside-bound sialic acid was increased by 35-50% in Ts19 livers. This elevation in ganglioside content not explicable by a simple delay in development was mainly due to an increase in GD3 and fraction 2, which is likely to contain GD1a and GD1b. In contrast, GM2 which increased considerably with age in control mice persisted on a low level in Ts19 livers. Comparable alterations of the ganglioside pattern were neither observed in the spleen nor in the heart of Ts19 mice. The data presented give additional evidence that ganglioside synthesis in the liver is under a different regulation mechanism than that in the brain, heart, and spleen.

摘要

对产后4至12天的19号染色体三体(Ts19)小鼠的大脑、小脑、脑干、肝脏、心脏和脾脏的神经节苷脂组成进行了定量分析。Ts19小鼠和对照同窝小鼠大脑神经节苷脂的发育情况相似:总神经节苷脂唾液酸以及各神经节苷脂GD1a和GM1的比例随年龄增加,而GQ1b和GT1b的百分比在发育过程中下降。Ts19端脑的总神经节苷脂含量增加和各神经节苷脂组分的发育均延迟了2至3天。同样,神经节苷脂合成从b途径向a途径的转变也受到阻碍。Ts19小鼠的小脑和脑干中神经节苷脂的发育同样延迟。由于在Ts19小鼠中,几个脑区的形态发生同样延迟了2天,这些结果证实了神经节苷脂作为脑成熟生化标志物的有用性。与脑内神经节苷脂不同,Ts19肝脏的神经节苷脂组成与对照肝脏明显不同。Ts19肝脏中与神经节苷脂结合的总唾液酸增加了35%至50%。这种神经节苷脂含量的升高不能简单地用发育延迟来解释,主要是由于GD3和组分2的增加,组分2可能含有GD1a和GD1b。相比之下,GM2在对照小鼠中随年龄显著增加,在Ts19肝脏中则维持在低水平。在Ts19小鼠的脾脏和心脏中未观察到类似的神经节苷脂模式改变。所呈现的数据进一步证明,肝脏中的神经节苷脂合成受不同于脑、心脏和脾脏的调节机制调控。

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