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通过药理学抑制血清素信号传导破坏不对称分裂过程中的纺锤体定向和蛋白质定位。

Disruption of spindle orientation and protein localization during asymmetric cleavage by pharmacological inhibition of serotonin signaling.

作者信息

Nakamoto Ayaki, Nagy Lisa M

机构信息

Faculty of Pharmaceutical Sciences, Aomori University, Koubata 2-3-1, Aomori, 030-0943, Japan.

Department of Molecular and Cellular Biology, University of Arizona, Tucson, AZ, 85721, USA.

出版信息

Dev Biol. 2025 Jun 29;526:26-37. doi: 10.1016/j.ydbio.2025.06.025.

DOI:10.1016/j.ydbio.2025.06.025
PMID:40592399
Abstract

Cell polarity directs the orientation and size of asymmetric cell division and the segregation of cell fate determinants, processes fundamental to development in all multicellular organisms. During asymmetric cleavage, the mitotic spindle aligns with a specified polarity of the mother cell, and cell fate determinants are distributed asymmetrically along the division axis. Here, we report that pharmacological inhibition of serotonin signaling during the 4-to-8-cell division in early embryos of the mud snail Ilyanassa obsoleta (currently known as Tritia obsoleta) disrupts the typical unequal division pattern. The oblique axis of division common to spirally cleaving molluscan embryos is altered, and the position of the mitotic spindle is randomized in these treatments. Mother cells generate abnormally large, atypically positioned daughter cells. We also find that, in normal embryos, proteins recognized by phosphorylated PKC and Bazooka/PAR-3 antibodies typically co-localize with the spindle apparatus to the apical cortex of each mother cell. These antigens subsequently segregate to the smaller of the two daughter cells. In embryos treated with the serotonin-receptor antagonist, the localization of these asymmetrically segregating proteins is randomized, and their localization is independent of spindle position. These results suggest that serotonin signaling coordinates spindle orientation, cortical polarity, and cell size in early asymmetric cleavages.

摘要

细胞极性指导不对称细胞分裂的方向和大小以及细胞命运决定因子的分离,这些过程是所有多细胞生物发育的基础。在不对称分裂过程中,有丝分裂纺锤体与母细胞特定的极性对齐,细胞命运决定因子沿分裂轴不对称分布。在这里,我们报告称,在泥螺(Ilyanassa obsoleta,现称为Tritia obsoleta)早期胚胎的4细胞至8细胞分裂过程中,对血清素信号传导进行药理学抑制会破坏典型的不均等分裂模式。螺旋卵裂的软体动物胚胎常见的倾斜分裂轴发生改变,在这些处理中,有丝分裂纺锤体的位置随机化。母细胞产生异常大、位置异常的子细胞。我们还发现,在正常胚胎中,被磷酸化PKC和巴祖卡蛋白/ PAR - 3抗体识别的蛋白质通常与纺锤体装置共定位于每个母细胞的顶端皮质。这些抗原随后分离到两个子细胞中较小的那个。在用血清素受体拮抗剂处理的胚胎中,这些不对称分离蛋白质的定位随机化,并且它们的定位与纺锤体位置无关。这些结果表明,血清素信号传导在早期不对称分裂中协调纺锤体方向、皮质极性和细胞大小。

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