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着床前胚胎与畸胎瘤衍生细胞聚集过程中的细胞关系。

Cell relationships during aggregation between preimplantation embryos and teratocarcinoma-derived cells.

作者信息

Lehtonen E, Wartiovaara J, Reima I

出版信息

J Embryol Exp Morphol. 1984 Jun;81:17-35.

PMID:6470607
Abstract

Cleavage-stage mouse embryos aggregate and form chimaeric blastocysts with embryonal carcinoma (EC) cells. We used scanning and transmission electron microscopy to study cell relationships during aggregate formation between 8-cell-stage embryos and F9 EC cells. Relations between heterotypic cells were similarly studied in aggregation experiments with embryos and teratocarcinoma-derived visceral (PSA5-E) and parietal (PYS-2) endoderm cells and in experiments with EC cells and endoderm cells. The embryos and F9 cells always adhered to each other and rapidly formed compacted aggregates. Numerous microvilli and cell processes, originating from both embryo and EC cells, extended between the two cell types during adhesion and early phases of aggregation. The aggregation process involved spreading of the blastomeres on the EC cells. Frequent adherent junctions and close contacts, including possible focal gap or tight junctions were observed between the embryo and F9 cells after 3 h of culture. Apparent gap or tight junctions were infrequent during the early phases of aggregation but during further culture, extensive typical gap junctions were also seen between embryo and EC cells. The embryos adhered only irregularly and loosely to PSA5-E and PYS-2 cells; this interaction never led to aggregate formation comparable to that seen in the experiments with embryos and EC cells. Close contacts but no gap or tight junctions could be observed between the embryo and endoderm cells. On the other hand, both PSA5-E and PYS-2 cells readily adhered to and aggregated with EC cells. The present results suggest that microvilli and cell processes mediate membrane interactions during adhesion and early phases of aggregation between embryos and EC cells. During aggregation, blastomeres spread over the EC cells, and rapid formation of adherent junctions and close contacts, including possible focal gap or tight junctions is involved during the early phases of this process. After this initial phase, typical gap junctions are also seen between the embryo and EC cells. Interestingly, adhesive properties of embryo and EC cells differ: the former aggregate only with EC cells, whereas the latter do so also with teratocarcinoma-derived visceral and parietal endoderm cells. Mechanisms operating in the morphogenetic movement of cells in this experimental setup may be involved also in the development of the blastocyst in vivo.

摘要

卵裂期小鼠胚胎与胚胎癌细胞聚集并形成嵌合胚泡。我们利用扫描电子显微镜和透射电子显微镜研究了8细胞期胚胎与F9胚胎癌细胞在聚集形成过程中的细胞关系。在胚胎与畸胎癌衍生的内脏(PSA5-E)和壁层(PYS-2)内胚层细胞的聚集实验中,以及在胚胎癌细胞与内胚层细胞的实验中,对异型细胞之间的关系进行了类似的研究。胚胎和F9细胞总是相互粘附,并迅速形成紧密聚集物。在粘附和聚集早期,源自胚胎和胚胎癌细胞的大量微绒毛和细胞突起在两种细胞类型之间延伸。聚集过程涉及卵裂球在胚胎癌细胞上的铺展。培养3小时后,在胚胎和F9细胞之间观察到频繁的粘附连接和紧密接触,包括可能的局灶性间隙或紧密连接。在聚集早期,明显的间隙或紧密连接很少见,但在进一步培养过程中,胚胎和胚胎癌细胞之间也可见广泛的典型间隙连接。胚胎仅不规则且松散地粘附于PSA5-E和PYS-2细胞;这种相互作用从未导致形成与胚胎和胚胎癌细胞实验中所见相当的聚集物。在胚胎和内胚层细胞之间可观察到紧密接触,但无间隙或紧密连接。另一方面,PSA5-E和PYS-2细胞都很容易与胚胎癌细胞粘附并聚集。目前的结果表明,微绒毛和细胞突起在胚胎和胚胎癌细胞粘附及聚集早期介导膜相互作用。在聚集过程中,卵裂球铺展在胚胎癌细胞上,在此过程的早期阶段涉及粘附连接和紧密接触的快速形成,包括可能的局灶性间隙或紧密连接。在这个初始阶段之后,胚胎和胚胎癌细胞之间也可见典型的间隙连接。有趣的是,胚胎和胚胎癌细胞的粘附特性不同:前者仅与胚胎癌细胞聚集,而后者也与畸胎癌衍生的内脏和壁层内胚层细胞聚集。在这个实验装置中细胞形态发生运动中起作用的机制可能也参与了体内胚泡的发育。

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