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孤雌生殖细胞在胎鼠嵌合体中组织特异性增殖能力的丧失。

Tissue specific loss of proliferative capacity of parthenogenetic cells in fetal mouse chimeras.

作者信息

Bender R, Fundele R, Surani M A, Li L-L, Kothary R, Fürst D O, Christ B

机构信息

Institut für Biologie III der Universität Freiburg, Schänzlestrasse 1, D-79104, Freiburg, Germany.

Wellcome/CRC Institute of Cancer and Developmental Biology, Tennis Court Road, CB2 1QR, Cambridge.

出版信息

Rouxs Arch Dev Biol. 1995 Aug;204(7-8):436-443. doi: 10.1007/BF00360851.

DOI:10.1007/BF00360851
PMID:28305863
Abstract

Parthenogenetic cells are lost from fetal chimeras. This may be due to decreased proliferative potential. To address this question, we have made use of combined cell lineage and cell proliferation analysis. Thus, the incorporation of bromodeoxyuridine in S-phase was determined for both parthenogenetic and normal cells in several tissues of fetal day 13 and 17 chimeras. A pronounced reduction of bromodesoxyuridine incorporation by parthenogenetic cells at both developmental stages was only observed in cartilage. In brain, skeletal muscle, heart and intestinal epithelium, this reduction was either less pronounced or observed only at one of the developmental stages analysed. No difference between parthenogenetic and normal cells was observed in epidermis and ganglia. Our results show that a loss of proliferative potential of parthenogenetic cells during fetal development contributes to their rapid elimination in some tissues. The analysis of the fate of parthenogenetic cells in skeletal muscle and cartilage development demonstrated different selection mechanisms in these tissues. In skeletal muscle, parthenogenetic cells were largely excluded from the myogenic lineage proper by early post-midgestation. In primary hyaline cartilage, parthenogenetic cells persisted into adulthood but were lost from cartilages that undergo ossification during late fetal development.

摘要

孤雌生殖细胞会从胎儿嵌合体中消失。这可能是由于增殖潜能降低所致。为了解决这个问题,我们采用了细胞谱系和细胞增殖联合分析方法。因此,我们测定了胚胎第13天和17天嵌合体几个组织中孤雌生殖细胞和正常细胞在S期对溴脱氧尿苷的掺入情况。仅在软骨中观察到两个发育阶段的孤雌生殖细胞对溴脱氧尿苷的掺入明显减少。在脑、骨骼肌、心脏和肠上皮中,这种减少要么不太明显,要么仅在分析的其中一个发育阶段观察到。在表皮和神经节中,未观察到孤雌生殖细胞和正常细胞之间存在差异。我们的结果表明,胎儿发育过程中孤雌生殖细胞增殖潜能的丧失导致其在某些组织中迅速被清除。对骨骼肌和软骨发育过程中孤雌生殖细胞命运的分析表明,这些组织中存在不同的选择机制。在骨骼肌中,妊娠中期后早期,孤雌生殖细胞在很大程度上被排除在正常的肌源性谱系之外。在原发性透明软骨中,孤雌生殖细胞持续到成年期,但在胎儿发育后期发生骨化的软骨中消失。

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Tissue specific loss of proliferative capacity of parthenogenetic cells in fetal mouse chimeras.孤雌生殖细胞在胎鼠嵌合体中组织特异性增殖能力的丧失。
Rouxs Arch Dev Biol. 1995 Aug;204(7-8):436-443. doi: 10.1007/BF00360851.
2
Temporal and spatial selection against parthenogenetic cells during development of fetal chimeras.胎儿嵌合体发育过程中对孤雌生殖细胞的时空选择。
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Postnatal development of parthenogenetic in equilibrium with fertilized mouse aggregation chimeras.孤雌生殖与受精小鼠聚集嵌合体平衡状态下的产后发育。
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引用本文的文献

1
Proliferation and differentiation of androgenetic cells in fetal mouse chimeras.胎鼠嵌合体中孤雄生殖细胞的增殖与分化。
Rouxs Arch Dev Biol. 1995 Aug;204(7-8):494-501. doi: 10.1007/BF00360857.
2
Distribution of androgenetic cells in fetal mouse chimeras.雄激素生成细胞在胎鼠嵌合体中的分布。
Rouxs Arch Dev Biol. 1995 Aug;204(7-8):484-493. doi: 10.1007/BF00360856.
3
Brief report: Parthenogenetic embryonic stem cells are an effective cell source for therapeutic liver repopulation.简要报告:孤雌生殖胚胎干细胞是用于治疗性肝再植的有效细胞来源。

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Development. 1988 Sep;104(1):175-82. doi: 10.1242/dev.104.1.175.
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The developmental fate of androgenetic, parthenogenetic, and gynogenetic cells in chimeric gastrulating mouse embryos.
Genes Dev. 1988 Oct;2(10):1344-51. doi: 10.1101/gad.2.10.1344.
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Influence of chromosomal determinants on development of androgenetic and parthenogenetic cells.染色体决定因素对孤雄生殖细胞和孤雌生殖细胞发育的影响。
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