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Pax-3在节段性中胚层中的表达标志着生肌细胞特化的早期阶段。

Pax-3 expression in segmental mesoderm marks early stages in myogenic cell specification.

作者信息

Williams B A, Ordahl C P

机构信息

Department of Anatomy, University of California, San Francisco 94143-0452, USA.

出版信息

Development. 1994 Apr;120(4):785-96. doi: 10.1242/dev.120.4.785.

Abstract

Specification of the myogenic lineage begins prior to gastrulation and culminates in the emergence of determined myogenic precursor cells from the somites. The myoD family (MDF) of transcriptional activators controls late step(s) in myogenic specification that are closely followed by terminal muscle differentiation. Genes expressed in myogenic specification at stages earlier than MDFs are unknown. The Pax-3 gene is expressed in all the cells of the caudal segmental plate, the early mesoderm compartment that contains the precursors of skeletal muscle. As somites form from the segmental plate and mature, Pax-3 expression is progressively modulated. Beginning at the time of segmentation, Pax-3 becomes repressed in the ventral half of the somite, leaving Pax-3 expression only in the dermomyotome. Subsequently, differential modulation of Pax-3 expression levels delineates the medial and lateral halves of the dermomyotome, which contain precursors of axial (back) muscle and limb muscle, respectively. Pax-3 expression is then repressed as dermomyotome-derived cells activate MDFs. Quail-chick chimera and ablation experiments confirmed that the migratory precursors of limb muscle continue to express Pax-3 during migration. Since limb muscle precursors do not activate MDFs until 2 days after they leave the somite, Pax-3 represents the first molecular marker for this migratory cell population. A null mutation of the mouse Pax-3 gene, Splotch, produces major disruptions in early limb muscle development (Franz, T., Kothary, R., Surani, M. A. H., Halata, Z. and Grim, M. (1993) Anat. Embryol. 187, 153-160; Goulding, M., Lumsden, A. and Paquette, A. (1994) Development 120, 957-971). We conclude, therefore, that Pax-3 gene expression in the paraxial mesoderm marks earlier stages in myogenic specification than MDFs and plays a crucial role in the specification and/or migration of limb myogenic precursors.

摘要

肌源性谱系的特化在原肠胚形成之前就已开始,并最终导致从体节中出现已确定的肌源性前体细胞。转录激活因子的肌分化决定因子(MDF)家族控制着肌源性特化的后期步骤,随后紧接着是终末肌分化。在比MDFs更早阶段参与肌源性特化过程中表达的基因尚不清楚。Pax-3基因在尾侧节段板的所有细胞中表达,尾侧节段板是早期中胚层区域,包含骨骼肌的前体细胞。随着体节从节段板形成并成熟,Pax-3的表达逐渐受到调节。从分节时开始,Pax-3在体节的腹侧半部分受到抑制,仅在生皮节中保留Pax-3的表达。随后,Pax-3表达水平的差异调节划分出生皮节的内侧和外侧部分,它们分别包含轴(背)肌和肢体肌的前体细胞。随着生皮节来源的细胞激活MDFs,Pax-3的表达随后受到抑制。鹌鹑-鸡嵌合体和消融实验证实,肢体肌的迁移前体细胞在迁移过程中持续表达Pax-3。由于肢体肌前体细胞在离开体节后2天才激活MDFs,Pax-3代表了这一迁移细胞群体的首个分子标记。小鼠Pax-3基因的无效突变,即斑点(Splotch)突变,会在早期肢体肌发育过程中产生重大破坏(Franz, T., Kothary, R., Surani, M. A. H., Halata, Z.和Grim, M. (1993) Anat. Embryol. 187, 153 - 160;Goulding, M., Lumsden, A.和Paquette, A. (1994) Development 120, 957 - 971)。因此,我们得出结论,轴旁中胚层中Pax-3基因的表达标志着比MDFs更早的肌源性特化阶段,并且在肢体肌源性前体细胞的特化和/或迁移中起关键作用。

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