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Journal ArticleDOI

Regulation of anterior/posterior patterning of the axial skeleton by growth/differentiation factor 11

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TLDR
It is suggested that Gdf11 is a secreted signal that acts globally to specify positional identity along the anterior/posterior axis.
Abstract
The bones that comprise the axial skeleton have distinct morphological features characteristic of their positions along the anterior/posterior axis. We previously described a novel TGF-β family member, myostatin (encoded by the gene Mstn, formerly Gdf8), that has an essential role in regulating skeletal muscle mass1. We also identified a gene related to Mstn by low-stringency screening1. While the work described here was being completed, the cloning of this gene, designated Gdf11 (also called Bmp11), was also reported by other groups2,3. Here we show that Gdf11, a new transforming growth factor β (TGFβ) superfamily member, has an important role in establishing this skeletal pattern. During early mouse embryogenesis, Gdf11 is expressed in the primitive streak and tail bud regions, which are sites where new mesodermal cells are generated. Homozygous mutant mice carrying a targeted deletion of Gdf11 exhibit anteriorly directed homeotic transformations throughout the axial skeleton and posterior displacement of the hindlimbs. The effect of the mutation is dose dependent, as Gdf11+/– mice have a milder phenotype than Gdf11–/– mice. Mutant embryos show alterations in patterns of Hox gene expression, suggesting that Gdf11 acts upstream of the Hox genes. Our findings suggest that Gdf11 is a secreted signal that acts globally to specify positional identity along the anterior/posterior axis.

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Citations
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Regulation of myostatin activity and muscle growth

TL;DR: The findings suggest that the propeptide, follistatin, or other molecules that block signaling through this pathway may be useful agents for enhancing muscle growth for both human therapeutic and agricultural applications.
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Regulation of muscle mass by myostatin

TL;DR: The existence of circulating tissue-specific growth inhibitors of this type was hypothesized over 40 years ago to explain how sizes of individual tissues are controlled and skeletal muscle appears to be the first example of a tissue whose size is controlled by this type of regulatory mechanism.
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Bone Morphogenetic Protein (BMP) signaling in development and human diseases.

TL;DR: This review focuses on genetically manipulated mouse knockout models that have helped elucidate the role of BMPs in development and a significant portion of this review is devoted to the prominent human pathologies associated with dysregulated BMP signaling
Journal ArticleDOI

Genetic analysis of the mammalian transforming growth factor-beta superfamily.

TL;DR: This review attempts to collate and integrate the extensive body of in vivo mammalian studies produced over the last decade that revealed that TGF-β superfamily ligands, receptors, SMADs, and upstream and downstream regulators function in diverse developmental and physiological pathways.
References
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Journal ArticleDOI

Regulation of skeletal muscle mass in mice by a new TGF-beta superfamily member.

TL;DR: Results suggest that GDF-8 functions specifically as a negative regulator of skeletal muscle growth, which is significantly larger than wild-type animals and show a large and widespread increase in skeletal muscle mass.
Book

PCR 2 : a practical approach

TL;DR: Optimizing PCR Use of specialty phosphoramidites in PCR Chemical methods for 5' non-isotopic labelling of PCR probes and primers and Linear amplification for the in vitro study of ligand/DNA interactions Ligand-mediated PCR.
Journal ArticleDOI

A single protocol to detect transcripts of various types and expression levels in neural tissue and cultured cells: in situ hybridization using digoxigenin-labelled cRNA probes.

TL;DR: A simple non-radioactive in situ hybridization procedure for tissue sections and cultured cells using digoxigenin-labelled cRNA probes for the detection of various transcripts present at a wide range of expression levels in the central nervous system is developed.
Journal ArticleDOI

Expression of the proto-oncogene int-1 is restricted to specific neural cells in the developing mouse embryo.

TL;DR: The spatial distribution of expression of the mammary tumor proto-oncogene int-1 during mouse embryogenesis and the role it plays in the early stages of central nervous system development in the mouse embryo are studied.
Journal ArticleDOI

The signaling pathway mediated by the type IIB activin receptor controls axial patterning and lateral asymmetry in the mouse.

TL;DR: It is shown that the ActRIIB-/- mice die after birth with complicated cardiac defects including randomized heart position, malposition of the great arteries, and ventricular and atrial septal defects, recapitulating the clinical symptoms of the human asplenia syndrome.
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