Osteo-chondroprogenitor cells are derived from Sox9 expressing precursors

Akiyama, Haruhiko; Kim, Jung Eun; Nakashima, Kazuhisa; Balmes, Gener; Iwai, Naoharu; Deng, Jian Min; Zhang, Zhaoping; Martin, James F.; Behringer, Richard R.; Nakamura, Takashi; Crombrugghe, Benoít de

doi:10.1073/pnas.0504750102

Cited by 519 publications

(502 citation statements)

References 27 publications

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“…This role is similar to its function in the hair bulge, intestinal epithelium, and neural crest (Cheung and Briscoe, 2003;Blache et al, 2004;Vidal et al, 2005). Sox9 expression is first detected at $E10.5 in the early pancreatic MPC, and lineage tracing revealed that the ''first-wave'' Sox9 þ progenitors, like Pdx1 þ and Ptf1a þ progenitors, produce cells of all three pancreatic lineages (Akiyama et al, 2005). Sox9 expression persists in the endocrine/duct bipotent progenitor pool located in the central epithelial cords of the maturing epithelial arbor during the secondary transition (Seymour et al, 2007;Lynn et al, 2007).…”

Section: Sox9mentioning

confidence: 74%

Pancreas organogenesis: From bud to plexus to gland

Pan

Wright

2011

Developmental Dynamics

525

594

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Pancreas oganogenesis comprises a coordinated and highly complex interplay of signaling events and transcriptional networks that guide a step-wise process of organ development from early bud specification all the way to the final mature organ state. Extensive research on pancreas development over the last few years, largely driven by a translational potential for pancreatic diseases (diabetes, pancreatic cancer, and so on), is markedly advancing our knowledge of these processes. It is a tenable goal that we will one day have a clear, complete picture of the transcriptional and signaling codes that control the entire organogenetic process, allowing us to apply this knowledge in a therapeutic context, by generating replacement cells in vitro, or perhaps one day to the whole organ in vivo. This review summarizes findings in the past 5 years that we feel are amongst the most significant in contributing to the deeper understanding of pancreas development. Rather than try to cover all aspects comprehensively, we have chosen to highlight interesting new concepts, and to discuss provocatively some of the more controversial findings or proposals. At the end of the review, we include a perspective section on how the whole pancreas differentiation process might be able to be unwound in a regulated fashion, or redirected, and suggest linkages to the possible reprogramming of other pancreatic cell-types in vivo, and to the optimization of the forward-directed-differentiation of human embryonic stem cells (hESC), or induced pluripotential cells (iPSC), towards mature b-cells. Developmental Dynamics 240:530-565,

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Section: Sox9mentioning

confidence: 74%

Pancreas organogenesis: From bud to plexus to gland

Pan

Wright

2011

Developmental Dynamics

525

594

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“…In the skeleton, SOX9 expression precedes RUNX2, and subsequently, SOX9 expression is maintained during the whole process of bone formation, from chondrocytes to osteoblasts. (47) The coordination between SOX9 and RUNX2 is highly important for the determination of MSC fate. It has been shown previously that SOX9 is able to exert a dominant inhibitory effect on RUNX2 function (32) ; however, the precise mechanisms involved are unclear.…”

Section: Discussionmentioning

confidence: 99%

SOX9 determines RUNX2 transactivity by directing intracellular degradation

Cheng

Genever

2010

Journal of Bone and Mineral Research

133

112

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Mesenchymal stem cell differentiation is controlled by the cooperative activity of a network of signaling mechanisms. Among these, RUNX2 and SOX9 are the major transcription factors for osteogenesis and chondrogenesis, respectively. Their expression is overlapped both temporally and spatially during embryogenesis. Here we have demonstrated that RUNX2 and SOX9 physically interact in intact cells and have confirmed that SOX9 can inhibit the transactivation of RUNX2. In addition, RUNX2 exerts reciprocal inhibition on SOX9 transactivity. In analyses of the mechanism by which SOX9 regulated RUNX2 function, we demonstrated that SOX9 induced a dosedependent degradation of RUNX2. Although RUNX2 is normally degraded by the ubiquitin-proteasome pathway, we found that SOX9-mediated degradation was proteasome-independent but phosphorylation-dependent and required the presence of the RUNX2 Cterminal domain, which contains a nuclear matrix targeting sequence (NMTS). Furthermore, SOX9 was able to decrease the level of ubiquitinated RUNX2 and direct RUNX2 to the lysosome for degradation. SOX9 also preferentially directed b-catenin, an intracellular mediator of canonical Wnt signaling, for lysosomal breakdown. Consequently, the mechanisms by which SOX9 regulates RUNX2 function may underlie broader signaling pathways that can influence osteochondrogenesis and mesenchymal fate. ß

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“…This process requires the initial specification of precartilaginous cells (chondroprogenitors), which are not yet fully committed toward the cartilage lineage, and the following determination of a subset of these cells to form the definite cartilaginous condensation (Akiyama et al, 2005). The limb mesenchyme appears to have an intrinsic chondrogenic potential as a default fate, as can be seen in mesenchymal micromass cultures (see e.g., DeLise et al, 2000).…”

Section: Condensation Of the Digit Anlagenmentioning

confidence: 99%

“…Sox9 directly regulates the expression of Col2a1 (Lefebvre et al, 1997;Ng et al, 1997). However, the expression of Sox9 alone is not sufficient for definitive determination of the chondrogenic cell fate, because cells expressing Sox9 in vivo can still adopt other cell fates (Akiyama et al, 2005). Heterozygous mutations in SOX9 cause campomelic dysplasia, a generalized lethal chondrodysplasia with sex reversal (Wagner et al, 1994).…”

Section: Condensation Of the Digit Anlagenmentioning

confidence: 99%

Mechanisms of digit formation: Human malformation syndromes tell the story

Stricker

Mundlos

2011

Developmental Dynamics

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Identifying the genetic basis of human limb malformation disorders has been instrumental in improving our understanding of limb development. Abnormalities of the hands and/or feet include defects affecting patterning, establishment, elongation, and segmentation of cartilaginous condensations, as well as growth of the individual skeletal elements. While the phenotype of such malformations is highly diverse, the mutations identified to date cluster in genes implicated in a limited number of molecular pathways, namely hedgehog, Wnt, and bone morphogenetic protein. The latter pathway appears to function as a key molecular network regulating different phases of digit and joint development. Studies in animal models not only extended our insight into the pathogenesis of these conditions, but have also contributed to our understanding of the in vivo functions and interactions of these key players. This review is aimed at integrating the current understanding of human digit malformations into the increasing knowledge of the molecular mechanisms of digit development. Developmental Dynamics 240:990-1004,

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Osteo-chondroprogenitor cells are derived from Sox9 expressing precursors

Cited by 519 publications

References 27 publications

Pancreas organogenesis: From bud to plexus to gland

Pancreas organogenesis: From bud to plexus to gland

SOX9 determines RUNX2 transactivity by directing intracellular degradation

Mechanisms of digit formation: Human malformation syndromes tell the story

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