Expression of Hoxa2 in cells entering chondrogenesis impairs overall cartilage development

Massip, Laurent; Ectors, Fabien; Deprez, Pierre Henri; Maleki, M; Behets, Catherine; Lengelé, Benoît; Delahaut, Philippe; Picard, Jacques; Rezsöhazy, René

doi:10.1111/j.1432-0436.2006.00132.x

Cited by 29 publications

(23 citation statements)

References 45 publications

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“…For instance, Hoxa2, which is overexpressed in BA1 cells of Ezh2 cko embryos, is a well-known inhibitor of intramembranous bone formation from BAs, and when overexpressed in the Hox-negative domain of avian embryos impairs formation of the facial skeleton (Couly et al, 1998;Creuzet et al, 2002;Kanzler et al, 1998). Massip and colleagues have shown that ectopic expression of Hoxa2 in chondrocytes results in impaired differentiation, as demonstrated by the lack of Col2a1, and prevents cartilage formation (Massip et al, 2007). In BA2, Hoxa2 is a promoter of the hyoid fate of mesenchymal CNCCs and restricts the chondrogenic domains that arise during endochondral ossification (Pasqualetti et al, 2000).…”

Section: Ezh2 Activity Silences Hox Gene Expression In Cnccsmentioning

confidence: 99%

Ezh2 is required for neural crest-derived cartilage and bone formation

et al. 2014

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The emergence of craniofacial skeletal elements, and of the jaw in particular, was a crucial step in the evolution of higher vertebrates. Most facial bones and cartilage are generated during embryonic development by cranial neural crest cells, while an osteochondrogenic fate is suppressed in more posterior neural crest cells. Key players in this process are Hox genes, which suppress osteochondrogenesis in posterior neural crest derivatives. How this specific pattern of osteochondrogenic competence is achieved remains to be elucidated. Here we demonstrate that Hox gene expression and osteochondrogenesis are controlled by epigenetic mechanisms. Ezh2, which is a component of polycomb repressive complex 2 (PRC2), catalyzes trimethylation of lysine 27 in histone 3 (H3K27me3), thereby functioning as transcriptional repressor of target genes. Conditional inactivation of Ezh2 does not interfere with localization of neural crest cells to their target structures, neural development, cell cycle progression or cell survival. However, loss of Ezh2 results in massive derepression of Hox genes in neural crest cells that are usually devoid of Hox gene expression. Accordingly, craniofacial bone and cartilage formation is fully prevented in Ezh2 conditional knockout mice. Our data indicate that craniofacial skeleton formation in higher vertebrates is crucially dependent on epigenetic regulation that keeps in check inhibitors of an osteochondrogenic differentiation program.

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Section: Ezh2 Activity Silences Hox Gene Expression In Cnccsmentioning

confidence: 99%

Ezh2 is required for neural crest-derived cartilage and bone formation

et al. 2014

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“…It is thought that HOX regulation of collagen subtypes imparts regional differences in the mechanical properties of tissues. Further, HOXA family genes have been implicated in the regulation of expression of key proteins involved in dynamic tissue and ECM remodeling, including the MMPs and TIMPs, which inhibit MMP activity [21][22][23][24]. Tissue remodeling is a continuous process, and a balance between matrix synthesis and breakdown is necessary to maintain the integrity of the genital tissue.…”

Section: Introductionmentioning

confidence: 99%

Knockdown of Hoxa11 In Vivo in the Uterosacral Ligament and Uterus of Mice Results in Altered Collagen and Matrix Metalloproteinase Activity1

Guess

Datar

et al. 2012

Biology of Reproduction

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Homeobox (HOX) genes are evolutionarily conserved genes encoding transcription factors that regulate mammalian embryonic growth and development of the urogenital tract. In both humans and mice, HOXA11 persists in the adult reproductive tract and is thought to play an important role in maintaining tissue developmental plasticity by regulating the expression of genes involved in extracellular matrix metabolism in the reproductive organs. Previously, we have shown that HOXA11 is necessary for development of the uterosacral ligaments in mice and is deficient in women with pelvic organ prolapse. Therefore, we hypothesized that Hoxa11 regulates the synthesis and/or metabolism of collagens in the uterosacral ligaments and uterus, and tested this by establishing an in utero and peritoneal Hoxa11 gene knockdown system in C57/BL6 mice using vectors bearing Hoxa11 short hairpin RNA. Specific knockdown of Hoxa11 transcripts and protein levels were confirmed versus control vectors. Protein and mRNA expression of collagen types I and III exhibited significant decreases following Hoxa11 knockdown according to Western blot analysis and real-time PCR. Tissue inhibitor of matrix metalloproteinase 1 (MMP1) expression also exhibited a significant decrease. Gelatinase zymography confirmed increases in pro-MMP2 and MMP9, as well as activated MMP2, following Hoxa11 knockdown. These results reveal that Hoxa11 knockdown in the uterosacral ligaments and uterus increases extracellular matrix degradation. More importantly, it suggests a mechanism in the weakening of the pelvic floor support in women, because decreased HOXA11 gene expression has been reported to be associated with decreased collagen and increased MMP2 expression in the uterosacral ligaments of women with pelvic organ prolapse.

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“…In 2007, Massip and colleagues generated a transgenic mouse model which induced Hoxa2 gene expression in a Cre-mediated way [3]. Crossing these mice with Col2a1-Cre transgenics [24] provoked an ectopic and persistent expression of Hoxa2 in every Col2a1 expressing cell, i.e.…”

Section: Resultsmentioning

confidence: 99%

“…This reduction impacted the endochondral ossification process, resulting in a postnatal growth defect mimicking human PSS [3,4]. Indeed, whereas the transgenic mice were similar in size to the control animals at birth, they featured a significant but harmonious shortening of both the trunk and the appendicular skeleton as early as the day four.…”

Section: Introductionmentioning

confidence: 99%

Molecular Study of a Hoxa2 Gain-of-Function in Chondrogenesis: A Model of Idiopathic Proportionate Short Stature

Deprez

Nichane

Lengelé

et al. 2013

IJMS

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In a previous study using transgenic mice ectopically expressing Hoxa2 during chondrogenesis, we associated the animal phenotype to human idiopathic proportionate short stature. Our analysis showed that this overall size reduction was correlated with a negative influence of Hoxa2 at the first step of endochondral ossification. However, the molecular pathways leading to such phenotype are still unknown. Using protein immunodetection and histological techniques comparing transgenic mice to controls, we show here that the persistent expression of Hoxa2 in chondrogenic territories provokes a general down-regulation of the main factors controlling the differentiation cascade, such as Bapx1, Bmp7, Bmpr1a, Ihh, Msx1, Pax9, Sox6, Sox9 and Wnt5a. These data confirm the impairment of chondrogenic differentiation by Hoxa2 overexpression. They also show a selective effect of Hoxa2 on endochondral ossification processes since Gdf5 and Gdf10, and Bmp4 or PthrP were up-regulated and unmodified, respectively. Since Hoxa2 deregulation in mice induces a proportionate short stature phenotype mimicking human idiopathic conditions, our results give an insight into understanding proportionate short stature pathogenesis by highlighting molecular factors whose combined deregulation may be involved in such a disease.

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Expression of Hoxa2 in cells entering chondrogenesis impairs overall cartilage development

Cited by 29 publications

References 45 publications

Ezh2 is required for neural crest-derived cartilage and bone formation

Ezh2 is required for neural crest-derived cartilage and bone formation

Knockdown of Hoxa11 In Vivo in the Uterosacral Ligament and Uterus of Mice Results in Altered Collagen and Matrix Metalloproteinase Activity1

Molecular Study of a Hoxa2 Gain-of-Function in Chondrogenesis: A Model of Idiopathic Proportionate Short Stature

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