AI Article Synopsis
- Microarray analysis showed that genes from the posterior HOXD locus, which play a role in bone formation, are over-expressed in Ewing sarcoma (ES), independent of specific genetic translocations.
- Knocking down the DKK2 inhibitor suppressed the expression of certain HOXD genes, while increasing DKK2 or WNT signaling factors boosted their expression and led to enhanced bone-related gene activity.
- HOXD11 and HOXD13 not only promoted growth and invasiveness in ES but also were linked to increased metastasis, as shown in experiments with immune-deficient mice.
Article Abstract
Microarray analysis revealed genes of the posterior HOXD locus normally involved in bone formation to be over-expressed in primary Ewing sarcoma (ES). The expression of posterior HOXD genes was not influenced via ES pathognomonic EWS/ETS translocations. However, knock down of the dickkopf WNT signaling pathway inhibitor 2 (DKK2) resulted in a significant suppression of HOXD10, HOXD11 and HOXD13 while over-expression of DKK2 and stimulation with factors of the WNT signaling pathway such as WNT3a, WNT5a or WNT11 increased their expression. RNA interference demonstrated that individual HOXD genes promoted chondrogenic differentiation potential, and enhanced expression of the bone-associated gene RUNX2. Furthermore, HOXD genes increased the level of the osteoblast- and osteoclast-specific genes, osteocalcin (BGLAP) and platelet-derived growth factor beta polypeptide (PDGFB), and may further regulate endochondral bone development via induction of parathyroid hormone-like hormone (PTHLH). Additionally, HOXD11 and HOXD13 promoted contact independent growth of ES, while in vitro invasiveness of ES lines was enhanced by all 3 HOXD genes investigated and seemed mediated via matrix metallopeptidase 1 (MMP1). Consequently, knock down of HOXD11 or HOXD13 significantly suppressed lung metastasis in a xeno-transplant model in immune deficient mice, providing overall evidence that posterior HOXD genes promote clonogenicity and metastatic potential of ES.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5173095 | PMC |
| http://dx.doi.org/10.18632/oncotarget.9702 | DOI Listing |
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