Increased breast tissue stiffness is correlated with breast cancer risk and invasive cancer progression. However, its role in promoting bone metastasis, a major cause of mortality, is not yet understood. It is previously identified that the composition and stiffness of alginate‐based hydrogels mimicking normal (1–2 kPa) and cancerous (6–10 kPa) breast tissue govern phenotype of breast cancer cells (including MDA‐MB‐231) in vitro. Here, to understand the causal effect of primary tumor stiffness on metastatic potential, a new breast‐to‐bone in vitro model is described. Together with alginate‐gelatin hydrogels to mimic breast tissue, 3D printed biohybrid poly‐caprolactone (PCL)‐composite scaffolds, decellularized following bone‐ECM deposition through Saos‐2 engraftment, are used to mimic the bone tissue. It is reported that higher hydrogel stiffness results in the increased migration and invasion capacity of MDA‐MB 231 cells. Interestingly, increased expression of osteolytic factors PTHrP and IL‐6 is observed when MDA‐MB‐231 cells pre‐conditioned in stiffer hydrogels (10 kPa, 3% w/v gelatin) colonize the bone/PCL scaffolds. The new breast‐to‐bone in vitro models herein described are designed with relevant tissue microenvironmental factors and could emerge as future non‐animal technological platforms for monitoring metastatic processes and therapeutic efficacy.
In the main article from pages 120 to 127 of volume 86, issue 1 (January 2017) of Clinical Endocrinology, 1 the correct phrases are written below:• On page 121, under the section Statistical Analyses, this should be "HDL cholesterol <1.3 mmol L −1 in women (n = 430) and HDL cholesterol <1.0 mmol L −1 in men (n = 239)."• On page 124, under the section Effect of exclusion of participants with high-risk baseline lipid values from longitudinal regression analyses, itshould read "(β = 0.04, SE = 0.02, P = 003) could be detected in women (data not shown)."
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