A humanized orthotopic tumor microenvironment alters the bone metastatic tropism of prostate cancer cells

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作者
Jacqui A. McGovern
Nathalie Bock
Abbas Shafiee
Laure C. Martine
Ferdinand Wagner
Jeremy G. Baldwin
Marietta Landgraf
Christoph A. Lahr
Christoph Meinert
Elizabeth D. Williams
Pamela M. Pollock
Jim Denham
Pamela J. Russell
Gail P. Risbridger
Judith A. Clements
Daniela Loessner
Boris M. Holzapfel
Dietmar W. Hutmacher
机构
[1] Queensland University of Technology (QUT),Centre in Regenerative Medicine
[2] Centre for Biomedical Technologies,School of Mechanical, Medical and Process Engineering (MMPE)
[3] Faculty of Engineering,School of Biomedical Sciences at Translational Research Institute (TRI)
[4] QUT,Australian Prostate Cancer Research Centre—Queensland (APCRC
[5] Faculty of Health,Q)
[6] QUT,UQ Diamantina Institute, Translational Research Institute
[7] QUT,Herston Biofabrication Institute
[8] Queensland Bladder Cancer Initiative (QBCI),Musculoskeletal University Centre Munich, Department of Orthopedics and Trauma Surgery
[9] The University of Queensland,Department of Pediatric Surgery, Dr. von Hauner Children’s Hospital
[10] Metro North Hospital and Health Service,School of Medicine and Population Health
[11] University Hospital Munich,Department of Anatomy and Developmental Biology, Faculty of Medicine, Nursing and Health Sciences
[12] Ludwig-Maximilians University,Department of Chemical Engineering and Department of Materials Science and Engineering, Faculty of Engineering
[13] Campus Großhadern,ARC Industrial Transformation Training Centre in Additive Biomanufacturing
[14] Ludwig-Maximilians-University of Munich,undefined
[15] University of Newcastle,undefined
[16] Monash University,undefined
[17] Monash University,undefined
[18] QUT,undefined
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摘要
Prostate cancer (PCa) is the second most commonly diagnosed cancer in men, and bone is the most frequent site of metastasis. The tumor microenvironment (TME) impacts tumor growth and metastasis, yet the role of the TME in PCa metastasis to bone is not fully understood. We used a tissue-engineered xenograft approach in NOD-scid IL2Rγnull (NSG) mice to incorporate two levels of humanization; the primary tumor and TME, and the secondary metastatic bone organ. Bioluminescent imaging, histology, and immunohistochemistry were used to study metastasis of human PC-3 and LNCaP PCa cells from the prostate to tissue-engineered bone. Here we show pre-seeding scaffolds with human osteoblasts increases the human cellular and extracellular matrix content of bone constructs, compared to unseeded scaffolds. The humanized prostate TME showed a trend to decrease metastasis of PC-3 PCa cells to the tissue-engineered bone, but did not affect the metastatic potential of PCa cells to the endogenous murine bones or organs. On the other hand, the humanized TME enhanced LNCaP tumor growth and metastasis to humanized and murine bone. Together this demonstrates the importance of the TME in PCa bone tropism, although further investigations are needed to delineate specific roles of the TME components in this context.
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