Transcriptomic and proteomic analyses in bone tumor cells: Deciphering parathyroid hormone-related protein regulation of the cell cycle and apoptosis

abstract

Abstract Giant cell tumor of bone (GCT) is an aggressive skeletal tumor characterized by local bone destruction, high recurrence rates, and metastatic potential. Previous works in our laboratory, including functional assays, have shown that neutralization of parathyroid hormone-related protein (PTHrP) in the cell environment inhibits cell proliferation and induces cell death in GCT stromal cells, indicating a role for PTHrP in cell propagation and survival. The objective of this study was to investigate the global gene and protein expression patterns of GCT cells in order to identify the underlying pathways and mechanisms of neoplastic proliferation provided by PTHrP in the bone microenvironment. Primary stromal cell cultures from 10 patients with GCT were used in this study. Cells were exposed to optimized concentrations of either PTHrP peptide or anti-PTHrP neutralizing antiserum and were analyzed with both cDNA microarray and proteomic microarray assays in triplicate. Hierarchical clustering and principal component analyses confirmed that counteraction of PTHrP in GCT stromal cells results in a clear-cut gene expression pattern distinct from all other treatment groups and the control cell line human fetal osteoblast (hFOB). Multiple bioinformatics tools were used to analyze changes in gene/protein expression and identify important gene ontologies and pathways common to this anti-PTHrP–induced regulatory gene network. PTHrP neutralization interferes with multiple cell survival and apoptosis signaling pathways by triggering both death receptors and cell cycle–mediated apoptosis, particularly via the caspase pathway, TRAIL pathway, JAK-STAT signaling pathway, and cyclin E/CDK2-associated G1/S cell cycle progression. These findings indicate that PTHrP neutralization exhibits anticancer potential by regulating cell-cycle progression and apoptosis in bone tumor cells, with the corollary being that PTHrP is a pro-neoplastic factor that can be targeted in the treatment of bone tumors. © 2012 American Society for Bone and Mineral Research.

authors

Mak, Isabella WY
Turcotte, Robert E
Ghert, Michelle

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published

publication date

September 1, 2012

has subject area

06 Biological Sciences (FoR)
09 Engineering (FoR)
11 Medical and Health Sciences (FoR)
Anatomy & Morphology (Science Metrix)
Apoptosis (MeSH)
Bone Neoplasms (MeSH)
Cell Cycle (MeSH)
Cluster Analysis (MeSH)
Databases, Genetic (MeSH)
Gene Expression Profiling (MeSH)
Gene Expression Regulation, Neoplastic (MeSH)
Genes, Neoplasm (MeSH)
Humans (MeSH)
Oligonucleotide Array Sequence Analysis (MeSH)
Parathyroid Hormone-Related Protein (MeSH)
Principal Component Analysis (MeSH)
Protein Array Analysis (MeSH)
Proteomics (MeSH)
Real-Time Polymerase Chain Reaction (MeSH)
Reproducibility of Results (MeSH)
Signal Transduction (MeSH)

published in

Journal of Bone and Mineral Research Journal

Transcriptomic and proteomic analyses in bone tumor cells: Deciphering parathyroid hormone-related protein regulation of the cell cycle and apoptosis Journal Articles

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