Increased expression of a set of genes enriched in oxygen binding function discloses a predisposition of breast cancer bone metastases to generate metastasis spread in multiple organs

Capulli, Mattia; Angelucci, Adriano; Driouch, Keltouma; García, Teresa; Clément-Lacroix, Philippe; Martella, Francesco; Ventura, Laura; Bologna, Mauro; Flamini, Stefano; Moreschini, O.; Lidereau, Rosette; Ricevuto, Enrico; Muraca, Maurizio; Teti, Anna; Rucci, Nadia

doi:10.1002/jbmr.1686

Cited by 25 publications

(24 citation statements)

References 36 publications

(38 reference statements)

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“…Likewise attempts to reconstruct cancer cell transcriptomes from unpurified CTCs by transcript subtraction need to be viewed with caution (38). Our findings are consistent with previous observations, such as a transcriptome study of 15 single prostate CTCs from one M1-stage patient revealing low-level expression of EPCAM, PTPRC (CD45), and CD34 (39), expression of hemoglobins in breast cancer epithelial cells (40,41) and ovarian cancer epithelial cells transdifferentiating into erythroid cells expressing hemoglobins (42). The observed expression of hematopoietic and erythroid transcripts by bone marrow-DCCs may reflect adaptation to the specific environment.…”

Section: Discussionsupporting

confidence: 90%

Combined Genome and Transcriptome Analysis of Single Disseminated Cancer Cells from Bone Marrow of Prostate Cancer Patients Reveals Unexpected Transcriptomes

et al. 2014

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Bone is the most frequent site of metastasis in prostate cancer and patients with bone metastases are deemed incurable. Targeting prostate cancer cells that disseminated to the bone marrow before surgery and before metastatic outgrowth may therefore prevent lethal metastasis. This prompted us to directly analyze the transcriptome of disseminated cancer cells (DCC) isolated from patients with nonmetastatic (UICC stage M0) prostate cancer. We screened 105 bone marrow samples of patients with M0-stage prostate cancer and 18 bone marrow samples of patients without malignancy for the presence of EpCAM þ single cells.

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Section: Discussionsupporting

confidence: 90%

Combined Genome and Transcriptome Analysis of Single Disseminated Cancer Cells from Bone Marrow of Prostate Cancer Patients Reveals Unexpected Transcriptomes

et al. 2014

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“…Our current analysis, based on the rate of progression of metastasis emphasizes growth properties of different metastatic clones [29]–[32]. However, differences in the ability to colonize the lung microenvironment following primary tumor resection may also account for observed differences between oligo- and poly- metastatic phenotypes [33].…”

Section: Discussionmentioning

confidence: 99%

Oligo- and Polymetastatic Progression in Lung Metastasis(es) Patients Is Associated with Specific MicroRNAs

et al. 2012

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RationaleStrategies to stage and treat cancer rely on a presumption of either localized or widespread metastatic disease. An intermediate state of metastasis termed oligometastasis(es) characterized by limited progression has been proposed. Oligometastases are amenable to treatment by surgical resection or radiotherapy.MethodsWe analyzed microRNA expression patterns from lung metastasis samples of patients with ≤5 initial metastases resected with curative intent.ResultsPatients were stratified into subgroups based on their rate of metastatic progression. We prioritized microRNAs between patients with the highest and lowest rates of recurrence. We designated these as high rate of progression (HRP) and low rate of progression (LRP); the latter group included patients with no recurrences. The prioritized microRNAs distinguished HRP from LRP and were associated with rate of metastatic progression and survival in an independent validation dataset.ConclusionOligo- and poly- metastasis are distinct entities at the clinical and molecular level.

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“…Such acidification might promote the pathogenic process in bone; however, the association between the ability to localize in the bone and the ability to secrete high levels of protons has never been evaluated. We compared the MDA cell line with the bmMDA clone, which is more prone to form BM when injected into the left ventricle of nude mice [ 16 ]. Compared with the parental MDA cells, the bmMDA cells showed higher mRNA (Figure 1A ) expression of key regulators of intracellular pH [ 12 , 17 ], such as carbonic anhydrase 9 (CA9; mRNA p = 0.0209) and monocarboxylate transporter 4 (MCT4; mRNA p =0.0209, protein p =0.0495), and glucose transporter 1 (GLUT-1; mRNA p =0.045), an indirect marker of glycolysis.…”

Section: Resultsmentioning

confidence: 99%

Intratumoral acidosis fosters cancer-induced bone pain through the activation of the mesenchymal tumor-associated stroma in bone metastasis from breast carcinoma

et al. 2017

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Cancer-induced bone pain (CIBP) is common in patients with bone metastases (BM), significantly impairing quality of life. The current treatments for CIBP are limited since they are often ineffective. Local acidosis derived from glycolytic carcinoma and tumor-induced osteolysis is only barely explored cause of pain. We found that breast carcinoma cells that prefer bone as a metastatic site have very high extracellular proton efflux and expression of pumps/ion transporters associated with acid-base balance (MCT4, CA9, and V-ATPase). Further, the impairment of intratumoral acidification via V-ATPase targeting in xenografts with BM significantly reduced CIBP, as measured by incapacitance test. We hypothesize that in addition to the direct acid-induced stimulation of nociceptors in the bone, a novel mechanism mediated by the acid-induced and tumor-associated mesenchymal stroma might ultimately lead to nociceptor sensitization and hyperalgesia. Consistent with this, short-term exposure of cancer-associated fibroblasts, mesenchymal stem cells, and osteoblasts to pH 6.8 promotes the expression of inflammatory and nociceptive mediators (NGF, BDNF, IL6, IL8, IL1b and CCL5). This is also consistent with a significant correlation between breakthrough pain, measured by pain questionnaire, and combined high serum levels of BDNF and IL6 in patients with BM, and also by immunofluorescence staining showing IL8 expression that was more in mesenchymal stromal cells rather than in tumors cells, and close to LAMP-2 positive acidifying carcinoma cells in BM tissue sections.In summary, intratumoral acidification in BM might promote CIBP also by activating the tumor-associated stroma, offering a new target for palliative treatments in advanced cancer.

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Increased expression of a set of genes enriched in oxygen binding function discloses a predisposition of breast cancer bone metastases to generate metastasis spread in multiple organs

Cited by 25 publications

References 36 publications

Combined Genome and Transcriptome Analysis of Single Disseminated Cancer Cells from Bone Marrow of Prostate Cancer Patients Reveals Unexpected Transcriptomes

Combined Genome and Transcriptome Analysis of Single Disseminated Cancer Cells from Bone Marrow of Prostate Cancer Patients Reveals Unexpected Transcriptomes

Oligo- and Polymetastatic Progression in Lung Metastasis(es) Patients Is Associated with Specific MicroRNAs

Intratumoral acidosis fosters cancer-induced bone pain through the activation of the mesenchymal tumor-associated stroma in bone metastasis from breast carcinoma

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