Mouse models of advanced spontaneous metastasis for experimental therapeutics

Francia, Giulio; Cruz‐Muñoz, William; Man, Shan; Xu, Ping; Kerbel, Robert S.

doi:10.1038/nrc3001

Cited by 330 publications

(296 citation statements)

References 67 publications

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“…These features are not recapitulated by subcutaneously growing PDACs, which lack the abundant desmoplastic stroma and high interstitial pressure that limits blood vessel functionality in autochthonous (or orthotopic) tumors. Even orthotopic xenotransplant PDAC tumors growing in the pancreas are hypervascular in comparison to genetically engineered mouse models (GEMMs) and human PDACs (Olive et al., 2009); for other tumor types, however, orthotopic transplants may more accurately reflect the bona fide angiogenic and stromal components of the tumor microenvironment, and as such present an important experimental alternative to subcutaneous tumor xenografts (Francia et al., 2011). …”

Section: Variability and Dynamics Of Stromal Cell Componentsmentioning

confidence: 99%

“…Because metastatic disease represents the ultimate target of anticancer therapies, preclinical models that can recapitulate organ‐specific metastasis should be developed and employed to more realistically assay the therapeutic potential of candidate drugs. Orthotopic transplants (including PDX models) may enhance the incidence of distant metastatic spread compared with subcutaneous transplants (Derose et al., 2011), especially if the primary tumor is surgically removed to allow the development of macroscopic metastases from the disseminated tumor cells (Francia et al., 2011). Highly metastatic human tumor variants can also be generated through multiple rounds of in vivo growth of tumor cell lines in immunodeficient mice, each involving orthotopic tumor cell transplantation/growth/resection, and isolation of metastatic cells from the visceral organs (Francia et al., 2011; Kerbel et al., 1984).…”

Section: Harnessing Mouse Models Of Cancer To Investigate Individualimentioning

confidence: 99%

“…Orthotopic transplants (including PDX models) may enhance the incidence of distant metastatic spread compared with subcutaneous transplants (Derose et al., 2011), especially if the primary tumor is surgically removed to allow the development of macroscopic metastases from the disseminated tumor cells (Francia et al., 2011). Highly metastatic human tumor variants can also be generated through multiple rounds of in vivo growth of tumor cell lines in immunodeficient mice, each involving orthotopic tumor cell transplantation/growth/resection, and isolation of metastatic cells from the visceral organs (Francia et al., 2011; Kerbel et al., 1984). This approach has been used to select highly metastatic tumor cell lines that may be representative of various human cancer types/subtypes (Francia et al., 2011); in some cases, genetic modification of the tumor cells was used to introduce relevant driver oncogenic mutations in the tumor cells (du Manoir et al., 2006).…”

Section: Harnessing Mouse Models Of Cancer To Investigate Individualimentioning

confidence: 99%

“…Highly metastatic human tumor variants can also be generated through multiple rounds of in vivo growth of tumor cell lines in immunodeficient mice, each involving orthotopic tumor cell transplantation/growth/resection, and isolation of metastatic cells from the visceral organs (Francia et al., 2011; Kerbel et al., 1984). This approach has been used to select highly metastatic tumor cell lines that may be representative of various human cancer types/subtypes (Francia et al., 2011); in some cases, genetic modification of the tumor cells was used to introduce relevant driver oncogenic mutations in the tumor cells (du Manoir et al., 2006). However, this approach is not easily applicable to the derivation of patient‐specific tumor cell lines that can inform on treatment options for the individual, as the in vivo selection procedure is laborious and lengthy (Francia et al., 2011).…”

Section: Harnessing Mouse Models Of Cancer To Investigate Individualimentioning

confidence: 99%

“…This approach has been used to select highly metastatic tumor cell lines that may be representative of various human cancer types/subtypes (Francia et al., 2011); in some cases, genetic modification of the tumor cells was used to introduce relevant driver oncogenic mutations in the tumor cells (du Manoir et al., 2006). However, this approach is not easily applicable to the derivation of patient‐specific tumor cell lines that can inform on treatment options for the individual, as the in vivo selection procedure is laborious and lengthy (Francia et al., 2011). …”

Section: Harnessing Mouse Models Of Cancer To Investigate Individualimentioning

confidence: 99%

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The biology of personalized cancer medicine: Facing individual complexities underlying hallmark capabilities

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It is a time of great promise and expectation for the applications of knowledge about mechanisms of cancer toward more effective and enduring therapies for human disease. Conceptualizations such as the hallmarks of cancer are providing an organizing principle with which to distill and rationalize the abject complexities of cancer phenotypes and genotypes across the spectrum of the human disease. A countervailing reality, however, involves the variable and often transitory responses to most mechanism‐based targeted therapies, returning full circle to the complexity, arguing that the unique biology and genetics of a patient's tumor will in the future necessarily need to be incorporated into the decisions about optimal treatment strategies, the frontier of personalized cancer medicine. This perspective highlights considerations, metrics, and methods that may prove instrumental in charting the landscape of evaluating individual tumors so to better inform diagnosis, prognosis, and therapy. Integral to the consideration is remarkable heterogeneity and variability, evidently embedded in cancer cells, but likely also in the cell types composing the supportive and interactive stroma of the tumor microenvironment (e.g., leukocytes and fibroblasts), whose diversity in form, regulation, function, and abundance may prove to rival that of the cancer cells themselves. By comprehensively interrogating both parenchyma and stroma of patients' cancers with a suite of parametric tools, the promise of mechanism‐based therapy may truly be realized.

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Section: Variability and Dynamics Of Stromal Cell Componentsmentioning

confidence: 99%

Section: Harnessing Mouse Models Of Cancer To Investigate Individualimentioning

confidence: 99%

Section: Harnessing Mouse Models Of Cancer To Investigate Individualimentioning

confidence: 99%

Section: Harnessing Mouse Models Of Cancer To Investigate Individualimentioning

confidence: 99%

Section: Harnessing Mouse Models Of Cancer To Investigate Individualimentioning

confidence: 99%

See 3 more Smart Citations

The biology of personalized cancer medicine: Facing individual complexities underlying hallmark capabilities

2012

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Epithelial–mesenchymal transition in tumor metastasis

2016

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The Epithelial–Mesenchymal Transition (EMT) is a developmental program that enables stationery epithelial cells to gain the ability to migrate and invade as single cells. Tumor cells reactivate EMT to acquire molecular alterations that enable the partial loss of epithelial features and partial gain of a mesenchymal phenotype. Our understanding of the contribution EMT to tumor invasion, migration, and metastatic outgrowth has evolved over the past decade. In this review, we provide a summary of both historic and recent studies on the role of EMT in the metastatic cascade from various experimental systems, including cancer cell lines, genetic mouse tumor models, and clinical human breast cancer tissues.

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Cancer Models

2012

Cancer as a Metabolic Disease

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Mouse models of advanced spontaneous metastasis for experimental therapeutics

Cited by 330 publications

References 67 publications

The biology of personalized cancer medicine: Facing individual complexities underlying hallmark capabilities

The biology of personalized cancer medicine: Facing individual complexities underlying hallmark capabilities

Epithelial–mesenchymal transition in tumor metastasis

Cancer Models

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