Prediction of Response to Paclitaxel by <i>ChemoFx a</i>ssay Correlates with Estrogen Receptor Status and Changes in Apoptosis Pathway in Human Breast Cancers.

Wang, D.; Rice, Shara D.; Song, Nan; Gingrich, D; Shen, Kui; Hancher, L. M.

doi:10.1158/0008-5472.sabcs-09-2028

Cited by 2 publications

(13 citation statements)

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“…The PI model characterizes the net rates of growth and invasion of the glioma cells contributing to this overall profile, a sum of individual cell behaviors. Swanson et al have demonstrated that D and ρ can be calculated on a patient-specific basis and can vary widely, even for patients within the same histological grade (Harpold et al, 2007; Swanson et al, 2008a; Szeto et al, 2009b; Wang et al, 2009; Rockne et al, 2010). (B) A simulation of the reaction-diffusion mathematical model on an anatomically accurate brain phantom (Cocosco et al, 2004) with differential motility in gray and white matter as proposed by Swanson (1999).…”

Section: The Clinical Challenge Of Patient-specific Prognosis and Trementioning

confidence: 99%

“…The MRI-detectable edge of the lesion is superimposed as a dark gray contour emphasizing the extent of invasion well beyond the threshold of detection. From Wang et al (2009) with permission from Cancer Research.…”

Section: The Clinical Challenge Of Patient-specific Prognosis and Trementioning

confidence: 99%

“…The PI model can further incorporate differential motility of glioma cells through gray and white matter of the brain, providing predictions of diffuse tumor invasion through the regions of the brain that are specific to the patient’s tumor (Figure 2). This simple model has served as a foundation for patient-specific MNO and provided numerous insights into clinical behaviors such as survival outcome (Pallud et al, 2006; Swanson et al, 2008b; Wang et al, 2009; Rockne et al, 2010), hypoxia development (Szeto et al, 2009b), response to surgical resection (Swanson et al, 2008b), chemo- and radiation therapies (Rockne et al, 2010), biological aggressiveness (Szeto et al, 2009a; Ellingson et al, 2010b), and to date is the single most applied patient-specific clinical scale model for glioma growth and response to therapy. Extensions to this model include consideration of anisotropic growth in white matter tracts (Jbabdi et al, 2005).…”

Section: Individual Tumor Growth Kinetics: a Predictable Patternmentioning

confidence: 99%

“…The authors are only aware of work based on such an outline in the context of gliomas by the Swanson group (Swanson et al, 2002a, 2008b; Szeto et al, 2009b; Wang et al, 2009; Neal and Kerckhoffs, 2010; Rockne et al, 2010; Baldock et al, 2012a,b; Gu et al, 2012; Neal et al, 2012, 2013). But that is not to say that other efforts are not informative or useful.…”

Section: Individual Tumor Growth Kinetics: a Predictable Patternmentioning

confidence: 99%

“…In a study of 32 newly diagnosed glioblastoma patients, Wang et al (2009) used the PI model to find relationships between the Patient-specific model (PSM) parameters for glioma cell net dispersal ( D ), proliferation (ρ), and prognosis. As illustrated in Figure 1, patient-specific estimates D and ρ combine with the patient’s MRI to yield a map of the diffuse gradient of glioma cells that is expected to lie beyond thresholds visible to imaging (Figure 1).…”

Section: Individual Tumor Growth Kinetics: a Predictable Patternmentioning

confidence: 99%

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From Patient-Specific Mathematical Neuro-Oncology to Precision Medicine

Baldock¹,

Rockne²,

Boone³

et al. 2013

Front. Oncol.

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Gliomas are notoriously aggressive, malignant brain tumors that have variable response to treatment. These patients often have poor prognosis, informed primarily by histopathology. Mathematical neuro-oncology (MNO) is a young and burgeoning field that leverages mathematical models to predict and quantify response to therapies. These mathematical models can form the basis of modern “precision medicine” approaches to tailor therapy in a patient-specific manner. Patient-specific models (PSMs) can be used to overcome imaging limitations, improve prognostic predictions, stratify patients, and assess treatment response in silico. The information gleaned from such models can aid in the construction and efficacy of clinical trials and treatment protocols, accelerating the pace of clinical research in the war on cancer. This review focuses on the growing translation of PSM to clinical neuro-oncology. It will also provide a forward-looking view on a new era of patient-specific MNO.

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Section: The Clinical Challenge Of Patient-specific Prognosis and Trementioning

confidence: 99%

Section: The Clinical Challenge Of Patient-specific Prognosis and Trementioning

confidence: 99%

Section: Individual Tumor Growth Kinetics: a Predictable Patternmentioning

confidence: 99%

Section: Individual Tumor Growth Kinetics: a Predictable Patternmentioning

confidence: 99%

Section: Individual Tumor Growth Kinetics: a Predictable Patternmentioning

confidence: 99%

See 3 more Smart Citations

From Patient-Specific Mathematical Neuro-Oncology to Precision Medicine

Baldock¹,

Rockne²,

Boone³

et al. 2013

Front. Oncol.

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Modeling Tumor-Associated Edema in Gliomas during Anti-Angiogenic Therapy and Its Impact on Imageable Tumor

Hawkins-Daarud¹,

Rockne²,

Anderson³

et al. 2013

Front. Oncol.

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Glioblastoma, the most aggressive form of primary brain tumor, is predominantly assessed with gadolinium-enhanced T1-weighted (T1Gd) and T2-weighted magnetic resonance imaging (MRI). Pixel intensity enhancement on the T1Gd image is understood to correspond to the gadolinium contrast agent leaking from the tumor-induced neovasculature, while hyperintensity on the T2/FLAIR images corresponds with edema and infiltrated tumor cells. None of these modalities directly show tumor cells; rather, they capture abnormalities in the microenvironment caused by the presence of tumor cells. Thus, assessing disease response after treatments impacting the microenvironment remains challenging through the obscuring lens of MR imaging. Anti-angiogenic therapies have been used in the treatment of gliomas with spurious results ranging from no apparent response to significant imaging improvement with the potential for extremely diffuse patterns of tumor recurrence on imaging and autopsy. Anti-angiogenic treatment normalizes the vasculature, effectively decreasing vessel permeability and thus reducing tumor-induced edema, drastically altering T2-weighted MRI. We extend a previously developed mathematical model of glioma growth to explicitly incorporate edema formation allowing us to directly characterize and potentially predict the effects of anti-angiogenics on imageable tumor growth. A comparison of simulated glioma growth and imaging enhancement with and without bevacizumab supports the current understanding that anti-angiogenic treatment can serve as a surrogate for steroids and the clinically driven hypothesis that anti-angiogenic treatment may not have any significant effect on the growth dynamics of the overall tumor cell populations. However, the simulations do illustrate a potentially large impact on the level of edematous extracellular fluid, and thus on what would be imageable on T2/FLAIR MR. Additionally, by evaluating virtual tumors with varying growth kinetics, we see tumors with lower proliferation rates will have the most reduction in swelling from such treatments.

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Prediction of Response to Paclitaxel by ChemoFx assay Correlates with Estrogen Receptor Status and Changes in Apoptosis Pathway in Human Breast Cancers.

Cited by 2 publications

References 0 publications

From Patient-Specific Mathematical Neuro-Oncology to Precision Medicine

From Patient-Specific Mathematical Neuro-Oncology to Precision Medicine

Modeling Tumor-Associated Edema in Gliomas during Anti-Angiogenic Therapy and Its Impact on Imageable Tumor

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