C. Scott Manatt scite author profile

Background: Tumor metastasis and changes in host immunosurveillance are important components in cancer development. Tumor cell invasion into the bloodstream is an essential step for systemic metastasis. Currently, the detection of tumor cells in the circulation is mainly dependent upon the utilization of known epithelial cell markers. However, expression of these molecules is not limited to cancer patients; healthy people also have a small number of epithelial cells in their circulation. Utilizing these markers to detect circulating tumor cells (CTCs) cannot adequately explain the mechanisms of tumor cell survival or their development of metastatic potential in peripheral blood. The immune system can also evolve along with the cancer, actually promoting or selecting the outgrowth of tumor variants. Unfortunately, both metastasis and immunosurveillance remain mysterious and are debatable because we have yet to define the molecules that participate in these processes. We are interested in identifying the existence of expressed genes, or mRNA species, that are specifically associated with circulating cells of cancerbearing patients using prostate cancer (PCa) as a model.

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Hydronephrosis in a Woman Undergoing In Vitro Fertilization

Califano

Confer

Galati

et al. 2007

Urology

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Contributors

Abbruzzese¹,

Abeloff²,

Abou‐Alfa³

et al. 2008

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601: Differential Utilization of Growth Factor and Androgen Receptor Pathways by 5 α -Androstane,3 α ,17 β -Diol and 5 α - Dihydrotestosterone in Human Prostate Cancer Lncap Cells

Burks¹,

Manatt²

2004

Journal of Urology

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C. Scott Manatt

Operative Versus Nonoperative Management of Ureteropelvic Junction Obstruction in Children

Screening and identification of differentially expressed transcripts in circulating cells of prostate cancer patients using suppression subtractive hybridization

Hydronephrosis in a Woman Undergoing In Vitro Fertilization

Contributors

601: Differential Utilization of Growth Factor and Androgen Receptor Pathways by 5 α -Androstane,3 α ,17 β -Diol and 5 α - Dihydrotestosterone in Human Prostate Cancer Lncap Cells

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