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Merck
CN
  • CSF1 receptor targeting in prostate cancer reverses macrophage-mediated resistance to androgen blockade therapy.

CSF1 receptor targeting in prostate cancer reverses macrophage-mediated resistance to androgen blockade therapy.

Cancer research (2015-03-05)
Jemima Escamilla, Shiruyeh Schokrpur, Connie Liu, Saul J Priceman, Diana Moughon, Ziyue Jiang, Frederic Pouliot, Clara Magyar, James L Sung, Jingying Xu, Gang Deng, Brian L West, Gideon Bollag, Yves Fradet, Louis Lacombe, Michael E Jung, Jiaoti Huang, Lily Wu
摘要

Growing evidence suggests that tumor-associated macrophages (TAM) promote cancer progression and therapeutic resistance by enhancing angiogenesis, matrix-remodeling, and immunosuppression. In this study, prostate cancer under androgen blockade therapy (ABT) was investigated, demonstrating that TAMs contribute to prostate cancer disease recurrence through paracrine signaling processes. ABT induced the tumor cells to express macrophage colony-stimulating factor 1 (M-CSF1 or CSF1) and other cytokines that recruit and modulate macrophages, causing a significant increase in TAM infiltration. Inhibitors of CSF1 signaling through its receptor, CSF1R, were tested in combination with ABT, demonstrating that blockade of TAM influx in this setting disrupts tumor promotion and sustains a more durable therapeutic response compared with ABT alone.

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Sigma-Aldrich
苯均三酸, 95%
Sigma-Aldrich
苯均三酸, Vetec, reagent grade, 94%