Determining Prostate Cancer-Specific Death through Quantification of Stromogenic Carcinoma Area in Prostatectomy Specimens

Ayala, Gustavo; Müezzínoğlu, Bahar; Hammerich, Kai; Frolov, Anna; Líu, Hao; Scardino, Peter T.; Li, Rile; Sayeeduddin, Mohammad; Ittmann, Michael; Kadmon, Dov; Miles, Brian J.; Wheeler, Thomas M.; Rowley, David R.

doi:10.1016/j.ajpath.2010.09.042

Cited by 58 publications

(53 citation statements)

References 46 publications

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“…Both invasive and microinvasive mPCa is usually associated with reactive stroma changes, whereas human PCa typically elicits very little stromal reaction, at least when evaluated by histology alone[10]. It should be noted, however, that when reactive stroma is observed in human PCa patients by additional immunohistochemistry (IHC), it correlates with poor prognosis[31,32], and stroma derived from PCa patients (Carcinoma Associated Fibroblasts, CAF, [33]), can transform non-tumorigenic immortalized epithelial cell lines, clearly suggesting an important role for the stroma in human PCa. For a comparison of human and mouse PCa progression, see Figure 1.…”

Section: Human Versus Mousementioning

confidence: 99%

Mouse models of prostate cancer: picking the best model for the question

Grabowska

DeGraff

et al. 2014

Cancer Metastasis Rev

108

102

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When the NIH Mouse Models of Human Cancer Consortium (MMCC) initiated the Prostate Steering Committee 15 years ago, there were no genetically engineered mouse (GEM) models of prostate cancer (PCa). Today, a PubMed search for “prostate cancer mouse model” yields 3,200 publications and this list continues to grow. The first generation of GEM utilized the newly discovered and characterized probasin (PB) promoter driving viral oncogenes such as SV40 large T antigen to yield the LADY and TRAMP models. As the PCa research field has matured, the second generation of models has incorporated the single and multiple molecular changes observed in human disease, such as loss of PTEN and over-expression of Myc. Application of these models has revealed that mice are particularly resistant to developing invasive PCa, and once they achieve invasive disease, the PCa rarely resembles human disease. Nevertheless, these models and their application have provided vital information on human PCa progression. The aim of this review is to provide a brief primer on mouse and human prostate histology and pathology, provide descriptions of mouse models, as well as attempt to answer the age old question: Which GEM model of PCa is the best for my research question?

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Section: Human Versus Mousementioning

confidence: 99%

Mouse models of prostate cancer: picking the best model for the question

Grabowska

DeGraff

et al. 2014

Cancer Metastasis Rev

108

102

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“…These protumorigenic actions of the tumor microenvironment are largely mediated via the secretion of paracrine‐acting factors, including chemokines, cytokines, growth factors, extracellular matrix (ECM) components and ECM remodeling enzymes 5. The importance of the tumor‐associated stroma as a driver of PCa progression and independent predictor of PCa prognosis is underscored by clinical data 6, 7. Thus, there is considerable interest in targeting the tumor microenvironment as a therapeutic strategy for PCa.…”

mentioning

confidence: 99%

Inhibition of Nox4‐dependent ROS signaling attenuates prostate fibroblast activation and abrogates stromal‐mediated protumorigenic interactions

Sampson

Brunner

Weber

et al. 2018

Intl Journal of Cancer

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Carcinoma‐associated fibroblasts (CAFs) play a key onco‐supportive role during prostate cancer (PCa) development and progression. We previously reported that the reactive oxygen species (ROS)‐producing enzyme NADPH oxidase 4 (Nox4) is essential for TGFβ1‐mediated activation of primary prostate human fibroblasts to a CAF‐like phenotype. This study aimed to further investigate the functional relevance of prostatic Nox4 and determine whether pharmacological inhibition of stromal Nox4 abrogates paracrine‐mediated PCa‐relevant processes. RNA in situ hybridization revealed significantly elevated Nox4 mRNA levels predominantly in the peri‐tumoral stroma of clinical PCa with intense stromal Nox4 staining adjacent to tumor foci expressing abundant TGFβ protein levels. At pharmacologically relevant concentrations, the Nox1/Nox4 inhibitor GKT137831 attenuated ROS production, CAF‐associated marker expression and migration of TGFβ1‐activated but not nonactivated primary human prostate fibroblasts. Similar effects were obtained upon shRNA‐mediated silencing of Nox4 but not Nox1 indicating that GKT137831 primarily abrogates TGFβ1‐driven fibroblast activation via Nox4 inhibition. Moreover, inhibiting stromal Nox4 abrogated the enhanced proliferation and migration of PCa cell lines induced by TGFβ1‐activated prostate fibroblast conditioned media. These effects were not restricted to recombinant TGFβ1 as conditioned media from PCa cell lines endogenously secreting high TGFβ1 levels induced fibroblast activation in a stromal Nox4‐ and TGFβ receptor‐dependent manner. Importantly, GKT137831 also attenuated PCa cell‐driven fibroblast activation. Collectively, these findings suggest the TGFβ‐Nox4 signaling axis is a key interface to dysregulated reciprocal stromal–epithelial interactions in PCa pathophysiology and provide a strong rationale for further investigating the applicability of Nox4 inhibition as a stromal‐targeted approach to complement current PCa treatment modalities.

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“…Reactive stroma is found in most cancers and is typified by the coevolution of myofibroblasts (5)(6)(7). Importantly, the volume of reactive stroma relative to cancer is predictive of the rate of cancer progression in several tumor types (8)(9)(10)(11)(12)(13)(14)(15). Furthermore, in vivo modeling has shown that reactive stroma is tumor-promoting (16)(17)(18)(19).…”

mentioning

confidence: 99%

RUNX1 is essential for mesenchymal stem cell proliferation and myofibroblast differentiation

Kim

Barron²,

Martin³

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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124

126

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Myofibroblasts are a key cell type in wound repair, cardiovascular disease, and fibrosis and in the tumor-promoting microenvironment. The high accumulation of myofibroblasts in reactive stroma is predictive of the rate of cancer progression in many different tumors, yet the cell types of origin and the mechanisms that regulate proliferation and differentiation are unknown. We report here, for the first time to our knowledge, the characterization of normal human prostate-derived mesenchymal stem cells (MSCs) and the TGF-β1-regulated pathways that modulate MSC proliferation and myofibroblast differentiation. Human prostate MSCs combined with prostate cancer cells expressing TGF-β1 resulted in commitment to myofibroblasts. TGF-β1-regulated runt-related transcription factor 1 (RUNX1) was required for cell cycle progression and proliferation of progenitors. RUNX1 also inhibited, yet did not block, differentiation. Knockdown of RUNX1 in prostate or bone marrow-derived MSCs resulted in cell cycle arrest, attenuated proliferation, and constitutive differentiation to myofibroblasts. These data show that RUNX1 is a key transcription factor for MSC proliferation and cell fate commitment in myofibroblast differentiation. This work also shows that the normal human prostate gland contains tissue-derived MSCs that exhibit multilineage differentiation similar to bone marrow-derived MSCs. Targeting RUNX1 pathways may represent a therapeutic approach to affect myofibroblast proliferation and biology in multiple disease states. myofibroblast | MSC | RUNX1 | TGF-β1 | reactive stroma

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Determining Prostate Cancer-Specific Death through Quantification of Stromogenic Carcinoma Area in Prostatectomy Specimens

Cited by 58 publications

References 46 publications

Mouse models of prostate cancer: picking the best model for the question

Mouse models of prostate cancer: picking the best model for the question

Inhibition of Nox4‐dependent ROS signaling attenuates prostate fibroblast activation and abrogates stromal‐mediated protumorigenic interactions

RUNX1 is essential for mesenchymal stem cell proliferation and myofibroblast differentiation

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