Stromal fibroblasts impaired in TGF-beta signaling prime the microenvironment with extracellular hydrogen peroxide and mitogenic factors to support the oncogenic transformation of adjacent epithelia
Epithelial cancers arise when the homeostatic interaction between epithelial cells and stromal fibroblasts is perturbed, and the fibroblasts can support the development of a tumor microenvironment by providing the necessary oncogenic signals. Transforming growth factor p (TGFp),...
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sg-ntu-dr.10356-651282023-02-28T18:40:33Z Stromal fibroblasts impaired in TGF-beta signaling prime the microenvironment with extracellular hydrogen peroxide and mitogenic factors to support the oncogenic transformation of adjacent epithelia Tan, Ming Jie Andrew Tan School of Biological Sciences DRNTU::Science::Biological sciences Epithelial cancers arise when the homeostatic interaction between epithelial cells and stromal fibroblasts is perturbed, and the fibroblasts can support the development of a tumor microenvironment by providing the necessary oncogenic signals. Transforming growth factor p (TGFp), which signals through the canonical Smad cascade and several non-canonical TGFP activated kinase-1 (TAK1)-dependent cascades, is an important cytokine that regulates tumorstroma interactions. However, the effects of TAK1 and Smad signaling in stromal fibroblasts on the oncogenic potential of adjacent epithelia remain unclear. We observed that TGFP Type II receptor (TGFPRII), Smad3 and TAK1 are frequently downregulated in human squamous cell carcinomas (SCC). Organotypic cocultures (OTCs) constructed using normal keratinocytes and fibroblasts- that are deficient in TGFPRII, Smad3 or TAK1 (FrGFpRih Fsmad3, FrAKI) revealed that the attenuation of TGFP signaling in fibroblasts led to increased proliferation of the overlying epithelia. Interestingly, we observed that intracellular reactive oxygen species (ROSs) were increased in FrGFPRih Fsmad3 and FrAKI fibroblasts concomitant with increased extracellular hydrogen peroxide (H20 2). The prolonged exposure of keratinocytes to H202 was sufficient to induce colony formation in soft agar, and this was in part due to the oxidative modification of phosphatase and tensin homolog (PTEN) and proto-oncogene tyrosine-protein kinase (Src) and the subsequent augmentation of phosphatidylinositol-3-kinase (PBK)/protein kinase Ba (PKBa) signaling. Furthermore, conditioned media from the various OTCs contained elevated levels of mitogenic factors that were differentially regulated by Smad3 and TAKl. Collectively, these mitogenic factors primed the gene expression and signaling activity of the epithelia towards tumorigenesis. Our study revealed that the tumor-suppressive function of stromal TGFP signaling includes modulating the microenvironmental redox state, and this work may aid in the identification of novel therapeutic targets to reverse or delay cancer progression. Master of Science 2015-06-15T03:35:29Z 2015-06-15T03:35:29Z 2014 2014 Thesis http://hdl.handle.net/10356/65128 en 177 p. application/pdf |
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DRNTU::Science::Biological sciences Tan, Ming Jie Stromal fibroblasts impaired in TGF-beta signaling prime the microenvironment with extracellular hydrogen peroxide and mitogenic factors to support the oncogenic transformation of adjacent epithelia |
| description |
Epithelial cancers arise when the homeostatic interaction between epithelial cells and stromal
fibroblasts is perturbed, and the fibroblasts can support the development of a tumor
microenvironment by providing the necessary oncogenic signals. Transforming growth factor p
(TGFp), which signals through the canonical Smad cascade and several non-canonical TGFP
activated kinase-1 (TAK1)-dependent cascades, is an important cytokine that regulates tumorstroma
interactions. However, the effects of TAK1 and Smad signaling in stromal fibroblasts on
the oncogenic potential of adjacent epithelia remain unclear. We observed that TGFP Type II
receptor (TGFPRII), Smad3 and TAK1 are frequently downregulated in human squamous cell
carcinomas (SCC). Organotypic cocultures (OTCs) constructed using normal keratinocytes and
fibroblasts- that are deficient in TGFPRII, Smad3 or TAK1 (FrGFpRih Fsmad3, FrAKI) revealed that
the attenuation of TGFP signaling in fibroblasts led to increased proliferation of the overlying
epithelia. Interestingly, we observed that intracellular reactive oxygen species (ROSs) were
increased in FrGFPRih Fsmad3 and FrAKI fibroblasts concomitant with increased extracellular
hydrogen peroxide (H20 2). The prolonged exposure of keratinocytes to H202 was sufficient to
induce colony formation in soft agar, and this was in part due to the oxidative modification of
phosphatase and tensin homolog (PTEN) and proto-oncogene tyrosine-protein kinase (Src) and
the subsequent augmentation of phosphatidylinositol-3-kinase (PBK)/protein kinase Ba (PKBa)
signaling. Furthermore, conditioned media from the various OTCs contained elevated levels of
mitogenic factors that were differentially regulated by Smad3 and TAKl. Collectively, these
mitogenic factors primed the gene expression and signaling activity of the epithelia towards
tumorigenesis. Our study revealed that the tumor-suppressive function of stromal TGFP signaling includes modulating the microenvironmental redox state, and this work may aid in the
identification of novel therapeutic targets to reverse or delay cancer progression. |
| author2 |
Andrew Tan |
| author_facet |
Andrew Tan Tan, Ming Jie |
| format |
Theses and Dissertations |
| author |
Tan, Ming Jie |
| author_sort |
Tan, Ming Jie |
| title |
Stromal fibroblasts impaired in TGF-beta signaling prime the microenvironment with extracellular hydrogen peroxide and mitogenic factors to support the oncogenic transformation of adjacent epithelia |
| title_short |
Stromal fibroblasts impaired in TGF-beta signaling prime the microenvironment with extracellular hydrogen peroxide and mitogenic factors to support the oncogenic transformation of adjacent epithelia |
| title_full |
Stromal fibroblasts impaired in TGF-beta signaling prime the microenvironment with extracellular hydrogen peroxide and mitogenic factors to support the oncogenic transformation of adjacent epithelia |
| title_fullStr |
Stromal fibroblasts impaired in TGF-beta signaling prime the microenvironment with extracellular hydrogen peroxide and mitogenic factors to support the oncogenic transformation of adjacent epithelia |
| title_full_unstemmed |
Stromal fibroblasts impaired in TGF-beta signaling prime the microenvironment with extracellular hydrogen peroxide and mitogenic factors to support the oncogenic transformation of adjacent epithelia |
| title_sort |
stromal fibroblasts impaired in tgf-beta signaling prime the microenvironment with extracellular hydrogen peroxide and mitogenic factors to support the oncogenic transformation of adjacent epithelia |
| publishDate |
2015 |
| url |
http://hdl.handle.net/10356/65128 |
| _version_ |
1759855565948846080 |