<i>Ras</i>Mutation Impairs Epithelial Barrier Function to a Wide Range of Nonelectrolytes

Mullin, James M.; Leatherman, James M.; Valenzano, Mary Carmen; Huerta, Erika Rendon; Verrechio, Jon J.; Smith, David M.; Snetselaar, Karen M.; Liu, Mantao; Francis, Mary Kay; Sell, Christian

doi:10.1091/mbc.e05-04-0294

Cited by 37 publications

(31 citation statements)

References 50 publications

(60 reference statements)

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“…It can thus be suggested that the elevated pathogenic character of RASV12 transfected FTC-133 cells involves the increase of CLAUDIN-1 protein expression. This increase in CLAUDIN-1 expression after RASV12 transfection was also observed in normal renal epithelial cells, whereby in these normal cells CLAUDIN-1 was localized in the cell membrane (Mullin et al 2005). As a side note, we tried CLAUDIN-1 downregulation by CLAUDIN-1 siRNA transfection of RASV12 transfected FTC-133 cells, which resulted in cell death within a few hours, potentially due to the augmented stress of cells, and irrespective if cells were transfected either with control siRNA or CLAUDIN-1 siRNA transfection mixture (unpublished observation).…”

Section: Discussionsupporting

confidence: 63%

The impact of CLAUDIN-1 on follicular thyroid carcinoma aggressiveness

Zwanziger¹,

Badziong²,

Ting³

et al. 2015

Endocrine-Related Cancer

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CLAUDIN-1 belongs to the family of transmembrane tight junction proteins tightening the paracellular cleft of epithelial cells. In human malignancies, CLAUDIN-1 is often dysregulated and located in subcellular compartments, particularly in the nucleus where it may influence cellular behaviour. Here, we studied CLAUDIN-1 in relation to the biological characteristics of follicular thyroid carcinoma (FTC). CLAUDIN-1 immuno-staining showed loss of membrane expression and increased nuclear CLAUDIN-1 localization in FTC metastases. CLAUDIN-1 function was further investigated in two different follicular thyroid carcinoma cell lines: FTC-133 isolated from a regional lymph node metastasis and FTC-238 derived from a lung metastasis. In both cell lines CLAUDIN-1 expression was demonstrated in the cell nuclei with a significantly higher protein expression in FTC-238 compared to FTC-133 cells. Interestingly, in vitro scratch assay revealed enriched nuclear CLAUDIN-1 expression near the scratch. Furthermore, the increase of the pathogenic character of FTC-133 cells by RASV12 transfection was associated with elevated CLAUDIN-1 expression and enhanced cell migration, invasion and proliferation. Likewise over-expression of nuclear CLAUDIN-1 in FTC-133 cells resulted in increased cell migration and invasion. Conversely, CLAUDIN-1 downregulation in FTC-238 cells by siRNA resulted in decreased cell migration and invasion and was accompanied by reduced phosphoPKC expression. Moreover, activation and inhibition of PKC resulted in CLAUDIN-1 up-and downregulation in FTC cells respectively. These data suggest an impact of CLAUDIN-1 on follicular thyroid carcinoma aggressiveness, which could potentially be influenced by PKC activity.

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Section: Discussionsupporting

confidence: 63%

The impact of CLAUDIN-1 on follicular thyroid carcinoma aggressiveness

Zwanziger¹,

Badziong²,

Ting³

et al. 2015

Endocrine-Related Cancer

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“…The penetration of factors such as IGF-I into these areas may signify a local loss of epithelial barrier function, and it has been suggested that a local breach in the epithelial barrier may be an early event in tumor formation (22). We have shown that oncogenic conversion of epithelial cells produces profound changes in epithelial barrier function (23), and it has been reported that seminal fluid can alter epithelial barrier function in vitro (24,25). This supports the idea that factors from the seminal fluid enter the basal compartment in the prostate where these factors can influence basal cell proliferation.…”

Section: Discussionmentioning

confidence: 73%

Insulin-Like Growth Factor-I Produced by Seminal Vesicles: Relationship to Intraepithelial Basal Cell Hyperplasia in the Prostate

Garcia

Urbańska²,

Koltowski³

et al. 2007

Clinical Cancer Research

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Purpose: This study examined the seminal vesicle fluid (SVF) as a potential local source of insulin-like growth factor-I (IGF-I) in the peripheral zone of the prostate. Experimental Design: IGF-I levels in seminal fluid were measured. The levels of the IGF-I receptor (IGF-IR) in its active, phosphorylated form as well as direct downstream targets were examined in the peripheral zone of the prostate. Results: In situ, we find that the IGF-IR is activated in the peripheral zone in areas of atrophy, prostatic intraepithelial hyperplasia, and cancer. In addition, immunostaining reveals preferential activation of the IGF-IR in p63-positive cells in areas of intermediate basal cell hyperplasia in the peripheral zone, indicating that prostate progenitor cells are highly sensitive to increases in local IGF-I levels. These areas of basal cell hyperplasia occur at high incidence in the peripheral zone of the prostate. Relatively high levels of IGF-I were identified in SVF. In addition, we find that SVF can stimulate the proliferation of both normal and cancer-derived prostate cells. Conclusions: These results suggest that SVF is a local source of IGF-I that provides chronic stimulation of prostate cells. This chronic stimulation could contribute to the development of prostate cancer in older men.Prostate cancer exhibits a prominent zonal distribution. The peripheral zone harbors over 70% of prostate cancers, and this region of the prostate is also the primary site of high-grade prostatic intraepithelial neoplasia (HGPIN; ref. 1). In terms of tissue architecture, glands throughout the prostate are characterized by a basal cell compartment, which is believed to include potential stem cells, and a secretory compartment (2, 3). Cells within the basal cell compartment may represent the population that undergoes malignant transformation during the formation of prostate cancer (4, 5). The regional variation in prostate cancer suggests that basal cells within the peripheral zone are affected by the presence of local factors responsible for differential progression of the disease. A greater understanding of the zonal distribution of basal cells and the local factors that influence their proliferation and/or differentiation might help explain the localization of precursor lesions and prostate carcinoma.In an attempt to identify local factors that influence cell proliferation and differentiation in the prostate, we have examined seminal vesicle fluid (SVF) as a source of insulinlike growth factor-I (IGF-I). This effort was prompted by the growing realization of the importance of local production of IGF-I. Both IGF and IGF binding proteins have been identified in the semen (6 -8), but the recent focus of interest has been on circulating IGF as a potential indicator of relative risk for prostate cancer. The seminal fluid is a potential source of factors that influence the peripheral zone of the prostate specifically because the ejaculatory ducts merge with the urethra upstream of the terminal ducts of the peripheral zone.In h...

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“… ERK has a variable effect on the integrity of epithelial tight junctions; it can disrupt tight junction integrity in some cases 121,122,125,126 whereas, it can also protect tight junction integrity in other cases. 94,123 The mechanistic basis for this paradoxical ERK activity in tight junction regulation remains unclear.…”

Section: Chapter 5: Discussionmentioning

confidence: 99%

“…124 Another study showed that a mutation in Ras (a signaling molecule upstream of ERK) is associated with increase in extra cellular signal-regulated kinase-2 phosphorylation and produces leakiness of tight junctions to certain types of solutes. 125 Similarly, Raf-1-another signaling molecule upstream of ERK has been implicated in causing disruption of epithelial TJs via downregulation of occludin. 126 Another study demonstrated that downregulation of the MAPK signaling pathway causes the restoration of epithelial cell morphology and the assembly of tight junctions in Ras-transformed epithelial cells and that tyrosine phosphorylation of occludin and ZO-1 may play a role in some aspects of tight junction formation.…”

Section: Erk In Regulation Of Tight Junctionsmentioning

confidence: 99%

“…Some of the previous studies that showed the disruptive effect of MAPK pathway on tight junctions used under-differentiated cells or the cell types that do not differentiate. 121,122,125 On the other hand, highly differentiated cells were used when a protective response of MAPK pathway activation was observed on tight junction. 94 In the present study, we were able to demonstrate these opposing effects of ERK in the same cell type but at different stage of differentiation.…”

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Role of Extracellular Signal-Regulated Kinase (ERK) in Regulation of Intestinal Epithelial Tight Junctions

Aggarwal¹

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RasMutation Impairs Epithelial Barrier Function to a Wide Range of Nonelectrolytes

Cited by 37 publications

References 50 publications

The impact of CLAUDIN-1 on follicular thyroid carcinoma aggressiveness

The impact of CLAUDIN-1 on follicular thyroid carcinoma aggressiveness

Insulin-Like Growth Factor-I Produced by Seminal Vesicles: Relationship to Intraepithelial Basal Cell Hyperplasia in the Prostate

Role of Extracellular Signal-Regulated Kinase (ERK) in Regulation of Intestinal Epithelial Tight Junctions

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