In vitro effects of arsenic trioxide on head and neck squamous cells carcinoma

Chu, Wai-keung., 朱偉強.

January 2005

published_or_final_version / abstract / Medicine / Master / Master of Philosophy

Arsenic compounds.

Epidermal growth factor - Receptors.

Squamous cell carcinoma.

Head - Cancer.

Neck - Cancer.

Molecular genetics of esophageal squamous cell carcinoma

Law, Bic-fai, Fian., 羅璧輝.

January 2006

published_or_final_version / abstract / Pathology / Doctoral / Doctor of Philosophy

Esophagus - Cancer - Genetic aspects.

Molecular genetics.

Identification of differentially expressed genes in a newly established esophageal squamous cell carcinoma(ESCC) cell line HKESC-4of Chinese origin

Cheung, Chi-man, 張志文

January 2007

published_or_final_version / Surgery / Master / Master of Philosophy

Esophagus - Cancer - Genetic aspects.

Gene expression.

Dysregulation of microRNAs in tongue squamous cell carcinoma

Liu, Xiaobing, 劉小兵

January 2008

published_or_final_version / Surgery / Doctoral / Doctor of Philosophy

Small interfering RNA.

Tongue - Cancer - Genetic aspects.

Role of the Pediatric Dental Provider in Human Papillomavirus (HPV) Education

Dugoni, Meredith L

01 January 2017

Purpose: This study investigates knowledge about HPV and examines if pediatric dental providers should include HPV education for guardians of patients 10-18 years. Methods: Legal guardians of 10-18 year-old patients of the Virginia Commonwealth University Pediatric Dental Clinic were enrolled in this prospective cohort study. Participants completed a baseline survey, were provided HPV education, completed an initial follow-up survey, and then completed a 6-month follow-up survey. Results: A total of 54 participants completed the baseline and initial follow-up surveys and 17 completed the 6-month follow-up survey. The average number of correct responses was 3.4 of 6 knowledge questions, which significantly improved to 5.4 at follow-up (P<.0001). The greatest increase in the percent responding correctly was regarding HPV and oropharyngeal cancer from 22% baseline to 91% at initial follow-up (P<.0001). Regarding Stage of Change, 14 (23%) of those not initially in the Action group had improved at least 1 stage. At the 6-month follow-up, 3 (43%) guardians reported completing the HPV vaccine series. Conclusions: These results demonstrate limited knowledge about HPV and highlight the pediatric dental provider’s ability to educate. Since the greatest knowledge gap pertained to HPV and oropharyngeal cancer, it is important for pediatric dental providers to increase their role in HPV education. As oral cancers are the purview of dentists, practitioners should be involved with their patients’ consideration of the HPV vaccine.

Human Papillomavirus

Oropharyngeal Neoplasms

Oropharynx

Patient Education

Cancer

Squamous Cell Carcinoma

Pediatric Dentistry and Pedodontics

Psoas abscess secondary to retroperitoneal distant metastases from squamous cell carcinoma of the cervix with thrombosis of the inferior vena cava and duodenal infiltration treated by Whipple procedure

Mehdorn, Matthias, Petersen, Tim-Ole, Bartels, Michael, Jansen-Winkeln, Boris, Kassahun, Woubet Tefera

06 September 2016

Background: Psoas abscess is a rare clinical disease of various origins. Most common causes include hematogenous spread of bacteria from a different primary source, spondylodiscitis or perforated intestinal organs. But rarely some abscesses are related to malignant metastatic disease. Case presentation: In this case report we present the case of a patient with known squamous cell carcinoma of the cervix treated with radio-chemotherapy three years prior. She now presented with a psoas abscess and subsequent complete inferior vena cava thrombosis, as well as duodenal and vertebral infiltration. The abscess was drained over a prolonged period of time and later was found to be a complication caused by metastases of the cervical carcinoma. Due to the massive extent of the metastases a Whipple procedure was performed to successfully control the local progress of the metastasis. Conclusion: As psoas abscess is an unspecific disease which presents with non-specific symptoms adequate therapy may be delayed due to lack of early diagnostic results. This case report highlights the difficulties of managing a malignant abscess and demonstrates some diagnostic pitfalls that might be encountered. It stresses the necessity of adequate diagnostics to initiate successful therapy. Reports on psoas abscesses that are related to cervix carcinoma are scarce, probably due to the rarity of this event, and are limited to very few case reports. We are the first to report a case in which an extensive and complex abdominal procedure was needed for local control to improve quality of life.

Psoasabszess

Plattenepithelkarzinom

Gebärmutterhals

Whipple-Operation

malignant psoas abscess

squamous cell carcinoma of the cervix

Whipple procedure

ddc:601

Investigation of the role of ASPP2 in tumourigenesis

Tordella, Luca

January 2012

The skin is the site where two of the most common types of epithelial cancer, basal cell carcinoma (BCC) and squamous cell carcinoma (SCC), arise. In this work, we have investigated how ASPP2, a member of a family of proteins that interact with the p53 family, can affect skin tumourigenesis. ASPP2 is expressed in the squamous epithelia of various organs, localising exclusively in the upper and most differentiated layers. We show here that Balb/c ASPP2-null and heterozygous mice develop spontaneous SCCs. To investigate how the absence of ASPP2 from the epithelial compartment could lead to tumour formation, we analysed ASPP2’s relationship with pathways involved in the normal homeostasis of the epithelium, such as p63 and Notch. &Delta;Np63 is the main p63 isoform expressed in the adult epidermis, and its function is to drive the proliferation of the basal keratinocytes. Aberrant or misplaced activation of &Delta;Np63 in the epithelium is a known initiating cause for SCC. Consistent with this, &Delta;Np63 was found to be highly expressed in tumours derived from ASPP2-deficient mice. Our results indicate that ASPP2 is important in limiting &Delta;Np63 expression in the differentiated epithelium, preventing cell proliferation in the upper layers of the skin. This is achieved by antagonising &Delta;Np63 transcript and protein expression, resulting in a mutually exclusive expression pattern during differentiation of keratinocytes, as well as in epithelial cancer. ASPP2 expression was found reduced or lost in human SCC cell lines and during head and neck cancer progression, reflecting what was observed in ASPP2-deficient mice. Overall, our results indicate a possible mechanism by which p63 expression can be regulated in the skin, and provide a new model for the spontaneous formation of SCC in vivo. Additionally, we found that ASPP2 can cooperate with and enhance the activity of skin pro-differentiation pathways, such as Notch. In contrast to p63, ASPP2 and Notch1 are co-expressed in the differentiated layers of the squamous epithelium. Moreover, ASPP2 can interact with components of Notch nuclear transcriptional machinery, and it is shuttled into the nuclear compartment upon activation of Notch pathway. This recruitment results in modulation of Notch transcriptional activity on specific target genes with a differential pattern of binding sites, providing new insights into the understanding of Notch transcriptional regulation.

616.99

MUTANT P53 REGULATION OF CXC-CHEMOKINE EXPRESSION IN HEAD AND NECK SQUAMOUS CELL CARCINOMA

Field, Brittany

11 October 2012

Head and neck squamous cell carcinoma (HNSCC) is the 6th most common type of cancer in the western hemisphere with a five-year survival rate of only 50% for patients with a localized tumor, which decreases significantly to as low as 5% for those patients with tumors that have metastasized to distant sites of the body. It has been found that both mutant p53 and epidermal growth factor receptor (EGFR) signaling pathways function to increase the expression of CXCL5, which has been identified as a key mediator in the process of tumor metastasis. Previous data from our lab suggested that the p53 homolog, p63, may function as a negative regulator of CXCL5 and that mutant p53 may inhibit this molecule to elevate CXCL5 expression levels. In the current study we utilized an model system in which the H179L p53 mutant was expressed in HN4 cells to investigate the hypothesis that mutant p53 enhances expression of CXCL5 by both interfering with p63 function and cooperating with EGFR/EPS8 signaling, leading to increased cell proliferation and motility. The results of the current study indicate a role for mutant p53 in head and neck squamous cell carcinoma proliferation, migration and tumorigenicity, possibly through enhancement of CXCL5 expression. We were able to show that mutant p53 expression caused an increase in the expression of this chemokine in addition to increasing proliferation and migration of the cells compared to the vector control. Additionally, we showed that p63 protein is a negative regulator of CXCL5 that is downregulated in the cells expressing mutant p53, which suggests that through direct interaction, mutant p53 may function to inhibit p63 function as well as target it for degradation. These results support the hypothesis that GOF mutant p53 enhances expression of CXCL5 by interfering with p63 function in cancer cells. The results of the current study results also showed that upon treatment with EGF, HN4 cells expressing mutant p53 express elevated levels of CXCL5; and that the mutant p53-expressing HN4 cells cooperate with EGFR/EPS8 signaling to further deregulate chemokine expression. These data taken together suggest there are complex interactions taking place between mutant p53, p63, EGFR signaling, and CXCL5 to regulate the biological processes that promote tumor progression that could lead to metastasis. Additional studies are needed to further elucidate the molecules involved in the mutant p53 mechanism that promotes tumorigenesis.

p63

mutant p53

mp53

CXCL5

HNSCC

Squamous cell carcinoma

EPS8

EGF

Life Sciences

Physiology

P63, adhérence intra-épithéliale et cancers de l’oesophage / P63, intra-epithelial adhesion and esophageal cancer

Thepot-Duranton, Amélie

19 November 2009

Depuis sa découverte, le gène TP63 a soulevé un intérêt considérable grâce à son rôle majeur dans la morphogenèse des épithélia. La quasi-totalité de nos connaissances dérive de l’observation des phénotypes des souris déficientes qui présentent une absence d’épithélia pluristratifiés, due à un défaut d'expression des complexes d'adhérence cellule-matrice extra cellulaire et cellules-cellules. De plus, TP63 est amplifié et surexprimé dans environ 25% des carcinomes épidermoïdes de l’œsophage et est quasi absent des adénocarcinomes du même organe. Dans ce travail nous avons étudié l’expression de p63 dans la muqueuse œsophagienne, et nous avons montré que p63 exerce un rôle de régulateur de l’expression des complexes d’adhérence intra-épithéliaux lors de la transition entre les cellules basales/suprabasales hautement prolifératives et les couches les plus différenciées incapables de proliférer. Puis, nous avons étudié le rôle possible de p63 dans la formation de la métaplasie intestinale, une lésion précurseur de l’adénocarcinome. Dans ce contexte, nous avons établi qu’un traitement reconstituant le stress acido-biliaire induit une perte d’expression de p63 secondaire à une dégradation par le protéasome dans des cellules primaires et des lignées dérivées de carcinomes œsophagiens. Enfin, à l’aide d’un modèle de peau reconstruite, nous avons montré l’implication de p63 dans la stratification épithéliale, dans la prolifération, la différenciation et les interactions épithélium-mésenchyme. Ces réstultats clarifient le rôle de TP63 comme un ongène potentiel dans le carcinome épidermoïde de l’œsophage et comme potentiel suppresseur dans l’adénocarcinome / Since its discovery in 1998, the TP63 gene has raised considerable interest due to its major role in epithelial morphogenesis. The vast majority of our current knowledge is based on the phenotypes of TP63 deficient mice, which show a lack of stratified epithelia associated with defects in the expression of cell-cell and cell-matrix adhesion complexes. In addition, TP63 systematically overexpressed in squamous cell carcinomas and amplified in about 25% of œsophageal squamous cell carcinomas, whereas it is barely detectable in adenocarcinomas that arise in the same organ. This work analyzes the expression of p63 in normal œsophageal mucosa and demonstrates its regulatory role in the expression of cell-cell adhesion complexes at the transition between highly proliferative basal/suprabasal layers and more differentiated, non-proliferative superficial layers. Next, the role of p63 in the formation of intestinal metaplasia, a precursor of adenocarcinoma, is addressed in experiments reconstituting in vtro the effects of acid-bile gastro-oesophageal reflux. We show that this form of stress induces a loss of p63 in cell lines derived from oesophageal cancers, due to its rapid proteasome-dependent degradation. Finally, we have used an in vitro skin reconstruction model to demonstrate the involvement of p63 in the process of epidermal stratification, proliferation, differentiation, and epithelium-mesenchyme interactions. These results clarify the role of TP63 as a potential oncogene in œsophageal squamous cell carcinoma, and as a potential suppressor in adenocarcinoma

P63

Oesophage

Carcinome épidermoïde

Adénocarcinome

Peau reconstruite

P63

Esophagus

Squamous cell carcinoma

Adenocarcinoma

Reconstructed skin

571.6

N-glycosylation signaling pathways in oral squamous cell carcinoma

Almershed, Munirah EME

28 September 2016

Oral squamous cell carcinoma (OSCC) accounts for majority of head and neck cancers and ranks as the sixth most common cancer in the world. OSCC belongs to the most understudied cancers and little is known about molecular mechanisms underlying its etiology and progression to metastasis. A hallmark of cancer is the enhanced posttranslational modification of cell surface proteins with complex N-glycans. Our studies have shown that induced protein N-glycosylation via activation of the core N-glycosylation-regulating gene, DPAGT1, is associated with reduced E-cadherin adhesion, as well as deregulation of several oncogenic signaling pathways, including Wnt/β-catenin and Hippo. Modest increases in DPAGT1 expression are associated with dramatic amplification of Wnt/β-catenin activity and increased expression and nuclear localization of the Hippo pathway effectors TAZ /YAP. The goal of this study was to align the expression and localization of DPAGT1, complex N-glycans, β-catenin, and TAZ/YAP with the progression of oral cancer in vivo from dysplasia to OSCC. Human oral tissues from different stages of OSCC pathogenesis were characterized for DPAGT1/β-catenin/α-catenin/YAP/TAZ expression and localization and correlated with cell surface expression of complex N-glycans by PHA lectin staining and with expression of primitive cell surface markers, CD44, CD24 and CD29. Results showed that high DPAGT1 expression and nuclear TAZ became increasingly associated with disorganized E-cadherin junctions as oral epithelium progressed from mild to severe dysplasia to OSCC. This correlated with increasing expression of cell surface complex N-glycans and CD44. These studies suggest that DPAGT1/β-catenin/TAZ and high PHA staining represent novel signatures for OSCC pathogenesis.

Molecular biology

GPT

Hipp-pathway

N-glycosylation

OSCC

Wnt-pathway

Oral squamous cell carcinoma