Youwen Zhou

This study focuses on melanoma, a cancer of pigment-producing cells within the skin(melanocytes) which insidiously spreads (metastasizes) throughout the body. Thisdevastating disease often prevents patients from living beyond five years from diagnosis.Treatment options for melanoma are inept, which has necessitated a demand for research onthe molecular mechanisms of melanoma to aid in the development of novel therapeutictargets and treatments.The gene Sineoculis homeobox homolog 1 (SIX1) encodes for a homeoproteintranscription factor which is an important developmental regulator during embryogenesis. Apreliminary microarray analysis found that SIX1 was upregulated in melanoma. The purposeof this study was to pioneer the assessment of SIX1 in melanoma, including its role in themetastatic functions of melanoma in vitro as well as its clinical relevance. The specific aimsincluded: (1) to assess SIX1 expression in melanoma cell lines and clinical samples; (2) toinvestigate the functional significance and pathogenic role of Six1 in vitro; and (3) toevaluate Six1’s clinical significance in relation to prognosis and clinicopathologicalcharacteristics.Cell lines and clinical samples were tested for SIX1 transcript level using qPCR andprotein level using Western Blotting. Next, two malignant melanoma cell lines weretransfected with shRNA plasmids to generate stable clones with low Six1 expression. Thesealtered cell lines were used to study the functional implications of Six1 expression disparitiesin vitro. Furthermore, immunohistochemistry against Six1 was performed on a tissuemicroarray of 438 melanoma patient biopsies.We discovered that SIX1 was overexpressed in melanoma cell lines and clinicalsamples. Six1 knockdown cells demonstrated diminished cell growth and proliferation,increased apoptosis, and decreased migration and invasion. We also found that a profoundnuclear to cytoplasmic shift of Six1 accompanied melanoma progression and correlated withpoor five-year survival. Higher cytoplasmic Six1 was associated with increased tumorthickness, lower nuclear Six1 with ulceration and histological satellitosis, and both withadvanced AJCC stages and nodular melanoma.To summarize, these results hint that Six1 may play a role in the execution ofmetastatic functions in melanoma. Furthermore, Six1 presents as a tentative candidate for aprognostic marker in patient biopsies.

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Background: Melanoma is a devastating cancer with 17% 5-year survival rate when it is metastasized. Clinically, finding new biomarkers will provide more options in patient early diagnosis and treatments. Previously, Lysyl Oxidase-like 3 (LOXL3) was discovered as one of the most upregulated genes in metastatic melanoma compared to normal nevi and normal skin. LOXL3 is an extracellular protein that induces the cross-linkage formation in collagen and elastin. LOXL3 has never reported in melanoma and barely been studied in tumours. The previous knowledge about LOXL3 makes it an attractive gene to study in melanoma.Objective: The objectives of this study are to investigate LOXL3 expression profile, bio-functions, clinical significance, and potential downstream regulators in melanoma.Experimental Methods: A panel of cell lines and tissues was utilized to evaluate LOXL3 expression in mRNA and protein levels. Two melanoma cell lines, A375 and WM-115, were transfected with siRNAs to create transiently-decreased LOXL3 expression, to study the functional differences of LOXL3 in vitro. Further, immunohistochemical staining of tissue microarray with 373 biopsies was used to observe the correlation between LOXL3 expression levels and patient survival outcomes. Results: We detected a significantly higher expression of LOXL3 on mRNA and protein levels in melanoma compared to melanocytes and normal skins. LOXL3 deficiency could inhibit proliferation, migration and invasion in vitro. Tissue microarray revealed that higher LOXL3 cytoplasmic staining was associated with thicker tumour, the presence of mitosis, more advanced melanoma, and worse primary melanoma patient survival. LOXL3 knockdown did not induce any differences in FAK/Src phosphorylation levels or E-cadherin expression levels.Discussion: LOXL3 promotes cell proliferation, cell motility and cell invasion in vitro, and LOXL3 cytoplasmic overexpression is associated with enhanced tumour mitosis and thickness in melanoma in vivo. This suggests LOXL3 has an essential impact on melanoma growth and potentially metastasis due to the invasive potential. In addition, no correlations are found in FAK/Src activation and E-cadherin restoration by LOXL3, suggesting LOXL3 may use a different pathway beyond previous knowledge.Conclusion: LOXL3 positively regulates cellular growth and invasion in melanoma cells and tissues, making LOXL3 a promising prognostic marker and a therapeutic target.

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Background: Hyperhidrosis (HH) is a disorder in which patient suffers from excessive sweating without any known etiology such as the rise in temperature. Although there have been some epidemiological studies on hyperhidrosis, questions still remain regarding the prevalence of hyperhidrosis and associated demographical, ethnic or geographical factors. Similarly, the association of hyperhidrosis with anxiety and depression has not been systematically investigated. Finally, the relationship between daytime hyperhidrosis and nighttime sweating has not been examined. Methods: One thousand and ten consecutive subjects attending dermatology outpatient clinics in Shanghai Skin Disease Hospital and 1017 subjects in Skin Care Center of Vancouver General Hospital were investigated for this case-control, cross-sectional study after filling out a questionnaire on their presenting concerns, demographical information and mental stress and sweating symptoms. The subjects were then classified to have primary HH subtypes using the criteria of International Hyperhidrosis Society, late onset hyperhidrosis, or no-HH. Then the prevalence of HH and its correlation with anxiety, depression and NS was examined in both single variants and multivariate logistic regression analyses, stratified according to age at examination, sex, ethnicity, presenting diagnosis, BMI, and specific study cities. Results: The prevalence of total HH is very similar in Shanghai and Vancouver (about 18%). Primary HH subtypes have the highest prevalence in those younger than 30 years old, decreasing dramatically in later years. Caucasian subjects are more likely to develop axillary hyperhidrosis compared to Chinese subjects. The prevalence of anxiety and depression was 21.3% and 27.2% in hyperhidrosis patients, respectively, and 7.5% and 9.7% in patients without hyperhidrosis. Among the effects of ethnicity, mental stress symptoms and HH, which are correlated with NS, HH is the most associated factor with NS as more than half of the patients with HH suffer from NS.Conclusion: Prevalence of total HH is similar in different geographical locations.However, certain specific HH subtypes can show great variations according to ethnicity, age, body mass index and sex and based on the severity of sweating. Similar to NS, both anxiety and depression were more prevalent in patients with HH, than those without HH.

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Background: Vitiligo is a complex autoimmune skin condition characterized by the death of melanocytes, the principle pigment producing cells in the skin. Transcriptome analysis of vitiligo skin revealed significantly reduced levels of proteolipid 1 (PLP1) gene, which is known to be expressed by Schwann cells, as well as significantly up-regulation of genes that are associated with natural killer (NK) cell activity.Hypothesis and Objectives: Schwann cells may be adversely affected in vitiligo and NK cells may potentially play a role in the overall disease pathogenesis. Therefore, the purpose of this study is to characterize the down-regulation of PLP1 and assess the presence of NK cell infiltration in vitiligo skin biopsies.Materials and Methods: PLP1 expression analyses were performed on major types of skin cells as well as vitiligo and normal skin samples. Quantification of Schwann cells was performed on paired vitiligo samples using immunohistochemistry. Schwann cell conditioned medium was also tested for its ability to support the growth and survival of human melanocytes. To assess NK cell activity, explant skin cultures and immunofluorescence analyses were performed to localize activated NK cells in skin biopsies.Results: Schwann cells were the primary source of PLP1 in human skin, although it is also expressed by melanocytes. Schwann cells were found to be decreased in vitiligo lesional skin as compared to peri-lesional and normal skin. In addition, conditional medium prepared from cultured Schwann cells significantly increased the survival of human melanocytes. Furthermore, explant skin cultures and immunofluorescence studies revealed marked increase of NK cells with heightened activity in vitiligo lesional as well as peri-lesional vitiligo skin.Conclusion: Results from our study suggest that the loss of melanocytes and reduction in Schwann cells may account for the down-regulation of PLP1 in vitiligo lesional skin. In addition, Schwann cells may play a role in the growth and survival of melanocytes and their decrease may have facilitated the development of vitiligo. Furthermore, this study lends support to the direct involvement of NK cells in the pathogenesis of vitiligo and suggests that they should be explored as cellular targets for development of better therapies in the future.

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