Jill Whyte scite author profile

Background:Securing a diagnosis of ovarian cancer and establishing means to predict outcomes to therapeutics remain formidable clinical challenges. Early diagnosis is particularly important since survival rates are markedly improved if tumour is detected early.Methods:Comprehensive miRNA profiles were generated on presurgical plasma samples from 42 women with confirmed serous epithelial ovarian cancer, 36 women diagnosed with a benign neoplasm, and 23 comparably age-matched women with no known pelvic mass.Results:Twenty-two miRNAs were differentially expressed between healthy controls and the ovarian cancer group (P<0.05), while a six miRNA profile subset distinguished presurgical plasma from benign and ovarian cancer patients. There were also significant differences in miRNA profiles in presurgical plasma from women diagnosed with ovarian cancer who had short overall survival when compared to women with long overall survival (P<0.05).Conclusion:Our preliminary data support the utility of circulating plasma miRNAs to distinguish women with ovarian cancer from those with a benign mass and identify women likely to benefit from currently available treatment for serous epithelial ovarian cancer from those who may not.

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Identification of grade and origin specific cell populations in serous epithelial ovarian cancer by single cell RNA-seq

Shih

et al. 2018

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Here we investigated different cell populations within ovarian cancer using single-cell RNA seq: fourteen samples from nine patients with differing grades (high grade, low grade and benign) as well as different origin sites (primary and metastatic tumor site, ovarian in origin and fallopian in origin). We were able to identify sixteen distinct cell populations with specific cells correlated to high grade tumors, low grade tumors, benign and one population unique to a patient with a breast cancer relapse. Furthermore the proportion of these populations changes from primary to metastatic in a shift from mainly epithelial cells to leukocytes with few cancer epithelial cells in the metastases. Differential gene expression shows myeloid lineage cells are the primary cell group expressing soluble factors in primary samples while fibroblasts do so in metastatic samples. The leukocytes that were captured did not seem to be suppressed through known pro-tumor cytokines from any of the cell populations. Single cell RNA-seq is necessary to de-tangle cellular heterogeneity for better understanding of ovarian cancer progression.

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The role of the hairy gene during Drosophila morphogenesis: stripes in imaginal discs

Carroll¹,

Whyte²

1989

Genes Dev.

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The Drosophila pair-rule embryonic segmentation gene hairy is also required later in development to suppress the formation of certain adult sensory structures. Striking patterns of nuclear hairy protein distribution emerge during larval and pupal imaginal disc morphogenesis, hairy is expressed transiently in the cells just anterior to the morphogenetic furrow as it passes across the eye disc and in stripes along the proximo-distal axis of the leg discs and the developing veins of the wing disc. hairy expression is correlated with disc cell-cycle changes and is excluded from the sensory neurons that differentiate near or among the rows of hairy-expressing cells. It is likely that hairy regulates genes affecting neuronal determination, such as achaete, and is regulated by genes that specify anteroposterior polarity within imaginal discs.

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LPA receptor 2 mediates LPA-induced endometrial cancer invasion

Hope

Wang

Whyte

et al. 2009

Gynecologic Oncology

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Lymph node dissection in the surgical management of atypical endometrial hyperplasia

Whyte

Gurney

Curtin

et al. 2010

American Journal of Obstetrics and Gynecology

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Jill Whyte

Circulating biomarkers for detection of ovarian cancer and predicting cancer outcomes

Identification of grade and origin specific cell populations in serous epithelial ovarian cancer by single cell RNA-seq

The role of the hairy gene during Drosophila morphogenesis: stripes in imaginal discs

LPA receptor 2 mediates LPA-induced endometrial cancer invasion

Lymph node dissection in the surgical management of atypical endometrial hyperplasia

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