14 results on '"Kerslake, Rachel"'
Search Results
2. p38β - MAPK11 and its role in female cancers
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Katopodis, Periklis, Kerslake, Rachel, Zikopoulos, Athanasios, Beri, Nefeli, and Anikin, Vladimir
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- 2021
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3. The Early Intervention Readiness Program (EIRP): A Post-ASD Diagnosis Family Support Program
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Tolmie, Rhiannon S., Bruck, Susan, and Kerslake, Rachel
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A child's diagnosis with autism spectrum disorder (ASD) can be an extremely stressful time for families. Researchers suggest that the period immediately following ASD diagnosis is a key time for professionals to guide families by providing appropriate information about support options. This article describes a family support program, developed by Autism Spectrum Australia (Aspect). The Early Intervention Readiness Program (EIRP) is delivered during the challenging post-diagnosis period. During program involvement, families are provided with information and management strategies related to ASD-associated behaviors, and support options are identified. The EIRP aims to strengthen family confidence and facilitate a smooth transition into appropriate early intervention services. Preliminary program evaluation outcomes indicate that following program involvement, participants perceive a significant increase in their confidence in their understanding of ASD and capacity to independently make decisions about related supports. Participant post-program evaluations also verify the EIRP to be a useful post-ASD diagnosis support.
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- 2017
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4. Transcriptional Landscape of 3D vs. 2D Ovarian Cancer Cell Models.
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Kerslake, Rachel, Belay, Birhanu, Panfilov, Suzana, Hall, Marcia, Kyrou, Ioannis, Randeva, Harpal S., Hyttinen, Jari, Karteris, Emmanouil, and Sisu, Cristina
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ONLINE information services , *IN vitro studies , *DISEASE progression , *OVARIAN tumors , *CELL culture , *META-analysis , *SEQUENCE analysis , *STRUCTURAL models , *CARCINOGENESIS , *PHENOMENOLOGICAL biology , *RNA , *CELL physiology , *GENE expression profiling , *RESEARCH funding , *CELL lines , *MEDLINE , *GENETIC profile - Abstract
Simple Summary: Ovarian cancer is one of the most lethal female cancers. Numerous investigations into the development and progression of this disease have resulted in the creation of numerous three-dimensional culture models to better reflect the natural microenvironment of these tumours. In this study, we leverage the available transcriptomics and clinical and novel experimental data to evaluate the impact of the growth conditions on various cancer cells and examine whether they better approximate the behaviour of tumour cells compared to the classical two-dimensional models. Our results show that variability in the growth conditions can impact key genes and biological processes that are hallmarks of cancer, highlighting the need for future studies to identify which is the most appropriate in vitro/preclinical model to study tumour microenvironments. Three-dimensional (3D) cancer models are revolutionising research, allowing for the recapitulation of an in vivo-like response through the use of an in vitro system, which is more complex and physiologically relevant than traditional monolayer cultures. Cancers such as ovarian (OvCa) are prone to developing resistance, are often lethal, and stand to benefit greatly from the enhanced modelling emulated by 3D cultures. However, the current models often fall short of the predicted response, where reproducibility is limited owing to the lack of standardised methodology and established protocols. This meta-analysis aims to assess the current scope of 3D OvCa models and the differences in the genetic profiles presented by a vast array of 3D cultures. An analysis of the literature (Pubmed.gov) spanning 2012–2022 was used to identify studies with paired data of 3D and 2D monolayer counterparts in addition to RNA sequencing and microarray data. From the data, 19 cell lines were found to show differential regulation in their gene expression profiles depending on the bio-scaffold (i.e., agarose, collagen, or Matrigel) compared to 2D cell cultures. The top genes differentially expressed in 2D vs. 3D included C3, CXCL1, 2, and 8, IL1B, SLP1, FN1, IL6, DDIT4, PI3, LAMC2, CCL20, MMP1, IFI27, CFB, and ANGPTL4. The top enriched gene sets for 2D vs. 3D included IFN-α and IFN-γ response, TNF-α signalling, IL-6-JAK-STAT3 signalling, angiogenesis, hedgehog signalling, apoptosis, epithelial–mesenchymal transition, hypoxia, and inflammatory response. Our transversal comparison of numerous scaffolds allowed us to highlight the variability that can be induced by these scaffolds in the transcriptional landscape and identify key genes and biological processes that are hallmarks of cancer cells grown in 3D cultures. Future studies are needed to identify which is the most appropriate in vitro/preclinical model to study tumour microenvironments. [ABSTRACT FROM AUTHOR]
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- 2023
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5. Elevated Circulating Lactate Levels and Widespread Expression of Its Cognate Receptor, Hydroxycarboxylic Acid Receptor 1 (HCAR1), in Ovarian Cancer.
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Kerslake, Rachel, Panfilov, Suzana, Mustafa, Nashrah, Hall, Marcia, Kyrou, Ioannis, Randeva, Harpal S., Karteris, Emmanouil, and Godfrey, Richard
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OVARIAN cancer , *LACTIC acid fermentation , *LACTATES , *LACTATION , *CELL communication - Abstract
Background: Augmented glycolysis in cancer cells is a process required for growth and development. The Warburg effect provides evidence of increased glycolysis and lactic acid fermentation in cancer cells. The lactate end-product of glycolysis is receiving growing traction for its role as a cell signalling molecule. Ovarian cancer (OvCa) is also characterised by altered glucose metabolism. We aim to explore circulating lactate levels in patients with high-grade serous OvCa (HGSOC) and to elucidate the expression of the lactate receptor hydroxycarboxylic acid receptor 1 (HCAR1) in OvCa. Methods: HCAR1 expression was detected in patient biopsy cores using immunohistochemistry, while lactate was measured from whole blood with a Biosen-C line clinic measuring system. Results: We noted significantly elevated lactate levels in OvCa patients (4.3 ± 1.9 mmol/L) compared with healthy controls (1.4 ± 0.6 mmol/L; p < 0.0001), with an AUC of 0.96. The HCAR1 gene is overexpressed in OvCa compared to healthy controls (p < 0.001). Using an OvCa tissue microarray (>75% expression in 100 patients), high protein expression was also recorded across all epithelial OvCa subtypes and ovarian normal adjacent tissue (NAT). Conclusions: Lactate monitoring is a simple, cost-efficient test that can offer point-of-care results. Our data suggest that the potential of circulating lactate as a screening biomarker in OvCa merits further research attention. [ABSTRACT FROM AUTHOR]
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- 2023
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6. Differential Regulation of Genes by the Glucogenic Hormone Asprosin in Ovarian Cancer.
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Kerslake, Rachel, Sisu, Cristina, Panfilov, Suzana, Hall, Marcia, Khan, Nabeel, Jeyaneethi, Jeyarooban, Randeva, Harpal, Kyrou, Ioannis, and Karteris, Emmanouil
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OVARIAN cancer , *GENETIC regulation , *CIRCULATING tumor DNA , *ENERGY metabolism , *METABOLIC disorders , *CELL communication - Abstract
Background: Ovarian cancer (OvCa) is one of the most lethal forms of gynaecological malignancy. Altered energy metabolism and increased aerobic glycolysis in OvCa are hallmarks that demand attention. The glucogenic hormone asprosin is often dysregulated in metabolic disorders such as insulin resistance, diabetes (type 2 and gestational), and preeclampsia. Despite association with metabolic disorders, its role in energy metabolism within the tumour microenvironment is yet to be explored. Here, we study the role of asprosin in OvCa using transcriptomics and expand on functional studies with clinical samples. Methods: RNA sequencing, functional gene enrichment analysis, Western blotting and ImageStream. Results: Following treatment with 100 nM of asprosin, the serous OvCa cell line, SKOV-3, displayed 160 and 173 gene regulatory changes, at 4 and 12 h respectively, when compared with control samples (p < 0.05 and Log2FC > 1). In addition to energy metabolism and glucose-related pathways, asprosin was shown to alter pathways associated with cell communication, TGF-β signalling, and cell proliferation. Moreover, asprosin was shown to induce phosphorylation of ERK1/2 in the same in vitro model. Using liquid biopsies, we also report for novel expression of asprosin's predicted receptors OR4M1 and TLR4 in cancer-associated circulating cells; with significant reduction seen between pre-chemotherapy and end of first line chemotherapy, in addition to patients under maintenance with bevacizumab +/− olaparib for OR4M1. Conclusions: In relation to OvCa, asprosin appears to regulate numerous signalling pathways in-vitro. The prognostic potential of OR4M1 in liquid biopsies should also be explored further. [ABSTRACT FROM AUTHOR]
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- 2022
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7. ACBD3 Bioinformatic Analysis and Protein Expression in Breast Cancer Cells.
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Houghton-Gisby, Jack, Kerslake, Rachel, Karteris, Emmanouil, Mokbel, Kefah, and Harvey, Amanda J.
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BREAST , *PROTEIN analysis , *PROTEIN expression , *BREAST cancer , *CANCER cells , *BREAST cancer prognosis - Abstract
ACBD3 overexpression has previously been found to correlate with worse prognosis for breast cancer patients and, as an incredibly diverse protein in both function and cellular localisation, ACBD3 may have a larger role in breast cancer than previously thought. This study further investigated ACBD3′s role in breast cancer. Bioinformatic databases were queried to characterise ACBD3 expression and mutation in breast cancer and to investigate how overexpression affects breast cancer patient outcomes. Immunohistochemistry was carried out to examine ACBD3 location within cells and tissue structures. ACBD3 was more highly expressed in breast cancer than in any other cancer or matched normal tissue, and expression over the median level resulted in reduced relapse-free, overall, and distant metastasis-free survival for breast cancer patients as a whole, with some differences observed between subtypes. IHC analysis found that ACBD3 levels varied based on hormone receptor status, indicating that ACBD3 could be a candidate biomarker for poor patient prognosis in breast cancer and may possibly be a biomarker for ER signal reprogramming of precancerous breast tissue. [ABSTRACT FROM AUTHOR]
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- 2022
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8. Impact of Environmentally Relevant Concentrations of Bisphenol A (BPA) on the Gene Expression Profile in an In Vitro Model of the Normal Human Ovary.
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Zahra, Aeman, Kerslake, Rachel, Kyrou, Ioannis, Randeva, Harpal S., Sisu, Cristina, and Karteris, Emmanouil
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GENE expression profiling , *OVARIES , *ENDOCRINE disruptors , *OVARIAN diseases , *CELLULAR aging , *MEIOSIS - Abstract
Endocrine-disrupting chemicals (EDCs), including the xenoestrogen Bisphenol A (BPA), can interfere with hormonal signalling. Despite increasing reports of adverse health effects associated with exposure to EDCs, there are limited data on the effect of BPA in normal human ovaries. In this paper, we present a detailed analysis of the transcriptomic landscape in normal Human Epithelial Ovarian Cells (HOSEpiC) treated with BPA (10 and 100 nM). Gene expression profiles were determined using high-throughput RNA sequencing, followed by functional analyses using bioinformatics tools. In total, 272 and 454 differentially expressed genes (DEGs) were identified in 10 and 100 nM BPA-treated HOSEpiCs, respectively, compared to untreated controls. Biological pathways included mRNA surveillance pathways, oocyte meiosis, cellular senescence, and transcriptional misregulation in cancer. BPA exposure has a considerable impact on 10 genes: ANAPC2, AURKA, CDK1, CCNA2, CCNB1, PLK1, BUB1, KIF22, PDE3B, and CCNB3, which are also associated with progesterone-mediated oocyte maturation pathways. Future studies should further explore the effects of BPA and its metabolites in the ovaries in health and disease, making use of validated in vitro and in vivo models to generate data that will address existing knowledge gaps in basic biology, hazard characterisation, and risk assessment associated with the use of xenoestrogens such as BPA. [ABSTRACT FROM AUTHOR]
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- 2022
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9. Co-expression of peripheral olfactory receptors with SARS-CoV-2 infection mediators: Potential implications beyond loss of smell as a COVID-19 symptom.
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Kerslake, Rachel, Hall, Marcia, Randeva, Harpal S., Spandidos, Demetrios A., Chatha, Kamaljit, Kyrou, Ioannis, and Karteris, Emmanouil
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- 2020
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10. Investigation of training and support needs in rural and remote disability and mainstream service providers: implications for an online training model.
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Johnsson, Genevieve, Kerslake, Rachel, Crook, Sarah, and Cribb, Corinne
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MEDICAL personnel , *ALTERNATIVE education , *AUTISM , *CLINICAL competence , *CONFIDENCE , *LEARNING strategies , *PROFESSIONAL employee training , *RESEARCH funding , *RURAL health , *SURVEYS - Abstract
Objectives. It is known that there are difficulties in recruiting and retaining practitioners in rural and remote communities and that access to support and professional development can be key in breaking this cycle. Technology provides a possible solution not only for increasing access to these opportunities, but also in building community capacity to support children with autism. The aim of the present study was to investigate the current learning and support needs within rural and remote professionals prior to setting up a model of support. Methods. An online survey was used to gather information from service providers in rural and remote communities on their demographics, current skills and confidence in working with clients on the autism spectrum, current supervision and professional development, identified learning and support needs, and the availability and uptake of technology for accessing professional development. Results. Respondents reported below average levels of perceived confidence and skills when working with children with autism, most notably children with challenging behaviour. Half the respondents do not currently attend supervision sessions, with only 15% receiving regular supervision (fortnightly or more often), and 66% of respondents had travelled more than 3 h to access professional development workshops. The majority of participants had access to technology and over half had already used this for online training. Conclusion. Overall, service providers in rural and remote areas are generally not currently meeting their needs in terms of frequency of supervision and professional development. The present needs analysis identifies key areas for learning, the ideal frequency of support and the acceptability of using technology to deliver this support. This information will guide future researchers in the development of an evidence-based model that will be accessible and meaningful to its participants. [ABSTRACT FROM AUTHOR]
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- 2017
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11. Protein expression of transmembrane protease serine 4 in the gastrointestinal tract and in healthy, cancer, and SARS-CoV-2 infected lungs.
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Kerslake, Rachel, Randeva, Harpal S., Jonigk, Danny, Werlein, Christopher, Robertus, Jan L., Katopodis, Periklis, Jasker, Petra, Spandidos, Demetrios A., Kyrou, Ioannis, and Karteris, Emmanouil
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LUNGS , *SARS-CoV-2 , *GASTROINTESTINAL system , *PROTEIN expression , *COVID-19 , *MEMBRANE proteins - Abstract
In addition to the angiotensin-converting enzyme 2 (ACE2), a number of host cell entry mediators have been identified for severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2), including transmembrane protease serine 4 (TMPRSS4). The authors have recently demonstrated the upregulation of TMPRSS4 in 11 different cancers, as well as its specific expression within the central nervous system using in silico tools. The present study aimed to expand the initial observations and, using immunohistochemistry, TMPRSS4 protein expression in the gastrointestinal (GI) tract and lungs was further mapped. Immunohistochemistry was performed on tissue arrays and lung tissues of patients with non-small cell lung cancer with concurrent coronavirus disease 2019 (COVID-19) infection using TMPRSS4 antibody. The results revealed that TMPRSS4 was abundantly expressed in the oesophagus, stomach, small intestine, jejunum, ileum, colon, liver and pancreas. Moreover, the extensive TMPRSS4 protein expression in the lungs of a deceased patient with COVID-19 with chronic obstructive pulmonary disease and bronchial carcinoma, as well in the adjacent normal tissue, was demonstrated for the first time, at least to the best of our knowledge. On the whole, the immunohistochemistry data of the present study suggest that TMPRSS4 may be implicated in the broader (pulmonary and extra-pulmonary) COVID-19 symptomatology; thus, it may be responsible for the tropism of this coronavirus both in the GI tract and lungs. [ABSTRACT FROM AUTHOR]
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- 2022
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12. Differential Expression of RAD51AP1 in Ovarian Cancer: Effects of siRNA In Vitro.
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Filipe, Alice, Katopodis, Periklis, Chudasama, Dimple, Kerslake, Rachel, Jeyaneethi, Jeyarooban, Anikin, Vladimir, Silva, Elisabete, Kyrou, Ioannis, Randeva, Harpal S., Sisu, Cristina, Hall, Marcia, and Karteris, Emmanouil
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OVARIES ,DOUBLE-strand DNA breaks ,OVARIAN cancer ,TYPE 2 diabetes ,SMALL interfering RNA - Abstract
Background: DNA double strand breaks can affect genome integrity potentially leading to cancer. RAD51-associated protein 1 (RAD51AP1), an accessory protein to RAD51, is critical for homologous recombination, a key DNA damage response pathway. Emerging studies indicate a novel role for RAD51AP1 in carcinogenesis. Here we provide additional insight into the role of RAD51AP1 in ovarian cancer (OvCa). Methods: Gene expression and patient phenotype data were obtained from TCGA and GTEX project consortia for bioinformatics analysis. Immunohistochemistry of OvCa tissue microarray was undertaken. Functional analyses were performed in a SKOV3 OvCa cell line with down-regulation of RAD51AP1 using siRNA. Results: RAD51AP1 is overexpressed at gene level in primary and recurrent OvCa compared to controls. At protein level, RAD51AP1 was up-regulated in low grade serous tumors compared to high grade OvCa. There was higher expression of RAD51AP1 in OvCa metastatic to lymph nodes compared to primary cancer samples. Gene enrichment analyses identified 12 differentially expressed genes (DEGs) related to OvCa, eight of which are also common in tissue from patients with type 2 diabetes mellitus (T2DM). Conclusions: RAD51AP1 is overexpressed in OvCa, Given the link between OvCa and T2DM, the eight-gene signature shows potential for predictive value. [ABSTRACT FROM AUTHOR]
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- 2022
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13. A pancancer overview of FBN1, asprosin and its cognate receptor OR4M1 with detailed expression profiling in ovarian cancer.
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Kerslake, Rachel, Hall, Marcia, Vagnarelli, Paola, Jeyaneethi, Jeyarooban, Randeva, Harpal S., Pados, George, Kyrou, Ioannis, and Karteris, Emmanouil
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OVARIAN cancer , *OLFACTORY receptors , *TUMOR microenvironment , *MUCINOUS adenocarcinoma , *IMMUNOSTAINING - Abstract
Ovarian cancer affects >295,000 women worldwide and is the most lethal of gynaecological malignancies. Often diagnosed at a late stage, current research efforts seek to further the molecular understanding of its aetiopathogenesis and the development of novel biomarkers. The present study investigated the expression levels of the glucogenic hormone asprosin [encoded by fibrillin-1 (FBN1)], and its cognate receptor, olfactory receptor 4M1 (OR4M1), in ovarian cancer. A blend of in silico open access The Cancer Genome Atlas data, as well as in vitro reverse transcription-quantitative PCR (RT-qPCR), immunohistochemistry and immunofluorescence data were used. RT-qPCR revealed expression levels of OR4M1 and FBN1 in clinical samples and in ovarian cancer cell lines (SKOV-3, PEO1, PEO4 and MDAH-2774), as well as the normal human ovarian surface epithelial cell line (HOSEpiC). Immunohistochemical staining of a tissue microarray was used to identify the expression levels of OR4M1 and asprosin in ovarian cancer samples of varying histological subtype and grade, including clear cell carcinoma, serous ovarian cancer and mucinous adenocarcinoma. Immunofluorescence analysis revealed asprosin expression in SKOV-3 and HOSEpiC cells. These results demonstrated the expression of both asprosin and OR4M1 in normal and malignant human ovarian tissues. This research invokes further investigation to advance the understanding of the role of asprosin and OR4M1 within the ovarian tumour microenvironment. [ABSTRACT FROM AUTHOR]
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- 2021
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14. COVID-19 and SARS-CoV-2 host cell entry mediators: Expression profiling of TMRSS4 in health and disease.
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Katopodis, Periklis, Kerslake, Rachel, Davies, Julie, Randeva, Harpal S., Chatha, Kamaljit, Hall, Marcia, Spandidos, Demetrios A., Anikin, Vladimir, Polychronis, Andreas, Robertus, Jan L., Kyrou, Ioannis, and Karteris, Emmanouil
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- 2021
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