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1. Determining an approximate minimum toxic dosage of diphacinone in horses and corresponding serum, blood, and liver diphacinone concentrations: a pilot study

Author

Romano, Megan C, Francis, Kyle A, Janes, Jennifer G, Poppenga, Robert H, Filigenzi, Michael S, Stefanovski, Darko, and Gaskill, Cynthia L

Subjects
Veterinary Sciences, Agricultural, Veterinary and Food Sciences, Digestive Diseases, Prevention, Liver Disease, Animals, Anticoagulants, Horses, Liver, Phenindione, Pilot Projects, Rodenticides, Serum, anticoagulants, diphacinone, horses, pesticides, rodenticides, Zoology, Veterinary sciences
Abstract

Poisoning of nontarget species is a major concern with the use of anticoagulant rodenticides (ARs). At postmortem examination, differentiating toxicosis from incidental exposure is sometimes difficult. Clotting profiles cannot be performed on postmortem samples, and clinically significant serum, blood, and liver AR concentrations are not well-established in most species. We chose diphacinone for our study because, at the time, it was the publicly available AR most commonly detected in samples analyzed at the University of Kentucky Veterinary Diagnostic Laboratory. We determined an approximate minimum toxic dosage (MTD) of oral diphacinone in 3 horses and measured corresponding serum, blood, and liver diphacinone concentrations. Diphacinone was administered orally to healthy horses. Prothrombin time (PT), activated partial thromboplastin time (aPTT), and serum and blood diphacinone concentrations were measured daily. At the study endpoint, the horses were euthanized, and diphacinone concentration was measured in each liver lobe. The horse that received 0.2 mg/kg diphacinone developed prolonged (>1.5× baseline) PT and aPTT; the horse that received 0.1 mg/kg did not. This suggests an approximate oral MTD in horses of 0.2 mg/kg diphacinone. Median liver diphacinone concentration at this dosage was 1,780 (range: 1,590-2,000) ppb wet weight. Marginal (model-adjusted) mean diphacinone concentrations of liver lobes were not significantly different from one another (p = NS). Diphacinone was present in similar concentrations in both serum and blood at each time after administration, indicating that both matrices are suitable for detection of diphacinone exposure in horses.

Published
2022

2. Regional perturbation of gene transcription is associated with intrachromosomal rearrangements and gene fusion transcripts in high grade ovarian cancer.

Author

Krzyzanowski, Paul, Sircoulomb, Fabrice, Yousif, Fouad, Normand, Josee, La Rose, Jose, E Francis, Kyle, Suarez, Fernando, Beck, Tim, McPherson, John, Stein, Lincoln, and Rottapel, Robert

Abstract

Genomic rearrangements are a hallmark of cancer biology and progression, allowing cells to rapidly transform through alterations in regulatory structures, changes in expression patterns, reprogramming of signaling pathways, and creation of novel transcripts via gene fusion events. Though functional gene fusions encoding oncogenic proteins are the most dramatic outcomes of genomic rearrangements, we investigated the relationship between rearrangements evidenced by fusion transcripts and local expression changes in cancer using transcriptome data alone. 9,953 gene fusion predictions from 418 primary serious ovarian cancer tumors were analyzed, identifying depletions of gene fusion breakpoints within coding regions of fused genes as well as an N-terminal enrichment of breakpoints within fused genes. We identified 48 genes with significant fusion-associated upregulation and furthermore demonstrate that significant regional overexpression of intact genes in patient transcriptomes occurs within 1 megabase of 78 novel gene fusions that function as central markers of these regions. We reveal that cancer transcriptomes select for gene fusions that preserve protein and protein domain coding potential. The association of gene fusion transcripts with neighboring gene overexpression supports rearrangements as mechanism through which cancer cells remodel their transcriptomes and identifies a new way to utilize gene fusions as indicators of regional expression changes in diseased cells with only transcriptomic data.

Published
2019

4. Characterisation of checkpoint kinase 1 and 2 in ovarian cancer

Author

Francis, Kyle Evan, Langdon, Simon, and Harrison, David

Subjects
616.99, ovarian cancer, CHEK1, CHEK2, DNA damage response
Abstract

CHEK1 inhibitors are currently in clinical trials for their ability to abrogate chemotherapy-induced CHEK1 activation and S phase arrest resulting in cancer cell apoptosis. No studies have yet identified ovarian cancers that could benefit from CHEK1-targeting therapy. I hypothesised that knowledge of CHEK1 and CHEK2 signalling in the DNA damage response can assist in identifying potential biomarkers for platinum responsiveness and CHEK-targeting therapy in ovarian cancer. In vitro studies investigated the CHEK1/2 inhibitor AZD7762 (AZD) and cisplatin (CP) in same patient-derived platinum-sensitive/resistant high-grade serous ovarian cancer cell lines (PEO1/PEO4 and PEO14/PEO23). Cytotoxicity assays confirmed higher CP IC50’s for PEO4 and PEO23 relative to PEO1 and PEO14 cell lines, respectively. AZD was more toxic to PEO1 cells and an additive effect of AZD with CP relative to CP alone was seen. A nontoxic AZD treatment to PEO4 cells sensitised the cells to CP when applied in combination. PEO14 and PEO23 cells had similar cytotoxicity profiles for combination treatments. BRDU DNA synthesis assays and cell cycle analysis revealed increased BRDU incorporation and accumulation in S phase when all cell lines were treated with CP. AZD treatment had a similar effect in PEO14 and PEO23 cells and increased the sub-G1 population, a marker of apoptotic DNA fragmentation, relative to control. Drug combination had no major effect on cell cycle distributions of both PEO14 and PEO23 cells relative to single agents but resulted in BRDU incorporation levels below CP and control levels for PEO14 cells. In PEO1 and PEO4 cells, AZD did not affect the cell cycle or DNA synthesis levels relative to control. Drug combination did not alter the cell cycle relative to CP treatment for PEO1 cells but decreased S phase and increased G2/M and sub-G1 populations in PEO4 cells. This was coupled with a decrease of CP-induced BRDU levels in PEO4 control levels. Apoptotic PARP cleavage/total PARP occurred early in CP treated PEO1 and PEO14 cells. A surrogate CHEK1/2 activity marker, p-CDC2 (Y15), decreased in all lines treated with AZD relative to control. Within PEO1 and PEO4 cells, greatest PARP cleavage was observed with combination treatment and coincided with high p-H2AX (S139), a DNA damage marker. p-CHEK1 (S317) and p-CHEK2 (T68), both ATR and ATM phosphorylation sites during DNA damage, increased for lone drug treatment and, to a greater extent, the combination drug treatments. PARP cleavage occurs across all treatments in PEO1 cells while it only occurs in the combination treatment for PEO4 cells. The latter coincides with a decrease in p-CHEK1 (S296) a CHEK1 autophosphorylation site, p-TP53 (S15), and p-BRCA1 (S1524), a homologous recombination marker, relative to the CP treated sample. In PEO14 and PEO23 cells, lone AZD and combination treatments had similar cleaved PARP/total PARP levels compared to the PEO14 CP treated cells. This was coupled with increased p-H2AX (S139), decreased CHEK1, and decreased CHEK2 autophosphorylation p-CHEK2 (S516). A human ovarian cancer xenograft model identified increases in p-H2AX (S139), CHEK1, p-CHEK1 (S317), p-CHEK2 (T68), and p-BRCA1 (S1524) in the carboplatin responsive cancers. In the paired pre- and post-chemotherapy human ovarian cancer samples, p-CHEK1 (S317) was elevated in post-chemotherapy responsive samples. In the first cohort, high p-CHEK1 (S317) was an independent poor overall survival biomarker and correlated with high p-H2AX (S139), MYC, p-CHEK1 (S296), p-CHEK2 (T68), p-CHEK2 (S516), and p-TP53 (S15). p-CHEK1 (S317) was associated with poor overall survival in serous ovarian cancers within the second pre-treatment ovarian cancer cohort. In conclusion, AZD can induce apoptosis in CP resistant cancer cells by synergising with CP to abrogate the S phase checkpoint, increase DNA damage, and inhibit CHEK1, and BRCA1 function. As a single agent, AZD can induce apoptosis by decreasing CHEK1 levels and CHEK2 activity. p- CHEK1 (S317) is a platinum responsive / poor prognostic biomarker.

Published
2016

7. Inhibition of relaxin autocrine signaling confers therapeutic vulnerability in ovarian cancer

Author

Burston, Helen E., Kent, Oliver A., Communal, Laudine, Udaskin, Molly L., Sun, Ren X., Brown, Kevin R., Jung, Euihye, Francis, Kyle E., La Rose, Jose, Lowitz, Joshua, Drapkin, Ronny, Mes-Masson, Anne-Marie, and Rottapel, Robert

Subjects
Relaxin -- Health aspects, Cellular signal transduction -- Genetic aspects -- Health aspects, Ovarian cancer -- Genetic aspects -- Development and progression -- Care and treatment, Health care industry
Abstract

Ovarian cancer (OC) is the most deadly gynecological malignancy, with unmet clinical need for new therapeutic approaches. The relaxin peptide is a pleiotropic hormone with reproductive functions in the ovary. Relaxin induces cell growth in several types of cancer, but the role of relaxin in OC is poorly understood. Here, using cell lines and xenograft models, we demonstrate that relaxin and its associated GPCR RXFP1 form an autocrine signaling loop essential for OC in vivo tumorigenesis, cell proliferation, and viability. We determined that relaxin signaling activates expression of prooncogenic pathways, including RHO, MAPK, Wnt, and Notch. We found that relaxin is detectable in patient-derived OC tumors, ascites, and serum. Further, inflammatory cytokines IL-6 and TNF-[alpha] activated transcription of relaxin via recruitment of STAT3 and NF-[kappa]B to the proximal promoter, initiating an autocrine feedback loop that potentiated expression. Inhibition of RXFP1 or relaxin increased cisplatin sensitivity of OC cell lines and abrogated in vivo tumor formation. Finally, we demonstrate that a relaxin-neutralizing antibody reduced OC cell viability and sensitized cells to cisplatin. Collectively, these data identify the relaxin/RXFP1 autocrine loop as a therapeutic vulnerability in OC., Introduction Ovarian cancer (OC) has the highest mortality rate of all gynecological malignancies. High-grade serous ovarian carcinoma (HGSOC) is the most common and aggressive subtype, with a dismal 5-year survival [...]

Published
2021
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8. The Correlation of Papanicolaou Smears and Clinical Features to Identify the Common Risk Factors for Cervical Cancer: A Retrospective and Descriptive Study from a Tertiary Care Hospital in Trinidad

Author

Umakanthan, Srikanth, primary, Bukelo, Maryann M., additional, Ghany, Saudah, additional, Gay, La Donna, additional, Gilkes, Tia, additional, Freeman, Jamila, additional, Francis, Andre, additional, Francis, Kyle, additional, Gajadhar, Gabriel, additional, and Fraser, Junea, additional

Published
2023
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10. Comprehensive Evaluation of an HPLC–MS-MS Method for Quantitation of Seven Anti-Coagulant Rodenticides and Dicoumarol in Animal Serum.

Author

Francis, Kyle A, Tkachenko, Andriy, Johnson, Joseph T, Smith, Lori L, Noonan, Robyn T, Filigenzi, Michael S, Gaskill, Cynthia L, and Romano, Megan C

Subjects
*ELECTROSPRAY ionization mass spectrometry, *LIQUID chromatography-mass spectrometry, *RODENTICIDES, *ANTICOAGULANTS, *RODENT populations, *EVALUATION methodology, *ACETONE
Abstract

Anti-coagulant rodenticides (ARs) are commonly utilized for controlling rodent populations; however, non-target companion and wildlife animals are also exposed. A method was developed for quantitation of seven ARs (chlorophacinone, coumachlor, bromadiolone, brodifacoum, difethialone, diphacinone and warfarin) and dicoumarol (a naturally occurring anti-coagulant) in animal serum. Analytes were extracted with 10% (v/v) acetone in methanol and analyzed by reverse phase high-performance liquid chromatography–tandem mass spectrometry using electrospray ionization (negative mode) combined with multiple reaction monitoring. In-house method validation in the originating laboratory using non-blinded samples revealed method limits of quantitation at 2.5 ng/mL for all analytes. The inter-assay accuracy ranged from 99% to 104%, and the relative standard deviation ranged from 3.5% to 20.5%. Method performance was then verified in the originating laboratory during an exercise organized by an independent party using blinded samples. The method was successfully transferred to two naïve laboratories and further evaluated for reproducibility among three laboratories by means of Horwitz ratio (HorRat(R)) values. Such extensive validation provides a high degree of confidence that the method is rugged, robust, and will perform as expected if used by others in the future. [ABSTRACT FROM AUTHOR]

Published
2023
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11. The Correlation of Papanicolaou Smears and Clinical Features to Identify the Common Risk Factors for Cervical Cancer: a Retrospective and Descriptive Study From a Tertiary Care Hospital in Trinidad

Author

Umakanthan, Srikanth, primary, Ghany, Saudah, additional, Gay, La Donna, additional, Gilkes, Tia, additional, Freeman, Jamila, additional, Francis, Andre, additional, Francis, Kyle, additional, Gajadhar, Gabriel, additional, and Fraser, Junea, additional

Published
2022
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15. Feasibility Study on Establishment of More Pancit Canton at Heroesville 3, Gaya Gaya, San Jose del Monte, Bulacan

Author

Ong, Salvador, Remarca, Charity, Magsael, Leomer Jay, Legaspi, Francis Kyle, Fermia, Janromano, Orden, Kevin, Bangalisan, Reynold, Ong, Salvador, Remarca, Charity, Magsael, Leomer Jay, Legaspi, Francis Kyle, Fermia, Janromano, Orden, Kevin, and Bangalisan, Reynold

Abstract

More Pancit Canton wants to penetrate the market, meet the demand of the customers, and satisfy the potential customers. More Pancit Canton will serve high-quality services to easily reach the customers and vice versa. Hence, the researchers conducted this study. First, due to the seeking of feasible strategy for descriptive research design, secondary data from books and the Internet were used. Second, the financial statement was analyzed concerning the areas if it is profitable. The business used a survey questionnaire to obtain the valid primary data of 50 respondents and guided with SWOT analysis. The gathered data from the respondents showed that the potential customers love the business and are in favor of ages 18 and above. Second, the secondary data from books and the Internet were used to get more information such as from foreign and local related studies, history, and the updated sales forecast of the product. Third, the financial statement’s general purpose is to provide information about the result of the operation, that is, the return of investment (ROI). The ROI is 13.63% in 2019, 8.90% in 2020, 13.63% in 2021, 19.08% in 2022, and 25.35% in 2023. This study recommended the following. The owners need to continuously improve what the business offers and its promos to meet people’s satisfaction, which changes over time. This is a good strategy to catch every customer’s attention and loyalty. The researchers need to be aware of the latest technology and be able to compete with other companies.

Published
2020

16. A Novel Role for NUAK1 in Promoting Ovarian Cancer Metastasis through Regulation of Fibronectin Production in Spheroids

Author

Fritz, Jamie Lee, primary, Collins, Olga, additional, Saxena, Parima, additional, Buensuceso, Adrian, additional, Ramos Valdes, Yudith, additional, Francis, Kyle E., additional, Brown, Kevin R., additional, Larsen, Brett, additional, Colwill, Karen, additional, Gingras, Anne-Claude, additional, Rottapel, Robert, additional, and Shepherd, Trevor G., additional

Published
2020
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18. Regional perturbation of gene transcription is associated with intrachromosomal rearrangements and gene fusion transcripts in high grade ovarian cancer.

Author

Krzyzanowski, Paul M, Krzyzanowski, Paul M, Sircoulomb, Fabrice, Yousif, Fouad, Normand, Josee, La Rose, Jose, E Francis, Kyle, Suarez, Fernando, Beck, Tim, McPherson, John D, Stein, Lincoln D, Rottapel, Robert K, Krzyzanowski, Paul M, Krzyzanowski, Paul M, Sircoulomb, Fabrice, Yousif, Fouad, Normand, Josee, La Rose, Jose, E Francis, Kyle, Suarez, Fernando, Beck, Tim, McPherson, John D, Stein, Lincoln D, and Rottapel, Robert K

Abstract

Genomic rearrangements are a hallmark of cancer biology and progression, allowing cells to rapidly transform through alterations in regulatory structures, changes in expression patterns, reprogramming of signaling pathways, and creation of novel transcripts via gene fusion events. Though functional gene fusions encoding oncogenic proteins are the most dramatic outcomes of genomic rearrangements, we investigated the relationship between rearrangements evidenced by fusion transcripts and local expression changes in cancer using transcriptome data alone. 9,953 gene fusion predictions from 418 primary serious ovarian cancer tumors were analyzed, identifying depletions of gene fusion breakpoints within coding regions of fused genes as well as an N-terminal enrichment of breakpoints within fused genes. We identified 48 genes with significant fusion-associated upregulation and furthermore demonstrate that significant regional overexpression of intact genes in patient transcriptomes occurs within 1 megabase of 78 novel gene fusions that function as central markers of these regions. We reveal that cancer transcriptomes select for gene fusions that preserve protein and protein domain coding potential. The association of gene fusion transcripts with neighboring gene overexpression supports rearrangements as mechanism through which cancer cells remodel their transcriptomes and identifies a new way to utilize gene fusions as indicators of regional expression changes in diseased cells with only transcriptomic data.

Published
2019

21. Abstract A17: NUAK1 acts as a growth suppressor in epithelial ovarian cancer

Author

Saxena, Parima, primary, Collins, Olga, additional, Valdes, Yudith Ramos, additional, Buensuceso, Adrian, additional, Francis, Kyle, additional, Brown, Kevin, additional, Colwill, Karen, additional, Gingras, Anne-Claude, additional, Rottapel, Robert, additional, DiMattia, Gabriel E., additional, and Shepherd, Trevor G., additional

Published
2018
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23. Dynamic modulation of phosphoprotein expression in ovarian cancer xenograft models

Author

Koussounadis, A, Langdon, Simon, Um, Inhwa, Kay, Charlene, Francis, Kyle, Harrison, David, Smith, V Anne, University of St Andrews. School of Medicine, University of St Andrews. School of Biology, University of St Andrews. Scottish Oceans Institute, University of St Andrews. Institute of Behavioural and Neural Sciences, University of St Andrews. Centre for Research into Ecological & Environmental Modelling, and University of St Andrews. Centre for Biological Diversity

Subjects
RC0254, Pacltaxel, SDG 3 - Good Health and Well-being, Ovarian cancer, RC0254 Neoplasms. Tumors. Oncology (including Cancer), Xenograft, DAS, Prognosis, Phosphoproteins, Carboplatin
Abstract

The authors thank Medical Research Scotland and the Scottish Funding Council. This work was su pported by Medical Research Scotland [FRG353 to V.A.S.]; the FP7 -­‐ Directorate -­‐ General for Research and Innovation of the European Commission [EU HEALTH -­‐ F4 -­‐ 2012 -­‐ 305033 to Coordinating Action Systems Medicine -­‐ D.J.H.]; the Chief Scientist Office of Scotland [D.J.H.], the Scottish Funding Council [D.J.H. and S.P.L.]. Health Canada Scholarship (Indspire) [KEF], Scottish Overseas Research Student Award Scheme (University of Edinburgh)[KEF] and the Three Fires Award (Wikwemikong Board of Education)[KEF]. Background: The dynamic changes that occur in protein expression after treatment of a cancer in vivo are poorly described. In this study we measure the effect of chemotherapy over time on the expression of a panel of proteins in ovarian cancer xenograft models. The objective was to identify phosphoprotein and other protein changes indicative of pathway activation that might link with drug response. Methods: Two xenograft models, platinum-responsive OV1002 and platinum-unresponsive HOX424, were used. Treatments were carboplatin and carboplatin-paclitaxel. Expression of 49 proteins over 14 days post treatment was measured by quantitative immunofluorescence and analysed by AQUA . Results: Carboplatin treatment in the platinum-sensitive OV1002 model triggered up-regulation of cell cycle, mTOR and DDR pathways, while at late time points WNT, invasion , EMT and MAPK pathways were modulated. Estrogen receptor-alpha (ESR1) and ERBB pathways were down-regulated early, within 24h from treatment administration. Combined carboplatin-paclitaxel treatment triggered a more extensive response in the OV1002 model modulating expression of 23 of 49 proteins. Therefore the cell cycle and DDR pathways showed similar or more pronounced changes than with carboplatin alone . In addition to expression of pS6 and pERK increasing, components of the AKT pathway were modulated with pAKT increasing while its regulator PTEN was down-regulated early. WNT signaling, EMT and invasion markers were modulated at later time points. Additional pathways were also observed with the NFκB and JAK/STAT pathways being up-regulated. ESR1 was down-regulated as was HER4, while further protein members of the ERB B pathway were upregulated late. By contrast, in the carboplatin-unresponsive HOX 424 xenograft, carboplatin only modulated expression of MLH1 while carboplatin-paclitaxel treatment modulated ESR1 and pMET. Publisher PDF

Published
2016
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30. Quantitation of fumonisin B1 and B2 in feed using FMOC pre-column derivatization with HPLC and fluorescence detection.

Author

Smith, Lori L., Francis, Kyle A., Johnson, Joseph T., and Gaskill, Cynthia L.

Subjects
*FUMONISINS, *HIGH performance liquid chromatography, *METHYL formate, *IMMUNOAFFINITY chromatography, *SOLID phase extraction
Abstract

Pre-column derivatization with 9-fluorenylmethyl chloroformate (FMOC-Cl) was determined to be effective for quantitation of fumonisins B 1 and B 2 in feed. Liquid-solid extraction, clean-up using immunoaffinity solid phase extraction chromatography, and FMOC-derivatization preceded analysis by reverse phase HPLC with fluorescence. Instrument response was unchanged in the presence of matrix, indicating no need to use matrix-matched calibrants. Furthermore, high method recoveries indicated calibrants do not need to undergo clean-up to account for analyte loss. Established method features include linear instrument response from 0.04–2.5 µg/mL and stable derivatized calibrants over 7 days. Fortified cornmeal method recoveries from 0.1–30.0 μg/g were determined for FB 1 (75.1%–109%) and FB 2 (96.0%–115.2%). Inter-assay precision ranged from 1.0%–16.7%. Method accuracy was further confirmed using certified reference material. Inter-laboratory comparison with naturally-contaminated field corn demonstrated equivalent results with conventional derivatization. These results indicate FMOC derivatization is a suitable alternative for fumonisins B 1 and B 2 quantitation in corn-based feeds. [ABSTRACT FROM AUTHOR]

Published
2017
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36. Dynamic modulation of phosphoprotein expression in ovarian cancer xenograft models

Author

Koussounadis, Antonis, Langdon, Simon P., Um, Inhwa, Kay, Charlene, Francis, Kyle E., Harrison, David J., and Smith, V. Anne

Subjects
Ovarian Neoplasms, Cancer Research, Paclitaxel, TOR Serine-Threonine Kinases, Xenograft, Cell Cycle, Apoptosis, Prognosis, Phosphoproteins, Xenograft Model Antitumor Assays, Neoplasm Proteins, Carboplatin, Gene Expression Regulation, Neoplastic, Mice, Oncology, Ovarian cancer, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, Genetics, Animals, Humans, Female, Research Article, Signal Transduction
Abstract

Background The dynamic changes that occur in protein expression after treatment of a cancer in vivo are poorly described. In this study we measure the effect of chemotherapy over time on the expression of a panel of proteins in ovarian cancer xenograft models. The objective was to identify phosphoprotein and other protein changes indicative of pathway activation that might link with drug response. Methods Two xenograft models, platinum-responsive OV1002 and platinum-unresponsive HOX424, were used. Treatments were carboplatin and carboplatin-paclitaxel. Expression of 49 proteins over 14 days post treatment was measured by quantitative immunofluorescence and analysed by AQUA. Results Carboplatin treatment in the platinum-sensitive OV1002 model triggered up-regulation of cell cycle, mTOR and DDR pathways, while at late time points WNT, invasion, EMT and MAPK pathways were modulated. Estrogen receptor-alpha (ESR1) and ERBB pathways were down-regulated early, within 24 h from treatment administration. Combined carboplatin-paclitaxel treatment triggered a more extensive response in the OV1002 model modulating expression of 23 of 49 proteins. Therefore the cell cycle and DDR pathways showed similar or more pronounced changes than with carboplatin alone. In addition to expression of pS6 and pERK increasing, components of the AKT pathway were modulated with pAKT increasing while its regulator PTEN was down-regulated early. WNT signaling, EMT and invasion markers were modulated at later time points. Additional pathways were also observed with the NFκB and JAK/STAT pathways being up-regulated. ESR1 was down-regulated as was HER4, while further protein members of the ERBB pathway were upregulated late. By contrast, in the carboplatin-unresponsive HOX 424 xenograft, carboplatin only modulated expression of MLH1 while carboplatin-paclitaxel treatment modulated ESR1 and pMET. Conclusions Thirteen proteins were modulated by carboplatin and a more robust set of changes by carboplatin-paclitaxel. Early changes included DDR and cell cycle regulatory proteins associating with tumor volume changes, as expected. Changes in ESR1 and ERBB signaling were also observed. Late changes included components of MAPK signaling, EMT and invasion markers and coincided in time with reversal in tumor volume reduction. These results suggest potential therapeutic roles for inhibitors of such pathways that may prolong chemotherapeutic effects. Electronic supplementary material The online version of this article (doi:10.1186/s12885-016-2212-6) contains supplementary material, which is available to authorized users.

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37. Equity arbitrage: The literal million-dollar difference in the sale of your dental practice.

Author

Francis, Kyle

Subjects
PRACTICE of dentistry, DENTISTS, ARBITRAGE, DENTAL economics, PRIVATE equity, DENTAL care
Abstract

The article states that by maximizing value of dental practice equity before and after its sale, equity arbitrage has become popular with the emergence of private equity investments in the dental industry. It mentions that during a merger wave, dental service organizations backed by private equity can combine the equity of multiple practices, resulting in higher financial returns. It suggests that dentists looking to explore equity arbitrage should seek the guidance of professional advisors.

Published
2022

38. Transitions Roundtable: We ask two experts the same question on a complex issue.

Author

WERHAN, J. HADEN and FRANCIS, KYLE

Subjects
DISCOUNTED cash flow, ACCOUNTANTS, VALUATION of corporations, PRACTICE of dentistry, DENTAL economics
Abstract

In this article the author talks to experts the same question on a complex issue and discussed their views. Topics discussed include The income approach uses three methods to determine the value of a business based on the future economic benefit to be derived by a buyer, and Discounted cash flow (DCF) and capitalized earnings are both effective, and both work in dentistry are methods rely completely on assumptions that can dramatically skew the implied value of a practice.

Published
2020

40. Measurement of the Feline Hippocampus Using Magnetic Resonance Imaging

Author

Francis, Kyle Andrew

Subjects
Veterinary Services, MRI, magnetic resonance imaging, hippocampus, feline, cat, FIC
Abstract

The human hippocampus has several unique attributes and is one of the more structurally discrete structures of the limbic system. Humans exposed to chronic stress or pain, most notably patients with posttraumatic stress disorder and chronic pelvic pain syndromes, have detectably smaller hippocampal structures. Interstitial cystitis (IC) in humans is a recognized syndrome of chronic pelvic pain. Feline interstitial cystitis (FIC) is a spontaneous animal model for IC. Therefore, documenting volume changes in the hippocampus in cats may lead to further understanding of chronic pain in all species. The aim of this study is to evaluate the feasibility of measuring the volume of the feline hippocampus using magnetic resonance imaging (MRI). Brain MRI of 3 cats (2 nonsymptomatic cats from an FIC colony and 1 normal cat from an unrelated study) was performed using 3 Tesla (T) and 7T MR systems. T2w images were made with extremity coils designed specifically for each magnet, and a smaller surface coil in the 7T magnet. Transverse, sagittal, and dorsal plane images were acquired in each imaging session. Cats were imaged in vivo, post perfusion fixation, and at various durations (4-181 days) of immersion fixation of the brain in 10% formalin using both magnets. DICOM images were imported into ImageJ and each hippocampus was manually outlined on all images. The areas were then multiplied by the image thickness (including spacing) and the area from each slice was summed to obtain a volume. The average measured in vivo hippocampal volume was 277.2 + 18.9 mm3 on the transverse images of the 3T system which equated to 1% of the total brain volume (each hippocampus). The average volumes obtained in the 3T system in the other planes were 228.0 + 47.2 mm3 on the sagittal images and 207.0 + 47.5 mm3 on the dorsal images. Average volumes obtained in vivo in the 7T system were 286.8 + 47.1 mm3 on the transverse images, 221.5 + 41.0 mm3 on the sagittal images, and 273.5 + 9.5 mm3 on the dorsal images. Detection of changes in volume of the hippocampus using MRI is possible in populations of cats, but not likely to be useful in individuals.

Published
2011

41. Mail Bag.

Author

Boylan, Barbara, Johnson, Joleana, McGraw, Noël, Carlson, Cindy, Kintz, Lisa, Francis, Kyle, Dunbar, Amy, and Colalucci, Victoria

Subjects
LETTERS to the editor
Abstract

Letters are presented from readers responding to content from prior issues including articles about actor Patrick Swayze, the family of actor John Travolta, and amputees Bill Hansbury and Jake Bainter.

Published
2009

43. Evaluation of a Diagnostic Method to Quantify Aflatoxins B1 and M1 in Animal Liver by High-Performance Liquid Chromatography with Fluorescence Detection.

Author

XIANGWEI DU, SCHRUNK, DWAYNE E., IMERMAN, PAULA M., SMITH, LORI, FRANCIS, KYLE, TAHARA, JOHN, TKACHENKO, ANDRIY, REIMSCHUESSEL, RENATE, and RUMBEIHA, WILSON K.

Subjects
*AFLATOXINS, *HIGH performance liquid chromatography, *FLUORESCENCE, *EVALUATION methodology, *FOOD recall, *METABOLITES, *LIVER analysis
Abstract

Background: Aflatoxins (AFs) are secondary metabolites of fungi and are one of the causes of toxin-related pet food recalls. An intralaboratory method was previously developed to quantify aflatoxin B1 (AFB1) and aflatoxin M1 (AFM1) in animal liver by HPLC with fluorescence detection. Objective: The aim of this study was to extensively evaluate the method performance with a single-laboratory blinded method test (BMT-S) and a multilaboratory blinded method test (BMT-M). Methods: Blinded tissue samples were prepared by a third-party laboratory and sent out to participating laboratories for both BMT-S and BMT-M. Results: In both tests, participants analyzed blinded samples prepared by an independent laboratory. In the BMT-S, accuracy ranged between 111 and 154% for AFB1 and 113 and 159% for AFM1 within the quantitation range of 0.1-0.5 ng/g. The HorRat values for repeatability ranged between 0.1 and 0.3 for AFB1 and 0.3 and 0.6 for AFM1. In the BMT-M, the interlaboratory accuracy ranged between 77 and 81% for AFB1 and 83 and 85% for AFM1 within the quantitation range of 0.2-10 ng/g. The HorRat values for reproducibility ranged between 0.4 and 0.7 for AFB1 and 0.4 and 0.9 for AFM1. Both recovery and reproducibility were acceptable. Conclusions: BMT-M evaluation demonstrated that the method was suitable for quantitation of aflatoxins B1 and M1 in animal liver between laboratories. Highlights: The BMT-S and BMT-M results demonstrated that the method is rugged and reproducible among the participating laboratories. [ABSTRACT FROM AUTHOR]

Published
2019
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44. Evaluation of a Diagnostic Method to Quantify Aflatoxins B 1 and M 1 in Animal Liver by High-Performance Liquid Chromatography with Fluorescence Detection.

Author

Du X, Schrunk DE, Imerman PM, Smith L, Francis K, Tahara J, Tkachenko A, Reimschuessel R, and Rumbeiha WK

Subjects
Animals, Fluorescence, Reproducibility of Results, Aflatoxin B1 analysis, Aflatoxin M1 analysis, Chromatography, High Pressure Liquid methods, Liver chemistry
Abstract

Background: Aflatoxins (AFs) are secondary metabolites of fungi and are one of the causes of toxin-related pet food recalls. An intralaboratory method was previously developed to quantify aflatoxin B 1 (AFB 1 ) and aflatoxin M 1 (AFM 1 ) in animal liver by HPLC with fluorescence detection. Objective: The aim of this study was to extensively evaluate the method performance with a single-laboratory blinded method test (BMT-S) and a multilaboratory blinded method test (BMT-M). Methods: Blinded tissue samples were prepared by a third-party laboratory and sent out to participating laboratories for both BMT-S and BMT-M. Results: In both tests, participants analyzed blinded samples prepared by an independent laboratory. In the BMT-S, accuracy ranged between 111 and 154% for AFB 1 and 113 and 159% for AFM 1 within the quantitation range of 0.1-0.5 ng/g. The HorRat values for repeatability ranged between 0.1 and 0.3 for AFB 1 and 0.3 and 0.6 for AFM 1 . In the BMT-M, the interlaboratory accuracy ranged between 77 and 81% for AFB 1 and 83 and 85% for AFM 1 within the quantitation range of 0.2-10 ng/g. The HorRat values for reproducibility ranged between 0.4 and 0.7 for AFB 1 and 0.4 and 0.9 for AFM 1 . Both recovery and reproducibility were acceptable. Conclusions: BMT-M evaluation demonstrated that the method was suitable for quantitation of aflatoxins B 1 and M 1 in animal liver between laboratories. Highlights: The BMT-S and BMT-M results demonstrated that the method is rugged and reproducible among the participating laboratories.

Published
2019
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