Your search keyword '"O'Flaherty, Linda"' showing total 27 results

1. Development of novel in vitro and in vivo models for determining primary events in HLRCC tumourigenesis

Author

O'Flaherty, Linda H., Ratcliffe, Peter, and Pollard, Patrick

Subjects

616.994, Oncology, Biology, Medical Sciences

Abstract

Germline mutations of fumarate hydratase (FH), encoding an enzyme of the tricarboxylic acid (TCA) cycle, predispose affected individuals to hereditary leiomyomatosis and renal cell cancer (HLRCC). FH-deficient cells and tissues have been shown to accumulate fumarate, exhibit S-(2-succinyl) cysteine (2SC) protein modifications and to constitutively express hypoxia-inducible factor alpha (HIF-1α and -2α), under normoxic conditions. This thesis presents a phenotypic characterisation of Fh1-/- mouse embryonic fibroblasts (MEFs), generated from previously reported conditional Fh1 knockout mice, as a new in vitro system for investigating and identifying biochemical and metabolic pathways that are dysregulated as a result of Fh1 inactivation. These cell lines reproduced the aforementioned phenotypes, in addition to an observed shift from oxidative phosphorylation (OXPHOS) to glycolytic metabolism. Re-expression of either full length, mitochondrial-targeted FH (Fh1-/- +FH) or cytoplasmic FH (Fh1-/- +FHΔMTS) in Fh1-deficient MEFs was sufficient to reduce intracellular fumarate and to correct for the dysregulation of the Hif pathway. These results were of particular interest as they demonstrated that normoxic stabilisation of Hif-1α occurs independently of the persistent mitochondrial defect observed in Fh1-/- +FHΔMTS MEFs. These findings were corroborated in vivo following the development of transgenic mouse models, ubiquitously expressing either FH or FHΔMTS in mice with targeted inactivation of Fh1 in renal tubular cells. Surprisingly, the cytoplasmic-restricted FH (FHΔMTS) transgene was just as efficient as the transgenic mice expressing mitochondrial-targeted FH at rescuing the cystic phenotype associated with Fh1-deficiency in the kidneys. As the function of cytoplasmic FH has remained poorly understood, these results go some way to extricating a role for this isoform of FH. The results of this thesis demonstrate that these novel in vitro and in vivo models, used either alone or in combination, are a versatile and robust paradigm for studying altered cell metabolism in not only HLRCC but other diseases associated with metabolic dysregulation.

Published

2012

2. Massage has no observable effect on distress in children with burns: A randomized, observer-blinded trial

Author

van Dijk, Monique, O’Flaherty, Linda Anne, Hoedemaker, Tessa, van Rosmalen, Joost, and Rode, Heinz

Published

2018

3. Data from Expression Profiling in Progressive Stages of Fumarate-Hydratase Deficiency: The Contribution of Metabolic Changes to Tumorigenesis

Author

Ashrafian, Houman, primary, O'Flaherty, Linda, primary, Adam, Julie, primary, Steeples, Violetta, primary, Chung, Yuen-Li, primary, East, Phil, primary, Vanharanta, Sakari, primary, Lehtonen, Heli, primary, Nye, Emma, primary, Hatipoglu, Emine, primary, Miranda, Melroy, primary, Howarth, Kimberley, primary, Shukla, Deepa, primary, Troy, Helen, primary, Griffiths, John, primary, Spencer-Dene, Bradley, primary, Yusuf, Mohammed, primary, Volpi, Emanuela, primary, Maxwell, Patrick H., primary, Stamp, Gordon, primary, Poulsom, Richard, primary, Pugh, Christopher W., primary, Costa, Barbara, primary, Bardella, Chiara, primary, Di Renzo, Maria Flavia, primary, Kotlikoff, Michael I., primary, Launonen, Virpi, primary, Aaltonen, Lauri, primary, El-Bahrawy, Mona, primary, Tomlinson, Ian, primary, and Pollard, Patrick J., primary

Published

2023

4. Supplementary Figure 1 from Expression Profiling in Progressive Stages of Fumarate-Hydratase Deficiency: The Contribution of Metabolic Changes to Tumorigenesis

Author

Ashrafian, Houman, primary, O'Flaherty, Linda, primary, Adam, Julie, primary, Steeples, Violetta, primary, Chung, Yuen-Li, primary, East, Phil, primary, Vanharanta, Sakari, primary, Lehtonen, Heli, primary, Nye, Emma, primary, Hatipoglu, Emine, primary, Miranda, Melroy, primary, Howarth, Kimberley, primary, Shukla, Deepa, primary, Troy, Helen, primary, Griffiths, John, primary, Spencer-Dene, Bradley, primary, Yusuf, Mohammed, primary, Volpi, Emanuela, primary, Maxwell, Patrick H., primary, Stamp, Gordon, primary, Poulsom, Richard, primary, Pugh, Christopher W., primary, Costa, Barbara, primary, Bardella, Chiara, primary, Di Renzo, Maria Flavia, primary, Kotlikoff, Michael I., primary, Launonen, Virpi, primary, Aaltonen, Lauri, primary, El-Bahrawy, Mona, primary, Tomlinson, Ian, primary, and Pollard, Patrick J., primary

Published

2023

5. Supplementary Methods from Expression Profiling in Progressive Stages of Fumarate-Hydratase Deficiency: The Contribution of Metabolic Changes to Tumorigenesis

Author

Ashrafian, Houman, primary, O'Flaherty, Linda, primary, Adam, Julie, primary, Steeples, Violetta, primary, Chung, Yuen-Li, primary, East, Phil, primary, Vanharanta, Sakari, primary, Lehtonen, Heli, primary, Nye, Emma, primary, Hatipoglu, Emine, primary, Miranda, Melroy, primary, Howarth, Kimberley, primary, Shukla, Deepa, primary, Troy, Helen, primary, Griffiths, John, primary, Spencer-Dene, Bradley, primary, Yusuf, Mohammed, primary, Volpi, Emanuela, primary, Maxwell, Patrick H., primary, Stamp, Gordon, primary, Poulsom, Richard, primary, Pugh, Christopher W., primary, Costa, Barbara, primary, Bardella, Chiara, primary, Di Renzo, Maria Flavia, primary, Kotlikoff, Michael I., primary, Launonen, Virpi, primary, Aaltonen, Lauri, primary, El-Bahrawy, Mona, primary, Tomlinson, Ian, primary, and Pollard, Patrick J., primary

Published

2023

6. Supplementary Table 1 from Expression Profiling in Progressive Stages of Fumarate-Hydratase Deficiency: The Contribution of Metabolic Changes to Tumorigenesis

Author

Ashrafian, Houman, primary, O'Flaherty, Linda, primary, Adam, Julie, primary, Steeples, Violetta, primary, Chung, Yuen-Li, primary, East, Phil, primary, Vanharanta, Sakari, primary, Lehtonen, Heli, primary, Nye, Emma, primary, Hatipoglu, Emine, primary, Miranda, Melroy, primary, Howarth, Kimberley, primary, Shukla, Deepa, primary, Troy, Helen, primary, Griffiths, John, primary, Spencer-Dene, Bradley, primary, Yusuf, Mohammed, primary, Volpi, Emanuela, primary, Maxwell, Patrick H., primary, Stamp, Gordon, primary, Poulsom, Richard, primary, Pugh, Christopher W., primary, Costa, Barbara, primary, Bardella, Chiara, primary, Di Renzo, Maria Flavia, primary, Kotlikoff, Michael I., primary, Launonen, Virpi, primary, Aaltonen, Lauri, primary, El-Bahrawy, Mona, primary, Tomlinson, Ian, primary, and Pollard, Patrick J., primary

Published

2023

7. Supplementary Figure 2 from Expression Profiling in Progressive Stages of Fumarate-Hydratase Deficiency: The Contribution of Metabolic Changes to Tumorigenesis

Author

Ashrafian, Houman, primary, O'Flaherty, Linda, primary, Adam, Julie, primary, Steeples, Violetta, primary, Chung, Yuen-Li, primary, East, Phil, primary, Vanharanta, Sakari, primary, Lehtonen, Heli, primary, Nye, Emma, primary, Hatipoglu, Emine, primary, Miranda, Melroy, primary, Howarth, Kimberley, primary, Shukla, Deepa, primary, Troy, Helen, primary, Griffiths, John, primary, Spencer-Dene, Bradley, primary, Yusuf, Mohammed, primary, Volpi, Emanuela, primary, Maxwell, Patrick H., primary, Stamp, Gordon, primary, Poulsom, Richard, primary, Pugh, Christopher W., primary, Costa, Barbara, primary, Bardella, Chiara, primary, Di Renzo, Maria Flavia, primary, Kotlikoff, Michael I., primary, Launonen, Virpi, primary, Aaltonen, Lauri, primary, El-Bahrawy, Mona, primary, Tomlinson, Ian, primary, and Pollard, Patrick J., primary

Published

2023

8. Aromatherapy massage seems effective in critically ill children:an observational before-after study

Author

van der Heijden, Marianne J E, O'Flaherty, Linda-Anne, van Rosmalen, Joost, de Vos, Simone, McCulloch, Mignon, van Dijk, Monique, van der Heijden, Marianne J E, O'Flaherty, Linda-Anne, van Rosmalen, Joost, de Vos, Simone, McCulloch, Mignon, and van Dijk, Monique

Abstract

Children treated in a pediatric intensive care unit (PICU) are at risk of distress and pain. This study investigated if aromatherapy massage can reduce children's distress and improve comfort. This observational before-after study was performed in a 22-bed PICU in Cape Town, South Africa. The aromatherapy massage consisted of soft massaging using the "M-technique" and a 1% blend of essential oils of Lavender (Lavandula angustifolia), German Chamomile (Matricatia recutita) and Neroli (Citrus aurantium) mixed with a grapeseed carrier oil. All present children were eligible, except those who had recently returned, were asleep or deemed unstable. The primary outcome was distress measured with the COMFORT-Behavior scale (COMFORT-B). Secondary outcomes were heart rate, oxygen saturation (SatO2), the Numeric Rating Scale (NRS)-Anxiety and pain assessed by the NRS-Pain scale. Outcomes variables were evaluated with Wilcoxon signed-rank test and multiple regression analysis. The intervention was applied to 111 children, fifty-one of whom (45.9%) were younger than three years old. The group median COMFORT-B score before intervention was 15 (IQR 12-19), versus 10 (IQR 6-14) after intervention. Heart rate and NRS-Anxiety were significantly lower after the intervention (P < 0.001). Multiple regression analysis showed that interrupted massages were less effective than the uninterrupted massages. Parental presence did not influence the outcome variables. We did not find a significant change on the NRS-Pain scale or for SatO2. Aromatherapy massage appears beneficial in reducing distress, as measured by the COMFORT-B scale, heart rate and the NRS-Anxiety scale, in critically ill children. Thus, the potential of aromatherapy in clinical practice deserves further consideration.

Published

2022

9. Aromatherapy massage seems to enhance relaxation in children with burns: An observational pilot study

Author

O’Flaherty, Linda-Anne, van Dijk, Monique, Albertyn, Rene, Millar, Alastair, and Rode, Heinz

Published

2012

10. Renal Cyst Formation in Fh1-Deficient Mice Is Independent of the Hif/Phd Pathway: Roles for Fumarate in KEAP1 Succination and Nrf2 Signaling

Author

Adam, Julie, Hatipoglu, Emine, O'Flaherty, Linda, Ternette, Nicola, Sahgal, Natasha, Lockstone, Helen, Baban, Dilair, Nye, Emma, Stamp, Gordon W., Wolhuter, Kathryn, Stevens, Marcus, Fischer, Roman, Carmeliet, Peter, Maxwell, Patrick H., Pugh, Chris W., Frizzell, Norma, Soga, Tomoyoshi, Kessler, Benedikt M., El-Bahrawy, Mona, Ratcliffe, Peter J., and Pollard, Patrick J.

Published

2011

11. Aromatherapy massage seems effective in critically ill children: an observational before‐after study

Author

van der Heijden, Marianne J. E., primary, O’Flaherty, Linda‐Anne, additional, van Rosmalen, Joost, additional, de Vos, Simone, additional, McCulloch, Mignon, additional, and van Dijk, Monique, additional

Published

2022

12. Determination of PD-L1 Expression in Circulating Tumor Cells of NSCLC Patients and Correlation with Response to PD-1/PD-L1 Inhibitors

Author

Janning, Melanie, primary, Kobus, Franca, additional, Babayan, Anna, additional, Wikman, Harriet, additional, Velthaus, Janna-Lisa, additional, Bergmann, Sonja, additional, Schatz, Stefanie, additional, Falk, Markus, additional, Berger, Lars-Arne, additional, Böttcher, Lisa-Marie, additional, Päsler, Sarina, additional, Gorges, Tobias M., additional, O’Flaherty, Linda, additional, Hille, Claudia, additional, Joosse, Simon A., additional, Simon, Ronald, additional, Tiemann, Markus, additional, Bokemeyer, Carsten, additional, Reck, Martin, additional, Riethdorf, Sabine, additional, Pantel, Klaus, additional, and Loges, Sonja, additional

Published

2019

13. Tumor growth suppression using a combination of taxol-based therapy and GSK3 inhibition in non-small cell lung cancer

Author

O’Flaherty, Linda, primary, Shnyder, Steven D., additional, Cooper, Patricia A., additional, Cross, Stephen J., additional, Wakefield, James G., additional, Pardo, Olivier E., additional, Seckl, Michael J., additional, and Tavaré, Jeremy M., additional

Published

2019

14. Development of novel in vitro and in vivo models for determining primary events in HLRCC tumourigenesis

Author

O'Flaherty, L, O'Flaherty, Linda, Peter Ratcliffe, P, and Patrick Pollard, P

Subjects

Medical Sciences, Oncology, Biology

Abstract

Germline mutations of fumarate hydratase (FH), encoding an enzyme of the tricarboxylic acid (TCA) cycle, predispose affected individuals to hereditary leiomyomatosis and renal cell cancer (HLRCC). FH-deficient cells and tissues have been shown to accumulate fumarate, exhibit S-(2-succinyl) cysteine (2SC) protein modifications and to constitutively express hypoxia-inducible factor alpha (HIF-1α and -2α), under normoxic conditions. This thesis presents a phenotypic characterisation of Fh1-/- mouse embryonic fibroblasts (MEFs), generated from previously reported conditional Fh1 knockout mice, as a new in vitro system for investigating and identifying biochemical and metabolic pathways that are dysregulated as a result of Fh1 inactivation. These cell lines reproduced the aforementioned phenotypes, in addition to an observed shift from oxidative phosphorylation (OXPHOS) to glycolytic metabolism. Re-expression of either full length, mitochondrial-targeted FH (Fh1-/- +FH) or cytoplasmic FH (Fh1-/- +FHΔMTS) in Fh1-deficient MEFs was sufficient to reduce intracellular fumarate and to correct for the dysregulation of the Hif pathway. These results were of particular interest as they demonstrated that normoxic stabilisation of Hif-1α occurs independently of the persistent mitochondrial defect observed in Fh1-/- +FHΔMTS MEFs. These findings were corroborated in vivo following the development of transgenic mouse models, ubiquitously expressing either FH or FHΔMTS in mice with targeted inactivation of Fh1 in renal tubular cells. Surprisingly, the cytoplasmic-restricted FH (FHΔMTS) transgene was just as efficient as the transgenic mice expressing mitochondrial-targeted FH at rescuing the cystic phenotype associated with Fh1-deficiency in the kidneys. As the function of cytoplasmic FH has remained poorly understood, these results go some way to extricating a role for this isoform of FH. The results of this thesis demonstrate that these novel in vitro and in vivo models, used either alone or in combination, are a versatile and robust paradigm for studying altered cell metabolism in not only HLRCC but other diseases associated with metabolic dysregulation.

Published

2017

15. Clinical applications of the CellSearch platform in cancer patients

Author

Riethdorf, Sabine, primary, O'Flaherty, Linda, additional, Hille, Claudia, additional, and Pantel, Klaus, additional

Published

2018

16. Biology and clinical significance of circulating tumor cell subpopulations in lung cancer

Author

O’Flaherty, Linda, primary, Wikman, Harriet, additional, and Pantel, Klaus, additional

Published

2017

17. Glycogen Synthase Kinase 3 Protein Kinase Activity Is Frequently Elevated in Human Non-Small Cell Lung Carcinoma and Supports Tumour Cell Proliferation

Author

Vincent, Emma E., primary, Elder, Douglas J. E., additional, O′Flaherty, Linda, additional, Pardo, Olivier E., additional, Dzien, Piotr, additional, Phillips, Lois, additional, Morgan, Carys, additional, Pawade, Joya, additional, May, Margaret T., additional, Sohail, Muhammad, additional, Hetzel, Martin R., additional, Seckl, Michael J., additional, and Tavaré, Jeremy M., additional

Published

2014

18. A Role for Cytosolic Fumarate Hydratase in Urea Cycle Metabolism and Renal Neoplasia

Author

Adam, Julie, primary, Yang, Ming, additional, Bauerschmidt, Christina, additional, Kitagawa, Mitsuhiro, additional, O’Flaherty, Linda, additional, Maheswaran, Pratheesh, additional, Özkan, Gizem, additional, Sahgal, Natasha, additional, Baban, Dilair, additional, Kato, Keiko, additional, Saito, Kaori, additional, Iino, Keiko, additional, Igarashi, Kaori, additional, Stratford, Michael, additional, Pugh, Christopher, additional, Tennant, Daniel A., additional, Ludwig, Christian, additional, Davies, Benjamin, additional, Ratcliffe, Peter J., additional, El-Bahrawy, Mona, additional, Ashrafian, Houman, additional, Soga, Tomoyoshi, additional, and Pollard, Patrick J., additional

Published

2013

19. Inhibition of Mitochondrial Aconitase by Succination in Fumarate Hydratase Deficiency

Author

Ternette, Nicola, primary, Yang, Ming, additional, Laroyia, Mahima, additional, Kitagawa, Mitsuhiro, additional, O’Flaherty, Linda, additional, Wolhulter, Kathryn, additional, Igarashi, Kaori, additional, Saito, Kaori, additional, Kato, Keiko, additional, Fischer, Roman, additional, Berquand, Alexandre, additional, Kessler, Benedikt M., additional, Lappin, Terry, additional, Frizzell, Norma, additional, Soga, Tomoyoshi, additional, Adam, Julie, additional, and Pollard, Patrick J., additional

Published

2013

20. Cells Lacking the Fumarase Tumor Suppressor Are Protected from Apoptosis through a Hypoxia-Inducible Factor-Independent, AMPK-Dependent Mechanism

Author

Bardella, Chiara, primary, Olivero, Martina, additional, Lorenzato, Annalisa, additional, Geuna, Massimo, additional, Adam, Julie, additional, O'Flaherty, Linda, additional, Rustin, Pierre, additional, Tomlinson, Ian, additional, Pollard, Patrick J., additional, and Di Renzo, Maria Flavia, additional

Published

2012

21. Aberrant succination of proteins in fumarate hydratase‐deficient mice and HLRCC patients is a robust biomarker of mutation status

Author

Bardella, Chiara, primary, El‐Bahrawy, Mona, additional, Frizzell, Norma, additional, Adam, Julie, additional, Ternette, Nicola, additional, Hatipoglu, Emine, additional, Howarth, Kimberley, additional, O'Flaherty, Linda, additional, Roberts, Ian, additional, Turner, Gareth, additional, Taylor, Jennifer, additional, Giaslakiotis, Konstantinos, additional, Macaulay, Valentine M, additional, Harris, Adrian L, additional, Chandra, Ashish, additional, Lehtonen, Heli J, additional, Launonen, Virpi, additional, Aaltonen, Lauri A, additional, Pugh, Christopher W, additional, Mihai, Radu, additional, Trudgian, David, additional, Kessler, Benedikt, additional, Baynes, John W, additional, Ratcliffe, Peter J, additional, Tomlinson, Ian P, additional, and Pollard, Patrick J, additional

Published

2011

22. Human AlkB Homologue 5 Is a Nuclear 2-Oxoglutarate Dependent Oxygenase and a Direct Target of Hypoxia-Inducible Factor 1α (HIF-1α)

Author

Thalhammer, Armin, primary, Bencokova, Zuzana, additional, Poole, Rachel, additional, Loenarz, Christoph, additional, Adam, Julie, additional, O'Flaherty, Linda, additional, Schödel, Johannes, additional, Mole, David, additional, Giaslakiotis, Konstantinos, additional, Schofield, Christopher J., additional, Hammond, Ester M., additional, Ratcliffe, Peter J., additional, and Pollard, Patrick J., additional

Published

2011

23. Expression Profiling in Progressive Stages of Fumarate-Hydratase Deficiency: The Contribution of Metabolic Changes to Tumorigenesis

Author

Ashrafian, Houman, primary, O'Flaherty, Linda, additional, Adam, Julie, additional, Steeples, Violetta, additional, Chung, Yuen-Li, additional, East, Phil, additional, Vanharanta, Sakari, additional, Lehtonen, Heli, additional, Nye, Emma, additional, Hatipoglu, Emine, additional, Miranda, Melroy, additional, Howarth, Kimberley, additional, Shukla, Deepa, additional, Troy, Helen, additional, Griffiths, John, additional, Spencer-Dene, Bradley, additional, Yusuf, Mohammed, additional, Volpi, Emanuela, additional, Maxwell, Patrick H., additional, Stamp, Gordon, additional, Poulsom, Richard, additional, Pugh, Christopher W., additional, Costa, Barbara, additional, Bardella, Chiara, additional, Di Renzo, Maria Flavia, additional, Kotlikoff, Michael I., additional, Launonen, Virpi, additional, Aaltonen, Lauri, additional, El-Bahrawy, Mona, additional, Tomlinson, Ian, additional, and Pollard, Patrick J., additional

Published

2010

24. Dysregulation of hypoxia pathways in fumarate hydratase-deficient cells is independent of defective mitochondrial metabolism

Author

O'Flaherty, Linda, primary, Adam, Julie, additional, Heather, Lisa C., additional, Zhdanov, Alexander V., additional, Chung, Yuen-Li, additional, Miranda, Melroy X., additional, Croft, Joanne, additional, Olpin, Simon, additional, Clarke, Kieran, additional, Pugh, Christopher W., additional, Griffiths, John, additional, Papkovsky, Dmitri, additional, Ashrafian, Houman, additional, Ratcliffe, Peter J., additional, and Pollard, Patrick J., additional

Published

2010

25. Tumor growth suppression using a combination of taxol-based therapy and GSK3 inhibition in non-small cell lung cancer.

Author

O'Flaherty L, Shnyder SD, Cooper PA, Cross SJ, Wakefield JG, Pardo OE, Seckl MJ, and Tavaré JM

Subjects

Animals, Antineoplastic Agents, Phytogenic pharmacology, Cell Line, Tumor, Cell Proliferation drug effects, Chromosome Aberrations drug effects, Drug Synergism, Drug Therapy, Combination, Glycogen Synthase Kinase 3 antagonists & inhibitors, Glycogen Synthase Kinase 3 genetics, Humans, Male, Mice, Mice, Nude, Paclitaxel pharmacology, Pyridines pharmacology, Pyrimidines pharmacology, RNA Interference, RNA, Small Interfering metabolism, Antineoplastic Agents, Phytogenic therapeutic use, Carcinoma, Non-Small-Cell Lung drug therapy, Glycogen Synthase Kinase 3 metabolism, Lung Neoplasms drug therapy, Paclitaxel therapeutic use, Pyridines therapeutic use, Pyrimidines therapeutic use

Abstract

Glycogen synthase kinase-3 (GSK3) is over-expressed and hyperactivated in non-small cell lung carcinoma (NSCLC) and plays a role in ensuring the correct alignment of chromosomes on the metaphase plate during mitosis through regulation of microtubule stability. This makes the enzyme an attractive target for cancer therapy. We examined the effects of a selective cell-permeant GSK3 inhibitor (CHIR99021), used alone or in combination with paclitaxel, using an in vitro cell growth assay, a quantitative chromosome alignment assay, and a tumor xenograft model. CHIR99021 inhibits the growth of human H1975 and H1299 NSCLC cell lines in a synergistic manner with paclitaxel. CHIR99021 and paclitaxel promoted a synergistic defect in chromosomal alignment when compared to each compound administered as monotherapy. Furthermore, we corroborated our in vitro findings in a mouse tumor xenograft model. Our results demonstrate that a GSK3 inhibitor and paclitaxel act synergistically to inhibit the growth of NSCLC cells in vitro and in vivo via a mechanism that may involve converging modes of action on microtubule spindle stability and thus chromosomal alignment during metaphase. Our findings provide novel support for the use of the GSK3 inhibitor, CHIR99021, alongside taxol-based chemotherapy in the treatment of human lung cancer., Competing Interests: The authors have declared that no competing interests exist.

Published

2019

26. Biology and clinical significance of circulating tumor cell subpopulations in lung cancer.

Author

O'Flaherty L, Wikman H, and Pantel K

Abstract

By identifying and tracking genetic changes in primary tumors and metastases, patients can be stratified for the most efficient therapeutic regimen by screening for known biomarkers. However, retrieving tissues biopsies is not always feasible due to tumor location or risk to patient. Therefore, a liquid biopsies approach offers an appealing solution to an otherwise invasive procedure. The rapid growth of the liquid biopsy field has been aided by improvements in the sensitivity and specificity of enrichment assays for isolating circulating tumor cells (CTCs) from normal surrounding blood cells. Furthermore, the identification and molecular characterization of CTCs has been shown in numerous studies to be of diagnostic and prognostic relevance in breast, prostate and colon cancer patients. Despite these advancements, and the highly metastatic nature of lung cancer, it remains a challenge to detect CTCs in advanced non-small cell lung cancer (NSCLC). It may be that loss of epithelial features, in favor of a mesenchymal phenotype, and the highly heterogeneous nature of NSCLC CTCs contribute to their evasion from current detection methods. By identifying a broader spectrum of biomarkers that could better differentiate the various NSCLC CTCs subpopulations, it may be possible to not only improve detection rates but also to shed light on which CTC clones are likely to drive metastatic initiation. Here we review the biology of CTCs and describe a number of proteins and genetic targets which could potentially be utilized for the dissemination of heterogenic subpopulations of CTCs in NSCLC., Competing Interests: Conflicts of Interest: The authors have no conflicts of interest to declare.

Published

2017

27. Aromatherapy massage seems to enhance relaxation in children with burns: an observational pilot study.

Author

O'Flaherty LA, van Dijk M, Albertyn R, Millar A, and Rode H

Subjects

Burns physiopathology, Child, Preschool, Female, Heart Rate physiology, Humans, Male, Pilot Projects, Prospective Studies, Relaxation Therapy methods, Respiratory Rate physiology, South Africa, Anxiety prevention & control, Aromatherapy methods, Burns therapy, Massage methods

Abstract

Objective: This observational pilot study investigated effects of aromatherapy massage in paediatric burn patients., Methods: The setting was a 17 beds level I burn unit in Cape Town, South Africa. Between January and October 2009 heart rates and respiratory rates of patients who underwent aromatherapy massage sessions were read before and after the sessions. Primary outcomes were decline in heart rates and respiratory rates, a sign of relaxation. Behavioural responses (sleep/awake state, facial expression, body posture) were documented as secondary outcomes., Results: A convenience sample of 71 paediatric burn patients (median age 3 years) underwent a total of 126 massage sessions. Mean heart rate decreased significantly from 118 (SD 20) to 109 (SD 21), t=9.8, p<0.001. Mean respiratory rate decreased significantly from 34 (SD 8) to 30 (SD 8), t=10.2, p<0.001. Most massage sessions (92.8%) elicited positive behaviour to the massage, e.g. the child fell asleep, calmed or asked to continue. Nine patients (7.2%) with a median age of 15 months who underwent a single massage session did not show positive behaviour but cried, wriggled or were distressed., Conclusions: Aromatherapy massage seems to be a helpful nonpharmacological approach to reduce hospitalized paediatric burn patients' distress. Future studies with better research designs and validated outcome measures should confirm our findings., (Copyright © 2012 Elsevier Ltd and ISBI. All rights reserved.)

Published

2012