Showing total 367 results

1. Invited papers.

Subjects

*CANCER, *TUMORS

Abstract

Presents invited papers on cancer. 'Preliminary Results of a MRC Randomised Controlled Trial of Post-Operative Irrigation of Superficial Bladder Cancer,' by P. Whelan, G. Griffiths, M. Stower, D. Wallace, J. Hetherington, T. Hargreave, P. English, P. Weston, M. Parmar; 'New Ways to Exploit Tumour Hypoxia,' by M. Brown; 'Measuring Tumour Hypoxia in the Clinic,' by C. West.

Published

2001

2. Routine psychosocial distress screening in radiotherapy: implementation and evaluation of a computerised procedure.

Author

Dinkel, A., Berg, P., Pirker, C., Geinitz, H., Sehlen, S., Emrich, M., Marten-Mittag, B., Henrich, G., Book, K., and Herschbach, P.

Subjects

PSYCHOSOCIAL factors, PSYCHOLOGICAL distress, RADIOTHERAPY, PHYSICIANS, EMOTIONS, TUMORS & psychology, RESEARCH, COMPUTERS, RESEARCH evaluation, PHYSICIAN-patient relations, RESEARCH methodology, PATIENT satisfaction, PSYCHOLOGY, MEDICAL cooperation, EVALUATION research, COMPARATIVE studies, INTERPERSONAL relations, QUALITY of life, TUMORS, PATIENT-professional relations, DEMOGRAPHY, PSYCHOLOGICAL stress, ONCOLOGY

Abstract

Background: To implement distress screening in routine radiotherapy practice and to compare computerised and paper-and-pencil screening in terms of acceptability and utility.Methods: We used the Stress Index RadioOncology (SIRO) for screening. In phase 1, 177 patients answered both a computerised and a paper version, and in phase 2, 273 patients filled out either the computerised or the paper assessment. Physicians received immediate feedback of the psycho-oncological results. Patients, nurses/radiographers (n=27) and physicians (n=15) evaluated the screening procedure.Results: The agreement between the computerised and the paper assessment was high (intra-class correlation=0.92). Patients' satisfaction did not differ between the two administration modes. Nurses/radiographers rated the computerised assessment less time consuming (3.7 vs 18.5%), although the objective data did not reveal a difference in time demand. Physicians valued the psycho-oncological results as interesting and informative (46.7%). Patients and staff agreed that the distress screening did not lead to an increase in the discussion of psychosocial issues in clinician-patient encounters.Conclusion: The implementation of a distress screening was feasible and highly accepted, regardless of the administration mode. Communication trainings should be offered in order to increase the discussion of psychosocial topics in clinician-patient encounters. [ABSTRACT FROM AUTHOR]

Published

2010

3. Steering decision making by terminology: oligometastatic versus argometastatic.

Author

Szturz, Petr and Vermorken, Jan B.

Subjects

*ANTHROPOMETRY, *METASTASIS, *DECISION making, *TUMORS, *ONCOLOGY

Abstract

Allowing selected patients with few distant metastases to undergo potentially curative local ablation, the designation "oligometastatic" has become a widely popular concept in oncology. However, accumulating evidence suggests that many of these patients harbour an unrecognised microscopic disease, leading either to the continuous development of new metastases or to an overt polymetastatic state and questioning thus an indiscriminate use of potentially harmful local ablation. In this paper, reviewing data on oligometastatic disease, we advocate the importance of identifying a true oligometastatic disease, characterised by a slow speed of development, instead of relying solely on a low number of lesions as the term "oligometastatic" implies. This is particularly relevant in clinical practice, where terminology has been shown to influence decision making. To define a true oligometastatic disease in the context of its still elusive biology and interaction with the immune system, we propose using clinical criteria. As discussed further in the paper, these criteria can be classified into three categories involving a low probability of occult metastases, low tumour growth rate and low tumour burden. Such cases with slow tumour-cell shedding and slow proliferation leave a sufficiently broad window-of-opportunity to detect and treat accessible lesions, increasing thus the odds of a cure. [ABSTRACT FROM AUTHOR]

Published

2022

4. The COSMIC (Catalogue of Somatic Mutations in Cancer) database and website.

Author

Bamford, S., Dawson, E., Forbes, S., Clements, J., Pettett, R., Dogan, A., Flanagan, A., Teague, J., Futreal, P. A., Stratton, M. R., and Wooster, R.

Subjects

GENETIC mutation, GENETICS, GENES, CANCER, HUMAN gene mapping, GENOMES, COMPARATIVE studies, DATABASES, INTERNET, RESEARCH methodology, MEDICAL cooperation, ONCOGENES, PROTEINS, RESEARCH, TRANSFERASES, TUMORS, EVALUATION research

Abstract

The discovery of mutations in cancer genes has advanced our understanding of cancer. These results are dispersed across the scientific literature and with the availability of the human genome sequence will continue to accrue. The COSMIC (Catalogue of Somatic Mutations in Cancer) database and website have been developed to store somatic mutation data in a single location and display the data and other information related to human cancer. To populate this resource, data has currently been extracted from reports in the scientific literature for somatic mutations in four genes, BRAF, HRAS, KRAS2 and NRAS. At present, the database holds information on 66 634 samples and reports a total of 10 647 mutations. Through the web pages, these data can be queried, displayed as figures or tables and exported in a number of formats. COSMIC is an ongoing project that will continue to curate somatic mutation data and release it through the website. [ABSTRACT FROM AUTHOR]

Published

2004

5. Patient attrition in Molecular Tumour Boards: a systematic review.

Author

Frost, Hannah, Graham, Donna M., Carter, Louise, O'Regan, Paul, Landers, Dónal, and Freitas, André

Subjects

*TUMOR treatment, *SYSTEMATIC reviews, *RESEARCH funding, *TUMORS

Abstract

Background: Molecular Tumour Boards (MTBs) were created with the purpose of supporting clinical decision-making within precision medicine. Though in use globally, reporting on these meetings often focuses on the small percentages of patients that receive treatment via this process and are less likely to report on, and assess, patients who do not receive treatment.Methods: A literature review was performed to understand patient attrition within MTBs and barriers to patients receiving treatment. A total of 51 papers were reviewed spanning a 6-year period from 11 different countries.Results: In total, 20% of patients received treatment through the MTB process. Of those that did not receive treatment, the main reasons were no mutations identified (27%), no actionable mutations (22%) and clinical deterioration (15%). However, data were often incomplete due to inconsistent reporting of MTBs with only 55% reporting on patients having no mutations, 55% reporting on the presence of actionable mutations with no treatment options and 59% reporting on clinical deterioration.Discussion: As patient attrition in MTBs is an issue which is very rarely alluded to in reporting, more transparent reporting is needed to understand barriers to treatment and integration of new technologies is required to process increasing omic and treatment data. [ABSTRACT FROM AUTHOR]

Published

2022

6. HPV vaccination among ethnic minorities in the UK: knowledge, acceptability and attitudes.

Author

Marlow, L. A. V.

Subjects

HUMAN papillomavirus vaccines, MEDICAL care of minorities, CANCER prevention, CERVICAL cancer, HEALTH attitudes, MEDLINE, PAPILLOMAVIRUS disease prevention, TUMOR prevention, CULTURE, ETHNIC groups, IMMUNIZATION, MEDICAL protocols, PAPILLOMAVIRUS diseases, PARENTS, TUMORS, VERTEBRATES, VIRUS diseases, CERVIX uteri tumors, SYSTEMATIC reviews, PATIENTS' attitudes, DISEASE complications

Abstract

Background: Human papillomavirus (HPV) vaccination offers a unique opportunity for the primary prevention of cervical cancer. Studies suggest that knowledge and attitudes about the vaccine are likely to influence uptake. One limitation of most studies assessing HPV vaccine knowledge, attitudes and acceptability is their under representation of ethnic minorities. It is important to ensure that our understanding of HPV knowledge and attitudes include all ethnic groups in the UK. This article reviews research that has considered knowledge, acceptability and attitudes about HPV and the HPV vaccine among ethnic minorities in the UK.Methods: Articles in Medline, CINAHL and PsycINFO (January 2000-March 2010) were searched.Results: A total of 17 UK-based papers examined knowledge, attitudes or acceptability related to HPV vaccination in the 'lay' population (parents, adolescents or the general population as opposed to health professionals) and reported findings by ethnicity.Conclusion: Findings seem to suggest lower awareness of HPV and lower acceptability of the vaccination, which could be important if they are reflected in uptake. More research is needed with ethnic minority groups, particularly in the context of the vaccination programme. [ABSTRACT FROM AUTHOR]

Published

2011

7. Cell-free DNA analysis in current cancer clinical trials: a review.

Author

Cisneros-Villanueva, M, Hidalgo-Pérez, L, Rios-Romero, M, Cedro-Tanda, A, Ruiz-Villavicencio, C A, Page, K, Hastings, R, Fernandez-Garcia, D, Allsopp, R, Fonseca-Montaño, M A, Jimenez-Morales, S, Padilla-Palma, V, Shaw, J A, and Hidalgo-Miranda, A

Subjects

*TUMOR diagnosis, *FERRANS & Powers Quality of Life Index, *CLINICAL trials, *METASTASIS, *EARLY detection of cancer, *QUESTIONNAIRES, *RESEARCH funding, *TUMORS

Abstract

Cell-free DNA (cfDNA) analysis represents a promising method for the diagnosis, treatment selection and clinical follow-up of cancer patients. Although its general methodological feasibility and usefulness has been demonstrated, several issues related to standardisation and technical validation must be addressed for its routine clinical application in cancer. In this regard, most cfDNA clinical applications are still limited to clinical trials, proving its value in several settings. In this paper, we review the current clinical trials involving cfDNA/ctDNA analysis and highlight those where it has been useful for patient stratification, treatment follow-up or development of novel approaches for early diagnosis. Our query included clinical trials, including the terms 'cfDNA', 'ctDNA', 'liquid biopsy' AND 'cancer OR neoplasm' in the FDA and EMA public databases. We identified 1370 clinical trials (FDA = 1129, EMA = 241) involving liquid-biopsy analysis in cancer. These clinical trials show promising results for the early detection of cancer and confirm cfDNA as a tool for real-time monitoring of acquired therapy resistance, accurate disease-progression surveillance and improvement of treatment, situations that result in a better quality of life and extended overall survival for cancer patients. [ABSTRACT FROM AUTHOR]

Published

2022

8. Proportion of infiltrating IgG-binding immune cells predict for tumour hypoxia.

Author

Collingridge, D R, Hill, S A, and Chaplin, D J

Subjects

HYPOXEMIA, TUMORS, MACROPHAGES, NEOVASCULARIZATION

Abstract

Macrophages can account for up to 50% of tumour mass and secrete many angiogenic factors. Furthermore, tumour hypoxia is thought to play a major role in the activation of macrophages and the regulation of angiogenesis. In this paper, we demonstrate a strong correlation between hypoxia and the recruitment of immune cells binding to IgG in 8 experimental tumours. We provide evidence that IgG binding immune cells in 3 tumour lines are predominately composed of macrophages. Reduced oxygenation may act as a stimulus for recruitment of immune cells to the tumour mass, and the detection of either IgG-positive host cells or macrophages may offer an alternative method for monitoring tumour hypoxia. [ABSTRACT FROM AUTHOR]

Published

2001

9. New treatments for advanced cancer: an approach to prioritization.

Author

Ferguson, J S J, Summerhayes, M, Masters, S, Schey, S, Smith, I E, and Ferguson, J S

Subjects

CANCER treatment, ANTINEOPLASTIC agents, DRUG therapy, COMPARATIVE studies, COST effectiveness, DECISION making, HEALTH care rationing, RESEARCH methodology, MEDICAL cooperation, HEALTH policy, POLICY sciences, RESEARCH, EVIDENCE-based medicine, TUMORS, GOVERNMENT aid, PHARMACY, EVALUATION research, ECONOMICS

Abstract

The allocation of funding for new anticancer treatments within the UK has not kept pace with demand. Clinicians find themselves restricted in the use of licensed drugs which they feel are in the best interests of individual patients. Against this, health authorities have a duty to ensure that scarce resources are used equitably to meet the needs of the local population as a whole. Differential levels of funding for new treatments across the country have led to concerns about rationing by postcode. This paper outlines an approach to the prioritization of new treatment for advanced cancer developed jointly by clinicians and health authorities in South London. The approach involves evidence reviews and consensus meetings. Existing and new treatments are rated on a four-point 'relative effectiveness scale', which takes account of the impact of the treatment on quality of life and on survival. The strength of evidence supporting each effectiveness rating is also classified. Health Authorities have used these ratings to determine overall funding levels, while leaving decisions on individual patients to the relevant Trusts. [ABSTRACT FROM AUTHOR]

Published

2000

10. Cancer survivorship, excess body fatness and weight-loss intervention-where are we in 2020?

Author

Anderson, Annie S., Martin, Richard M., Renehan, Andrew G., Cade, Janet, Copson, Ellen R., Cross, Amanda J., Grimmett, Chloe, Keaver, Laura, King, Angela, Riboli, Elio, Shaw, Clare, Saxton, John M., On behalf of the UK NIHR Cancer and Nutrition Collaboration (Population Health Stream), Anderson, Annie, Beeken, Rebecca, Cross, Amanda, Martin, Richard, Mitrou, Giota, Saxton, John, and Renehan, Andrew

Subjects

*PREVENTION of obesity, *BODY composition, *FERRANS & Powers Quality of Life Index, *WEIGHT loss, *IMPACT of Event Scale, *RESEARCH funding, *TUMORS, *ADIPOSE tissues, TUMOR prevention

Abstract

Earlier diagnosis and more effective treatments mean that the estimated number of cancer survivors in the United Kingdom is expected to reach 4 million by 2030. However, there is an increasing realisation that excess body fatness (EBF) is likely to influence the quality of cancer survivorship and disease-free survival. For decades, the discussion of weight management in patients with cancer has been dominated by concerns about unintentional weight loss, low body weight and interventions to increase weight, often re-enforced by the existence of the obesity paradox, which indicates that high body weight is associated with survival benefits for some types of cancer. However, observational evidence provides strong grounds for testing the hypothesis that interventions for promoting intentional loss of body fat and maintaining skeletal muscle in overweight and obese cancer survivors would bring important health benefits in terms of survival outcomes and long-term impact on treatment-related side effects. In this paper, we outline the need for studies to improve our understanding of the health benefits of weight-loss interventions, such as hypocaloric healthy-eating plans combined with physical activity. In particular, complex intervention trials that are pragmatically designed are urgently needed to develop effective, clinically practical, evidence-based strategies for reducing EBF and optimising body composition in people living with and beyond common cancers. [ABSTRACT FROM AUTHOR]

Published

2021

11. Antithrombotic therapy and survival in patients with malignant disease.

Author

Kakkar, A. K. and Macbeth, F.

Subjects

FIBRINOLYTIC agents, ANTICOAGULANTS, BLOOD coagulation, THROMBOEMBOLISM, THERAPEUTIC use of fibrinolytic agents, ENOXAPARIN, VEINS, TUMORS, DISEASE complications

Abstract

A broad range of studies suggest a two-way relationship between cancer and venous thromboembolism (VTE). Patients with cancer have consistently been shown to be at elevated risk for VTE; this risk is partly driven by an intrinsic hypercoagulable state elicited by the tumour itself. Conversely, thromboembolic events in patients without obvious risk factors are often the first clinical manifestation of an undiagnosed malignancy. The relationship between VTE and cancer is further supported by a number of trials and meta-analyses which, when taken together, strongly suggest that antithrombotic therapy can extend survival in patients with cancer by a mechanism that extends beyond its effect in preventing VTE. Moreover, accumulating evidence from in vitro and in vivo studies has shown that tumour growth, invasion, and metastasis are governed, in part, by elements of the coagulation system. On 22 May 2009, a group of health-care providers based in the United Kingdom met in London, England, to examine recent advances in cancer-associated thrombosis and its implications for UK clinical practice. As part of the discussion, attendees evaluated evidence for and against an effect of antithrombotic therapy on survival in cancer. This paper includes a summary of the data presented at the meeting and explores potential mechanisms by which antithrombotic agents might exert antitumour effects. The summary is followed by a consensus statement developed by the group. [ABSTRACT FROM AUTHOR]

Published

2010

12. Immunisation with 'naïve' syngeneic dendritic cells protects mice from tumour challenge.

Author

Grimshaw, M J, Papazisis, K, Picco, G, Bohnenkamp, H, Noll, T, Taylor-Papadimitriou, J, and Burchell, J

Subjects

DENDRITIC cells, IMMUNIZATION, TUMOR growth, MICE, IMMUNE response, TUMOR treatment, ANIMAL experimentation, B cells, CELL lines, COMPARATIVE studies, FLOW cytometry, GLYCOPROTEINS, IMMUNOTHERAPY, INTERFERONS, INTERLEUKINS, RESEARCH methodology, MEDICAL cooperation, RESEARCH, RESEARCH funding, SPLEEN, SURVIVAL, T cells, TUMORS, PHENOTYPES, EVALUATION research

Abstract

Dendritic cells (DCs) 'pulsed' with an appropriate antigen may elicit an antitumour immune response in mouse models. However, while attempting to develop a DC immunotherapy protocol for the treatment of breast cancer based on the tumour-associated MUC1 glycoforms, we found that unpulsed DCs can affect tumour growth. Protection from RMA-MUC1 tumour challenge was achieved in C57Bl/6 MUC1 transgenic mice by immunising with syngeneic DCs pulsed with a MUC1 peptide. However, unpulsed DCs gave a similar level of protection, making it impossible to evaluate the effect of immunisation of mice with DCs pulsed with the specific peptide. Balb/C mice could also be protected from tumour challenge by immunisation with unpulsed DCs prior to challenge with murine mammary tumour cells (410.4) or these cells transfected with MUC1 (E3). Protection was achieved with as few as three injections of 50,000 naïve DCs per mouse per week, was not dependent on injection route, and was not specific to cell lines expressing human MUC1. However, the use of Rag2-knockout mice demonstrated that the adaptive immune response was required for tumour rejection. Injection of unpulsed DCs into mice bearing the E3 tumour slowed tumour growth. In vitro, production of IFN-gamma and IL-4 was increased in splenic cells isolated from mice immunised with DCs. Depleting CD4 T cells in vitro partially decreased cytokine production by splenocytes, but CD8 depletion had no effect. This paper shows that naïve syngeneic DCs may induce an antitumour immune response and has implications for DC immunotherapy preclinical and clinical trials. [ABSTRACT FROM AUTHOR]

Published

2008

13. A simple, reproducible method for monitoring the treatment of tumours using dynamic contrast-enhanced MR imaging.

Author

Morgan, B., Utting, J. F., Higginson, A., Thomas, A. L., Steward, W. P., and Horsfield, M. A.

Subjects

CANCER treatment, TUMORS, MAGNETIC resonance imaging, TUMOR markers, BIOMARKERS

Abstract

Dynamic contrast-enhanced MR imaging (DCE-MRI) may act as a biomarker for successful cancer therapy. Simple, reproducible techniques may widen this application. This paper demonstrates a single slice imaging technique. The image acquisition is performed in less than 500 ms making it relatively insensitive to respiratory motion. Data from phantom studies and a reproducibility study in solid human tumours are presented. The reproducibility study showed a coefficient of variation (CoV) of 19.1% for K(trans) and 15.8% for the initial area under the contrast enhancement curve (IAUC). This was improved to 16 and 13.9% if tumours of diameter less than 3 cm were excluded. The individual repeatability (the range within which individual measurements are expected to fall) was 30.6% for K(trans) and 26.5% for IAUC for tumours greater than 3 cm diameter. This approach to DCE-MRI image acquisition can be performed with standard clinical scanners, and data analysis is straightforward. For treatment trials with 10 patients in a cohort, the CoV implies that the method would be sensitive to a treatment effect of greater than 18%. The individual repeatability is well inside the 40% change shown to be important in clinical studies using this DCE-MRI technique. [ABSTRACT FROM AUTHOR]

Published

2006

14. What should the detection rates of cancers be in breast screening programmes?

Author

Duffy, S. W. and Gabe, R.

Subjects

BREAST cancer, TUMORS, CARCINOGENS, MEDICAL screening, MEDICAL care, HEALTH risk assessment

Abstract

Minimum detection rates at screening are sometimes laid down as standards for breast cancer screening programmes, based on underlying incidence of the disease in the age group screened. Detection rates should also depend on desired sensitivity, mean sojourn time, interscreening interval and the screening round--that is, prevalent (first) or incident (second or subsequent). In this paper, we use these quantities to derive expected, minimum and maximum detection rates proportional to the underlying incidence as well as estimated underlying incidence rates from extrapolation of prescreening trends in England and Wales to derive alternative standard minimum, expected and maximum detection rates per 1000 women screened for the UK Breast Screening Programme, as follows: minimum detection rates should be 4.1 and 4.3 at prevalence screen and incidence screens, respectively; expected rates should be 6.9 and 4.8 and maximum rates of 9.6 and 5.5. These are consistent with observed detection rates in the UK programme. [ABSTRACT FROM AUTHOR]

Published

2005

15. A micro costing of NHS cancer genetic services.

Author

Griffith, G. L., Tudor-Edwards, R., Gray, J., Butler, R., Wilkinson, C., Turner, J., France, B., Bennett, P., and GenQuest Research Team

Subjects

CANCER patients, HEALTH counseling, COLON cancer, MEDICAL care costs, MEDICAL care, GENETICS, LABORATORIES, NATIONAL health services, COMPARATIVE studies, FAMILY health, GENETIC counseling, RESEARCH methodology, MEDICAL cooperation, MEDICAL personnel, MEDICAL referrals, RESEARCH, RISK assessment, TUMORS, COST analysis, EVALUATION research, ECONOMICS

Abstract

This paper presents the first full micro costing of a commonly used cancer genetic counselling and testing protocol used in the UK. Costs were estimated for the Cardiff clinic of the Cancer Genetics Service in Wales by issuing a questionnaire to all staff, conducting an audit of clinic rooms and equipment and obtaining gross unit costs from the finance department. A total of 22 distinct event pathways were identified for patients at risk of developing breast, ovarian, breast and ovarian or colorectal cancer. The mean cost per patient were pound sterling 97- pound sterling 151 for patients at moderate risk, pound sterling 975- pound sterling 3072 for patients at high risk of developing colorectal cancer and pound sterling 675- pound sterling 2909 for patients at high risk of developing breast or ovarian cancer. The most expensive element of cancer genetic services was labour. Labour costs were dependent upon the amount of labour, staff grade, number of counsellors used and the proportion of staff time devoted to indirect patient contact. With the growing demand for cancer genetic services and the growing number of national and regional cancer genetic centers, there is a need for the different protocols being used to be thoroughly evaluated in terms of costs and outcomes. [ABSTRACT FROM AUTHOR]

Published

2005

16. Predicting aggressive outcome in T1N0M0 breast cancer.

Author

Kronqvist, P., Kuopio, T., Nykänen, M., Helenius, H., Anttinen, J., Klemi, P., and Nykänen, M

Subjects

PROGNOSIS, BREAST cancer, PATIENTS, IMMUNOHISTOCHEMISTRY, TUMORS, ONCOLOGY

Abstract

Despite the excellent overall prognosis, unpredictable breast cancer recurrences and deaths also occur among T1N0M0 patients. We have evaluated clinically applicable methods for identifying aggressive outcome in T1N0M0 breast cancer. The material is based on aggressive T1N0M0 invasive ductal and lobular carcinomas diagnosed in Turku University Hospital and Jyväskylä Central Hospital, Finland, during 1987-1997. We studied all the T1N0M0 breast cancers that had led to recurrency or death (n=21, 95% T1cN0M0) during the follow-up period (4-14 years). The study is based on statistical analyses of matched case-control data in which the prognostic factors of each individual patient with aggressive disease were compared with control patients (n=45) individually matched by tumour size, age at diagnosis, histological type of tumour and length of follow-up. The cancer cases were examined for clinically applicable conventional and immunohistochemical pathologic prognostic factors. High Ki-67 immunopositivity was the strongest prognosticator of breast cancer death or recurrence in T1N0M0 breast cancer. Also, high p53 immunopositivity, low oestrogen receptor immunopositivity and Her-2/neu oncogene amplification by chromogen in situ hybridisation were reliable indicators of unfavourable outcome. Our statistical methods also allowed us to determine for the present material a range of clinical significance for each immunohistochemical prognostic feature with the associated relative risk for breast cancer death and recurrence. The paper suggests guidelines for predicting aggressive outcome in T1N0M0 breast cancer. [ABSTRACT FROM AUTHOR]

Published

2004

17. The meanings of cancer and perceptions of cancer services among South Asians in Luton, UK.

Author

Randhawa, G. and Owens, A.

Subjects

CANCER education, SOCIAL networks, SOUTH Asians, MUSLIMS, TUMOR treatment, RESEARCH, HEALTH services accessibility, SOCIAL support, FOCUS groups, INFORMATION services, RESEARCH methodology, SENSORY perception, MEDICAL care, PROGNOSIS, EVALUATION research, SURVEYS, COMPARATIVE studies, HEALTH attitudes, COMMUNICATION, TUMORS

Abstract

Recent research has suggested that there is limited awareness of and information about cancer and cancer services among South Asian communities. This study explores the meanings of cancer and perceptions of cancer services among South Asians living in Luton. Six single-sex focus groups were conducted among the three main South Asian groups in Luton: (1) Punjabi-speaking Muslims originating from Pakistan (Pakistani Punjabi); (2) Sylheti-speaking Muslims originating from Bangladesh (Bangladeshi Sylheti); and (3) Punjabi-speaking Sikhs originating from the Indian Punjab (Indian Punjabi). Overall, it was found that the information relating to cancer for South Asian communities was limited. Participants in the study expressed a keen desire for this information to be made available via their community social networks. This lack of information resulted in low levels of awareness about cancer and related issues. Cancer was often perceived as an incurable disease, a reflection of the fact that access to appropriate services had been experienced at a relatively late stage of the illness. Informed education, therefore, is clearly essential to influence how people manage cancer and access cancer services. This paper describes the challenges that service providers and users face in ensuring effective and informed awareness. [ABSTRACT FROM AUTHOR]

Published

2004

18. Cardiac abnormalities 15 years and more after adriamycin therapy in 229 childhood survivors of a solid tumour at the Institut Gustave Roussy.

Author

Pein, F., Sakiroglu, O., Dahan, M., Lebidois, J., Merlet, P., Shamsaldin, A., Villain, E., de Vathaire, F., Sidi, D., and Hartmann, O.

Subjects

HEART diseases, DOXORUBICIN, HEART failure, CARDIAC contraction, DRUG therapy, RADIOTHERAPY, ANTINEOPLASTIC antibiotics, RESEARCH, TIME, LEFT ventricular dysfunction, RESEARCH methodology, EVALUATION research, COMPARATIVE studies, DOSE-effect relationship in pharmacology, RADIATION injuries, TUMORS, LONGITUDINAL method

Abstract

The purpose of this paper was to determine the cardiac status in children 15 years or more after adriamycin therapy for a solid tumour. Of the 447 pts, 229 pts were fully studied and 218 were not. The following cardiac evaluations were proposed to all the 447 consecutive patients (pts): (1) cardiac Doppler US by one of two expert cardiologists; (2) cardiac rhythm and conduction abnormalities including 24-hour holter ECG; (3) (131)l-mlBG myocardial scintigraphy; (4) serum brain natriuretic peptide levels at rest; (5) an exercise test with VO(2) max measurement. The radiation doses delivered to 6 points in the heart were estimated for all patients who had received radiotherapy. Congestive heart failure was diagnosed in 24 of 229 (10%) evaluated pts, with a median interval of 15 years (0.3-24 years) from the first symptom after adriamycin treatment. Among the 205 remaining pts, 13 asymptomatic pts (6%) had severe (n=4) (FS<20%) or marked (n=9) (20< or =FS<25%) systolic dysfunction. In the 192 others, the median meridional end-systolic wall stress was 91 (53-135) and it exceeded 100 g cm(-2) in 52 pts. Using a Cox model, only the cumulative dose of adriamycin and the average radiation dose to the heart, were identified as risk factors for a pathological cardiac status. In conclusion, the risk of cardiac failure or severe abnormalities increases with adriamycin treatment, radiotherapy and time since treatment, even after a follow-up of 15 years or more. In our series, after an average follow-up of 18 years, 39% of the children had a severe cardiac dysfunction or major ventricular overload conditions. The risk increases with the dose of adriamycin and radiation received to the heart, without evidence for threshold. [ABSTRACT FROM AUTHOR]

Published

2004

19. Interleukin-2 improves tumour response to DNP-modified autologous vaccine for the treatment of metastatic malignant melanoma.

Author

Lotem, M., Shiloni, E., Pappo, I., Drize, O., Hamburger, T., Weitzen, R., Isacson, R., Kaduri, L., Merims, S., Frankenburg, S., and Peretz, T.

Subjects

INTERLEUKIN-2, MELANOMA, DINITROBENZENES, CANCER invasiveness, DRUG therapy, METASTASIS, TUMORS, VACCINATION

Abstract

This paper is a report of response rate (RR) and survival of 34 metastatic melanoma patients who received a dinitrophenyl (DNP)-modified autologous melanoma cell vaccine. In all, 27 patients started the vaccine as a primary treatment for metastatic melanoma and seven started it as an adjuvant, with no evidence of disease at the time, but had developed new metastases. Interleukin-2 (IL-2) was administered in 24 out of the 34 patients: 19 who progressed on vaccine alone and five who had the combination from start. Interleukin-2 was administered in the intravenous, bolus high-dose regimen (seven patients) or as subcutaneous (s.c.) low-dose treatment (17). Overall response for the entire group was 35% (12 patients out of 34), 12% having a complete response (CR) and 23% a partial response (PR). However, only two patients had tumour responses while on the vaccine alone, whereas the other 10 demonstrated objective tumour regression following the combination with IL-2 (two CR, eight PR), lasting for a median duration of 6 months (range 3-50 months). Of the 12 responding patients, 11 attained strong skin reactivity to the s.c. injection of irradiated, unmodified autologous melanoma cells. None of the patients with a negative reactivity experienced any tumour response. Patients with positive skin reactions survived longer (median survival - 54 months). The results suggest enhanced RRs to the combination of IL-2 and autologous melanoma vaccine. Skin reactivity to unmodified autologous melanoma cells may be a predictor of response and improved survival, and therefore a criterion for further pursuing of immunotherapeutic strategies.British Journal of Cancer (2004) 90, 773-780. doi:10.1038/sj.bjc.6601563 www.bjcancer.com [ABSTRACT FROM AUTHOR]

Published

2004

20. Cost-effectiveness of stereotactic large-core needle biopsy for nonpalpable breast lesions compared to open-breast biopsy.

Author

Groenewoud, J.H., Pijnappel, R.M., Birnie, E., Marle, M.E. van den Akker-van, Buijs, van der Woude, T., Mali, W.P.Th.M., de Koning, H.J., and Busken, E.

Subjects

BREAST cancer, BIOPSY, TUMORS, CANCER, ONCOLOGY

Abstract

This paper demonstrates that the introduction of large-core needle biopsy (LCNB) replacing needle-localised breast biopsy (NLBB) for nonpalpable (screen-detected) breast lesions could result in substantial cost savings at the expense of a possible slight increase in breast cancer mortality. The cost-effectiveness of LCNB and NLBB was estimated using a microsimulation model. The sensitivity of LCNB (0.97) and resource use and costs of LCNB and NLBB were derived from a multicentre consecutive cohort study among 973 women who consented in getting LCNB and NLBB, if LCNB was negative. Sensitivity analyses were performed. Replacing NLBB with LCNB would result in approximately six more breast cancer deaths per year (in a target population of 2.1?million women), or in 1000 extra life-years lost from breast cancer (effect over 100 years). The total costs of management of breast cancer (3% discounted) are estimated at £4676 million with NLBB; introducing LCNB would save £13 million. The incremental cost-effectiveness ratio of continued NLBB vs LCNB would be £12?482 per additional life-year gained (3% discounted); incremental costs range from £-21?687 (low threshold for breast biopsy) to £74?378 (high sensitivity of LCNB).British Journal of Cancer (2004) 90, 383-392. doi:10.1038/sj.bjc.6601520 www.bjcancer.com [ABSTRACT FROM AUTHOR]

Published

2004

21. HPV infection and number of lifetime sexual partners are strong predictors for 'natural' regression of CIN 2 and 3.

Author

Chan, J.K., Monk, B.J., Brewer, C., Keefe, K.A., Osann, K., McMeekin, S., Rose, G.S., Youssef, M., Wilczynski, S.P., Meyskens, F.L., and Berman, M.L.

Subjects

PAPILLOMAVIRUS diseases, POLYMERASE chain reaction, SPONTANEOUS cancer regression, SEX surrogates, CERVICAL vertebrae diseases, CERVIX uteri disease diagnosis, BETA carotene, DNA analysis, EPIDEMIOLOGY of sexually transmitted diseases, CERVIX uteri diseases, CLINICAL trials, COLPOSCOPY, COMPARATIVE studies, DYSPLASIA, LONGITUDINAL method, MARITAL status, RESEARCH methodology, MEDICAL cooperation, PAPILLOMAVIRUSES, RESEARCH, SEXUALLY transmitted diseases, TUMORS, VIRUS diseases, CERVIX uteri tumors, EVALUATION research, RANDOMIZED controlled trials, DISEASE incidence, BLIND experiment, SEXUAL partners, CERVICAL intraepithelial neoplasia, DIAGNOSIS, THERAPEUTICS

Abstract

The aim of this paper was to evaluate the factors that predict regression of untreated CIN 2 and 3. A total of 93 patients with colposcopic persistent CIN 2 and 3 lesions after biopsy were followed for 6 months. Human papillomavirus (HPV) types were determined by polymerase chain reaction at enrolment. We analysed the biologic and demographic predictors of natural regression using univariate and multivariate methods. The overall regression rate was 52% (48 out of 93), including 58% (22 out of 38) of CIN 2 and 47% (26 out of 55) of CIN 3 lesions (P=0.31 for difference). Human papillomavirus was detected in 84% (78 out of 93) of patients. In univariate analysis, 80% (12 out of 15) of lesions without HPV regressed compared to 46% (36 out of 78) of lesions with HPV infection (P=0.016). Women without HPV and those who had a resolution of HPV had a four-fold higher chance of regression than those with persistent HPV (relative odds=3.5, 95% CI=1.4-8.6). Women with five or fewer lifetime sexual partners had higher rates of regression than women with more than five partners (P=0.003). In multivariate analysis, HPV status and number of sexual partners remained as significant independent predictors of regression. In conclusion, HPV status and number of lifetime sexual partners were strongly predictive of regression of untreated CIN 2 and 3. [ABSTRACT FROM AUTHOR]

Published

2003

22. Gene delivery to hypoxic cells in vitro.

Author

Dachs, G U, Coralli, C, Hart, S L, and Tozer, G M

Subjects

HYPOXEMIA, TUMORS, GENE transfection, GENETIC transformation, GENE therapy, OXYGEN metabolism, ANIMAL experimentation, CELL lines, CELL separation, COMPARATIVE studies, FLOW cytometry, GENES, GENETIC techniques, RESEARCH methodology, MEDICAL cooperation, MICE, PEPTIDES, PHOSPHOLIPIDS, RESEARCH, TIME, PILOT projects, EVALUATION research, CANCER cell culture

Abstract

Hypoxia in solid tumours has been correlated with poor prognosis and resistance to radiation and chemotherapy. Hypoxia is also a strong stimulus for gene expression. We previously proposed a gene therapy approach which exploits the presence of severe hypoxia in tumours for the induction of therapeutic genes. Hypoxic cells are known to have a reduced metabolic rate, transcription and translation. These facts may prevent gene transfer and therefore warranted further investigation. In this paper the feasibility of gene delivery in vitro under tumour conditions was demonstrated. DNA was delivered in vitro using a peptide-mediated non-viral system. Across a range of oxygen tensions and mammalian cell lines (including human tumour and endothelial cells) it was shown that hypoxic cells could be transfected. Transfection efficiencies varied depending on the level of hypoxia, cell characteristics and gene promoters used. An in vitro model of hypoxia/reoxygenation, designed to mimic the variable nature of tumour hypoxia, showed that hypoxic preconditioning and reoxygenation alone did not reduce transfection efficiency significantly; only chronic anoxia reduced transfection. The fact that neither intermediate hypoxia nor intermittent anoxia significantly reduced transfection is promising for future hypoxia-targeted gene therapy strategies. [ABSTRACT FROM AUTHOR]

Published

2000

23. Fluorescence in situ hybridization techniques for the rapid detection of genetic prognostic factors in neuroblastoma. United Kingdom Children's Cancer Study Group.

Author

Taylor, C P F, Bown, N P, McGuckin, A G, Lunec, J, Malcolm, A J, Pearson, A D J, Sheer, D, Taylor, C P, and Pearson, A D

Subjects

NEUROBLASTOMA, TUMORS, FLUORESCENCE, IN situ hybridization, ANEUPLOIDY, BIOPSY, BONE marrow, CELL nuclei, CHROMOSOME abnormalities, CHROMOSOMES, COMPARATIVE studies, DISEASE susceptibility, GENE amplification, IMMUNOBLOTTING, KARYOTYPES, RESEARCH methodology, MEDICAL cooperation, NUCLEOTIDE separation, ONCOGENES, PROGNOSIS, RESEARCH, FLUORESCENCE in situ hybridization, EVALUATION research

Abstract

Neuroblastoma is the commonest extracranial solid tumour in children. There are a number of molecular genetic features known which are of prognostic importance and which are used to direct therapy. Identification and targeting of high-risk individuals with intensive therapeutic regimens may allow an improvement in survival rates. The most powerful biological parameters associated with prognosis in this malignancy are chromosomal changes, especially MYCN amplification, deletion of chromosome 1p and aneuploidy. Rapid characterization of these aberrations at the time of diagnosis is paramount if stratification according to risk group is to be achieved. This paper describes the rapid detection of del(1p), MYCN amplification and trisomy using interphase fluorescence in situ hybridization on imprints from fresh tumour biopsies. The results are related to those obtained by standard molecular methods and karyotyping. [ABSTRACT FROM AUTHOR]

Published

2000

24. High incidence of SV40-like sequences detection in tumour and peripheral blood cells of Japanese osteosarcoma patients.

Author

Yamamoto, H, Nakayama, T, Murakami, H, Hosaka, T, Nakamata, T, Tsuboyama, T, Oka, M, Nakamura, T, and Toguchida, J

Subjects

TUMORS, PERIPHERAL circulation, OSTEOSARCOMA

Abstract

Recent studies have revealed the evidence for the significance of SV40 genome in human malignancies. In this paper, the presence of SV40-like sequences was investigated in 54 Japanese osteosarcomas in which mutations of the retinoblastoma (Rb), p53, MDM2, and CDK4 genes had been already analysed. Using polymerase chain reaction and Southern hybridization, SV40-like sequences were detected in 25 cases (46.3%). In most cases, only a part of SV40 genome was detected, and the regulatory region containing enhancer sequences was most frequently found (21/54, 38.9%). There was no apparent relationship between the presence of SV40-like sequences and tumour suppressor genes mutations in each tumour. The SV40-like sequences were also detected in peripheral blood cells of substantial proportion of the patients (43.3%), whereas the incidence was much lower (4.7%) in normal healthy controls. This difference is statistically highly significant (P < 0.0001), suggesting that the presence of SV40-like sequences, even if only a part, may play some roles to predispose individuals to osteosarcoma. [ABSTRACT FROM AUTHOR]

Published

2000

25. Reducing DCO registrations through electronic matching of cancer registry data and routine hospital data.

Author

Pollock, A M and Vickers, N

Subjects

DEATH certificates, TUMORS

Abstract

The Thames Cancer Registry (TCR) has registered a high proportion of tumours from death certificate information only (DCO) registrations. This paper describes the results of a study set up to establish whether this proportion could be reduced by linking cancer registrations with routine hospital data from the Hospital Episodes Statistics (HES) data set using computerized matching. A total of 67752 registrations were identified from the TCR. Matches were found in the HES data set for 66%. The proportion of cases retrieved for each tumour site was: 72% for colorectal cancer; 62% for cancer of the lung, trachea or bronchus; and 65% for female breast cancer. For all three tumour sites the proportion of matches found for patients registered from hospital case notes was higher than the proportion found for patients registered as DCOs (P < 0.0001 for all three tumour sites). Among matched DCO cases, 58% had at least one procedure recorded. DCO rates might be reduced by as much as 43% (from 17% of total registrations to less than 10%) for the three most common cancers if the method of electronic matching outlined here was used. Younger age groups, prognosis of tumour site and residence in North Thames region were all positively associated with successful matching (P < 0.0001 in all three cases). Many matched DCO cases were found to have had more than one admission for cancer. Among ordinary in-patient admissions, admissions to patients ratios of 1.5, 1.4 and 1.9 were found for colorectal, lung and breast cancers respectively. Of 5190 matched DCOs a procedure was recorded for 3013 (58%). HES data offer a useful aid to follow-up of case notes on patients identified to the registry by death certificates. Doubts about the completeness and accuracy of HES data mean case notes must remain the 'gold standard'. [ABSTRACT FROM AUTHOR]

Published

2000

26. Labelling indices in human tumours: to apply corrections or not – that is the question.

Author

Bergström, C, Begg, A, Palmqvist, R, Waites, A, and Denekamp, J

Subjects

TUMORS, PYRIMIDINES

Abstract

The advent of halogenated pyrimidines (bromodeoxyuridine, BrdU; idoxuridine, IdU) and antibodies to recognize them has opened new horizons for the measurement of proliferation in human tumours. These precursors of DNA can be given to patients and a single biopsy can be taken to measure in a flow cytometer both the fraction of labelled cells and their rate of movement through the S phase. From these two parameters the potential doubling time, T[SUBPOT], can be calculated. To measure both parameters simultaneously a compromise is made in the time of assessing the labelling index (LI). LI should ideally be assessed after a very short interval, e.g. 0.5-1 h, to avoid the contaminating influence of any cells dividing between injection and biopsy. However, an interval of 4-8 h is considered necessary to assess TS from the relative movement of cells through the S phase. Several techniques exist to correct for cell division if the interval is long. The simplest correction, which only corrects for the division of labelled cells, is most widely used. Downward correction factors of at least 10% are commonly applied, reducing the observed LI values. In this paper we illustrate graphically the dependence of the appropriate correction factor on various cell kinetic parameters. The duration of G2 is the most critical parameter for both the size and direction of any correction factor. The G2 phase has previously been shown to be about three times longer in human tumours than in rodents. If G2+M is as long as 6 h, the main artefact of the intervals between injection and biopsy up to 7 h is that the observed LI is too low because of division of unlabelled G2 cells. A correction of up to 10% is needed but in an upward direction. A nomogram of probable correction factors as a function of sampling interval is provided. We show from flow cytometric data that G2+M may be shorter than 4 h for head and neck tumours. It is recommended that the correction factor established by gating the... [ABSTRACT FROM AUTHOR]

Published

1999

27. Pharmacologically directed strategies in academic anticancer drug discovery based on the European NCI compounds initiative.

Author

Hendriks, Hans R, Govaerts, Anne-Sophie, Fichtner, Iduna, Burtles, Sally, Westwell, Andrew D, and Peters, Godefridus J

Subjects

*ANTINEOPLASTIC agents, *DRUG design, *RESEARCH, *TUMORS

Abstract

Background: The European NCI compounds programme, a joint initiative of the EORTC Research Branch, Cancer Research Campaign and the US National Cancer Institute, was initiated in 1993. The objective was to help the NCI in reducing the backlog of in vivo testing of potential anticancer compounds, synthesised in Europe that emerged from the NCI in vitro 60-cell screen.Methods: Over a period of more than twenty years the EORTC-Cancer Research Campaign panel reviewed ∼2000 compounds of which 95 were selected for further evaluation. Selected compounds were stepwise developed with clear go/no go decision points using a pharmacologically directed programme.Results: This approach eliminated quickly compounds with unsuitable pharmacological properties. A few compounds went into Phase I clinical evaluation. The lessons learned and many of the principles outlined in the paper can easily be applied to current and future drug discovery and development programmes.Conclusions: Changes in the review panel, restrictions regarding numbers and types of compounds tested in the NCI in vitro screen and the appearance of targeted agents led to the discontinuation of the European NCI programme in 2017 and its transformation into an academic platform of excellence for anticancer drug discovery and development within the EORTC-PAMM group. This group remains open for advice and collaboration with interested parties in the field of cancer pharmacology. [ABSTRACT FROM AUTHOR]

Published

2017

28. Cancer screening and preventative care among long-term cancer survivors in the United Kingdom.

Author

Khan, N. F., Carpenter, L., Watson, E., and Rose, P. W.

Subjects

MEDICAL screening, CANCER prevention, CANCER patients, PROSTATE cancer patients, MAMMOGRAMS, TUMOR prevention, BREAST tumors, COLON tumors, COMPARATIVE studies, LONGITUDINAL method, MATHEMATICAL models, RESEARCH methodology, MEDICAL cooperation, MULTIVARIATE analysis, PREVENTIVE health services, PROSTATE tumors, RECTUM tumors, RESEARCH, RESEARCH funding, TUMORS, THEORY, EVALUATION research, EARLY detection of cancer

Abstract

Background: Long-term cancer survivors in the United Kingdom are mostly followed up in a primary care setting by their general practitioner; however, there is little research on the use of services. This study examines whether cancer survivors receive adequate screening and preventative care in UK primary care.Patients and Methods: We identified a cohort of long-term survivors of breast, colorectal and prostate cancer with at least a 5-year survival using the General Practice Research Database, with controls matched for age, gender and practice. We compared adherence with cancer screening and the use of preventative care between cancer survivors and controls.Results: The cancer survivors' cohort consisted of 18 612 breast, 5764 colorectal and 4868 prostate cancer survivors. Most cancer survivors receive cancer screening at the same levels as controls, except for breast cancer survivors who were less likely to receive a mammogram than controls (OR=0.78, 95% CI: 0.66-0.92). Long-term cancer survivors received comparable levels of influenza vaccinations and cholesterol tests, but breast (OR 0.81, 95% CI: 0.74-0.87) and prostate cancer survivors (OR=0.70, 95% CI: 0.57-0.87) were less likely to receive a blood pressure test. All survivors were more likely to receive bone densitometry.Conclusion: The provision and uptake of preventive care in a primary care setting in the United Kingdom is comparable between the survivors of three common cancers and those who have not had cancer. However, long-term breast cancer survivors in this cohort were less likely to receive a mammogram. [ABSTRACT FROM AUTHOR]

Published

2010

29. Where is VEGF in the body? A meta-analysis of VEGF distribution in cancer.

Author

Kut, C., Mac Gabhann, F., and Popel, A. S.

Subjects

VASCULAR endothelial growth factors, CANCER treatment, TUMORS, META-analysis, LEUCOCYTES

Abstract

Vascular endothelial growth factor (VEGF) is a major target for the inhibition of tumour vascularisation and the treatment of human cancer. Many tumours produce large quantities of VEGF, and as a result, diagnosis and prognosis of cancer may be predicted by measuring changes in VEGF concentrations in blood. In blood, the VEGF may be located in the plasma, or in the blood-borne cells and formed elements, in particular, platelets and leukocytes. In this study, we collate the measurements of VEGF in platelets, leukocytes, plasma and serum for breast, prostate, colorectal and other cancers. In addition, we analysed the concentration of VEGF in tumour tissue itself, as well as for other tissues in the human body. Although the concentration of VEGF in tumours is high, the size of tumours is small compared to other tissues, in particular, skeletal muscle. Thus, the total quantity of VEGF in tumours and in blood is small compared to the quantity in muscles. This large reservoir of VEGF may have important implications for the treatment of cancer. [ABSTRACT FROM AUTHOR]

Published

2007

30. Are microRNAs located in genomic regions associated with cancer?

Author

Lamy, P., Andersen, C. L., Dyrskjøt, L., Torring, N., Ørntoft, T., and Wiuf, C.

Subjects

RNA, TUMORS, HUMAN genome, BLADDER tumors, PROSTATE tumors, COLON tumors

Abstract

We report on the location of 283 miRNAs in the human genome in relation to copy number changes in three distinct types of tumours: prostate, bladder and colon. In prostate and colon tumours, we find miRNAs over-represented in regions with copy number gain and under-represented in regions with copy number loss. Surprisingly this pattern appears to be reversed in bladder cancer. We compared our miRNA copy number data to published miRNA expression data; unexpectedly, we did not find a statistically significant relationship between miRNA copy number and expression level. This suggests that miRNA expression is regulated through different mechanisms than mRNA expression.British Journal of Cancer (2006) 95, 1415–1418. doi:10.1038/sj.bjc.6603381 www.bjcancer.com Published online 26 September 2006 [ABSTRACT FROM AUTHOR]

Published

2006

31. Anti-HER-2 DNA vaccine protects Syrian hamsters against squamous cell carcinomas.

Author

Berta, G. N., Mognetti, B., Spadaro, M., Trione, E., Amici, A., Forni, G., di Carlo, F., and Cavallo, F.

Subjects

*HAMSTERS, *DNA vaccines, *SQUAMOUS cell carcinoma, *VACCINATION, *TUMORS, *MEDICAL research, *RODENTS, *RESEARCH, *VACCINES, *MOUTH tumors, *XENOGRAFTS, *ANIMAL experimentation, *RESEARCH methodology, *CELL receptors, *CELL physiology, *MEDICAL cooperation, *EVALUATION research, *ANTIBODY formation, *COMPARATIVE studies, *CANCER vaccines, *CYTOLOGY

Abstract

This paper illustrates the efficacy of DNA vaccination through electroporation in the prevention of oral transplantable carcinoma in Syrian hamsters. At 21 and 7 days before tumour challenge, 19 hamsters were vaccinated with plasmids coding for the extracellular and transmembrane domains of rat HER-2 receptor (EC-TM plasmids), whereas 19 control hamsters were injected intramuscularly with the empty plasmid. Immediately following plasmid injection, hamsters of both groups received two square-wave 25 ms, 375 V cm(-1) electric pulses via two electrodes placed on the skin of the injection area. At day 0, all hamsters were challenged in the submucosa of the right cheek pouch with HER-2-positive HCPC I cells established in vitro from an 7,12-dimethylbenz[a]anthracene-induced oral carcinoma. This challenge gave rise to HER-2-positive buccal neoplastic lesions in 14 controls (73.37%), compared with only seven (36.8%, P<0.0027) vaccinated hamsters. In addition, the vaccinated hamsters displayed both a stronger proliferative and cytotoxic response than the controls and a significant anti-HER-2 antibody response. Most of the hamsters that rejected the challenge displayed the highest antibody titres. These findings suggest that DNA vaccination may have a future in the prevention of HER-2-positive human oral cancer. [ABSTRACT FROM AUTHOR]

Published

2005

32. REporting recommendations for tumour MARKer prognostic studies (REMARK).

Author

McShane, L. M., Altman, D. G., Sauerbrei, W., Taube, S. E., Gion, M., Clark, G. M., and Statistics Subcommittee of the NCI-EORTC Working Group on Cancer Diagnostics

Subjects

TUMORS, CANCER patients, CANCER, ONCOLOGY, TUMOR markers, DIAGNOSIS

Abstract

Despite years of research and hundreds of reports on tumour markers in oncology, the number of markers that have emerged as clinically useful is pitifully small. Often initially reported studies of a marker show great promise, but subsequent studies on the same or related markers yield inconsistent conclusions or stand in direct contradiction to the promising results. It is imperative that we attempt to understand the reasons that multiple studies of the same marker lead to differing conclusions. A variety of methodological problems have been cited to explain these discrepancies. Unfortunately, many tumour marker studies have not been reported in a rigorous fashion, and published articles often lack sufficient information to allow adequate assessment of the quality of the study or the generalisability of the study results. The development of guidelines for the reporting of tumour marker studies was a major recommendation of the US National Cancer Institute and the European Organisation for Research and Treatment of Cancer (NCI-EORTC) First International Meeting on Cancer Diagnostics in 2000. Similar to the successful CONSORT initiative for randomised trials and the STARD statement for diagnostic studies, we suggest guidelines to provide relevant information about the study design, preplanned hypotheses, patient and specimen characteristics, assay methods, and statistical analysis methods. In addition, the guidelines suggest helpful presentations of data and important elements to include in discussions. The goal of these guidelines is to encourage transparent and complete reporting so that the relevant information will be available to others to help them to judge the usefulness of the data and understand the context in which the conclusions apply. [ABSTRACT FROM AUTHOR]

Published

2005

33. Major depression in outpatients attending a regional cancer centre: screening and unmet treatment needs.

Author

Sharpe, M., Strong, V., Allen, K., Rush, R., Postma, K., Tulloh, A., Maguire, P., House, A., Ramirez, A., and Cull, A.

Subjects

MENTAL depression, PATIENTS, TUMORS, CANCER, ONCOLOGY

Abstract

A screening programme designed to identify cases of Major Depressive Disorder (MDD) in patients attending a Regional Cancer Centre outpatient department was established. It comprised two stages: (1) The Hospital Anxiety and Depression Scale (HADS) self-rating questionnaire administered by a touch-screen computer; (2) we interviewed patients with high scores on the HADS (15 or more total score) over the telephone using the depression section of the Structured Clinical Interview for DSMIV (SCID). A large consecutive sample (5613) of oncology clinic attenders was screened, and practical difficulties in the screening process were identified. The estimated prevalence of major depressive disorder (MDD) in the sample surveyed was approximately 8% (7.8%; 95% confidence intervals 6.9-8.5%). We assessed a consecutive series of 150 patients identified as having MDD to determine how many had received evidence-based treatment for MDD. Only half had discussed their low mood with their general practitioner, only one-third had been prescribed any antidepressant medication, and very few had taken a therapeutic dose for an adequate period. Very few had received psychological treatment or had been referred to mental health services. Most were receiving no potentially effective therapy.British Journal of Cancer (2004) 90, 314-320. doi:10.1038/sj.bjc.6601578 www.bjcancer.com [ABSTRACT FROM AUTHOR]

Published

2004

34. The United Kingdom Childhood Cancer Study of exposure to domestic sources of ionising radiation: 1: radon gas.

Author

UK Childhood Cancer Study Investigators

Subjects

*RESEARCH, *RADIATION-induced leukemia, *RADON, *RESEARCH methodology, *INDOOR air pollution, *POPULATION geography, *CASE-control method, *EVALUATION research, *COMPARATIVE studies, *TUMORS, *HOUSING, *ENVIRONMENTAL exposure

Abstract

This paper reports the results of the United Kingdom Childhood Cancer Study relating to risks associated with radon concentrations in participants homes at the time of diagnosis of cancer and for at least 6 months before. Results are given for 2226 case and 3773 control homes. No evidence to support an association between higher radon concentrations and risk of any of the childhood cancers was found. Indeed, evidence of decreasing cancer risks with increasing radon concentrations was observed. Adjustment for deprivation score for area of residence made little difference to this trend and similar patterns were evident in all regions and in all diagnostic groups. The study suggests that control houses had more features, such as double glazing and central heating, leading to higher radon levels than case houses. Further, case houses have features more likely to lead to lower radon levels, e.g. living-rooms above ground level. Consequently the case-control differences could have arisen because of differences between houses associated with deprivation that are not adequately allowed for by the deprivation score. [ABSTRACT FROM AUTHOR]

Published

2002

35. Hand pattern indicates prostate cancer risk.

Author

Rahman, A. A., Lophatananon, A., Stewart-Brown, S., Harriss, D., Anderson, J., Parker, T., Easton, D., Kote-Jarai, Z., Pocock, R., Dearnaley, D., Guy, M., O'Brien, L., Wilkinson, R. A., Hall, A. L., Sawyer, E., Page, E., Liu, J.-F., Eeles, R. A., Muir, K., and UK Genetic Prostate Cancer Study Collaborators

Subjects

PROSTATE cancer, MALE reproductive organs, CANCER patients, TUMORS, PATHOLOGY, HAND physiology, FINGERS, COMPARATIVE studies, RESEARCH methodology, MEDICAL cooperation, PROSTATE tumors, RESEARCH, EVALUATION research, CASE-control method, DIAGNOSIS, ANATOMY

Abstract

Background: The ratio of digit lengths is fixed in utero, and may be a proxy indicator for prenatal testosterone levels.Methods: We analysed the right-hand pattern and prostate cancer risk in 1524 prostate cancer cases and 3044 population-based controls.Results: Compared with index finger shorter than ring finger (low 2D : 4D), men with index finger longer than ring finger (high 2D : 4D) showed a negative association, suggesting a protective effect with a 33% risk reduction (odds ratio (OR) 0.67, 95% confidence interval (CI) 0.57-0.80). Risk reduction was even greater (87%) in age group <60 (OR 0.13, 95% CI 0.09-0.21).Conclusion: Pattern of finger lengths may be a simple marker of prostate cancer risk, with length of 2D greater than 4D suggestive of lower risk. [ABSTRACT FROM AUTHOR]

Published

2011

36. Prevalence of the metabolic syndrome and cardiovascular disease risk in chemotherapy-treated testicular germ cell tumour survivors.

Author

Willemse, P M, Burggraaf, J, Hamdy, N A T, Weijl, N I, Vossen, C Y, van Wulften, L, van Steijn-van Tol, A Q M J, Rosendaal, F R, and Osanto, S

Subjects

TUMORS, METABOLIC syndrome, CANCER chemotherapy, PATIENTS

Abstract

A correction to the article "Prevalence of the metabolic syndrome and cardiovascular disease risk in chemotherapy treated testicular germ cell tumour survivors" published in the 2013 issue is presented.

Published

2013

37. Multistage carcinogenesis.

Author

Weiss, R. A.

Subjects

CARCINOGENESIS, CANCER, GENETIC mutation, MUTAGENS, NEOPLASTIC cell transformation, TUMORS

Abstract

The article focuses on the multistage theory of carcinogenesis. Researchers Peter Armitage and Richard Doll showed that , for a variety of nonendocrine carcinomas, the incidence of tumors increased with the sixth power of age. From this observation they postulated the multistage theory of carcinogenesis and inferred six to seven independent, sequential and stable events occurring in the cancer lineage before malignancy became manifest. Despite the evidence that most carcinogens were mutagens, cancer was still not universally accepted as a somatic genetic disease. The development of familial cancers at relatively young ages can be attributed to the first mutational event being inherited, either as a dominant trait, or as a recessive tumour suppressor gene as elucidated for the Rb retinoblastosis locus.

Published

2004

38. Big Data: the challenge for small research groups in the era of cancer genomics.

Author

Noor, Aisyah Mohd, Holmberg, Lars, Gillett, Cheryl, and Grigoriadis, Anita

Subjects

BIG data, CANCER research, HUMAN genome, CANCER treatment, INFORMATION technology, INFORMATION retrieval, RESEARCH funding, TUMORS, GENOMICS, DATA analysis, SEQUENCE analysis, ECONOMICS

Abstract

In the past decade, cancer research has seen an increasing trend towards high-throughput techniques and translational approaches. The increasing availability of assays that utilise smaller quantities of source material and produce higher volumes of data output have resulted in the necessity for data storage solutions beyond those previously used. Multifactorial data, both large in sample size and heterogeneous in context, needs to be integrated in a standardised, cost-effective and secure manner. This requires technical solutions and administrative support not normally financially accounted for in small- to moderate-sized research groups. In this review, we highlight the Big Data challenges faced by translational research groups in the precision medicine era; an era in which the genomes of over 75,000 patients will be sequenced by the National Health Service over the next 3 years to advance healthcare. In particular, we have looked at three main themes of data management in relation to cancer research, namely (1) cancer ontology management, (2) IT infrastructures that have been developed to support data management and (3) the unique ethical challenges introduced by utilising Big Data in research. [ABSTRACT FROM AUTHOR]

Published

2015

39. International study of the place of death of people with cancer: a population-level comparison of 14 countries across 4 continents using death certificate data.

Author

Cohen, J, Pivodic, L, Miccinesi, G, Onwuteaka-Philipsen, B D, Naylor, W A, Wilson, D M, Loucka, M, Csikos, A, Pardon, K, Van den Block, L, Ruiz-Ramos, M, Cardenas-Turanzas, M, Rhee, Y, Aubry, R, Hunt, K, Teno, J, Houttekier, D, and Deliens, L

Subjects

HOSPITAL statistics, TERMINAL care statistics, COMPARATIVE studies, CAUSES of death, LONG-term health care, RESEARCH methodology, MEDICAL cooperation, PALLIATIVE treatment, RESEARCH, TUMORS, DEATH certificates, EVALUATION research, CROSS-sectional method

Abstract

Background: Where people die can influence a number of indicators of the quality of dying. We aimed to describe the place of death of people with cancer and its associations with clinical, socio-demographic and healthcare supply characteristics in 14 countries.Methods: Cross-sectional study using death certificate data for all deaths from cancer (ICD-10 codes C00-C97) in 2008 in Belgium, Canada, Czech Republic, England, France, Hungary, Italy, Mexico, the Netherlands, New Zealand, South Korea, Spain (2010), USA (2007) and Wales (N=1,355,910). Multivariable logistic regression analyses evaluated factors associated with home death within countries and differences across countries.Results: Between 12% (South Korea) and 57% (Mexico) of cancer deaths occurred at home; between 26% (Netherlands, New Zealand) and 87% (South Korea) occurred in hospital. The large between-country differences in home or hospital deaths were partly explained by differences in availability of hospital- and long-term care beds and general practitioners. Haematologic rather than solid cancer (odds ratios (ORs) 1.29-3.17) and being married rather than divorced (ORs 1.17-2.54) were most consistently associated with home death across countries.Conclusions: A large country variation in the place of death can partly be explained by countries' healthcare resources. Country-specific choices regarding the organisation of end-of-life cancer care likely explain an additional part. These findings indicate the further challenge to evaluate how different specific policies can influence place of death patterns. [ABSTRACT FROM AUTHOR]

Published

2015

40. The impact of patient comorbidity on cancer stage at diagnosis.

Author

Gurney, Jason, Sarfati, Diana, and Stanley, James

Subjects

TUMOR diagnosis, TUMORS, TUMOR classification, COMORBIDITY

Abstract

Background: It is known that cancer stage is affected by comorbidity, but the evidence regarding the magnitude and even direction of this effect is highly inconsistent and poorly understood. The aims of this study were to establish the impact of comorbidity on cancer stage at diagnosis, using both specific individual comorbid conditions and a global measure of comorbidity; and to assess whether this impact varied by cancer site, level of comorbidity burden and individual comorbidity type.Methods: We examined comorbidity among 14,096 patients with breast, colon, rectal, liver, stomach, ovarian, uterine, bladder or kidney cancer. Patients were identified from cancer registry data, and then linked to hospitalisation data to determine the presence of comorbidity in the 5 years preceding cancer diagnosis. Individual comorbid conditions were identified using ICD-10 codes, and overall burden of comorbidity attributed using a cancer-specific measure of comorbidity (C3 Index).Results: We observed that the presence of patient comorbidity (a) increases the odds of being diagnosed with distant metastases, (b) does not lead to earlier diagnosis and (c) increases the likelihood of a patient receiving no stage of disease at diagnosis.Conclusions: Patient comorbidity has a substantial impact on cancer stage at diagnosis; however, this impact varies considerably by cancer type, individual comorbid condition and overall comorbidity burden. [ABSTRACT FROM AUTHOR]

Published

2015

41. Serum lactate dehydrogenase and survival following cancer diagnosis.

Author

Wulaningsih, Wahyu, Holmberg, Lars, Garmo, Hans, Malmstrom, Håkan, Lambe, Mats, Hammar, Niklas, Walldius, Göran, Jungner, Ingmar, Ng, Tony, Van Hemelrijck, Mieke, Malmstrom, Håkan, and Walldius, Göran

Subjects

TUMOR diagnosis, LACTATE dehydrogenase, RESEARCH funding, TUMORS

Abstract

Background: There is evidence that high level of serum lactate dehydrogenase (LDH) is associated with poorer overall survival in several malignancies, but its link to cancer-specific survival is unclear.Methods: A total of 7895 individuals diagnosed with cancer between 1986 and 1999 were selected for this study. Multivariable Cox proportional hazards regression was used to assess overall and cancer-specific death by the z-score and clinical categories of serum LDH prospectively collected within 3 years before diagnosis. Site-specific analysis was performed for major cancers. Analysis was repeated by different lag times between LDH measurements and diagnosis.Results: At the end of follow-up, 5799 participants were deceased. Hazard ratios (HRs) and 95% confidence intervals (CIs) for overall and cancer-specific death in the multivariable model were 1.43 (1.31-1.56) and 1.46 (1.32-1.61), respectively, for high compared with low prediagnostic LDH. Site-specific analysis showed high LDH to correlate with an increased risk of death from prostate, pulmonary, colorectal, gastro-oesophageal, gynaecological and haematological cancers. Serum LDH assessed within intervals closer to diagnosis was more strongly associated with overall and cancer-specific death.Conclusions: Our findings demonstrated an inverse association of baseline serum LDH with cancer-specific survival, corroborating its role in cancer progression. [ABSTRACT FROM AUTHOR]

Published

2015

42. Decomposition of spontaneous fluctuations in tumour oxygenation using BOLD MRI and independent component analysis.

Author

Gonçalves, Miguel R, Johnson, S Peter, Ramasawmy, Rajiv, Pedley, R Barbara, Lythgoe, Mark F, Walker-Samuel, Simon, and Gonçalves, Miguel R

Subjects

OXYGEN metabolism, ANIMAL experimentation, HYPOXEMIA, CELL lines, HEMOGLOBINS, MAGNETIC resonance imaging, MICE, RESEARCH funding, TUMORS

Abstract

Background: Solid tumours can undergo cycles of hypoxia, followed by reoxygenation, which can have significant implications for the success of anticancer therapies. A need therefore exists to develop methods to aid its detection and to further characterise its biological basis. We present here a novel method for decomposing systemic and tumour-specific contributions to fluctuations in tumour deoxyhaemoglobin concentration, based on magnetic resonance imaging measurements.Methods: Fluctuations in deoxyhaemoglobin concentration in two tumour xenograft models of colorectal carcinoma were decomposed into distinct contributions using independent component analysis. These components were then correlated with systemic pulse oximetry measurements to assess the influence of systemic variations in blood oxygenation in tumours, compared with those that arise within the tumour itself (tumour-specific). Immunohistochemical staining was used to assess the physiological basis of each source of fluctuation.Results: Systemic fluctuations in blood oxygenation were found to contribute to cycling hypoxia in tumours, but tumour-specific fluctuations were also evident. Moreover, the size of the tumours was found to influence the degree of systemic, but not tumour-specific, oscillations. The degree of vessel maturation was related to the amplitude of tumour-specific, but not systemic, oscillations.Conclusions: Our results provide further insights into the complexity of spontaneous fluctuations in tumour oxygenation and its relationship with tumour pathophysiology. These observations could be used to develop improved drug delivery strategies. [ABSTRACT FROM AUTHOR]

Published

2015

43. PIK3CA oncogenic mutations represent a major mechanism of resistance to trastuzumab in HER2/neu overexpressing uterine serous carcinomas.

Author

Black, Jonathan D, Lopez, Salvatore, Cocco, Emiliano, Bellone, Stefania, Altwerger, Gary, Schwab, Carlton L, English, Diana P, Bonazzoli, Elena, Predolini, Federica, Ferrari, Francesca, Ratner, Elena, Silasi, Dan-Arin, Azodi, Masoud, Schwartz, Peter E, and Santin, Alessandro D

Subjects

ANTINEOPLASTIC agents, ANIMALS, CELL physiology, DRUG resistance in cancer cells, GENE amplification, MICE, GENETIC mutation, RESEARCH funding, TUMORS, UTERINE tumors, TRASTUZUMAB, PHARMACODYNAMICS

Abstract

Objectives: We evaluated the role of PIK3CA-mutations as mechanism of resistance to trastuzumab in primary HER2/neu-amplified uterine-serous-carcinoma (USC) cell lines.Methods: Fifteen whole-exome-sequenced USC cell lines were tested for HER2/neu-amplification and PIK3CA-mutations. Four HER2/neu-amplified USC (2-harbouring wild-type-PIK3CA-genes and 2-harbouring oncogenic-PIK3CA-mutations) were evaluated in in vitro dose-titration-proliferation-assays, cell-viability and HER2 and S6-protein-phosphorylation after exposure to trastuzumab. USC harbouring wild-type-PIK3CA were transfected with plasmids encoding oncogenic PIK3CA-mutations (i.e., H1047R/R93Q) and exposed to trastuzumab. Finally, trastuzumab efficacy was tested by using two USC xenograft mouse models.Results: Seven out of fifteen (46%) of the USC cell lines were HER2/neu-amplified by fluorescence in situ hybridisation. Within these tumours four out of seven (57%) were found to harbour oncogenic PIK3CA-mutations vs two out of eight (25%) of the HER2/neu not amplified cell lines (P=0.01). HER2/neu-amplified/PIK3CA-mutated USC were highly resistant to trastuzumab when compared with HER2/neu-amplified/wild-type-PIK3CA cell lines (P=0.02). HER2/neu-amplified/PIK3CA wild-type cell lines transfected with oncogenic PIK3CA-mutations increased their resistance to trastuzumab (P<0.0001). Trastuzumab was effective in reducing tumour growth (P=0.001) and improved survival (P=0.0001) in mouse xenografts harbouring HER2-amplified/PIK3CA wild-type USC but not in HER2-amplified/PIK3CA-mutated tumours.Conclusions: Oncogenic PIK3CA mutations are common in HER2/neu-amplified USC and may constitute a major mechanism of resistance to trastuzumab treatment. [ABSTRACT FROM AUTHOR]

Published

2015

44. Aspects of mental health dysfunction among survivors of childhood cancer.

Author

Fidler, Miranda M, Ziff, Oliver J, Wang, Sarra, Cave, Joshua, Janardhanan, Pradeep, Winter, David L, Kelly, Julie, Mehta, Susan, Jenkinson, Helen, Frobisher, Clare, Reulen, Raoul C, and Hawkins, Michael M

Subjects

MENTAL illness risk factors, TUMORS in children, CANCER patient psychology, HEALTH surveys, RESEARCH funding, PSYCHOLOGY of the sick, SURVEYS, TUMORS, DISEASE complications, PSYCHOLOGY

Abstract

Background: Some previous studies have reported that survivors of childhood cancer are at an increased risk of developing long-term mental health morbidity, whilst others have reported that this is not the case. Therefore, we analysed 5-year survivors of childhood cancer using the British Childhood Cancer Survivor Study (BCCSS) to determine the risks of aspects of long-term mental health dysfunction.Procedure: Within the BCCSS, 10 488 survivors completed a questionnaire that ascertained mental health-related information via 10 questions from the Short Form-36 survey. Internal analyses were conducted using multivariable logistic regression to determine risk factors for mental health dysfunction. External analyses were undertaken using direct standardisation to compare mental health dysfunction in survivors with UK norms.Results: This study has shown that overall, childhood cancer survivors had a significantly higher prevalence of mental health dysfunction for 6/10 questions analysed compared to UK norms. Central nervous system (CNS) and bone sarcoma survivors reported the greatest dysfunction, compared to expected, with significant excess dysfunction in 10 and 6 questions, respectively; the excess ranged from 4.4-22.3% in CNS survivors and 6.9-15.9% in bone sarcoma survivors. Compared to expected, excess mental health dysfunction increased with attained age; this increase was greatest for reporting 'limitations in social activities due to health', where the excess rose from 4.5% to 12.8% in those aged 16-24 and 45+, respectively. Within the internal analyses, higher levels of educational attainment and socio-economic classification were protective against mental health dysfunction.Conclusions: Based upon the findings of this large population-based study, childhood cancer survivors report significantly higher levels of mental health dysfunction than those in the general population, where deficits were observed particularly among CNS and bone sarcoma survivors. Limitations were also observed to increase with age, and thus it is important to emphasise the need for mental health evaluation and services across the entire lifespan. There is evidence that low educational attainment and being unemployed or having never worked adversely impacts long-term mental health. These findings provide an evidence base for risk stratification and planning interventions. [ABSTRACT FROM AUTHOR]

Published

2015

45. TNF-alpha and melphalan-based isolated limb perfusion: no evidence supporting the early destruction of tumour vasculature.

Author

Podleska, L E, Funk, K, Umutlu, L, Grabellus, F, Taeger, G, and de Groot, H

Subjects

OXYGEN metabolism, ANTINEOPLASTIC agents, BLOOD circulation, CANCER chemotherapy, EXTREMITIES (Anatomy), HEMOGLOBINS, MUSCLES, THERMOTHERAPY, TUMOR necrosis factors, TUMORS, PATHOLOGIC neovascularization, MELPHALAN

Published

2015

46. Target gene mutational pattern in Lynch syndrome colorectal carcinomas according to tumour location and germline mutation.

Author

Pinheiro, Manuela, Pinto, Carla, Peixoto, Ana, Veiga, Isabel, Lopes, Paula, Henrique, Rui, Baldaia, Helena, Carneiro, Fátima, Seruca, Raquel, Tomlinson, Ian, Kovac, Michal, Heinimann, Karl, and Teixeira, Manuel R

Subjects

HEREDITARY nonpolyposis colorectal cancer, TUMORS, GENETIC mutation, CARCINOGENESIS, GERM cells

Abstract

Background:We previously reported that the target genes in sporadic mismatch repair (MMR)-deficient colorectal carcinomas (CRCs) in the distal colon differ from those occurring elsewhere in the colon. This study aimed to compare the target gene mutational pattern in microsatellite instability (MSI) CRC from Lynch syndrome patients stratified by tumour location and germline mutation, as well as with that of sporadic disease.Methods:A series of CRC from Lynch syndrome patients was analysed for MSI in genes predicted to be selective MSI targets and known to be involved in several pathways of colorectal carcinogenesis.Results:The most frequently mutated genes belong to the TGF-β superfamily pathway, namely ACVR2A and TGFBR2. A significantly higher frequency of target gene mutations was observed in CRC from patients with germline mutations in MLH1 or MSH2 when compared with MSH6. Mutations in microsatellite sequences (A)7 of BMPR2 and (A)8 of MSH3 were significantly more frequent in the distal CRC. Additionally, we observed differences in MSH3 and TGFBR2 mutational frequency between Lynch syndrome and sporadic MSI CRC regarding tumour location.Conclusions:Our results indicate that the pattern of genetic changes differs in CRC depending on tumour location and between Lynch syndrome and sporadic MSI CRC, suggesting that carcinogenesis can occur by different pathways even if driven by generalised MSI. [ABSTRACT FROM AUTHOR]

Published

2015

47. Temporal trends in mode, site and stage of presentation with the introduction of colorectal cancer screening: a decade of experience from the West of Scotland.

Author

Mansouri, D, McMillan, D C, Crearie, C, Morrison, D S, Crighton, E M, and Horgan, P G

Subjects

COLON cancer diagnosis, MORTALITY, TUMORS, RECTAL cancer, DIAGNOSIS

Abstract

Background:Population colorectal cancer screening programmes have been introduced to reduce cancer-specific mortality through the detection of early-stage disease. The present study aimed to examine the impact of screening introduction in the West of Scotland.Methods:Data on all patients with a diagnosis of colorectal cancer between January 2003 and December 2012 were extracted from a prospectively maintained regional audit database. Changes in mode, site and stage of presentation before, during and after screening introduction were examined.Results:In a population of 2.4 million, over a 10-year period, 14 487 incident cases of colorectal cancer were noted. Of these, 7827 (54%) were males and 7727 (53%) were socioeconomically deprived. In the postscreening era, 18% were diagnosed via the screening programme. There was a reduction in both emergency presentation (20% prescreening vs 13% postscreening, P⩽0.001) and the proportion of rectal cancers (34% prescreening vs 31% pos-screening, P⩽0.001) over the timeframe. Within non-metastatic disease, an increase in the proportion of stage I tumours at diagnosis was noted (17% prescreening vs 28% postscreening, P⩽0.001).Conclusions:Within non-metastatic disease, a shift towards earlier stage at diagnosis has accompanied the introduction of a national screening programme. Such a change should lead to improved outcomes in patients with colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2015

48. Ethnicity, deprivation and screening: survival from breast cancer among screening-eligible women in the West Midlands diagnosed from 1989 to 2011.

Author

Morris, M, Woods, L M, Rogers, N, O'Sullivan, E, Kearins, O, and Rachet, B

Subjects

EQUALITY research, BREAST cancer research, ETHNICITY, WOMEN, TUMORS

Abstract

Background:Social inequalities in breast cancer survival are smaller when the cancer is screen-detected. We examined survival from screen-detected and non screen-detected breast cancer by ethnicity and deprivation.Methods:Cancer registry data for 20 283 women aged 50-70 years, diagnosed between 1989-2011 and invited for screening, were linked with screening and ethnicity data. We examined Asian, Black and White groups, less deprived and middle/more deprived women. Net survival was estimated using ethnic- and deprivation-specific life tables. Estimates were corrected for lead-time bias and over-diagnosis.Results:Net survival varied by screening history. No significant differences in survival were found by ethnicity. Five-year net survival was 90.0% (95% CI, 89.3-90.8%) in less deprived groups and 86.7% (85.9-87.4%) among middle/more deprived women. Screening benefitted all ethnic and both deprivation groups. Whether screen-detected or not, more deprived women had significantly poorer outcomes: 5-year net survival was 78.0% (76.7-79.2%) for deprived women who were not screen-detected compared with 94.0% (93.1-95.1%) for less deprived women who were screen-detected.Conclusions:The three ethnic groups differed little in their breast cancer survival. Although screening confers a survival benefit to all, there are still wide disparities in survival by deprivation. More needs to be done to determine what underlies these differences and tackle them. [ABSTRACT FROM AUTHOR]

Published

2015

49. BRCA1 and BRCA2 mutations sensitize to chemotherapy in patient-derived pancreatic cancer xenografts.

Author

Lohse, I, Borgida, A, Cao, P, Cheung, M, Pintilie, M, Bianco, T, Holter, S, Ibrahimov, E, Kumareswaran, R, Bristow, R G, Tsao, M-S, Gallinger, S, and Hedley, D W

Subjects

GERM cells, TUMORS, BRCA genes, CISPLATIN, PANCREATIC cancer

Abstract

Background:Germline mutations of the BRCA tumour suppressors have been associated with increased risk of pancreatic cancer. Clinical evidence suggests that these patients may be more sensitive to treatment with cisplatin. As the frequency of germline BRCA mutations is low, definitive experimental data to support the clinical observations are still missing.Methods:We tested gemcitabine and cisplatin sensitivity of four BRCA1 and BRCA2 mutant and three BRCA1 and BRCA2 wild-type (WT) patient-derived pancreatic cancer xenografts.Results:We observed treatment sensitivity to gemcitabine and cisplatin in the BRCA WT and mutant models. The BRCA1 and BRCA2 mutant xenografts were significantly more sensitive to cisplatin although these models also showed sensitivity to gemcitabine. The BRCA1 and BRCA2 WT models showed sensitivity to gemcitabine but not cisplatin. Treatment sensitivity in the xenograft models closely resembled treatment response in the corresponding patients.Discussion:We have characterised a panel of xenografts derived from pancreatic cancer patients carrying germline BRCA mutations, and shown that their genetic features resemble the patient donor. Our results support further clinical testing of treatment regimens combining gemcitabine and platinum drugs in this patient population, as well as preclinical research aiming to identify mechanisms of cisplatin resistance in BRCA mutant pancreatic cancers. [ABSTRACT FROM AUTHOR]

Published

2015

50. Overexpression of the RNA-binding proteins Lin28B and IGF2BP3 (IMP3) is associated with chemoresistance and poor disease outcome in ovarian cancer.

Author

Hsu, K-F, Shen, M-R, Huang, Y-F, Cheng, Y-M, Lin, S-H, Chow, N-H, Cheng, S-W, Chou, C-Y, and Ho, C-L

Subjects

MESSENGER RNA, TUMORS, CARCINOGENESIS, SOMATOMEDIN

Abstract

Background:RNA-binding proteins have an important role in messenger RNA (mRNA) regulation during tumour development and carcinogenesis. In the present study, we examined the insulin-like growth factor 2 mRNA-binding proteins (IGF2BPs; hereafter refered to as IMPs) and Lin28 family expressions in epithelial ovarian carcinoma (EOC) patients and correlated their expression levels with the response to chemotherapy, hCTR1 expression and patient survival.Methods:Patients clinical information, real-time RT-PCR, immunohistochemistry, western blot, Transwell migration invasion assays, and cytotoxicity assays were used.Results:From 140 EOC patients, high expression of IMP3 or Lin28B was associated with poor survival, and women diagnosed at advanced stages with elevated IMP3 and Lin28B were at higher risk of developing chemoresistance. High IMP3 levels combined with high Lin28B levels significantly correlated with the poorest 5-year survival rates. Knockdown of IMP3 or Lin28B decreased cell proliferation, migration, and invasion, and increased the platinum sensitivity, but not taxol sensitivity, of ovarian cancer cells through increased expression of hCTR1, a copper transporter involved in platinum uptake. High expression of hCTR1 correlated with low expression of IMP3/Lin28B and better progression-free survival in advanced-stage EOC patients.Conclusion:Testing for a combination of elevated IMP3 and Lin28B levels could further facilitate the identification of a patient subgroup with the worst prognosis. [ABSTRACT FROM AUTHOR]

Published

2015