Molecular evaluation of radiosensitivity in bladder cancer

Lyrakos, Nikolaos

January 2004

No description available.

616.99462

Clinical and molecular prognostic factors in superficial bladder cancer

Bhardwa, Jeetesh Maganlal

January 2008

Aim: To identify molecular clinical and molecular prognostic indicators markers for superficial bladder cancer. Univariate statistical analysis of the clinical database revealed grade (p<0.001, Log rank test) and positive urine cytology at presentation (p= 0.002 Log rank test) are highly significant for recurrence and progression.

616.99462

Isolation and characterisation of a novel gene involved in urothelial tissue integrity and cell adhesion

Hailes, Fiona

January 2003

No description available.

616.99462

Growth and survival of normal and paramalignant human urothelial cells

MacLaine, Nicola J.

January 2005

No description available.

616.99462

The role of epidermal growth factor inhibitors on bladder cancer growth and invasion

Lazarowicz, Henry Peter

January 2007

No description available.

616.99462

Physical and functional mapping of a candidate tumour suppressor region on the short arm of chromosome 8 in bladder cancer

Adams, Jacqueline

January 2003

No description available.

616.99462

Molecular epidemiology of DNA damage response to double strand breaks in bladder cancer

Choudhury, Ananya

January 2008

No description available.

616.99462

Proteomic-based approaches to the identification of bladder tumour markers

Munro, Nicholas Pitt

January 2006

No description available.

616.99462

Surrogate markers in transitional cell carcinoma of bladder

McKnight, J. J.

January 2004

No description available.

616.99462

Plasma protein profiling for bladder cancer biomarker discovery using UPLC-HDMS^E label-free quantitation

Hakimi, Amirmansoor

January 2013

In the UK, bladder cancer is the 4th most common cancer in men and 11th most common in women. In 2010, just over 10,000 new cases were diagnosed and 4,900 deaths were recorded. At their first diagnosis, the majority of bladder cancer patients (75-85%) present with non-muscle invasive disease. In 50-70% of these patients the tumour will recur and in 10-20% of them it will progress to muscle invasive disease. Mass spectrometry based proteomics has been chosen for clinical biomarker discovery due to its ability to perform qualitative and quantitative protein profiling on clinical samples. In total 90 plasma samples were used in this study in two groups of disease and control. An optimised and evaluated UPLC-IMS-DIA-MS^E label-free quantitation method was used for plasma protein profiling. To our knowledge, this is the first report investigating the biomarkers of bladder cancer incorporating label-free quantitation and UPLC-IMS-DIA-MS^E methodology. To assess expression level of proteins of samples in different groups a plan consisting of four data processing packages was used. Each of the packages uses different statistical means by which to identify proteins and/or compare expression levels alteration. Optimisation of the methodology helped in the thorough investigation of the plasma proteome with coverage of up to five orders of magnitude of plasma protein concentration dynamic range. In total, 11 proteins were found as possible markers of diagnosis for bladder cancer. Four of these candidates (afamin, alpha 1-B-glycoprotein, apolipoprotein-A1 and haptoglobin) were previously reported to be urinary markers of bladder cancer. CRP was overexpressed when plasma samples from patients with low grade-Ta tumours were compared to every other sample and may be used as a diagnostic marker. Similarly, afamin and haptoglobin were overexpressed in plasma samples from patients with high grade-high stage tumours when compared to samples from patients with high grade-low stage disease.

616.99462