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Dive into the research topics where Claire Blesing is active.

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Featured researches published by Claire Blesing.


Clinical Cancer Research | 2016

Clinical Trial of Oral Nelfinavir before and during Radiation Therapy for Advanced Rectal Cancer.

Esme J. Hill; Corran Roberts; Jamie Franklin; Monica Enescu; Nicholas P. West; Thomas P. MacGregor; Kwun-Ye Chu; Lucy Boyle; Claire Blesing; Lai-Mun Wang; Somnath Mukherjee; Ewan M. Anderson; Gina Brown; Susan Dutton; Sharon Love; Julia A. Schnabel; Phil Quirke; Ruth J. Muschel; W.G. McKenna; Michael Partridge; Ricky A. Sharma

Purpose: Nelfinavir, a PI3K pathway inhibitor, is a radiosensitizer that increases tumor blood flow in preclinical models. We conducted an early-phase study to demonstrate the safety of nelfinavir combined with hypofractionated radiotherapy (RT) and to develop biomarkers of tumor perfusion and radiosensitization for this combinatorial approach. Experimental Design: Ten patients with T3-4 N0-2 M1 rectal cancer received 7 days of oral nelfinavir (1,250 mg b.i.d.) and a further 7 days of nelfinavir during pelvic RT (25 Gy/5 fractions/7 days). Perfusion CT (p-CT) and DCE-MRI scans were performed pretreatment, after 7 days of nelfinavir and prior to the last fraction of RT. Biopsies taken pretreatment and 7 days after the last fraction of RT were analyzed for tumor cell density (TCD). Results: There were 3 drug-related grade 3 adverse events: diarrhea, rash, and lymphopenia. On DCE-MRI, there was a mean 42% increase in median Ktrans, and a corresponding median 30% increase in mean blood flow on p-CT during RT in combination with nelfinavir. Median TCD decreased from 24.3% at baseline to 9.2% in biopsies taken 7 days after RT (P = 0.01). Overall, 5 of 9 evaluable patients exhibited good tumor regression on MRI assessed by tumor regression grade (mrTRG). Conclusions: This is the first study to evaluate nelfinavir in combination with RT without concurrent chemotherapy. It has shown that nelfinavir-RT is well tolerated and is associated with increased blood flow to rectal tumors. The efficacy of nelfinavir-RT versus RT alone merits clinical evaluation, including measurement of tumor blood flow. Clin Cancer Res; 22(8); 1922–31. ©2016 AACR. See related commentary by Meyn et al., p. 1834


Neuro-Oncology Practice | 2016

Bevacizumab in Neurofibromatosis type 2 (NF2) related vestibular schwannomas: a nationally coordinated approach to delivery and prospective evaluation

John F. Golding; Patrick Axon; Shazia K. Afridi; Claire Blesing; Rosalie E. Ferner; Dorothy Halliday; Raj Jena; Pieter Pretorius; D. Gareth Evans; Martin McCabe; Allyson Parry

Background NF2 patients develop multiple nervous system tumors including bilateral vestibular schwannomas (VS). The tumors and their surgical treatment are associated with deafness, neurological disability, and mortality.Medical treatment with bevacizumab has been reported to reduce VS growth and to improve hearing. In addition to evaluating these effects, this study also aimed to determine other important consequences of treatment including patient-reported quality of life and the impact of treatment on surgical VS rates. Methods Patients treated with bevacizumab underwent serial prospective MRI, audiology, clinical, CTCAE-4.0 adverse events, and NFTI-QOL quality-of-life assessments. Tumor volumetrics were classified according to the REiNs criteria and annual VS surgical rates reviewed. Results Sixty-one patients (59% male), median age 25 years (range, 10-57), were reviewed. Median follow-up was 23 months (range, 3-53). Partial volumetric tumor response (all tumors) was seen in 39% and 51% had stabilization of previously growing tumors. Age and pretreatment growth rate were predictors of response. Hearing was maintained or improved in 86% of assessable patients. Mean NFTI-QOL scores improved from 12.0 to 10.7 (P < .05). Hypertension was observed in 30% and proteinuria in 16%. Twelve treatment breaks occurred due to adverse events. The rates of VS surgery decreased after the introduction of bevacizumab. Conclusion Treatment with bevacizumab in this large, UK-wide cohort decreased VS growth rates and improved hearing and quality of life. The potential risk of surgical iatrogenic damage was also reduced due to an associated reduction in VS surgical rates. Ongoing follow-up of this cohort will determine the long-term benefits and risks of bevacizumab treatment.


Nature Reviews Clinical Oncology | 2009

Cerebral primitive neuroectodermal tumor in an adult with a heterozygous MSH2 mutation

Alexander Jeans; Ian Frayling; Bharat Jasani; Lucy Side; Claire Blesing; Olaf Ansorge

Background. A 37-year-old woman presented with a supratentorial cerebral mass, which was diagnosed histologically as a primitive neuroectodermal tumor. She had been treated for rectal adenocarcinoma 7 years previously. A family history revealed a young-onset colorectal carcinoma in the patients father.Investigations. Immunohistochemical analysis for DNA mismatch repair proteins, germline mutation analysis of MSH2.Diagnosis. Lynch syndrome with a heterozygous germline mutation in MSH2.Management. Debulking of the cerebral tumor, craniospinal axis radiotherapy, and genetic counseling of family.


Radiotherapy and Oncology | 2011

930 poster CHEMO-RADIOTHERAPY IN GLIOBLASTOMA MULTIFORME. THE EFFECT OF MGMT PROMOTER HYPERMETHYLATION ON SURVIVAL

P.R. Jampana; Claire Blesing; N. Warner; O. Ansorge

CHEMO-RADIOTHERAPY IN GLIOBLASTOMA MULTIFORME. THE EFFECT OF MGMT PROMOTER HYPERMETHYLATION ON SURVIVAL P. R. Jampana1, C. Blesing2, N. Warner1, O. Ansorge3 1 OXFORD CANCER CENTRE, CHURCHILL HOSPITAL, Oxford, United Kingdom 2 OXFORD CANCER CENTRE, CHURCHILL HOSPITAL, Clinical Oncology, Oxford, United Kingdom 3 OXFORD RADCLIFFE HOSPITALS NHS TRUST, Department of NeuroPathology, Oxford, United Kingdom


Journal of Neuro-oncology | 2017

Toxicity profile of bevacizumab in the UK Neurofibromatosis type 2 cohort

John F. Golding; Claire Blesing; D. Gareth Evans; Rosalie E. Ferner; Karen Foweraker; Dorothy Halliday; Raj Jena; Catherine McBain; Martin McCabe; Angela Swampillai; Nicola Warner; Shaun Wilson; Allyson Parry; Shazia K. Afridi


Radiotherapy and Oncology | 2010

A reply to evidence-based radiation oncology: oesophagus

R. S. Gillies; Mark R. Middleton; Claire Blesing


Annals of Oncology | 2017

P-044Weekly carboplatin/paclitaxel (CP) based definitive chemoradiotherapy (dCRT) for patients with inoperable oesophageal cancer unsuitable for cisplatin-fluoropyrimidine based dCRT: A single centre experience

Robert Owens; Nicola Warner; Claire Blesing; Faouzi Djebbari; Gavin Reilly; Somnath Mukherjee


Archive | 2016

Bevacizumab in NF2-related vestibular schwannomas: a nationally coordinated approach to delivery and prospective evaluation

John F. Golding; Shazia K. Afridi; Claire Blesing; Rosalie E. Ferner; Dorothy Halliday; Raj Jena; P.M. Pretorius; Allyson Parry; Patrick Axon; D.G. Evans; Martin McCabe


Annals of Oncology | 2016

PD-039Role of adjuvant radiotherapy following neo-adjuvant chemotherapy (NACT) and surgery in oesophageal cancer – a multi-centre retrospective cohort study

S. Teoh; P S Virdee; J. Mason; Nicola Warner; Claire Blesing; K. Patel; R. Marshall; N. Maynard; B. Sgromo; R. Gillies; C. Streets; C. Barham; A. Hollowood; Jane M Blazeby; D. Titcomb; Stephen Falk; Somnath Mukherjee


Journal of Clinical Oncology | 2014

Oral nelfinavir before and during radiation therapy for rectal cancer: Changes in tumor perfusion and correlation between tissue and radiological markers of response.

Esme J. Hill; Monica Enescu; Nicholas P. West; Jamie Franklin; Kwun-Ye Chu; Jun Li; Deborah Whittington; Thomas P. MacGregor; Shazad Ashraf; Claire Blesing; Somnath Mukherjee; Margaret Betts; Andrew Slater; Ewan M. Anderson; Gina Brown; Julia A. Schnabel; Mike Partridge; P. Quirke; Ricky A. Sharma

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John F. Golding

University of Westminster

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Martin McCabe

University of Manchester

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Raj Jena

University of Cambridge

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Shazia K. Afridi

Guy's and St Thomas' NHS Foundation Trust

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