Your search keyword '"Price PM"' showing total 152 results

51. Increasing expression of hypoxia-inducible proteins in the Barrett's metaplasia-dysplasia-adenocarcinoma sequence.

Author

Griffiths EA, Pritchard SA, McGrath SM, Valentine HR, Price PM, Welch IM, and West CM

Subjects

Adenocarcinoma genetics, Barrett Esophagus genetics, Biopsy, Disease Progression, Epithelial Cells cytology, Epithelial Cells pathology, Esophageal Diseases pathology, Esophageal Neoplasms genetics, Esophagus cytology, Esophagus pathology, Immunohistochemistry, Ki-67 Antigen metabolism, Metaplasia, Receptors, Erythropoietin metabolism, Reference Values, Vascular Endothelial Growth Factor A metabolism, Adenocarcinoma pathology, Barrett Esophagus pathology, Basic Helix-Loop-Helix Transcription Factors metabolism, Esophageal Neoplasms pathology, Hypoxia-Inducible Factor 1, alpha Subunit metabolism

Abstract

Hypoxia-associated markers are involved in the progression of several malignancies, but are relatively unstudied in Barrett's carcinogenesis. Our aim was to assess the immunohistochemical expression of hypoxia-inducible factor (HIF)-1alpha, HIF-2alpha, erythropoietin (Epo), Epo receptor (Epo-R), Glut-1 and vascular endothelial growth factor (VEGF) along with Ki67/MIB-1 in the Barrett's metaplasia-dysplasia-adenocarcinoma sequence. Endoscopic biopsies of normal squamous epithelium (NSE) (n=20), columnar-lined oesophagus (CLO) (n=15), CLO with intestinal metaplasia (n=20), dysplasia (n=17) and Barrett's type adenocarcinoma (n=20) were obtained. Immunohistochemistry was performed on the paraffin-embedded tissue. A score was calculated for each marker (range 0-300) by multiplying intensity (none 0, weak 1, moderate 2, strong 3) by percentage of expression (range 0-100). Significant increases in the expression of HIF-2alpha (P=0.014), VEGF (P<0.0001), Epo-R (P<0.0001) and Ki67 (P<0.0001) were found as tissue progressed from NSE to adenocarcinoma. HIF-2alpha was expressed late in the sequence and was only seen in dysplasia and adenocarcinoma. High HIF-2alpha expression was seen in 12 out of 20 Barrett's type adenocarcinoma. The late expression of HIF-2alpha in the Barrett's carcinogenesis sequence and its high expression in adenocarcinoma suggest that it is worth further investigation as a marker of disease progression and therapeutic target.

Published

2007

52. Diabetes: caught in the Akt?

Author

Price PM

Subjects

Animals, Cell Cycle, Cell Line, Phosphatidylinositol 3-Kinases drug effects, Proto-Oncogene Proteins c-akt drug effects, Diabetic Nephropathies physiopathology, Glucose pharmacology, Kidney Diseases physiopathology, Phosphatidylinositol 3-Kinases metabolism, Proto-Oncogene Proteins c-akt metabolism

Abstract

One complication of diabetes is a pronounced renal cellular hypertrophy, inevitably resulting in chronic fibrotic changes. Chuang and colleagues demonstrate that hypertrophy in vitro is dependent on an increased phosphoinositide 3-kinase (PI3K) activity and is correlated with increased levels of p21(WAF1/Cip1), a cell-cycle regulator that was previously associated with renal fibrosis and sclerosis from nondiabetic causes.

Published

2007

53. Hypoxia-inducible factor-1alpha expression in the gastric carcinogenesis sequence and its prognostic role in gastric and gastro-oesophageal adenocarcinomas.

Author

Griffiths EA, Pritchard SA, Valentine HR, Whitchelo N, Bishop PW, Ebert MP, Price PM, Welch IM, and West CM

Subjects

Adenocarcinoma surgery, Aged, Aged, 80 and over, Biopsy, Disease Progression, Esophageal Neoplasms surgery, Female, Follow-Up Studies, Humans, Hypoxia-Inducible Factor 1, alpha Subunit chemistry, Immunohistochemistry, Male, Middle Aged, Multivariate Analysis, Neoplasm Invasiveness, Predictive Value of Tests, Prognosis, Staining and Labeling, Stomach Neoplasms surgery, Survival Rate, Adenocarcinoma diagnosis, Adenocarcinoma metabolism, Esophageal Neoplasms diagnosis, Esophageal Neoplasms metabolism, Hypoxia-Inducible Factor 1, alpha Subunit biosynthesis, Stomach Neoplasms diagnosis, Stomach Neoplasms metabolism

Abstract

Hypoxia-inducible factor-1 (HIF-1)alpha expression was studied in the gastric carcinogenesis sequence and as a prognostic factor in surgically resected gastric and gastro-oesophageal junction tumours. Protein expression was examined using immunohistochemistry on formalin-fixed biopsies of normal mucosa (n=20), Helicobacter pylori associated gastritis (n=24), intestinal metaplasia (n=24), dysplasia (n=12) and intestinal (n=19) and diffuse (n=21) adenocarcinoma. The relationship between HIF-1alpha expression and prognosis was assessed in resection specimens from 177 patients with gastric and gastro-oesophageal junction adenocarcinoma. Hypoxia-inducible factor-1alpha expression was not observed in normal gastric mucosa but increased in density (P<0.01) and intensity (P<0.01) with progression from H. pylori-associated gastritis, intestinal metaplasia, dysplasia to adenocarcinoma. The pattern of staining in the resection specimens was focally positive in 49 (28%) and at the invasive tumour edge in 41 (23%). Invasive edge expression was associated with lymph node metastases (P=0.034), advanced TNM stage (P=0.001) and was an adverse prognostic factor for cancer-specific survival (P=0.019). In univariate analysis and in comparison with tumours not expressing HIF-1alpha, invasive edge staining was associated with a hazard ratio of 1.6 (95% CI 1.0-2.5) and focally positive staining a hazard ratio of 0.7 (95% CI 0.5-1.2). Hypoxia-inducible factor-1alpha lost prognostic significance in multivariate analysis. The results suggest HIF-1alpha is involved in gastric carcinogenesis and disease progression, but is only a weak prognostic factor for survival.

Published

2007

54. Neurocognitive dysfunction post-cardiac surgery and the neuroprotective effects of erythropoietin.

Author

Bhimji Z, Estabrooks L, and Price PM

Subjects

Cognition Disorders etiology, Erythropoietin metabolism, Humans, Hypoxia metabolism, Hypoxia physiopathology, Inflammation metabolism, Inflammation physiopathology, Recombinant Proteins, Cardiac Surgical Procedures adverse effects, Cognition Disorders prevention & control, Erythropoietin therapeutic use, Hematinics therapeutic use

Abstract

Neurocognitive dysfunction is a common postoperative complication exacerbated by cardiopulmonary bypass triggering a systemic inflammatory response. This clinical column focuses on the up-regulation of endogenous erythropoietin related to neurological inflammation and the use of recombinant erythropoietin as a neuroprotective pharmacotherapeutic agent.

Published

2007

55. Dependence of cisplatin-induced cell death in vitro and in vivo on cyclin-dependent kinase 2.

Author

Price PM, Yu F, Kaldis P, Aleem E, Nowak G, Safirstein RL, and Megyesi J

Subjects

Adenine analogs & derivatives, Adenine pharmacology, Animals, Cells, Cultured, Creatinine blood, Cyclin-Dependent Kinase 2 antagonists & inhibitors, Cyclin-Dependent Kinase Inhibitor p21 biosynthesis, Kidney Tubules, Proximal cytology, Kidney Tubules, Proximal drug effects, Mice, Up-Regulation, Apoptosis drug effects, Cisplatin pharmacology, Cyclin-Dependent Kinase 2 physiology

Abstract

Cisplatin is one of the most effective chemotherapeutics, but its usefulness is limited by its toxicity to normal tissues, including cells of the kidney proximal tubule. The purpose of these studies was to determine the mechanism of cisplatin cytotoxicity. It was shown in vivo that cisplatin administration induces upregulation of the gene for the p21 cyclin-dependent kinase (cdk) inhibitor in kidney cells. This protein is a positive effector on the fate of cisplatin-exposed renal tubule cells in vivo and in vitro; adenoviral transduction of p21 completely protected proximal tubule cells from cisplatin toxicity. Herein is reported that cdk2 inhibitory drugs protect kidney cells in vivo and in vitro, that transduction of kidney cells in vitro with dominant-negative cdk2 also protected, and that cdk2 knockout cells were resistant to cisplatin. The cdk2 knockout cells regained cisplatin sensitivity after transduction with wild-type cdk2. It is concluded that cisplatin cytotoxicity depends on cdk2 activation and that the mechanism of p21 protection is by direct inhibition of cdk2. This demonstrated the involvement of a protein that previously was associated with cell-cycle progression with pathways of apoptosis. It also was demonstrated that this pathway of cisplatin-induced cell death can be interceded in vivo to prevent nephrotoxicity.

Published

2006

56. Carbogen and nicotinamide increase blood flow and 5-fluorouracil delivery but not 5-fluorouracil retention in colorectal cancer metastases in patients.

Author

Gupta N, Saleem A, Kötz B, Osman S, Aboagye EO, Phillips R, Vernon C, Wasan H, Jones T, Hoskin PJ, and Price PM

Subjects

Administration, Inhalation, Administration, Oral, Aged, Colorectal Neoplasms pathology, Drug Interactions, Female, Humans, Liver Neoplasms secondary, Male, Middle Aged, Regional Blood Flow, Tissue Distribution, Antimetabolites, Antineoplastic pharmacokinetics, Carbon Dioxide pharmacology, Colorectal Neoplasms drug therapy, Fluorouracil pharmacokinetics, Liver Neoplasms drug therapy, Niacinamide pharmacology, Oxygen pharmacology, Radiation-Sensitizing Agents pharmacology, Vitamin B Complex pharmacology

Abstract

Purpose: To examine whether carbogen and nicotinamide increases 5-fluorouracil (5-FU) delivery to colorectal cancer metastases., Experimental Design: Six patients were scanned using positron emission tomography. Two scans were done to coincide with the start of separate chemotherapy cycles. At the second positron emission tomography session, 60 mg/kg nicotinamide was given orally 2 to 3 hours before 10-minute carbogen inhalation. In the middle of carbogen treatment, [15O]H2O (to measure regional tissue perfusion) and then [18F]5-FU (to measure 5-FU tissue pharmacokinetics) were administered., Results: Regions of interest were drawn in 12 liver metastases, 6 spleens, 6 livers, and 12 kidneys. Nicotinamide and carbogen administration increased mean blood pO2 from 93 mm Hg (95% confidence interval, 79-198) to 278 mm Hg (95% confidence interval, 241-316; P = 0.031). Regional perfusion (mL(blood)/min/mL(tissue)) increased in metastases (mean change = 52%, range -32% to +261%, P = 0.024), but decreased in kidney (mean change = -42%, range -82% to -11%, P = 0.0005) and liver (mean change = -34%, range -43% to -26%, P = 0.031). 5-FU uptake at 3.75 minutes (m(2)/mL) increased in tumor (mean change = 40%, range -39% to +196%, P = 0.06) and decreased in kidney (mean change = -25%, range -71% to 12%, P = 0.043). 5-FU delivery measured as K1 increased in tumor (mean change = 74%, range -23% to +293%, P = 0.0039). No differences were seen in [18F]5-FU tumor exposure (net area under curve) and retention., Conclusion: Nicotinamide and carbogen administration can increase 5-FU delivery to colorectal cancer liver metastases. Despite an increase in perfusion and 5-FU delivery, the effects were not directly related and did not increase 5-FU retention or tissue exposure.

Published

2006

57. Minimally invasive pharmacokinetic and pharmacodynamic technologies in hypothesis-testing clinical trials of innovative therapies.

Author

Workman P, Aboagye EO, Chung YL, Griffiths JR, Hart R, Leach MO, Maxwell RJ, McSheehy PM, Price PM, and Zweit J

Subjects

Apoptosis, Biomarkers metabolism, Blood Flow Velocity, Cell Hypoxia, Clinical Trials as Topic, Clinical Trials, Phase I as Topic, Clinical Trials, Phase II as Topic, Humans, Neoplasms diagnostic imaging, Radiopharmaceuticals, Sensitivity and Specificity, Ultrasonography methods, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents pharmacology, Magnetic Resonance Imaging methods, Magnetic Resonance Spectroscopy, Neoplasms drug therapy, Neoplasms metabolism, Positron-Emission Tomography, Tomography, X-Ray Computed methods

Abstract

Clinical trials of new cancer drugs should ideally include measurements of parameters such as molecular target expression, pharmacokinetic (PK) behavior, and pharmacodynamic (PD) endpoints that can be linked to measures of clinical effect. Appropriate PK/PD biomarkers facilitate proof-of-concept demonstrations for target modulation; enhance the rational selection of an optimal drug dose and schedule; aid decision-making, such as whether to continue or close a drug development project; and may explain or predict clinical outcomes. In addition, measurement of PK/PD biomarkers can minimize uncertainty associated with predicting drug safety and efficacy, reduce the high levels of drug attrition during development, accelerate drug approval, and decrease the overall costs of drug development. However, there are many challenges in the development and implementation of biomarkers that probably explain their disappointingly low implementation in phase I trials. The Pharmacodynamic/Pharmacokinetic Technologies Advisory committee of Cancer Research UK has found that submissions for phase I trials of new cancer drugs in the United Kingdom often lack detailed information about PK and/or PD endpoints, which leads to suboptimal information being obtained in those trials or to delays in starting the trials while PK/PD methods are developed and validated. Minimally invasive PK/PD technologies have logistic and ethical advantages over more invasive technologies. Here we review these technologies, emphasizing magnetic resonance spectroscopy and positron emission tomography, which provide detailed functional and metabolic information. Assays that measure effects of drugs on important biologic pathways and processes are likely to be more cost-effective than those that measure specific molecular targets. Development, validation, and implementation of minimally invasive PK/PD methods are encouraged.

Published

2006

58. Imaging vascular physiology to monitor cancer treatment.

Author

Laking GR, West C, Buckley DL, Matthews J, and Price PM

Subjects

Angiogenesis Inhibitors therapeutic use, Antineoplastic Agents therapeutic use, Blood Flow Velocity, Clinical Trials as Topic, Drug Monitoring, Humans, Magnetic Resonance Imaging, Neoplasms pathology, Neoplasms therapy, Neovascularization, Pathologic therapy, Positron-Emission Tomography, Reproducibility of Results, Ultrasonography, Doppler, Diagnostic Imaging, Monitoring, Physiologic methods, Neoplasms blood supply, Neovascularization, Pathologic diagnosis

Abstract

The primary physiological function of the vasculature is to support perfusion, the nutritive flow of blood through the tissues. Vascular physiology can be studied non-invasively in human subjects using imaging methods such as positron emission tomography (PET), magnetic resonance imaging (MRI), X-ray computed tomography (CT), and Doppler ultrasound (DU). We describe the physiological rationale for imaging vascular physiology with these methods. We review the published data on repeatability. We review the literature on 'before-and-after' studies using these methods to monitor response to treatment in human subjects, in five broad clinical settings: (1) antiangiogenic agents, (2) vascular disruptive agents, (3) conventional cytotoxic drugs, (4) radiation treatment, and (5) agents affecting drug delivery. We argue that imaging of vascular physiology offers an attractive 'functional endpoint' for clinical trials of anticancer treatment. More conventional measures of tumour response, such as size criteria and the uptake of fluorodeoxyglucose, may be insensitive to therapeutically important changes in vascular function.

Published

2006

59. Is the hypoxia-inducible factor pathway important in gastric cancer?

Author

Griffiths EA, Pritchard SA, Welch IM, Price PM, and West CM

Subjects

Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Antigens, Neoplasm metabolism, Biomarkers, Tumor metabolism, Carbonic Anhydrase IX, Carbonic Anhydrases metabolism, Cyclooxygenase 2 metabolism, Drug Resistance, Neoplasm, Forecasting, Genes, Tumor Suppressor, Glucose Transporter Type 1 metabolism, Helicobacter Infections complications, Helicobacter pylori, Humans, Immunohistochemistry, Microcirculation, Prognosis, Stomach Neoplasms blood supply, Vascular Endothelial Growth Factor A metabolism, Cell Hypoxia physiology, Hypoxia-Inducible Factor 1, alpha Subunit metabolism, Neoplasm Proteins metabolism, Stomach Neoplasms metabolism

Abstract

Tumour hypoxia is well recognised in oncology to be a key factor resulting in treatment resistance and poor prognosis. Hypoxia leads to the expression of a number of gene products that are involved in tumour progression, invasion and metastasis formation. The most important of these proteins is thought to be hypoxia-inducible factor-1alpha (HIF-1alpha), which appears to be a master regulator of the cellular response to hypoxia. HIF-1alpha expression is associated with a poor prognosis and treatment response in a number of tumour sites. There is some evidence that the HIF-1alpha pathway might be involved in gastric carcinogenesis. Studies have shown reactive oxygen species from Helicobacter pylori, associated with the development of gastric cancer, stabilise HIF-1alpha. Non-steroidal anti-inflammatory drugs, shown to reduce the risk of gastric cancer, can decrease HIF-1alpha expression. Although a large study correlating HIF-1alpha expression with prognosis is lacking in gastric cancer, the immunohistochemical expression of HIF-1alpha target genes (Glut-1, VEGF, CA9, iNOS) is associated with a poor prognosis. In addition, the targeted inhibition of HIF-1alpha has been shown to inhibit the growth of gastric tumours in animals. Increased understanding of the importance of hypoxia and the HIF-1alpha pathways may therefore hold the key to prevention strategies, improved selection of patients for adjuvant therapy and new treatments for the disease.

Published

2005

60. Identification of the functional domain of p21(WAF1/CIP1) that protects cells from cisplatin cytotoxicity.

Author

Yu F, Megyesi J, Safirstein RL, and Price PM

Subjects

Acute Kidney Injury physiopathology, Adenoviridae genetics, Apoptosis physiology, CDC2-CDC28 Kinases genetics, CDC2-CDC28 Kinases metabolism, Cell Cycle Proteins chemistry, Cell Line, Cyclin-Dependent Kinase 2, Cyclin-Dependent Kinase Inhibitor p21, Humans, Kidney cytology, Protein Binding, Protein Structure, Tertiary, Acute Kidney Injury chemically induced, Antineoplastic Agents toxicity, Cell Cycle Proteins genetics, Cell Cycle Proteins metabolism, Cisplatin toxicity

Abstract

The p21 cyclin-dependent kinase (cdk) inhibitor protects cells from cisplatin cytotoxicity in vivo and in vitro. However, the mechanism of protection is not known. Separate p21 domains are known to interact with several different proteins having proapoptotic functions. To investigate the mechanism of protection by p21, we have constructed adenoviruses encoding the different domains of p21. We were able to localize the protective activity to a region of 54 amino acids containing the cyclin-cdk interacting moiety. Other protein binding domains of p21, including the NH2-terminal procaspase-3 interactive region and the COOH-terminal region containing the proliferating cell nuclear antigen binding domain and the nuclear localization signal, had little protective effect on cisplatin cytotoxicity. The dependence of cisplatin cytotoxicity on cdk2 activity was also demonstrated because 1) cisplatin caused a marked increase in cdk2 activity, which was prevented by the p21 expression adenovirus, and 2) a cdk2 dominant-negative adenovirus also protected cells from cisplatin-induced apoptosis. Thus the data suggest that the mechanism of p21 protection is by direct inhibition of cdk2 activity and that cisplatin-induced apoptosis is caused by a cdk2-dependent pathway.

Published

2005

61. Glucose metabolism in brain tumours can be estimated using [18F]2-fluorodeoxyglucose positron emission tomography and a population-derived input function scaled using a single arterialised venous blood sample.

Author

Brock CS, Young H, Osman S, Luthra SK, Jones T, and Price PM

Subjects

Arteries, Brain Neoplasms blood supply, Fluorodeoxyglucose F18, Glioma blood supply, Humans, Radiopharmaceuticals, Reference Values, Reproducibility of Results, Sensitivity and Specificity, Brain Neoplasms diagnostic imaging, Brain Neoplasms metabolism, Glioma diagnostic imaging, Glioma metabolism, Glucose metabolism, Positron-Emission Tomography

Abstract

The aim of this study was to assess simplified methods for deriving input functions for estimating glucose metabolism using 18F-FDG-PET. Nine glioma patients underwent paired 18F-FDG-PET scans as part of a phase II study and the data used to estimate the metabolic rate of glucose (MRGlu) using a population-derived input function (arterial data from 14 scans) scaled using a single arterial blood sample taken at 20 min. Paired studies were performed in four further glioma patients with stable disease at least four months following radiotherapy to determine whether scaling the population-derived input function using a 20-min arterialised venous or venous sample further simplified the method. The heated hand method was used to obtain arterialised venous blood that approximated arterial blood. In the 9 phase II glioma patients, there was a good, statistically significant correlation between the MRGlu values estimated using the individual arterial input functions and the single arterial sample scaled population-derived input functions (r(2)=0.88, p<0.001, n=36). Blood samples collected during three scans on two of the stable disease patients showed no significant difference between the arterialised venous and arterial plasma concentrations of 18F (p>0.1, n=15) when the degree of arterialisation of the blood was monitored and maintained using a thermocouple. A significant difference was found between the plasma arterial and venous levels of 18F. There was an excellent correlation between MRGlu estimated using an arterial input function and a population-derived input function scaled using a single arterialised venous blood sample (r(2)=0.98, n=12). The method was reproducible with less than 4.4% variation between repeat tumour scans. Therefore, a population-derived input function scaled using a single arterialised venous blood sample at 20 min can be used for estimating MRGlu using 18F-FDG PET in glioma patients.

Published

2005

62. The uptake of 3'-deoxy-3'-[18F]fluorothymidine into L5178Y tumours in vivo is dependent on thymidine kinase 1 protein levels.

Author

Barthel H, Perumal M, Latigo J, He Q, Brady F, Luthra SK, Price PM, and Aboagye EO

Subjects

Animals, Male, Metabolic Clearance Rate, Mice, Organ Specificity, Radionuclide Imaging, Radiopharmaceuticals pharmacokinetics, Tissue Distribution, Biomarkers, Tumor metabolism, Dideoxynucleosides pharmacokinetics, Lymphoma diagnostic imaging, Lymphoma metabolism, Thymidine Kinase metabolism

Abstract

Purpose: The aim of this study was to investigate the role of thymidine kinase 1 (TK1) protein in 3'-deoxy-3'-[18F]fluorothymidine ([18F]FLT) positron emission tomography (PET) studies., Methods: We investigated the in vivo kinetics of [18F]FLT in TK1+/- and TK1-/- L5178Y mouse lymphoma tumours that express different levels of TK1 protein., Results: [18F]FLT-derived radioactivity, measured by a dedicated small animal PET scanner, increased within the tumours over 60 min. The area under the normalised tumour time-activity curve were significantly higher for the TK1+/- compared with the -/- variant (0.89+/-0.02 vs 0.79+/-0.03 MBq ml(-1) min, P=0.043; n=5 for each tumour type). Ex vivo gamma counting of tissues excised at 60 min p.i. (n=8) also revealed significantly higher tumour [18F]FLT uptake for the TK1+/- variant (6.2+/-0.6 vs 4.6+/-0.4%ID g(-1), P=0.018). The observed differences between the cell lines with respect to [18F]FLT uptake were in keeping with a 48% higher TK1 protein in the TK1+/- tumours versus the -/- variant (P=0.043). On average, there were no differences in ATP levels between the two tumour variants (P=1.00). A positive correlation between [18F]FLT accumulation and TK1 protein levels (r=0.68, P=0.046) was seen. Normalisation of the data for ATP content further improved the correlation (r=0.86, P=0.003)., Conclusion: This study shows that in vivo [18F]FLT kinetics depend on TK1 protein expression. ATP may be important in realising this effect. Thus, [18F]FLT-PET has the potential to yield specific information on tumour proliferation in diagnostic imaging and therapy monitoring.

Published

2005

63. Hypoxia-inducible factor 1alpha expression as an intrinsic marker of hypoxia: correlation with tumor oxygen, pimonidazole measurements, and outcome in locally advanced carcinoma of the cervix.

Author

Hutchison GJ, Valentine HR, Loncaster JA, Davidson SE, Hunter RD, Roberts SA, Harris AL, Stratford IJ, Price PM, and West CM

Subjects

Antigens, Neoplasm metabolism, Carbonic Anhydrase IX, Carbonic Anhydrases metabolism, Disease-Free Survival, Female, Humans, Hypoxia-Inducible Factor 1, alpha Subunit, Ion-Selective Electrodes, Middle Aged, Neoplasm Recurrence, Local metabolism, Neoplasm Recurrence, Local pathology, Neoplasm Recurrence, Local radiotherapy, Oxygen metabolism, Prognosis, Survival Rate, Treatment Outcome, Uterine Cervical Neoplasms radiotherapy, Uterine Cervical Neoplasms secondary, Biomarkers, Tumor metabolism, Hypoxia metabolism, Nitroimidazoles therapeutic use, Radiation-Sensitizing Agents therapeutic use, Transcription Factors metabolism, Uterine Cervical Neoplasms metabolism

Abstract

Purpose: Hypoxia-inducible factor (HIF)-1alpha expression was studied retrospectively in locally advanced carcinoma of the cervix in relation to other methods for measuring/assessing tumor hypoxia and outcome after radiotherapy., Experimental Design: HIF-1alpha expression was examined in formalin-fixed tumor biopsies using a semiquantitative scoring system and correlated with measurements of hypoxia obtained using oxygen electrodes, pimonidazole staining, and carbonic anhydrase 9., Results: High HIF-1alpha expression showed a weak correlation with low pO2 (r = -0.26; P = 0.030; n = 72). Weak significant correlations were found between HIF-1alpha and pimonidazole staining (r = 0.34; P = 0.040; n = 36) and carbonic anhydrase IX (r = 0.27; P = 0.001; n = 160). There was no relationship with surviving fraction at 2 Gy. The relationship between HIF-1alpha expression and radiotherapy outcome was examined in 99 patients. HIF-1alpha expression did not correlate with disease stage, grade, tumor size, and patient age. HIF-1alpha alone was not a significant prognostic factor for disease-free survival, metastasis-free survival, or local recurrence-free survival. High HIF-1alpha expression tended to be associated with poor outcome in small tumors but good outcome in large tumors, with statistically significant interactions between HIF-1alpha and tumor size for survival (P = 0.046) and local control (P = 0.009)., Conclusions: In this study, HIF-1alpha had no prognostic significance in locally advanced carcinoma of the cervix. The possible switch in large tumors for an association between high HIF-1alpha expression and good outcome might relate to tumor size-related changes in the balance of genes up-regulated by HIF-1alpha. Whereas angiogenesis-promoting genes might be preferentially up-regulated in small tumors, proapoptotic genes might be induced in large tumors. This hypothesis needs testing in future work.

Published

2004

64. Cisplatin-induced cell death is EGFR/src/ERK signaling dependent in mouse proximal tubule cells.

Author

Arany I, Megyesi JK, Kaneto H, Price PM, and Safirstein RL

Subjects

Animals, Caspase 3, Caspases metabolism, Cell Line, Transformed, Enzyme Inhibitors pharmacology, ErbB Receptors antagonists & inhibitors, Kidney Tubules, Proximal drug effects, Kidney Tubules, Proximal enzymology, Male, Mice, Mice, Inbred Strains, Mitogen-Activated Protein Kinases metabolism, Quinazolines, Tyrphostins pharmacology, src-Family Kinases antagonists & inhibitors, src-Family Kinases metabolism, Antineoplastic Agents toxicity, Apoptosis drug effects, Cisplatin toxicity, ErbB Receptors metabolism, Kidney Tubules, Proximal cytology, MAP Kinase Signaling System drug effects

Abstract

Cisplatin treatment induces extensive death of the proximal tubules in mice. We also demonstrated that treatment of immortalized mouse proximal tubule cells (TKPTS) with 25 microM cisplatin induces apoptotic death in vitro. Here, we demonstrate that members of the MAPKs such as ERK, JNK, and p38 are all activated after cisplatin treatment both in vivo and in vitro. Because MAPKs mediate cell survival and death, we studied their role in cisplatin-induced cell death in vitro. Apoptosis was confirmed by cell morphology, fluorescence-activated cell-sorting analysis, annexin V/propidium iodide binding, and caspase-3 activation in TKPTS cells. Inhibition of ERK, but not JNK or p38, abolished caspase-3 activation and apoptotic death, suggesting a prodeath role of ERK in cisplatin-induced injury. We also determined that cisplatin-induced ERK as well as caspase-3 activation are epidermal growth factor receptor (EGFR) and c-src dependent because inhibition of these genes inhibited ERK and caspase-3 activation and attenuated apoptotic death. These results suggest that caspase-3 mediates cisplatin-induced cell death in TKPTS cells via an EGFR/src/ERK-dependent pathway. We also suggest that the prodeath effect of ERK is injury type dependent because during oxidant injury, ERK supports survival rather than death in the same cells. We propose that injury-specific outcome diverges downstream from ERK in cisplatin- or H(2)O(2)-mediated cell survival and death.

Published

2004

65. Cell cycle regulation: repair and regeneration in acute renal failure.

Author

Price PM, Megyesi J, and Saf Irstein RL

Subjects

Animals, Cyclin-Dependent Kinase Inhibitor p21, Humans, Kidney metabolism, Kidney pathology, Acute Kidney Injury metabolism, Acute Kidney Injury pathology, Cell Cycle Proteins metabolism, Cyclins metabolism

Abstract

Research into mechanisms of acute renal failure has begun to reveal molecular targets for possible therapeutic intervention. Much useful knowledge into the causes and prevention of this syndrome has been gained by the study of animal models. Most recently, investigation of the effects on acute renal failure of selected gene knock-outs in mice has contributed to our recognition of many previously unappreciated molecular pathways. Particularly, experiments have revealed the protective nature of two highly induced genes whose functions are to inhibit and control the cell cycle after acute renal failure. By use of these models we have started to understand the role of increased cell cycle activity after renal stress, and the role of proteins induced by these stresses that limit this proliferation.

Published

2004

66. Radiosynthesis of 4-[(2-chloroethyl)(2-[(11)C]ethyl)amino]-phenoxycarbonyl-l-glutamic acid a half mustard prodrug as a potential probe for imaging antibody- and gene-directed enzyme prodrug therapy with positron emission tomography.

Author

Malik N, Luthra SK, Burke P, Price PM, Aboagye EO, Latigo J, Zhao Y, and Brady F

Subjects

Acetaldehyde, Aniline Mustard pharmacokinetics, Indicators and Reagents, Isotope Labeling methods, Radiopharmaceuticals, Substrate Specificity, Tomography, Emission-Computed, gamma-Glutamyl Hydrolase, Aniline Mustard analogs & derivatives, Aniline Mustard chemical synthesis

Abstract

The potential antibody directed prodrug therapy half-mustard prodrug 4-[(2-chloroethyl)(2-ethyl)amino]-phenoxycarbonyl-L-glutamic acid was synthesised by reductive alkylation of 4-[(2-chloroethyl)amino]-phenoxycarbonyl-L-glutamic acid using acetaldehyde. 4-[(2-chloroethyl)[(11)C](2-ethyl)amino]phenoxycarbonyl-L-glutamic acid was synthesized with 18-22% decay corrected radiochemical yield in 45 min from EOB by reductive alkylation of 4-[(2-chloroethyl)amino]-phenoxycarbonyl-L-glutamic acid using [(11)C]acetaldehyde. [(11)C]Acetaldehyde was prepared in 60% decay corrected radiochemical yield by oxidation of [(11)C]ethanol over heated copper oxide. The radiosynthesis of [(11)C]ethanol was re-examined and optimized. 4-[(2-chloroethyl)(2-ethyl)amino]-phenoxycarbonyl-L-glutamic acid was found to have affinity for carboxypeptidase G2; the K(m) and V(max) were 99.4-115.9 microM (n=3) and 3.6-5.0 microM/min, respectively, at a carboxypeptidase G2 concentration of 0.0247 U/ml.

Published

2004

67. Positron emission tomography imaging of cell proliferation in oncology.

Author

Kenny LM, Aboagye EO, and Price PM

Subjects

Antiviral Agents, Cyclins pharmacology, DNA biosynthesis, Dideoxynucleosides, Humans, Kinetics, Phenotype, Thymidine, Cell Cycle, Neoplasms diagnostic imaging, Neoplasms physiopathology, Tomography, Emission-Computed

Abstract

Tumour-cell proliferation is a hallmark of the malignant phenotype. Positron emission tomography (PET) offers a unique method of imaging biological and biochemical changes in vivo. Radiolabelled thymidine and thymidine analogues are currently in development as PET tracers. By studying the uptake and kinetics of such compounds using PET, a measure of DNA synthesis and hence cell proliferation can be obtained. Molecular imaging of cellular proliferation with PET is now possible, and has the potential to play an important role in the evaluation of efficacy of new anti-cancer agents.

Published

2004

68. Protection of renal cells from cisplatin toxicity by cell cycle inhibitors.

Author

Price PM, Safirstein RL, and Megyesi J

Subjects

14-3-3 Proteins, Animals, Apoptosis drug effects, Biomarkers, Tumor metabolism, Caspase 3, Caspase Inhibitors, Caspases metabolism, Cell Cycle drug effects, Cells, Cultured, Cyclin-Dependent Kinase Inhibitor p21, Cyclins metabolism, Epithelial Cells cytology, Exonucleases metabolism, Exoribonucleases, Kidney Tubules, Proximal cytology, Mice, Neoplasm Proteins metabolism, Poly(ADP-ribose) Polymerases metabolism, Purines pharmacology, Roscovitine, Tumor Suppressor Protein p53 metabolism, Antineoplastic Agents toxicity, Cisplatin toxicity, Epithelial Cells drug effects, Kidney Tubules, Proximal drug effects

Abstract

The optimal use of cisplatin as a chemotherapeutic drug has been limited by its nephrotoxicity. Murine models have been used to study cisplatin-induced acute renal failure. After cisplatin administration, cells of the S3 segment in the renal proximal tubule are especially sensitive and undergo extensive necrosis in vivo. Similarly, cultured proximal tubule cells undergo apoptosis in vitro after cisplatin exposure. We have shown in vivo that kidney cells enter the cell cycle after cisplatin administration but that cell cycle-inhibitory proteins p21 and 14-3-3sigma are also upregulated. These proteins coordinate the cell cycle, and deletion of either of the genes resulted in increased nephrotoxicity in vivo or increased cell death in vitro after exposure to cisplatin. However, it was not known whether cell cycle inhibition before acute renal failure could protect from cisplatin-induced cell death, especially in cells with functional p21 and 14-3-3sigma genes. Using several cell cycle inhibitors, including a p21 adenovirus, and the drugs roscovitine and olomoucine, we have been able to completely protect a mouse kidney proximal tubule cell culture from cisplatin-induced apoptosis. The protection by p21 was independent of an effect on the cell cycle and was likely caused by selective inhibition of caspase-dependent and -independent cell death pathways in the cells.

Published

2004

69. Lack of a functional p21WAF1/CIP1 gene accelerates caspase-independent apoptosis induced by cisplatin in renal cells.

Author

Nowak G, Price PM, and Schnellmann RG

Subjects

Animals, Antineoplastic Agents pharmacology, Caspase Inhibitors, Cells, Cultured, Cyclin-Dependent Kinase Inhibitor p21, Enzyme Activation, Enzyme Inhibitors pharmacology, Kidney Tubules, Proximal enzymology, Mice, Mice, Knockout, Apoptosis drug effects, Caspases metabolism, Cisplatin pharmacology, Cyclins genetics, Cyclins metabolism, Kidney Tubules, Proximal cytology, Kidney Tubules, Proximal drug effects

Abstract

The lack of cyclin-dependent kinase inhibitor p21WAF1/CIP1 (p21) in mice increases renal proximal tubular cell death and enhances sensitivity to acute renal failure produced by the chemotherapeutic agent cisplatin. We used primary cultures of mouse renal proximal tubular cells (MPTC) grown in optimized culture conditions to investigate the cellular basis for increased apoptosis in p21 knockout mice. Cisplatin (15 microM) activated caspase-3 but not caspase-8 or caspase-9 and produced phosphatidylserine externalization, chromatin condensation, and nuclear fragmentation in wild-type [p21(+/+)] MPTC. Caspase-3 activation and apoptosis were accelerated in cisplatin-treated MPTC lacking p21 [p21(-/-) MPTC]. In contrast to p21(+/+) MPTC, cisplatin activated caspase-9 but not caspase-8 in p21(-/-) MPTC before caspase-3 activation. The caspase-3 inhibitor Asp-Glu-Val-Asp-fluoromethylketone (DEVD-fmk) inhibited caspase-3 activity but did not abolish apoptosis in p21(+/+) and p21(-/-) MPTC. General caspase inhibitor Z-Val-Ala-Asp(OCH3)-fluoromethylketone (ZVAD-fmk) inhibited caspase activity and decreased chromatin condensation by 51% in p21(-/-) but not in p21(+/+) MPTC. However, cisplatin-induced phosphatidylserine externalization was not inhibited by ZVAD-fmk in p21(-/-) MPTC. We conclude that 1) in the presence of p21, cisplatin activates caspase-3 through a mechanism independent of caspase-8 or caspase-9; 2) in the absence of p21, caspase-9 activation precedes caspase-3 activation; 3) the lack of p21 accelerates caspase-3 activation and cisplatin-induced MPTC apoptosis; and 4) MPTC apoptosis is caspase independent in the presence of p21 but partially dependent on caspases in the absence of p21.

Published

2003

70. Cell cycle regulation: repair and regeneration in acute renal failure.

Author

Price PM, Megyesi J, and Safirstein RL

Subjects

Acute Kidney Injury chemically induced, Acute Kidney Injury etiology, Acute Kidney Injury genetics, Animals, Antineoplastic Agents adverse effects, Cell Cycle genetics, Cell Cycle Proteins antagonists & inhibitors, Cell Death physiology, Cell Division physiology, Cisplatin adverse effects, Cyclin-Dependent Kinase Inhibitor p21, Cyclins physiology, Gene Expression Regulation physiology, Humans, Mice, Models, Animal, Recovery of Function physiology, Acute Kidney Injury physiopathology, Cell Cycle physiology, Cell Cycle Proteins physiology, Kidney physiology, Regeneration physiology

Abstract

Research into mechanisms of acute renal failure has begun to reveal molecular targets for possible therapeutic intervention. Much useful knowledge into the causes and prevention of this syndrome has been gained by the study of animal models. Most recently, investigation of the effects on acute renal failure of selected gene knock-outs in mice has contributed to our recognition of many previously unappreciated molecular pathways. Particularly, experiments have revealed the protective nature of 2 highly induced genes whose functions are to inhibit and control the cell cycle after acute renal failure. By use of these models we have started to understand the role of increased cell cycle activity after renal stress and the role of proteins induced by these stresses that limit this proliferation.

Published

2003

71. Phase I clinical trial of weekly combretastatin A4 phosphate: clinical and pharmacokinetic results.

Author

Rustin GJ, Galbraith SM, Anderson H, Stratford M, Folkes LK, Sena L, Gumbrell L, and Price PM

Subjects

Adult, Aged, Antineoplastic Agents, Phytogenic adverse effects, Area Under Curve, Bibenzyls adverse effects, Chromatography, High Pressure Liquid, Drug Administration Schedule, Female, Humans, Infusion Pumps, Magnetic Resonance Imaging, Male, Middle Aged, Neoplasms diagnostic imaging, Statistics, Nonparametric, Treatment Outcome, Antineoplastic Agents, Phytogenic administration & dosage, Antineoplastic Agents, Phytogenic pharmacokinetics, Bibenzyls administration & dosage, Bibenzyls pharmacokinetics, Neoplasms drug therapy, Stilbenes, Tomography, Emission-Computed

Abstract

Purpose: A phase I trial was performed with combretastatin A4 phosphate (CA4P), a novel tubulin-binding agent that has been shown to rapidly reduce blood flow in animal tumors., Patients and Methods: The drug was delivered by a 10-minute weekly infusion for 3 weeks followed by a week gap, with intrapatient dose escalation. Dose escalation was accomplished by doubling until grade 2 toxicity was seen. The starting dose was 5 mg/m2., Results: Thirty-four patients received 167 infusions. CA4P was rapidly converted to the active combretastatin A4 (CA4), which was further metabolized to the glucuronide. CA4 area under the curve (AUC) increased from 0.169 at 5 mg/m2 to 3.29 micromol * h/L at 114 mg/m2. The mean CA4 AUC in eight patients at 68 mg/m2 was 2.33 micromol * h/L compared with 5.8 micromol * h/L at 25 mg/kg (the lowest effective dose) in the mouse. The only toxicity that possibly was related to the drug dose up to 40 mg/m2 was tumor pain. Dose-limiting toxicity was reversible ataxia at 114 mg/m2, vasovagal syncope and motor neuropathy at 88 mg/m2, and fatal ischemia in previously irradiated bowel at 52 mg/m2. Other drug-related grade 2 or higher toxicities seen in more than one patient were pain, lymphopenia, fatigue, anemia, diarrhea, hypertension, hypotension, vomiting, visual disturbance, and dyspnea. One patient at 68 mg/m2 had improvement in liver metastases of adrenocortical carcinoma., Conclusion: CA4P was well tolerated in 14 of 16 patients at 52 or 68 mg/m2; these are doses at which tumor blood flow reduction has been recorded.

Published

2003

72. Assessment of pharmacodynamic vascular response in a phase I trial of combretastatin A4 phosphate.

Author

Anderson HL, Yap JT, Miller MP, Robbins A, Jones T, and Price PM

Subjects

Adult, Antineoplastic Agents, Phytogenic administration & dosage, Antineoplastic Agents, Phytogenic pharmacokinetics, Dose-Response Relationship, Drug, Female, Humans, Image Processing, Computer-Assisted, Infusion Pumps, Kidney blood supply, Male, Middle Aged, Neoplasms blood supply, Neoplasms diagnostic imaging, Spleen blood supply, Statistics, Nonparametric, Stilbenes administration & dosage, Stilbenes pharmacokinetics, Treatment Outcome, Antineoplastic Agents, Phytogenic pharmacology, Neoplasms drug therapy, Stilbenes pharmacology, Tomography, Emission-Computed

Abstract

Purpose: Clinical evaluation of novel agents that target tumor blood vessels requires pharmacodynamic end points that measure vascular damage. Positron emission tomography (PET) was used to measure the effects of the vascular targeting agent combretastatin A4 phosphate (CA4P) on tumor and normal tissue perfusion and blood volume., Patients and Methods: Patients with advanced solid tumors were enrolled onto part of a phase I, accelerated-titration, dose-escalation study. The effects of 5 to 114 mg/m2 CA4P on tumor, spleen, and kidney were investigated. Tissue perfusion was measured using oxygen-15 (15O)-labeled water and blood volume was measured using 15O-labeled carbon monoxide (C15O). Scans were performed immediately before, and 30 minutes and 24 hours after the first infusion of each dose level of CA4P. All statistical tests were two sided., Results: PET data were obtained for 13 patients with intrapatient dose escalation. Significant dose-dependent reductions were seen in tumor perfusion 30 minutes after CA4P administration (mean change, -49% at >or= 52 mg/m2; P =.0010). Significant reductions were also seen in tumor blood volume (mean change, -15% at >or= 52 mg/m2; P =.0070). Although by 24 hours there was tumor vascular recovery, for doses >or= 52 mg/m2 the reduction in perfusion remained significant (P =.013). Thirty minutes after CA4P administration borderline significant changes were seen in spleen perfusion (mean change, -35%; P =.018), spleen blood volume (mean change, -18%; P =.022), kidney perfusion (mean change, -6%; P =.026), and kidney blood volume (mean change, -6%; P =.014). No significant changes were seen at 24 hours in spleen or kidney., Conclusion: CA4P produces rapid changes in the vasculature of human tumors that can be assessed using PET measurements of tumor perfusion.

Published

2003

73. 3'-deoxy-3'-[18F]fluorothymidine as a new marker for monitoring tumor response to antiproliferative therapy in vivo with positron emission tomography.

Author

Barthel H, Cleij MC, Collingridge DR, Hutchinson OC, Osman S, He Q, Luthra SK, Brady F, Price PM, and Aboagye EO

Subjects

Adenosine Triphosphate metabolism, Animals, Drug Monitoring methods, Fluorodeoxyglucose F18 pharmacokinetics, Humans, Mice, Mice, Inbred C3H, Mice, Nude, Neoplasms diagnostic imaging, Neoplasms, Experimental diagnostic imaging, Radiopharmaceuticals pharmacokinetics, Tissue Distribution, Tomography, Emission-Computed, Transplantation, Heterologous, Dideoxynucleosides pharmacokinetics, Fluorine Radioisotopes pharmacokinetics, Fluorouracil therapeutic use, Neoplasms drug therapy

Abstract

3'-Deoxy-3'-[(18)F]fluorothymidine ([(18)F]FLT) has been proposed as a new marker for imaging tumor proliferation by positron emission tomography (PET). The uptake of [(18)F]FLT is regulated by cytosolic S-phase-specific thymidine kinase 1 (TK1). In this article, we have investigated the use of [(18)F]FLT to monitor the response of tumors to antiproliferative treatment in vivo. C3H/Hej mice bearing the radiation-induced fibrosarcoma 1 tumor were treated with 5-fluorouracil (5-FU; 165 mg/kg i.p.). Changes in tumor volume and biodistribution of [(18)F]FLT and 2-[(18)F]fluoro-2-deoxy-D-glucose ([(18)F]FDG) were measured in three groups of mice (n = 8-12/group): (a) untreated controls; (b) 24 h after 5-FU; and (c) 48 h after 5-FU. In addition, dynamic [(18)F]FLT-PET imaging was performed on a small animal scanner for 60 min. The metabolism of [(18)F]FLT in tumor, plasma, liver, and urine was determined chromatographically. Proliferation was determined by staining histological sections for proliferating cell nuclear antigen (PCNA). Tumor levels of TK1 protein and cofactor (ATP) were determined by Western blotting and bioluminescence, respectively. Tumor [(18)F]FLT uptake decreased after 5-FU treatment (47.8 +/- 7.0 and 27.1 +/- 3.7% for groups b and c, respectively, compared with group a; P < 0.001). The drug-induced reduction in tumor [(18)F]FLT uptake was significantly more pronounced than that of [(18)F]FDG. The PET image data confirmed lower tumor [(18)F]FLT retention in group c compared with group a, despite a trend toward higher radiotracer delivery for group c. Other than phosphorylation in tumors, [(18)F]FLT was found to be metabolically stable in vivo. The decrease in tumor [(18)F]FLT uptake correlated with the PCNA-labeling index (r = 0.71, P = 0.031) and tumor volume changes after 5-FU treatment (r = 0.58, P = 0.001). In this model system, the decrease in [(18)F]FLT uptake could be explained by changes in catalytic activity but not translation of TK1 protein. Compared with group a, TK1 levels were lower in group b (78.2 +/- 5.2%) but higher in group c (141.3 +/- 9.1%, P < 0.001). In contrast, a stepwise decrease in ATP levels was observed from group a to b to c (P < 0.001). In conclusion, we have demonstrated the ability to measure tumor response to antiproliferative treatment with [(18)F]FLT and PET. In our model system, the radiotracer uptake was correlated with PCNA-labeling index. The decrease in [(18)F]FLT uptake after 5-FU was more pronounced than that of [(18)F]FDG. [(18)F]FLT is, therefore, a promising marker for monitoring antiproliferative drug activity in oncology that warrants additional testing.

Published

2003

74. 2-[11C]thymidine positron emission tomography as an indicator of thymidylate synthase inhibition in patients treated with AG337.

Author

Wells P, Aboagye E, Gunn RN, Osman S, Boddy AV, Taylor GA, Rafi I, Hughes AN, Calvert AH, Price PM, and Newell DR

Subjects

Adult, Aged, Antimetabolites, Antineoplastic pharmacokinetics, Antimetabolites, Antineoplastic therapeutic use, Area Under Curve, Carbon Radioisotopes, Case-Control Studies, Enzyme Inhibitors pharmacokinetics, Enzyme Inhibitors therapeutic use, Female, Gastrointestinal Neoplasms enzymology, Humans, Liver drug effects, Liver enzymology, Male, Middle Aged, Quinazolines pharmacokinetics, Quinazolines therapeutic use, Regression Analysis, Thymidine, Antimetabolites, Antineoplastic pharmacology, Enzyme Inhibitors pharmacology, Gastrointestinal Neoplasms diagnostic imaging, Gastrointestinal Neoplasms drug therapy, Quinazolines pharmacology, Thymidylate Synthase antagonists & inhibitors, Tomography, Emission-Computed methods

Abstract

Background: Some anticancer drugs inhibit thymidylate synthase (TS), a key enzyme for thymidine nucleotide biosynthesis. Cells can compensate for depleted thymidine levels by taking up extracellular thymidine via a salvage pathway. We investigated the use of 2-[11C]thymidine positron emission tomography (PET) to measure thymidine salvage kinetics in vivo in humans., Methods: Five patients with advanced gastrointestinal cancer were PET scanned both before and 1 hour after oral administration of the TS inhibitor AG337 (THYMITAQ [nolatrexed]); seven control patients were scanned twice but not treated with AG337. Thymidine salvage kinetics were measured in vivo using 2-[11C]thymidine PET and spectral analysis to obtain the standardized uptake values (SUV), the area under the time-activity curve (AUC), and the fractional retention of thymidine (FRT). Changes in PET parameters between scans in the AG337-treated and control groups were compared using the Mann-Whitney U test. The relationship between AG337 exposure and AG337-induced changes in tumor FRT and in plasma deoxyuridine levels (a conventional pharmacodynamic systemic measure of TS inhibition) was examined using Spearman's regression analysis. Statistical tests were two-sided., Results: The between-scan change in FRT in patients treated with AG337 (38% increase, 95% confidence interval [CI] = 8% to 68%) was higher than that in control patients (3% increase, 95% CI = -11% to 17%) (P =.028). The level of AG337-induced increase in both 2-[11C]thymidine FRT and plasma deoxyuridine levels was statistically significantly correlated with AG337 exposure (r = 1.00, P =.01 for both)., Conclusions: AG337 administration was associated with increased tumor tracer retention that was consistent with tumor cell uptake of exogenous 2-[11C]thymidine as a result of TS inhibition. 2-[11C]Thymidine PET can be used to measure thymidine salvage kinetics directly in the tissue of interest.

Published

2003

75. Use of positron emission tomography in anticancer drug development.

Author

Aboagye EO and Price PM

Subjects

Animals, Antineoplastic Agents blood, Humans, Antineoplastic Agents metabolism, Models, Biological, Technology, Pharmaceutical methods, Tomography, Emission-Computed methods

Abstract

Positron emission tomography (PET) is increasingly being used in anticancer drug development. The technique is applicable to studies of drug delivery, and where specific probes are available, to provide pharmacodynamic readouts noninvasively in patients. Mathematical modeling of the imaging data enhances the quality of information that is obtained from such studies. This section provides a review of the PET methodologies that have been used for the development of new cancer therapies. Other than imaging of radiolabeled drugs, PET modeling has found extensive application in studies with 2-[11C]thymidine, [18F]fluorodeoxyglucose, H2(15)O, C15O, and receptor ligands.

Published

2003

76. On the development of rational standards for nuclear response evaluation.

Author

Laking GR and Price PM

Subjects

Follow-Up Studies, Humans, Neoplasms drug therapy, Neoplasms radiotherapy, Radiopharmaceuticals, Reference Standards, Sensitivity and Specificity, Tomography, Emission-Computed methods, Treatment Outcome, Fluorodeoxyglucose F18, Neoplasms diagnostic imaging, Neoplasms therapy, Tomography, Emission-Computed standards, Tomography, Emission-Computed statistics & numerical data

Abstract

Aim: Small variations in test protocols can disproportionately affect the sensitivity and specificity of response evaluation in nuclear medicine. Although use of standardised methods can remedy this, standards must be shown to add value. We think a concept of "societal efficacy" is the benchmark criterion for value of medical interventions. This paper gives an overview of literature on nuclear response evaluation, and promotes a decision-analytic approach to the synthesis of standards., Methods: A Medline search using the OVID database, 1966-January 2002. Reports were organised in relation to mode of treatment and timing of follow-up evaluation. Protocols of multimodality treatment were classified according to the treatment with the greatest tissue-inflammatory potential. The database will be made available on-line at the Website of the European Organisation for the Research and Treatment of Cancer (EORTC) Functional Imaging Group (http://www.eortc.be)., Results: Two hundred and twelve reports could be classified as primary studies in humans. 125 were formal "before-and-after" studies of response to anticancer therapy. More than 60 reported the use of serial positron emission tomography (PET) with fluorodeoxyglucose (FDG)., Conclusion: Descriptive reports of the accuracy and applications of new diagnostic technologies need to be linked to an expectation of improved research or clinical outcomes. To manage the large volume of information will require a trans-disciplinary perspective and use of advanced decision-analytic, Methods: At stake is the possibility of an "industrial" upscaling of one of nuclear oncology' strongest applications.

Published

2003

77. Pharmacokinetics of radiolabelled anticancer drugs for positron emission tomography.

Author

Hutchinson OC, Collingridge DR, Barthel H, Price PM, and Aboagye EO

Subjects

Acridines pharmacokinetics, Animals, Antineoplastic Agents chemistry, Dacarbazine chemistry, Dacarbazine pharmacokinetics, Fluorouracil chemistry, Fluorouracil pharmacokinetics, Humans, Molecular Structure, Radioactive Tracers, Radiopharmaceuticals chemistry, Temozolomide, Tissue Distribution, Tomography, Emission-Computed, Antineoplastic Agents pharmacokinetics, Dacarbazine analogs & derivatives, Radiopharmaceuticals pharmacokinetics

Abstract

Positron emission tomography (PET) provides the oncologist with information on tumour diagnosis, and treatment response monitoring. Mathematical modelling of tissue data, and online plasma radioactive metabolite profiling, enables important tissue kinetic parameters relating to the uptake, distribution and washout as well as arterial input function to be derived. The resultant kinetic data allow for not only diagnosis but also the assessment of therapeutic response endpoints. These endpoints can be used to measure specific therapeutic effects. This novel application of PET can provide information that is often difficult to measure in the intact animal or patient. The pharmacokinetics of radiolabelled N-[2-(dimethylamino)ethyl]acridine-4-carboxamide (DACA), temozolomide and 5-fluorouracil (5-FU) are described.

Published

2003

78. Positron emission tomographic imaging of angiogenesis and vascular function.

Author

Laking GR and Price PM

Subjects

Cell Hypoxia, Humans, Integrins metabolism, Tissue Inhibitor of Metalloproteinases metabolism, Vascular Endothelial Growth Factor A metabolism, Neoplasms diagnostic imaging, Neovascularization, Pathologic diagnostic imaging, Oxygen Radioisotopes, Positron-Emission Tomography methods

Abstract

Surrogate markers of clinical outcome are important in anticancer drug research, since clinical criteria of response develop only slowly and may be confounded by other processes than drug effect. The need for surrogate outcome markers is especially great with newer agents that may act by tumour stabilization as opposed to shrinkage. Neoplastic angiogenesis is associated with a number of detectable changes at molecular and microcirculatory levels. Therefore, direct study of angiogenic molecular biology and tumour circulation before during and after treatment may offer useful surrogate markers for vascular-targeted therapies. The main advantage of radiotracer imaging with positron emission tomography (PET) is its functional specificity. This article will review two main areas: (a) the methodology behind PET imaging of tumour blood supply with 15O-oxygen labelled compounds; and (b) newer tracers in development as markers of angiogenetic biology.

Published

2003

79. Publishing your findings.

Author

King KM and Price PM

Subjects

Humans, Professional Competence standards, Nursing Research organization & administration, Peer Review, Research methods, Periodicals as Topic, Writing

Abstract

The road to publication often seems complicated for newer authors. Therefore, in this column, the authors will clarify the publication process. Topics including why publication is important, choosing a journal, preparing the manuscript-as well as some tips for writing and understanding and responding to peer review-are addressed.

Published

2003

80. Antitumor imidazotetrazines. 40. Radiosyntheses of [4-11C-carbonyl]- and [3-N-11C-methyl]-8-carbamoyl-3-methylimidazo[5,1-d]-1,2,3,5-tetrazin-4(3H)-one (temozolomide) for positron emission tomography (PET) studies.

Author

Brown GD, Luthra SK, Brock CS, Stevens MF, Price PM, and Brady F

Subjects

Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Brain Diseases diagnostic imaging, Carbon Radioisotopes, Cyclization, Dacarbazine chemistry, Dacarbazine pharmacology, Gas Chromatography-Mass Spectrometry, Humans, Isotope Labeling, Magnetic Resonance Spectroscopy, Parietal Lobe diagnostic imaging, Prodrugs chemistry, Prodrugs pharmacology, Structure-Activity Relationship, Temozolomide, Tomography, Emission-Computed, Antineoplastic Agents chemical synthesis, Dacarbazine analogs & derivatives, Dacarbazine chemical synthesis, Prodrugs chemical synthesis

Abstract

8-Carbamoyl-3-methylimidazo[5,1-d]-1,2,3,5-tetrazin-4(3H)-one (temozolomide, 1) is an anticancer prodrug. As part of investigations to probe its postulated mode of action using PET we have developed two rapid radiosynthetic routes for the preparation of temozolomide labeled with the short-lived positron emitter, carbon-11 (t(1/2) = 20.4 min). Reaction of 5-diazoimidazole-4-carboxamide (7) with the novel labeling agent [(11)C-methyl]methyl isocyanate (8) gave [3-N-(11)C-methyl]temozolomide (9) in 14-20% radiochemical yield from [(11)C-methyl]methyl isocyanate (8) (decay corrected). The position of radiolabeling in the 3-N-methyl group was confirmed by [(11/13)C]colabeling and subsequent carbon-13 NMR spectroscopy. Similarly, the reaction of 5-diazoimidazole-4-carboxamide (7) with [(11)C-carbonyl]methyl isocyanate (10) gave [4-(11)C-carbonyl]temozolomide (11) in 10-15% radiochemical yield from [(11)C-carbonyl]methyl isocyanate (10) (decay corrected). Apyrogenic samples of [3-N-(11)C-methyl]temozolomide (9) and [4-(11)C-carbonyl]temozolomide (11), with good chemical and radiochemical purities, have been prepared and used in human PET studies.

Published

2002

81. Clinical impact of (18)F-FDG PET in thyroid carcinoma patients with elevated thyroglobulin levels and negative (131)I scanning results after therapy.

Author

Laking GR and Price PM

Subjects

Carcinoma blood, Carcinoma therapy, Humans, Thyroid Neoplasms blood, Thyroid Neoplasms therapy, Carcinoma diagnostic imaging, Fluorodeoxyglucose F18, Iodine Radioisotopes, Radiopharmaceuticals, Thyroglobulin blood, Thyroid Neoplasms diagnostic imaging, Tomography, Emission-Computed

Published

2002

82. Assessment of the technology for functional imaging in cancer.

Author

Laking GR, Price PM, and Sculpher MJ

Subjects

Decision Making, Decision Support Techniques, Diagnostic Imaging standards, Forecasting, Humans, Magnetic Resonance Imaging methods, Magnetic Resonance Imaging standards, Monte Carlo Method, Randomized Controlled Trials as Topic, Sensitivity and Specificity, Technology Assessment, Biomedical, Tomography, Emission-Computed methods, Tomography, Emission-Computed standards, Tomography, X-Ray Computed methods, Tomography, X-Ray Computed standards, Diagnostic Imaging methods, Neoplasms diagnosis

Abstract

Functional imaging can address hitherto irresolvable questions about cancer biology in both research and practice. In the clinic, by combining features of systemic and local disease markers into reference standards for the diagnosis of new disease entities functional imaging has the potential to literally redefine illness. Clinical assessments can be conducted at two levels: establishment of new reference standards, and evaluation of successor technologies that will substitute for a reference standard in practice. A union of functional imaging with anatomical criteria of disease has shown great promise in the management of numerous cancers. More work is required to use functional imaging to develop 'functional' approaches to diagnosis and therapy. Many methodologies exist for the acquisition of primary data on imaging technology efficacy. A form of economic cost-effectiveness modelling called iterative decision analysis can be used to set research and service priorities. Cancer clinicians need to take an increased role in functional imaging research, as they have primary expertise in the development and use of treatments modifying cell and tissue function.

Published

2002

83. PET for in vivo pharmacokinetic and pharmacodynamic measurements.

Author

Gupta N, Price PM, and Aboagye EO

Subjects

Animals, Antibodies therapeutic use, Antineoplastic Agents pharmacology, Antineoplastic Agents therapeutic use, Apoptosis, Cell Division, Cell Hypoxia, Clinical Trials, Phase I as Topic, Drug Resistance, Multiple, Humans, Imaging, Three-Dimensional methods, Neoplasms diagnostic imaging, Neoplasms drug therapy, Prodrugs, Radiopharmaceuticals, Receptors, Drug analysis, Antineoplastic Agents pharmacokinetics, Neoplasms metabolism, Tomography, Emission-Computed methods

Abstract

Positron emission tomography (PET) scanning is evolving as a unique tool for drug development in oncology for improving both the efficacy of established treatment and in evaluating novel anticancer agents. As a non-invasive functional imaging modality, PET has an unrivalled sensitivity when monitoring the pharmacokinetics and pharmacodynamics of drugs and biochemicals when radiolabelled with short living positron-emitting radioisotopes. This is of particular relevance in assessing newer molecular-targeted therapy where conventional evaluation criteria (maximum tolerated dose and tumour shrinkage for example) may be inappropriate. PET has already been applied to a wide number of drugs to demonstrate activity in vivo from standard chemotherapy such as 5-fluorouracil (5-FU) [J Clin Oncol 17 (1999) 1580], to novel molecular agents such as those involved in tumour angiogenesis [Br J Cancer 83 (2000) P6] and antivascular therapy [Proc Annu Meet Am Soc Clin Oncol 19 (2000) 179a]. This review will evaluate the achievements of PET in the drug development process, an approach that promises to facilitate the rapid translation of scientific research into current clinical practice.

Published

2002

84. Coordination of the cell cycle is an important determinant of the syndrome of acute renal failure.

Author

Megyesi J, Andrade L, Vieira JM Jr, Safirstein RL, and Price PM

Subjects

Animals, Blotting, Northern, Cell Death physiology, Cell Nucleus pathology, Cisplatin pharmacology, Hydrogen Peroxide toxicity, In Situ Hybridization, Kidney pathology, Mice, Mice, Knockout, Oncogene Protein p21(ras) genetics, Oxidants toxicity, Protein Synthesis Inhibitors pharmacology, RNA, Messenger biosynthesis, Acute Kidney Injury pathology, Cell Cycle physiology

Abstract

Recovery from injury is usually accompanied by cell replication, in which new cells replace those irreparably damaged. After acute renal failure, normally quiescent kidney cells enter the cell cycle, which in tubule segments is accompanied by the induction of cell cycle inhibitors. We found that after acute renal failure induced by either cisplatin injection or renal ischemia, induction of the p21 cyclin-dependent kinase (cdk) inhibitor is protective. Mice lacking this gene developed more widespread kidney cell death, more severe renal failure, and had reduced survival, compared with mice with a functional p21 gene. Here, we show induction of 14-3-3sigma, a regulator of G(2)-to-M transition, after acute renal failure. Our findings, using both in vivo and in vitro models of acute renal failure, show that this protein likely helps to coordinate cell cycle activity to maximize recovery of renal epithelial cells from injury and reduce the extent of the injury itself. Because in terminally differentiated cells, these proteins are highly expressed only after injury, we propose that cell cycle coordination by induction of these proteins could be a general model of tissue recovery from stress and injury.

Published

2002

85. Aprotinin: antifibrinolytic and anti-inflammatory mechanisms of action in cardiac surgery with cardiopulmonary bypass.

Author

Donahue MA and Price PM

Subjects

Aprotinin administration & dosage, Aprotinin pharmacokinetics, Cost-Benefit Analysis, Drug Interactions, Fibrinolysis drug effects, Hemostatics administration & dosage, Hemostatics pharmacokinetics, Humans, Inflammation Mediators pharmacology, Aprotinin pharmacology, Cardiopulmonary Bypass, Hemostatics pharmacology

Abstract

Cardiopulmonary bypass results in activation of the coagulation, fibrinolytic, inflammatory, and complement cascades. These activated cascades result in a decrease in the number of circulating coagulation factors, hyperfibrinolysis, thrombocytopenia, platelet defects, coagulopathies, and an acute inflammatory response. Patients experiencing cardiac surgery with cardiopulmonary bypass are at risk for many potential problems. The use of aprotinin, an antifibrinolytic agent, has multiple effects that tend to reduce hematological defects and blunts the inflammatory response that is associated with cardiac surgery. The pathophysiological consequences of cellular activation associated with cardiopulmonary bypass, basic mechanisms of action of aprotinin, pharmacodynamic and pharmacokinetic properties, dosing, adverse reactions, and cost/benefit ratio are discussed in this article. Critical care nurses need to know about aprotinin to understand its role in reducing blood loss and transfusions during and after cardiac surgery.

Published

2002

86. Clinical value of positron emission tomography.

Author

Laking GR and Price PM

Subjects

Female, Fluorodeoxyglucose F18, Humans, Radiopharmaceuticals, Neoplasm Recurrence, Local diagnostic imaging, Ovarian Neoplasms diagnostic imaging, Tomography, Emission-Computed

Published

2002

87. FDG-PET for response assessment: answers in search of questions.

Author

Laking GR and Price PM

Subjects

Chemotherapy, Adjuvant, Esophageal Neoplasms pathology, Esophageal Neoplasms therapy, Humans, Radiotherapy, Adjuvant, Remission Induction, Treatment Outcome, Esophageal Neoplasms diagnostic imaging, Fluorodeoxyglucose F18, Radiopharmaceuticals, Tomography, Emission-Computed

Published

2002

88. Radiolabelled tracers and anticancer drugs for assessment of therapeutic efficacy using PET.

Author

Brady F, Luthra SK, Brown GD, Osman S, Aboagye E, Saleem A, and Price PM

Subjects

Animals, Antineoplastic Agents pharmacokinetics, Drug Resistance, Neoplasm, Humans, Isotope Labeling, Neoplasms genetics, Neoplasms pathology, Antineoplastic Agents therapeutic use, Neoplasms diagnostic imaging, Neoplasms drug therapy, Radiopharmaceuticals pharmacokinetics, Tomography, Emission-Computed

Abstract

Positron Emission Tomography (PET) has the potential to improve efficacy of established and novel cancer therapies and to assist more rapid and rational progression of promising novel therapies into the clinic. This is due to PET's unrivalled sensitivity and ability to monitor the pharmacokinetics and pharmacodynamics of drugs and biochemicals radiolabelled with short -lived positron emitting radioisotopes. PET is a multidisciplinary science which employs chemists, biologists, mathematical modellers, pharmacologists as well as clinicians. Clinical research questions in oncology determine the methodological challenges faced by these other disciplines. Within this context we focus on the developments of the radiolabelled compounds that have underpinned the clinical work in oncology for monitoring tumour and normal tissue pharmacokinetics, assessment of tumour response, cell proliferation, gene expression, hypoxia, multidrug resistance and status of receptors on tumours.

Published

2001

89. Positive effect of the induction of p21WAF1/CIP1 on the course of ischemic acute renal failure.

Author

Megyesi J, Andrade L, Vieira JM Jr, Safirstein RL, and Price PM

Subjects

Animals, Cyclin-Dependent Kinase Inhibitor p21, Ischemia pathology, Ischemia physiopathology, Mice, Mice, Knockout genetics, Reperfusion Injury pathology, Survival Analysis, Acute Kidney Injury etiology, Acute Kidney Injury physiopathology, Cyclins genetics, Gene Expression Regulation physiology, Ischemia complications, Renal Circulation

Abstract

Background: The p21 protein is found in the nucleus of most cells where it modulates cell cycle activity. At low levels, p21 stabilizes interactions between D cyclins and their cyclin-dependent kinases (cdks), but at high levels after induction by several different stress pathways, it causes cell cycle arrest. The p21 mRNA is induced in murine kidney after several types of acute renal failure, including cisplatin administration, ischemia-reperfusion, and ureteral obstruction. We reported that after cisplatin injection, mice with a p21 gene deletion developed much more severe renal damage than wild-type mice. To dissociate the effects of cisplatin-induced DNA damage and subsequent initiation of DNA damage-dependent cell death pathways from effects of acute renal failure, we have now examined mice after ischemia-reperfusion, a model of renal failure not associated with genotoxin-induced DNA damage early after the injury., Methods: Wild-type and p21(-/-) mice were made ischemic by clamping both renal hila for 30 or 50 minutes. At various times after reflow, mortality and parameters of renal function and morphology were quantified. Also, the nuclear proteins p21 and proliferating cell nuclear antigen (PCNA) were localized in kidney sections by immunohistochemistry., Results: Kidney function was more impaired and mortality increased significantly in p21(-/-) mice as compared with p21(+/+) mice. We found more cell cycle activity, indicated by increased number of mitotic cells and nuclear PCNA-positive cells, in kidney of p21(-/-) mice., Conclusions: In this study, p21(-/-) mice were more susceptible to ischemia-induced acute renal failure, with similarly elevated levels of parameters of cell cycle activity. We propose that the increased and inappropriate cell cycle activity in kidney cells is responsible for the increased kidney impairment and mortality.

Published

2001

90. Two routes to [11C-carbonyl]organo-isocyanates utilizing [11C]phosgene ([11C]organo-isocyanates from [11C]phosgene).

Author

Brown GD, Henderson D, Steel C, Luthra S, Price PM, and Brady F

Subjects

Chromatography, High Pressure Liquid, Isocyanates chemistry, Isotope Labeling, Phosgene chemistry, Carbon Radioisotopes, Isocyanates chemical synthesis

Abstract

Two generic radiosynthetic routes for the preparation of [11C-carbonyl]isocyanates have been developed. Reaction of N-organo-sulfinylamines; RNSO, (R = Me, Et, allyl, cyclohexyl and phenyl) with [11C]phosgene gave the corresponding [11C-carbonyl]isocyanates in good radiochemical yield (53-68%) from [11C]phosgene (decay corrected) in ca 16 min from EOB. Alternatively, the reaction of [11C]phosgene with N,N'-organo-ureas; (RNH)(2)CO, (R = Me, Et, Pr and phenyl) also gave the corresponding [11C-carbonyl]isocyanates in moderate radiochemical yield (9-37%) from [11C]phosgene (decay corrected) in ca 16 min from EOB. For identification, the [11C-carbonyl]organo-isocyanates were derivatized with 1-(2-methoxyphenyl)piperazine in situ to [11C-carbonyl]carboxamides and the position of radiolabelling in the carbonyl group confirmed by [11/13C]co-labeling and subsequent carbon-13 NMR spectroscopy.

Published

2001

91. Extraction of 5-fluorouracil by tumor and liver: a noninvasive positron emission tomography study of patients with gastrointestinal cancer.

Author

Aboagye EO, Saleem A, Cunningham VJ, Osman S, and Price PM

Subjects

Antimetabolites, Antineoplastic blood, Antimetabolites, Antineoplastic metabolism, Dihydrouracil Dehydrogenase (NADP), Enzyme Inhibitors pharmacology, Fluorine Radioisotopes, Fluorouracil blood, Fluorouracil metabolism, Gastrointestinal Neoplasms blood, Humans, Liver Neoplasms metabolism, Liver Neoplasms secondary, Models, Biological, Oxidoreductases antagonists & inhibitors, Pancreatic Neoplasms blood, Pancreatic Neoplasms metabolism, Tomography, Emission-Computed, Uracil pharmacology, Antimetabolites, Antineoplastic pharmacokinetics, Fluorouracil pharmacokinetics, Gastrointestinal Neoplasms metabolism, Liver metabolism, Uracil analogs & derivatives

Abstract

Tumor and normal tissue pharmacokinetics of 5-Fluorouracil (5-FU) in patients can be determined with positron emission tomography scanning. However, the data obtained are of limited value because of the inability to distinguish catabolites (inactive species) from parent 5-FU and anabolites (cytotoxic species). In this paper, we have blocked 5-FU catabolism in one arm of a paired study with eniluracil, an inactivator of dihydropyrimidine dehydrogenase, enabling catabolite correction and calculation of tissue pharmacokinetic parameters to be achieved. Using this novel approach, we report for the first time that the net clearance of 5-[(18)F]FU from plasma into tumors (liver metastases and pancreatic tumor) of patients is low (K(I) = 0.0033 +/- 0.0005 ml plasma/ml tissue/min). In contrast, the initial (up to 10 min) clearance through catabolism in liver was high (K(I) = 0.7313 +/- 0.092 ml plasma/ml tissue/min). In the absence of eniluracil, catabolites in tumors accounted for 83% of total tumor exposure (range, 66-91%), whereas catabolites in liver accounted for 96% of total liver exposure (range, 94-98%). This study provides definitive evidence that the cytotoxicity of 5-FU in patients with gastrointestinal cancer could be compromised by its intrinsically low uptake by tumors, as well as decreased systemic availability through hepatic catabolism.

Published

2001

92. Comparative biodistribution and metabolism of carbon-11-labeled N-[2-(dimethylamino)ethyl]acridine-4-carboxamide and DNA-intercalating analogues.

Author

Osman S, Rowlinson-Busza G, Luthra SK, Aboagye EO, Brown GD, Brady F, Myers R, Gamage SA, Denny WA, Baguley BC, and Price PM

Subjects

Acridines chemistry, Acridines metabolism, Acridines toxicity, Animals, Antineoplastic Agents metabolism, Antineoplastic Agents toxicity, Carbon Radioisotopes, Female, Glioma drug therapy, Glioma metabolism, HT29 Cells, Humans, Inhibitory Concentration 50, Intercalating Agents metabolism, Intercalating Agents toxicity, Isotope Labeling, Melanoma drug therapy, Melanoma metabolism, Mice, Mice, Inbred ICR, Mice, Nude, Tissue Distribution, Tomography, Emission-Computed, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Acridines pharmacokinetics, Antineoplastic Agents pharmacokinetics, Intercalating Agents pharmacokinetics

Abstract

The tricyclic carboxamide N-[2-(dimethylamino)ethyl]acridine-4-carboxamide (DACA) is a DNA-intercalating agent capable of inhibiting both topoisomerases I and II and is currently in Phase II clinical trial. Many related analogues have been developed, but despite their potent in vitro cytotoxicities, they exhibit poor extravascular distribution. As part of an ongoing drug development program to obtain related "minimal intercalators" with lower DNA association constants, we have compared the biodistribution and metabolite profiles of the prototype compound, DACA, with three analogues to aid rational drug selection. All of these compounds share a common structural feature, N-dimethyl side chain, which was radiolabeled with the positron-emitting radioisotope, carbon-11. This strategy was selected because it allows promising candidates emerging from preclinical studies in animals to be evaluated rapidly in humans using positron emission tomography (PET). The acridine DACA, the phenazine SN 23490, the pyridoquinoline SN 23719, and the dibenzodioxin SN 23935 were found to be cytotoxic in in vitro assays with an IC50 of 1.4-1.8 microM, 0.4-0.6 microM, 1.3-1.6 microM, and 24-36 microM, respectively, in HT29, U87MG, and A375M cell lines. Ex vivo biodistribution studies with carbon-11 radiolabeled compounds in mice bearing human tumor xenografts showed rapid clearance of 11C-radioactivity (parent drug and metabolites) from blood and the major organs. Rapid hepatobiliary clearance and renal excretion were also observed. There was low [<5% of injected dose/gram (%ID/g)] and variable uptake of 11C-radioactivity in three tumor types for all of the compounds. Tumor (U87MG) to blood 11C-radioactivity for [11C]DACA, [11C](9-methoxyphenazine-1-carboxamide (SN 23490), [11C]2-(4-pyridyl)quinoline-8-carboxamide (SN 23719), and [11C]dibenzo[1,4]dioxin-1-carboxamide (SN 23935) at 30 min were 2.9 +/- 1.1, 2.3 +/- 0.6, 2.6 +/- 0.6, and 0.7 +/- 0.2, respectively. For SN 23719, the distribution of 11C-radioactivity in normal tissues and tumors determined ex vivo was in broad agreement with that determined in vivo by whole body PET scanning. [11C]DACA was rapidly and extensively metabolized to several plasma metabolites and a major tumor metabolite. In contrast, [11C]SN 23935, [11C]SN 23490, and [11C]SN 23719 showed less extensive metabolism. In the tumor samples, the parent [11C]DACA and [11C]SN 23935 represented between 0.3 and 1.5%ID/g, whereas [11C]SN 23490 and [11C]SN 23719 represented between 1.5 and 2.8%ID/g. In conclusion, by using a strategy with 11C-labeling, we have determined the tissue distribution and metabolic stability of novel tricyclic carboxamides with the view of selecting analogues with potentially better in vivo activity against solid tumors. SN 23490 and SN 23719 had more favorable distribution and metabolic stability compared with DACA and SN 23935 and may warrant further development. The radiolabeling strategy used allows ex vivo and in vivo evaluation of promising anticancer agents in animals and offers the potential of rapid translation to studies in humans using PET.

Published

2001

93. In vivo pharmacokinetics and pharmacodynamics in drug development using positron-emission tomography.

Author

Aboagye EO, Price PM, and Jones T

Abstract

Positron-emission tomography (PET) is a sensitive technique that can be used to measure drug pharmacokinetics and pharmacodynamics non-invasively in target tissues of patients. Here we focus on the application of this technology to address some of the bottlenecks in drug development, including: elucidation of pathophysiology, evaluation of pharmacokinetics, proof of principle of mechanism, and assessment of efficacy and/or response to therapy.

Published

2001

94. Pharmacokinetic evaluation of N-[2-(dimethylamino)ethyl]acridine-4-carboxamide in patients by positron emission tomography.

Author

Saleem A, Harte RJ, Matthews JC, Osman S, Brady F, Luthra SK, Brown GD, Bleehen N, Connors T, Jones T, Price PM, and Aboagye EO

Subjects

Adult, Aged, Aged, 80 and over, Area Under Curve, Carbon Radioisotopes, Female, Humans, Kinetics, Male, Middle Aged, Neoplasms drug therapy, Tissue Distribution, Acridines pharmacokinetics, Antineoplastic Agents pharmacokinetics, Tomography, Emission-Computed

Abstract

Purpose: To evaluate tumor, normal tissue, and plasma pharmacokinetics of N-[2-(dimethylamino)ethyl]acridine-4-carboxamide (DACA). The study aimed to determine the pharmacokinetics of carbon-11-labeled DACA ([11C]DACA) and evaluate the effect of pharmacologic doses of DACA on radiotracer kinetics., Patients and Methods: [11C]DACA (at 1/1,000 phase I starting dose) was administered to 24 patients with advanced cancer (pre-phase I) or during a phase I trial of DACA in five patients. Positron emission tomography (PET) was performed to assess pharmacokinetics and tumor blood flow. Plasma samples were analyzed for metabolite profile of [11C]DACA., Results: There was rapid systemic clearance of [11C]DACA over 60 minutes (1.57 and 1.46 L x min(-1) x m(-2) in pre-phase I and phase I studies, respectively) with the production of several radiolabeled plasma metabolites. Tumor, brain, myocardium, vertebra, spleen, liver, lung, and kidneys showed appreciable uptake of 11C radioactivity. The area under the time-versus-radioactivity curves (AUC) showed the highest variability in tumors. Of interest to potential toxicity, maximum radiotracer concentrations (Cmax) in brain and vertebra were low (0.67 and 0.54 m(2) x mL(-1), respectively) compared with other tissues. A moderate but significant correlation was observed for tumor blood flow with AUC (r = 0.76; P =.02) and standardized uptake value (SUV) at 55 minutes (r = 0.79; P =.01). A decrease in myocardial AUC ( P =.03) and splenic and myocardial SUV ( P =.01 and.004, respectively) was seen in phase I studies. Significantly higher AUC, SUV, and Cmax were observed in tumors in phase I studies., Conclusion: The distribution of [11C]DACA and its radiolabeled metabolites was observed in a variety of tumors and normal tissues. In the presence of unlabeled DACA, pharmacokinetics were altered in myocardium, spleen, and tumors. These data have implications for predicting activity and toxicity of DACA and support the use of PET early in drug development.

Published

2001

95. Modulation of fluorouracil tissue pharmacokinetics by eniluracil: in-vivo imaging of drug action.

Author

Saleem A, Yap J, Osman S, Brady F, Suttle B, Lucas SV, Jones T, Price PM, and Aboagye EO

Subjects

Administration, Oral, Adult, Aged, Antimetabolites, Antineoplastic administration & dosage, Antimetabolites, Antineoplastic therapeutic use, Dihydrouracil Dehydrogenase (NADP), Drug Interactions, Enzyme Inhibitors administration & dosage, Female, Fluorouracil administration & dosage, Fluorouracil therapeutic use, Gastrointestinal Neoplasms drug therapy, Half-Life, Humans, Injections, Intravenous, Liver drug effects, Liver metabolism, Male, Middle Aged, Tissue Distribution, Tomography, Emission-Computed, Uracil administration & dosage, Uracil pharmacology, Antimetabolites, Antineoplastic pharmacokinetics, Enzyme Inhibitors pharmacology, Fluorouracil pharmacokinetics, Gastrointestinal Neoplasms metabolism, Oxidoreductases antagonists & inhibitors, Uracil analogs & derivatives

Abstract

Background: Fluorouracil is widely used for chemotherapy of gastrointestinal cancer, but response rates are poor. Eniluracil is being developed as an inactivator of dihydropyrimidine dehydrogenase, the enzyme that brings about first-pass degradation of fluorouracil. We studied the mechanism of action of eniluracil by measuring with positron emission tomography (PET) the effect of eniluracil on tumour and normal-tissue pharmacokinetics of fluorine-18-labelled fluorouracil., Methods: Six patients with advanced gastrointestinal cancers were studied. PET scanning was done after injection of oxygen-15-labelled water to assess tissue blood flow, followed by 1 mg/m2 18F-fluorouracil. We compared the pharmacokinetics of 18F-fluorouracil when the patients had not received eniluracil, during a 4-day course of oral eniluracil, and during a 28-day course of oral fluorouracil plus eniluracil., Findings: In eniluracil-naïve patients, 18F-fluorouracil localised more strongly (mean 0.0234% [SE 0.0019] of injected activity per mL tissue at 11 min) in liver than in tumours (0.0032% [0.0004]). There was substantial inhibition, after eniluracil administration, of radiotracer uptake and retention in normal liver (mean area under the time versus radioactivity curve 0.927 [SE 0.086] vs 1.857 [0.169] m2 mL(-1) s) and kidneys (1.096 [0.048] vs 5.043 [0.915] m2 mL(-1) s). There was also an increase in plasma uracil and unmetabolised 18F-fluorouracil and an increase in the radiotracer half-life in tumours (2.3 h to >4.0 h)., Interpretation: Two events strongly suggested increased exposure of 18F-fluorouracil and its anabolites in the tumours, consistent with the inactivation of dihydropyrimidine dehydrogenase: a selective decrease in radiotracer exposure in normal liver and kidneys compared with tumours; and an increase in radiotracer half-life in tumours.

Published

2000

96. Prepare to publish.

Author

Price PM

Subjects

Humans, Critical Care, Nursing Staff, Hospital, Publishing, Writing

Abstract

"I couldn't possibly write an article." "I don't have anything worthwhile to write about." "I am not qualified to write for publication." Do any of these statements sound familiar? This article is intended to dispel these beliefs. You can write an article. You care for the most complex patients in the health care system so you do have something worthwhile to write about. Beside correct spelling and grammar there are no special skills, certificates or diplomas required for publishing. You are qualified to write for publication. The purpose of this article is to take the mystique out of the publication process. Each step of publishing an article will be explained, from idea formation to framing your first article. Practical examples and recommendations will be presented. The essential components of the APA format necessary for Dynamics: The Official Journal of the Canadian Association of Critical Care Nurses will be outlined and resources to assist you will be provided.

Published

2000

97. In vivo monitoring of drugs using radiotracer techniques.

Author

Saleem A, Aboagye EO, and Price PM

Subjects

Drug Administration Schedule, Fluconazole pharmacokinetics, Fluorouracil pharmacokinetics, Humans, Models, Biological, Receptors, Cell Surface metabolism, Tomography, Emission-Computed, Tomography, Emission-Computed, Single-Photon, Drug Monitoring, Radionuclide Imaging

Abstract

There is an increasing realization of the role of non-invasive monitoring of drug pharmacology. In this review, we discuss the role of positron emission tomography in such monitoring of tumour and normal tissue drug pharmacokinetics as well as assessment of tumour response, drug-receptor interactions and mechanisms of drug action and resistance. These studies represent a multidisciplinary research effort involving radiochemists, imaging scientists, clinicians, pharmacologists and mathematical modellers. This review evaluates achievements in the field from assessment of commonly used therapeutic agents such as 5-fluorouracil to target specific molecules such as markers for gene expression. It is envisaged that application of this technology will facilitate rational drug design and rapid translation of new ideas to the bedside.

Published

2000

98. Early evaluation of tumour metabolic response using [18F]fluorodeoxyglucose and positron emission tomography: a pilot study following the phase II chemotherapy schedule for temozolomide in recurrent high-grade gliomas.

Author

Brock CS, Young H, O'Reilly SM, Matthews J, Osman S, Evans H, Newlands ES, and Price PM

Subjects

Adult, Brain Neoplasms diagnostic imaging, Dacarbazine therapeutic use, Evaluation Studies as Topic, Female, Glioma diagnostic imaging, Humans, Male, Middle Aged, Neoplasm Recurrence, Local, Pilot Projects, Temozolomide, Tomography, Emission-Computed, Antineoplastic Agents, Alkylating therapeutic use, Brain Neoplasms drug therapy, Dacarbazine analogs & derivatives, Fluorodeoxyglucose F18, Glioma drug therapy, Radiopharmaceuticals

Abstract

Quantitation of metabolic changes in tumours may provide an objective measure of clinical and subclinical response to anticancer therapy. This pilot study assesses the value of quantitation of metabolic rate of glucose (MRGlu) measured in mmol min(-1) ml(-1) to assess early subclinical response to therapy in a relatively non-responsive tumour. Nine patients receiving the CRC Phase II study schedule of temozolomide were assessed with [18F]fluorodeoxyglucose ([18F]FDG) dynamic positron emission tomography (PET) scans prior to and 14 days after treatment with temozolomide given as 750-1000 mg m(-2) over 5 days every 28 days. Tumour MRGlu was calculated and compared with objective response at 8 weeks. Pretreatment MRGlu was higher in responders than non-responders. The responding patient group had a greater than 25% reduction in MRGlu in regions of high focal tumour uptake (HFU). Whole tumour changes in MRGlu did not correlate with response. Percentage change in HFU standardized uptake value (SUV) did discriminate the responding from the non-responding patients, but not as well as with MRGlu. Large differences also occurred in the normal brain SUV following treatment. Thus, MRGlu appeared to be a more sensitive discriminator of response than the simplified static SUV analysis. Changes in MRGlu may reflect the degree of cell kill following chemotherapy and so may provide an objective, quantitative subclinical measure of response to therapy.

Published

2000

99. An automated radiosynthesis of 2-[11C]thymidine using anhydrous [11C]urea derived from [11C]phosgene.

Author

Steel CJ, Brady F, Luthra SK, Brown G, Khan I, Poole KG, Sergis A, Jones T, and Price PM

Subjects

Carbon Tetrachloride chemical synthesis, Chromatography, High Pressure Liquid, Isotope Labeling methods, Methane chemical synthesis, Quality Control, Radiochemistry, Carbon Radioisotopes chemistry, Phosgene chemical synthesis, Radiopharmaceuticals chemical synthesis, Thymidine chemical synthesis, Urea chemical synthesis

Abstract

2-[11C]Thymidine has been produced from [11C]methane via [11C]phosgene and [11C]urea. Anhydrous [11C]urea was prepared from [11C]phosgene by reaction with liquid ammonia. This novel approach avoids the problems associated with the synthesis of anhydrous [11C]urea from [11C]cyanide. A fully automated system based on a modular approach and under PLC control has been developed. The system provides 2-[11C]thymidine reliably and reproducibly for clinical PET studies. The radiosynthesis takes 45-50 min from [11C]methane and the average yield was 1.5-3.3 GBq (40-90 mCi). The specific radioactivity was typically in the range 29.6-51.8 GBq mumol-1 (0.8-1.4 Ci mumol-1) at EOS corresponding to 6-12 micrograms of stable thymidine. The radiochemical yield of 2-[11C]thymidine was ca. 14% from [11C]methane.

Published

1999

100. The lack of a functional p21(WAF1/CIP1) gene ameliorates progression to chronic renal failure.

Author

Megyesi J, Price PM, Tamayo E, and Safirstein RL

Subjects

Animals, Blood Pressure, Body Weight, Cell Cycle, Cyclin-Dependent Kinase Inhibitor p21, Disease Models, Animal, Glomerulosclerosis, Focal Segmental genetics, Glomerulosclerosis, Focal Segmental metabolism, Hypertrophy, In Situ Hybridization, Insulin pharmacokinetics, Kidney anatomy & histology, Kidney metabolism, Kidney physiology, Male, Mice, Mutagenesis, Renal Insufficiency metabolism, Time Factors, Cyclins genetics, Cyclins physiology, Renal Insufficiency genetics

Abstract

Partial renal ablation leads to progressive renal insufficiency and is a model of chronic renal failure from diverse causes. We find that mice develop functional and morphologic characteristics of chronic renal failure after partial renal ablation, including glomerular sclerosis, systemic hypertension, and reduced glomerular filtration. However, we now report that littermates with a homozygous deletion of the gene for the cyclin-dependent kinase inhibitor, p21(WAF1/CIP1), do not develop chronic renal failure after ablation. The markedly different reactions of the p21(+/+) and p21(-/-) animals was not because of differences in glomerular number or degree of renal growth but rather because of the presence or absence of a normal p21 gene. Although the reaction to the stress of renal ablation is both hyperplastic and hypertrophic in the presence of a functional p21 gene, it would appear that the absence of the p21 gene may induce a more hyperplastic reaction because proliferating-cell nuclear antigen expression, a marker of cell-cycle progression, in the renal epithelium of the remnant kidney was more than five times greater in the p21(-/-) mice than in the p21(+/+) animals. Because p21 is a potent inhibitor of the cell cycle, we speculate that p21 regulates the balance between hyperplasia and hypertrophy after renal ablation. We propose that this change in response inhibits the development of chronic renal failure. These studies suggest that controlling p21 function may ameliorate or even prevent progressive end-stage renal disease.

Published

1999