Your search keyword '"Morris GM"' showing total 10 results

1. Enhancement of the radiation response of EMT-6 tumours by a copper octabromotetracarboranylphenylporphyrin.

Author

Miura M, Morris GM, Hopewell JW, Micca PL, Makar MS, Nawrocky MM, and Renner MW

Subjects

Animals, Dose-Response Relationship, Drug, Electrochemistry, Female, Metalloporphyrins pharmacokinetics, Mice, Mice, Inbred BALB C, Porphyrins pharmacokinetics, Skin radiation effects, Tissue Distribution, Metalloporphyrins pharmacology, Neoplasms, Experimental radiotherapy, Porphyrins pharmacology, Radiation-Sensitizing Agents pharmacology

Abstract

Objective: The carborane-containing porphyrin, copper (II) 2,3,7,8,12,13,17,18-octabromo-5,10,15,20-tetrakis(3-[1,2-dicarba-closo-dodecaboranyl]methoxyphenyl)-porphyrin (CuTCPBr), was investigated as a potential radiation enhancing agent for X-ray radiotherapy (XRT) in a subcutaneously implanted EMT-6 murine carcinoma., Method: The biodistribution and toxicological profile of this porphyrin has been shown to be favourable for another bimodal radiotherapy technique, boron neutron-capture therapy. For the XRT studies, CuTCPBr was formulated in either 9% Cremophor (BASF Corporation, Ludwigschafen, Germany) EL and 18% propylene glycol (9% CRM) or a revised formulation comprising 1% Cremophor ELP, 2% Tween 80 (JT Baker, Mansfield, MA), 5% ethanol and 2.2% PEG 400 (CTEP formulation), which would be more clinically acceptable than the original 9% CRM formulation. Using the 9% CRM formulation of CuTCPBr, doses of 100, 210 or 400 mg kg(-1) of body weight were used in combination with single doses of 25-35 Gy 100 kVp X-rays., Results: While doses of 100 mg kg(-1) and 210 mg kg(-1) did not result in any significant enhancement of tumour response, the 400 mg kg(-1) dose did. A dose modification factor of 1.20±0.10 was obtained based on the comparison of doses that produced a 50% local tumour control probability. With the CTEP formulation of CuTCPBr, doses of 83 and 170 mg kg(-1) produced significant radiation enhancement, with dose modification factors based on the TCP(50) of 1.29±0.15 and 1.84±0.24, respectively., Conclusion: CuTCPBr significantly enhanced the efficacy of XRT in the treatment of EMT-6 carcinomas in mice. The CTEP formulation showed a marked improvement, with over 9% CRM being associated with higher dose modification factors. Moreover, the radiation response in the skin was not enhanced.

Published

2012

2. Synthesis of copper octabromotetracarboranylphenylporphyrin for boron neutron capture therapy and its toxicity and biodistribution in tumour-bearing mice.

Author

Miura M, Morris GM, Micca PL, Nawrocky MM, Makar MS, Cook SP, and Slatkin DN

Subjects

Animals, Boron pharmacokinetics, Boron Neutron Capture Therapy adverse effects, Carcinoma, Squamous Cell radiotherapy, Dose-Response Relationship, Drug, Female, Mammary Neoplasms, Experimental radiotherapy, Metalloporphyrins chemical synthesis, Mice, Mice, Inbred BALB C, Mice, Inbred C3H, Neoplasm Transplantation, Tissue Distribution, Boron Neutron Capture Therapy methods, Carcinoma, Squamous Cell metabolism, Mammary Neoplasms, Experimental metabolism, Metalloporphyrins pharmacokinetics

Abstract

Copper tetracarboranyltetraphenylporphyrin (CuTCPH) is a minimally toxic carborane-containing porphyrin that has safely delivered high concentrations of boron for experimental boron neutron capture therapy (BNCT). Copper octabromotetracarboranylphenylporphyrin (CuTCPBr), synthesized by bromination of CuTCPH, is one of several new minimally toxic analogues of CuTCPH being studied in our laboratory, which could possess comparable or better tumour-targeting properties with enhanced tumour cytotoxicity. Its biodistribution, biokinetics and toxicity in mice with subcutaneous EMT-6 (mammary) or SCCVII (squamous cell) carcinomas were compared with those of CuTCPH. The administration of approximately 200 mg kg(-1) of either porphyrin in six intraperitoneal injections over 2 days had no apparent effect, but administration of approximately 400 mg kg(-1) slightly lowered body weights, elevated alanine and aspartate transaminase activities in blood plasma, and depressed blood platelet counts for several days. Enzymes and platelets returned to normal within 5 days after those injections and body weights returned to normal within 2 weeks. High average concentrations of boron from either porphyrin were achieved in the two tumour models from a total dose of approximately 200 mg kg(-1). The high tumour boron concentration decreased slowly while concentrations in blood decreased rapidly. Boron concentrations in brain and skin were consistently lower than in tumour by a factor of 10 or more. Although either CuTCPH or CuTCPBr can be labelled with (64)Cu for imaging by positron emission tomography (PET), CuTCPBr can also be labelled by (76)Br, another PET-imageable nuclide.

Published

2004

3. Changes in epidermal radiosensitivity with time associated with increased colony numbers.

Author

van den Aardweg GJ, Morris GM, Bywaters A, Bakker EJ, and Mooi WJ

Subjects

Analysis of Variance, Animals, Biopsy, Bromodeoxyuridine metabolism, Cell Survival, Colony-Forming Units Assay, Cytokines physiology, Epidermal Cells, Female, Hair Follicle cytology, Hair Follicle radiation effects, Immunohistochemistry, Swine, Time Factors, Epidermis radiation effects, Radiation Tolerance

Abstract

Epidermal clonogenic cell survival and colony formation following irradiation were investigated and related to radiosensitivity. A rapid in vivo/in vitro assay was developed for the quantification of colonies arising from surviving clonogenic cells in pig epidermis after irradiation. Bromodeoxyuridine (BrdU)-labelled cells in full thickness epidermal sheets were visualized using standard immunohistochemistry. In unirradiated skin, approximately 900 BrdU-positive cells mm(-2) were counted. In a time sequence experiment, BrdU-positive cell numbers increased from an average of 900 cells mm(-2) to approximately 1400 cells mm(-2) after BrdU-labelling for 2-24 h. In irradiated skin, colonies containing >/=16 BrdU-positive cells were seen for the first time at days 14/15 after irradiation. The number of these colonies per cm(2) as a function of skin surface dose yielded a cell survival curve with a D(0)-value (+/-SE) of 3.9+/-0.6 Gy. This relatively high D(0)-value is possibly due to a rapid fall off in depth dose distribution for the iridium-192 source and consequently a substantial contribution of hair follicular epithelium to colony formation. At 14/15 days after irradiation, the ED(50) level of 33.6 Gy for the in vivo response of moist desquamation corresponded with 2.7 colonies cm(-2). Surprisingly, the number of colonies increased with time after irradiation with an estimated doubling time of approximately 4 days, while the D(0)-value remained virtually unchanged. This increase in colony numbers could be due to migration of clonogenic cells, to the recruitment of dormant clonogenic cell survivors by elevated levels of cytokines, or to both. Although frequent biopsying caused increased cytokine levels, which had a systemic effect on unirradiated skin, it had no influence on colony formation in irradiated skin. Smaller colonies, containing 4-8 cells or 9-15 cells, were abundant, particularly after higher doses, which resulted in higher D(0)-values. The majority of these small colonies were abortive and did not progress to larger colonies. There was no statistical evidence for significant variations in the interanimal responses.

Published

2001

4. Effects of Lipochromin and Levosinum in the modulation of radiation-induced injury to pig skin.

Author

Rezvani M, Uzlenkova N, Whitehouse E, Frenkel L, Wilkinson JH, Ross G, Morris GM, Hopewell JW, and Pilipenko N

Subjects

Administration, Cutaneous, Animals, Drug Combinations, Necrosis, Ointments, Skin drug effects, Swine, Time Factors, Anticarcinogenic Agents administration & dosage, Carotenoids administration & dosage, Models, Animal, Radiation Injuries, Experimental drug therapy, Radiation-Protective Agents administration & dosage, Skin radiation effects

Abstract

Pig skin was used as a model to study the effectiveness of two topically applied creams, Lipochromin and Levosinum, in modifying the development of both early and late radiation damage to pig skin. Irradiated skin sites that received daily topical application of Levosinum or Lipochromin after exposure were compared with sites on the contralateral flank of the same animal that received irradiation only. Irradiation was with graded doses of 90Sr/90Y beta-rays. Incidence of moist desquamation (acute) and ischaemic dermal necrosis (late) were used as end-points. The latency period for the development of moist desquamation and its healing time was also assessed. The latency period for the development of moist desquamation in this model ranged from 4.00-6.75 weeks. There was no significant difference between the cream treatment and control sites. Application of Levosinum shortened the healing time of moist desquamation at each dose level by 5-10 days. In three out of four dose levels used, this shortening of the healing time was statistically significant (p < 0.03). Treatment with these topical applications also reduced the incidence of late dermal necrosis and increased the ED50 values for the incidence of dermal necrosis. This increase in ED50 values was equivalent to a dose modification factor of 1.11-1.13.

Published

2000

5. Boron neutron capture therapy of the rat 9L gliosarcoma: evaluation of the effects of shark cartilage.

Author

Morris GM, Coderre JA, Micca PL, Lombardo DT, and Hopewell JW

Subjects

Angiogenesis Inhibitors therapeutic use, Animals, Brain Neoplasms pathology, Brain Neoplasms therapy, Gliosarcoma pathology, Gliosarcoma therapy, Neoplasm Transplantation, Rats, Rats, Inbred F344, Sharks, Survival Rate, Tumor Cells, Cultured, Boron Neutron Capture Therapy, Brain Neoplasms radiotherapy, Cartilage, Gliosarcoma radiotherapy, Radiation-Sensitizing Agents therapeutic use, Tissue Extracts therapeutic use

Abstract

A number of anti-angiogenic substances are now under evaluation, both experimentally and clinically, as potential agents for the treatment of cancer. It has recently been demonstrated that anti-angiogenic agents can increase the therapeutic potential of photon irradiation in a range of tumour models. In the present communication a preliminary assessment is made of the effects of shark cartilage on the response of the rat 9L gliosarcoma to boron neutron capture therapy (BNCT). Shark cartilage was administered orally as an aqueous suspension at a daily dose of approximately 2000 mg kg-1 body weight. The mean survival time of rats receiving no treatment was 20.7 +/- 0.5 days post intracranial tumour implantation. Administration of shark cartilage alone extended the survival time. Two of the rats treated with shark cartilage were healthy and fully active at the end of the evaluation period (43 days post implantation). At autopsy the brain tumours of these animals were a factor of approximately 4 smaller than controls. In a repeat study with shark cartilage alone the survival time was extended by approximately 30%. After boronophenylalanine-mediated BNCT, with or without shark cartilage, the survival time of rats that eventually became moribund was increased by a factor of approximately 2 relative to controls. In both treatment groups approximately 20% of rats were healthy at 1 year after BNCT. There was no evidence of residual tumour at post-mortem. It was concluded that shark cartilage, when given alone, significantly increased the survival time of tumour-bearing rats, presumably owing to an anti-angiogenic effect. However, the survival data suggested that boronophenylalanine-mediated BNCT did not appear to be enhanced by the administration of shark cartilage.

Published

2000

6. Review article: effects of radiation on the cell proliferation kinetics of epithelial tissues--therapeutic implications.

Author

Morris GM

Subjects

Animals, Cell Division radiation effects, Epithelial Cells, Humans, Radiation Dosage, Epithelium radiation effects, Radiotherapy methods

Abstract

The cell kinetic responses of the epithelia of the skin, oral mucosa and intestine to photon irradiation are reviewed. One of the fundamental assumptions made in the development of mathematical models, used to predict the acute response of normal tissues to changes in fractionation protocols, is "equal effect per fraction". There is now accumulating cell kinetic data to indicate that this assumption is unlikely to be valid. The implications of these findings are discussed.

Published

1996

7. A comparison of the effects of methotrexate and misonidazole on the germinal cells of the subependymal plate of the rat.

Author

Morris GM, Hopewell JW, and Morris AD

Subjects

Animals, Cell Survival drug effects, Cerebral Ventricles, Male, Mitotic Index drug effects, Rats, Rats, Sprague-Dawley, Stem Cells drug effects, Time Factors, Methotrexate toxicity, Misonidazole toxicity, Neuroglia drug effects

Abstract

The cytotoxic effects of the drugs methotrexate (MTX) and misonidazole have been assessed in the rat brain by quantifying changes in the constituent cell populations of a glial cell progenitor layer, the subependymal plate (SEP). Three distinct cell types can be identified in the SEP on the basis of their nuclear morphology: cells with small dark (SD), small light (SL) or large light (LL) nuclei. The cells with SD nuclei may present pluripotential glial cell precursors. A reduction in the total nuclear density of the SEP, after the local ventricular administration of MTX, could be accounted for largely by a loss of cells with SD nuclei; to approximately 45% of control values 2 days after MTX followed by a full recovery in numbers by day 5. A further decline in the number of cells with SD nuclei occurred at 12 weeks after MTX administration. The pattern of changes in the cellularity of the SEP, after misonidazole administration, were similar to those observed after MTX treatment, although the magnitude of the response was reduced. It was concluded that both drugs, but MTX in particular, could have a potential additive effect on glial progenitor cells when used in combination with other forms of cancer therapy including radiation.

Published

1995

8. The influence of methotrexate on radiation-induced damage to different lengths of the rat spinal cord.

Author

Morris GM, Hopewell JW, and Morris AD

Subjects

Animals, Dose-Response Relationship, Drug, Female, Rats, Rats, Inbred Strains, Methotrexate adverse effects, Paralysis chemically induced, Radiation Injuries, Experimental chemically induced, Spinal Cord radiation effects

Abstract

An experimental model in the rat has been used to assess the possible enhancement of damage to the spinal cord when radiation is given in the presence of methotrexate (MTX). The dose of MTX used, 4 mg/kg, was the maximum dose that could be given to the rat, when administered into the cerebral spinal fluid circulation, without risk of serious neurological effects. Lengths of 4, 8 and 16 mm of the cervical spine were irradiated with single doses of X rays. For animals that developed paralysis within 30 weeks, caused predominantly by the presence of white matter necrosis, there was no evidence to indicate that MTX enhanced the radiation response of the rat spinal cord, at least at a more clinically relevant level of effect i.e. a low incidence of paralysis. However, for the doses associated with the 50% level of effect (ED50) to an 8 mm long field a significant (p less than 0.005) enhancement of the response was seen, suggesting a dose modification factor of 1.19 +/- 0.07. This was interpreted in terms of an hypothesis to explain the well documented volume effect for very small fields in the rat spinal cord which is based on the migration of viable cells in the periphery of the irradiated site. The apparent smaller effect seen when only 4 mm of the spine was irradiated might be related to the nature of the lesion induced at doses required to produce paralysis in these small fields; the lesions were not restricted to white matter but were more severe and also involved the grey matter and nerve roots after a slightly shorter latent period.

Published

1992

9. Cell kinetic changes in the follicular epithelium of pig skin after irradiation with single and fractionated doses of X rays.

Author

Morris GM and Hopewell JW

Subjects

Animals, Basement Membrane cytology, Basement Membrane radiation effects, Cell Division radiation effects, Dose-Response Relationship, Radiation, Female, Hair cytology, Swine, Hair radiation effects

Abstract

Changes in the cell kinetics of the follicular epithelium of the pig have been studied after irradiation with single and fractionated doses (30 fractions/39 days) of X rays and the results compared with previously published data for the epidermis. In the follicular epithelium there was an initial degenerative phase, during which the rate of cell depletion was independent of the radiation dose and the mode of administration. Evidence for repopulation was seen between the 14th and 18th days after single doses (15 or 20 Gy) and by the 28th day after the start of irradiation with fractionated doses (52.3-80.0 Gy). However, the degree of cell depletion and the subsequent rate of repopulation were independent of dose. The regenerative phase was characterized by an increased cell proliferation as indicated by an elevation of the labelling index. Islands of cells (colonies), with an appearance similar to cells in the normal follicular epithelium, were seen 18 days after a single dose of 20 Gy and 42 days after the start of fractionated irradiation. When compared with the epidermis, the follicular epithelium exhibited considerably less evidence of damage after both single and fractionated doses of X rays. There was a lower incidence of degenerate cells and reduced levels of cell depletion in the follicular epithelium, suggesting that cells from this region play an important role in the repopulation of the epidermis after high-dose irradiation.

Published

1989

10. Changes in the cell kinetics of pig epidermis after single doses of X rays.

Author

Morris GM and Hopewell JW

Subjects

Animals, Cell Count radiation effects, Cell Cycle radiation effects, Cell Division radiation effects, Cell Survival radiation effects, Dose-Response Relationship, Radiation, Epidermal Cells, Swine, Epidermis radiation effects

Abstract

Changes in the cell kinetics of pig epidermis have been investigated after irradiation with single doses of 15 Gy and 20 Gy of X rays. The epidermis exhibited an initial degenerative phase when the rate of cell depletion was independent of radiation dose. Changes consistent with repopulation were evident between the 14th and 18th day after irradiation. The severity of cell depletion and the rate of recovery of the epidermis were dose dependent. The regenerative phase was characterized by an increased cell proliferation; values for the labelling index (LI) were greater than those in the non-irradiated epidermis, from 14 days after 15 Gy and from 18 days after 20 Gy. The LI was still elevated at the end of the observation period, i.e. Day 56. No change in the time for DNA synthesis was found. Eighteen days after 15 Gy and 22 days after 20 Gy, islands of cells (colonies), with an appearance similar to the cells in the normal epidermis, were seen. The minimum turnover time (TT) for the proliferating cells of the basal layer of the epidermis in radiation-damaged skin was 61-68 h as compared with 125 h in unirradiated skin. For the basal cells in the colonies, TT was 16-22 h.

Published

1988