Long duration mild temperature hyperthermia and brachytherapy

Armour, Elwood P.; Raaphorst, G. P.

doi:10.1080/02656730310001609335

Cited by 19 publications

(18 citation statements)

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“…16 However, both in vitro and in vivo, when combined simultaneously with LDR irradiation, MTH had been reported to inhibit effi ciently cell recovery caused by the decrease in the irradiation dose rate. 5 In the current study, the usefulness of MTH as a manipulation for suppressing PLDR and sublethal damage repair (SLDR) in both total and Q tumor cell populations was evaluated by applying MTH right after HDR irradiation and during LDR irradiation using γ-ray radiation, respectively, in terms of the responses of the total and Q-cell populations in solid tumors using our unique method for selectively detecting the response of Q-cell populations in vivo. 10 Two major pathways for the repair of potentially lethal DNA double-stranded breaks (dsbs) exist in mammalian cells.…”

Section: Discussionmentioning

confidence: 99%

“…3 Meanwhile, the effects of mild temperature hyperthermia (MTH) (39°-42°C for 1-2 h) on tissues are subtle and have been largely ignored until recently. However, the subtle effects of MTH, including heat-mediated tumor reoxygenation 4 and inhibition of sublethal and potentially lethal damage repair, 5 provide a strong rationale for using MTH in combination with radiotherapy.…”

Section: Introductionmentioning

confidence: 99%

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Inhibition of repair of radiation-induced damage by mild temperature hyperthermia, referring to the effect on quiescent cell populations

et al. 2007

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Inhibition of repair of radiation-induced damage by mild temperature hyperthermia, referring to the effect on quiescent cell populations

et al. 2007

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“…Desde el punto de visto radio-biológico, la aplicación simultánea de calor y radiación es considerada ideal para la termorradioterapia 29 . En concreto, el concepto de combinar la hipertermia suave con la radiación LDR ha sido propuesto de manera prometedora, pero, que nosotros sepamos nunca se ha llevado a cabo clínicamente 30 . Con este fin, hemos comenzado en nuestra institución un estudio de Fase II en pacientes con cán-cer de próstata clínicamente localizado y con criterio de riesgo intermedio (PSA 10-20ng/ml o suma de Gleason 7), que no habían sido tratados previamente.…”

Section: Discusión Y Perspectivas Futurasunclassified

Termoterapia en cáncer de próstata mediante el uso de nanopartículas magnéticas

Johannsen

Gneveckow²,

Taymoorian

et al. 2007

Actas Urol Esp

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En recientes ensayos clínicos, se ha evaluado en tumores malignos humanos, un nuevo método de dispensación de calor en pequeños espacios (intersticios) utilizando nanopartículas magnéticas y una técnica de inyección directa. En el cáncer de próstata, este procedimiento se ha investigado en dos estudios fase I separados empleando en uno solamente termoterapia de nanopartículas magnéticas y en otro en combinación con braquiterapia (implantes permanentes). En ambos estudios se demostró viabilidad y buena tolerancia, usando el primer prototipo de un aplicador de campo magnético. Como con cualquier otra técnica por calor, este nuevo procedimiento requiere herramientas específicas para su planificación, control de calidad y monitorización térmica, basado en una imagen apropiada y en técnicas de planificación. En estos primeros estudios, se evalúa un nuevo método que permite una planificación y distribución tridimensional no invasiva de la temperatura basado en la tomografía computerizada (TC). En la actualidad, los factores limitantes de este procedimiento son el malestar del paciente a altas intensidades de campos magnéticos y la distribución intratumoral subóptima de las nanopartículas. Hasta que estas limitaciones sean superadas y la termoablación pueda ser aplicada con seguridad como monoterapia, esta modalidad de tratamiento está siendo evaluada en combinación con la irradiación en pacientes con cáncer de próstata localizado.Palabras clave: Termoterapia. Cáncer de próstata. Nanopartículas magnéticas. ABSTRACT THERMAL THERAPY OF PROSTATE CANCER USING MAGNETIC NANOPARTICLESA novel method of interstitial heating using magnetic nanoparticles and a direct injection technique has been evaluated in human cancers in recent clinical trials. In prostate cancer, this approach was investigated in two separate phase-I-studies, employing magnetic nanoparticle thermotherapy alone and in combination with permanent seed brachytherapy. The feasibility and good tolerability was shown in both trials, using the first prototype of a magnetic field applicator. As with any other heating technique, this novel approach requires specific tools for planning, quality control and thermal monitoring, based on appropriate imaging and modelling techniques. In these first clinical trials, a newly developed method for planning and non-invasive calculations of the 3-dimensional temperature distribution based on computed tomography could be validated. Limiting factors of this approach at present are patient discomfort at high magnetic field strengths and suboptimal intratumoral distribution of nanoparticles. Until these limitations will be overcome and thermal ablation can safely be applied as a monotherapy, this treatment modality is being evaluated in combination with irradiation in patients with localized prostate cancer.

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“…Scc Vii squamous cell carcinomas (department of radiotherapy, Kyoto university) derived from c3h/he mice were maintained in vitro in eagle's minimum essential medium supplemented with 12.5% fetal bovine serum. the cells (1.0x10 5 ) were inoculated subcutaneously into the left hind legs of 8-to 11-week-old syngeneic female c3h/he mice (Japan animal co., ltd., osaka, Japan). after 14 days, tumors with a diameter of ~1 cm were selected for use in the experiments.…”

Section: Methodsmentioning

confidence: 99%

“…meanwhile, until recently the effects of mild temperature hyperthermia (MTH) (39-42˚C for 1-2 h) on tissue have largely been ignored. however, mth has subtle effects, including heat-mediated tumor reoxygenation (4) and the inhibition of sublethal and potentially lethal damage repair (5), which provide a very strong rationale for using mth in combination with radiotherapy. in addition, the physiological and cellular effects of mth can improve the delivery of drug vehicles (6), activate promoters for heat-mediated gene therapy (7) and increase immune response to tumors through a variety of mechanisms (8).…”

Section: Introductionmentioning

confidence: 99%

Adverse effect of mild temperature hyperthermia combined with hexamethylenetetramine compared to its effect combined with tirapazamine in the treatment of solid tumors

Masunaga¹

2009

Exp Ther Med

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Abstract. this study aimed to assess the effect on solid tumors of mild temperature hyperthermia (mth) combined with hexamethylenetetramine (hmta) or tirapazamine (tpZ). Squamous cell carcinoma (Scc Vii) tumor-bearing mice were continuously administered 5-bromo-2'-deoxyuridine (Brdu) to label intratumor proliferating (p) cells. mice received hmta or tpZ through intraperitoneal single or subcutaneous continuous administration, with or without MTH (40˚C, 60 min), followed or not by γ-ray irradiation or cisplatin treatment. after hmta or tpZ administration without γ-ray irradiation or cisplatin treatment, immediately after γ-ray irradiation, or 1 h after cisplatin treatment, the response of quiescent (Q) cells was assessed in terms of micronucleus frequency using immunofluorescence staining for Brdu. the response of the total (p + Q) tumor cells was determined based on a comparison with non-Brdu-treated tumors. Without mth, hmta and tpZ had a nearly equal radiosensitizing and cisplatin sensitivity-enhancing effect on both total and Q cells. With mth, radio-and cisplatin-sensitizing effects by hmta were reduced, particularly in the Q cells. in contrast, the enhancing effects of tpZ were increased, particularly in the Q cells. continuous administration of hmta and tpZ resulted in higher radio-and cisplatin-sensitizing effects than intraperitoneal single administration. in terms of tumor cytotoxicity as a whole, including Q cells, the administration of γ-ray irradiation or cisplatin treatment combined with continuous hmta administration is promising, taking into account the clinical use of hmta. however, mth should not be combined with hmta administration. Introductionhyperthermia is a heat treatment that directly targets cancer cells or the environment surrounding them (1). according to the tenets of hyperthermic oncology, significant tumor cell killing could theoretically be achieved if cells or tissues were heated to over 42˚C for 1 h or more (2). It is speculated that such heat treatment would induce radio-and chemosensitization, in part by inhibiting dna damage repair (1). however, clinical experience over the past 25 years has shown that it is not possible to routinely achieve thermal doses of over 42˚C for 1 h or more. it is now known that, during typical hyperthermia treatments with currently available heating technologies (except for thermal ablation), cytotoxic temperatures are only achieved in small sub-volumes of tumors (3). meanwhile, until recently the effects of mild temperature hyperthermia (MTH) (39-42˚C for 1-2 h) on tissue have largely been ignored. however, mth has subtle effects, including heat-mediated tumor reoxygenation (4) and the inhibition of sublethal and potentially lethal damage repair (5), which provide a very strong rationale for using mth in combination with radiotherapy. in addition, the physiological and cellular effects of mth can improve the delivery of drug vehicles (6), activate promoters for heat-mediated gene therapy (7) and increase immune response to tumors through a variety ...

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Long duration mild temperature hyperthermia and brachytherapy

Cited by 19 publications

References 65 publications

Inhibition of repair of radiation-induced damage by mild temperature hyperthermia, referring to the effect on quiescent cell populations

Inhibition of repair of radiation-induced damage by mild temperature hyperthermia, referring to the effect on quiescent cell populations

Termoterapia en cáncer de próstata mediante el uso de nanopartículas magnéticas

Adverse effect of mild temperature hyperthermia combined with hexamethylenetetramine compared to its effect combined with tirapazamine in the treatment of solid tumors

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