Tumor Induction and Life Shortening in BC3F 1 Female Mice at Low Doses of Fast Neutrons and X Rays

Covelli, Vincenzo; Coppola, M.; Majo, V. Di; Rebessi, Simonetta; Bassani, B.

doi:10.2307/3577210

Cited by 43 publications

(13 citation statements)

References 15 publications

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“…The high incidence of liver and lung tumours influenced the life shortening of the neutron-exposed animals. These data were consistent with a previous report (Covelli et al 1988), in which the decrease of latency for the elicitation of solid tumours increased with dose. In case of the A-bomb survivors in Hiroshima, the estimated excess relative risk at 1 Sv for the cancer of ovary was highest at an exposed age of 0-9 years followed by over 40 years (Thompson 1994).…”

Section: Discussionsupporting

confidence: 94%

“…The relative biological effectiveness (RBE) for different radiations on oocyte killing (Straume et al 1987, Satow et al 1989 does not explain directly the efficiency of the development of ovarian stromal cell tumours (Ullrich et al 1977). The relationship between the ovarian tumour spectrum and radiation quality with regard to the age at exposure has not been described to date, although a low incidence of granulosa cell tumours following high linear energy transfer (LET)-radiation exposure at 4-6 weeks of age was reported (Covelli et al 1988). …”

Section: Introductionmentioning

confidence: 96%

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Relationship between oocyte apoptosis and ovarian tumours induced by high and low LET radiations in mice

Nitta

Hoshi

2003

International Journal of Radiation Biology

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Section: Discussionsupporting

confidence: 94%

Section: Introductionmentioning

confidence: 96%

Relationship between oocyte apoptosis and ovarian tumours induced by high and low LET radiations in mice

Nitta

Hoshi

2003

International Journal of Radiation Biology

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“…Models for experimental tumor induction by ionizing radiation are not entirely satisfactory because of their long duration, while often only a moderate rate of tumor development is achieved (Broerse et al, 1985;Coggle, 1988;Covelli et al, 1988;Fry, 1981;Mole, 1984;Twentyman et al, 1980;Ullrich, 1983). Little work has been directed towards the question of how radioproteetive agents influence radiation carcinogenesis in vivo.…”

mentioning

confidence: 99%

Radiation‐induced lymphoid tumors and radiation lethality are inhibited by combined treatment with small doses of zinc aspartate and wr 2721

Floersheim

Christ

Koenig

et al. 1992

Intl Journal of Cancer

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Combined small doses of zinc aspartate and WR 2721 provided additive protection against radiation lethality in mice. Survival obtained with a small dose of WR 2721 which was ineffective alone could be enhanced to 83% by combining the drug with zinc aspartate, which on its own also displayed no effect. The survival of 25% provided by a higher dose of WR 2721 was increased significantly by adding zinc aspartate. Additivity was also tested in a model of radiation carcinogenesis. For this purpose, lethality and occurrence of lymphoid tumors induced by fractionated total-body irradiation were studied in C57B1/6 mice treated with zinc aspartate and WR 2721. In order to reveal additive effects, both agents were used at sub-optimal dosages. In mice subjected to 5 daily exposures of 1.9 Gy, the combination of zinc aspartate and WR 2721 was effective and enhanced the survival to 83% as compared with 25% afforded by WR 2721 alone (p < 0.005). Similarly, histological assessment of organ involvement with lymphoma revealed that zinc aspartate and WR 2721 alone did not bring about a significant reduction of lymphoma incidence. On the other hand, the combined agents diminished organ involvement with lymphoma to 9.1% as against 90% in the controls (p < 0.0005) and 62.5% with WR 2721 alone (p < 0.025). Thus, combined treatment with zinc aspartate and WR 2721 also inhibited radiation-induced lymphoid tumors.

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“…However , as previously observed for X rays, a threshold-model cannot be excluded to describe the dose-response relationship for neutrons. In fact, a linear relationship fits well the data (P=0.58) with a threshold-dose of 6 cGy (Covelli, et al 1988)').…”

Section: Myeloid Leukemiamentioning

confidence: 57%

The Dose-response Relationships for Tumor Induction after High-LET Radiation.

Covelli

Coppola

Majo³

et al. 1991

JRR

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Dose-response relationship/Neutron/Malignant Lymphoma/Myeloid Leukemia/Liver Tumor/Ovarian Tumor This paper presents a review of several studies conducted in our laboratory to examine the carcinogenic effects in mice of high-LET radiation and, for comparison, of low-LET reference radiation. For some specific end-points the following conclusions can be formulated: i) the dose-response curves for myeloid leukemia and malignant lymphoma can be interpreted in terms of induction and inactivation; in particular, the data confirmed that a linear dependence of the induction on dose is adequate to describe the response to fission neutrons, while a pure quadratic dependence is consistent with the experimental data for low-LET radiation; ii) in the liver, a marked age-dependence was demonstrated for radiation-induced tumors with a much higher susceptibility in young than in old mice; also for these tumors the dose-effect curves can be described by a linear and a quadratic relationships for high and low-LET radiation, respectively; iii) data on ovarian tumor induction suggested threshold-like dose responses: these peculiar shapes as well as the absence of a clear radiation quality dependence of the curves are difficult findings to explain using a simple model of radiation action, and they might better be related to a non-stochastic effect of hormonal imbalance following irradiation.

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Tumor Induction and Life Shortening in BC3F 1 Female Mice at Low Doses of Fast Neutrons and X Rays

Cited by 43 publications

References 15 publications

Relationship between oocyte apoptosis and ovarian tumours induced by high and low LET radiations in mice

Relationship between oocyte apoptosis and ovarian tumours induced by high and low LET radiations in mice

Radiation‐induced lymphoid tumors and radiation lethality are inhibited by combined treatment with small doses of zinc aspartate and wr 2721

The Dose-response Relationships for Tumor Induction after High-LET Radiation.

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