Fumio Sagami scite author profile

Fumio Sagami

5Publications

123Citation Statements Received

78Citation Statements Given

How they've been cited

223

120

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Affiliations

Eisai (Japan), Japan Medical Association, Chiba University

Publications

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In vivo genotoxicity and DNA adduct levels in the liver of rats treated with safrole

Daimon

Shibata²,

Asakura³

et al. 1998

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The induction of chromosome aberrations, sister chromatid exchanges (SCEs), and the formation of DNA adducts was studied in hepatocytes of F344 rats exposed in vivo to safrole. Hepatocytes were isolated 24 h after a single dose of safrole or five repeated doses (once a day) by gastric intubation and allowed to proliferate in Williams' medium E supplemented with epidermal growth factor. Cells were fixed after 48 h in culture. Safrole-DNA adducts were detected by a nuclease P1-enhanced 32P-post-labeling assay in isolated hepatocytes from the rats. While a single dose was not sufficient to induce detectable levels of chromosome aberrations at the time of assay, five repeated doses induced these changes with a maximum frequency of 13.4%, compared with the control value of 1.8%. Both a single dose and five repeated doses induced significant SCEs, to a maximum frequency of 0.81 SCEs per chromosome, while the control value was 0.59 SCEs per chromosome. Two major and two minor DNA adducts were detected after treatment with either a single dose or five repeated doses. The maximum amount of total DNA adducts was 89.8 DNA adducts/10(7) nucleotides. These results show that safrole is a genotoxic carcinogen in the rat liver in vivo and suggest that the cytogenetic effects of this compound may result from covalent DNA modification in the rat liver. This in vivo cytogenetic assay should provide a useful means of evaluation of the genotoxicity of hepatocarcinogens.

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Comparison of the mutational spectra of the lacZ transgene in four organs of the Muta™Mouse treated with benzo[a]pyrene: target organ specificity

Hakura

Tsutsui

Sonoda

et al. 2000

Mutation Research/Fundamental and Molecular Mechanisms of Mutag

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Reproductive and Developmental Toxicity Study of Gadobenate Dimeglumine Formulation (E7155) (3) : Study of Embryo-Fetal Toxicity in Rabbits by Intravenous Administration

Okuda¹,

Sagami²,

Tirone³

et al. 1999

J. Toxicol. Sci.

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Collaborative work on evaluation of ovarian toxicity by repeated-dose and fertility studies in female rats

Sanbuissho

Yoshida²,

Hisada

et al. 2009

J. Toxicol. Sci.

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-The National Institute of Health Sciences (NIHS) and 18 pharmaceutical companies of the Japan Pharmaceutical Manufacturers Association (JPMA) have conducted a validation study intended to evaluate whether a 2-week repeated general toxicity period with histopathological examination is -ing that it is adequate. Evaluation of ovarian toxicity by comprehensive histopathological examination of the female reproductive organs based on the underlying morphology of a normal cycle of the reproductive tract including the ovary and additional immunohistochemical staining with proliferative cell nuclear antigen (PCNA) to identify small follicles may be a good tool to assess female reproductive function. In the collaborative study, 2-or 4-week repeated dose toxicity studies with ovarian histopathological examinations were conducted. A female fertility study was also conducted to compare the results with those of hormone analogues, primordial follicle damaging agents, metabolite imbalance inducers, and endocrine imbalance inducers. Based on the results, ovarian toxicity could be detected by a careful histopatholgi--female fertility parameters (irregular estrous cycle, pre-implantation loss).

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Inhibition of sulfotransferase affecting in vivo genotoxicity and DNA adducts induced by safrole in rat liver

Daimon

Shibata

Asakura

et al. 1997

Teratog. Carcinog. Mutagen.

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The effect of pretreatment with pentachlorophenol (PCP), a known inhibitor of sulfotransferases, on the induction of chromosomal aberrations, sister chromatid exchanges (SCEs), replicative DNA synthesis (RDS), and the formation of DNA adducts was studied in the liver of rats treated with safrole (1‐allyl‐3,4‐methylenedioxybenzene). Rats were given a single oral dose (1,000 mg/kg body weight) or 5 repeated doses (500 mg/kg body weight) of safrole, with or without intraperitoneal pretreatment with PCP (10 mg/kg body weight). Hepatocytes were isolated 24 hr after administration of safrole and allowed to proliferate in Williams' medium E supplemented with epidermal growth factor to test for chromosomal aberrations and SCEs. For examination of RDS, hepatocytes were incubated in Williams' medium E containing 5‐bromo‐2′‐deoxyuridine. Safrole‐DNA adducts were detected by a nuclease P1‐enhanced 32P‐postlabeling assay. A single dose of safrole induced significant SCEs and RDS, while chromosomal aberrations were induced by 5 repeated doses. Two major and 2 minor DNA adducts were detected by both a single dose and 5 repeated doses. PCP significantly decreased safrole‐induced cytogenetic effects and RDS, and caused a decrease in DNA adducts formed by safrole. These results suggest that safrole is capable of inducing SCEs, chromosomal aberrations, and RDS in the rat liver in vivo and that these effects may be induced by the sulfuric acid ester metabolite that can bind DNA. Teratogenesis Carcinog. Mutagen. 17:327–337, 1997/98. © 1998 Wiley‐Liss, Inc.

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Fumio Sagami

In vivo genotoxicity and DNA adduct levels in the liver of rats treated with safrole

Comparison of the mutational spectra of the lacZ transgene in four organs of the Muta™Mouse treated with benzo[a]pyrene: target organ specificity

Reproductive and Developmental Toxicity Study of Gadobenate Dimeglumine Formulation (E7155) (3) : Study of Embryo-Fetal Toxicity in Rabbits by Intravenous Administration

Collaborative work on evaluation of ovarian toxicity by repeated-dose and fertility studies in female rats

Inhibition of sulfotransferase affecting in vivo genotoxicity and DNA adducts induced by safrole in rat liver

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