Photomutagenesis by chlorinated phenothiazine tranquilizers.

Jose, Jule Griebrok

doi:10.1073/pnas.76.1.469

Cited by 67 publications

(16 citation statements)

References 23 publications

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“…The lack of genotoxicity of CPZ alone is consistent with a previous study that showed CPZ to be strongly positive for mitotic recombination in strain D7 under conditions of photomutagenicity, but not under conventional assay conditions in the dark [Gocke, 1996]. Despite its capacity to intercalate, CPZ without photoactivation gave negative results in bacterial assays for frameshift mutations [Jose, 1979;Mortelmans et al, 1986;Gocke, 1996].…”

Section: Discussionsupporting

confidence: 91%

Potentiation of the mutagenicity and recombinagenicity of bleomycin in yeast by unconventional intercalating agents

Hoffmann

Laterza

Sylvia

et al. 2011

Environ and Mol Mutagen

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Interactions between bleomycin (BLM) and conventional or unconventional intercalating agents were analyzed in an assay for mitotic gene conversion at the trp5 locus and reversion of the ilv1-92 allele in Saccharomyces cerevisiae strain D7. BLM is a potent recombinagen and mutagen in the assay. Various chemicals modulate the genetic activity of BLM, producing either antimutagenic effects or enhanced genotoxicity. Effects of cationic amino compounds include enhancement of BLM activity by aminoacridines and protection against BLM by aliphatic amines. The potentiation of BLM is similar to findings in a micronucleus-based BLM amplification assay in Chinese hamster V79 cells. In this study, the amplification of BLM activity was explored in yeast using known intercalators, compounds structurally related to known intercalators, and unconventional intercalators that were identified on the basis of computer modeling or results in the Chinese hamster BLM amplification assay. As shown in previous studies, the classical intercalator 9-aminoacridine (9AA) caused dose-dependent enhancement of BLM activity. Other compounds found to enhance the induction of mitotic recombination and point mutations in strain D7 were chlorpromazine, chloroquine, mefloquine, tamoxifen, diphenhydramine, benzophenone, and 3-hydroxybenzophenone. The increased activity was detectable by cotreatment of yeast with BLM and the modulator compound in growth medium or by separate interaction of the intercalator with DNA followed by BLM treatment of nongrowing cells in buffer. The data support the interpretation drawn from micronucleus assays in mammalian cells that BLM enhancement results from DNA intercalation and may be useful in detecting noncovalent interactions with DNA. Environ.

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Section: Discussionsupporting

confidence: 91%

Potentiation of the mutagenicity and recombinagenicity of bleomycin in yeast by unconventional intercalating agents

Hoffmann

Laterza

Sylvia

et al. 2011

Environ and Mol Mutagen

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“…Nishio, Y., T. Kakizoe, M. Ohtani, S. Sato, T. Sugimura and S. (1)(2)(3)(4)(5)(6)(7). Although many phototoxic compounds are photomutagenic, others, such as retinoids and nitro-benzodiazepines are not photomutagenic (8,9).…”

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confidence: 99%

Interrelationship of Photocarcinogenicity, Photomutagenicity and Phototoxicity

Loveday¹

1996

Photochem & Photobiology

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“…The results of this study suggest for the first time that drugs with weak photosensitivity when administered long-term also are carcinogenic. The enhanced tumour development in the case of CPZ seems likely to have stemmed from that drug's phototoxicity since the drug has no known immunosuppressive or mutagenic properties although in vitro it is photomutagenic when activated by UVR (Jose, 1979). In this study, combined CPZ-UVR therapy compared to UVR alone reduced the latent period of appearance of premalignant skin lesions (papillomas and keratoacanthomas) and increased the rate of conversion of premalignant to malignant lesions.…”

Section: Discl'ssionmentioning

confidence: 67%

Enhancement of Uv‐induced Skin Carcinogenesis by Azathioprine: Role of Photochemical Sensitisation

Kelly¹,

Meikle²,

Moore³

1989

Photochem & Photobiology

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The phototoxicity of various drugs (chlorpromazine (CPZ), metronidazole (MET), 8‐methoxypsoralen (8‐MOP), azathioprine (AZA) and the azathioprine metabolites, 6‐mercaptopurine (6‐MP), methylnitrothio‐imidazole (MNTI), methylnitroimidazole (MNI)) was determined in hairless (Skh‐hrl) mice exposed to a light source with broad emission (290–700 nm). Chlorpromazine, MET, 8‐MOP, AZA, MNI and 6‐MP were phototoxic, as determined by the oedematous response of skin, at doses comparable to those used clinically. The effects of long‐term drug therapy and UV radiation on skin carcinogenesis were then determined. Chlorpromazine and MET, and to a lesser extent AZA, MNTI and 6‐MP, enhanced photocarcinogen‐esis. In each case, both the tumour yield and the proportion of malignant:benign skin tumours were increased. The results of this study imply that prolonged treatment of mice with low‐level phototoxins predisposes to photocarcinogenesis.

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Photomutagenesis by chlorinated phenothiazine tranquilizers.

Cited by 67 publications

References 23 publications

Potentiation of the mutagenicity and recombinagenicity of bleomycin in yeast by unconventional intercalating agents

Potentiation of the mutagenicity and recombinagenicity of bleomycin in yeast by unconventional intercalating agents

Interrelationship of Photocarcinogenicity, Photomutagenicity and Phototoxicity

Enhancement of Uv‐induced Skin Carcinogenesis by Azathioprine: Role of Photochemical Sensitisation

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