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      Toxicity determined in vitro by morphological alterations and neutral red absorption

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      Toxicology Letters
      Elsevier BV

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          The pharmacological relevance of vital staining with neutral red.

          The uptake of neutral red into the renin-containing juxtaglomerular granules does not inhibit the release of renin either in basal or in stimulated states of renin secretion. The vasodilating effect of neutral red may be due to a nonspecific binding to noradrenaline-receptors in the vascular smooth muscle cells.
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            In vitro cytotoxicity assays. Potential alternatives to the Draize ocular allergy test.

            A short-term cytotoxicity assay carried out in multiwell test plates and a supplementary colony forming assay are both useful for screening and range finding of toxic concentrations of test agents. The highest tolerated dose (HTD), a concentration at which only minimal morphological changes were observed, was designated as endpoint in the assay. Epithelial rabbit cornea cells, murine fibroblasts, Chinese hamster lung cells, human hepatoma cells and mouse macrophage cultures were used as targets. Several of the alcohols tested at HTD in the colony forming assay were found to inhibit colony formation. An ID50 of colony formation was used as a quantitative corroborating test. The ranking of 34 toxicants was found to be virtually the same with all cell types examined. This easily reproducible, rapid in vitro test is cost-effective and can be used for preliminary large scale screening of potential toxicants.
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              Uridine uptake inhibition as a cytotoxicity test: Correlations with the Draize test

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                Author and article information

                Journal
                Toxicology Letters
                Toxicology Letters
                Elsevier BV
                03784274
                February 1985
                February 1985
                : 24
                : 2-3
                : 119-124
                Article
                10.1016/0378-4274(85)90046-3
                3983963
                ab925e7d-2b08-40aa-ba13-c74c82bd5491
                © 1985

                http://www.elsevier.com/tdm/userlicense/1.0/

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