Literature DB >> 17059891

Automated human blood micronucleated reticulocyte measurements for rapid assessment of chromosomal damage.

Stephen D Dertinger1, Richard K Miller, Kelly Brewer, Therese Smudzin, Dorothea K Torous, Daniel J Roberts, Svetlana L Avlasevich, Steven M Bryce, Siva Sugunan, Yuhchyau Chen.   

Abstract

This study evaluated the utility of human blood micronucleated reticulocyte (MNCD71+) frequency measurement as a cytogenetic damage biomarker. The analytical methodology was flow cytometry in conjunction with a previously described three color fluorescence labeling technique that includes anti-CD71 to focus analyses on the most immature fraction of reticulocytes [S.D. Dertinger, K. Camphausen, J.T. MacGregor, M.E. Bishop, D.K. Torous, S. Avlasevich, et al., Three-color labeling method for flow cytometric measurement of cytogenetic damage in rodent and human blood, Environ. Mol. Mutagen. 44 (2004) 427-435]. Blood specimens from 50 self-reported healthy adult volunteers were studied. In addition to MNCD71+ measurements, blood plasma folate and B12 levels were assessed, since these variables tend to influence other indices of cytogenetic damage. Time-course data are also provided for 10 cancer patients undergoing treatment. For these subjects, frequency of MNCD71+ was measured immediately before therapy, and daily during the first week of chemotherapy and/or fractionated radiotherapy. For the group of healthy volunteers, the variables of age, and folate and B12 levels demonstrated no significant effect on MNCD71+ frequency. In addition, no difference was observed between pre-treatment MNCD71+ values for cancer patients compared with healthy volunteers. Regarding chemotherapy and/or partial body radiotherapy, elevated frequencies were observed upon initiation of treatment for 9 of the 10 patients studied. Maximal effects were observed 3-5 days following initiation of therapy. The largest increases in frequency of MNCD71+ (up to 25.9-fold) were observed in those patients exposed to anti-neoplastic drugs, presumably due to the systemic red marrow exposure provided by these agents. Taken together, these data support the hypothesis that the MNCD71+ endpoint represents a valuable biomarker of cytogenetic damage that does not require cell culture or microscopy-based scoring.

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Year:  2006        PMID: 17059891      PMCID: PMC1796663          DOI: 10.1016/j.mrgentox.2006.09.003

Source DB:  PubMed          Journal:  Mutat Res        ISSN: 0027-5107            Impact factor:   2.433


  43 in total

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Authors:  Stephen D Dertinger; Dorothea K Torous; Nikki E Hall; Francis G Murante; Sarah E Gleason; Richard K Miller; Carol R Tometsko
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9.  Comparative scoring of micronucleated reticulocytes in rat peripheral blood by flow cytometry and microscopy.

Authors:  Dorothea K Torous; Nikki E Hall; Francis G Murante; Sarah E Gleason; Carol R Tometsko; Stephen D Dertinger
Journal:  Toxicol Sci       Date:  2003-05-28       Impact factor: 4.849

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3.  Assessment of genotoxicity associated with hydroxyurea therapy in children with sickle cell anemia.

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4.  Dose-response assessment of four genotoxic chemicals in a combined mouse and rat micronucleus (MN) and Comet assay protocol.

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7.  Elevated frequencies of micronucleated erythrocytes in infants exposed to zidovudine in utero and postpartum to prevent mother-to-child transmission of HIV.

Authors:  Kristine L Witt; Coleen K Cunningham; Kristine B Patterson; Grace E Kissling; Stephen D Dertinger; Elizabeth Livingston; Jack B Bishop
Journal:  Environ Mol Mutagen       Date:  2007 Apr-May       Impact factor: 3.216

Review 8.  Molecular markers of radiation-related normal tissue toxicity.

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