Confirmation of Pig-a mutation in flow cytometry-identified CD48-deficient T-lymphocytes from F344 rats

The Pig-a assay is used for monitoring somatic cell mutation in laboratory animals and humans. The assay detects haematopoietic cells deficient in glycosylphosphatidylinositol (GPI)-anchored protein surface markers using flow cytometry. However, given that synthesis of the protein markers (and the e...

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Published in	Mutagenesis Vol. 30; no. 3; pp. 315 - 324
Main Authors	Revollo, Javier, Pearce, Mason G., Petibone, Dayton M., Mittelstaedt, Roberta A., Dobrovolsky, Vasily N.
Format	Journal Article
Language	English
Published	England 01.05.2015
Subjects	Animals Antigens, CD - genetics Antigens, CD - metabolism Base Sequence CD48 Antigen Cells, Cultured DNA Mutational Analysis Ethylnitrosourea - pharmacology Flow Cytometry High-Throughput Nucleotide Sequencing Immunomagnetic Separation Male Membrane Proteins - genetics Mutagenesis Mutagenicity Tests Mutagens - pharmacology Mutation Phenotype Rats, Inbred F344 T-Lymphocytes - metabolism
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Abstract	The Pig-a assay is used for monitoring somatic cell mutation in laboratory animals and humans. The assay detects haematopoietic cells deficient in glycosylphosphatidylinositol (GPI)-anchored protein surface markers using flow cytometry. However, given that synthesis of the protein markers (and the expression of their genes) is independent of the expression of the X-linked Pig-a gene and the function of its enzyme product, the deficiency of markers at the surface of the cells may be caused by a number of events (e.g. by mutation or epigenetic silencing in the marker gene itself or in any of about two dozen autosomal genes involved in the synthesis of GPI). Here we provide direct evidence that the deficiency of the GPI-anchored surface marker CD48 in rat T-cells is accompanied by mutation in the endogenous X-linked Pig-a gene. We treated male F344 rats with N-ethyl-N-nitrosourea (ENU), and established colonies from flow cytometry-identified and sorted CD48-deficient spleen T-lymphocytes. Molecular analysis confirmed that the expanded sorted cells have mutations in the Pig-a gene. The spectrum of Pig-a mutation in our model was consistent with the spectrum of ENU-induced mutation determined in other in vivo models, mostly base-pair substitutions at A:T with the mutated T on the non-transcribed strand of Pig-a genomic DNA. We also used next generation sequencing to derive a similar mutational spectrum from a pool of 64 clones developed from flow-sorted CD48-deficient lymphocytes. Our findings confirm that Pig-a assays detect what they are designed to detect-gene mutation in the Pig-a gene.
AbstractList	The Pig-a assay is used for monitoring somatic cell mutation in laboratory animals and humans. The assay detects haematopoietic cells deficient in glycosylphosphatidylinositol (GPI)-anchored protein surface markers using flow cytometry. However, given that synthesis of the protein markers (and the expression of their genes) is independent of the expression of the X-linked Pig-a gene and the function of its enzyme product, the deficiency of markers at the surface of the cells may be caused by a number of events (e.g. by mutation or epigenetic silencing in the marker gene itself or in any of about two dozen autosomal genes involved in the synthesis of GPI). Here we provide direct evidence that the deficiency of the GPI-anchored surface marker CD48 in rat T-cells is accompanied by mutation in the endogenous X-linked Pig-a gene. We treated male F344 rats with N-ethyl-N-nitrosourea (ENU), and established colonies from flow cytometry-identified and sorted CD48-deficient spleen T-lymphocytes. Molecular analysis confirmed that the expanded sorted cells have mutations in the Pig-a gene. The spectrum of Pig-a mutation in our model was consistent with the spectrum of ENU-induced mutation determined in other in vivo models, mostly base-pair substitutions at A:T with the mutated T on the non-transcribed strand of Pig-a genomic DNA. We also used next generation sequencing to derive a similar mutational spectrum from a pool of 64 clones developed from flow-sorted CD48-deficient lymphocytes. Our findings confirm that Pig-a assays detect what they are designed to detect-gene mutation in the Pig-a gene. The Pig-a assay is used for monitoring somatic cell mutation in laboratory animals and humans. The assay detects haematopoietic cells deficient in glycosylphosphatidylinositol (GPI)-anchored protein surface markers using flow cytometry. However, given that synthesis of the protein markers (and the expression of their genes) is independent of the expression of the X-linked Pig-a gene and the function of its enzyme product, the deficiency of markers at the surface of the cells may be caused by a number of events (e.g. by mutation or epigenetic silencing in the marker gene itself or in any of about two dozen autosomal genes involved in the synthesis of GPI). Here we provide direct evidence that the deficiency of the GPI-anchored surface marker CD48 in rat T-cells is accompanied by mutation in the endogenous X-linked Pig-a gene. We treated male F344 rats with N-ethyl-N-nitrosourea (ENU), and established colonies from flow cytometry-identified and sorted CD48-deficient spleen T-lymphocytes. Molecular analysis confirmed that the expanded sorted cells have mutations in the Pig-a gene. The spectrum of Pig-a mutation in our model was consistent with the spectrum of ENU-induced mutation determined in other in vivo models, mostly base-pair substitutions at A:T with the mutated T on the non-transcribed strand of Pig-a genomic DNA. We also used next generation sequencing to derive a similar mutational spectrum from a pool of 64 clones developed from flow-sorted CD48-deficient lymphocytes. Our findings confirm that Pig-a assays detect what they are designed to detect-gene mutation in the Pig-a gene.The Pig-a assay is used for monitoring somatic cell mutation in laboratory animals and humans. The assay detects haematopoietic cells deficient in glycosylphosphatidylinositol (GPI)-anchored protein surface markers using flow cytometry. However, given that synthesis of the protein markers (and the expression of their genes) is independent of the expression of the X-linked Pig-a gene and the function of its enzyme product, the deficiency of markers at the surface of the cells may be caused by a number of events (e.g. by mutation or epigenetic silencing in the marker gene itself or in any of about two dozen autosomal genes involved in the synthesis of GPI). Here we provide direct evidence that the deficiency of the GPI-anchored surface marker CD48 in rat T-cells is accompanied by mutation in the endogenous X-linked Pig-a gene. We treated male F344 rats with N-ethyl-N-nitrosourea (ENU), and established colonies from flow cytometry-identified and sorted CD48-deficient spleen T-lymphocytes. Molecular analysis confirmed that the expanded sorted cells have mutations in the Pig-a gene. The spectrum of Pig-a mutation in our model was consistent with the spectrum of ENU-induced mutation determined in other in vivo models, mostly base-pair substitutions at A:T with the mutated T on the non-transcribed strand of Pig-a genomic DNA. We also used next generation sequencing to derive a similar mutational spectrum from a pool of 64 clones developed from flow-sorted CD48-deficient lymphocytes. Our findings confirm that Pig-a assays detect what they are designed to detect-gene mutation in the Pig-a gene.
Author	Dobrovolsky, Vasily N. Revollo, Javier Pearce, Mason G. Petibone, Dayton M. Mittelstaedt, Roberta A.
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References_xml	– volume: 52 start-page: 419 year: (2011) ident: key 20170517095528_CIT0010 article-title: Analysis of mutations in the Pig-a gene of spleen T-cells from N-ethyl-N-nitrosourea-treated fisher 344 rats publication-title: Environ. Mol. Mutagen doi: 10.1002/em.20654 – volume: 721 start-page: 163 year: (2011) ident: key 20170517095528_CIT0016 article-title: When pigs fly: immunomagnetic separation facilitates rapid determination of Pig-a mutant frequency by flow cytometric analysis publication-title: Mutat. Res doi: 10.1016/j.mrgentox.2011.01.009 – volume: 27 start-page: 577 year: (2007) ident: key 20170517095528_CIT0006 article-title: The role of flow cytometry in the diagnosis of paroxysmal nocturnal hemoglobinuria in the clinical laboratory publication-title: Clin. Lab. Med doi: 10.1016/j.cll.2007.05.012 – volume: 62 start-page: 175 year: (1999) ident: key 20170517095528_CIT0003 article-title: Paroxysmal nocturnal hemoglobinuria: An acquired genetic disease publication-title: Am. J. Hematol doi: 10.1002/(SICI)1096-8652(199911)62:3<175::AID-AJH7>3.0.CO;2-8 – volume: 52 start-page: 690 year: (2011) ident: key 20170517095528_CIT0007 article-title: International Pig-a gene mutation assay trial: evaluation of transferability across 14 laboratories publication-title: Environ. Mol. Mutagen doi: 10.1002/em.20672 – volume: 144 start-page: 287 year: (2008) ident: key 20170517095528_CIT0004 article-title: Biosynthesis, remodelling and functions of mammalian GPI-anchored proteins: recent progress publication-title: J. Biochem doi: 10.1093/jb/mvn090 – volume: 380 start-page: 503 year: (1999) ident: key 20170517095528_CIT0005 article-title: Biosynthesis of glycosylphosphatidylinositols in mammals and unicellular microbes publication-title: Biol. Chem doi: 10.1515/BC.1999.066 – volume: 130 start-page: 328 year: (2012) ident: key 20170517095528_CIT0008 article-title: Efficient monitoring of in vivo pig-a gene mutation and chromosomal damage: summary of 7 published studies and results from 11 new reference compounds publication-title: Toxicol. Sci doi: 10.1093/toxsci/kfs258 – volume: 21 start-page: 715 year: (2000) ident: key 20170517095528_CIT0017 article-title: LacI mutation spectra following benzo[a]pyrene treatment of Big Blue mice publication-title: Carcinogenesis doi: 10.1093/carcin/21.4.715 – volume: 49 start-page: 622 year: (2008) ident: key 20170517095528_CIT0009 article-title: Development of an in vivo gene mutation assay using the endogenous Pig-A gene: II. Selection of Pig-A mutant rat spleen T-cells with proaerolysin and sequencing Pig-A cDNA from the mutants publication-title: Environ. Mol. Mutagen doi: 10.1002/em.20413 – volume: 12 start-page: 245 year: (2011) ident: key 20170517095528_CIT0015 article-title: Accuracy and quality assessment of 454 GS-FLX Titanium pyrosequencing publication-title: BMC Genomics doi: 10.1186/1471-2164-12-245 – volume: 51 start-page: 138 year: (2010) ident: key 20170517095528_CIT0012 article-title: Flow cytometric detection of Pig-A mutant red blood cells using an erythroid-specific antibody: application of the method for evaluating the in vivo genotoxicity of methylphenidate in adolescent rats publication-title: Environ. Mol. Mutagen doi: 10.1002/em.20519 – volume: 51 start-page: 825 year: (2010) ident: key 20170517095528_CIT0001 article-title: The in vivo Pig-a gene mutation assay, a potential tool for regulatory safety assessment publication-title: Environ. Mol. Mutagen doi: 10.1002/em.20627 – volume: 16 start-page: 317 year: (2006) ident: key 20170517095528_CIT0002 article-title: Paroxysmal nocturnal hemoglobinuria: an acquired X-linked genetic disease with somatic-cell mosaicism publication-title: Curr. Opin. Genet. Dev doi: 10.1016/j.gde.2006.04.015 – volume: 1044 start-page: 79 year: (2013) ident: key 20170517095528_CIT0013 article-title: Detection of in vivo mutation in the Hprt and Pig-a genes of rat lymphocytes publication-title: Methods Mol. Biol doi: 10.1007/978-1-62703-529-3_4 – volume: 723 start-page: 36 year: (2011) ident: key 20170517095528_CIT0011 article-title: Manifestation of Pig-a mutant bone marrow erythroids and peripheral blood erythrocytes in mice treated with N-ethyl-N-nitrosourea: direct sequencing of Pig-a cDNA from bone marrow cells negative for GPI-anchored protein expression publication-title: Mutat. Res doi: 10.1016/j.mrgentox.2011.03.016 – volume: 26 start-page: 261 year: (1995) ident: key 20170517095528_CIT0014 article-title: Analysis of in vivo mutation induced by N-ethyl-N-nitrosourea in the hprt gene of rat lymphocytes publication-title: Environ. Mol. Mutagen doi: 10.1002/em.2850260402
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SubjectTerms	Animals Antigens, CD - genetics Antigens, CD - metabolism Base Sequence CD48 Antigen Cells, Cultured DNA Mutational Analysis Ethylnitrosourea - pharmacology Flow Cytometry High-Throughput Nucleotide Sequencing Immunomagnetic Separation Male Membrane Proteins - genetics Mutagenesis Mutagenicity Tests Mutagens - pharmacology Mutation Phenotype Rats, Inbred F344 T-Lymphocytes - metabolism
Title	Confirmation of Pig-a mutation in flow cytometry-identified CD48-deficient T-lymphocytes from F344 rats
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