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A genetic and genomic analysis identifies a cluster of genes associated with hematopoietic cell turnover

Hematopoietic stem cells from different strains of mice vary widely with respect to their cell cycle activity. In the present study we used complementary genetic and genomic approaches to identify molecular pathways affecting this complex trait. We identified a major quantitative trait locus (QTL) a...

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Published in:	Blood 2002-09, Vol.100 (6), p.2056-2062
Main Authors:	de Haan, Gerald, Bystrykh, Leonid V., Weersing, Ellen, Dontje, Bert, Geiger, Hartmut, Ivanova, Natalia, Lemischka, Ihor R., Vellenga, Edo, Van Zant, Gary
Format:	Article
Language:	English
Subjects:	Animals Biological and medical sciences Cell differentiation, maturation, development, hematopoiesis Cell Division - genetics Cell physiology Chromosome Mapping Chromosomes Cytogenetic Analysis Female Fundamental and applied biological sciences. Psychology Gene Expression Profiling Genome Hematopoietic Stem Cells - cytology Hematopoietic Stem Cells - metabolism Mice Mice, Congenic Mice, Inbred C57BL Mice, Inbred DBA Molecular and cellular biology Multigene Family - genetics Multigene Family - physiology Oligonucleotide Array Sequence Analysis
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creator	de Haan, Gerald Bystrykh, Leonid V. Weersing, Ellen Dontje, Bert Geiger, Hartmut Ivanova, Natalia Lemischka, Ihor R. Vellenga, Edo Van Zant, Gary
description	Hematopoietic stem cells from different strains of mice vary widely with respect to their cell cycle activity. In the present study we used complementary genetic and genomic approaches to identify molecular pathways affecting this complex trait. We identified a major quantitative trait locus (QTL) associated with variation in cell proliferation in C57BL/6 and DBA/2 mice to a 10 centimorgan (cM) region on chromosome 11. A congenic mouse model confirmed that a genomic interval on chromosome 11 in isolation confers the proliferation phenotype. To detect candidate genes we performed subtractive hybridizations and gene arrays using cDNA from highly enriched stem cells from parental strains. Intriguingly, a disproportionate number of differentially expressed genes mapped to chromosome 11 and, more specifically, these transcripts occurred in 3 distinct clusters. The largest cluster colocalized exactly with the cell cycling QTL. Such clustering suggested the involvement of genetic variation that affects higher-order chromosomal organization. This hypothesis was reinforced by the fact that differentially expressed genes mapped to recombination “coldspots,” as a consequence of which clustered genes are collectively inherited. These findings suggest the functional interdependence of these closely linked genes. Our data are consistent with the hypothesis that this isolated cell cycle QTL does not result from a mutation in a single gene but rather is a consequence of variable expression of a collection of highly linked genes.
doi_str_mv	10.1182/blood-2002-03-0808
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This hypothesis was reinforced by the fact that differentially expressed genes mapped to recombination “coldspots,” as a consequence of which clustered genes are collectively inherited. These findings suggest the functional interdependence of these closely linked genes. 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In the present study we used complementary genetic and genomic approaches to identify molecular pathways affecting this complex trait. We identified a major quantitative trait locus (QTL) associated with variation in cell proliferation in C57BL/6 and DBA/2 mice to a 10 centimorgan (cM) region on chromosome 11. A congenic mouse model confirmed that a genomic interval on chromosome 11 in isolation confers the proliferation phenotype. To detect candidate genes we performed subtractive hybridizations and gene arrays using cDNA from highly enriched stem cells from parental strains. Intriguingly, a disproportionate number of differentially expressed genes mapped to chromosome 11 and, more specifically, these transcripts occurred in 3 distinct clusters. The largest cluster colocalized exactly with the cell cycling QTL. Such clustering suggested the involvement of genetic variation that affects higher-order chromosomal organization. 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subjects	Animals Biological and medical sciences Cell differentiation, maturation, development, hematopoiesis Cell Division - genetics Cell physiology Chromosome Mapping Chromosomes Cytogenetic Analysis Female Fundamental and applied biological sciences. Psychology Gene Expression Profiling Genome Hematopoietic Stem Cells - cytology Hematopoietic Stem Cells - metabolism Mice Mice, Congenic Mice, Inbred C57BL Mice, Inbred DBA Molecular and cellular biology Multigene Family - genetics Multigene Family - physiology Oligonucleotide Array Sequence Analysis
title	A genetic and genomic analysis identifies a cluster of genes associated with hematopoietic cell turnover
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