GeneSet Information

Tier II GS136021 • hematopoietic stem cell frequency regulator (Hscfr, Published QTL Chr 17)

DESCRIPTION:

QTL associated with hematopoietic stem cell frequency regulator. This interval was obtained by using a fixed interval width of 25 Mbp around the peak marker (47690141)

LABEL:

QTL-Hscfr-Mouse-Chr 17

SCORE TYPE:

Binary

DATE ADDED:

2012-04-02

DATE UPDATED:

2024-04-25

SPECIES:

URI:

http://www.informatics.jax.org/searches/accession_report.cgi?id=MGI:2665081

AUTHORS:

Jawad M, Giotopoulos G, Cole C, Plumb M

TITLE:

Target cell frequency is a genetically determined risk factor in radiation leukaemogenesis.

JOURNAL:

The British journal of radiology Sep 2007, Vol 80 Spec No 1, pp. S56-62

ABSTRACT:

Whole body exposure to ionizing radiation increases the risk of radiation-induced acute myeloid leukaemia (r-AML). r-AML is the result of the accumulation of mutations in a single haemopoietic stem cell, so risk is therefore a function of the number of mutations required to transform the stem cell and the mutation rate. There is a genetic component to the risk of AML within the general population, and low penetrance variant alleles encoding DNA repair enzymes have been genetically implicated in therapy-related AML susceptibility. However, what is largely ignored is that target cell number, which defines the number of genomes at risk from DNA damaging agents, is also part of the equation that defines risk. We will review the evidence from genetic studies of inbred mouse models that target cell frequency is a risk factor in radiation leukaemogenesis. Inbred mouse strains that differ in their susceptibility to radiation-induced r-AML and thymic lymphoma (r-TL), spontaneous TL and pristane-induced plasmacytoma (PCT) have been exploited to identify susceptibility loci. The target cell in AML is the haemopoietic stem cell, whereas TLs and PCT arise from more mature lymphoid progenitor cells. Inbred mice also differ significantly in all aspects of haemopoiesis, and these differences have been used to identify quantitative trait loci (QTL) that determine the frequency of specific haemopoietic stem, progenitor or mature blood cells. The co-localization of QTL that determine risk and target cell frequency in all three haemopoietic malignancies is strong evidence that target cell frequency is a risk factor in radiation leukaemogenesis. PUBMED: 17704327
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Annotation Information

No sequence read archive data associated with this GeneSet.


Radiation, Ionizing (D011839)
Review (D016454)
Alleles (D000483)
DNA (D004247)
Lymphoma (D008223)
Mice (D051379)
Quantitative Trait Loci (D040641)
Plasmacytoma (D010954)
Blood Cells (D001773)
Enzymes (D004798)
DNA Repair Enzymes (D045643)
Radiation (D011827)
Risk Factors (D012307)
Risk (D012306)
Mice, Inbred Strains (D008815)
Microscopy, Electron, Scanning Transmission (D017348)
Lymphoid Progenitor Cells (D054503)
Cells (D002477)
Blood (D001769)
Stem Cells (D013234)
DNA Repair (D004260)
Cell Count (D002452)
Mutation (D009154)
Penetrance (D019683)
Hematopoietic Stem Cells (D006412)
blood (MA:0000059)
cell (GO:0005623)
DNA repair (GO:0006281)
hemopoiesis (GO:0030097)
QTL map (EDAM_data:1860)

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Supported by NIH R01 AA18776 jointly funded by NIAAA and NIDA, and JAX Center for Precision Genetics NIH U54 OD 020351