A mouse chromosome 4 balancer ENU-mutagenesis screen isolates eleven lethal lines

Melissa K. Boles; Bonney M. Wilkinson; Andrea Maxwell; Lihua Lai; Alea A. Mills; Ichiko Nishijima; Andrew P. Salinger; Ivan Moskowitz; Karen K. Hirschi; Bin Liu; Allan Bradley; Monica J. Justice

doi:10.1186/1471-2156-10-12

A mouse chromosome 4 balancer ENU-mutagenesis screen isolates eleven lethal lines

Melissa K. Boles, Bonney M. Wilkinson, Andrea Maxwell, Lihua Lai, Alea A. Mills, Ichiko Nishijima, Andrew P. Salinger, Ivan Moskowitz, Karen K. Hirschi, Bin Liu, Allan Bradley, Monica J. Justice

Epigenetics & Molecular Carcinogenesis

Research output: Contribution to journal › Article › peer-review

13 Scopus citations

Abstract

Background: ENU-mutagenesis is a powerful technique to identify genes regulating mammalian development. To functionally annotate the distal region of mouse chromosome 4, we performed an ENU-mutagenesis screen using a balancer chromosome targeted to this region of the genome. Results: We isolated 11 lethal lines that map to the region of chromosome 4 between D4Mit117 and D4Mit281. These lines form 10 complementation groups. The majority of lines die during embryonic development between E5.5 and E12.5 and display defects in gastrulation, cardiac development, and craniofacial development. One line displayed postnatal lethality and neurological defects, including ataxia and seizures. Conclusion: These eleven mutants allow us to query gene function within the distal region of mouse chromosome 4 and demonstrate that new mouse models of mammalian developmental defects can easily and quickly be generated and mapped with the use of ENU-mutagenesis in combination with balancer chromosomes. The low number of mutations isolated in this screen compared with other balancer chromosome screens indicates that the functions of genes in different regions of the genome vary widely.

Original language	English (US)
Pages (from-to)	12
Number of pages	1
Journal	BMC genetics
Volume	10
DOIs	https://doi.org/10.1186/1471-2156-10-12
State	Published - Mar 6 2009

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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title = "A mouse chromosome 4 balancer ENU-mutagenesis screen isolates eleven lethal lines",

abstract = "Background: ENU-mutagenesis is a powerful technique to identify genes regulating mammalian development. To functionally annotate the distal region of mouse chromosome 4, we performed an ENU-mutagenesis screen using a balancer chromosome targeted to this region of the genome. Results: We isolated 11 lethal lines that map to the region of chromosome 4 between D4Mit117 and D4Mit281. These lines form 10 complementation groups. The majority of lines die during embryonic development between E5.5 and E12.5 and display defects in gastrulation, cardiac development, and craniofacial development. One line displayed postnatal lethality and neurological defects, including ataxia and seizures. Conclusion: These eleven mutants allow us to query gene function within the distal region of mouse chromosome 4 and demonstrate that new mouse models of mammalian developmental defects can easily and quickly be generated and mapped with the use of ENU-mutagenesis in combination with balancer chromosomes. The low number of mutations isolated in this screen compared with other balancer chromosome screens indicates that the functions of genes in different regions of the genome vary widely.",

author = "Boles, {Melissa K.} and Wilkinson, {Bonney M.} and Andrea Maxwell and Lihua Lai and Mills, {Alea A.} and Ichiko Nishijima and Salinger, {Andrew P.} and Ivan Moskowitz and Hirschi, {Karen K.} and Bin Liu and Allan Bradley and Justice, {Monica J.}",

note = "Funding Information: We would like to acknowledge Maritess Alviento and Hisashi Nakamura for technical assistance. We gratefully acknowledge the entertaining wisdom of Dr. Frank Probst in his critical reading of this manuscript. This research was funded by NIH grants U01 HD39372 and R01 CA115503 to MJJ and R01 HL76260 to KKH and MJJ.",

year = "2009",

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day = "6",

doi = "10.1186/1471-2156-10-12",

language = "English (US)",

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TY - JOUR

T1 - A mouse chromosome 4 balancer ENU-mutagenesis screen isolates eleven lethal lines

AU - Boles, Melissa K.

AU - Wilkinson, Bonney M.

AU - Maxwell, Andrea

AU - Lai, Lihua

AU - Mills, Alea A.

AU - Nishijima, Ichiko

AU - Salinger, Andrew P.

AU - Moskowitz, Ivan

AU - Hirschi, Karen K.

AU - Liu, Bin

AU - Bradley, Allan

AU - Justice, Monica J.

N1 - Funding Information: We would like to acknowledge Maritess Alviento and Hisashi Nakamura for technical assistance. We gratefully acknowledge the entertaining wisdom of Dr. Frank Probst in his critical reading of this manuscript. This research was funded by NIH grants U01 HD39372 and R01 CA115503 to MJJ and R01 HL76260 to KKH and MJJ.

PY - 2009/3/6

Y1 - 2009/3/6

N2 - Background: ENU-mutagenesis is a powerful technique to identify genes regulating mammalian development. To functionally annotate the distal region of mouse chromosome 4, we performed an ENU-mutagenesis screen using a balancer chromosome targeted to this region of the genome. Results: We isolated 11 lethal lines that map to the region of chromosome 4 between D4Mit117 and D4Mit281. These lines form 10 complementation groups. The majority of lines die during embryonic development between E5.5 and E12.5 and display defects in gastrulation, cardiac development, and craniofacial development. One line displayed postnatal lethality and neurological defects, including ataxia and seizures. Conclusion: These eleven mutants allow us to query gene function within the distal region of mouse chromosome 4 and demonstrate that new mouse models of mammalian developmental defects can easily and quickly be generated and mapped with the use of ENU-mutagenesis in combination with balancer chromosomes. The low number of mutations isolated in this screen compared with other balancer chromosome screens indicates that the functions of genes in different regions of the genome vary widely.

AB - Background: ENU-mutagenesis is a powerful technique to identify genes regulating mammalian development. To functionally annotate the distal region of mouse chromosome 4, we performed an ENU-mutagenesis screen using a balancer chromosome targeted to this region of the genome. Results: We isolated 11 lethal lines that map to the region of chromosome 4 between D4Mit117 and D4Mit281. These lines form 10 complementation groups. The majority of lines die during embryonic development between E5.5 and E12.5 and display defects in gastrulation, cardiac development, and craniofacial development. One line displayed postnatal lethality and neurological defects, including ataxia and seizures. Conclusion: These eleven mutants allow us to query gene function within the distal region of mouse chromosome 4 and demonstrate that new mouse models of mammalian developmental defects can easily and quickly be generated and mapped with the use of ENU-mutagenesis in combination with balancer chromosomes. The low number of mutations isolated in this screen compared with other balancer chromosome screens indicates that the functions of genes in different regions of the genome vary widely.

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A mouse chromosome 4 balancer ENU-mutagenesis screen isolates eleven lethal lines

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