Low diversity of t haplotypes in the eastern form of the house mouse, Mus musculus L.

Abstract In previous studies, 13 different recessive embryonic lethal genes have been associated with t haplotypes in the wild mice of the species Mus domesticus. In this communication we have analyzed five populations of Mus musculus for the presence and identity of t haplotypes. The populations occupy geographically distant regions in the Soviet Union: Altai Mountains, western and eastern Siberia, Azerbaijan and Turkmenistan. No t haplotypes were found in mice from eastern Siberia. In the remaining four populations, t haplotypes occurred with frequencies ranging from 0.07 to 0.21. All the t haplotypes extracted from these populations and analyzed by the genetic complementation test were shown to carry the same lethal gene tcl-w73. In one population (that of western Siberia), another lethal gene (tcl-w5) was found to be present on the same chromosome as tcl-w73. This situation is in striking contrast to that found in the populations of the western form of the house mouse, M. domesticus. In the latter species, tcl-w73 has not been found at all and the different populations are characterized by the presence of several different lethal genes. The low diversity of t haplotypes in M. musculus is consistent with lower genetic variability of other traits and indicates a different origin and speciation mode compared to M. domesticus. Serological typing for H-2 antigenic determinants suggests that most, if not all, of the newly described t haplotypes might have arisen by recombination of tw73 from M. musculus with t haplotypes from M. domesticus either in the hybrid zone between the two species or in regions where the two species mixed accidentally.

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Insights into mammalian biology from the wild house mouse Mus musculus

eLife ◽

10.7554/elife.05959 ◽

2015 ◽

Vol 4 ◽

Cited By ~ 45

Author(s):

Megan Phifer-Rixey ◽

Michael W Nachman

Keyword(s):

House Mouse ◽

Mus Musculus ◽

Genetic Model ◽

Inbred Strains ◽

Mendelian Inheritance ◽

Model Organisms ◽

House Mice ◽

Small Subset ◽

Wild Mice ◽

Wide Range

The house mouse, Mus musculus, was established in the early 1900s as one of the first genetic model organisms owing to its short generation time, comparatively large litters, ease of husbandry, and visible phenotypic variants. For these reasons and because they are mammals, house mice are well suited to serve as models for human phenotypes and disease. House mice in the wild consist of at least three distinct subspecies and harbor extensive genetic and phenotypic variation both within and between these subspecies. Wild mice have been used to study a wide range of biological processes, including immunity, cancer, male sterility, adaptive evolution, and non-Mendelian inheritance. Despite the extensive variation that exists among wild mice, classical laboratory strains are derived from a limited set of founders and thus contain only a small subset of this variation. Continued efforts to study wild house mice and to create new inbred strains from wild populations have the potential to strengthen house mice as a model system.

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Polymorphism of t-complex genes in European wild mice

Genetics Research ◽

10.1017/s0016672300026239 ◽

1984 ◽

Vol 44 (1) ◽

pp. 39-46 ◽

Cited By ~ 87

Author(s):

Jan Klein ◽

Peter Sipos ◽

Felipe Figueroa

Keyword(s):

Soviet Union ◽

North America ◽

Common Ancestor ◽

Complementation Test ◽

Homozygous State ◽

Wild Mice ◽

T Complex ◽

The Soviet Union ◽

Complementation Groups ◽

The Individual

SummaryThirty-two t haplotypes were extracted from wild mice captured in Central Europe, Spain, the Soviet Union, Israel, Egypt, the Orkneys and South and North America, and tested for lethality in the homozygous state. Twenty-two proved to be homozygous lethals, 8 semilethals and 2 viables. The lethal t haplotypes were then tested by the genetic complementation test for identity with representatives of known complementation groups and with each other. Five of the 22 haplotypes proved to carry previously identified lethality factors (tw5, tw73, and tLub-1), while the rest carried new factors. The 17 haplotypes fell into 8 new complementation groups. Two of the new groups are partially overlapping in that they seem to share some lethality factors and differ in others. These tests raise the total number of known complementation groups to 16. The distribution of the individual t haplotypes among wild mice populations seems to reflect their differentiation from a common ancestor haplotype.

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Genetic and Taxonomic Diversity of the House Mouse Mus musculus from the Asian Part of the Former Soviet Union

Russian Journal of Genetics ◽

10.1023/b:ruge.0000044757.65886.bb ◽

2004 ◽

Vol 40 (10) ◽

pp. 1134-1143 ◽

Cited By ~ 10

Author(s):

L. N. Spiridonova ◽

G. N. Chelomina ◽

K. Moriwaki ◽

H. Yonekawa ◽

A. S. Bogdanov

Keyword(s):

Soviet Union ◽

House Mouse ◽

Mus Musculus ◽

Former Soviet Union ◽

Taxonomic Diversity

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Pen and field trials of flupropadine against the house mouse (Mus musculus L.)

Journal of Hygiene ◽

10.1017/s0022172400062938 ◽

1985 ◽

Vol 95 (2) ◽

pp. 513-518 ◽

Cited By ~ 3

Author(s):

F. P. Rowe ◽

A. Bradfield ◽

T. Swinney

Keyword(s):

House Mouse ◽

Mus Musculus ◽

Second Generation ◽

Treatment Success ◽

Field Trials ◽

Mortality Data ◽

Wild Mice ◽

Anticoagulant Rodenticides ◽

Farm Buildings ◽

Family Groups

SUMMARYLaboratory and field trials were conducted to determine the efficacy of the candidate rodenticide flupropadine against the house mouse (Mus musculus L.). In laboratory feeding tests, family groups of wild mice maintained in pens and conditioned to feeding on plain foods were offered flupropadine at either 0·10%, 0·15%, 0·18% or 0·20% in pinhead oatmeal bait. Overall mortalities in replicated 21-day treatments were 66/71 (93·0%), 71/79 (89·9%), 72/70 (94·7%) and 69/75 (92·0%) respectively.In 17 field trials carried out against mice infesting farm buildings, flupropadine was used at 0·10%, 0·15% and 0·18% in oatmeal bait. Mean treatment success, estimated from live-capture and mortality data, was 88·6%, 96·2% and 96·6% respectively.Flupropadine was found to be as near effective against mice as calciferol/warfarin and the second-generation anticoagulant rodenticides difenacoum, bromadiolone and brodifacoum. In further comparison with the anticoagulants, treatment with flupropadine bait achieved markedly quicker control.

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Pen and field trials of a new anticoagulant rodenticide flocoumafen against the house mouse (Mus musculus L.)

Journal of Hygiene ◽

10.1017/s0022172400060721 ◽

1985 ◽

Vol 95 (3) ◽

pp. 623-627 ◽

Cited By ~ 16

Author(s):

F. P. Rowe ◽

A. Bradfield ◽

T. Swinney

Keyword(s):

House Mouse ◽

Mus Musculus ◽

Treatment Success ◽

Field Trials ◽

Mortality Data ◽

House Mice ◽

Anticoagulant Rodenticide ◽

Free Living ◽

Wild Mice ◽

Farm Buildings

SUMMARYThe efficacy of flocoumafen, a novel anticoagulant rodentide, was evaluated in feeding tests on confined and free-living populations of house mice (Mus musculus L.). In four pen trials, family groups of laboratory-reared wild mice were conditioned to feeding on plain foods and then offered flocoumafen at 0.005% in pinhead oatmeal bait. All 68 mice, comprising juvenile and adult animals, died within 10 days.Ten field trials were carried out, using the same formulated poison bait, against mice infesting farm buildings. Mean treatment success, estimated from live-capture and mortality data, ranged between 87–1 and 100%.The performance of flocoumafen is compared with that of difenacoum, bromadiolone and brodifacoum used at the same concentration in oatmeal bait. Flocoumafen gave an equally effective but quicker kill of mice. It is concluded that flocoumafen is a promising new rodenticide for the control of M. musculus.

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