B6.129S2-Ighm^tm1Cgn/CgnOrl

Status	Available to order
EMMA ID	EM:00001
Citation information	RRID:IMSR_EM:00001 Research Resource Identifiers (RRID) are persistent unique ID numbers assigned to help researchers cite key resources (e.g. antibodies, model organisms and software projects) in the biomedical literature to improve transparency and reproducibility in research. See https://www.rrids.org/ for more information.
International strain name	B6.129S2-Ighm^tm1Cgn/CgnOrl
Alternative name	muMT°(muKO)
Strain type	Targeted Mutant Strains : Knock-out
Allele/Transgene symbol	Ighm^tm1Cgn
Gene/Transgene symbol	Ighm

Information from provider

Provider	Klaus Rajewsky
Provider affiliation	CBR Institute for Biomedical Research, Immune Disease Institute
Genetic information	Mutant mice in the constant region of the immunoglobulin heavy chain 6 (heavy chain of IgM, Ighm) gene. Obtained by mutation of the gene by homologous recombination (insertion of the neo gene into the membrane domain-coding exon).
Phenotypic information	Normal development of B cells in heterozygous animals. Absent in homozygotes; development stops at pre-B stage.
Breeding history	129S2/Sv ES cells; 10 generations of backcross to C57BL/6, then intercross.
References	A B cell-deficient mouse by targeted disruption of the membrane exon of the immunoglobulin mu chain gene.;Kitamura D, Roes J, Kühn R, Rajewsky K, ;1991;Nature;350;423-6; 1901381

Information from EMMA

Archiving centre	Institut de Transgenose, INTRAGENE, Orléans, France
Animals used for archiving	heterozygous C57BL/6J males, wild-type C57BL/6J females
Breeding at archiving centre	Males homozygous or heterozygous

Disease and phenotype information

MGI allele-associated human disease models

type 1 diabetes mellitus / DOID:9744

Orphanet associated rare diseases, based on orthologous gene matching

Autosomal agammaglobulinemia / Orphanet_33110

MGI phenotypes (allele matching)

increased susceptibility to autoimmune diabetes / MGI
arrested B cell differentiation / MGI
decreased bone mineral density / MGI
abnormal trabecular bone morphology / MGI
decreased compact bone thickness / MGI
abnormal spleen morphology / MGI
abnormal cardiovascular system physiology / MGI
abnormal humoral immune response / MGI
decreased IgG level / MGI
abnormal respiratory system physiology / MGI
decreased immunoglobulin level / MGI
decreased IgE level / MGI
abnormal cytokine secretion / MGI
abnormal compact bone morphology / MGI
decreased spleen weight / MGI
increased susceptibility to parasitic infection / MGI
decreased susceptibility to injury / MGI
immune system phenotype / MGI
decreased CD4-positive, alpha beta T cell number / MGI
decreased CD8-positive, alpha-beta T cell number / MGI
decreased dendritic cell number / MGI
decreased IgG1 level / MGI
decreased trabecular bone thickness / MGI
decreased compact bone volume / MGI
decreased susceptibility to autoimmune diabetes / MGI
abnormal T cell proliferation / MGI
abnormal T cell number / MGI
absent B cells / MGI
abnormal spleen B cell follicle morphology / MGI
insulitis / MGI
abnormal intestinal epithelium morphology / MGI
abnormal CD8 positive, alpha-beta intraepithelial T cell morphology / MGI
decreased IgA level / MGI
abnormal antigen presentation / MGI
abnormal spleen marginal sinus morphology / MGI
increased susceptibility to induced arthritis / MGI
increased osteoclast cell number / MGI
decreased T cell proliferation / MGI
abnormal CD4-positive, alpha-beta T cell physiology / MGI
decreased susceptibility to type IV hypersensitivity reaction / MGI
absent follicular dendritic cells / MGI
absent mature B cells / MGI
abnormal spleen marginal zone macrophage morphology / MGI
abnormal metallophilic macrophage morphology / MGI
decreased IgM level / MGI
abnormal lymphatic vessel morphology / MGI
abnormal B cell differentiation / MGI
abnormal response to infection / MGI
respiratory system phenotype / MGI
absent immature B cells / MGI

MGI phenotypes (gene matching)

decreased bone mineral density / MGI
abnormal trabecular bone morphology / MGI
decreased compact bone thickness / MGI
abnormal intestinal epithelium morphology / MGI
abnormal spleen morphology / MGI
abnormal cardiovascular system physiology / MGI
abnormal immune system physiology / MGI
abnormal humoral immune response / MGI
arrested B cell differentiation / MGI
decreased IgG level / MGI
decreased IgM level / MGI
decreased IgA level / MGI
abnormal antigen presentation / MGI
kidney inflammation / MGI
abnormal lymphatic vessel morphology / MGI
abnormal respiratory system physiology / MGI
abnormal B cell differentiation / MGI
no abnormal phenotype detected / MGI
small lymph nodes / MGI
abnormal spleen white pulp morphology / MGI
abnormal spleen periarteriolar lymphoid sheath morphology / MGI
abnormal spleen germinal center morphology / MGI
abnormal spleen marginal zone morphology / MGI
abnormal spleen marginal sinus morphology / MGI
increased susceptibility to viral infection / MGI
abnormal B cell physiology / MGI
decreased immunoglobulin level / MGI
abnormal complement pathway / MGI
impaired complement classical pathway / MGI
decreased IgE level / MGI
increased IgM level / MGI
increased IgA level / MGI
abnormal immune serum protein physiology / MGI
abnormal cytokine secretion / MGI
no phenotypic analysis / MGI
increased susceptibility to induced arthritis / MGI
increased autoantibody level / MGI
abnormal compact bone morphology / MGI
insulitis / MGI
increased anti-double stranded DNA antibody level / MGI
increased susceptibility to autoimmune diabetes / MGI
decreased susceptibility to autoimmune diabetes / MGI
abnormal class switch recombination / MGI
decreased spleen weight / MGI
increased B-1 B cell number / MGI
decreased B-1 B cell number / MGI
increased osteoclast cell number / MGI
increased B cell number / MGI
decreased B cell number / MGI
abnormal immature B cell morphology / MGI
abnormal response to infection / MGI
increased susceptibility to parasitic infection / MGI
decreased B cell proliferation / MGI
abnormal T cell proliferation / MGI
decreased T cell proliferation / MGI
increased B cell proliferation / MGI
decreased susceptibility to injury / MGI
immune system phenotype / MGI
respiratory system phenotype / MGI
abnormal CD4-positive, alpha-beta T cell physiology / MGI
decreased susceptibility to type IV hypersensitivity reaction / MGI
abnormal T cell number / MGI
absent B cells / MGI
decreased CD4-positive, alpha beta T cell number / MGI
decreased CD8-positive, alpha-beta T cell number / MGI
increased plasma cell number / MGI
abnormal plasma cell differentiation / MGI
decreased dendritic cell number / MGI
decreased Peyer's patch number / MGI
small Peyer's patches / MGI
abnormal B-1a B cell morphology / MGI
abnormal mature B cell morphology / MGI
decreased follicular B cell number / MGI
increased marginal zone B cell number / MGI
decreased marginal zone B cell number / MGI
increased pro-B cell number / MGI
decreased transitional stage B cell number / MGI
abnormal follicular dendritic cell antigen presentation / MGI
absent follicular dendritic cells / MGI
decreased pre-B cell number / MGI
decreased mature B cell number / MGI
absent mature B cells / MGI
absent immature B cells / MGI
decreased immature B cell number / MGI
abnormal B cell activation / MGI
abnormal spleen marginal zone macrophage morphology / MGI
abnormal metallophilic macrophage morphology / MGI
abnormal CD8 positive, alpha-beta intraepithelial T cell morphology / MGI
abnormal spleen B cell follicle morphology / MGI
decreased IgG1 level / MGI
decreased IgG2a level / MGI
decreased IgG2b level / MGI
decreased IgG3 level / MGI
increased IgG2a level / MGI
increased IgG3 level / MGI
abnormal splenic cell ratio / MGI
decreased trabecular bone thickness / MGI
decreased compact bone volume / MGI

Literature references

A B cell-deficient mouse by targeted disruption of the membrane exon of the immunoglobulin mu chain gene.;Kitamura D, Roes J, Kühn R, Rajewsky K, ;1991;Nature;350;423-6; 1901381
Invariant NKT cells sustain specific B cell responses and memory.;Galli Grazia, Pittoni Paola, Tonti Elena, Malzone Carmine, Uematsu Yasushi, Tortoli Marco, Maione Domenico, Volpini Gianfranco, Finco Oretta, Nuti Sandra, Tavarini Simona, Dellabona Paolo, Rappuoli Rino, Casorati Giulia, Abrignani Sergio, ;2007;Proceedings of the National Academy of Sciences of the United States of America;104;3984-9; 17360464

Information on how we integrate external resources can be found here

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Availabilities

Requesting frozen sperm or embryos is generally advisable wherever possible, in order to minimise the shipment of live mice.

Frozen embryos. Delivered in 4 weeks (after paperwork in place). €1740^*
Frozen sperm. Delivered in 4 weeks (after paperwork in place). €1740^*
Rederivation of mice from frozen stock, delivery time available upon request . €3880^*

Due to the dynamic nature of our processes strain availability may change at short notice. The local repository manager will advise you in these circumstances.

^* In addition users have to cover all the shipping costs (including the cost for returning dry-shippers, where applicable).

More details on pricing and delivery times

Practical information

Genotyping protocol

Example health report
(Current health report will be provided later)

Material Transfer Agreement (MTA)
For this strain no provider MTA is needed. Distribution is based on the EMMA conditions only.

EMMA conditions
Legally binding conditions for the transfer

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B6.129S2-Ighmtm1Cgn/CgnOrl