Description

The genotypes of the animals provided may not reflect those discussed in the strain description or the mating scheme utilized by The Jackson Laboratory prior to cryopreservation. Please inquire for possible genotypes for this specific strain.

Strain Information

Type Mutant Strain; Targeted Mutation; Additional information on Genetically Engineered and Mutant Mice. Visit our online Nomenclature tutorial. Species laboratory mouse   Donating Investigator Klaus Rajewsky,   Max-Delbruck-Ctr. for Molecular Medicine

Appearance
white-bellied agouti
Related Genotype: A^w/A^w

Description
Mice homozygous for the Cd5^tm1Cgn targeted mutation are viable and apparently healthy. Both T and B cells in homozygous mutant mice lack surface CD5. Mice show normal immune responses to both T cell-dependent and -independent antigens.

Control Information

	Control
	000690 129P3/J	(approximate)
Considerations for Choosing Controls

Related Strains

Strains carrying other alleles of Cd5

000408	B6.Cg-Cd5a/CyJ
001282	C3.B6/(86NS)CyJ

View Strains carrying other alleles of Cd5     (2 strains)

Additional Web Information

New 129 Nomenclature Bulletin

Phenotype

Phenotype Information

View Mammalian Phenotype Terms

Mammalian Phenotype Terms provided by MGI

      assigned by genotype

The following phenotype information may relate to a genetic background differing from this JAX^® Mice strain.

Cd5^tm1Cgn/Cd5^tm1Cgn

        involves: 129P2/OlaHsd * C57BL/6

• normal phenotype
• no abnormal phenotype detected
  • mutant mice are viable, healthy and exhibit no changes in B and T cell populations, serum Ig content, and are able to mount effective T-cell dependent immune responses   (MGI Ref ID J:19317)

Cd5^tm1Cgn/Cd5^tm1Cgn

        B6.129P2-Cd5^tm1Cgn

• immune system phenotype
• abnormal T cell anergy
  • T cells treated with anti-CD3 or MOG35-55 are resistant to development of anergy   (MGI Ref ID J:189919)
• decreased susceptibility to experimental autoimmune encephalomyelitis
  • delayed onset and reduced severity of MOG-induced experimental autoimmune encephalomyelitis   (MGI Ref ID J:189919)
• increased T cell proliferation
  • in CD4+ T cells stimulated with anti-CD3 or cognate peptide, rested then restimulated with anti-CD3 or MOG35-55   (MGI Ref ID J:189919)
  • in CD8+ T cells when restimulated   (MGI Ref ID J:189919)
• increased regulatory T cell number   (MGI Ref ID J:189919)
• cellular phenotype
• increased T cell proliferation
  • in CD4+ T cells stimulated with anti-CD3 or cognate peptide, rested then restimulated with anti-CD3 or MOG35-55   (MGI Ref ID J:189919)
  • in CD8+ T cells when restimulated   (MGI Ref ID J:189919)
• hematopoietic system phenotype
• increased T cell proliferation
  • in CD4+ T cells stimulated with anti-CD3 or cognate peptide, rested then restimulated with anti-CD3 or MOG35-55   (MGI Ref ID J:189919)
  • in CD8+ T cells when restimulated   (MGI Ref ID J:189919)
• increased regulatory T cell number   (MGI Ref ID J:189919)

View Research Applications

Research Applications

This mouse can be used to support research in many areas including:

Cd5^tm1Cgn related

Immunology, Inflammation and Autoimmunity Research
CD Antigens, Antigen Receptors, and Histocompatibility Markers

Genes & Alleles

Gene & Allele Information provided by MGI

Allele Symbol		Cd5tm1Cgn
Allele Name		targeted mutation 1, University of Cologne
Allele Type		Targeted (knock-out)
Common Name(s)		CD5-; CD50; CD5T;
Mutation Made By		Alexander Tarakhovsky,   The Rockefeller University
Strain of Origin		129P2/OlaHsd
ES Cell Line Name		E14.1
ES Cell Line Strain		129P2/OlaHsd
Gene Symbol and Name		Cd5, CD5 antigen
Chromosome		19
Gene Common Name(s)		LEU1; Ly-1; Ly-12; Ly-A; Lyt-1; T-lymphocyte antigen 1; T1; lymphocyte antigen 1; lymphocyte antigen 12;
Molecular Note		A neomycin gene replaced part of exon 7, which encodes the transmembrane domain. An additional frameshift mutation was introduced into exon 3. Flow cytometry analysis on cells derived from thymus, spleen and the peritoneal cavity of homozygous mice confirmed that no detectable protein was expressed from this allele. [MGI Ref ID J:19317]

Genotyping

Genotyping Information

Helpful Links

Genotyping resources and troubleshooting

References

References provided by MGI

Selected Reference(s)

Tarakhovsky A; Muller W; Rajewsky K. 1994. Lymphocyte populations and immune responses in CD5-deficient mice. Eur J Immunol 24(7):1678-84. [PubMed: 7517879]  [MGI Ref ID J:19317]

Additional References

Joliat MJ; Lang PA; Lyons BL; Burzenski L; Lynes MA; Yi T; Sundberg JP; Shultz LD. 2002. Absence of CD5 Dramatically Reduces Progression of Pulmonary Inflammatory Lesions in SHP-1 Protein-Tyrosine Phosphatase-Deficient 'Viable Motheaten' Mice. J Autoimmun 18(2):105-17. [PubMed: 11908943]  [MGI Ref ID J:76141]

Cd5^tm1Cgn related

Axtell RC; Webb MS; Barnum SR; Raman C. 2004. Cutting edge: critical role for CD5 in experimental autoimmune encephalomyelitis: inhibition of engagement reverses disease in mice. J Immunol 173(5):2928-32. [PubMed: 15322150]  [MGI Ref ID J:92725]

Axtell RC; Xu L; Barnum SR; Raman C. 2006. CD5-CK2 binding/activation-deficient mice are resistant to experimental autoimmune encephalomyelitis: protection is associated with diminished populations of IL-17-expressing T cells in the central nervous system. J Immunol 177(12):8542-9. [PubMed: 17142752]  [MGI Ref ID J:140670]

Azzam HS; DeJarnette JB; Huang K; Emmons R; Park CS; Sommers CL; El-Khoury D; Shores EW; Love PE. 2001. Fine tuning of TCR signaling by CD5. J Immunol 166(9):5464-72. [PubMed: 11313384]  [MGI Ref ID J:106735]

Hayes SM; Li L; Love PE. 2005. TCR signal strength influences alphabeta/gammadelta lineage fate. Immunity 22(5):583-93. [PubMed: 15894276]  [MGI Ref ID J:99104]

Hippen KL; Tze LE; Behrens TW. 2000. CD5 maintains tolerance in anergic B cells. J Exp Med 191(5):883-90. [PubMed: 10704468]  [MGI Ref ID J:124695]

Joliat MJ; Lang PA; Lyons BL; Burzenski L; Lynes MA; Yi T; Sundberg JP; Shultz LD. 2002. Absence of CD5 Dramatically Reduces Progression of Pulmonary Inflammatory Lesions in SHP-1 Protein-Tyrosine Phosphatase-Deficient 'Viable Motheaten' Mice. J Autoimmun 18(2):105-17. [PubMed: 11908943]  [MGI Ref ID J:76141]

Laky K; Fowlkes BJ. 2007. Presenilins regulate alphabeta T cell development by modulating TCR signaling. J Exp Med 204(9):2115-29. [PubMed: 17698590]  [MGI Ref ID J:126088]

Li R; Page DM. 2001. Requirement for a complex array of costimulators in the negative selection of autoreactive thymocytes in vivo. J Immunol 166(10):6050-6. [PubMed: 11342622]  [MGI Ref ID J:110925]

Mizoguchi A; Mizoguchi E; de Jong YP; Takedatsu H; Preffer FI; Terhorst C; Bhan AK. 2003. Role of the CD5 molecule on TCR gammadelta T cell-mediated immune functions: development of germinal centers and chronic intestinal inflammation. Int Immunol 15(1):97-108. [PubMed: 12502730]  [MGI Ref ID J:110967]

Ordonez-Rueda D; Lozano F; Sarukhan A; Raman C; Garcia-Zepeda EA; Soldevila G. 2009. Increased numbers of thymic and peripheral CD4+ CD25+Foxp3+ cells in the absence of CD5 signaling. Eur J Immunol 39(8):2233-47. [PubMed: 19609976]  [MGI Ref ID J:151986]

Pena-Rossi C; Zuckerman LA; Strong J; Kwan J; Ferris W; Chan S; Tarakhovsky A; Beyers AD; Killeen N. 1999. Negative regulation of CD4 lineage development and responses by CD5. J Immunol 163(12):6494-501. [PubMed: 10586041]  [MGI Ref ID J:112133]

Sestero CM; McGuire DJ; De Sarno P; Brantley EC; Soldevila G; Axtell RC; Raman C. 2012. CD5-dependent CK2 activation pathway regulates threshold for T cell anergy. J Immunol 189(6):2918-30. [PubMed: 22904299]  [MGI Ref ID J:189919]

Tabbekh M; Franciszkiewicz K; Haouas H; Lecluse Y; Benihoud K; Raman C; Mami-Chouaib F. 2011. Rescue of tumor-infiltrating lymphocytes from activation-induced cell death enhances the antitumor CTL response in CD5-deficient mice. J Immunol 187(1):102-9. [PubMed: 21622855]  [MGI Ref ID J:175940]

Tarakhovsky A; Kanner SB; Hombach J; Ledbetter JA; Muller W; Killeen N; Rajewsky K. 1995. A role for CD5 in TCR-mediated signal transduction and thymocyte selection. Science 269(5223):535-7. [PubMed: 7542801]  [MGI Ref ID J:89249]

Teh SJ; Killeen N; Tarakhovsky A; Littman DR; Teh HS. 1997. CD2 regulates the positive selection and function of antigen-specific CD4- CD8+ T cells. Blood 89(4):1308-18. [PubMed: 9028954]  [MGI Ref ID J:111606]

Xu Z; Butfiloski EJ; Sobel ES; Morel L. 2004. Mechanisms of peritoneal B-1a cells accumulation induced by murine lupus susceptibility locus Sle2. J Immunol 173(10):6050-8. [PubMed: 15528340]  [MGI Ref ID J:132281]

Zou X; Smith JA; Corcos D; Matheson LS; Osborn MJ; Bruggemann M. 2008. Removal of the BiP-retention domain in Cmu permits surface deposition and developmental progression without L-chain. Mol Immunol 45(13):3573-9. [PubMed: 18584871]  [MGI Ref ID J:137831]

Health & husbandry

Health & Colony Maintenance Information

Animal Health Reports

Production of mice from cryopreserved embryos or sperm occurs in a maximum barrier room, G200.

Colony Maintenance

Diet Information	LabDiet® 5K52/5K67

Pricing and Purchasing

Pricing, Supply Level & Notes, Controls

General Supply Notes

• Genomic DNA is available for this strain from the Mouse DNA Resource.

Control Information

	Control
	000690 129P3/J	(approximate)
Considerations for Choosing Controls
Control Pricing Information for Genetically Engineered Mutant Strains.

Payment Terms and Conditions

Terms are granted by individual review and stated on the customer invoice(s) and account statement. These transactions are payable in U.S. currency within the granted terms. Payment for services, products, shipping containers, and shipping costs that are rendered are expected within the payment terms indicated on the invoice or stated by contract. Invoices and account balances in arrears of stated terms may result in The Jackson Laboratory pursuing collection activities including but not limited to outside agencies and court filings.

See Terms of Use tab for General Terms and Conditions

The Jackson Laboratory's Genotype Promise

The Jackson Laboratory has rigorous genetic quality control and mutant gene genotyping programs to ensure the genetic background of JAX^® Mice strains as well as the genotypes of strains with identified molecular mutations. JAX^® Mice strains are only made available to researchers after meeting our standards. However, the phenotype of each strain may not be fully characterized and/or captured in the strain data sheets. Therefore, we cannot guarantee a strain's phenotype will meet all expectations. To ensure that JAX^® Mice will meet the needs of individual research projects or when requesting a strain that is new to your research, we suggest ordering and performing tests on a small number of mice to determine suitability for your particular project.

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