Description

Strain Information

Former Names B6.FVB-Tg(CD46)2Olds/J    (Changed: 27-NOV-06 ) B6.FVB-Tg(MCP)2Olds/J    (Changed: 02-OCT-06 ) Type Congenic; Mutant Strain; Transgenic; Additional information on Genetically Engineered Mutant Mice. Species laboratory mouse   Donating Investigator Michael Oldstone,   The Scripps Research Institute

Description
These mice carry the YAC-CD46 transgene coding for the human CD46 protein (also known as MCP), which serves as the receptor for the human measles virus, group B adenoviruses, the human herpes simplex VI virus and Neisseria gonorrhoeae. The expression of this transgene is under the direction of the human CD46 promoter. Transgene expression is detected by in situ hybridization examination of whole animal sections, by Northern blot analysis of brain, spleen, lymph nodes, thymus, kidney, liver, gut and lung, and by FACS analysis of CD4⁺/CD8⁺ lymphocytes. Levels of transgenic protein on cell surfaces are similar to levels found in human cells. This line carries 10 to 12 copies of the transgene. Transgenic mice are susceptible to measles virus (MV) infection, expressing MV antigens and releasing infectious viral particles. The spread of the virus throughout the nervous system and the suppression of the immune system mimic the course of MV infection in humans. Transgenic mice infected with MV exhibit reduced numbers of macrophages, neutrophils and IFN-gamma producing T-cells, and are more susceptible to Listeria monocytogenes bacteria infection. Mice that are homozygous for the targeted mutation are viable and fertile. This mutant mouse strain may be useful in the study of pathogenesis and treatment of microbial infections by the various viruses that are able to utilize CD46/MCP as a receptor.

Development
The YAC-CD46 transgene (containing a full-length human CD46 gene (also called MCP)) was injected into FVB/N pronuclei. Founder animals (line 2) were bred to C57BL/6 mice. The strain has been backcrossed for 12 generations on the C57BL/6 background (October 2003).

Control Information

	Control
	Noncarrier
	000664 C57BL/6J
Considerations for Choosing Controls

Additional Web Information

Congenic Nomenclature
Genetic Quality Control Annual Report

Phenotype

Phenotype Information

View Mammalian Phenotype Terms

Mammalian Phenotype Terms

      assigned by genotype

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

Tg(CD46)2Gsv/0

        involves: C57BL/6 * FVB/N

• life span-post-weaning/aging
• premature death (MGI Ref ID J:109895)
  • 94% of transgenic mice (mortality of all transgenics is similar, regardless of background) die within 3 weeks of infection (regardless of background), but no non-transgenic littermates become ill
• immune system phenotype
• abnormal cell-mediated immunity (MGI Ref ID J:109895)
  • infected transgenic mice that were primed with LCMV virus 60-90 days earlier can not mount an MHC-restricted cytotoxic T lymphocyte response to LCMV-infected targets
• defective cytotoxic T cell cytolysis (MGI Ref ID J:109895)
  • cytotoxic T cells can only lyse LCMV-infected MHC class I but not class II targets
• abnormal chemokine physiology (MGI Ref ID J:109895)
  • CC chemokines (RANTES, MIP-alpha and -beta, and MCP-1) and CXC chemokines (IP-10 and TCA-3, or MIG) are detected in brains of infected mice but EOTXN, LTN and MIP-2 are not
• abnormal cytokine secretion (MGI Ref ID J:109895)
  • at 6 days postinfection, a 6-fold increase in Il-12 expression (RNA), an 11-fold increase in lymphotoxin-beta and a 17-fold increase in TNFalpha expression are detected in brains of transgenic mice
• abnormal humoral immune response (MGI Ref ID J:109895)
  • humoral immune response is suppressed in infected transgenic mice; no antibody response to sheep red blood cells is generated while transgenic mice inoculated with vehicle instead of MV generated a significant antibody response
• abnormal response to transplant (MGI Ref ID J:113644)
  • transplanted hearts expressing the transgene slow down initially upon human serum perfusion, but recover while non-transgenic hearts (8/8) cease beating entirely
• increased susceptibility to viral infection (MGI Ref ID J:109895)
  • multiple cell types from transgene-expressing mice, including transgenic mice on varios other mixed or congenic backgrounds can be infected with measles virus (MV); cells become infected, express virus antigens, and release infectious viral progeny when cocultivated with permissive Vero cells (African green monkey kidney epithelial) compared to wild-type mouse cells
  • neurons and lymphoid cells in the blood, spleen and lymph nodes express viral proteins and RNA upon injection of 10³ pfu; in spleen and lymph nodes, MV is expressed primarily in T cell-enriched areas whereas cells from non-transgenic mice don't express viral proteins
• cardiovascular system phenotype
• abnormal heart morphology (MGI Ref ID J:113644)
  • transgenic and normal hearts develop white discoloration upon slowing or cessation of heart beat after normal human serum perfusion, but transgenic hearts resume beating and normal coloration within 15 minutes
  • 7/10 transgenic hearts resume functioning after ~3-5 minutes and begin beating normally within 15 minutes
• decreased heart rate (MGI Ref ID J:113644)
  • heart rate of transgenic hearts perfused with normal human serum after transplantion slows down similar to normal hearts perfused with decomplemented human serum; all non transgenic hearts perfused with normal human serum slow down immediately, resulting in white discoloration and complete cessation of heart beat within 3-5 minutes
• nervous system phenotype
• abnormal neuron morphology (MGI Ref ID J:109895)
  • viral proteins and RNA are expressed in the CNS after inoculation; numerous MV nucleocapsids are present in neurons in optic tegmentum, cerebral cortex, hippocampus and cerebellum, moving into axons with normal and disorganized microtubules
• increased neuron apoptosis (MGI Ref ID J:109895)
  • MV-infected transgenic mice have 50 to 100-fold more apoptotic primary neurons than innoculated non-transgenic mice or transgenic mice that received a needle wound in the brain
• astrocytosis (MGI Ref ID J:109895)
  • generalized astrocytosis accompanies MV replication and spread, with infiltration of CD4+ and some CD8+ T cells into the brain parenchyma

View Research Applications

Research Applications

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

Research Tools
Immunology and Inflammation Research (genes regulating susceptibility to infectious disease and endotoxin)

Virology Research

Genes & Alleles

Gene & Allele Information

Allele Symbol		Tg(CD46)2Gsv
Allele Name		transgene insertion 2, Frank Grosveld
Allele Type		Transgenic (random, expressed)
Common Name(s)		MCP YAC; MCP-YAC line 2; MY II; Tg(CD46)2Olds; Tg(MCP)Olds2; YAC CD46 line 2; YAC-CD46;
Mutation Made By		Nikos Yannoutsos,   Innsbruck Medical University
Expressed Gene		CD46, CD46 molecule, complement regulatory protein, human
Promoter		CD46, CD46 molecule, complement regulatory protein, human
Molecular Note		The transgene comprises a partially intact, approximately 420-kb yeast artificial chromosome (YAC) from the Imperial Cancer Research Fund (ICRF, London, UK), designatied AM2: 6C10, that contains the complete human CD46/MCP gene including its 5' and 3' flanking regions. The genome of transgenic mice of line MY II contains 10-12 intact copies of CD46. The expected 4.5 - 4.8-kb transcript, as well as several smaller RNAs, are expressed at high levels in all tissues examined from transgenic mice. Immunohistochemistry likewise detects patterns of expression of human CD46 protein in transgenic mouse tissues similar to those in human tissues. FACS analysis detects CD46 on transgenic spleen cells at approximately 10-fold higher levels than on human splenocytes. [MGI Ref ID J:113644]

Genotyping

Genotyping Information

Genotyping Protocols

Tg(CD46)2Gsv, STD PCR, vers. 1

Helpful Links

Optimizing PCR Protocols

References

References

Selected Reference(s)

Oldstone MB; Lewicki H; Thomas D; Tishon A; Dales S; Patterson J; Manchester M; Homann D; Naniche D; Holz A. 1999. Measles virus infection in a transgenic model: virus-induced immunosuppression and central nervous system disease. Cell 98(5):629-40. [PubMed: 10490102]  [MGI Ref ID J:109895]

Yannoutsos N; Ijzermans JN; Harkes C; Bonthuis F; Zhou CY; White D; Marquet RL; Grosveld F. 1996. A membrane cofactor protein transgenic mouse model for the study of discordant xenograft rejection. Genes Cells 1(4):409-19. [PubMed: 9135084]  [MGI Ref ID J:113644]

Additional References

Tg(CD46)2Gsv related

Oldstone MB; Dales S; Tishon A; Lewicki H; Martin L. 2005. A role for dual viral hits in causation of subacute sclerosing panencephalitis. J Exp Med 202(9):1185-90. [PubMed: 16260490]  [MGI Ref ID J:118755]

Health & husbandry

Health & Colony Maintenance Information

Colony Maintenance

Breeding & Husbandry	This strain originated on an FVB/N background and was backcrossed for 12 generations on the C57BL/6 background (October 2003). The strain is maintained as a hemizygote. SPF conditions are recommended.

Purchasing information

Pricing, Supply Level & Notes, Controls, General Terms & Conditions

Pricing

Supply Details

Standard Supply

Repository-Cryopreserved. Must Be Recovered. Please refer to pricing and supply notes for further information.

Supply Notes

Cryorecovery - Standard. The recovery process begins when a signed agreement form is returned to the Customer Service Department after order placement. Although results vary by strain, at least two males and two females (two pairs) will be provided, typically within 15 weeks of our receipt of the signed agreement form. If the first recovery attempt is unsuccessful or only one pair is recovered, a second recovery will be done, extending the delivery time to approximately 25 weeks. At least one member of each pair will be of known genotype and will carry the mutation if it is a mutant strain. Please note that pairs may not reflect the mating scheme utilized by The Jackson Laboratory prior to cryopreservation of the strain. Mating schemes are sometimes modified for successful cryopreservation. Price represents a repository maintenance fee, which includes the cost of recovery of the strain from the cryopreservation resource and the periodic replacement of the frozen embryos used for recovery. Cryorecovery to establish a Dedicated Supply for greater quantities of mice. One to two pairs will be recovered to establish a Dedicated Supply of mice. Price by quotation. For more information on Dedicated Supply, please contact JAX® Services, Tel: 1-800-422-6423 or 1-207-288-5845. This strain is included in the Induced Mutant Resource Colony collection. Genomic DNA is available for this strain from the Mouse DNA Resource.

Control Information

	Control
	Noncarrier
	000664 C57BL/6J
Considerations for Choosing Controls
USA, Canada and Mexico - Control Pricing Information for Genetically Engineered Mutant Strains.
International - Control Pricing Information for Genetically Engineered Mutant Strains.

General Terms and Conditions

See Terms of Use

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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Ordering and Purchasing Information

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Contact Information
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Tel: 800.422.6423 or 207.288.5845
Fax: 207.288.6150
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Terms of Use

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General Terms and Conditions

For Licensing and Use Restrictions view the link(s) below:
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Contact information

General inquiries

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phone:	207-288-6470
fax:	207-288-6655

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“Each recipient institution, including its employees and other researchers under its control (RECIPIENT), of mice or services using mice from The Jackson Laboratory (TJL) agrees that such mice, descendants of those mice derived by inbreeding or crossbreeding, including unmodified derivatives of those mice or their descendants (“MICE”) shall not be: (i) used for any purpose other than the internal research of the RECIPIENT, (ii) sold or otherwise provided to any third party for any use, or (iii) provided to any agent or other third party to provide breeding or other services with respect to MICE. Acceptance of MICE from TJL shall be deemed agreement by RECIPIENT to these conditions, and departure from these conditions requires The Jackson Laboratory’s prior written authorization.”

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