C57BL/6N-Mir96tm2.2(IMPC)Wtsi/WtsiH

Status

Available to order

EMMA IDEM:14179
International strain nameC57BL/6N-Mir96tm2.2(IMPC)Wtsi/WtsiH
Alternative nameMir96+13G>A
Strain typeTargeted Mutant Strains : Point mutation
Allele/Transgene symbolMir96tm2.2(IMPC)Wtsi
Gene/Transgene symbolMir96
DisclaimerPlease note that for EUCOMM and KOMP-CSD mice supplied to the scientific community by INFRAFRONTIER/EMMA:
  1. We can not guarantee a null mutation for Knock-out first alleles (tm1a alleles, see http://www.mousephenotype.org/about-ikmc/targeting-strategies) as the critical exon has not been deleted.
  2. That the structure of the targeted mutation in the ES cells obtained from EUCOMM/KOMP to generate EUCOMM/KOMP mice is not verified by INFRAFRONTIER/EMMA. It is recommended that the recipient confirms the mutation structure.
  3. No check for determining the copy number of the targeting construct in ES cells obtained from EUCOMM/KOMP is done by INFRAFRONTIER/EMMA.
  4. The level of quality control before mice are released is to confirm the individual mouse genotype by short range PCR.

Information from provider

Provider Wellcome Trust Sanger Institute
Provider affiliationWellcome Trust Sanger Institute
Genetic informationThis mouse line originates from ES clone BEPD0019_D04. Point mutation: Mir96+13G to A (also known as Mir96-nt28G-A or Mir96Tm2.1Wtsi). This is a knock-in of a human single base change described in the MIR96 gene in family s403, where G has been changed to A at location 13 of the seed region of the microRNA Mir96. For further details on the construction of this clone see the page at the IMPC portal. Potential phenotyping data in the IMPC portal.
References
  • Pathological mechanisms and candidate therapeutic approaches in the hearing loss of mice carrying human MIR96 mutations.;Lewis Morag A, Lachgar-Ruiz Maria, Di Domenico Francesca, Duddy Graham, Chen Jing, Fernandez Sergio, Morin Matias, Williams Gareth, Moreno Pelayo Miguel Angel, Steel Karen P, ;2024;Genome medicine;16;121; 39434156

Information from EMMA

Archiving centreMary Lyon Centre at MRC Harwell, Oxford, United Kingdom

Disease and phenotype information

Orphanet associated rare diseases, based on orthologous gene matching

    • Autosomal dominant non-syndromic sensorineural deafness type DFNA / Orphanet_90635
IMPC phenotypes (allele matching)
  • increased leukocyte cell number / IMPC
  • abnormal gait / IMPC
  • stereotypic behavior / IMPC
  • trunk curl / IMPC
  • impaired righting response / IMPC
  • increased lean body mass / IMPC
  • abnormal auditory brainstem response / IMPC
  • absent pinna reflex / IMPC
IMPC phenotypes (gene matching)
  • abnormal startle reflex / IMPC
  • abnormal auditory brainstem response / IMPC
  • increased leukocyte cell number / IMPC
  • trunk curl / IMPC
  • decreased body length / IMPC
  • increased bone mineral content / IMPC
  • increased thermal nociceptive threshold / IMPC
  • abnormal gait / IMPC
  • impaired righting response / IMPC
  • abnormal behavior / IMPC
  • decreased body weight / IMPC
  • increased circulating iron level / IMPC
  • increased lean body mass / IMPC
  • decreased heart weight / IMPC
  • increased circulating amylase level / IMPC
  • decreased lean body mass / IMPC
  • abnormal bone mineralization / IMPC
  • stereotypic behavior / IMPC
  • increased total body fat amount / IMPC
  • decreased bone mineral density / IMPC
  • limb grasping / IMPC
  • abnormal cornea morphology / IMPC
  • absent pinna reflex / IMPC
MGI phenotypes (gene matching)
  • circling / MGI
  • abnormal gait / MGI
  • head bobbing / MGI
  • abnormal pinna reflex / MGI
  • deafness / MGI
  • no abnormal phenotype detected / MGI
  • cochlear hair cell degeneration / MGI
  • cochlear outer hair cell degeneration / MGI
  • decreased cochlear hair cell number / MGI
  • absent cochlear nerve compound action potential / MGI
  • decreased cochlear nerve compound action potential / MGI
  • fused vestibular hair cell stereocilia / MGI
  • abnormal cochlear hair cell stereociliary bundle morphology / MGI
  • impaired hearing / MGI
  • absent pinna reflex / MGI

Literature references

  • Pathological mechanisms and candidate therapeutic approaches in the hearing loss of mice carrying human MIR96 mutations.;Lewis Morag A, Lachgar-Ruiz Maria, Di Domenico Francesca, Duddy Graham, Chen Jing, Fernandez Sergio, Morin Matias, Williams Gareth, Moreno Pelayo Miguel Angel, Steel Karen P, ;2024;Genome medicine;16;121; 39434156

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 sperm. Delivered in 4 weeks (after paperwork in place). €1740*
  • Tissue - Types of tissue, service fee and delivery time available upon request

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).

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