C57BL/6N-Syk^{tm1b(EUCOMM)Hmgu}/Ieg

Status	Available to order
EMMA ID	EM:09307
International strain name	C57BL/6N-Syk^{tm1b(EUCOMM)Hmgu}/Ieg
Alternative name	HEPD0722_4_A07
Strain type	Targeted Mutant Strains
Allele/Transgene symbol	Syk^{tm1b(EUCOMM)Hmgu}
Gene/Transgene symbol	Syk
Disclaimer	Please note that for EUCOMM and KOMP-CSD mice supplied to the scientific community by INFRAFRONTIER/EMMA: 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. 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. No check for determining the copy number of the targeting construct in ES cells obtained from EUCOMM/KOMP is done by INFRAFRONTIER/EMMA. The level of quality control before mice are released is to confirm the individual mouse genotype by short range PCR.

Provider	Helmholtz Zentrum Muenchen - German Research Center for Environmental Health (GmbH)
Provider affiliation	Institute of Experimental Genetics, Helmholtz Zentrum Muenchen - German Research Center for Environmental Health (GmbH)
Genetic information	This mouse line originates from EUCOMM ES clone HEPD0722_4_A07. For further details on the construction of this clone see the page at the IMPC portal. The critical exon(s) were flanked by loxP sites, and subsequent cre expression excised this critical sequence resulting in a knockout reporter allele (Gt(ROSA)26Sortm1(ACTB-cre,-EGFP)Ics (MGI:5285392)). Click here for more information on EUCOMM final vectors.
Phenotypic information	Potential phenotyping data in the IMPC portal
References	None available

Archiving centre	Helmholtz Zentrum Muenchen - German Research Center for Environmental Health (GmbH), Oberschleißheim, Germany
Animals used for archiving	heterozygous C57BL/6NTac

IMPC phenotypes (allele matching)

decreased exploration in new environment / IMPC
decreased lean body mass / IMPC
increased total body fat amount / IMPC
decreased grip strength / IMPC
preweaning lethality, complete penetrance / IMPC

IMPC phenotypes (gene matching)

preweaning lethality, complete penetrance / IMPC
decreased lean body mass / IMPC
decreased grip strength / IMPC
increased total body fat amount / IMPC
decreased exploration in new environment / IMPC

MGI phenotypes (gene matching)

increased neutrophil cell number / MGI
absent pre-B cells / MGI
decreased bone marrow cell number / MGI
abnormal foot pad morphology / MGI
abnormal lung morphology / MGI
abnormal blood vessel morphology / MGI
arrested B cell differentiation / MGI
decreased inflammatory response / MGI
abnormal lymphatic vessel morphology / MGI
hemorrhage / MGI
intracranial hemorrhage / MGI
intracerebral hemorrhage / MGI
abnormal B cell differentiation / MGI
hydrops fetalis / MGI
abnormal dendritic cell antigen presentation / MGI
abnormal B cell physiology / MGI
abnormal neutrophil physiology / MGI
impaired neutrophil phagocytosis / MGI
increased IgM level / MGI
glomerulonephritis / MGI
abnormal renal glomerular capsule morphology / MGI
increased anti-insulin autoantibody level / MGI
increased urine protein level / MGI
no phenotypic analysis / MGI
lymphatic vessel hyperplasia / MGI
dilated vasculature / MGI
abnormal brain vasculature morphology / MGI
decreased bone resorption / MGI
decreased B cell number / MGI
abnormal late pro-B cell / MGI
impaired granulocyte bactericidal activity / MGI
increased B cell proliferation / MGI
immune system phenotype / MGI
decreased circulating creatinine level / MGI
increased circulating glucose level / MGI
decreased blood urea nitrogen level / MGI
spinal hemorrhage / MGI
abnormal T cell number / MGI
abnormal NK cell differentiation / MGI
increased CD4-positive, alpha beta T cell number / MGI
increased CD8-positive, alpha-beta T cell number / MGI
decreased marginal zone B cell number / MGI
decreased transitional stage B cell number / MGI
decreased mature B cell number / MGI
abnormal osteoclast differentiation / MGI
decreased IgG1 level / MGI
decreased IgG2a level / MGI
decreased IgG2b level / MGI
increased tumor necrosis factor secretion / MGI
decreased tumor necrosis factor secretion / MGI
abnormal lymphangiogenesis / MGI
increased B cell apoptosis / MGI
decreased transitional stage T1 B cell number / MGI
decreased transitional stage T2 B cell number / MGI
decreased DN1 thymic pro-T cell number / MGI
increased DN3 thymocyte number / MGI
abnormal lymphatic vessel endothelium morphology / MGI
decreased lymphatic vessel endothelial cell number / MGI
enlarged lymphatic vessel / MGI
primary atelectasis / MGI
increased CD4-positive, alpha-beta memory T cell number / MGI
increased CD8-positive, alpha-beta memory T cell number / MGI
postnatal lethality, complete penetrance / MGI
neonatal lethality, incomplete penetrance / MGI
perinatal lethality, incomplete penetrance / MGI
abnormal renal glomerulus basement membrane morphology / MGI
expanded mesangial matrix / MGI
mesangial cell hyperplasia / MGI
chylous ascites / MGI

C57BL/6N-Syk^{tm1b(EUCOMM)Hmgu}/Ieg

Information from provider

Information from EMMA

Disease and phenotype information

Information on how we integrate external resources can be found here

Availabilities

Practical information

Other EMMA strains

C57BL/6N-Syktm1b(EUCOMM)Hmgu/Ieg

Information from provider

Information from EMMA

Disease and phenotype information

Information on how we integrate external resources can be found here

Availabilities

Practical information

Other EMMA strains

C57BL/6N-Syk^{tm1b(EUCOMM)Hmgu}/Ieg