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Phenotypes associated with this allele
Allele Symbol
Allele Name
Allele ID
Tg(Camk2a-Bdnf)A9Stl
transgene insertion A9, Susumu Tonegawa
MGI:3709467
Summary 2 genotypes
Jump to Allelic Composition Genetic Background Genotype ID
tg1
Tg(Camk2a-Bdnf)A9Stl/0 C57BL/6-Tg(Camk2a-Bdnf)A9Stl/J MGI:5617753
tg2
Tg(Camk2a-Bdnf)A9Stl/0 involves: C57BL/6 * DBA/2 MGI:3709983


Genotype
MGI:5617753
tg1
Allelic
Composition
Tg(Camk2a-Bdnf)A9Stl/0
Genetic
Background
C57BL/6-Tg(Camk2a-Bdnf)A9Stl/J
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Tg(Camk2a-Bdnf)A9Stl mutation (1 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
behavior/neurological
• mice bury less marbles than wild-type mice
• however, mice show normal behavior in the social approach test and in the forced swim test
• mice spend more time in the open arms of the elevated plus-maze and make more entries to the open arms than wild-type mice
• mice exhibit spontaneous seizures after 5 months of age, with 3 of 12 mice showing seizures at 9 months of age
• seizure behavior includes head bobbing, forelimb and hindlimb clonus that progresses into running and jumping seizures followed by falling and the continuation of head bobbing and forelimb clonus
• seizures are similar to stage 5 limbic seizures

growth/size/body
• mice show decreased body weight that becomes more pronounced with age

nervous system
• mice exhibit spontaneous seizures after 5 months of age, with 3 of 12 mice showing seizures at 9 months of age
• seizure behavior includes head bobbing, forelimb and hindlimb clonus that progresses into running and jumping seizures followed by falling and the continuation of head bobbing and forelimb clonus
• seizures are similar to stage 5 limbic seizures

Mouse Models of Human Disease
DO ID OMIM ID(s) Ref(s)
NOT autism spectrum disorder DOID:0060041 J:216846
epilepsy DOID:1826 J:216846




Genotype
MGI:3709983
tg2
Allelic
Composition
Tg(Camk2a-Bdnf)A9Stl/0
Genetic
Background
involves: C57BL/6 * DBA/2
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Tg(Camk2a-Bdnf)A9Stl mutation (1 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
nervous system
N
• brain development at 4 weeks is grossly normal; cortex is of normal thickness, and lamination is intact with normal neuronal cell density in the visual cortex
• development of GABAergic neurons is accelerated in the primary visual cortex of transgenic mice between P12 and P35, relative to wild-type mice
• at P17, number of Parvalbumin-positive interneurons in the visual cortex is ~double the number found in wild-type brains
• these interneurons have larger soma sizes and more extensive neurite arborizations than in wild-type at P17
• at 5 weeks, BDNF mRNA levels in neocortex of transgenic mice are ~3-fold higher than in wild-type littermates
• ocular dominance (OD) plasticity ends prematurely in transgenic mice relative to wild-type; the OD shift induced by 4-day monocular deprivation (MD) is blocked when done at P28, near the peak of OD shift in wild-type
• shifts in the contralateral/ipsilateral visual-evoked potential (C/I VEP) ratios are larger in transgenics when MD is done with a difference of ~1 week compared to wild-type
• in layer III pyramidal neurons in hippoccampal slices, amplitude of the maximal IPSC (462 pA) is consistently large than in wild-type (279 pA)
• stimulus intensity required to recruit a saturating IPSC is similar in wild-type and transgenic brain slices
• EPSC amplitudes and whole-cell capacitances are similar between transgenic and wild-type mice
• theta burst stimulation (TBS) at the white matter-layer IV border (WM->III) induces little LTP in transgenic mice (101%), compared to the robust LTP induced in wild-type mice (122%)
• WM->III LTP undergoes a sharp decline between 3 and 4 weeks postnatal, which is 1 week earlier than observed in wild-type littermates (between 4 and 5 weeks of age)
• when inhibition is induced in cortical slices from transgenic mice with picrotoxin application, WM->III LTP can be supported by mice at P23-P25

vision/eye
• visual acuity is accelerated in transgenic mice relative to wild-type; visual acuity reaches adult levels by P24-25, a week sooner than in wild-type

cellular
• development of GABAergic neurons is accelerated in the primary visual cortex of transgenic mice between P12 and P35, relative to wild-type mice





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last database update
12/10/2024
MGI 6.24
The Jackson Laboratory