Phenotypes Associated with This Genotype

Genotype
MGI:3695479

• Allelic Composition: Ephb2^tm2Paw/Ephb2^tm2Paw; Ephb3^tm1Kln/Ephb3^tm1Kln
• Genetic Background: involves: 129S1/Sv * 129X1/SvJ * CD-1

• ♀: phenotype observed in females
• ♂: phenotype observed in males
• N: normal phenotype

mortality/aging

premature death ( J:62565 )

• on a predominantly CD-1 background, only 18% of the expected double homozygotes survive to adulthood

behavior/neurological

circling ( J:62565 )

• on a predominantly CD-1 background (5 to 9 backcross generations), 91% of double homozygotes that survive to adulthood exhibit circling

nervous system

delayed axon extension ( J:62565 )

• at E13.5, double homozygotes show delayed outgrowth of efferent projections into both the ipsilateral and contralateral inner ears

abnormal axon guidance ( J:62565 )

• at E13.5, both ipsilateral and contralateral projections of inner ear efferent (IEE) axons are disoriented and exhibit a temporary difficulty in reaching their targets

• as a result, ectopic caudal extensions are formed at the midline of the hindbrain with a 1- to 2-day delay in arriving at the ear end organs

• at E14.5 or later, axon tracing of IEEs shows a fairly normal number of crossed and uncrossed fibers in mutant mice

abnormal sensory neuron innervation pattern ( J:62565 )

• at E13.5, double homozygotes display delayed growth of efferent projections into both the ipsilateral and contralateral inner ears

• at this stage, growth cones have not yet reached into the sensory epithelia of the semicircular canals and there is an aberrant pausity of axons destined for the saccule and utricle

• in contrast, growth of afferent projections into the inner ear are normal, with afferents reaching all sensory epithelia by E12.5

hearing/vestibular/ear

abnormal semicircular canal morphology ( J:62565 )

• all adult circling mutants display much thinner semicircular canals (SCCs), with a significantly reduced (5-fold) cross-sectional diameter, esp. in the anterior vertical SCC

small endolymphatic duct ( J:62565 )

• at P7, the endolymph-filled membranous ducts are severely reduced by 53-fold in accord with a collapsed lumen and deflated SCCs

abnormal endolymph physiology ( J:116671 )

• on a CD-1 background, reduced endolymph-filled lumens lead to a significant reduction in the flow of endolymph fluid through the semicircular canals

• [K⁺] is significantly reduced from a mean of 118 mM in wild-type mice to 29 mM in double homozygotes

abnormal vestibular endolymph physiology ( J:116671 )

• on a CD-1 background, transepithelial utricular potential (UP) of the vestibular endolymph is significantly reduced from a mean of 0.4 mV in wild-type mice to -14.0 mV in double homozygotes

abnormal vestibular endolymph ionic homeostasis ( J:116671 )

• on a CD-1 background, double homozygotes fail to properly regulate the ionic homeostasis of vestibular endolymph

• however, blood hematocrit, [K+], and osmolarity appear to be nomal

abnormal vestibular system physiology ( J:62565 )

• severe vestibular dysfunction is associated with a drastic reduction in the volume of endolymph fluid within the vestibular apparatus

digestive/alimentary system

cleft palate ( J:173636 )

• severe cleft palate in 41% of mice at E18.5

abnormal large intestine crypts of Lieberkuhn morphology ( J:115873 )

• about a 50% decrease in the number of proliferating cells is seen in the colon; however, no change in the number of apoptotic cells is seen and the number of proliferating cells in small intestinal crypts is similar to wild-type

abnormal Paneth cell morphology ( J:115873 )

• in the small intestine Paneth cells are displaced from the base of the crypts by proliferating cells while the number of proliferating cells in the normal progenitor niche (along the sides of the crypt) are reduced

ectopic Paneth cells ( J:157019 )

• differentiated Paneth cells are mispositioned and spread throughout the crypt-villus axis

abnormal digestive system physiology ( J:157019 )

• decrease in proliferation in colon crypts

endocrine/exocrine glands

abnormal large intestine crypts of Lieberkuhn morphology ( J:115873 )

• about a 50% decrease in the number of proliferating cells is seen in the colon; however, no change in the number of apoptotic cells is seen and the number of proliferating cells in small intestinal crypts is similar to wild-type

abnormal Paneth cell morphology ( J:115873 )

• in the small intestine Paneth cells are displaced from the base of the crypts by proliferating cells while the number of proliferating cells in the normal progenitor niche (along the sides of the crypt) are reduced

ectopic Paneth cells ( J:157019 )

• differentiated Paneth cells are mispositioned and spread throughout the crypt-villus axis

craniofacial

cleft palate ( J:173636 )

• severe cleft palate in 41% of mice at E18.5

cellular

delayed axon extension ( J:62565 )

• at E13.5, double homozygotes show delayed outgrowth of efferent projections into both the ipsilateral and contralateral inner ears

abnormal axon guidance ( J:62565 )

• at E13.5, both ipsilateral and contralateral projections of inner ear efferent (IEE) axons are disoriented and exhibit a temporary difficulty in reaching their targets

• as a result, ectopic caudal extensions are formed at the midline of the hindbrain with a 1- to 2-day delay in arriving at the ear end organs

• at E14.5 or later, axon tracing of IEEs shows a fairly normal number of crossed and uncrossed fibers in mutant mice

growth/size/body

cleft palate ( J:173636 )

• severe cleft palate in 41% of mice at E18.5