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Fig. 4

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ZDB-IMAGE-190723-45
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Figures for Bremer et al., 2019
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Fig. 4

Mutation in phr is causative for the regeneration defect in phr mutants. ac Mauthner axon at 48 hpt distal and proximal to the transection site in stitched, low magnification images of a wild-type phr+/+ axon (a), a heterozygous phrtn207b/+ axon (b) and a compound heterozygous phrtn207b/tp03 axon (c). Transection sites marked by a yellow arrowhead; rostrally directed projections in the phrtn207b/tp03 compound heterozygote are marked by white arrows (C). Scale bar for ac : 30 µm. Quantification of the extent of caudally directed regrowth in number of segments regrown caudally (d) and quantification of regrowth direction at the transection site (e), showing normal extent and directionality of regrowth in phr+/+ and phrtn207b/+ but reduced extent and misdirected regrowth in compound heterozygous phrtn207b/tp03. This shows that the regeneration deficits observed in phr mutants are indeed caused by a mutation in phr. N = 48 phr+/+, n = 53 heterozygous phrtn207b/+ and n = 13 compound heterozygous phrtn207b/tp03 were analyzed in (d, e). P-values were determined using two-tailed Student’s t-test (d), or Fisher exact test (e)

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