Eggs from females expressing PlexA^GD14483 under the control of Scer\GAL4^NP1624 are rounder than from controls.

Follicle cell clones expressing PlexA^GD14483 under the control of Scer\GAL4^Act5C.PU show mostly normal basal protrusions.

Expression of PlexA^GD14483 under the control of Scer\GAL4^VGlut-OK371 results in defective walking pattern (uncoordinated walk with short steps and leg dragging) and impaired innervation of the leg muscles in proximal femur (failed defasciculation or insufficient elongation of axon branches) as well as distal tibia (increase in the number of branches that exit the main nerve). Similarly, expression under the Scer\GAL4^{VGlut.VGN6341} driver results in axon mis-projection phenotypes in the leg muscles - lack of innervation of the muscles of the femur and excessive innervation of the muscles of the tibia, expression under Scer\GAL4^GMR60B11 also leads to lack of innervation in the femur.

Adults expressing PlexA^GD14483 under the control of the cardioblast-specific Scer\GAL4^tin.CΔ4 driver show significantly reduced survival on day 6 after a shift to 29[o]C compared to control flies.

Adults expressing PlexA^GD14483 under the control of Scer\GAL4^elav.PLu (in the presence of Dcr-2^Scer\UAS.cDa to increase the efficiency of RNAi) show significantly reduced avoidance of noxious temperature (46[o]C) compared to control flies.

PlexA^GD14483, Scer\GAL4^Act5C.PU is a suppressor | partially of follicle cell | somatic clone phenotype of Scer\GAL4^Act5C.PU, Sema5c^UAS.EGFP

PlexA^GD14483, Scer\GAL4^Act5C.PU is a suppressor | partially of actin-based cell projection | somatic clone | oogenesis phenotype of Scer\GAL4^Act5C.PU, Sema5c^UAS.EGFP