No significant dopaminergic loss is observed in 20 or 60-day old flies expressing Hsap\LRRK2^{G2385R.Scer\UAS.T:Hsap\MYC} under the control of Scer\GAL4^Ddc.PU.

Scer\GAL4^elav.PU-mediated expression of Hsap\LRRK2^{G2385R.Scer\UAS.T:Hsap\MYC} does not appear to compromise the overall anatomical integrity of the fly brain up to 60 d after eclosion. Scanning electron microscope analysis reveals no apparent eye abnormalities in flies expressing Hsap\LRRK2^{G2385R.Scer\UAS.T:Hsap\MYC} under the control of Scer\GAL4^GMR.PU at 20 d after eclosion. Similar observations are made when these flies are aged to 60 d. In 60 day old, but not 1 or 20 day old, flies expressing Hsap\LRRK2^{G2385R.Scer\UAS.T:Hsap\MYC} via Scer\GAL4^Ddc.PL, there is significant degeneration of DA neurons in the PPM clusters 1 and 3 (but not PAL, PPM2, PPL1 or PPL2) compared with age-matched normal control flies. Flies expressing Hsap\LRRK2^{G2385R.Scer\UAS.T:Hsap\MYC} via Scer\GAL4^Ddc.PL record similar climbing scores as controls but exhibit a reduced lifespan. There is an accelerated loss of DA neurons in the PPM 2/3, PAL and PPL1 clusters of rotenone-treated flies expressing Hsap\LRRK2^{G2385R.Scer\UAS.T:Hsap\MYC} via Scer\GAL4^Ddc.PL, compared to controls.