Cerebellum development

Mice were housed in a room with 12/12 hr light/dark controlled environment. Embryos were obtained from timed pregnant females at midnight of the day when a vaginal plug was detected; this was considered embryonic day 0 (E0). Pregnant females were cervically dislocated and embryos were harvested from the uterus. The cerebellum was isolated from each embryo, pooled with littermates of like genotype, and snap-frozen in liquid nitrogen. 3-4 replicate pools of 3-10 whole cerebella samples were collected from 12 time points across cerebellar development (embryonic days 11-18 at 24 hour intervals and every 72hrs until postnatal day 9)
Laser capture microdissection (LCM), a technique that can isolate specific cell types of interest from regions of tissue, was used to obtain pure populations of granule cells from early-stages of mouse cerebellar development. Fresh frozen brain tissue from mouse embryo (aged E13, 15 and 18) were collected and cyro-sectioned into 8 µm thick sections. The sections were then stained with cresyl violet for histological identification of the EGL. Veritas automated LCM system (Arcturus Veritus) was used to capture cells from external granular layer with infrared laser. Finally, the captured cells were lysed and RNA from pure granule cell population was extracted.

Bioanalyzer analysis was performed to check RNA quality. All RNA samples used for the time series achieved high RNA Integrity (RIN) Score. 34 out of 36 samples had RIN score of 9.7 or higher (10 being the best).
Figure 2: CAGE expression of marker genes in TPM.

References:
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[4] Goldowitz, D. and K. Hamre, The cells and molecules that make a cerebellum. Trends Neurosci, 1998. 21(9): p. 375-82.