| Literature DB >> 21359116 |
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Year: 2011 PMID: 21359116 PMCID: PMC3043604 DOI: 10.1038/cddis.2010.94
Source DB: PubMed Journal: Cell Death Dis Impact factor: 8.469
Figure 1Nec-1 inhibited RIP1 mediated necroptosis in striatal cell model of HD in vitro. (a) Addition of zVAD-fmk (20 μM) or IETD-fmk (40 μM) to ST14A 8plx cells resulted in cell death, which was inhibited by RIP1 inhibitor Nec-1 (20 μM). Photos were taken 36 h after treatment, Bar=50 μm; and (b) supernatant was collected for evaluating cell death by LDH assay. (c) Lysates from ST14A 8plx cells treated with zVAD-fmk/IETD-fmk/Nec-1 for 36 h were blotted by RIP1 antibodies. (d) Parental ST14A cells and ST14A 8plx cells were treated with 20 μM zVAD-fmk in the presence/absence of 20 μM Nec-1. Cell death was measured 36 h after treatment. (e) Mutant Htt expressing ST14A 8plx cells were treated with 20 μM zVAD-fmk in the presence/absence of serum. Cell death was measured 24 h after treatment. (f) Lysates from ST14A 8plx cells treated with 20 μM zVAD-fmk for 24 h were analyzed in western blot by antibodies against phospho- or total-ERK1/2. *P<0.05
Figure 2Nec-1 maintains the body weight and motor function in R6/2 mouse model of HD in vivo. Behavior and disease progression data were generated from the same cohort of mice. Motor performance of R6/2 mice was evaluated by recording the time that they remained on a rotarod tuning at 15 r.p.m. (a) and 5 r.p.m. (b). *P<0.05. Mice were treated with vehicle or Nec-1 by intracerebroventricular delivery using osmotic pump. (c) The age (in days) at disease onset and at death was tabulated for both Nec-1- and vehicle-treated animals; data were processed by student's t-test. (d) The body weight of the R6/2 mice was recorded on a weekly basis. For vehicle treated mice n=6 and for Nec-1 treated mice n=7. *P<0.05. (e) Cumulative probability of onset in Nec-1- and vehicle-treated R6/2 mice. P=0.023 by logrank test. (f) Cumulative probability of survival in Nec-1- and vehicle-treated R6/2 mice. P=0.079 by logrank test