Backbone and side-chain chemical shift assignments of a cellular FLICE-inhibitory protein (c-FLIPS).

Zhi-Qiang BaiBin LiuXiaofang MaKaifeng Hu

Published in: Biomolecular NMR assignments (2020)

Cellular FLICE-inhibitory protein (c-FLIP), which is involved in regulating the apoptosis of the extrinsic cell death pathway contains two death effector domains (DED). There are several splicing variants including short-form (c-FLIPS) and long-form (c-FLIPL). The death-inducing signaling complex (DISC) initiates apoptosis and programmed necrosis, DISC assembly and activation are regulated by c-FLIP. Here we report the NMR chemical shift assignments of c-FLIPs, which pave the way for investigating the molecular basis of the anti-apoptotic function of c-FLIPS.

Keyphrases

cell death
cell cycle arrest
oxidative stress
endoplasmic reticulum stress
protein protein
magnetic resonance
high resolution
amino acid
binding protein
regulatory t cells
copy number
dendritic cells
small molecule
mass spectrometry
cell proliferation
dna methylation
signaling pathway
immune response