ISDA: 6M6O

Deposition Date 2020-03-16

Release Date 2021-03-17

Last Version Date 2024-05-15

Entry Detail

PDB ID:

6M6O

Keywords:

APOPTOSIS

Title:

NMR SOLUTION STRUCTURE OF A C-FLIPs

Biological Source:

Source Organism(s):

Homo sapiens (Taxon ID: 9606)

Expression System(s):

Escherichia coli

Method Details:

Experimental Method:

SOLUTION NMR

Conformers Calculated:

120

Conformers Submitted:

Selection Criteria:

structures with the lowest energy

Download Validation Report

Macromolecular Entities

Structures with similar UniProt ID

Protein Blast

Polymer Type:polypeptide(L)
Molecule:CASP8 and FADD-like apoptosis
Gene (Uniprot):CFLAR
Mutagens:F114G
Chain IDs:A
Chain Length:185
Number of Molecules:1
Biological Source:Homo sapiens

UniProt ID:O15519 Pfam ID:PF01335

Ligand Molecules

Primary Citation

Solution structure of c-FLIP death effector domains.

Bai, Z.Q, Ma, X, Liu, B, Huang, T, Hu, K.Show

Biochem.Biophys.Res.Commun. 617 1 6 (2022)

PMID: 35688044 DOI: 10.1016/j.bbrc.2022.05.086

Abstact

The formation of death-inducing signaling complex (DISC) and death effector domain (DED) filament initiates extrinsic apoptosis. Recruitment and activation of procaspase-8 at the DISC are regulated by c-FLIP. The interaction between c-FLIP and procaspase-8 is mediated by their tandem DEDs (tDED). However, the structure of c-FLIPtDED and how c-FLIP interferes with procaspase-8 activation at the DISC remain elusive. Here, we solved the monomeric structure of c-FLIPtDED (F114G) at near physiological pH by solution nuclear magnetic resonance (NMR). Structural superimposition reveals c-FLIPtDED (F114G) adopts a structural topology similar to that of procaspase-8tDED. Our results provide a structural basis for understanding how c-FLIP interacts with procaspase-8 and the molecular mechanisms of c-FLIP in regulating cell death.

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Protein

Chemical

Disease

Primary Citation of related structures

Abstact

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