Amyloid formation modulates the biological activity of a bacterial protein

Bieler, Sylvain; Estrada, Lisbell D.; Lagos Mónaco, Rosalba; Baeza Cancino, Marcelo; Castilla, Joaquín; Soto, Claudio

Artículo de revista

Fecha

2005-07-22

Registro en:

JOURNAL OF BIOLOGICAL CHEMISTRY 280 (29): 26880-26885 JUL 22 2005

0260-8774

https://repositorio.uchile.cl/handle/2250/118603

Autor

Bieler, Sylvain

Estrada, Lisbell D.

Lagos Mónaco, Rosalba

Baeza Cancino, Marcelo

Castilla, Joaquín

Soto, Claudio

Institución

Universidad de Chile

Resumen

The aggregation of proteins into amyloid fibrils is the hallmark feature of a group of late-onset degenerative diseases including Alzheimer, Parkinson, and prion diseases. We report here that microcin E492, a peptide naturally produced by Klebsiella pneumoniae that kills bacteria by forming pores in the cytoplasmic membrane, assembles in vitro into amyloid-like fibrils. The fibrils have the same structural, morphological, tinctorial, and biochemical properties as the aggregates observed in the disease conditions. In addition, we found that amyloid formation also occurs in vivo where it is associated with a loss of toxicity of the protein. The finding that microcin E492 naturally exists both as functional toxic pores and as harmless fibrils suggests that protein aggregation into amyloid fibrils is an evolutionarily conserved property of proteins that can be successfully employed by bacteria to fulfill specific physiological needs.

Materias

CHANNEL-FORMING BACTERIOCIN

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