The toxicity of prion protein fragment PrP(106-126) is not mediated by membrane permeabilization as shown by a M112W substitution

Henriques, Sónia Troeira; Pattenden, Leonard Keith; Aguilar, Marie-Isabel; Castanho, Miguel A. R. B.

http://hdl.handle.net/10451/7239

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Autores

Henriques, Sónia Troeira

Pattenden, Leonard Keith

Aguilar, Marie-Isabel

Castanho, Miguel A. R. B.

Resumo(s)

Prion diseases result from a post-translational modification of the physiological prion protein (PrPC) into a scrapie isoform (PrPSc). The PrP(106-126) fragment is conserved among various abnormal variants and shows PrPSc pathogenic properties. It has been proposed that the PrP(106-126) fragment may exhibit its toxic effects through membrane pore formation. Our previous studies showed that PrP(106-126) does not interact with membranes under physiological conditions. In the present study, PrP(106-126) affinity for membranes was increased by modifying PrP(106-126) with a M112W substitution, and pore formation was further evaluated. However, while the peptide exhibited an increased local concentration in the membrane, this did not lead to the induction of membrane permeabilization, as verified by fluorescence methodologies and surface plasmon resonance. These results further support the idea that PrP(106-126) toxicity is not a consequence of peptide-membrane interaction and pore formation.

Descrição

URI

hhtp://dx.doi.org/10.1021/bi900009d
http://hdl.handle.net/10451/7239

Citação

Biochemistry 2009, 48, 4198–4208

Editora

American Chemical Society

Coleções

IMM - Artigos em Revistas Internacionais

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