Design and Synthesis of a Quenched Fluorogenic Peptide Substrate for Human Cytomegalovirus Proteinase

Artigo Revisado por pares

Design and Synthesis of a Quenched Fluorogenic Peptide Substrate for Human Cytomegalovirus Proteinase

1995; SAGE Publishing; Volume: 6; Issue: 4 Linguagem: Inglês

10.1177/095632029500600408

ISSN

2040-2066

Autores

B.K. Handa, Elizabeth Keech, Elizabeth A. Conway, Anne V. Broadhurst, Alison J. Ritchie,

Tópico(s)

Glycosylation and Glycoproteins Research

Resumo

A fluorogenic peptide substrate for HCMV proteinase was synthesized by solid-phase peptide synthesis. The amino acid sequence of this substrate is derived from the maturation cleavage site (M site) of the natural substrate, the assembly protein precursor. The minimum sequence for efficient cleavage requires at least seven residues (P 4 -P 3 ′). A systematic modification of the peptide substrate was carried out to identify positions suitable for the introduction of the fluorescent donor and the quencher acceptor groups.

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Design and Synthesis of a Quenched Fluorogenic Peptide Substrate for Human Cytomegalovirus Proteinase