The plasma protein binding proteome of ertapenem: a novel compound-centric proteomic approach for elucidating drug-plasma protein binding interactions

Baker, Mark A.; Schneider, Elena K.; Huang, Johnny X.; Cooper, Matthew A.; Li, Jian; Velkov, Tony

Title: The plasma protein binding proteome of ertapenem: a novel compound-centric proteomic approach for elucidating drug-plasma protein binding interactions
Creator: Baker, Mark A.; Schneider, Elena K.; Huang, Johnny X.; Cooper, Matthew A.; Li, Jian; Velkov, Tony
Relation: NHMRC.1064896
Relation: ACS Chemical Biology Vol. 11, Issue 12, p. 3353-3364
Publisher Link: http://dx.doi.org/10.1021/acschembio.6b00700
Publisher: American Chemical Society
Resource Type: journal article
Date: 2016
Description: Ertapenem is an important first-line carbapenem antibiotic used for the treatment of aerobic Gram-negative bacterial infections. It is the only marketed carbapenem that is highly bound to plasma proteins and displays a concentration-dependent and saturable plasma protein binding profile. To date, the plasma components responsible for sequestering ertapenems antibacterial activity remain uncharacterized. In the present study, we have employed an orthogonal, multiplatform approach, including novel compound-centric displacement proteomics and surface plasmon resonance to characterize the plasma protein binding proteome of ertapenem. In proof-of-concept, the capacity of physiological cocktails of the identified plasma proteins to inhibit the antibacterial activity of ertapenem was assessed with in vitro microbiological assays. We show that fibrinogen, complement C4, haptoglobulin, α-1-antitrypsin, fibronectin, transferrin, immunoglobulin G, hemopexin, and humans serum albumin are responsible for the majority of the sequestering activity in plasma. No binding was observed to α-1-acid-glycoprotein. The findings of this study have broad reaching implications for antibiotic drug design and for dose tailoring to suit the plasma protein levels of individual patients in order to maximize the clinical efficacy of important first-line antibiotics such as ertapenem.
Subject: ertapenem; antibiotics; aerobic Gram-negative bacterial infections; carbapenem
Identifier: http://hdl.handle.net/1959.13/1334226
Identifier: uon:27252
Identifier: ISSN:1554-8929
Language: eng
Reviewed

Hits: 1780
Visitors: 1739
Downloads: 0

		Thumbnail	File	Description	Size	Format